Your search keyword '"Pair 5"' showing total 139 results

1. Whole-Genome Sequencing Identifies Novel Functional Loci Associated with Lung Function in Puerto Rican Youth.

Author

Lee, Eunice Y, Mak, Angel CY, Hu, Donglei, Sajuthi, Satria, White, Marquitta J, Keys, Kevin L, Eckalbar, Walter, Bonser, Luke, Huntsman, Scott, Urbanek, Cydney, Eng, Celeste, Jain, Deepti, Abecasis, Gonçalo, Kang, Hyun M, Germer, Soren, Zody, Michael C, Nickerson, Deborah A, Erle, David, Ziv, Elad, Rodriguez-Santana, Jose, Seibold, Max A, and Burchard, Esteban G

Subjects

Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Genetics, Human Genome, Biotechnology, Pediatric, Asthma, Clinical Research, Lung, Respiratory, Adolescent, Black People, Bronchi, Case-Control Studies, Cell Line, Child, Chromatin Immunoprecipitation, Chromosome Mapping, Chromosomes, Human, Pair 1, Chromosomes, Human, Pair 5, Esophageal Mucosa, Female, Forced Expiratory Volume, Gene Expression, Humans, Indians, North American, Linkage Disequilibrium, Male, Membrane Proteins, Myocytes, Smooth Muscle, Nasal Mucosa, Polymorphism, Single Nucleotide, Puerto Rico, Quantitative Trait Loci, Sequence Analysis, RNA, White People, Whole Genome Sequencing, Young Adult, admixed, FEV1, RNA sequencing, inflammatory, TMEM9 airway epithelial cells, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences

Abstract

Rationale: Puerto Ricans have the highest childhood asthma prevalence in the United States (23.6%); however, the etiology is uncertain.Objectives: In this study, we sought to uncover the genetic architecture of lung function in Puerto Rican youth with and without asthma who were recruited from the island (n = 836).Methods: We used admixture-mapping and whole-genome sequencing data to discover genomic regions associated with lung function. Functional roles of the prioritized candidate SNPs were examined with chromatin immunoprecipitation sequencing, RNA sequencing, and expression quantitative trait loci data.Measurements and Main Results: We discovered a genomic region at 1q32 that was significantly associated with a 0.12-L decrease in the lung volume of exhaled air (95% confidence interval, -0.17 to -0.07; P = 6.62 × 10-8) with each allele of African ancestry. Within this region, two SNPs were expression quantitative trait loci of TMEM9 in nasal airway epithelial cells and MROH3P in esophagus mucosa. The minor alleles of these SNPs were associated with significantly decreased lung function and decreased TMEM9 gene expression. Another admixture-mapping peak was observed on chromosome 5q35.1, indicating that each Native American ancestry allele was associated with a 0.15-L increase in lung function (95% confidence interval, 0.08-0.21; P = 5.03 × 10-6). The region-based association tests identified four suggestive windows that harbored candidate rare variants associated with lung function.Conclusions: We identified common and rare genetic variants that may play a critical role in lung function among Puerto Rican youth. We independently validated an inflammatory pathway that could potentially be used to develop more targeted treatments and interventions for patients with asthma.

Published

2020

2. Lung Cancer Risk in Never-Smokers of European Descent is Associated With Genetic Variation in the 5p15.33 TERT-CLPTM1Ll Region

Author

Hung, Rayjean J, Spitz, Margaret R, Houlston, Richard S, Schwartz, Ann G, Field, John K, Ying, Jun, Li, Yafang, Han, Younghun, Ji, Xuemei, Chen, Wei, Wu, Xifeng, Gorlov, Ivan P, Na, Jie, de Andrade, Mariza, Liu, Geoffrey, Brhane, Yonathan, Diao, Nancy, Wenzlaff, Angela, Davies, Michael PA, Liloglou, Triantafillos, Timofeeva, Maria, Muley, Thomas, Rennert, Hedy, Saliba, Walid, Ryan, Bríd M, Bowman, Elise, Barros-Dios, Juan-Miguel, Pérez-Ríos, Mónica, Morgenstern, Hal, Zienolddiny, Shanbeh, Skaug, Vidar, Ugolini, Donatella, Bonassi, Stefano, van der Heijden, Erik HFM, Tardon, Adonina, Bojesen, Stig E, Landi, Maria Teresa, Johansson, Mattias, Bickeböller, Heike, Arnold, Susanne, Le Marchand, Loic, Melander, Olle, Andrew, Angeline, Grankvist, Kjell, Caporaso, Neil, Teare, M Dawn, Schabath, Matthew B, Aldrich, Melinda C, Kiemeney, Lambertus A, Wichmann, H-Erich, Lazarus, Philip, Mayordomo, Jose, Neri, Monica, Haugen, Aage, Zhang, Zuo-Feng, Ruano-Raviña, Alberto, Brenner, Hermann, Harris, Curtis C, Orlow, Irene, Rennert, Gadi, Risch, Angela, Brennan, Paul, Christiani, David C, Amos, Christopher I, Yang, Ping, and Gorlova, Olga Y

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Human Genome, Lung Cancer, Tobacco, Prevention, Cancer, Genetics, Clinical Research, Tobacco Smoke and Health, Lung, 2.1 Biological and endogenous factors, Aetiology, Good Health and Well Being, Case-Control Studies, Chromosomes, Human, Pair 5, Europe, Female, Genetic Predisposition to Disease, Genetic Variation, Genome-Wide Association Study, Genotyping Techniques, Humans, Lung Neoplasms, Membrane Proteins, Middle Aged, Polymorphism, Single Nucleotide, Risk Factors, Telomerase, Lung cancer, Never smokers, Genome-wide association study, Genetic susceptibility, Cardiorespiratory Medicine and Haematology, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

IntroductionInherited susceptibility to lung cancer risk in never-smokers is poorly understood. The major reason for this gap in knowledge is that this disease is relatively uncommon (except in Asians), making it difficult to assemble an adequate study sample. In this study we conducted a genome-wide association study on the largest, to date, set of European-descent never-smokers with lung cancer.MethodsWe conducted a two-phase (discovery and replication) genome-wide association study in never-smokers of European descent. We further augmented the sample by performing a meta-analysis with never-smokers from the recent OncoArray study, which resulted in a total of 3636 cases and 6295 controls. We also compare our findings with those in smokers with lung cancer.ResultsWe detected three genome-wide statistically significant single nucleotide polymorphisms rs31490 (odds ratio [OR]: 0.769, 95% confidence interval [CI]: 0.722-0.820; p value 5.31 × 10-16), rs380286 (OR: 0.770, 95% CI: 0.723-0.820; p value 4.32 × 10-16), and rs4975616 (OR: 0.778, 95% CI: 0.730-0.829; p value 1.04 × 10-14). All three mapped to Chromosome 5 CLPTM1L-TERT region, previously shown to be associated with lung cancer risk in smokers and in never-smoker Asian women, and risk of other cancers including breast, ovarian, colorectal, and prostate.ConclusionsWe found that genetic susceptibility to lung cancer in never-smokers is associated to genetic variants with pan-cancer risk effects. The comparison with smokers shows that top variants previously shown to be associated with lung cancer risk only confer risk in the presence of tobacco exposure, underscoring the importance of gene-environment interactions in the etiology of this disease.

Published

2019

3. Genome-wide meta-analysis of SNP-by9-ACEI/ARB and SNP-by-thiazide diuretic and effect on serum potassium in cohorts of European and African ancestry

Author

Irvin, Marguerite R, Sitlani, Colleen M, Noordam, Raymond, Avery, Christie L, Bis, Joshua C, Floyd, James S, Li, Jin, Limdi, Nita A, Srinivasasainagendra, Vinodh, Stewart, James, de Mutsert, Renée, Mook-Kanamori, Dennis O, Lipovich, Leonard, Kleinbrink, Erica L, Smith, Albert, Bartz, Traci M, Whitsel, Eric A, Uitterlinden, Andre G, Wiggins, Kerri L, Wilson, James G, Zhi, Degui, Stricker, Bruno H, Rotter, Jerome I, Arnett, Donna K, Psaty, Bruce M, and Lange, Leslie A

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Health Disparities, Human Genome, Genetics, Prevention, Minority Health, Black or African American, Aged, Antihypertensive Agents, Chromosomes, Human, Pair 5, Europe, Female, Genome-Wide Association Study, Genotype, Humans, Male, Middle Aged, Peptidyl-Dipeptidase A, Polymorphism, Single Nucleotide, Potassium, Sodium Chloride Symporter Inhibitors, White People, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences

Abstract

We evaluated interactions of SNP-by-ACE-I/ARB and SNP-by-TD on serum potassium (K+) among users of antihypertensive treatments (anti-HTN). Our study included seven European-ancestry (EA) (N = 4835) and four African-ancestry (AA) cohorts (N = 2016). We performed race-stratified, fixed-effect, inverse-variance-weighted meta-analyses of 2.5 million SNP-by-drug interaction estimates; race-combined meta-analysis; and trans-ethnic fine-mapping. Among EAs, we identified 11 significant SNPs (P

Published

2019

4. Genome-Wide Association Study to Find Modifiers for Tetralogy of Fallot in the 22q11.2 Deletion Syndrome Identifies Variants in the GPR98 Locus on 5q14.3

Author

Guo, Tingwei, Repetto, Gabriela M, McDonald McGinn, Donna M, Chung, Jonathan H, Nomaru, Hiroko, Campbell, Christopher L, Blonska, Anna, Bassett, Anne S, Chow, Eva WC, Mlynarski, Elisabeth E, Swillen, Ann, Vermeesch, Joris, Devriendt, Koen, Gothelf, Doron, Carmel, Miri, Michaelovsky, Elena, Schneider, Maude, Eliez, Stephan, Antonarakis, Stylianos E, Coleman, Karlene, Tomita-Mitchell, Aoy, Mitchell, Michael E, Digilio, M Cristina, Dallapiccola, Bruno, Marino, Bruno, Philip, Nicole, Busa, Tiffany, Kushan-Wells, Leila, Bearden, Carrie E, Piotrowicz, Małgorzata, Hawuła, Wanda, Roberts, Amy E, Tassone, Flora, Simon, Tony J, van Duin, Esther DA, van Amelsvoort, Thérèse A, Kates, Wendy R, Zackai, Elaine, Johnston, H Richard, Cutler, David J, Agopian, AJ, Goldmuntz, Elizabeth, Mitchell, Laura E, Wang, Tao, Emanuel, Beverly S, and Morrow, Bernice E

Subjects

Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Genetics, Rare Diseases, Congenital Structural Anomalies, Clinical Research, Human Genome, Heart Disease, Cardiovascular, Pediatric, 2.1 Biological and endogenous factors, Aetiology, Congenital, Chromatin, Chromosomes, Human, Pair 5, DiGeorge Syndrome, Genetic Loci, Genome-Wide Association Study, Genotype, High-Throughput Nucleotide Sequencing, Humans, Linkage Disequilibrium, MEF2 Transcription Factors, Oligonucleotide Array Sequence Analysis, Phenotype, Polymorphism, Single Nucleotide, Receptors, G-Protein-Coupled, Sequence Analysis, DNA, Tetralogy of Fallot, chromosomes, DiGeorge syndrome, genotype, ivelo-cardio-facial syndrome, tetralogy of Fallot, International 22q11.2 Consortium/Brain and Behavior Consortium*, Medical Biotechnology, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology

Abstract

The 22q11.2 deletion syndrome (22q11.2DS; DiGeorge syndrome/velocardiofacial syndrome) occurs in 1 of 4000 live births, and 60% to 70% of affected individuals have congenital heart disease, ranging from mild to severe. In our cohort of 1472 subjects with 22q11.2DS, a total of 62% (n=906) have congenital heart disease and 36% (n=326) of these have tetralogy of Fallot (TOF), comprising the largest subset of severe congenital heart disease in the cohort. To identify common genetic variants associated with TOF in individuals with 22q11.2DS, we performed a genome-wide association study using Affymetrix 6.0 array and imputed genotype data. In our cohort, TOF was significantly associated with a genotyped single-nucleotide polymorphism (rs12519770, P=2.98×10-8) in an intron of the adhesion GPR98 (G-protein-coupled receptor V1) gene on chromosome 5q14.3. There was also suggestive evidence of association between TOF and several additional single-nucleotide polymorphisms in this region. Some genome-wide significant loci in introns or noncoding regions could affect regulation of genes nearby or at a distance. On the basis of this possibility, we examined existing Hi-C chromatin conformation data to identify genes that might be under shared transcriptional regulation within the region on 5q14.3. There are 6 genes in a topologically associated domain of chromatin with GPR98, including MEF2C (Myocyte-specific enhancer factor 2C). MEF2C is the only gene that is known to affect heart development in mammals and might be of interest with respect to 22q11.2DS. In conclusion, common variants may contribute to TOF in 22q11.2DS and may function in cardiac outflow tract development.

Published

2017

5. Duplication events downstream of IRX1 cause North Carolina macular dystrophy at the MCDR3 locus.

Author

Cipriani, Valentina, Silva, Raquel S, Arno, Gavin, Pontikos, Nikolas, Kalhoro, Ambreen, Valeina, Sandra, Inashkina, Inna, Audere, Mareta, Rutka, Katrina, Puech, Bernard, Michaelides, Michel, van Heyningen, Veronica, Lace, Baiba, Webster, Andrew R, and Moore, Anthony T

Subjects

Retina, Chromosomes, Human, Pair 5, Chromosomes, Human, Pair 6, Fetus, Humans, Corneal Dystrophies, Hereditary, Homeodomain Proteins, Eye Proteins, Transcription Factors, Tomography, Optical Coherence, Sequence Analysis, DNA, Family, Gene Expression, Base Sequence, Haplotypes, Adult, Female, Male, Genetic Loci, Chromosome Duplication, ADAMTS Proteins, Chromosomes, Human, Pair 5, Pair 6, Corneal Dystrophies, Hereditary, Sequence Analysis, DNA, Tomography, Optical Coherence

Abstract

Autosomal dominant North Carolina macular dystrophy (NCMD) is believed to represent a failure of macular development. The disorder has been linked to two loci, MCDR1 (chromosome 6q16) and MCDR3 (chromosome 5p15-p13). Recently, non-coding variants upstream of PRDM13 (MCDR1) and a duplication including IRX1 (MCDR3) have been identified. However, the underlying disease-causing mechanism remains uncertain. Through a combination of sequencing studies on eighteen NCMD families, we report two novel overlapping duplications at the MCDR3 locus, in a gene desert downstream of IRX1 and upstream of ADAMTS16. One duplication of 43 kb was identified in nine families (with evidence for a shared ancestral haplotype), and another one of 45 kb was found in a single family. Three families carry the previously reported V2 variant (MCDR1), while five remain unsolved. The MCDR3 locus is thus refined to a shared region of 39 kb that contains DNAse hypersensitive sites active at a restricted time window during retinal development. Publicly available data confirmed expression of IRX1 and ADAMTS16 in human fetal retina, with IRX1 preferentially expressed in fetal macula. These findings represent a major advance in our understanding of the molecular genetics of NCMD and provide insights into the genetic pathways involved in human macular development.

Published

2017

6. Evidence that the 5p12 Variant rs10941679 Confers Susceptibility to Estrogen-Receptor-Positive Breast Cancer through FGF10 and MRPS30 Regulation

Author

Ghoussaini, Maya, French, Juliet D, Michailidou, Kyriaki, Nord, Silje, Beesley, Jonathan, Canisus, Sander, Hillman, Kristine M, Kaufmann, Susanne, Sivakumaran, Haran, Marjaneh, Moradi, Lee, Jason S, Dennis, Joe, Bolla, Manjeet K, Wang, Qin, Dicks, Ed, Milne, Roger L, Hopper, John L, Southey, Melissa C, Schmidt, Marjanka K, Broeks, Annegien, Muir, Kenneth, Lophatananon, Artitaya, Fasching, Peter A, Beckmann, Matthias W, Fletcher, Olivia, Johnson, Nichola, Sawyer, Elinor J, Tomlinson, Ian, Burwinkel, Barbara, Marme, Frederik, Guénel, Pascal, Truong, Thérèse, Bojesen, Stig E, Flyger, Henrik, Benitez, Javier, González-Neira, Anna, Alonso, M Rosario, Pita, Guillermo, Neuhausen, Susan L, Anton-Culver, Hoda, Brenner, Hermann, Arndt, Volker, Meindl, Alfons, Schmutzler, Rita K, Brauch, Hiltrud, Hamann, Ute, Tessier, Daniel C, Vincent, Daniel, Nevanlinna, Heli, Khan, Sofia, Matsuo, Keitaro, Ito, Hidemi, Dörk, Thilo, Bogdanova, Natalia V, Lindblom, Annika, Margolin, Sara, Mannermaa, Arto, Kosma, Veli-Matti, Investigators, kConFab AOCS, Wu, Anna H, Van Den Berg, David, Lambrechts, Diether, Floris, Giuseppe, Chang-Claude, Jenny, Rudolph, Anja, Radice, Paolo, Barile, Monica, Couch, Fergus J, Hallberg, Emily, Giles, Graham G, Haiman, Christopher A, Le Marchand, Loic, Goldberg, Mark S, Teo, Soo H, Yip, Cheng Har, Borresen-Dale, Anne-Lise, Collaborators, NBCS, Zheng, Wei, Cai, Qiuyin, Winqvist, Robert, Pylkäs, Katri, Andrulis, Irene L, Devilee, Peter, Tollenaar, Rob AEM, García-Closas, Montserrat, Figueroa, Jonine, Hall, Per, Czene, Kamila, Brand, Judith S, Darabi, Hatef, Eriksson, Mikael, Hooning, Maartje J, Koppert, Linetta B, Li, Jingmei, Shu, Xiao-Ou, Zheng, Ying, Cox, Angela, Cross, Simon S, Shah, Mitul, and Rhenius, Valerie

Subjects

Prevention, Genetics, Cancer, Breast Cancer, Human Genome, 2.1 Biological and endogenous factors, Aetiology, Alleles, Breast Neoplasms, Case-Control Studies, Cell Line, Tumor, Chromosomes, Human, Pair 5, Enhancer Elements, Genetic, Fibroblast Growth Factor 10, Genetic Predisposition to Disease, Haplotypes, Humans, Polymorphism, Single Nucleotide, Promoter Regions, Genetic, Quantitative Trait Loci, Receptor, Fibroblast Growth Factor, Type 2, Receptors, Estrogen, kConFab/AOCS Investigators, NBCS Collaborators, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Genome-wide association studies (GWASs) have revealed increased breast cancer risk associated with multiple genetic variants at 5p12. Here, we report the fine mapping of this locus using data from 104,660 subjects from 50 case-control studies in the Breast Cancer Association Consortium (BCAC). With data for 3,365 genotyped and imputed SNPs across a 1 Mb region (positions 44,394,495-45,364,167; NCBI build 37), we found evidence for at least three independent signals: the strongest signal, consisting of a single SNP rs10941679, was associated with risk of estrogen-receptor-positive (ER+) breast cancer (per-g allele OR ER+ = 1.15; 95% CI 1.13-1.18; p = 8.35 × 10-30). After adjustment for rs10941679, we detected signal 2, consisting of 38 SNPs more strongly associated with ER-negative (ER-) breast cancer (lead SNP rs6864776: per-a allele OR ER- = 1.10; 95% CI 1.05-1.14; p conditional = 1.44 × 10-12), and a single signal 3 SNP (rs200229088: per-t allele OR ER+ = 1.12; 95% CI 1.09-1.15; p conditional = 1.12 × 10-05). Expression quantitative trait locus analysis in normal breast tissues and breast tumors showed that the g (risk) allele of rs10941679 was associated with increased expression of FGF10 and MRPS30. Functional assays demonstrated that SNP rs10941679 maps to an enhancer element that physically interacts with the FGF10 and MRPS30 promoter regions in breast cancer cell lines. FGF10 is an oncogene that binds to FGFR2 and is overexpressed in ∼10% of human breast cancers, whereas MRPS30 plays a key role in apoptosis. These data suggest that the strongest signal of association at 5p12 is mediated through coordinated activation of FGF10 and MRPS30, two candidate genes for breast cancer pathogenesis.

Published

2016

7. Genome-wide association study confirms lung cancer susceptibility loci on chromosomes 5p15 and 15q25 in an African-American population

Author

Zanetti, Krista A, Wang, Zhaoming, Aldrich, Melinda, Amos, Christopher I, Blot, William J, Bowman, Elise D, Burdette, Laurie, Cai, Qiuyin, Caporaso, Neil, Chung, Charles C, Gillanders, Elizabeth M, Haiman, Christopher A, Hansen, Helen M, Henderson, Brian E, Kolonel, Laurence N, Le Marchand, Loic, Li, Shengchao, McNeill, Lorna Haughton, Ryan, Bríd M, Schwartz, Ann G, Sison, Jennette D, Spitz, Margaret R, Tucker, Margaret, Wenzlaff, Angela S, Wiencke, John K, Wilkens, Lynne, Wrensch, Margaret R, Wu, Xifeng, Zheng, Wei, Zhou, Weiyin, Christiani, David, Palmer, Julie R, Penning, Trevor M, Rieber, Alyssa G, Rosenberg, Lynn, Ruiz-Narvaez, Edward A, Su, Li, Vachani, Anil, Wei, Yongyue, Whitehead, Alexander S, Chanock, Stephen J, and Harris, Curtis C

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Lung, Women's Health, Human Genome, Clinical Research, Prevention, Genetics, Lung Cancer, 2.1 Biological and endogenous factors, Respiratory, Black or African American, Case-Control Studies, Chromosomes, Human, Pair 15, Chromosomes, Human, Pair 5, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Lung Neoplasms, Polymorphism, Single Nucleotide, Population Surveillance, Quantitative Trait Loci, Genome-wide association study, Lung neoplasms, Smoking, African Americans, Telomerase, Receptors, Cholinergic, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

ObjectivesGenome-wide association studies (GWAS) of lung cancer have identified regions of common genetic variation with lung cancer risk in Europeans who smoke and never-smoking Asian women. This study aimed to conduct a GWAS in African Americans, who have higher rates of lung cancer despite smoking fewer cigarettes per day when compared with Caucasians. This population provides a different genetic architecture based on underlying African ancestry allowing the identification of new regions and exploration of known regions for finer mapping.Materials and methodsWe genotyped 1,024,001 SNPs in 1737 cases and 3602 controls in stage 1, followed by a replication phase of 20 SNPs (p

Published

2016

8. Genome-wide Association Studies of Posttraumatic Stress Disorder in 2 Cohorts of US Army Soldiers

Author

Stein, Murray B, Chen, Chia-Yen, Ursano, Robert J, Cai, Tianxi, Gelernter, Joel, Heeringa, Steven G, Jain, Sonia, Jensen, Kevin P, Maihofer, Adam X, Mitchell, Colter, Nievergelt, Caroline M, Nock, Matthew K, Neale, Benjamin M, Polimanti, Renato, Ripke, Stephan, Sun, Xiaoying, Thomas, Michael L, Wang, Qian, Ware, Erin B, Borja, Susan, Kessler, Ronald C, and Smoller, Jordan W

Subjects

Mental Health, Clinical Research, Anxiety Disorders, Human Genome, Genetics, Post-Traumatic Stress Disorder (PTSD), Brain Disorders, 2.3 Psychological, social and economic factors, Aetiology, Inflammatory and immune system, Mental health, Good Health and Well Being, Adult, Carrier Proteins, Case-Control Studies, Chromosomes, Human, Pair 19, Chromosomes, Human, Pair 5, Cohort Studies, Female, Genetic Loci, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Male, Military Personnel, Polymorphism, Single Nucleotide, Stress Disorders, Post-Traumatic, Young Adult, Army Study to Assess Risk and Resilience in Servicemembers (STARRS) Collaborators, Other Medical and Health Sciences, Psychology, Cognitive Sciences

Abstract

ImportancePosttraumatic stress disorder (PTSD) is a prevalent, serious public health concern, particularly in the military. The identification of genetic risk factors for PTSD may provide important insights into the biological foundation of vulnerability and comorbidity.ObjectiveTo discover genetic loci associated with the lifetime risk for PTSD in 2 cohorts from the Army Study to Assess Risk and Resilience in Servicemembers (Army STARRS).Design, setting, and participantsTwo coordinated genome-wide association studies of mental health in the US military contributed participants. The New Soldier Study (NSS) included 3167 unique participants with PTSD and 4607 trauma-exposed control individuals; the Pre/Post Deployment Study (PPDS) included 947 unique participants with PTSD and 4969 trauma-exposed controls. The NSS data were collected from February 1, 2011, to November 30, 2012; the PDDS data, from January 9 to April 30, 2012. The primary analysis compared lifetime DSM-IV PTSD cases with trauma-exposed controls without lifetime PTSD. Data were analyzed from March 18 to December 27, 2015.Main outcomes and measuresAssociation analyses for PTSD used logistic regression models within each of 3 ancestral groups (European, African, and Latino American) by study, followed by meta-analysis. Heritability and genetic correlation and pleiotropy with other psychiatric and immune-related disorders were estimated.ResultsThe NSS population was 80.7% male (6277 of 7774 participants; mean [SD] age, 20.9 [3.3] years); the PPDS population, 94.4% male (5583 of 5916 participants; mean [SD] age, 26.5 [6.0] years). A genome-wide significant locus was found in ANKRD55 on chromosome 5 (rs159572; odds ratio [OR], 1.62; 95% CI, 1.37-1.92; P = 2.34 × 10-8) and persisted after adjustment for cumulative trauma exposure (adjusted OR, 1.64; 95% CI, 1.39-1.95; P = 1.18 × 10-8) in the African American samples from the NSS. A genome-wide significant locus was also found in or near ZNF626 on chromosome 19 (rs11085374; OR, 0.77; 95% CI, 0.70-0.85; P = 4.59 × 10-8) in the European American samples from the NSS. Similar results were not found for either single-nucleotide polymorphism in the corresponding ancestry group from the PPDS sample, in other ancestral groups, or in transancestral meta-analyses. Single-nucleotide polymorphism-based heritability was nonsignificant, and no significant genetic correlations were observed between PTSD and 6 mental disorders or 9 immune-related disorders. Significant evidence of pleiotropy was observed between PTSD and rheumatoid arthritis and, to a lesser extent, psoriasis.Conclusions and relevanceIn the largest genome-wide association study of PTSD to date, involving a US military sample, limited evidence of association for specific loci was found. Further efforts are needed to replicate the genome-wide significant association with ANKRD55-associated in prior research with several autoimmune and inflammatory disorders-and to clarify the nature of the genetic overlap observed between PTSD and rheumatoid arthritis and psoriasis.

Published

2016

9. Fine mapping of chromosome 5p15.33 based on a targeted deep sequencing and high density genotyping identifies novel lung cancer susceptibility loci

Author

Kachuri, Linda, Amos, Christopher I, McKay, James D, Johansson, Mattias, Vineis, Paolo, Bueno-de-Mesquita, H Bas, Boutron-Ruault, Marie-Christine, Johansson, Mikael, Quirós, J Ramón, Sieri, Sabina, Travis, Ruth C, Weiderpass, Elisabete, Le Marchand, Loic, Henderson, Brian E, Wilkens, Lynne, Goodman, Gary E, Chen, Chu, Doherty, Jennifer A, Christiani, David C, Wei, Yongyue, Su, Li, Tworoger, Shelley, Zhang, Xuehong, Kraft, Peter, Zaridze, David, Field, John K, Marcus, Michael W, Davies, Michael PA, Hyde, Russell, Caporaso, Neil E, Landi, Maria Teresa, Severi, Gianluca, Giles, Graham G, Liu, Geoffrey, McLaughlin, John R, Li, Yafang, Xiao, Xiangjun, Fehringer, Gord, Zong, Xuchen, Denroche, Robert E, Zuzarte, Philip C, McPherson, John D, Brennan, Paul, and Hung, Rayjean J

Subjects

Lung, Human Genome, Genetics, Cancer, Prevention, Lung Cancer, 2.1 Biological and endogenous factors, Aetiology, Case-Control Studies, Chromosome Mapping, Chromosomes, Human, Pair 5, Female, Genetic Loci, Genetic Predisposition to Disease, Genotyping Techniques, Humans, Lung Neoplasms, Male, Middle Aged, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Chromosome 5p15.33 has been identified as a lung cancer susceptibility locus, however the underlying causal mechanisms were not fully elucidated. Previous fine-mapping studies of this locus have relied on imputation or investigated a small number of known, common variants. This study represents a significant advance over previous research by investigating a large number of novel, rare variants, as well as their underlying mechanisms through telomere length. Variants for this fine-mapping study were identified through a targeted deep sequencing (average depth of coverage greater than 4000×) of 576 individuals. Subsequently, 4652 SNPs, including 1108 novel SNPs, were genotyped in 5164 cases and 5716 controls of European ancestry. After adjusting for known risk loci, rs2736100 and rs401681, we identified a new, independent lung cancer susceptibility variant in LPCAT1: rs139852726 (OR = 0.46, P = 4.73×10(-9)), and three new adenocarcinoma risk variants in TERT: rs61748181 (OR = 0.53, P = 2.64×10(-6)), rs112290073 (OR = 1.85, P = 1.27×10(-5)), rs138895564 (OR = 2.16, P = 2.06×10(-5); among young cases, OR = 3.77, P = 8.41×10(-4)). In addition, we found that rs139852726 (P = 1.44×10(-3)) was associated with telomere length in a sample of 922 healthy individuals. The gene-based SKAT-O analysis implicated TERT as the most relevant gene in the 5p15.33 region for adenocarcinoma (P = 7.84×10(-7)) and lung cancer (P = 2.37×10(-5)) risk. In this largest fine-mapping study to investigate a large number of rare and novel variants within 5p15.33, we identified novel lung and adenocarcinoma susceptibility loci with large effects and provided support for the role of telomere length as the potential underlying mechanism.

Published

2016

10. Candidate locus analysis of the TERT–CLPTM1L cancer risk region on chromosome 5p15 identifies multiple independent variants associated with endometrial cancer risk

Author

Carvajal-Carmona, Luis G, O’Mara, Tracy A, Painter, Jodie N, Lose, Felicity A, Dennis, Joe, Michailidou, Kyriaki, Tyrer, Jonathan P, Ahmed, Shahana, Ferguson, Kaltin, Healey, Catherine S, Pooley, Karen, Beesley, Jonathan, Cheng, Timothy, Jones, Angela, Howarth, Kimberley, Martin, Lynn, Gorman, Maggie, Hodgson, Shirley, National Study of Endometrial Cancer Genetics Group (NSECG), The Australian National Endometrial Cancer Study Group (ANECS), Wentzensen, Nicholas, Fasching, Peter A, Hein, Alexander, Beckmann, Matthias W, Renner, Stefan P, Dörk, Thilo, Hillemanns, Peter, Dürst, Matthias, Runnebaum, Ingo, Lambrechts, Diether, Coenegrachts, Lieve, Schrauwen, Stefanie, Amant, Frederic, Winterhoff, Boris, Dowdy, Sean C, Goode, Ellen L, Teoman, Attila, Salvesen, Helga B, Trovik, Jone, Njolstad, Tormund S, Werner, Henrica MJ, Scott, Rodney J, Ashton, Katie, Proietto, Tony, Otton, Geoffrey, Wersäll, Ofra, Mints, Miriam, Tham, Emma, RENDOCAS, Hall, Per, Czene, Kamila, Liu, Jianjun, Li, Jingmei, Hopper, John L, Southey, Melissa C, Australian Ovarian Cancer Study (AOCS), Ekici, Arif B, Ruebner, Matthias, Johnson, Nichola, Peto, Julian, Burwinkel, Barbara, Marme, Frederik, Brenner, Hermann, Dieffenbach, Aida K, Meindl, Alfons, Brauch, Hiltrud, The GENICA Network, Lindblom, Annika, Depreeuw, Jeroen, Moisse, Matthieu, Chang-Claude, Jenny, Rudolph, Anja, Couch, Fergus J, Olson, Janet E, Giles, Graham G, Bruinsma, Fiona, Cunningham, Julie M, Fridley, Brooke L, Børresen-Dale, Anne-Lise, Kristensen, Vessela N, Cox, Angela, Swerdlow, Anthony J, Orr, Nicholas, Bolla, Manjeet K, Wang, Qin, Weber, Rachel Palmieri, Chen, Zhihua, Shah, Mitul, Pharoah, Paul DP, Dunning, Alison M, Tomlinson, Ian, Easton, Douglas F, Spurdle, Amanda B, and Thompson, Deborah J

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Oncology and Carcinogenesis, Genetic Testing, Human Genome, Prevention, Cancer, Uterine Cancer, 2.1 Biological and endogenous factors, Aetiology, Chromosomes, Human, Pair 5, Databases, Nucleic Acid, Female, Gene Expression Regulation, Neoplastic, Genetic Loci, Haplotypes, Humans, Membrane Proteins, Models, Genetic, Neoplasm Proteins, Polymorphism, Single Nucleotide, Promoter Regions, Genetic, Risk Factors, Telomerase, National Study of Endometrial Cancer Genetics Group, Australian National Endometrial Cancer Study Group, RENDOCAS, Australian Ovarian Cancer Study, GENICA Network, Complementary and Alternative Medicine, Paediatrics and Reproductive Medicine, Genetics & Heredity, Reproductive medicine

Abstract

Several studies have reported associations between multiple cancer types and single-nucleotide polymorphisms (SNPs) on chromosome 5p15, which harbours TERT and CLPTM1L, but no such association has been reported with endometrial cancer. To evaluate the role of genetic variants at the TERT-CLPTM1L region in endometrial cancer risk, we carried out comprehensive fine-mapping analyses of genotyped and imputed SNPs using a custom Illumina iSelect array which includes dense SNP coverage of this region. We examined 396 SNPs (113 genotyped, 283 imputed) in 4,401 endometrial cancer cases and 28,758 controls. Single-SNP and forward/backward logistic regression models suggested evidence for three variants independently associated with endometrial cancer risk (P = 4.9 × 10(-6) to P = 7.7 × 10(-5)). Only one falls into a haplotype previously associated with other cancer types (rs7705526, in TERT intron 1), and this SNP has been shown to alter TERT promoter activity. One of the novel associations (rs13174814) maps to a second region in the TERT promoter and the other (rs62329728) is in the promoter region of CLPTM1L; neither are correlated with previously reported cancer-associated SNPs. Using TCGA RNASeq data, we found significantly increased expression of both TERT and CLPTM1L in endometrial cancer tissue compared with normal tissue (TERT P = 1.5 × 10(-18), CLPTM1L P = 1.5 × 10(-19)). Our study thus reports a novel endometrial cancer risk locus and expands the spectrum of cancer types associated with genetic variation at 5p15, further highlighting the importance of this region for cancer susceptibility.

Published

2015

11. Splice-site mutations identified in PDE6A responsible for retinitis pigmentosa in consanguineous Pakistani families.

Author

Khan, Shahid Y, Ali, Shahbaz, Naeem, Muhammad Asif, Khan, Shaheen N, Husnain, Tayyab, Butt, Nadeem H, Qazi, Zaheeruddin A, Akram, Javed, Riazuddin, Sheikh, Ayyagari, Radha, Hejtmancik, J Fielding, and Riazuddin, S Amer

Subjects

Biomedical and Clinical Sciences, Ophthalmology and Optometry, Rare Diseases, Clinical Research, Eye Disease and Disorders of Vision, Genetics, Human Genome, Aetiology, 2.1 Biological and endogenous factors, Adult, Chromosomes, Human, Pair 5, Consanguinity, Cyclic Nucleotide Phosphodiesterases, Type 6, DNA Mutational Analysis, Eye Proteins, Female, Genes, Recessive, Genetic Markers, Humans, Lod Score, Male, Middle Aged, Mutation, Pakistan, Pedigree, RNA Splice Sites, Retinitis Pigmentosa, Young Adult, Opthalmology and Optometry, Ophthalmology & Optometry, Ophthalmology and optometry

Abstract

PurposeThis study was conducted to localize and identify causal mutations associated with autosomal recessive retinitis pigmentosa (RP) in consanguineous familial cases of Pakistani origin.MethodsOphthalmic examinations that included funduscopy and electroretinography (ERG) were performed to confirm the affectation status. Blood samples were collected from all participating individuals, and genomic DNA was extracted. A genome-wide scan was performed, and two-point logarithm of odds (LOD) scores were calculated. Sanger sequencing was performed to identify the causative variants. Subsequently, we performed whole exome sequencing to rule out the possibility of a second causal variant within the linkage interval. Sequence conservation was performed with alignment analyses of PDE6A orthologs, and in silico splicing analysis was completed with Human Splicing Finder version 2.4.1.ResultsA large multigenerational consanguineous family diagnosed with early-onset RP was ascertained. An ophthalmic clinical examination consisting of fundus photography and electroretinography confirmed the diagnosis of RP. A genome-wide scan was performed, and suggestive two-point LOD scores were observed with markers on chromosome 5q. Haplotype analyses identified the region; however, the region did not segregate with the disease phenotype in the family. Subsequently, we performed a second genome-wide scan that excluded the entire genome except the chromosome 5q region harboring PDE6A. Next-generation whole exome sequencing identified a splice acceptor site mutation in intron 16: c.2028-1G>A, which was completely conserved in PDE6A orthologs and was absent in ethnically matched 350 control chromosomes, the 1000 Genomes database, and the NHLBI Exome Sequencing Project. Subsequently, we investigated our entire cohort of RP familial cases and identified a second family who harbored a splice acceptor site mutation in intron 10: c.1408-2A>G. In silico analysis suggested that these mutations will result in the elimination of wild-type splice acceptor sites that would result in either skipping of the respective exon or the creation of a new cryptic splice acceptor site; both possibilities would result in retinal photoreceptor cells that lack PDE6A wild-type protein.Conclusionswe report two splice acceptor site variations in PDE6A in consanguineous Pakistani families who manifested cardinal symptoms of RP. Taken together with our previously published work, our data suggest that mutations in PDE6A account for about 2% of the total genetic load of RP in our cohort and possibly in the Pakistani population as well.

Published

2015

12. Mutations in GRM6 identified in consanguineous Pakistani families with congenital stationary night blindness.

Author

Naeem, Muhammad Asif, Gottsch, Alexander DH, Ullah, Inayat, Khan, Shaheen N, Husnain, Tayyab, Butt, Nadeem H, Qazi, Zaheeruddin A, Akram, Javed, Riazuddin, Sheikh, Ayyagari, Radha, Hejtmancik, J Fielding, and Riazuddin, S Amer

Subjects

Biomedical and Clinical Sciences, Ophthalmology and Optometry, Clinical Research, Genetics, Aetiology, 2.1 Biological and endogenous factors, Adult, Aged, Amino Acid Sequence, Animals, Base Sequence, Chromosomes, Human, Pair 5, Consanguinity, Electroretinography, Exons, Eye Diseases, Hereditary, Female, Gene Expression, Genes, Recessive, Genetic Diseases, X-Linked, Homozygote, Humans, Male, Molecular Sequence Data, Mutation, Myopia, Night Blindness, Pakistan, Pedigree, Receptors, Glutamate, Sequence Alignment, Sequence Analysis, DNA, Opthalmology and Optometry, Ophthalmology & Optometry, Ophthalmology and optometry

Abstract

PurposeThis study was undertaken to investigate the causal mutations responsible for autosomal recessive congenital stationary night blindness (CSNB) in consanguineous Pakistani families.MethodsTwo consanguineous families with multiple individuals manifesting symptoms of stationary night blindness were recruited. Affected individuals underwent a detailed ophthalmological examination, including fundus examination and electroretinography. Blood samples were collected and genomic DNA was extracted. Exclusion analyses were completed by genotyping closely spaced microsatellite markers, and two-point logarithm of odds (LOD) scores were calculated. All coding exons, along with the exon-intron boundaries of GRM6, were sequenced bidirectionally.ResultsAccording to the medical history available to us, affected individuals in both families had experienced night blindness from the early years of their lives. Fundus photographs of affected individuals in both the families appeared normal, with no signs of attenuated arteries or bone spicule pigmentation. The scotopic electroretinogram (ERG) response were absent in all of the affected individuals, while the photopic measurements show reduced b-waves. During exclusion analyses, both families localized to a region on chromosome 5q that harbors GRM6, a gene previously associated with autosomal recessive CSNB. Bidirectional sequencing of GRM6 identified homozygous single base pair changes, specifically c.1336C>T (p.R446X) and c.2267G>A (p.G756D) in families PKRP170 and PKRP172, respectively.ConclusionsWe identified a novel nonsense and a previously reported missense mutation in GRM6 that were responsible for autosomal recessive CSNB in patients of Pakistani decent.

Published

2015

13. Fine-Scale Mapping of the 5q11.2 Breast Cancer Locus Reveals at Least Three Independent Risk Variants Regulating MAP3K1

Author

Glubb, Dylan M, Maranian, Mel J, Michailidou, Kyriaki, Pooley, Karen A, Meyer, Kerstin B, Kar, Siddhartha, Carlebur, Saskia, O’Reilly, Martin, Betts, Joshua A, Hillman, Kristine M, Kaufmann, Susanne, Beesley, Jonathan, Canisius, Sander, Hopper, John L, Southey, Melissa C, Tsimiklis, Helen, Apicella, Carmel, Schmidt, Marjanka K, Broeks, Annegien, Hogervorst, Frans B, van der Schoot, C Ellen, Muir, Kenneth, Lophatananon, Artitaya, Stewart-Brown, Sarah, Siriwanarangsan, Pornthep, Fasching, Peter A, Ruebner, Matthias, Ekici, Arif B, Beckmann, Matthias W, Peto, Julian, dos-Santos-Silva, Isabel, Fletcher, Olivia, Johnson, Nichola, Pharoah, Paul DP, Bolla, Manjeet K, Wang, Qin, Dennis, Joe, Sawyer, Elinor J, Tomlinson, Ian, Kerin, Michael J, Miller, Nicola, Burwinkel, Barbara, Marme, Frederik, Yang, Rongxi, Surowy, Harald, Guénel, Pascal, Truong, Thérèse, Menegaux, Florence, Sanchez, Marie, Bojesen, Stig E, Nordestgaard, Børge G, Nielsen, Sune F, Flyger, Henrik, González-Neira, Anna, Benitez, Javier, Zamora, M Pilar, Perez, Jose Ignacio Arias, Anton-Culver, Hoda, Neuhausen, Susan L, Brenner, Hermann, Dieffenbach, Aida Karina, Arndt, Volker, Stegmaier, Christa, Meindl, Alfons, Schmutzler, Rita K, Brauch, Hiltrud, Ko, Yon-Dschun, Brüning, Thomas, Network, The GENICA, Nevanlinna, Heli, Muranen, Taru A, Aittomäki, Kristiina, Blomqvist, Carl, Matsuo, Keitaro, Ito, Hidemi, Iwata, Hiroji, Tanaka, Hideo, Dörk, Thilo, Bogdanova, Natalia V, Helbig, Sonja, Lindblom, Annika, Margolin, Sara, Mannermaa, Arto, Kataja, Vesa, Kosma, Veli-Matti, Hartikainen, Jaana M, Investigators, kConFab, Wu, Anna H, Tseng, Chiu-chen, Van Den Berg, David, Stram, Daniel O, Lambrechts, Diether, Zhao, Hui, Weltens, Caroline, van Limbergen, Erik, Chang-Claude, Jenny, Flesch-Janys, Dieter, Rudolph, Anja, Seibold, Petra, and Radice, Paolo

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Oncology and Carcinogenesis, Human Genome, Prevention, Breast Cancer, Cancer, Estrogen, 2.1 Biological and endogenous factors, Aetiology, Alleles, Breast Neoplasms, Case-Control Studies, Cell Line, Tumor, Chromosome Mapping, Chromosomes, Human, Pair 5, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Genotyping Techniques, Humans, MAP Kinase Kinase Kinase 1, MCF-7 Cells, Polymorphism, Single Nucleotide, Promoter Regions, Genetic, Quantitative Trait Loci, Racial Groups, Risk Factors, GENICA Network, kConFab Investigators, Norwegian Breast Cancer Study, Medical and Health Sciences, Genetics & Heredity, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Genome-wide association studies (GWASs) have revealed SNP rs889312 on 5q11.2 to be associated with breast cancer risk in women of European ancestry. In an attempt to identify the biologically relevant variants, we analyzed 909 genetic variants across 5q11.2 in 103,991 breast cancer individuals and control individuals from 52 studies in the Breast Cancer Association Consortium. Multiple logistic regression analyses identified three independent risk signals: the strongest associations were with 15 correlated variants (iCHAV1), where the minor allele of the best candidate, rs62355902, associated with significantly increased risks of both estrogen-receptor-positive (ER(+): odds ratio [OR] = 1.24, 95% confidence interval [CI] = 1.21-1.27, ptrend = 5.7 × 10(-44)) and estrogen-receptor-negative (ER(-): OR = 1.10, 95% CI = 1.05-1.15, ptrend = 3.0 × 10(-4)) tumors. After adjustment for rs62355902, we found evidence of association of a further 173 variants (iCHAV2) containing three subsets with a range of effects (the strongest was rs113317823 [pcond = 1.61 × 10(-5)]) and five variants composing iCHAV3 (lead rs11949391; ER(+): OR = 0.90, 95% CI = 0.87-0.93, pcond = 1.4 × 10(-4)). Twenty-six percent of the prioritized candidate variants coincided with four putative regulatory elements that interact with the MAP3K1 promoter through chromatin looping and affect MAP3K1 promoter activity. Functional analysis indicated that the cancer risk alleles of four candidates (rs74345699 and rs62355900 [iCHAV1], rs16886397 [iCHAV2a], and rs17432750 [iCHAV3]) increased MAP3K1 transcriptional activity. Chromatin immunoprecipitation analysis revealed diminished GATA3 binding to the minor (cancer-protective) allele of rs17432750, indicating a mechanism for its action. We propose that the cancer risk alleles act to increase MAP3K1 expression in vivo and might promote breast cancer cell survival.

Published

2015

14. Imputation and subset-based association analysis across different cancer types identifies multiple independent risk loci in the TERT-CLPTM1L region on chromosome 5p15.33

Author

Wang, Zhaoming, Zhu, Bin, Zhang, Mingfeng, Parikh, Hemang, Jia, Jinping, Chung, Charles C, Sampson, Joshua N, Hoskins, Jason W, Hutchinson, Amy, Burdette, Laurie, Ibrahim, Abdisamad, Hautman, Christopher, Raj, Preethi S, Abnet, Christian C, Adjei, Andrew A, Ahlbom, Anders, Albanes, Demetrius, Allen, Naomi E, Ambrosone, Christine B, Aldrich, Melinda, Amiano, Pilar, Amos, Christopher, Andersson, Ulrika, Andriole, Gerald, Andrulis, Irene L, Arici, Cecilia, Arslan, Alan A, Austin, Melissa A, Baris, Dalsu, Barkauskas, Donald A, Bassig, Bryan A, Beane Freeman, Laura E, Berg, Christine D, Berndt, Sonja I, Bertazzi, Pier Alberto, Biritwum, Richard B, Black, Amanda, Blot, William, Boeing, Heiner, Boffetta, Paolo, Bolton, Kelly, Boutron-Ruault, Marie-Christine, Bracci, Paige M, Brennan, Paul, Brinton, Louise A, Brotzman, Michelle, Bueno-de-Mesquita, H Bas, Buring, Julie E, Butler, Mary Ann, Cai, Qiuyin, Cancel-Tassin, Geraldine, Canzian, Federico, Cao, Guangwen, Caporaso, Neil E, Carrato, Alfredo, Carreon, Tania, Carta, Angela, Chang, Gee-Chen, Chang, I-Shou, Chang-Claude, Jenny, Che, Xu, Chen, Chien-Jen, Chen, Chih-Yi, Chen, Chung-Hsing, Chen, Constance, Chen, Kuan-Yu, Chen, Yuh-Min, Chokkalingam, Anand P, Chu, Lisa W, Clavel-Chapelon, Francoise, Colditz, Graham A, Colt, Joanne S, Conti, David, Cook, Michael B, Cortessis, Victoria K, Crawford, E David, Cussenot, Olivier, Davis, Faith G, De Vivo, Immaculata, Deng, Xiang, Ding, Ti, Dinney, Colin P, Di Stefano, Anna Luisa, Diver, W Ryan, Duell, Eric J, Elena, Joanne W, Fan, Jin-Hu, Feigelson, Heather Spencer, Feychting, Maria, Figueroa, Jonine D, Flanagan, Adrienne M, Fraumeni, Joseph F, Freedman, Neal D, Fridley, Brooke L, Fuchs, Charles S, Gago-Dominguez, Manuela, Gallinger, Steven, Gao, Yu-Tang, Gapstur, Susan M, and Garcia-Closas, Montserrat

Subjects

Biological Sciences, Genetics, Cancer, Clinical Research, Human Genome, Prevention, Aetiology, 2.1 Biological and endogenous factors, Alleles, Chromosomes, Human, Pair 5, Computational Biology, DNA Methylation, Epigenesis, Genetic, Female, Gene Expression Regulation, Neoplastic, Gene Frequency, Genetic Loci, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Male, Membrane Proteins, Neoplasm Proteins, Neoplasms, Odds Ratio, Polymorphism, Single Nucleotide, Risk, Telomerase, Medical and Health Sciences, Genetics & Heredity

Abstract

Genome-wide association studies (GWAS) have mapped risk alleles for at least 10 distinct cancers to a small region of 63 000 bp on chromosome 5p15.33. This region harbors the TERT and CLPTM1L genes; the former encodes the catalytic subunit of telomerase reverse transcriptase and the latter may play a role in apoptosis. To investigate further the genetic architecture of common susceptibility alleles in this region, we conducted an agnostic subset-based meta-analysis (association analysis based on subsets) across six distinct cancers in 34 248 cases and 45 036 controls. Based on sequential conditional analysis, we identified as many as six independent risk loci marked by common single-nucleotide polymorphisms: five in the TERT gene (Region 1: rs7726159, P = 2.10 × 10(-39); Region 3: rs2853677, P = 3.30 × 10(-36) and PConditional = 2.36 × 10(-8); Region 4: rs2736098, P = 3.87 × 10(-12) and PConditional = 5.19 × 10(-6), Region 5: rs13172201, P = 0.041 and PConditional = 2.04 × 10(-6); and Region 6: rs10069690, P = 7.49 × 10(-15) and PConditional = 5.35 × 10(-7)) and one in the neighboring CLPTM1L gene (Region 2: rs451360; P = 1.90 × 10(-18) and PConditional = 7.06 × 10(-16)). Between three and five cancers mapped to each independent locus with both risk-enhancing and protective effects. Allele-specific effects on DNA methylation were seen for a subset of risk loci, indicating that methylation and subsequent effects on gene expression may contribute to the biology of risk variants on 5p15.33. Our results provide strong support for extensive pleiotropy across this region of 5p15.33, to an extent not previously observed in other cancer susceptibility loci.

Published

2014

15. Myeloid Malignancies with Chromosome 5q Deletions Acquire a Dependency on an Intrachromosomal NF-κB Gene Network

Author

Fang, Jing, Barker, Brenden, Bolanos, Lyndsey, Liu, Xiaona, Jerez, Andres, Makishima, Hideki, Christie, Susanne, Chen, Xiaoting, Rao, Dinesh S, Grimes, H Leighton, Komurov, Kakajan, Weirauch, Matthew T, Cancelas, Jose A, Maciejewski, Jaroslaw P, and Starczynowski, Daniel T

Subjects

Hematology, Pediatric Research Initiative, Pediatric Cancer, Childhood Leukemia, Genetics, Stem Cell Research, Pediatric, Cancer, Rare Diseases, Stem Cell Research - Nonembryonic - Non-Human, Adaptor Proteins, Signal Transducing, Animals, Apoptosis, Case-Control Studies, Cell Cycle, Cell Proliferation, Cells, Cultured, Chromosome Deletion, Chromosomes, Human, Pair 5, Gene Regulatory Networks, Humans, Leukemia, Myeloid, Acute, Mice, MicroRNAs, Myelodysplastic Syndromes, Myeloid Progenitor Cells, NF-kappa B, Sequestosome-1 Protein, Signal Transduction, TNF Receptor-Associated Factor 6, Biochemistry and Cell Biology, Medical Physiology

Abstract

Chromosome 5q deletions (del[5q]) are common in high-risk (HR) myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML); however, the gene regulatory networks that sustain these aggressive diseases are unknown. Reduced miR-146a expression in del(5q) HR MDS/AML and miR-146a(-/-) hematopoietic stem/progenitor cells (HSPCs) results in TRAF6/NF-κB activation. Increased survival and proliferation of HSPCs from miR-146a(low) HR MDS/AML is sustained by a neighboring haploid gene, SQSTM1 (p62), expressed from the intact 5q allele. Overexpression of p62 from the intact allele occurs through NF-κB-dependent feedforward signaling mediated by miR-146a deficiency. p62 is necessary for TRAF6-mediated NF-κB signaling, as disrupting the p62-TRAF6 signaling complex results in cell-cycle arrest and apoptosis of MDS/AML cells. Thus, del(5q) HR MDS/AML employs an intrachromosomal gene network involving loss of miR-146a and haploid overexpression of p62 via NF-κB to sustain TRAF6/NF-κB signaling for cell survival and proliferation. Interfering with the p62-TRAF6 signaling complex represents a therapeutic option in miR-146a-deficient and aggressive del(5q) MDS/AML.

Published

2014

16. Amelioration of the typical cognitive phenotype in a patient with the 5pter deletion associated with Cri‐du‐chat syndrome in addition to a partial duplication of CTNND2

Author

Sardina, Jennifer M, Walters, Allyson R, Singh, Kathryn E, Owen, Renius X, and Kimonis, Virginia E

Subjects

Intellectual and Developmental Disabilities (IDD), Pediatric, Mental Health, Genetics, Brain Disorders, Neurosciences, Catenins, Child, Chromosome Deletion, Chromosomes, Human, Pair 5, Comparative Genomic Hybridization, Cri-du-Chat Syndrome, Facies, Female, Gene Duplication, Humans, Phenotype, Delta Catenin, Cri-du-chat syndrome, 5p minus syndrome, 5p deletion syndrome, cognitive phenotype, intellectual disability, CTNND2 protein, human, catenin delta 2, catenin, delta 2, Chromosome 5, partial duplication, DNA microarrays, oligo-SNP microarrays, CTNND2 protein, human, catenin (cadherin-associated protein), delta 2, human, catenin delta 2, human, Clinical Sciences

Abstract

Cri-du-chat is a rare congenital syndrome characterized by intellectual disability, severe speech/developmental delay, dysmorphic features, and additional syndromic findings. The etiology of this disorder is well known, and is attributed to a large deletion on chromosome 5 that typically ranges from band 5p15.2 to the short arm terminus. This region contains CTNND2, a gene encoding a neuronal-specific protein, delta-catenin, which plays a critical role in cellular motility and brain function. The exact involvement of CTNND2 in the cognitive functionality of individuals with Cri-du-chat has not been fully deciphered, but it is thought to be significant. This report describes an 8-year-old African-American female with a complex chromosome 5 abnormality and a relatively mild case of cri-du-chat syndrome. Because of the surprisingly mild cognitive phenotype, although a karyotype had confirmed the 5p deletion at birth, an oligo-SNP microarray was obtained to further characterize her deletion. The array revealed a complex rearrangement, including a breakpoint in the middle of CTNND2, which resulted in a partial deletion and partial duplication of that gene. The array also verified the expected 5p terminal deletion. Although the patient has a significant deletion in CTNND2, half of the gene (including the promoter region) is not only preserved, but is duplicated. The patient's milder cognitive and behavioral presentation, in conjunction with her atypical 5p alteration, provides additional evidence for the role of CTNND2 in the cognitive phenotype of individuals with Cri-du-chat.

Published

2014

17. A Genome-Wide Association Study of Depressive Symptoms

Author

Hek, Karin, Demirkan, Ayse, Lahti, Jari, Terracciano, Antonio, Teumer, Alexander, Cornelis, Marilyn C, Amin, Najaf, Bakshis, Erin, Baumert, Jens, Ding, Jingzhong, Liu, Yongmei, Marciante, Kristin, Meirelles, Osorio, Nalls, Michael A, Sun, Yan V, Vogelzangs, Nicole, Yu, Lei, Bandinelli, Stefania, Benjamin, Emelia J, Bennett, David A, Boomsma, Dorret, Cannas, Alessandra, Coker, Laura H, de Geus, Eco, De Jager, Philip L, Diez-Roux, Ana V, Purcell, Shaun, Hu, Frank B, Rimm, Eric B, Hunter, David J, Jensen, Majken K, Curhan, Gary, Rice, Kenneth, Penman, Alan D, Rotter, Jerome I, Sotoodehnia, Nona, Emeny, Rebecca, Eriksson, Johan G, Evans, Denis A, Ferrucci, Luigi, Fornage, Myriam, Gudnason, Vilmundur, Hofman, Albert, Illig, Thomas, Kardia, Sharon, Kelly-Hayes, Margaret, Koenen, Karestan, Kraft, Peter, Kuningas, Maris, Massaro, Joseph M, Melzer, David, Mulas, Antonella, Mulder, Cornelis L, Murray, Anna, Oostra, Ben A, Palotie, Aarno, Penninx, Brenda, Petersmann, Astrid, Pilling, Luke C, Psaty, Bruce, Rawal, Rajesh, Reiman, Eric M, Schulz, Andrea, Shulman, Joshua M, Singleton, Andrew B, Smith, Albert V, Sutin, Angelina R, Uitterlinden, André G, Völzke, Henry, Widen, Elisabeth, Yaffe, Kristine, Zonderman, Alan B, Cucca, Francesco, Harris, Tamara, Ladwig, Karl-Heinz, Llewellyn, David J, Räikkönen, Katri, Tanaka, Toshiko, van Duijn, Cornelia M, Grabe, Hans J, Launer, Lenore J, Lunetta, Kathryn L, Mosley, Thomas H, Newman, Anne B, Tiemeier, Henning, and Murabito, Joanne

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Mental Illness, Clinical Research, Brain Disorders, Depression, Human Genome, Mental Health, 2.1 Biological and endogenous factors, Aged, Aged, 80 and over, Chromosomes, Human, Pair 5, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Center for Epidemiologic Studies Depression Scale, CHARGE consortium, depression, depressive symptoms, genetics, genome-wide association study, meta-analysis, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Biological sciences, Biomedical and clinical sciences, Psychology

Abstract

BackgroundDepression is a heritable trait that exists on a continuum of varying severity and duration. Yet, the search for genetic variants associated with depression has had few successes. We exploit the entire continuum of depression to find common variants for depressive symptoms.MethodsIn this genome-wide association study, we combined the results of 17 population-based studies assessing depressive symptoms with the Center for Epidemiological Studies Depression Scale. Replication of the independent top hits (p

Published

2013

18. Fine-mapping of the 5p15.33, 6p22.1-p21.31, and 15q25.1 Regions Identifies Functional and Histology-Specific Lung Cancer Susceptibility Loci in African-Americans

Author

Walsh, Kyle M, Gorlov, Ivan P, Hansen, Helen M, Wu, Xifeng, Spitz, Margaret R, Zhang, Huifeng, Lu, Emily Y, Wenzlaff, Angela S, Sison, Jennette D, Wei, Chongjuan, Lloyd, Stacy M, Chen, Wei, Frazier, Marsha L, Seldin, Michael F, Bierut, Laura J, Bracci, Paige M, Wrensch, Margaret R, Schwartz, Ann G, Wiencke, John K, and Amos, Christopher I

Subjects

Epidemiology, Biomedical and Clinical Sciences, Health Sciences, Oncology and Carcinogenesis, Clinical Research, Cancer, Lung, Genetics, Human Genome, Lung Cancer, Aetiology, 2.1 Biological and endogenous factors, Adenocarcinoma, Black or African American, Aged, Biomarkers, Tumor, Carcinoma, Squamous Cell, Case-Control Studies, Chromosome Mapping, Chromosomes, Human, Pair 15, Chromosomes, Human, Pair 5, Chromosomes, Human, Pair 6, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Linkage Disequilibrium, Lung Neoplasms, Male, Middle Aged, Nerve Tissue Proteins, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Prognosis, Proteins, Receptors, Nicotinic, Risk Factors, Small Cell Lung Carcinoma, Telomerase, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences

Abstract

BackgroundGenome-wide association studies of European and East Asian populations have identified lung cancer susceptibility loci on chromosomes 5p15.33, 6p22.1-p21.31, and 15q25.1. We investigated whether these regions contain lung cancer susceptibly loci in African-Americans and refined previous association signals by using the reduced linkage disequilibrium observed in African-Americans.Methods1,308 African-American cases and 1,241 African-American controls from 3 centers were genotyped for 760 single-nucleotide polymorphisms (SNP) spanning 3 regions, and additional SNP imputation was carried out. Associations between polymorphisms and lung cancer risk were estimated using logistic regression, stratified by tumor histology where appropriate.ResultsThe strongest associations were observed on 15q25.1 in/near CHRNA5, including a missense substitution [rs16969968: OR, 1.57; 95% confidence interval (CI), 1.25-1.97; P, 1.1 × 10(-4)) and variants in the 5'-UTR. Associations on 6p22.1-p21.31 were histology specific and included a missense variant in BAT2 associated with squamous cell carcinoma (rs2736158: OR, 0.64; 95% CI, 0.48-0.85; P, 1.82 × 10(-3)). Associations on 5p15.33 were detected near TERT, the strongest of which was rs2735940 (OR, 0.82; 95% CI, 0.73-0.93; P, 1.1 × 10(-3)). This association was stronger among cases with adenocarcinoma (OR, 0.75; 95% CI, 0.65-0.86; P, 8.1 × 10(-5)).ConclusionsPolymorphisms in 5p15.33, 6p22.1-p21.31, and 15q25.1 are associated with lung cancer in African-Americans. Variants on 5p15.33 are stronger risk factors for adenocarcinoma and variants on 6p21.33 associated only with squamous cell carcinoma.ImpactResults implicate the BAT2, TERT, and CHRNA5 genes in the pathogenesis of specific lung cancer histologies.

Published

2013

19. Thyroid cancer susceptibility polymorphisms: confirmation of loci on chromosomes 9q22 and 14q13, validation of a recessive 8q24 locus and failure to replicate a locus on 5q24

Author

Jones, Angela M, Howarth, Kimberley M, Martin, Lynn, Gorman, Maggie, Mihai, Radu, Moss, Laura, Auton, Adam, Lemon, Catherine, Mehanna, Hisham, Mohan, Hosahalli, Clarke, Susan EM, Wadsley, Jonathan, Macias, Elena, Coatesworth, Andrew, Beasley, Matthew, Roques, Tom, Martin, Craig, Ryan, Paul, Gerrard, Georgina, Power, Danielle, Bremmer, Caroline, Consortium, The TCUKIN, Tomlinson, Ian, and Carvajal-Carmona, Luis G

Subjects

Rare Diseases, Genetics, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Cancer, Chromosomes, Human, Pair 14, Chromosomes, Human, Pair 5, Chromosomes, Human, Pair 8, Chromosomes, Human, Pair 9, Genes, Recessive, Genetic Association Studies, Genetic Loci, Genetic Predisposition to Disease, Haplotypes, Humans, Linkage Disequilibrium, MicroRNAs, Polymorphism, Single Nucleotide, Sequence Analysis, DNA, Thyroid Neoplasms, TCUKIN Consortium, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Five single nucleotide polymorphisms (SNPs) associated with thyroid cancer (TC) risk have been reported: rs2910164 (5q24); rs6983267 (8q24); rs965513 and rs1867277 (9q22); and rs944289 (14q13). Most of these associations have not been replicated in independent populations and the combined effects of the SNPs on risk have not been examined. This study genotyped the five TC SNPs in 781 patients recruited through the TCUKIN study. Genotype data from 6122 controls were obtained from the CORGI and Wellcome Trust Case-Control Consortium studies. Significant associations were detected between TC and rs965513A (p=6.35×10(-34)), rs1867277A (p=5.90×10(-24)), rs944289T (p=6.95×10(-7)), and rs6983267G (p=0.016). rs6983267 was most strongly associated under a recessive model (P(GG vs GT + TT)=0.004), in contrast to the association of this SNP with other cancer types. However, no evidence was found of an association between rs2910164 and disease under any risk model (p>0.7). The rs1867277 association remained significant (p=0.008) after accounting for genotypes at the nearby rs965513 (p=2.3×10(-13)) and these SNPs did not tag a single high risk haplotype. The four validated TC SNPs accounted for a relatively large proportion (∼11%) of the sibling relative risk of TC, principally owing to the large effect size of rs965513 (OR 1.74).

Published

2012

20. Segment-wise genome-wide association analysis identifies a candidate region associated with schizophrenia in three independent samples.

Author

Gladwin, Thomas E, Derks, Eske M, Genetic Risk and Outcome of Psychosis (GROUP), Rietschel, Marcella, Mattheisen, Manuel, Breuer, René, Schulze, Thomas G, Nöthen, Markus M, Levinson, Douglas, Shi, Jianxin, Gejman, Pablo V, Cichon, Sven, and Ophoff, Roel A

Subjects

Genetic Risk and Outcome of Psychosis, Chromosomes, Human, Pair 5, Humans, Genetic Predisposition to Disease, Case-Control Studies, Chromosome Mapping, Schizophrenia, Genome-Wide Association Study, Chromosomes, Human, Pair 5, General Science & Technology

Abstract

Recent studies suggest that variation in complex disorders (e.g., schizophrenia) is explained by a large number of genetic variants with small effect size (Odds Ratio ≈ 1.05-1.1). The statistical power to detect these genetic variants in Genome Wide Association (GWA) studies with large numbers of cases and controls (v 15,000) is still low. As it will be difficult to further increase sample size, we decided to explore an alternative method for analyzing GWA data in a study of schizophrenia, dramatically reducing the number of statistical tests. The underlying hypothesis was that at least some of the genetic variants related to a common outcome are collocated in segments of chromosomes at a wider scale than single genes. Our approach was therefore to study the association between relatively large segments of DNA and disease status. An association test was performed for each SNP and the number of nominally significant tests in a segment was counted. We then performed a permutation-based binomial test to determine whether this region contained significantly more nominally significant SNPs than expected under the null hypothesis of no association, taking linkage into account. Genome Wide Association data of three independent schizophrenia case/control cohorts with European ancestry (Dutch, German, and US) using segments of DNA with variable length (2 to 32 Mbp) was analyzed. Using this approach we identified a region at chromosome 5q23.3-q31.3 (128-160 Mbp) that was significantly enriched with nominally associated SNPs in three independent case-control samples. We conclude that considering relatively wide segments of chromosomes may reveal reliable relationships between the genome and schizophrenia, suggesting novel methodological possibilities as well as raising theoretical questions.

Published

2012

21. Reversed clinical phenotype due to a microduplication of Sotos syndrome region detected by array CGH: Microcephaly, developmental delay and delayed bone age

Author

Zhang, Han, Lu, Xianglan, Beasley, Julie, Mulvihill, John J, Liu, Ruizhi, Li, Shibo, and Lee, Ji‐Yun

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Congenital Structural Anomalies, Rare Diseases, Intellectual and Developmental Disabilities (IDD), Pediatric, Brain Disorders, 2.1 Biological and endogenous factors, Aetiology, Chromosome Duplication, Chromosomes, Human, Pair 5, Comparative Genomic Hybridization, Gene Dosage, Histone Methyltransferases, Histone-Lysine N-Methyltransferase, Humans, In Situ Hybridization, Fluorescence, Infant, Intracellular Signaling Peptides and Proteins, Male, Nuclear Proteins, Phenotype, Sotos Syndrome, Biochemistry and Cell Biology, Mental Health, Adolescent, Adult, Animals, Caspases, Cell Death, Child, Child, Preschool, Chromosome Disorders, Down-Regulation, Drosophila melanogaster, Female, Gene Duplication, Leucine, Pedigree, Signal Transduction, TOR Serine-Threonine Kinases, Young Adult, Complementary and Alternative Medicine, Paediatrics and Reproductive Medicine, Genetics & Heredity, Reproductive medicine

Abstract

PurposeNuclear receptor binding SET domain protein 1, NSD1, encodes a histone methyltransferase H3K36. NSD1 is responsible for the phenotype of the reciprocal 5q35.2q35.3 microdeletion-microduplication syndromes. We expand the phenotype and demonstrate the functional role of NSD1 in microduplication 5q35 syndrome.MethodsThrough an international collaboration, we report nine new patients, contributing to the emerging phenotype, highlighting psychiatric phenotypes in older affected individuals. Focusing specifically on the undergrowth phenotype, we have modeled the effects of Mes-4/NSD overexpression in Drosophila melanogaster.ResultsThe individuals (including a family) from diverse backgrounds with duplications ranging in size from 0.6 to 4.5 Mb, have a consistent undergrowth phenotype. Mes-4 overexpression in the developing wing causes undergrowth, increased H3K36 methylation, and increased apoptosis. We demonstrate that altering the levels of insulin receptor (IR) rescues the apoptosis and the wing undergrowth phenotype, suggesting changes in mTOR pathway signaling. Leucine supplementation rescued Mes-4/NSD induced cell death, demonstrating decreased mTOR signaling caused by NSD1.ConclusionGiven that we show mTOR inhibition as a likely mechanism and amelioration of the phenotype by leucine supplementation in a fly model, we suggest further studies should evaluate the therapeutic potential of leucine or branched chain amino acids as an adjunct possible treatment to ameliorate human growth and psychiatric phenotypes and propose inclusion of 5q35-microduplication as part of the differential diagnosis for children and adults with delayed bone age, short stature, microcephaly, developmental delay, and psychiatric phenotypes.

Published

2011

22. A genome-wide association study identifies pancreatic cancer susceptibility loci on chromosomes 13q22.1, 1q32.1 and 5p15.33.

Author

Petersen, Gloria M, Amundadottir, Laufey, Fuchs, Charles S, Kraft, Peter, Stolzenberg-Solomon, Rachael Z, Jacobs, Kevin B, Arslan, Alan A, Bueno-de-Mesquita, H Bas, Gallinger, Steven, Gross, Myron, Helzlsouer, Kathy, Holly, Elizabeth A, Jacobs, Eric J, Klein, Alison P, LaCroix, Andrea, Li, Donghui, Mandelson, Margaret T, Olson, Sara H, Risch, Harvey A, Zheng, Wei, Albanes, Demetrius, Bamlet, William R, Berg, Christine D, Boutron-Ruault, Marie-Christine, Buring, Julie E, Bracci, Paige M, Canzian, Federico, Clipp, Sandra, Cotterchio, Michelle, de Andrade, Mariza, Duell, Eric J, Gaziano, J Michael, Giovannucci, Edward L, Goggins, Michael, Hallmans, Göran, Hankinson, Susan E, Hassan, Manal, Howard, Barbara, Hunter, David J, Hutchinson, Amy, Jenab, Mazda, Kaaks, Rudolf, Kooperberg, Charles, Krogh, Vittorio, Kurtz, Robert C, Lynch, Shannon M, McWilliams, Robert R, Mendelsohn, Julie B, Michaud, Dominique S, Parikh, Hemang, Patel, Alpa V, Peeters, Petra HM, Rajkovic, Aleksandar, Riboli, Elio, Rodriguez, Laudina, Seminara, Daniela, Shu, Xiao-Ou, Thomas, Gilles, Tjønneland, Anne, Tobias, Geoffrey S, Trichopoulos, Dimitrios, Van Den Eeden, Stephen K, Virtamo, Jarmo, Wactawski-Wende, Jean, Wang, Zhaoming, Wolpin, Brian M, Yu, Herbert, Yu, Kai, Zeleniuch-Jacquotte, Anne, Fraumeni, Joseph F, Hoover, Robert N, Hartge, Patricia, and Chanock, Stephen J

Subjects

Chromosomes, Human, Pair 1, Chromosomes, Human, Pair 5, Chromosomes, Human, Pair 13, Humans, Carcinoma, Pancreatic Neoplasms, Genetic Predisposition to Disease, Case-Control Studies, Cohort Studies, Linkage Disequilibrium, Polymorphism, Single Nucleotide, Genome-Wide Association Study, Genetic Loci, Rare Diseases, Cancer, Genetics, Clinical Research, Pancreatic Cancer, Digestive Diseases, Human Genome, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

We conducted a genome-wide association study of pancreatic cancer in 3,851 affected individuals (cases) and 3,934 unaffected controls drawn from 12 prospective cohort studies and 8 case-control studies. Based on a logistic regression model for genotype trend effect that was adjusted for study, age, sex, self-described ancestry and five principal components, we identified eight SNPs that map to three loci on chromosomes 13q22.1, 1q32.1 and 5p15.33. Two correlated SNPs, rs9543325 (P = 3.27 x 10(-11), per-allele odds ratio (OR) 1.26, 95% CI 1.18-1.35) and rs9564966 (P = 5.86 x 10(-8), per-allele OR 1.21, 95% CI 1.13-1.30), map to a nongenic region on chromosome 13q22.1. Five SNPs on 1q32.1 map to NR5A2, and the strongest signal was at rs3790844 (P = 2.45 x 10(-10), per-allele OR 0.77, 95% CI 0.71-0.84). A single SNP, rs401681 (P = 3.66 x 10(-7), per-allele OR 1.19, 95% CI 1.11-1.27), maps to the CLPTM1L-TERT locus on 5p15.33, which is associated with multiple cancers. Our study has identified common susceptibility loci for pancreatic cancer that warrant follow-up studies.

Published

2010

23. A genome-wide linkage and association scan reveals novel loci for autism.

Author

Weiss, Lauren A, Arking, Dan E, Gene Discovery Project of Johns Hopkins & the Autism Consortium, Daly, Mark J, and Chakravarti, Aravinda

Subjects

Gene Discovery Project of Johns Hopkins & the Autism Consortium, Brain, Chromosomes, Human, Pair 5, Humans, Genetic Predisposition to Disease, Semaphorins, Membrane Proteins, Nerve Tissue Proteins, Sample Size, Chromosome Mapping, Autistic Disorder, Polymorphism, Single Nucleotide, Internationality, Genome-Wide Association Study, Genetic Linkage, Human Genome, Intellectual and Developmental Disabilities (IDD), Mental Health, Pediatric, Clinical Research, Autism, Biotechnology, Brain Disorders, Genetics, 2.1 Biological and endogenous factors, Aetiology, General Science & Technology

Abstract

Although autism is a highly heritable neurodevelopmental disorder, attempts to identify specific susceptibility genes have thus far met with limited success. Genome-wide association studies using half a million or more markers, particularly those with very large sample sizes achieved through meta-analysis, have shown great success in mapping genes for other complex genetic traits. Consequently, we initiated a linkage and association mapping study using half a million genome-wide single nucleotide polymorphisms (SNPs) in a common set of 1,031 multiplex autism families (1,553 affected offspring). We identified regions of suggestive and significant linkage on chromosomes 6q27 and 20p13, respectively. Initial analysis did not yield genome-wide significant associations; however, genotyping of top hits in additional families revealed an SNP on chromosome 5p15 (between SEMA5A and TAS2R1) that was significantly associated with autism (P = 2 x 10(-7)). We also demonstrated that expression of SEMA5A is reduced in brains from autistic patients, further implicating SEMA5A as an autism susceptibility gene. The linkage regions reported here provide targets for rare variation screening whereas the discovery of a single novel association demonstrates the action of common variants.

Published

2009

24. NR2F1 deletion in a patient with a de novo paracentric inversion, inv(5)(q15q33.2), and syndromic deafness

Author

Brown, Kerry K, Alkuraya, Fowzan S, Matos, Michael, Robertson, Richard L, Kimonis, Virginia E, and Morton, Cynthia C

Subjects

Genetics, Human Genome, Pediatric, Congenital, COUP Transcription Factor I, Child, Preschool, Chromosome Inversion, Chromosome Mapping, Chromosomes, Human, Pair 5, Female, Gene Deletion, Hearing Loss, Bilateral, Hearing Loss, Sensorineural, Humans, In Situ Hybridization, Fluorescence, NR2F1, deafness, chromosomal inversion, microdeletion, FISH, 5q, Clinical Sciences

Abstract

In an effort to discover genes important for human development, we have ascertained patients with congenital anomalies and cytogenetically balanced chromosomal rearrangements. Herein, we report a 4-year-old girl with profound deafness, a history of feeding difficulties, dysmorphism, strabismus, developmental delay, and an apparently balanced de novo paracentric chromosome 5 inversion, inv(5)(q15q33.2). Molecular cytogenetic analysis of the inversion revealed the presence of microdeletions of approximately 400-500 kb at or near both breakpoints. The 5q15 microdeletion completely removes the nuclear receptor NR2F1 (COUP-TFI) from the inverted chromosome 5. We propose haploinsufficiency of NR2F1 to be the cause of the patient's deafness and many of the other associated anomalies based on striking similarity with the Nr2f1 null mouse. Additionally, this study further highlights the need for high resolution analysis of clinical samples with chromosomal rearrangements as associated deletions may be primarily responsible for the clinical features of these patients.

Published

2009

25. Duplication of 5q15‐q23.2: Case report and literature review

Author

Douyard, Jaclyn, Hawley, Pamela, Shaham, Meira, and Kimonis, Virginia

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Intellectual and Developmental Disabilities (IDD), Brain Disorders, Pediatric, Clinical Research, Chromosome Mapping, Chromosomes, Human, Pair 5, Craniofacial Abnormalities, Failure to Thrive, Female, Gene Duplication, Humans, Infant, Newborn, Male, Speech Disorders, Trisomy, Paediatrics and Reproductive Medicine, Public Health and Health Services, Genetics & Heredity, Paediatrics, Reproductive medicine

Abstract

BackgroundPure partial trisomy of chromosome 5q is rare and cases have ranged over the entire region, making it difficult to describe a good phenotypic correlation to the cytogenetic duplication.CaseWe present a 4.5-year-old girl with a de novo direct duplication of chromosome 5q15-q23.2. She has moderate developmental delay with lack of speech, microcephaly, and subtle dysmorphic features including prominent forehead, bulbous nose, epicanthic folds, protruding tongue, and slightly posteriorly-rotated ears.ConclusionsA comparison is made with other similar duplication cases reported in the literature and a general description of a proximal 5q duplication phenotype is given, with lack of speech as the principal feature.

Published

2006

26. Cornelia de Lange syndrome is caused by mutations in NIPBL, the human homolog of Drosophila melanogaster Nipped-B.

Author

Krantz, Ian D, McCallum, Jennifer, DeScipio, Cheryl, Kaur, Maninder, Gillis, Lynette A, Yaeger, Dinah, Jukofsky, Lori, Wasserman, Nora, Bottani, Armand, Morris, Colleen A, Nowaczyk, Malgorzata JM, Toriello, Helga, Bamshad, Michael J, Carey, John C, Rappaport, Eric, Kawauchi, Shimako, Lander, Arthur D, Calof, Anne L, Li, Hui-Hua, Devoto, Marcella, and Jackson, Laird G

Subjects

Chromosomes, Human, Pair 5, Animals, Humans, Mice, Drosophila melanogaster, De Lange Syndrome, DNA-Binding Proteins, Drosophila Proteins, In Situ Hybridization, Fluorescence, Species Specificity, Mutation, Genes, Insect, Molecular Sequence Data, Female, Male, Genetic Linkage, Chromosomes, Human, Pair 5, In Situ Hybridization, Fluorescence, Genes, Insect, Pediatric, Brain Disorders, Intellectual and Developmental Disabilities, Genetics, Rare Diseases, 2.1 Biological and endogenous factors, Congenital Disorders, Developmental Biology, Medical and Health Sciences, Biological Sciences

Abstract

Cornelia de Lange syndrome (CdLS; OMIM 122470) is a dominantly inherited multisystem developmental disorder characterized by growth and cognitive retardation; abnormalities of the upper limbs; gastroesophageal dysfunction; cardiac, ophthalmologic and genitourinary anomalies; hirsutism; and characteristic facial features. Genital anomalies, pyloric stenosis, congenital diaphragmatic hernias, cardiac septal defects, hearing loss and autistic and self-injurious tendencies also frequently occur. Prevalence is estimated to be as high as 1 in 10,000 (ref. 4). We carried out genome-wide linkage exclusion analysis in 12 families with CdLS and identified four candidate regions, of which chromosome 5p13.1 gave the highest multipoint lod score of 2.7. This information, together with the previous identification of a child with CdLS with a de novo t(5;13)(p13.1;q12.1) translocation, allowed delineation of a 1.1-Mb critical region on chromosome 5 for the gene mutated in CdLS. We identified mutations in one gene in this region, which we named NIPBL, in four sporadic and two familial cases of CdLS. We characterized the genomic structure of NIPBL and found that it is widely expressed in fetal and adult tissues. The fly homolog of NIPBL, Nipped-B, facilitates enhancer-promoter communication and regulates Notch signaling and other developmental pathways in Drosophila melanogaster.

Published

2004

27. Genetic heterogeneity of Usher syndrome type II: localisation to chromosome 5q

Author

Pieke-Dahl, S, Möller, CG, Kelley, PM, Astuto, LM, Cremers, CW, Gorin, MB, and Kimberling, WJ

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Clinical Research, Usher Syndrome, Neurosciences, Rare Diseases, Eye Disease and Disorders of Vision, Aetiology, 2.1 Biological and endogenous factors, Chromosome Mapping, Chromosomes, Human, Pair 5, Female, Genetic Heterogeneity, Hearing Loss, Sensorineural, Humans, Male, Pedigree, Retinitis Pigmentosa, Syndrome, Medical and Health Sciences, Genetics & Heredity, Clinical sciences

Abstract

Usher syndrome is a group of autosomal recessive disorders that includes retinitis pigmentosa (RP) with hearing loss. Usher syndrome type II is defined as moderate to severe hearing loss with RP. The USH2A gene at 1q41 has been isolated and characterised. In 1993, a large Usher II family affected with a mild form of RP was found to be unlinked to 1q41 markers. Subsequent linkage studies of families in our Usher series identified several type II families unlinked to USH2A and USH3 on 3q25. After a second unlinked family with many affected members and a mild retinal phenotype was discovered, a genome search using these two large families showed another Usher II locus on 5q (two point lod = 3.1 at D5S484). To date, we have identified nine unrelated 5q linked families (maximum combined multipoint lod = 5.86) as well as three Usher II families that show no significant linkage to any known Usher loci. Haplotype analysis of 5q markers indicates that the new locus is flanked by D5S428 and D5S433. Review of ophthalmological data suggests that RP symptoms are milder in 5q linked families; the RP is often not diagnosed until patients near their third decade. Enamel hypoplasia and severe, very early onset RP were observed in two of the three unlinked families; dental anomalies have not been previously described as a feature of Usher type II.

Published

2000

28. Whole-Genome Sequencing Identifies Novel Functional Loci Associated with Lung Function in Puerto Rican Youth

Author

David J. Erle, Walter L. Eckalbar, Max A. Seibold, Celeste Eng, Jose R. Rodriguez-Santana, Scott Huntsman, Esteban G. Burchard, Marquitta J. White, Cydney Urbanek, Luke R. Bonser, Kevin L. Keys, Eunice Y. Lee, Donglei Hu, Satria Sajuthi, Angel C.Y. Mak, Hyun Min Kang, Gonçalo R. Abecasis, Michael C. Zody, Deborah A. Nickerson, Soren Germer, Deepti Jain, and Elad Ziv

Subjects

Male, Esophageal Mucosa, Respiratory System, Gene Expression, Puerto rican, Critical Care and Intensive Care Medicine, Medical and Health Sciences, Linkage Disequilibrium, FEV1, 0302 clinical medicine, Indians, TMEM9 airway epithelial cells, Smooth Muscle, Forced Expiratory Volume, Medicine, 030212 general & internal medicine, Child, Lung, Lung function, Pediatric, Genetics, Chromosome Mapping, RNA sequencing, Single Nucleotide, admixed, Blacks, Chromosomes, Human, Pair 1, Pair 1, Respiratory, Chromosomes, Human, Pair 5, Female, Pair 5, Sequence Analysis, North American, geographic locations, Human, Biotechnology, Pulmonary and Respiratory Medicine, Chromatin Immunoprecipitation, Adolescent, Myocytes, Smooth Muscle, Quantitative Trait Loci, Black People, Bronchi, inflammatory, Polymorphism, Single Nucleotide, Chromosomes, White People, Cell Line, Young Adult, 03 medical and health sciences, Clinical Research, Humans, Polymorphism, Whole genome sequencing, Myocytes, Childhood asthma, Whole Genome Sequencing, Whites, Sequence Analysis, RNA, business.industry, Human Genome, Puerto Rico, Membrane Proteins, Asthma, Nasal Mucosa, 030228 respiratory system, Case-Control Studies, Indians, North American, Etiology, RNA, business

Abstract

Rationale: Puerto Ricans have the highest childhood asthma prevalence in the United States (23.6%); however, the etiology is uncertain.Objectives: In this study, we sought to uncover the genetic architecture of lung function in Puerto Rican youth with and without asthma who were recruited from the island (n = 836).Methods: We used admixture-mapping and whole-genome sequencing data to discover genomic regions associated with lung function. Functional roles of the prioritized candidate SNPs were examined with chromatin immunoprecipitation sequencing, RNA sequencing, and expression quantitative trait loci data.Measurements and Main Results: We discovered a genomic region at 1q32 that was significantly associated with a 0.12-L decrease in the lung volume of exhaled air (95% confidence interval, -0.17 to -0.07; P = 6.62 × 10-8) with each allele of African ancestry. Within this region, two SNPs were expression quantitative trait loci of TMEM9 in nasal airway epithelial cells and MROH3P in esophagus mucosa. The minor alleles of these SNPs were associated with significantly decreased lung function and decreased TMEM9 gene expression. Another admixture-mapping peak was observed on chromosome 5q35.1, indicating that each Native American ancestry allele was associated with a 0.15-L increase in lung function (95% confidence interval, 0.08-0.21; P = 5.03 × 10-6). The region-based association tests identified four suggestive windows that harbored candidate rare variants associated with lung function.Conclusions: We identified common and rare genetic variants that may play a critical role in lung function among Puerto Rican youth. We independently validated an inflammatory pathway that could potentially be used to develop more targeted treatments and interventions for patients with asthma.

Published

2020

29. 5q35 duplication presents with psychiatric and undergrowth phenotypes mediated by NSD1 overexpression and mTOR signaling downregulation.

Author

Quintero-Rivera, Fabiola, Quintero-Rivera, Fabiola, Eno, Celeste C, Sutanto, Christine, Jones, Kelly L, Nowaczyk, Małgorzata JM, Wong, Derek, Earl, Dawn, Mirzaa, Ghayda, Beck, Anita, Martinez-Agosto, Julian A, Quintero-Rivera, Fabiola, Quintero-Rivera, Fabiola, Eno, Celeste C, Sutanto, Christine, Jones, Kelly L, Nowaczyk, Małgorzata JM, Wong, Derek, Earl, Dawn, Mirzaa, Ghayda, Beck, Anita, and Martinez-Agosto, Julian A

Abstract

PurposeNuclear receptor binding SET domain protein 1, NSD1, encodes a histone methyltransferase H3K36. NSD1 is responsible for the phenotype of the reciprocal 5q35.2q35.3 microdeletion-microduplication syndromes. We expand the phenotype and demonstrate the functional role of NSD1 in microduplication 5q35 syndrome.MethodsThrough an international collaboration, we report nine new patients, contributing to the emerging phenotype, highlighting psychiatric phenotypes in older affected individuals. Focusing specifically on the undergrowth phenotype, we have modeled the effects of Mes-4/NSD overexpression in Drosophila melanogaster.ResultsThe individuals (including a family) from diverse backgrounds with duplications ranging in size from 0.6 to 4.5 Mb, have a consistent undergrowth phenotype. Mes-4 overexpression in the developing wing causes undergrowth, increased H3K36 methylation, and increased apoptosis. We demonstrate that altering the levels of insulin receptor (IR) rescues the apoptosis and the wing undergrowth phenotype, suggesting changes in mTOR pathway signaling. Leucine supplementation rescued Mes-4/NSD induced cell death, demonstrating decreased mTOR signaling caused by NSD1.ConclusionGiven that we show mTOR inhibition as a likely mechanism and amelioration of the phenotype by leucine supplementation in a fly model, we suggest further studies should evaluate the therapeutic potential of leucine or branched chain amino acids as an adjunct possible treatment to ameliorate human growth and psychiatric phenotypes and propose inclusion of 5q35-microduplication as part of the differential diagnosis for children and adults with delayed bone age, short stature, microcephaly, developmental delay, and psychiatric phenotypes.

Published

2021

30. Genome-wide meta-analysis of SNP-by9-ACEI/ARB and SNP-by-thiazide diuretic and effect on serum potassium in cohorts of European and African ancestry.

Author

Irvin, Marguerite, Irvin, Marguerite, Sitlani, Colleen, Noordam, Raymond, Avery, Christie, Bis, Joshua, Floyd, James, Li, Jin, Limdi, Nita, Srinivasasainagendra, Vinodh, Stewart, James, de Mutsert, Renée, Mook-Kanamori, Dennis, Lipovich, Leonard, Kleinbrink, Erica, Smith, Albert, Bartz, Traci, Whitsel, Eric, Uitterlinden, Andre, Wiggins, Kerri, Wilson, James, Zhi, Degui, Stricker, Bruno, Arnett, Donna, Psaty, Bruce, Lange, Leslie, Rotter, Jerome, Irvin, Marguerite, Irvin, Marguerite, Sitlani, Colleen, Noordam, Raymond, Avery, Christie, Bis, Joshua, Floyd, James, Li, Jin, Limdi, Nita, Srinivasasainagendra, Vinodh, Stewart, James, de Mutsert, Renée, Mook-Kanamori, Dennis, Lipovich, Leonard, Kleinbrink, Erica, Smith, Albert, Bartz, Traci, Whitsel, Eric, Uitterlinden, Andre, Wiggins, Kerri, Wilson, James, Zhi, Degui, Stricker, Bruno, Arnett, Donna, Psaty, Bruce, Lange, Leslie, and Rotter, Jerome

Abstract

We evaluated interactions of SNP-by-ACE-I/ARB and SNP-by-TD on serum potassium (K+) among users of antihypertensive treatments (anti-HTN). Our study included seven European-ancestry (EA) (N = 4835) and four African-ancestry (AA) cohorts (N = 2016). We performed race-stratified, fixed-effect, inverse-variance-weighted meta-analyses of 2.5 million SNP-by-drug interaction estimates; race-combined meta-analysis; and trans-ethnic fine-mapping. Among EAs, we identified 11 significant SNPs (P < 5 × 10-8) for SNP-ACE-I/ARB interactions on serum K+ that were located between NR2F1-AS1 and ARRDC3-AS1 on chromosome 5 (top SNP rs6878413 P = 1.7 × 10-8; ratio of serum K+ in ACE-I/ARB exposed compared to unexposed is 1.0476, 1.0280, 1.0088 for the TT, AT, and AA genotypes, respectively). Trans-ethnic fine mapping identified the same group of SNPs on chromosome 5 as genome-wide significant for the ACE-I/ARB analysis. In conclusion, SNP-by-ACE-I /ARB interaction analyses uncovered loci that, if replicated, could have future implications for the prevention of arrhythmias due to anti-HTN treatment-related hyperkalemia. Before these loci can be identified as clinically relevant, future validation studies of equal or greater size in comparison to our discovery effort are needed.

Published

2019

31. Skin picking disorder in 97 Italian and Spanish Cri du chat patients

Author

Giovanni Albani, Marianna Spunton, Félix Casado, Maria Elena Liverani, Julián Nevado, Fabio Tognon, Isabel Larrea, Marta del Valle, Luisa Medolago, Giovanni Porta, Cesare Danesino, Andrea Guala, and Josefina Porras

Subjects

Adult, Cri-du-Chat Syndrome, Male, Obsessive-Compulsive Disorder, Pediatrics, medicine.medical_specialty, Adolescent, Cri du chat, Variable size, Population, Cri du Chat Syndrome, Stress, rare genetic disorder, Chromosomes, Age Distribution, Surveys and Questionnaires, Genetics, Humans, Medicine, Skin-picking, Age of Onset, Child, Preschool, education, Genetics (clinical), Skin, education.field_of_study, High prevalence, business.industry, Genetic disorder, skin picking, Infant, Child, Preschool, Female, Italy, Middle Aged, Spain, Stress, Psychological, Chromosome Deletion, Chromosomes, Human, Pair 5, medicine.disease, Psychological, Pair 5, business, Skin lesion, Human

Abstract

Skin picking (SP) disorder is characterized by recurrent SP resulting in skin lesions. Several studies estimated its prevalence as approximately 2-4 % of the general population. It is also present in a high percentage of patients with intellectual and developmental disabilities, such as Cri du chat (CdC) syndrome, a rare genetic disorder caused by variable size deletions of the short arm of chromosome 5. The aim of this study was to evaluate, in 97 patients with CdC syndrome, the following data: frequency of SP, patient's age at onset, type, and topographic-anatomic distribution of the lesions presented. The results show that 85% of patients confirm a SP disorder, usually concentrated on the hands, fingers, and the face, with onset between 6 and 10 years of age, regardless of patient's sex. Evidence for early appearance of SP behavior, high prevalence in stressful circumstances, and efficacy of distracting actions immediately suggest the possibility that proper parental information about SP behavior and parental education concerning the methods to deal with this problem may result in its efficient reduction already in childhood.

Published

2019

32. Deficiency and haploinsufficiency of histone macroH2A1.1 in mice recapitulate hematopoietic defects of human myelodysplastic syndrome

Author

Lumir Krejci, Manlio Vinciguerra, Marguerite Marie Le Pannérer, Oriana Lo Re, Valerio Pazienza, Šárka Pospíšilová, Carlo Riccardi, Fedor Nikulenkov, Oxana Bereshchenko, A. Francis Stewart, Giovanni Li Volti, Cesarina Giallongo, Marcus Buschbeck, Tommaso Mazza, Libor Červinek, Jana Kotašková, Giuseppe A. Palumbo, and Sara Flamini

Subjects

0301 basic medicine, Myeloid, Macrocytic, Cellular differentiation, Haploinsufficiency, Hematopoiesis, MacroH2A1, Myelodysplastic syndrome, Epigenesis, Genetic, Histones, Mice, 0302 clinical medicine, Anemia, Macrocytic, Genetics (clinical), Cell Differentiation, Anemia, 3. Good health, Haematopoiesis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Chromosomes, Human, Pair 5, Chromosome Deletion, Pair 5, Sequence Analysis, Human, Down-Regulation, Biology, Chromosomes, 03 medical and health sciences, Genetic, Cancer stem cell, Genetics, medicine, Animals, Humans, Epigenetics, Molecular Biology, Ineffective Hematopoiesis, Sequence Analysis, RNA, Animal, Myelodysplastic syndromes, Research, medicine.disease, Hematopoietic Stem Cells, Disease Models, Animal, 030104 developmental biology, Myelodysplastic Syndromes, Mutation, Disease Models, Cancer research, RNA, RNA Splice Sites, Developmental Biology, Epigenesis

Abstract

Background Epigenetic regulation is important in hematopoiesis, but the involvement of histone variants is poorly understood. Myelodysplastic syndromes (MDS) are heterogeneous clonal hematopoietic stem cell (HSC) disorders characterized by ineffective hematopoiesis. MacroH2A1.1 is a histone H2A variant that negatively correlates with the self-renewal capacity of embryonic, adult, and cancer stem cells. MacroH2A1.1 is a target of the frequent U2AF1 S34F mutation in MDS. The role of macroH2A1.1 in hematopoiesis is unclear. Results MacroH2A1.1 mRNA levels are significantly decreased in patients with low-risk MDS presenting with chromosomal 5q deletion and myeloid cytopenias and tend to be decreased in MDS patients carrying the U2AF1 S34F mutation. Using an innovative mouse allele lacking the macroH2A1.1 alternatively spliced exon, we investigated whether macroH2A1.1 regulates HSC homeostasis and differentiation. The lack of macroH2A1.1 decreased while macroH2A1.1 haploinsufficiency increased HSC frequency upon irradiation. Moreover, bone marrow transplantation experiments showed that both deficiency and haploinsufficiency of macroH2A1.1 resulted in enhanced HSC differentiation along the myeloid lineage. Finally, RNA-sequencing analysis implicated macroH2A1.1-mediated regulation of ribosomal gene expression in HSC homeostasis. Conclusions Together, our findings suggest a new epigenetic process contributing to hematopoiesis regulation. By combining clinical data with a discrete mutant mouse model and in vitro studies of human and mouse cells, we identify macroH2A1.1 as a key player in the cellular and molecular features of MDS. These data justify the exploration of macroH2A1.1 and associated proteins as therapeutic targets in hematological malignancies. Electronic supplementary material The online version of this article (10.1186/s13148-019-0724-z) contains supplementary material, which is available to authorized users.

Published

2019

33. Lung cancer risk in never-smokers of European descent is associated with genetic variation in the 5(p)15.33 TERT-CLPTM1Ll region

Author

Melinda C. Aldrich, Mónica Pérez-Ríos, Ping Yang, Walid Saliba, Neil E. Caporaso, Ann G. Schwartz, Donatella Ugolini, Jun Ying, Zuo-Feng Zhang, Thomas Muley, David C. Christiani, Xuemei Ji, Mariza de Andrade, Matthew B. Schabath, Kjell Grankvist, Rayjean J. Hung, Olle Melander, Yonathan Brhane, Alberto Ruano-Ravina, Monica Neri, Irene Orlow, Aage Haugen, M. Dawn Teare, Olga Y. Gorlova, Ivan P. Gorlov, Hedy S. Rennert, Hermann Brenner, Susanne M. Arnold, Jie Na, Erik H.F.M. van der Heijden, H-Erich Wichmann, Hal Morgenstern, Shanbeh Zienolddiny, Angela Risch, Maria Timofeeva, Adonina Tardón, Curtis C. Harris, Margaret R. Spitz, Geoffrey Liu, John K. Field, Lambertus A. Kiemeney, Gadi Rennert, Loic Le Marchand, Christopher I. Amos, Vidar Skaug, Triantafillos Liloglou, Angeline S. Andrew, Paul Brennan, Philip Lazarus, Elise D. Bowman, Younghun Han, Nancy Diao, Bríd M. Ryan, Wei V. Chen, Jose I. Mayordomo, Heike Bickeböller, Richard S. Houlston, Xifeng Wu, Stig E. Bojesen, Yafang Li, Maria Teresa Landi, Michael P.A. Davies, Juan-Miguel Barros-Dios, Stefano Bonassi, Angela S. Wenzlaff, and Mattias Johansson

Subjects

0301 basic medicine, Oncology, Lung Neoplasms, Genotyping Techniques, Genome-wide association study, Lung Cancer, Never Smokers, Genome-wide Association Study, Genetic Susceptibility, Disease, Cardiorespiratory Medicine and Haematology, 0302 clinical medicine, Risk Factors, 2.1 Biological and endogenous factors, Medicine, Aetiology, Telomerase, Lung, Cancer, Single Nucleotide, Middle Aged, 3. Good health, Europe, Urological cancers Radboud Institute for Health Sciences [Radboudumc 15], 030220 oncology & carcinogenesis, Genetic susceptibility, Lung cancer, Never smokers, Chromosomes, Human, Pair 5, Female, Pair 5, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Human, Pulmonary and Respiratory Medicine, medicine.medical_specialty, Clinical Sciences, Oncology and Carcinogenesis, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Article, Chromosomes, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, Clinical Research, Internal medicine, Tobacco, Genetics, Genetic predisposition, Humans, Genetic Predisposition to Disease, Oncology & Carcinogenesis, Polymorphism, Cancer och onkologi, Tobacco Smoke and Health, business.industry, Prevention, Human Genome, Membrane Proteins, Genetic Variation, Odds ratio, medicine.disease, Confidence interval, respiratory tract diseases, Good Health and Well Being, 030104 developmental biology, Case-Control Studies, Cancer and Oncology, Etiology, business, Genome-Wide Association Study

Abstract

Introduction: Inherited susceptibility to lung cancer risk in never-smokers is poorly understood. The major reason for this gap in knowledge is that this disease is relatively uncommon (except in Asians), making it difficult to assemble an adequate study sample. In this study we conducted a genome-wide association study on the largest, to date, set of European-descent never-smokers with lung cancer. Methods: We conducted a two-phase (discovery and replication) genome-wide association study in never-smokers of European descent. We further augmented the sample by performing a meta-analysis with never-smokers from the recent OncoArray study, which resulted in a total of 3636 cases and 6295 controls. We also compare our findings with those in smokers with lung cancer. Results: We detected three genome-wide statistically significant single nucleotide polymorphisms rs31490 (odds ratio [OR]: 0.769, 95% confidence interval [CI]: 0.722-0.820; p value 5.31 x 10(-16)), rs380286 (OR: 0.770, 95% CI: 0.723-0.820; p value 4.32 x 10(-16)), and rs4975616 OR: 0.778, 95% CI: 0.730-0.829; p value 1.04 x 10(-14)). All three mapped to Chromosome 5 CLPTM1L-TERT region, previously shown to be associated with lung cancer risk in smokers and in never-smoker Asian women, and risk of other cancers including breast, ovarian, colorectal, and prostate. Conclusions: We found that genetic susceptibility to lung cancer in never-smokers is associated to genetic variants with pan-cancer risk effects. The comparison with smokers shows that top variants previously shown to be associated with lung cancer risk only confer risk in the presence of tobacco exposure, underscoring the importance of gene-environment interactions in the etiology of this disease. (C) 2019 International Association for the Study of Lung Cancer. Published by Elsevier Inc. This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).

Published

2019

34. Disruption of the APC gene by t(5;7) translocation in a Turcot family

Author

Fausto Sessa, Ileana Carnevali, Alessandra Viel, Daniela Furlan, Maria Grazia Tibiletti, Nora Sahnane, and Barbara Bernasconi

Subjects

Adult, 0301 basic medicine, Cancer Research, Genes, APC, Genetic counseling, Translocation, Chromosomal translocation, Biology, medicine.disease_cause, Chromosomes, Translocation, Genetic, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, FISH, Genetic, Neoplastic Syndromes, Hereditary, MUTYH, Genetics, medicine, Humans, Neoplastic Syndromes, Multiplex ligation-dependent probe amplification, Molecular Biology, Conventional karyotype, Mutation, Brain Neoplasms, Medicine (all), Breakpoint, APC, Digital PCR, MLPA, Turcot syndrome, Colorectal Neoplasms, Female, Karyotyping, Chromosomes, Human, Pair 5, Chromosomes, Human, Pair 7, Hereditary, 030104 developmental biology, Genes, 030220 oncology & carcinogenesis, Pair 7, DNA mismatch repair, Pair 5, Human

Abstract

Turcot syndrome (TS) refers to the combination of colorectal polyps and primary tumours of the central nervous system. TS is a heterogeneous genetic condition due to APC and/or mismatch repair germline mutations. When APC is involved the vast majority of mutations are truncating, but in approximately 20%-30% of patients with familial polyposis no germline mutation can be found. A 30-year-old Caucasian woman with a positive pedigree for TS was referred to our Genetic Counselling Service. She was negative for APC and MUTYH but showed a reciprocal balanced translocation t(5;7)(q22;p15) at chromosome analysis. FISH analysis using specific BAC probes demonstrated that 5q22 breakpoint disrupted the APC gene. Transcript analysis by MLPA and digital PCR revealed that the cytogenetic rearrangement involving the 3' end of the APC gene caused a defective expression of a truncated transcript. This result allowed cytogenetic analysis to be offered to all the other family members and segregation analysis clearly demonstrated that all the carriers were affected, whereas non-carriers did not have the polyposis. A cytogenetic approach permitted the identification of the mutation-causing disease in this family, and the segregation analysis together with the transcript study supported the pathogenetic role of this mutation. Karyotype analysis was used as a predictive test in all members of this family. This family suggests that clinically positive TS and FAP cases, which test negative with standard molecular analysis, could be easily and cost-effectively resolved by a classical and molecular cytogenetic approach.

Published

2016

35. Lenalidomide treatment of myelodysplastic syndromes with chromosome 5q deletion: Results from the National Registry of the Italian Drug Agency

Author

Arcioni, F., Roncadori, A., Di Battista, V., Tura, S., Covezzoli, A., Cundari, S., Mecucci, C., Abbadessa, A., Alterini, R., Santini, V., Cantonetti, M., Buccisano, F., Bacigalupo, A., Sessarego, M., Tonso, A., Ferrero, D., D'Ardia, S., Tarella, C., Cascavilla, N., Bassan, R., Sancetta, R., Cortelezzi, A., Reda, G., Maria D'Arco, A., De Fabritiis, P., Di Renzo, N., Falini, B., Alimena, G., Avanzini, P., Ilariucci, F., Iuliano, F., La Nasa, G., Caocci, G., Defina, M., Latte, G., Palmas, A., Levis, A., Leone, G., Teresa Voso, M., Leoni, P., Poloni, A., Fozza, C., Crugnola, M., Montanaro, M., Spedini, P., Lanza, F., Pizzuti, M., Pane, F., Paolini, R., Borin, L., Rambaldi, A., Rossi, G., Maria Pelizzari, A., Russo, D., D'Emilio, A., Ruggeri, M., Semenzato, G., Specchia, G., Tagariello, G., Sartori, R., Testore, F., Ciravegna, G., Marasca, R., Cimarosto, L., Fontanive, O., Visani, G., Arcioni, F., Roncadori, A., Di Battista, V., Tura, S., Covezzoli, A., Cundari, S., Mecucci, C., Abbadessa, A., Alterini, R., Santini, V., Cantonetti, M., Buccisano, F., Bacigalupo, A., Sessarego, M., Tonso, A., Ferrero, D., D'Ardia, S., Tarella, C., Cascavilla, N., Bassan, R., Sancetta, R., Cortelezzi, A., Reda, G., Maria D'Arco, A., De Fabritiis, P., Di Renzo, N., Falini, B., Alimena, G., Avanzini, P., Ilariucci, F., Iuliano, F., La Nasa, G., Caocci, G., Defina, M., Latte, G., Palmas, A., Levis, A., Leone, G., Teresa Voso, M., Leoni, P., Poloni, A., Fozza, C., Crugnola, M., Montanaro, M., Spedini, P., Lanza, F., Pizzuti, M., Pane, F., Paolini, R., Borin, L., Rambaldi, A., Rossi, G., Maria Pelizzari, A., Russo, D., D'Emilio, A., Ruggeri, M., Semenzato, G., Specchia, G., Tagariello, G., Sartori, R., Testore, F., Ciravegna, G., Marasca, R., Cimarosto, L., Fontanive, O., and Visani, G.

Subjects

Oncology, Myeloid, Male, Group B, Immunologic Factor, 0302 clinical medicine, Retrospective Studie, hemic and lymphatic diseases, del(5q), Prospective Studies, Registries, Prospective cohort study, Hematology, Leukemia, registry study, Standard treatment, Remission Induction, General Medicine, Middle Aged, lenalidomide, myelodysplastic syndromes, Aged, Chromosomes, Human, Pair 5, Disease Progression, Female, Humans, Immunologic Factors, Italy, Karyotyping, Lenalidomide, Leukemia, Myeloid, Acute, Myelodysplastic Syndromes, Retrospective Studies, Thalidomide, Chromosome Deletion, 030220 oncology & carcinogenesis, Pair 5, medicine.drug, Human, medicine.medical_specialty, Myelodysplastic Syndrome, Acute, Chromosomes, NO, 03 medical and health sciences, Internal medicine, medicine, business.industry, Myelodysplastic syndromes, Retrospective cohort study, medicine.disease, Settore MED/15, Prospective Studie, business, 030215 immunology

Abstract

Objective The most typical cytogenetic aberration in myelodysplastic syndromes is del(5q), which, when isolated, is associated with refractory anaemia and good prognosis. Based on high rates of erythroid response and transfusion independence, Lenalidomide (LEN) became the standard treatment. This multi-centre study was designed to supplement Italian Registry data on LEN by addressing prescription, administration appropriateness, haematological and cytogenetic responses and disease evolution. Methods MORE study was an observational, non-interventional, multi-centre, retrospective and prospective study. Cases were recruited from 45 Haematological Centres throughout Italy. Data were collected from the Italian National Registry for Lenalidomide administration and supplemented by a MORE data form. Results Data from 190/213 patients were analysed. In all, 149 had been diagnosed by conventional cytogenetics (GROUP A) and 41 only by FISH (GROUP B). Overall erythroid response was obtained in 92.8% of cases. Overall cytogenetic remission was achieved in 22.6% of cases. Disease progression occurred in 15.6% of cases. Clonal cytogenetic evolution characterised progression to AML but not to higher risk MDS. Conclusions Erythroid response to Lenalidomide was similar in MDS with isolated del(5q) and with del(5q) plus one anomaly. Progression to AML or higher risk MDS showed different cytogenetic features.

Published

2018

36. Early lenalidomide treatment for low and intermediate-1 International Prognostic Scoring System risk myelodysplastic syndromes with del(5q) before transfusion dependence

Author

Grazia Sanpaolo, Agostino Cortelezzi, Ulrich Germing, Francesca Ronco, Antonio Volpe, Michael Lauseker, Irene Santacaterina, Enrico Balleari, Antonella Poloni, Giuseppe A. Palumbo, Maria Antonietta Aloe Spiriti, Andrea Kündgen, Caterina Alati, Maria Grazia D'Errigo, Roberto Latagliata, Esther Oliva, and Alessandra Ricco

Subjects

Cancer Research, Pediatrics, pair 5, Gastroenterology, Quality of life, middle aged, humans, Original Research, Aged, 80 and over, education.field_of_study, adult, chromosome deletion, 5q deletion syndrome, immunologic factors, anemia, myelodysplastic syndromes, follow-up studies, aged, female, Oncology, International Prognostic Scoring System, Chromosomes, Human, Pair 5, medicine.drug, chromosomes, medicine.medical_specialty, Anemia, lenalidomide, Population, nuclear medicine and imaging, quality of life, Radiology, Nuclear Medicine and Imaging, male, thalidomide, Internal medicine, medicine, Radiology, Nuclear Medicine and imaging, human, aged 80 and over, biomarkers, prognosis, treatment outcome, chromosomes, human, pair 5, oncology, radiology, nuclear medicine and imaging, cancer research, education, Lenalidomide, business.industry, Myelodysplastic syndromes, Clinical Cancer Research, medicine.disease, radiology, Thalidomide, Hemoglobin, business

Abstract

Lenalidomide is approved for the treatment of transfusion‐dependent (TD) del(5q) myelodysplastic syndromes (MDS). However, few data are available in patients with transfusion‐independent (TI) del(5q) MDS. In the first, observational, part of this 2‐part study, we assessed the impact of transfusion dependence on overall survival (OS) and non‐leukemic death in untreated del(5q) MDS patients who were TD (n = 136), TI with hemoglobin (Hb) ≥10 mg/dL (n = 88), or TI with Hb

Published

2015

37. Myelodysplastic syndrome with del (5q) and JAK2V617F mutation transformed to acute myeloid leukaemia with complex karyotype

Author

Achille Pich, Cristina Cavaliere, Simonetta Kerim, Laura Godio, Ludovica Riera, Lisa Bonello, and Paola Francia di Celle

Subjects

Myeloid, medicine.medical_specialty, NPM1, Macrocytic, Karyotype, Chromosomal translocation, Acute, Neutropenia, Chromosomes, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Internal medicine, Aged, Anemia, Macrocytic, Chromosome Deletion, Chromosomes, Human, Pair 5, Female, Humans, Janus Kinase 2, Leukemia, Myeloid, Acute, Mutation, Myelodysplastic Syndromes, Hematology, Medicine (all), Complex Karyotype, Medicine, Leukemia, business.industry, Myelodysplastic syndromes, breakpoint cluster region, Anemia, General Medicine, medicine.disease, Molecular biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, Bone marrow, Pair 5, business, Human, 030215 immunology

Abstract

Dear Editor, Myelodysplastic syndrome with isolated del (5q) and JAK2 mutation is a distinct entity within the World Health Organization (WHO) category myelodysplastic syndromes (MDS) [1]. JAK2 is a gain of function mutation, typically associated with myeloproliferative neoplasms (MPN) [2]. However, approximately 5 % of patients with isolated del (5q) also harbours the JAK2 mutation [3, 4]. No correlation was found between isolated del (5q) JAK2 mutated cases and clinical presentation, morphological features, disease transformation or patient outcome [4, 5], although a few cases presented with higher platelet and WBC count [3]. Lenalidomide was reported to be an effective treatment for the disease [6]. We have recently studied a patient with del (5q) and JAK2 mutation transformed to acute myeloid leukaemia (AML) with complex karyotype and increased JAK2 mutation load. A 66-year-old female presented with moderate anaemia and high platelet count (haemoglobin 100 g/l, WBC 7.2 × 10/l, platelets 800 × 10/l). Neutrophils were 4.95×10/l, eosinophils 0.21×10/l, monocytes 0.14×10/l and lymphocytes 1.9×10/l. No blast cell was present in the peripheral blood. There was no splenoor hepatomegaly. On marrow aspirate, only eight metaphases showing a normal karyotype (46,XX) could be analysed, due to the lack of growth of an adequate number of metaphases and the poor cellularity of the sample. FISH analysis was limited to the study of 5q and demonstrated 5q31 deletion in 12 % of the nuclei. Thus, additional aberrations could not be identified. BCR/ABL rearrangements (p210, p190) were absent, while JAK2 mutation displayed an allele burden of 4.28 %. Bone marrow (BM) biopsy showed a 70 % cellularity, slight dyserythropoiesis, moderate myeloid hyperplasia and marked proliferation of the megakaryocytic lineage with some dysplasia. A few megakaryocytes were large with hyperlobulated nuclei; others were medium-sized, with round and/or hypolobulated nuclei. There were 3 % CD34-positive blasts and moderate reticulin fibrosis (WHOMF-2). (Fig. 1a– c, e). A strong nuclear p53 immunostaining was detected in 2 % haematopoietic cells (Fig. 1d). We proposed a diagnosis of MDS with del (5q) and JAK2 mutation. The patient did not receive any therapy. No organomegaly nor leukoerythroblastosis was reported during the course of the disease. Twenty-seven months later, she was admitted to the hospital because of persistent fever, severe anaemia and neutropenia (Hb level 7.5 g/l, WBC 2.3×10/l, neutrophils 0.75×10/l, platelets 137×10/l). There were 5 % blast cells in the peripheral blood. Chromosome banding analysis showed the following: 46, XX [1] / 45,XX, −7, del(5)(q13q33), del(13)(q14q34) [7] / 45, idem, del(2)(p12) [2]. FISH analysis demonstrated −7, del(5)(q31), del(13)(q14) (80 %) without BCR/ABL, AML1/ETO, PML/RARA, inv(16), MLL(11q23) translocation and +8. Molecular analysis did not identify FLT3 (ITD, D835), NPM1 (exon 12) or MLL-PTD mutations. Real-time quantitative polymerase chain reaction (RQ-PCR) detected 4164 WT1 copies/10 ABL copies and 55.6 % JAK2 mutation load. p53 sequencing analysis of exons 2–11 showed * Achille Pich achille.pich@unito.it

Published

2016

38. Duplication events downstream of IRX1 cause North Carolina macular dystrophy at the MCDR3 locus

Author

Michel Michaelides, Valentina Cipriani, Sandra Valeina, Nikolas Pontikos, Andrew R. Webster, Gavin Arno, Bernard Puech, Inna Inashkina, Veronica van Heyningen, Raquel S. Silva, Mareta Audere, Baiba Lace, Anthony T. Moore, Katrina Rutka, and Ambreen Kalhoro

Subjects

Male, Gene Expression, Neurodegenerative, Eye, Macular Degeneration, ADAMTS Proteins, Gene duplication, Chromosome Duplication, 2.1 Biological and endogenous factors, Aetiology, Tomography, Corneal Dystrophies, Hereditary, Genetics, Hereditary, Chromosomes, Human, Pair 5, Medicine, Chromosomes, Human, Pair 6, Female, Pair 6, Pair 5, NORTH CAROLINA MACULAR DYSTROPHY, Sequence Analysis, Tomography, Optical Coherence, Human, IRX1, Adult, medicine.medical_specialty, Corneal Dystrophies, Science, Genomics, Locus (genetics), Biology, Article, Retina, Chromosomes, Fetus, Molecular genetics, medicine, Humans, Family, Eye Proteins, Gene, Eye Disease and Disorders of Vision, Homeodomain Proteins, Base Sequence, Haplotype, Human Genome, Sequence Analysis, DNA, DNA, Haplotypes, Optical Coherence, Genetic Loci, Transcription Factors

Abstract

Autosomal dominant North Carolina macular dystrophy (NCMD) is believed to represent a failure of macular development. The disorder has been assigned by linkage to two loci, MCDR1 on chromosome 6q16 and MCDR3 on chromosome 5p15-p13. Recently, noncoding variants upstream ofPRDM13and a large duplication includingIRX1have been identified. However, the underlying disease-causing mechanism remains uncertain. Through a combination of sequencing studies, we report two novel overlapping duplications at the MCDR3 locus, in a gene desert downstream ofIRX1and upstream ofADAMTS16.One duplication of 43 kb was identified in nine NCMD families (with evidence for a shared ancestral haplotype), and another one of 45 kb was found in a single family. The MCDR3 locus is thus refined to a shared region of 39 kb that contains DNAse hypersensitive sites active at a restricted time window during retinal development. Publicly available data confirmed expression ofIRX1andADAMTS16in human fetal retina, withIRX1preferentially expressed in fetal macula. These findings represent a major advance in our understanding of the molecular genetics of NCMD at the MCDR3 locus and provide insights into the genetic pathways involved in human macular development.Abbreviations listaCGHarray comparative genomic hybridizationCNVCopy number variantIBDIdentical-by-descentiPSCInduced pluripotent stem cellDHSDNase hypersensitive siteHHHomozygosity HaplotypeMCDRMacular dystrophy regionNCMDNorth Carolina macular dystrophyPCRPolymerase chain reactionRCHHRegion with a Conserved Homozygosity HaplotypeSNPSingle-nucleotide polymorphismSNVSingle nucleotide variantSVStructural variantWGSWhole-genome sequencing

Published

2017

39. Switch in FGFR3 and -4 expression profile during human renal development may account for transient hypercalcemia in patients with Sotos syndrome due to 5q35 microdeletions

Author

Mutsaers, Henricus A M, Levtchenko, Elena N, Martinerie, Laetitia, Pertijs, Jeanne C L M, Allegaert, Karel, Devriendt, Koenraad, Masereeuw, Roos, Monnens, Leo A H, Lombès, Marc, Sub General Pharmacology, Pharmacology, Sub General Pharmacology, and Pharmacology

Subjects

Fibroblast growth factor 23, Male, musculoskeletal diseases, medicine.medical_specialty, Fibroblast Growth Factor, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], Biology, Kidney, Biochemistry, Chromosomes, Article, Endocrinology, Fetus, Internal medicine, medicine, Humans, Receptor, Fibroblast Growth Factor, Type 3, Receptor, Fibroblast Growth Factor, Type 4, Klotho, Sotos Syndrome, Sotos syndrome, Biochemistry (medical), Genetic disorder, Infant, Newborn, Infant, Kidney metabolism, Switch, Fibroblast growth factor receptor 4, Newborn, medicine.disease, Fibroblast Growth Factor-23, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], medicine.anatomical_structure, Genes, Calcium ion homeostasis, Hypercalcemia, Chromosomes, Human, Pair 5, Pair 5, Chromosome Deletion, Type 4, Transcriptome, Type 3, Genes, Switch, Human, Receptor

Abstract

Contains fulltext : 136899.pdf (Publisher’s version ) (Closed access) CONTEXT: Sotos syndrome is a rare genetic disorder with a distinct phenotypic spectrum including overgrowth and learning difficulties. Here we describe a new case of Sotos syndrome with a 5q35 microdeletion, affecting the fibroblast growth factor receptor 4 (FGFR4) gene, presenting with infantile hypercalcemia. OBJECTIVE: We strove to elucidate the evanescent nature of the observed hypercalcemia by studying the ontogenesis of FGFR3 and FGFR4, which are both associated with fibroblast growth factor (FGF) 23-mediated mineral homeostasis, in the developing human kidney. DESIGN: Quantitative RT-PCR and immunohistochemical analyses were used on archival human kidney samples to investigate the expression of the FGFR signaling pathway during renal development. RESULTS: We demonstrated that renal gene and protein expression of both FGFRs increased during fetal development between the gestational ages (GAs) of 14-40 weeks. Yet FGFR4 expression increased more rapidly as compared with FGFR3 (slope 0.047 vs 0.0075, P = .0018). Moreover, gene and protein expression of the essential FGFR coreceptor, Klotho, also increased with a significant positive correlation between FGFR and Klotho mRNA expression during renal development. Interestingly, we found that perinatal FGFR4 expression (GA 38-40 wk) was 7-fold higher as compared with FGFR3 (P = .0035), whereas in adult kidney tissues, FGFR4 gene expression level was more than 2-fold lower compared with FGFR3 (P = .0029), thus identifying a molecular developmental switch of FGFR isoforms. CONCLUSION: We propose that the heterozygous FGFR4 deletion, as observed in the Sotos syndrome patient, leads to a compromised FGF23 signaling during infancy accounting for transient hypercalcemia. These findings represent a novel and intriguing view on FGF23 mediated calcium homeostasis.

Published

2014

40. Activation of the mTOR signaling pathway by L-leucine in 5q- syndrome and other RPS14-deficient erythroblasts

Author

Christina Mecucci, Bon Ham Yip, Jacqueline Boultwood, Andrea Pellagatti, Martin Attwood, David J. Roberts, Peter Vandenberghe, Jaroslaw P. Maciejewski, Chaitanya Vuppusetty, A A Lamikanra, A.A.N. Giagounidis, J. S. Wainscoat, and Ulrich Germing

Subjects

Ribosomal Proteins, 5q-syndrome, Cancer Research, medicine.medical_specialty, Erythroblasts, Macrocytic, Biology, Chromosomes, Enzyme activator, Anemia, Macrocytic, Chromosome Deletion, Chromosomes, Human, Pair 5, Enzyme Activation, Humans, Leucine, Signal Transduction, TOR Serine-Threonine Kinases, Hematology, Anesthesiology and Pain Medicine, Ribosomal protein, hemic and lymphatic diseases, Internal medicine, medicine, MTOR signaling pathway, Anemia, hemic and immune systems, Cell biology, Oncology, Biochemistry, Pair 5, Signal transduction, Human, circulatory and respiratory physiology

Abstract

Activation of the mTOR signaling pathway by L -leucine in 5q- syndrome and other RPS14-deficient erythroblasts

Published

2013

41. Fine mapping of chromosome 5p15.33 based on a targeted deep sequencing and high density genotyping identifies novel lung cancer susceptibility loci

Author

Neil E. Caporaso, James McKay, Jennifer A. Doherty, Brian E. Henderson, Gary E. Goodman, Ruth C. Travis, Robert E. Denroche, Peter Kraft, Rayjean J. Hung, Paul Brennan, Xuchen Zong, Philip C. Zuzarte, H. Bas Bueno-de-Mesquita, David C. Christiani, Gord Fehringer, John Douglas Mcpherson, Shelley S. Tworoger, Loic Le Marchand, David Zaridze, Xiangjun Xiao, Elisabete Weiderpass, Mikael Johansson, Li Su, John K. Field, Michael W. Marcus, Sabina Sieri, John R. McLaughlin, Marie-Christine Boutron-Ruault, Paolo Vineis, Geoffrey Liu, Lynne R. Wilkens, Yafang Li, Linda Kachuri, Graham G. Giles, Yongyue Wei, Maria Teresa Landi, Michael P.A. Davies, Mattias Johansson, Chu Chen, Xuehong Zhang, J. Ramón Quirós, Gianluca Severi, Russell Hyde, and Christopher I. Amos

Subjects

0301 basic medicine, Male, Cancer Research, Lung Neoplasms, Genotyping Techniques, Oncology and Carcinogenesis, Original Manuscript, Genome-wide association study, Locus (genetics), Single-nucleotide polymorphism, Biology, Deep sequencing, Chromosomes, 03 medical and health sciences, Genetics, Humans, 2.1 Biological and endogenous factors, Genetic Predisposition to Disease, Oncology & Carcinogenesis, Aetiology, Genotyping, Lung, Cancer, Prevention, Human Genome, Lung Cancer, Chromosome Mapping, General Medicine, respiratory system, Middle Aged, Lung cancer susceptibility, 030104 developmental biology, Genetic Loci, Case-Control Studies, Chromosomes, Human, Pair 5, Female, Pair 5, Imputation (genetics), Human

Abstract

Chromosome 5p15.33 has been identified as a lung cancer susceptibility locus, however the underlying causal mechanisms were not fully elucidated. Previous fine-mapping studies of this locus have relied on imputation or investigated a small number of known, common variants. This study represents a significant advance over previous research by investigating a large number of novel, rare variants, as well as their underlying mechanisms through telomere length. Variants for this fine-mapping study were identified through a targeted deep sequencing (average depth of coverage greater than 4000×) of 576 individuals. Subsequently, 4652 SNPs, including 1108 novel SNPs, were genotyped in 5164 cases and 5716 controls of European ancestry. After adjusting for known risk loci, rs2736100 and rs401681, we identified a new, independent lung cancer susceptibility variant in LPCAT1: rs139852726 (OR = 0.46, P = 4.73×10(-9)), and three new adenocarcinoma risk variants in TERT: rs61748181 (OR = 0.53, P = 2.64×10(-6)), rs112290073 (OR = 1.85, P = 1.27×10(-5)), rs138895564 (OR = 2.16, P = 2.06×10(-5); among young cases, OR = 3.77, P = 8.41×10(-4)). In addition, we found that rs139852726 (P = 1.44×10(-3)) was associated with telomere length in a sample of 922 healthy individuals. The gene-based SKAT-O analysis implicated TERT as the most relevant gene in the 5p15.33 region for adenocarcinoma (P = 7.84×10(-7)) and lung cancer (P = 2.37×10(-5)) risk. In this largest fine-mapping study to investigate a large number of rare and novel variants within 5p15.33, we identified novel lung and adenocarcinoma susceptibility loci with large effects and provided support for the role of telomere length as the potential underlying mechanism.

Published

2016

42. Mutations in GRM6 identified in consanguineous Pakistani families with congenital stationary night blindness

Author

Muhammad Asif Naeem, Gottsch, A. D. H., Ullah, I., Khan, S. N., Husnain, T., Butt, N. H., Qazi, Z. A., Akram, J., Riazuddin, S., Ayyagari, R., Hejtmancik, J. F., and Riazuddin, S. A.

Subjects

Adult, Male, Eye Diseases, genetic structures, Molecular Sequence Data, Gene Expression, Genes, Recessive, Ophthalmology & Optometry, Chromosomes, Consanguinity, Clinical Research, Opthalmology and Optometry, Night Blindness, Receptors, Genetics, Electroretinography, Myopia, Recessive, 2.1 Biological and endogenous factors, Animals, Humans, Pakistan, Amino Acid Sequence, Aged, Base Sequence, Homozygote, Eye Diseases, Hereditary, Genetic Diseases, X-Linked, DNA, Exons, Sequence Analysis, DNA, X-Linked, eye diseases, Pedigree, Hereditary, Genes, Receptors, Glutamate, Genetic Diseases, Mutation, Chromosomes, Human, Pair 5, Female, sense organs, Pair 5, Glutamate, Sequence Analysis, Sequence Alignment, Human, Research Article

Abstract

© 2015 Molecular Vision. Purpose: This study was undertaken to investigate the causal mutations responsible for autosomal recessive congenital stationary night blindness (CSNB) in consanguineous Pakistani families. Methods: Two consanguineous families with multiple individuals manifesting symptoms of stationary night blindness were recruited. Affected individuals underwent a detailed ophthalmological examination, including fundus examination and electroretinography. Blood samples were collected and genomic DNA was extracted. Exclusion analyses were completed by genotyping closely spaced microsatellite markers, and two-point logarithm of odds (LOD) scores were calculated. All coding exons, along with the exon–intron boundaries of GRM6, were sequenced bidirectionally. Results: According to the medical history available to us, affected individuals in both families had experienced night blindness from the early years of their lives. Fundus photographs of affected individuals in both the families appeared normal, with no signs of attenuated arteries or bone spicule pigmentation. The scotopic electroretinogram (ERG) response were absent in all of the affected individuals, while the photopic measurements show reduced b-waves. During exclusion analyses, both families localized to a region on chromosome 5q that harbors GRM6, a gene previously associated with autosomal recessive CSNB. Bidirectional sequencing of GRM6 identified homozygous single base pair changes, specifically c.1336C>T (p.R446X) and c.2267G>A (p.G756D) in families PKRP170 and PKRP172, respectively. Conclusions: We identified a novel nonsense and a previously reported missense mutation in GRM6 that were responsible for autosomal recessive CSNB in patients of Pakistani decent.

Published

2015

43. Candidate locus analysis of the TERT-CLPTM1L cancer risk region on chromosome 5p15 identifies multiple independent variants associated with endometrial cancer risk

Author

Carvajal-Carmona, L.G., O'Mara, T.A., Painter, J.N.., Lose, F.A., Dennis, J., Michailidou, K., Tyrer, J.P., Ahmed, S., Ferguson, K., Healey, C.S., Pooley, K., Beesley, J., Cheng, T., Jones, A., Howarth, K., Martin, L., Gorman, M., Hodgson, S., Wentzensen, N., Fasching, P.A., Hein, A., Beckmann, M.W., Renner, S.P., Doerk, T., Hillemanns, P., Duerst, M., Runnebaum, I., Lambrechts, D., Coenegrachts, L., Schrauwen, S., Amant, F., Winterhoff, B., Dowdy, S.C., Goode, E.L., Teoman, A., Salvesen, H.B., Trovik, J., Njolstad, T.S., Werner, H.M.J., Scott, R.J., Ashton, K., Proietto, T., Otton, G., Wersaell, O., Mints, M., Tham, E., Hall, P., Czene, K., Liu, J., Li, J., Hopper, J.L., Southey, M.C., Ekici, A.B., Ruebner, M., Johnson, N., Peto, J., Burwinkel, B., Marme, F., Brenner, H., Dieffenbach, A.K., Meindl, A., Brauch, H., Lindblom, A., Depreeuw, J., Moisse, M., Chang-Claude, J., Rudolph, A., Couch, F.J., Olson, J.E., Giles, G.G., Bruinsma, F., Cunningham, J.M., Fridley, B.L., Borresen-Dale, A.-L., Kristensen, V.N., Cox, A., Swerdlow, A.J., Orr, N., Bolla, M.K., Wang, Q., Weber, R.P., Chen, Z., Shah, M., Pharoah, P.D.P., Dunning, A.M., Tomlinson, I., Easton, D.F., Spurdle, A.B., Thompson, D.J., NSECG, ANECS, RENDOCAS, AOCS, Network, GENICA, Dennis, Joe [0000-0003-4591-1214], Tyrer, Jonathan [0000-0003-3724-4757], Pooley, Karen [0000-0002-1274-9460], Wang, Jean [0000-0002-9139-0627], Pharoah, Paul [0000-0001-8494-732X], Dunning, Alison [0000-0001-6651-7166], Easton, Douglas [0000-0003-2444-3247], and Apollo - University of Cambridge Repository

Subjects

National Study of Endometrial Cancer Genetics Group, Australian Ovarian Cancer Study, Polymorphism, Single Nucleotide, Chromosomes, Promoter Regions, Paediatrics and Reproductive Medicine, Databases, Uterine Cancer, Genetic, Complementary and Alternative Medicine, Risk Factors, Models, Australian National Endometrial Cancer Study Group, Genetics, 2.1 Biological and endogenous factors, Humans, Genetic Testing, Aetiology, Polymorphism, Promoter Regions, Genetic, Telomerase, Cancer, Genetics & Heredity, Neoplastic, Models, Genetic, Nucleic Acid, RENDOCAS, Prevention, Human Genome, Membrane Proteins, Single Nucleotide, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, Gene Expression Regulation, Haplotypes, Genetic Loci, Chromosomes, Human, Pair 5, Female, GENICA Network, Pair 5, Databases, Nucleic Acid, Human

Abstract

Several studies have reported associations between multiple cancer types and single-nucleotide polymorphisms (SNPs) on chromosome 5p15, which harbours TERT and CLPTM1L, but no such association has been reported with endometrial cancer. To evaluate the role of genetic variants at the TERT-CLPTM1L region in endometrial cancer risk, we carried out comprehensive fine-mapping analyses of genotyped and imputed SNPs using a custom Illumina iSelect array which includes dense SNP coverage of this region. We examined 396 SNPs (113 genotyped, 283 imputed) in 4,401 endometrial cancer cases and 28,758 controls. Single-SNP and forward/backward logistic regression models suggested evidence for three variants independently associated with endometrial cancer risk (P = 4.9 × 10(-6) to P = 7.7 × 10(-5)). Only one falls into a haplotype previously associated with other cancer types (rs7705526, in TERT intron 1), and this SNP has been shown to alter TERT promoter activity. One of the novel associations (rs13174814) maps to a second region in the TERT promoter and the other (rs62329728) is in the promoter region of CLPTM1L; neither are correlated with previously reported cancer-associated SNPs. Using TCGA RNASeq data, we found significantly increased expression of both TERT and CLPTM1L in endometrial cancer tissue compared with normal tissue (TERT P = 1.5 × 10(-18), CLPTM1L P = 1.5 × 10(-19)). Our study thus reports a novel endometrial cancer risk locus and expands the spectrum of cancer types associated with genetic variation at 5p15, further highlighting the importance of this region for cancer susceptibility. ispartof: Human Genetics vol:134 issue:2 pages:231-45 ispartof: location:Germany status: published

Published

2015

44. FOXP1 and TP63 involvement in the progression of myelodysplastic syndrome with 5q- and additional cytogenetic abnormalities

Author

Claudio Agostinelli, Alberto L'Abbate, Michelina Coco, Lucia Anna Muscarella, Crocifissa Lo Cunsolo, Clelia Tiziana Storlazzi, Nicoletta Testoni, Carla Minoia, Cristina Mecucci, Simona Salati, Ettore Macrì, Enrico Tagliafico, Attilio Guarini, Giacoma De Tullio, P. Iuzzolino, Claudio Doglioni, Alberto L’Abbate, Crocifissa Lo Cunsolo, Ettore Macrì, Paolo Iuzzolino, Cristina Mecucci, Claudio Doglioni, Michelina Coco, Lucia Muscarella, Simona Salati, Enrico Tagliafico, Carla Minoia, Giacoma De Tullio, Attilio Guarini, Nicoletta Testoni, Claudio Agostinelli, and Clelia Storlazzi

Subjects

Cancer Research, Case Report, Chromosomal translocation, Translocation, Genetic, Pathogenesis, hemic and lymphatic diseases, Gene activation, TP53, In Situ Hybridization, Fluorescence, In Situ Hybridization, Myeloid leukemia, Forkhead Transcription Factors, FOXP1, Prognosis, Oncology, Pair 3, Disease Progression, Chromosomes, Human, Pair 5, Female, Chromosomes, Human, Pair 3, TP63, Pair 5, Human, Tumor suppressor gene, Translocation, Biology, 5q, Double inversion, Chromosomes, Fluorescence, Genetic, medicine, Genetics, Humans, Aged, Chromosome Aberrations, Myelodysplastic syndromes, Tumor Suppressor Proteins, Myelodysplastic Syndromes, Repressor Proteins, Transcription Factors, medicine.disease, Chromosome 3, Cancer research, MYELODYSPLASTIC SYNDROMES (MDS)

Abstract

BACKGROUND: The progression of low-risk del(5q) myelodysplastic syndrome to acute myeloid leukemia is increased when associated with mutations of TP53, or with additional chromosomal abnormalities. However, to date the prognostic impact and molecular consequences of these rearrangements were poorly investigated. Single additional alterations to del(5q) by balanced chromosome rearrangements were rarely found in myelodysplasia. In particular, balanced alterations involving TP63 and FOXP1 genes were never reported in the literature. CASE PRESENTATION: Here we report on a 79-year woman with an aggressive form of myelodysplastic syndrome with del(5q), no TP53 mutation, and a novel complex rearrangement of chromosome 3 in bone marrow cells. Our results revealed that the FOXP1 and TP63 genes were both relocated along chromosome 3. Strikingly, immunohistochemistry analysis showed altered protein levels, disclosing that this rearrangement triggered the expression of FOXP1 and TP63 genes. FOXP1 was also found activated in other patients with myelodysplasia and acute myeloid leukemia, showing that it is an important, recurrent event. CONCLUSIONS:We document an apparent role of FOXP1 and TP63, up to now poorly documented, in the progression of MDS in our patient who is lacking mutations in the TP53 tumor suppressor gene normally associated with poor outcome in myelodysplastic syndrome with 5q-. Finally, our results may suggest a possible broader role of FOXP1 in the pathogenesis and progression of myelodysplasia and acute myeloid leukemia.

Published

2014

45. Cri-du-chat syndrome: clinical profile and prenatal diagnosis

Author

Tullu M, Muranjan M, Sharma S, Sahu D, Swami S, Deshmukh C, and Bharucha B

Subjects

Cri-du-Chat Syndrome, Male, diagnosis, lcsh:R, Infant, lcsh:Medicine, Case Report, Genetic Counseling, Chromosomes, Fatal Outcome, Pregnancy, Prenatal Diagnosis, embryonic structures, genetics, Female, Pair 5, reproductive and urinary physiology, Human

Abstract

Prenatal diagnosis of cri-du-chat syndrome is described in 2 pregnancies. In Case 1, the mother was a balanced translocation carrier and had 2 previously affected off springs. Prenatal diagnosis by chorion villus sampling and cordocentesis was successful in diagnosing an affected conceptus and the pregnancy was electively terminated. Case 2 was referred for nonimmune foetal hydrops and cordocentesis revealed deletion 5p. This second case was noteworthy for the fact that deletion 5p has not been reported to cause foetal hydrops.

Published

1998

46. A Genome-Wide Association Study of Depressive Symptoms

Author

Jari Lahti, Anne B. Newman, Vilmundur Gudnason, Aarno Palotie, Elisabeth Widen, Alessandra Cannas, Eric B. Rimm, Alexander Teumer, Toshiko Tanaka, Alan D. Penman, Ben A. Oostra, Andrea Schulz, Joshua M. Shulman, Luigi Ferrucci, Eric M. Reiman, Majken K. Jensen, Jens Baumert, Karestan C. Koenen, Shaun Purcell, Karl-Heinz Ladwig, Antonio Terracciano, David J. Llewellyn, Eco J. C. de Geus, Albert V. Smith, Kathryn L. Lunetta, Marilyn C. Cornelis, Osorio Meirelles, Brenda W.J.H. Penninx, Henry Völzke, Henning Tiemeier, Kristin D. Marciante, Emelia J. Benjamin, Maris Kuningas, Luke C. Pilling, Rajesh Rawal, Cornelis L. Mulder, David A. Bennett, David J. Hunter, Ana V. Diez-Roux, Rebecca T. Emeny, Yan V. Sun, Peter Kraft, Sharon L.R. Kardia, André G. Uitterlinden, Nona Sotoodehnia, Katri Räikkönen, Jerome I. Rotter, Erin Bakshis, Kristine Yaffe, Cornelia M. van Duijn, Lei Yu, Bruce M. Psaty, Philip L. De Jager, Margaret Kelly-Hayes, Hans J. Grabe, Angelina R. Sutin, Antonella Mulas, Anna Murray, Astrid Petersmann, Denis A. Evans, Gary C. Curhan, David Melzer, Frank B. Hu, Mike A. Nalls, Thomas H. Mosley, Lenore J. Launer, Myriam Fornage, Joanne M. Murabito, Laura H. Coker, Najaf Amin, Joseph M. Massaro, Alan B. Zonderman, Thomas Illig, Johan G. Eriksson, Ayse Demirkan, Francesco Cucca, Dorret I. Boomsma, Tamara B. Harris, Nicole Vogelzangs, Yongmei Liu, Jingzhong Ding, Kenneth Rice, Stefania Bandinelli, Albert Hofman, Andrew B. Singleton, Karin Hek, Biological Psychology, Neuroscience Campus Amsterdam - Neurobiology of Mental Health, Neuroscience Campus Amsterdam - Brain Mechanisms in Health & Disease, Neuroscience Campus Amsterdam - Brain Imaging Technology, EMGO+ - Mental Health, Psychiatry, NCA - Brain mechanisms in health and disease, NCA - Neurobiology of mental health, EMGO - Mental health, NCA - Brain imaging technology, Epidemiology, Immunology, Clinical Genetics, and Internal Medicine

Subjects

Male, Oncology, DISORDER, Netherlands Twin Register (NTR), CHARGE consortium, Genome-wide association study, Medical and Health Sciences, 0302 clinical medicine, depressive symptoms, Polymorphism (computer science), Epidemiology, 80 and over, 2.1 Biological and endogenous factors, genetics, Aetiology, Depression (differential diagnoses), POPULATION, Psychiatry, Aged, 80 and over, Genetics, 0303 health sciences, education.field_of_study, Depression, Single Nucleotide, Biological Sciences, Middle Aged, Center for Epidemiologic Studies Depression Scale, 3. Good health, Mental Health, Meta-analysis, depression, Chromosomes, Human, Pair 5, Female, Pair 5, Psychology, VITAL EXHAUSTION, Human, medicine.medical_specialty, CES-D, LIFE EVENTS, Population, Single-nucleotide polymorphism, ATHEROSCLEROSIS RISK, and over, Polymorphism, Single Nucleotide, Chromosomes, Article, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Internal medicine, Behavioral and Social Science, medicine, LINKAGE, Humans, Genetic Predisposition to Disease, Polymorphism, education, Biological Psychiatry, METAANALYSIS, Aged, 030304 developmental biology, genome-wide association study, Human Genome, Psychology and Cognitive Sciences, MAJOR DEPRESSION, GENE, Brain Disorders, meta-analysis, 030217 neurology & neurosurgery

Abstract

Background: Depression is a heritable trait that exists on a continuum of varying severity and duration. Yet, the search for genetic variants associated with depression has had few successes. We exploit the entire continuum of depression to find common variants for depressive symptoms.Methods: In this genome-wide association study, we combined the results of 17 population-based studies assessing depressive symptoms with the Center for Epidemiological Studies Depression Scale. Replication of the independent top hits (p Results: The discovery sample comprised 34,549 individuals (mean age of 66.5) and no loci reached genome-wide significance (lowest p = 1.05 x 10(-7)). Seven independent single nucleotide polymorphisms were considered for replication. In the replication set (n = 16,709), we found suggestive association of one single nucleotide polymorphism with depressive symptoms (rs161645, 5q21, p = 9.19 x 10(-3)). This 5q21 region reached genome-wide significance (p = 4.78 x 10(-8)) in the overall meta-analysis combining discovery and replication studies (n = 51,258).Conclusions: The results suggest that only a large sample comprising more than 50,000 subjects may be sufficiently powered to detect genes for depressive symptoms.

Published

2013

47. Identification and characterization of a spinal muscular atrophy-determining gene

Author

Jean Weissenbach, Lydie Burglen, Olivier Clermont, Philippe Burlet, Judith Melki, Corinne Cruaud, Denis Le Paslier, Sophie Reboullet, Suzie Lefebvre, Massimo Zeviani, Daniel Cohen, Bernard Bénichou, Philippe Millasseau, Arnold Munnich, Louis Viollet, and Jean Frézal

Subjects

Male, SMN1, Spinal Muscular Atrophies of Childhood, Polymerase Chain Reaction, Exon, Cyclic AMP Response Element-Binding Protein, Southern, Polymorphism, Single-Stranded Conformational, Genetics, Gel, Blotting, Single-Stranded Conformational, Chromosome Mapping, RNA-Binding Proteins, SMN Complex Proteins, Exons, Telomere, Electrophoresis, Gel, Pulsed-Field, Blotting, Southern, Multigene Family, Artificial, Chromosomes, Human, Pair 5, Nusinersen, Female, Pair 5, Human, Electrophoresis, Genetic Markers, RNA Splicing, Molecular Sequence Data, Nerve Tissue Proteins, Biology, General Biochemistry, Genetics and Molecular Biology, Chromosomes, Pulsed-Field, medicine, PLS3, Humans, Amino Acid Sequence, Polymorphism, Chromosomes, Artificial, Yeast, Proximal spinal muscular atrophy, Base Sequence, Gene Deletion, Mutation, Biochemistry, Genetics and Molecular Biology(all), Survival of motor neuron, Spinal muscular atrophy, medicine.disease, Spinal muscular atrophies, Molecular biology, Yeast

Abstract

Spinal muscular atrophy (SMA) is a common fatal autosomal recessive disorder characterized by degeneration of lower motor neurons, leading to progressive paralysis with muscular atrophy. The gene for SMA has been mapped to chromosome 5q13, where large-scale deletions have been reported. We describe here the inverted duplication of a 500 kb element in normal chromosomes and narrow the critical region to 140 kb within the telomeric region. This interval contains a 20 kb gene encoding a novel protein of 294 amino acids. An highly homologous gene is present in the centromeric element of 95% of controls. The telomeric gene is either lacking or interrupted in 226 of 229 patients, and patients retaining this gene (3 of 229) carry either a point mutation (Y272C) or short deletions in the consensus splice sites of introns 6 and 7. These data suggest that this gene, termed the survival motor neuron (SMN) gene, is an SMA-determining gene.

Published

1995

48. Thyroid cancer susceptibility polymorphisms: confirmation of loci on chromosomes 9q22 and 14q13, validation of a recessive 8q24 locus and failure to replicate a locus on 5q24

Author

Jones, A.M., Howarth, K.M., Martin, L., Gorman, M., Mihai, R., Moss, L., Auton, A., Lemon, C., Mehanna, H., Mohan, H., Clarke, S.E.M., Wadsley, J., Macias, E., Coatesworth, A., Beasley, M., Roques, T., Martin, C., Ryan, P., Gerrard, G., Power, D., Bremmer, C., The TCUKIN Consortium, ., Tomlinson, I., and Carvajal-Carmona, L.G.

Subjects

Genetics & Heredity, Pair 14, DNA, Single Nucleotide, Biological Sciences, Medical and Health Sciences, Chromosomes, Linkage Disequilibrium, MicroRNAs, Haplotypes, Genes, TCUKIN Consortium, Genetic Loci, Pair 8, Humans, Recessive, Genetic Predisposition to Disease, Thyroid Neoplasms, Pair 5, Polymorphism, Sequence Analysis, Genetic Association Studies, Human, Pair 9

Abstract

Five single nucleotide polymorphisms (SNPs) associated with thyroid cancer (TC) risk have been reported: rs2910164 (5q24); rs6983267 (8q24); rs965513 and rs1867277 (9q22); and rs944289 (14q13). Most of these associations have not been replicated in independent populations and the combined effects of the SNPs on risk have not been examined. This study genotyped the five TC SNPs in 781 patients recruited through the TCUKIN study. Genotype data from 6122 controls were obtained from the CORGI and Wellcome Trust Case-Control Consortium studies. Significant associations were detected between TC and rs965513A (p=6.35×10(-34)), rs1867277A (p=5.90×10(-24)), rs944289T (p=6.95×10(-7)), and rs6983267G (p=0.016). rs6983267 was most strongly associated under a recessive model (P(GG vs GT + TT)=0.004), in contrast to the association of this SNP with other cancer types. However, no evidence was found of an association between rs2910164 and disease under any risk model (p>0.7). The rs1867277 association remained significant (p=0.008) after accounting for genotypes at the nearby rs965513 (p=2.3×10(-13)) and these SNPs did not tag a single high risk haplotype. The four validated TC SNPs accounted for a relatively large proportion (∼11%) of the sibling relative risk of TC, principally owing to the large effect size of rs965513 (OR 1.74).

Published

2012

49. Segment-Wise Genome-Wide Association Analysis Identifies a Candidate Region Associated with Schizophrenia in Three Independent Samples

Author

Douglas F. Levinson, Markus M. Nöthen, Marcella Rietschel, Jianxin Shi, Sven Cichon, Manuel Mattheisen, René Breuer, Roel A. Ophoff, Genetic Risk, Pablo V. Gejman, Thomas E. Gladwin, Thomas G. Schulze, Eske M. Derks, Arking, Dan E, Germeys, Inez, Arking, Dan E., Psychiatrie & Neuropsychologie, RS: MHeNs School for Mental Health and Neuroscience, Amsterdam Neuroscience, Amsterdam Public Health, and Adult Psychiatry

Subjects

lcsh:Medicine, Genome-wide association study, Genetic analysis, Genome, 0302 clinical medicine, complex disorders, schizophrenia, genetic variants, 2.1 Biological and endogenous factors, Aetiology, lcsh:Science, Psychiatry, Genetics, 0303 health sciences, Multidisciplinary, Chromosome Mapping, Genomics, 3. Good health, Mental Health, Medicine, Chromosomes, Human, Pair 5, ddc:500, Pair 5, Research Article, Human, General Science & Technology, Binomial test, Single-nucleotide polymorphism, Biology, Genome Complexity, Chromosomes, 03 medical and health sciences, Genetic variation, Genome-Wide Association Studies, Humans, Genetic Predisposition to Disease, Gene Networks, Genetic Association Studies, 030304 developmental biology, Genetic Risk and Outcome of Psychosis, Human Genome, lcsh:R, Chromosome, Human Genetics, Brain Disorders, Sample size determination, Case-Control Studies, Genetics of Disease, Genetic Polymorphism, Schizophrenia, Structural Genomics, lcsh:Q, Population Genetics, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

Recent studies suggest that variation in complex disorders (e.g., schizophrenia) is explained by a large number of genetic variants with small effect size (Odds Ratio ≈ 1.05-1.1). The statistical power to detect these genetic variants in Genome Wide Association (GWA) studies with large numbers of cases and controls (v 15,000) is still low. As it will be difficult to further increase sample size, we decided to explore an alternative method for analyzing GWA data in a study of schizophrenia, dramatically reducing the number of statistical tests. The underlying hypothesis was that at least some of the genetic variants related to a common outcome are collocated in segments of chromosomes at a wider scale than single genes. Our approach was therefore to study the association between relatively large segments of DNA and disease status. An association test was performed for each SNP and the number of nominally significant tests in a segment was counted. We then performed a permutation-based binomial test to determine whether this region contained significantly more nominally significant SNPs than expected under the null hypothesis of no association, taking linkage into account. Genome Wide Association data of three independent schizophrenia case/control cohorts with European ancestry (Dutch, German, and US) using segments of DNA with variable length (2 to 32 Mbp) was analyzed. Using this approach we identified a region at chromosome 5q23.3-q31.3 (128-160 Mbp) that was significantly enriched with nominally associated SNPs in three independent case-control samples. We conclude that considering relatively wide segments of chromosomes may reveal reliable relationships between the genome and schizophrenia, suggesting novel methodological possibilities as well as raising theoretical questions. ispartof: PLoS One vol:7 issue:6 ispartof: location:United States status: published

Published

2012

50. Confirmation of 5p12 As a Susceptibility Locus for Progesterone-Receptor-Positive, Lower Grade Breast Cancer

Author

Peter Hillemanns, Roger L. Milne, Chiun-Sheng Huang, Jan Lubinski, Arif B. Ekici, Rita K. Schmutzler, Julian Peto, Qin Wang, Rob A. E. M. Tollenaar, Børge G. Nordestgaard, Chen-Yang Shen, Paolo Radice, Nicola Miller, Barbara Burwinkel, Suleeporn Sangrajrang, Núria Malats, James McKay, Gianluca Severi, Ian Tomlinson, Dong-Young Noh, Irene L. Andrulis, Xiaoqing Chen, Esther M. John, Katarzyna Durda, Anna Marie Mulligan, Anne Lise Børrensen-Dale, Frederik Marmé, Simon S. Cross, Elza Khusnutdinova, Joerg Heil, Gillian S. Dite, Melissa C. Southey, Thilo Dörk, Peter Kraft, Monica Barile, Graeme Elliot, Olivia Fletcher, Yuri I. Rogov, Arto Mannermaa, Nazneen Rahman, Annegien Broeks, Susan E. Hankinson, Xianshu Wang, Natalia Bogdanova, Mark E. Sherman, Volker Harth, Johann H. Karstens, Montserrat Garcia-Closas, Robert Winqvist, Alfons Meindl, Rebecca Hein, Laura J. van't Veer, Stefan Nickels, Manjeet K. Humphreys, Valerie Gaborieau, Lorna Gibson, Jose Ignacio Arias Perez, Giuseppe Floris, Christa Stegmaier, Gord Glendon, Heiko Müller, Marjanka K. Schmidt, Jonine D. Figueroa, Julia A. Knight, Graham G. Giles, Siranoush Manoukian, Ming-Feng Hou, Albina Farahtdinova, Gilles Thomas, Diether Lambrechts, Anna Jakubowska, Paul D.P. Pharoah, Alexander Miron, Michael J. Kerin, Iosif V. Zalutsky, Ian W. Brock, Laura Baglietto, Argyrios Ziogas, Claus R. Bartram, John L. Hopper, Marina Bermisheva, Grethe I. Grenaker Alnæs, Jaana M. Hartikainen, Sei Hyun Ahn, Hermann Brenner, Paul Brennan, Dieter Flesch-Janys, Stephen J. Chanock, Robert N. Hoover, Fergus J. Couch, Georgia Chenevix-Trench, Anthony Renwick, Sheila Seal, Mervi Grip, Matthias W. Beckmann, Karin Leunen, Javier Benitez, Peter Schürmann, Vesa Kataja, Arja Jukkola-Vuorinen, Peter A. Fasching, David J. Hunter, Christian M. Bayer, Rogier A. Oldenburg, Karen A. Pooley, Antoinette Hollestelle, Hoda Anton-Culver, Veli-Matti Kosma, P. Zamora, Jonathan Beesley, Paolo Peterlongo, Darya Prokofieva, Keun-Young Yoo, Isabel dos Santos Silva, Katarzyna Jaworska, Janet E. Olson, Carmel Apicella, U Hamann, Jyh-Cherng Yu, Shan Wang-Gohrke, Natalia Antonenkova, Sara Lindström, Andreas Schneeweiss, Katri Pylkäs, Douglas F. Easton, Charlotte Lanng, Alison M. Dunning, Vessela N. Kristensen, Daehee Kang, Elinor J. Sawyer, Jolanta Lissowska, Christina Justenhoven, Zachary S. Fredericksen, Madeleine M.A. Tilanus-Linthorst, Angela Cox, Maartje J. Hooning, Volker Arndt, Christof Sohn, Betül T. Yesilyurt, Jenny Chang-Claude, Ellen L. Goode, Stig E. Bojesen, Clare Turnbull, Medical Oncology, Clinical Genetics, and Surgery

Subjects

Oncology, Epidemiology, Estrogen receptor, Noninfiltrating, Cohort Studies, 0302 clinical medicine, Risk Factors, Ductal, Receptors, common variants, Breast, Progesterone, risk, 0303 health sciences, subtypes, Carcinoma, Ductal, Breast, Breast Neoplasms, Carcinoma, Intraductal, Noninfiltrating, Case-Control Studies, Chromosomes, Human, Pair 5, Female, Follow-Up Studies, Humans, Neoplasm Grading, Polymorphism, Single Nucleotide, Prognosis, Receptors, Estrogen, Receptors, Progesterone, Genetic Predisposition to Disease, Single Nucleotide, 3. Good health, 030220 oncology & carcinogenesis, alleles, Pair 5, Human, medicine.medical_specialty, Intraductal, Biology, Article, Chromosomes, 03 medical and health sciences, Breast cancer, SDG 3 - Good Health and Well-being, Internal medicine, Progesterone receptor, medicine, Genetic predisposition, Carcinoma, Polymorphism, 030304 developmental biology, Gynecology, Case-control study, Ductal carcinoma, confer susceptibility, medicine.disease, Estrogen, genome-wide association, Histopathology

Abstract

Background: The single-nucleotide polymorphism (SNP) 5p12-rs10941679 has been found to be associated with risk of breast cancer, particularly estrogen receptor (ER)-positive disease. We aimed to further explore this association overall, and by tumor histopathology, in the Breast Cancer Association Consortium. Methods: Data were combined from 37 studies, including 40,972 invasive cases, 1,398 cases of ductal carcinoma in situ (DCIS), and 46,334 controls, all of white European ancestry, as well as 3,007 invasive cases and 2,337 controls of Asian ancestry. Associations overall and by tumor invasiveness and histopathology were assessed using logistic regression. Results: For white Europeans, the per-allele OR associated with 5p12-rs10941679 was 1.11 (95% CI = 1.08–1.14, P = 7 × 10−18) for invasive breast cancer and 1.10 (95% CI = 1.01–1.21, P = 0.03) for DCIS. For Asian women, the estimated OR for invasive disease was similar (OR = 1.07, 95%CI = 0.99–1.15, P = 0.09). Further analyses suggested that the association in white Europeans was largely limited to progesterone receptor (PR)-positive disease (per-allele OR = 1.16, 95% CI = 1.12–1.20, P = 1 × 10−18 vs. OR = 1.03, 95% CI = 0.99–1.07, P = 0.2 for PR-negative disease; Pheterogeneity = 2 × 10−7); heterogeneity by ER status was not observed (P = 0.2) once PR status was accounted for. The association was also stronger for lower grade tumors [per-allele OR (95% CI) = 1.20 (1.14–1.25), 1.13 (1.09–1.16), and 1.04 (0.99–1.08) for grade 1, 2, and 3/4, respectively; Ptrend = 5 × 10−7]. Conclusion: 5p12 is a breast cancer susceptibility locus for PR-positive, lower grade breast cancer. Impact: Multicenter fine-mapping studies of this region are needed as a first step to identifying the causal variant or variants. Cancer Epidemiol Biomarkers Prev; 20(10); 2222–31. ©2011 AACR.

Published

2011