Your search keyword '"GENETIC epidemiology"' showing total 90 results

1. Population-based targeted sequencing of 54 candidate genes identifies PALB2 as a susceptibility gene for high-grade serous ovarian cancer

Author

Song, Honglin, Dicks, Ed M, Tyrer, Jonathan, Intermaggio, Maria, Chenevix-Trench, Georgia, Bowtell, David D, Traficante, Nadia, Group, AOCS, Brenton, James, Goranova, Teodora, Hosking, Karen, Piskorz, Anna, van Oudenhove, Elke, Doherty, Jen, Harris, Holly R, Rossing, Mary Anne, Duerst, Matthias, Dork, Thilo, Bogdanova, Natalia V, Modugno, Francesmary, Moysich, Kirsten, Odunsi, Kunle, Ness, Roberta, Karlan, Beth Y, Lester, Jenny, Jensen, Allan, Kjaer, Susanne Krüger, Høgdall, Estrid, Campbell, Ian G, Lázaro, Conxi, Pujara, Miguel Angel, Cunningham, Julie, Vierkant, Robert, Winham, Stacey J, Hildebrandt, Michelle, Huff, Chad, Li, Donghui, Wu, Xifeng, Yu, Yao, Permuth, Jennifer B, Levine, Douglas A, Schildkraut, Joellen M, Riggan, Marjorie J, Berchuck, Andrew, Webb, Penelope M, Group, OPAL Study, Cybulski, Cezary, Gronwald, Jacek, Jakubowska, Anna, Lubinski, Jan, Alsop, Jennifer, Harrington, Patricia, Chan, Isaac, Menon, Usha, Pearce, Celeste L, Wu, Anna H, de Fazio, Anna, Kennedy, Catherine J, Goode, Ellen, Ramus, Susan, Gayther, Simon, and Pharoah, Paul

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Oncology and Carcinogenesis, Orphan Drug, Ovarian Cancer, Prevention, Clinical Research, Rare Diseases, Cancer, 2.1 Biological and endogenous factors, Aetiology, Case-Control Studies, Fanconi Anemia Complementation Group N Protein, Female, Genetic Predisposition to Disease, Genetic Variation, Humans, Ovarian Neoplasms, Risk Assessment, cancer, endocrine, genetic epidemiology, cancer: endocrine, Medical and Health Sciences, Genetics & Heredity, Clinical sciences

Abstract

PurposeThe known epithelial ovarian cancer (EOC) susceptibility genes account for less than 50% of the heritable risk of ovarian cancer suggesting that other susceptibility genes exist. The aim of this study was to evaluate the contribution to ovarian cancer susceptibility of rare deleterious germline variants in a set of candidate genes.MethodsWe sequenced the coding region of 54 candidate genes in 6385 invasive EOC cases and 6115 controls of broad European ancestry. Genes with an increased frequency of putative deleterious variants in cases versus controls were further examined in an independent set of 14 135 EOC cases and 28 655 controls from the Ovarian Cancer Association Consortium and the UK Biobank. For each gene, we estimated the EOC risks and evaluated associations between germline variant status and clinical characteristics.ResultsThe ORs associated for high-grade serous ovarian cancer were 3.01 for PALB2 (95% CI 1.59 to 5.68; p=0.00068), 1.99 for POLK (95% CI 1.15 to 3.43; p=0.014) and 4.07 for SLX4 (95% CI 1.34 to 12.4; p=0.013). Deleterious mutations in FBXO10 were associated with a reduced risk of disease (OR 0.27, 95% CI 0.07 to 1.00, p=0.049). However, based on the Bayes false discovery probability, only the association for PALB2 in high-grade serous ovarian cancer is likely to represent a true positive.ConclusionsWe have found strong evidence that carriers of PALB2 deleterious mutations are at increased risk of high-grade serous ovarian cancer. Whether the magnitude of risk is sufficiently high to warrant the inclusion of PALB2 in cancer gene panels for ovarian cancer risk testing is unclear; much larger sample sizes will be needed to provide sufficiently precise estimates for clinical counselling.

Published

2021

2. Risk of metastatic pheochromocytoma and paraganglioma in SDHx mutation carriers: a systematic review and updated meta-analysis

Author

Junho Kang, Seongdo Jeong, Hokeun Sun, Je-Keun Rhee, Hansong Lee, Yeuni Yu, and Yun Hak Kim

Subjects

Oncology, medicine.medical_specialty, business.industry, SDHB, SDHA, 030209 endocrinology & metabolism, medicine.disease, Metastasis, Pheochromocytoma, 03 medical and health sciences, 0302 clinical medicine, Genetic epidemiology, Paraganglioma, 030220 oncology & carcinogenesis, Internal medicine, Mutation (genetic algorithm), Genetics, Medicine, SDHD, business, Genetics (clinical)

Abstract

BackgroundPheochromocytoma and paraganglioma (PPGL) are tumours that arise from chromaffin cells. Some genetic mutations influence PPGL, among which, those in genes encoding subunits of succinate dehydrogenase (SDHA, SDHB, SDHC and SDHD) and assembly factor (SDHAF2) are the most relevant. However, the risk of metastasis posed by these mutations is not reported except for SDHB and SDHD mutations. This study aimed to update the metastatic risks, considering prevalence and incidence of each SDHx mutation, which were dealt formerly all together.MethodsWe searched EMBASE and MEDLINE and selected 27 articles. The patients included in the studies were divided into three groups depending on the presence of PPGL. We checked the heterogeneity between studies and performed a meta-analysis using Hartung-Knapp-Sidik-Jonkman method based on a random effect model.ResultsThe highest PPGL prevalence was for SDHB mutation, ranging from 23% to 31%, and for SDHC mutation (23%), followed by that for SDHA mutation (16%). The lowest prevalence was for SDHD mutation, ranging from 6% to 8%. SDHAF2 mutation showed no metastatic events. The PPGL incidence showed a tendency similar to that of its prevalence with the highest risk of metastasis posed by SDHB mutation (12%–41%) and the lowest risk by SDHD mutation (~4%).ConclusionThere was no integrated evidence of how SDHx mutations are related to metastatic PPGL. However, these findings suggest that SDHA, SDHB and SDHC mutations are highly associated and should be tested as indicators of metastasis in patients with PPGL.

Published

2019

3. Genetic characteristics of retinitis pigmentosa in 1204 Japanese patients

Author

Chihiro Inai, Yuko Wada, Kentaro Kurata, Hiroko Terasaki, Koji M. Nishiguchi, Tatsuro Ishibashi, Yoshito Koyanagi, Yukihide Momozawa, Yusuke Murakami, Yoichiro Kamatani, Koh Hei Sonoda, Toshiaki Hirakata, Sadaaki Takata, Kazuko Omodaka, Shiori Komori, Yoshihiro Hotta, Shinji Ueno, Yusuke Iwasaki, Akira Murakami, Katsuhiro Hosono, Michiaki Kubo, Yasuhiro Ikeda, Toru Nakazawa, Toshiaki Abe, Mikako Kumano, Dan Gao, and Masato Akiyama

Subjects

Adult, Male, 0301 basic medicine, PRPF31, Adolescent, Population, Gene mutation, Biology, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Asian People, Gene Frequency, Japan, PDE6B, Retinitis pigmentosa, Genetics, medicine, Humans, Child, education, Gene, Genetics (clinical), Aged, Aged, 80 and over, education.field_of_study, Genetic Variation, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Middle Aged, medicine.disease, Minor allele frequency, 030104 developmental biology, Genetic epidemiology, Child, Preschool, Mutation, 030221 ophthalmology & optometry, Female, Usher Syndromes, Retinitis Pigmentosa

Abstract

BackgroundThe genetic profile of retinitis pigmentosa (RP) in East Asian populations has not been well characterised. Therefore, we conducted a large-scale sequencing study to investigate the genes and variants causing RP in a Japanese population.MethodsA total of 1209 Japanese patients diagnosed with typical RP were enrolled. We performed deep resequencing of 83 known causative genes of RP using next-generation sequencing. We defined pathogenic variants as those that were putatively deleterious or registered as pathogenic in the Human Gene Mutation Database or ClinVar database and had a minor allele frequency in any ethnic population of ≤0.5% for recessive genes or ≤0.01% for dominant genes as determined using population-based databases.ResultsWe successfully sequenced 1204 patients with RP and determined 200 pathogenic variants in 38 genes as the cause of RP in 356 patients (29.6%). Variants in six genes (EYS, USH2A, RP1L1, RHO, RP1 and RPGR) caused RP in 65.4% (233/356) of those patients. Among autosomal recessive genes, two known founder variants in EYS [p.(Ser1653fs) and p.(Tyr2935*)] and four East Asian-specific variants [p.(Gly2752Arg) in USH2A, p.(Arg658*) in RP1L1, p.(Gly2186Glu) in EYS and p.(Ile535Asn) in PDE6B] and p.(Cys934Trp) in USH2A were found in ≥10 patients. Among autosomal dominant genes, four pathogenic variants [p.(Pro347Leu) in RHO, p.(Arg872fs) in RP1, p.(Arg41Trp) in CRX and p.(Gly381fs) in PRPF31] were found in ≥4 patients, while these variants were unreported or extremely rare in both East Asian and non-East Asian population-based databases.ConclusionsEast Asian-specific variants in causative genes were the major causes of RP in the Japanese population.

Published

2019

4. Addition of a 161-SNP polygenic risk score to family history-based risk prediction: impact on clinical management in non-BRCA1/2breast cancer families

Author

Mar Rodríguez-Girondo, Edith Olah, Andy C. H. Lee, Hanne Meijers-Heijboer, Christi J. van Asperen, Maaike P.G. Vreeswijk, Nicoline Hoogerbrugge, Peter Devilee, Caroline Seynaeve, Jan C. Oosterwijk, Florentine Hilbers, Inge M. M. Lakeman, Antoinette Hollestelle, Hans F. A. Vasen, Human genetics, CCA - Cancer Treatment and quality of life, Amsterdam Neuroscience - Complex Trait Genetics, Epidemiology and Data Science, Amsterdam Reproduction & Development (AR&D), Targeted Gynaecologic Oncology (TARGON), Damage and Repair in Cancer Development and Cancer Treatment (DARE), Medical Oncology, Lakeman, Inge MM [0000-0002-2990-7154], Vreeswijk, Maaike PG [0000-0003-4068-9271], Apollo - University of Cambridge Repository, Academic Medical Center, and ARD - Amsterdam Reproduction and Development

Subjects

0301 basic medicine, Oncology, 030105 genetics & heredity, cancer: breast, 0302 clinical medicine, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Medicine, Family history, skin and connective tissue diseases, Genetics (clinical), Aged, 80 and over, education.field_of_study, Disease Management, Middle Aged, Prognosis, Pedigree, 030220 oncology & carcinogenesis, Medical genetics, Adult, medicine.medical_specialty, genetic epidemiology, Genotype, Clinical Decision-Making, Population, Breast Neoplasms, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Risk Assessment, Young Adult, 03 medical and health sciences, Breast cancer, SDG 3 - Good Health and Well-being, Internal medicine, Biomarkers, Tumor, Genetics, Humans, Genetic Predisposition to Disease, education, Alleles, Genetic Association Studies, Aged, Proportional Hazards Models, Genetic association, business.industry, Cancer, genetic screening/counselling, medicine.disease, Genetic epidemiology, Case-Control Studies, polygenic risk score, business, clinical genetics

Abstract

BackgroundThe currently known breast cancer-associated single nucleotide polymorphisms (SNPs) are presently not used to guide clinical management. We explored whether a genetic test that incorporates a SNP-based polygenic risk score (PRS) is clinically meaningful in non-BRCA1/2high-risk breast cancer families.Methods101 non-BRCA1/2high-risk breast cancer families were included; 323 cases and 262 unaffected female relatives were genotyped. The 161-SNP PRS was calculated and standardised to 327 population controls (sPRS). Association analysis was performed using a Cox-type random effect regression model adjusted by family history. Updated individualised breast cancer lifetime risk scores were derived by combining the Breast and Ovarian Analysis of Disease Incidence and Carrier Estimation Algorithm breast cancer lifetime risk with the effect of the sPRS.ResultsThe mean sPRS for cases and their unaffected relatives was 0.70 (SD=0.9) and 0.53 (SD=0.9), respectively. A significant association was found between sPRS and breast cancer, HR=1.16, 95% CI 1.03 to 1.28, p=0.026. Addition of the sPRS to risk prediction based on family history alone changed screening recommendations in 11.5%, 14.7% and 19.8 % of the women according to breast screening guidelines from the USA (National Comprehensive Cancer Network), UK (National Institute for Health and Care Excellence and the Netherlands (Netherlands Comprehensive Cancer Organisation), respectively.ConclusionOur results support the application of the PRS in risk prediction and clinical management of women from genetically unexplained breast cancer families.

Published

2019

5. CM-Score: a validated scoring system to predict CDKN2A germline mutations in melanoma families from Northern Europe

Author

Potjer, T.P., Helgadottir, H., Leenheer, M., Stoep, N. van der, Gruis, N.A., Hoiom, V., Olsson, H., Doorn, R. van, Vasen, H.F.A., Asperen, C.J. van, Dekkers, O.M., Hes, F.J., Dutch Working Grp Clinical Onc, and Medical Genetics

Subjects

cancer: head and neck, 0301 basic medicine, Oncology, medicine.medical_specialty, genetic epidemiology, Logistic regression, head and neck, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, cancer: dermatological, CDKN2A, Internal medicine, Genetics, Medicine, neoplasms, Genetics (clinical), Cancer, Medicine(all), business.industry, Area under the curve, genetic screening/counselling, genetic screening, medicine.disease, counselling, CM-Score, 030104 developmental biology, Genetic epidemiology, 030220 oncology & carcinogenesis, Cohort, Medical genetics, business, clinical genetics, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

BackgroundSeveral factors have been reported that influence the probability of a germline CDKN2A mutation in a melanoma family. Our goal was to create a scoring system to estimate this probability, based on a set of clinical features present in the patient and his or her family.MethodsFive clinical features and their association with CDKN2A mutations were investigated in a training cohort of 1227 Dutch melanoma families (13.7% with CDKN2A mutation) using multivariate logistic regression. Predefined features included number of family members with melanoma and with multiple primary melanomas, median age at diagnosis and presence of pancreatic cancer or upper airway cancer in a family member. Based on these five features, a scoring system (CDKN2A Mutation(CM)-Score) was developed and subsequently validated in a combined Swedish and Dutch familial melanoma cohort (n=421 families; 9.0% with CDKN2A mutation).ResultsAll five features were significantly associated (pCDKN2A mutation. At a CM-Score of 16 out of 49 possible points, the threshold of 10% mutation probability is approximated (9.9%; 95% CI 9.8 to 10.1). This probability further increased to >90% for families with ≥36 points. A CM-Score under 16 points was associated with a low mutation probability (≤4%). CM-Score performed well in both the training cohort (area under the curve (AUC) 0.89; 95% CI 0.86 to 0.92) and the external validation cohort (AUC 0.94; 95% CI 0.90 to 0.98).ConclusionWe developed a practical scoring system to predict CDKN2A mutation status among melanoma-prone families. We suggest that CDKN2A analysis should be recommended to families with a CM-Score of ≥16 points.

Published

2018

6. Deletion of the 5'exons of COL4A6 is not needed for the development of diffuse leiomyomatosis in patients with Alport syndrome.

Author

Nabais Sá, Maria João, Fieremans, Nathalie, de Brouwer, Arjan P. M., Sousa, Rita, Costa, Fernando Teixeira E., Brito, Maria José, Carvalho, Fernanda, Rodrigues, Márcia, de Sousa, Francisco Teixeira, Felgueiras, Joana, Neves, Fernando, Carvalho, Adelino, Ramos, Umbelina, Vizcaíno, José Ramón, Alves, Susana, Carvalho, Filipa, Froyen, Guy, and Oliveira, João Paulo

Subjects

EXONS (Genetics), GENETIC polymorphisms, ALPORT syndrome, GENETIC disorders, KIDNEY diseases, GENETIC epidemiology

Abstract

Background Alport syndrome (AS), a hereditary type IV collagen nephropathy, is a major cause of end-stage renal disease in young people. About 85% of the cases are X-linked (ATS), due to mutations in the COL4A5 gene. Rarely, families have a contiguous gene deletion comprising at least exon 1 of COL4A5 and the first exons of COL4A6, associated with the development of diffuse leiomyomatosis (ATS-DL). We report three novel deletions identified in families with AS, one of which challenges the current concepts on genotype-phenotype correlations of ATS/ATS-DL. Methods In the setting of a multicentric study aiming to describe the genetic epidemiology and molecular pathology of AS in Portugal, three novel COL4A5 deletions were identified in two families with x-linked Alport syndrome (ATS) and in one family with ATS-DL. These mutations were initially detected by PCR and Multiplex Ligation-dependent Probe Amplification, and further mapped by high-resolution X chromosomespecific oligo-array and PCR. Results In the ATS-DL family, a COL4A5 deletion spanning exons 2 through 51, extending distally beyond COL4A5 but proximally not into COL4A6, segregated with the disease phenotype. A COL4A5 deletion encompassing exons 2 through 29 was identified in one of the ATS families. In the second ATS family, a deletion of exon 13 of COL4A5 through exon 3 of COL4A6 was detected. Conclusions These observations suggest that deletion of the 50 exons of COL4A6 and of the common promoter of the COL4A5 and COL4A6 genes is not essential for the development of leiomyomatosis in patients with ATS, and that COL4A5_COL4A6 deletions extending into COL4A6 exon 3 may not result in ATS-DL. [ABSTRACT FROM AUTHOR]

Published

2013

7. Melanoma risk for CDKN2A mutation carriers who are relatives of population-based case carriers in Australia and the UK.

Author

Cust, Anne E, Harland, Mark, Makalic, Enes, Schmidt, Daniel, Dowty, James G, Aitken, Joanne F, Agha-Hamilton, Chantelle, Armstrong, Bruce K, Barrett, Jenny H, Chan, May, Chang, Yu-Mei, Gascoyne, Joanne, Giles, Graham G, Holland, Elizabeth A, Kefford, Richard F, Kukalizch, Kairen, Lowery, Johanna, Randerson-Moor, Juliette A, Schmid, Helen, and Taylor, Claire F

Abstract

Background mutations confer a substantial risk of cutaneous melanoma; however, the magnitude of risk is uncertain. Methods The study estimated the hazard ratio (HR) and the average age specific cumulative risk (ie, penetrance) of reported melanoma for mutation carriers in case families using a modified segregation analysis of the first and higher degree relatives of 35 population-based cases. The study sample included 223 relatives of 13 melanoma cases diagnosed when aged 18–39 years from Melbourne, Sydney and Brisbane, Australia, and 322 relatives of 22 melanoma cases diagnosed at any age from Yorkshire, UK. Results The estimated HR for melanoma for mutation carriers relative to the general population decreased with regions of increasing ambient ultraviolet (UV) irradiance, being higher for the UK than Australia (87, 95% CI 50 to 153 vs 31, 95% CI 20 to 50, p=0.008), and across Australia, 49 (95% CI 24 to 98) for Melbourne, 44 (95% CI 22 to 88) for Sydney, and 9 (95% CI 2 to 33) for Brisbane (p=0.02). Penetrance did not differ by geographic region. It is estimated that 16% (95% CI 10% to 27%) of UK and 20% (95% CI 13% to 30%) of Australian mutation carriers would be diagnosed with melanoma by age 50 years, and 45% (95% CI 29% to 65%) and 52% (95% CI 37% to 69%), respectively, by age 80 years. Conclusions Contrary to the strong association between UV radiation exposure and melanoma risk for the general population, mutation carriers appear to have the same cumulative risk of melanoma irrespective of the ambient UV irradiance of the region in which they live. [ABSTRACT FROM PUBLISHER]

Published

2011

8. Cranial meningiomas in 411 neurofibromatosis type 2 (NF2) patients with proven gene mutations: clear positional effect of mutations, but absence of female severity effect on age at onset.

Author

Smith, Miriam J, Higgs, Jenny E, Bowers, Naomi L, Halliday, Dorothy, Paterson, Joan, Gillespie, James, Huson, Susan M, Freeman, Simon R, Lloyd, Simon, Rutherford, Scott A, King, Andrew T, Wallace, Andrew J, Ramsden, Richard T, and Evans, D Gareth R

Abstract

Background Meningiomas have been reported to occur in approximately 50% of neurofibromatosis type 2 (NF2) patients. The gene is commonly biallelically inactivated in both schwannomas and meningiomas. The spectrum of mutations consists mainly of truncating (nonsense and frameshift) mutations. A smaller number of patients have missense mutations, which are associated with a milder disease phenotype. Methods This study analysed the cumulative incidence and gender effects as well as the genotype–phenotype correlation between the position of the mutation and the occurrence of cranial meningiomas in a cohort of 411 NF2 patients with proven mutations. Results and conclusion Patients with mutations in exon 14 or 15 were least likely to develop meningiomas. Cumulative risk of cranial meningioma to age 50 years was 70% for exons 1–3, 81% for exons 4–6, 49% for exons 7–9, 56% for exons 10–13, and 28% for exons 14–15. In the cohort of 411 patients, no overall gender bias was found for occurrence of meningioma in NF2 disease. Cumulative incidence of meningioma was close to 80% by 70 years of age for both males and females, but incidence by age 20 years was slightly increased in males (male 25%, female 18%; p=0.023). Conversely, an increased risk of meningiomas in women with mosaic NF2 disease was also found. [ABSTRACT FROM PUBLISHER]

Published

2011

9. Genetic architecture of open angle glaucoma and related determinants.

Author

Ramdas, Wishal D, Amin, Najaf, van Koolwijk, Leonieke M E, Janssens, A Cecile J W, Demirkan, Ayse, de Jong, Paulus T V M, Aulchenko, Yurii S, Wolfs, Roger C W, Hofman, Albert, Rivadeneira, Fernando, Uitterlinden, Andre G, Oostra, Ben A, Lemij, Hans G, Klaver, Caroline C W, Vingerling, Johannes R, Jansonius, Nomdo M, and van Duijn, Cornelia M

Abstract

Background Although the vertical cup-disc ratio (VCDR) and intraocular pressure (IOP) are important determinants of open angle glaucoma (OAG), it is unclear to what extent the genetic origin of these traits overlap with those of OAG. We evaluated whether the same genes that determine VCDR and IOP also predict OAG. Methods Genetic risk scores were constructed from single nucleotide polymorphisms (SNPs) using genome wide association data of 9326 participants from the Rotterdam Study cohorts (mean±SD age: 64.6±9.1 years). These risk scores were used to calculate the explained variance of VCDR and IOP in an independent cohort (Erasmus Rucphen Family study) consisting of 1646 participants (mean±SD age: 46.8±14.1 years) and the OAG risk in a subset of the Rotterdam Study cohorts. To evaluate false positive findings, we generated two new variables containing randomly sampled values to serve as a negative control. Results The explained variance of VCDR increased when increasing the number of SNPs included in the risk score, suggesting a polygenic model. We found no clear evidence for a similar model for IOP, suggesting that a small number of SNPs determine the susceptibility to IOP. The SNPs related to IOP in terms of p values contributed little to VCDR. The risk scores associated with VCDR were also associated significantly with OAG. This suggests a common polygenic background for VCDR and OAG Conclusions We found evidence for a polygenic model underlying one of the major traits of OAG, VCDR, and OAG itself. The IOP did not show any evidence for such a model. [ABSTRACT FROM PUBLISHER]

Published

2011

10. Cancer and neurologic degeneration in xeroderma pigmentosum: long term follow-up characterises the role of DNA repair.

Author

Bradford, Porcia T, Goldstein, Alisa M, Tamura, Deborah, Khan, Sikandar G, Ueda, Takahiro, Boyle, Jennifer, Oh, Kyu-Seon, Imoto, Kyoko, Inui, Hiroki, Moriwaki, Shin-Ichi, Emmert, Steffen, Pike, Kristen M, Raziuddin, Arati, Plona, Teri M, DiGiovanna, John J, Tucker, Margaret A, and Kraemer, Kenneth H

Abstract

Background The frequency of cancer, neurologic degeneration and mortality in xeroderma pigmentosum (XP) patients with defective DNA repair was determined in a four decade natural history study. Methods All 106 XP patients admitted to the National Institutes of Health from 1971 to 2009 were evaluated from clinical records and follow-up. Results In the 65 per cent (n=69) of patients with skin cancer, non-melanoma skin cancer (NMSC) was increased 10 000-fold and melanoma was increased 2000-fold in patients under age 20. The 9 year median age at diagnosis of first non-melanoma skin cancer (NMSC) (n=64) was significantly younger than the 22 year median age at diagnosis of first melanoma (n=38)—a relative age reversal from the general population suggesting different mechanisms of carcinogenesis between NMSC and melanoma. XP patients with pronounced burning on minimal sun exposure (n=65) were less likely to develop skin cancer than those who did not. This may be related to the extreme sun protection they receive from an earlier age, decreasing their total ultraviolet exposure. Progressive neurologic degeneration was present in 24% (n=25) with 16/25 in complementation group XP-D. The most common causes of death were skin cancer (34%, n=10), neurologic degeneration (31%, n=9), and internal cancer (17%, n=5). The median age at death (29 years) in XP patients with neurodegeneration was significantly younger than those XP patients without neurodegeneration (37 years) (p=0.02). Conclusion This 39 year follow-up study of XP patients indicates a major role of DNA repair genes in the aetiology of skin cancer and neurologic degeneration. [ABSTRACT FROM PUBLISHER]

Published

2011

11. CDKN2BAS is associated with periodontitis in different European populations and is activated by bacterial infection.

Author

Schaefer, Arne S, Richter, Gesa M, Dommisch, Henrik, Reinartz, Markus, Nothnagel, Michael, Noack, Barbara, Laine, Marja L, Folwaczny, Mathias, Groessner-Schreiber, Birte, Loos, Bruno G, Jepsen, Søren, and Schreiber, Stefan

Abstract

Epidemiological studies have indicated a relationship between coronary heart disease (CHD) and periodontitis. Recently, was reported as a shared genetic risk factor of CHD and aggressive periodontitis (AgP), but the causative variant has remained unknown. To identify and validate risk variants in different European populations, we first explored 150 kb of the genetic region of including the adjacent genes and , covering 51 tagging single nucleotide polymorphisms (tagSNPs) in AgP and chronic periodontitis (CP) in individuals of Dutch origin (n=313). In a second step, we tested the significant SNP associations in an independent AgP and CP population of German origin (n=1264). For the tagSNPs rs1360590, rs3217992, and rs518394, we could validate the associations with AgP before and after adjustment for the covariates smoking, gender and diabetes, with SNP rs3217992 being the most significant (OR 1.48, 95% CI 1.19 to 1.85; p=0.0004). We further showed in vivo gene expression of , and in healthy and inflamed gingival epithelium (GE) and connective tissue (CT), and detected a significantly higher expression of in healthy CT compared to GE (p=0.004). After 24 h of stimulation with in pre-treated gingival fibroblast (HGF) and cultured gingival epithelial cells (GECs), we observed a 25-fold and fourfold increase of gene expression in HGFs (p=0.003) and GECs (p=0.004), respectively. Considering the global importance of in the disease risk of CHD, this observation supports the theory of inflammatory components in the disease physiology of CHD. [ABSTRACT FROM PUBLISHER]

Published

2011

12. Germline DICER1 mutations and familial cystic nephroma.

Author

Bahubeshi, Amin, Bal, Nebil, Rio Frio, Thomas, Hamel, Nancy, Pouchet, Carly, Yilmaz, Ahmet, Bouron-Dal Soglio, Dorothée, Williams, Gretchen M, Tischkowitz, Marc, Priest, John R, and Foulkes, William D

Abstract

Background Multilocular cystic nephroma (CN) is a benign kidney tumour and is part of a family of kidney neoplasms including cystic partially differentiated nephroblastoma and Wilms tumour (WT). CN is rarely familial or bilateral, but it occurs in about 10% of families where pleuropulmonary blastoma (PPB) is present. Recently, germline mutations in were found in familial PPB. Objective To search for mutations in two families with familial CN; PPB was present in one family. Additionally, to test germline DNA from 50 children with sporadic WT for mutations. Results Both families with multiple CN were found to have mutations in leading to premature stop codons, predicted to result in loss of the ribonuclease and dsRNA binding domains. These domains are essential to the function of DICER1. No germline mutations were found in any of the 50 children who had developed WT. Conclusion It has been established that mutations cause familial CN and may be implicated in bilateral CN. No germline mutations were found in the patients with WT, suggesting that mutations are unlikely to have a major role in the aetiology of sporadic WT. These results provide further evidence implicating miRNA dysregulation in tumourigenesis. [ABSTRACT FROM PUBLISHER]

Published

2010

13. Ancestry informative markers for fine-scale individual assignment to worldwide populations.

Author

Paschou, Peristera, Lewis, Jamey, Javed, Asif, and Drineas, Petros

Abstract

Background and aims The analysis of large-scale genetic data from thousands of individuals has revealed the fact that subtle population genetic structure can be detected at levels that were previously unimaginable. Using the Human Genome Diversity Panel as reference (51 populations - 650,000 SNPs), this works describes a systematic evaluation of the resolution that can be achieved for the inference of genetic ancestry, even when small panels of genetic markers are used. Methods and results A comprehensive investigation of human population structure around the world is undertaken by leveraging the power of Principal Components Analysis (PCA). The problem is dissected into hierarchical steps and a decision tree for the prediction of individual ancestry is proposed. A complete leave-one-out validation experiment demonstrates that, using all available SNPs, assignment of individuals to their self-reported populations of origin is essentially perfect. Ancestry informative genetic markers are selected using two different metrics ( and correlation with PCA scores). A thorough cross-validation experiment indicates that, in most cases here, the number of SNPs needed for ancestry inference can be successfully reduced to less than 0.1% of the original 650,000 while retaining close to 100% accuracy. This reduction can be achieved using a novel clustering-based redundancy removal algorithm that is also introduced here. Finally, the applicability of our suggested SNP panels is tested on HapMap Phase 3 populations. Conclusion The proposed methods and ancestry informative marker panels, in combination with the increasingly more comprehensive databases of human genetic variation, open new horizons in a variety of fields, ranging from the study of human evolution and population history, to medical genetics and forensics. [ABSTRACT FROM PUBLISHER]

Published

2010

14. Associations of folate and choline metabolism gene polymorphisms with orofacial clefts.

Author

Mostowska, Adrianna, Hozyasz, Kamil K, Wojcicki, Piotr, Dziegelewska, Maja, and Jagodzinski, Pawel P

Abstract

Background Non-syndromic isolated cleft lip with or without cleft palate (NCL/P) is a common congenital anomaly in humans, the aetiology of which is complex and associated with both genetic and environmental factors. It has been reported that maternal nutritional factors are likely to play a major role in development of NCL/P in the embryo. Objective As the mechanism by which folic acid and choline supplementation prevents NCL/P is poorly understood, the relationship between 16 polymorphic variants of 12 genes encoding enzymes involved in the metabolism of these two nutrients and the risk of facial clefts was investigated. Results It was found that individuals with the AA genotype of the rs3733890 polymorphism have a significantly lower risk of orofacial clefts (OR 0.1450, 95% CI 0.0420 to 0.4995; p=0.0005; p=0.008). It was also demonstrated that the rs7639752 polymorphism of the gene increases the risk of NCL/P nearly twofold in the Polish population (OR 1.891, 95% CI 1.151 to 3.107; p=0.011), but this association would not withstand correction for multiple testing (p=0.176). The genetic variations in , , , , , , , , , and were not separately correlated with NCL/P risk. However, the Multifactor Dimensionality Reduction (MDR) analysis showed a significant epistatic between (rs1801133), (rs1805087), and (rs4646406) in NCL/P susceptibility. Conclusion This study demonstrates that choline metabolism may play an important role in the aetiology of NCL/P. Polymorphic variants of and and interactions between genes of choline and folate metabolism might influence the risk of NCL/P in the Polish population. [ABSTRACT FROM PUBLISHER]

Published

2010

15. BHD mutations, clinical and molecular genetic investigations of Birt-Hogg-Dubé syndrome: a new series of 50 families and a review of published reports.

Author

Toro, J R, Wei, M-H, Glenn, G M, Weinreich, M, Toure, O, Vocke, C, Turner, M, Choyke, P, Merino, M J, Pinto, P A, Steinberg, S M, Schmidt, L S, and Linehan, W M

Subjects

ESTRONE, GENETIC epidemiology, MOLECULAR epidemiology, PUBLIC health, EPIDEMIOLOGICAL transition

Abstract

Background: Birt-Hogg-Dubé syndrome (BHDS) (MIM 135150) is an autosomal dominant predisposition to the development of follicular hamartomas (fibrofolliculomas), lung cysts, spontaneous pneumothorax, and kidney neoplasms. Germline mutations in BHD are associated with the susceptibility for BHDS. We previously described 51 BHDS families with BHD germline mutations. Objective: To characterise the BHD mutation spectrum, novel mutations and new clinical features of one previously reported and 50 new families with BHDS. Methods: Direct bidirectional DNA sequencing was used to screen for mutations in the BHD gene, and insertion and deletion mutations were confirmed by subcloning. We analysed evolutionary conservation of folliculin by comparing human against the orthologous sequences. Results: The BHD mutation detection rate was 88% (51/ 58). Of the 23 different germline mutations identified, 13 were novel consisting of: four splice site, three deletions, two insertions, two nonsense, one deletion/insertion, and one missense mutation. We report the first germline missense mutation in BHD c.1978A>G (K508R) in a patient who presented with bilateral multifocal renal oncocytomas. This mutation occurs in a highly conserved amino acid in folliculin. 10% (5/51) of the families had individuals without histologically confirmed fibrofolliculomas. Of 44 families ascertained on the basis of skin lesions, 18 (41%) had kidney tumours. Patients with a germline BHD mutation and family history of kidney cancer had a statistically significantly increased probability of developing renal tumours compared to patients without a positive family history (p = 0.0032). Similarly, patients with a BHD germline mutation and family history of spontaneous pneumothorax had a significantly increased greater probability of having spontaneous pneumothorax than BHDS patients without a family history of spontaneous pneumothorax (p = 0.011). A comprehensive review of published reports of cases with BHD germline mutation is discussed. Conclusion: BHDS is characterised by a spectrum of mutations, and clinical heterogeneity both among and within families. [ABSTRACT FROM AUTHOR]

Published

2008

16. Rare, protein-truncating variants in ATM, CHEK2 and PALB2, but not XRCC2, are associated with increased breast cancer risks

Author

Decker, Brennan, Allen, Jamie, Luccarini, Craig, Pooley, Karen A, Shah, Mitul, Bolla, Manjeet K, Wang, Qin, Ahmed, Shahana, Baynes, Caroline, Conroy, Don M, Brown, Judith, Luben, Robert, Ostrander, Elaine A, Pharoah, Paul DP, Dunning, Alison M, and Easton, Douglas F

Subjects

Cancer: breast, Genetic Variation, Breast Neoplasms, Ataxia Telangiectasia Mutated Proteins, DNA-Binding Proteins, Checkpoint Kinase 2, Evidence Based Practice, Sequence Analysis, Protein, Genetic Epidemiology, Cancer Genetics, Humans, Female, Genetic Predisposition to Disease, Fanconi Anemia Complementation Group N Protein, Geneticscreening/counselling

Abstract

Background Breast cancer (BC) is the most common malignancy in women and has a major heritable component. The risks associated with most rare susceptibility variants are not well estimated. To better characterise the contribution of variants in ATM, CHEK2, PALB2 and XRCC2, we sequenced their coding regions in 13 087 BC cases and 5488 controls from East Anglia, UK. Methods Gene coding regions were enriched via PCR, sequenced, variant called and filtered for quality. ORs for BC risk were estimated separately for carriers of truncating variants and of rare missense variants, which were further subdivided by functional domain and pathogenicity as predicted by four in silico algorithms. Results Truncating variants in PALB2 (OR=4.69, 95% CI 2.27 to 9.68), ATM (OR=3.26; 95% CI 1.82 to 6.46) and CHEK2 (OR=3.11; 95% CI 2.15 to 4.69), but not XRCC2 (OR=0.94; 95% CI 0.26 to 4.19) were associated with increased BC risk. Truncating variants in ATM and CHEK2 were more strongly associated with risk of oestrogen receptor (ER)-positive than ER-negative disease, while those in PALB2 were associated with similar risks for both subtypes. There was also some evidence that missense variants in ATM, CHEK2 and PALB2 may contribute to BC risk, but larger studies are necessary to quantify the magnitude of this effect. Conclusions Truncating variants in PALB2 are associated with a higher risk of BC than those in ATM or CHEK2. A substantial risk of BC due to truncating XRCC2 variants can be excluded.

Published

2017

17. A risk prediction algorithm for ovarian cancer incorporating BRCA1, BRCA2, common alleles and other familial effects

Author

Jervis, Sarah, Song, Honglin, Lee, Andrew, Dicks, Ed, Harrington, Patricia, Baynes, Caroline, Manchanda, Ranjit, Easton, Douglas F, Jacobs, Ian, Pharoah, Paul PD, Antoniou, Antonis C, Song, Honglin [0000-0001-5076-7371], Lee, Andrew [0000-0003-0677-0252], Dicks, Ed [0000-0002-0617-0401], Easton, Douglas [0000-0003-2444-3247], Pharoah, Paul [0000-0001-8494-732X], Antoniou, Antonis [0000-0001-9223-3116], and Apollo - University of Cambridge Repository

Subjects

Ovarian Neoplasms, Multifactorial Inheritance, endocrine system diseases, Models, Genetic, Genes, BRCA2, Genes, BRCA1, Genetic screening/counselling, Genetic Counseling, Risk Assessment, Risk prediction, Ovarian Cancer, Cancer Genetics, Humans, Genetic epidemiology, Female, Genetic Predisposition to Disease, Genome-wide, skin and connective tissue diseases, Alleles

Abstract

BACKGROUND: Although BRCA1 and BRCA2 mutations account for only ∼27% of the familial aggregation of ovarian cancer (OvC), no OvC risk prediction model currently exists that considers the effects of BRCA1, BRCA2 and other familial factors. Therefore, a currently unresolved problem in clinical genetics is how to counsel women with family history of OvC but no identifiable BRCA1/2 mutations. METHODS: We used data from 1548 patients with OvC and their relatives from a population-based study, with known BRCA1/2 mutation status, to investigate OvC genetic susceptibility models, using segregation analysis methods. RESULTS: The most parsimonious model included the effects of BRCA1/2 mutations, and the residual familial aggregation was accounted for by a polygenic component (SD 1.43, 95% CI 1.10 to 1.86), reflecting the multiplicative effects of a large number of genes with small contributions to the familial risk. We estimated that 1 in 630 individuals carries a BRCA1 mutation and 1 in 195 carries a BRCA2 mutation. We extended this model to incorporate the explicit effects of 17 common alleles that are associated with OvC risk. Based on our models, assuming all of the susceptibility genes could be identified we estimate that the half of the female population at highest genetic risk will account for 92% of all OvCs. CONCLUSIONS: The resulting model can be used to obtain the risk of developing OvC on the basis of BRCA1/2, explicit family history and common alleles. This is the first model that accounts for all OvC familial aggregation and would be useful in the OvC genetic counselling process.

Published

2015

18. Otitis media susceptibility and shifts in the head and neck microbiome due to SPINK5 variants.

Author

Frank DN, Giese APJ, Hafren L, Bootpetch TC, Yarza TKL, Steritz MJ, Pedro M, Labra PJ, Daly KA, Tantoco MLC, Szeremeta W, Reyes-Quintos MRT, Ahankoob N, Llanes EGDV, Pine HS, Yousaf S, Ir D, Einarsdottir E, de la Cruz RAR, Lee NR, Nonato RMA, Robertson CE, Ong KMC, Magno JPM, Chiong ANE, Espiritu-Chiong MC, San Agustin ML, Cruz TLG, Abes GT, Bamshad MJ, Cutiongco-de la Paz EM, Kere J, Nickerson DA, Mohlke KL, Riazuddin S, Chan A, Mattila PS, Leal SM, Ryan AF, Ahmed ZM, Chonmaitree T, Sale MM, Chiong CM, and Santos-Cortez RLP

Subjects

Adult, Animals, Bacteria classification, Bacteria genetics, Child, Disease Susceptibility microbiology, Ear, External microbiology, Ear, Middle microbiology, Exome, Female, Genetic Predisposition to Disease, Humans, Male, Mice, Mouth microbiology, Nasopharynx microbiology, Pedigree, Sequence Analysis, DNA, Sequence Analysis, RNA, Microbiota, Otitis Media genetics, Otitis Media microbiology, Serine Peptidase Inhibitor Kazal-Type 5 genetics

Abstract

Background: Otitis media (OM) susceptibility has significant heritability; however, the role of rare variants in OM is mostly unknown. Our goal is to identify novel rare variants that confer OM susceptibility., Methods: We performed exome and Sanger sequencing of >1000 DNA samples from 551 multiethnic families with OM and unrelated individuals, RNA-sequencing and microbiome sequencing and analyses of swabs from the outer ear, middle ear, nasopharynx and oral cavity. We also examined protein localisation and gene expression in infected and healthy middle ear tissues., Results: A large, intermarried pedigree that includes 81 OM-affected and 53 unaffected individuals cosegregates two known rare A2ML1 variants, a common FUT2 variant and a rare, novel pathogenic variant c.1682A>G (p.Glu561Gly) within SPINK5 (LOD=4.09). Carriage of the SPINK5 missense variant resulted in increased relative abundance of Microbacteriaceae in the middle ear, along with occurrence of Microbacteriaceae in the outer ear and oral cavity but not the nasopharynx. Eight additional novel SPINK5 variants were identified in 12 families and individuals with OM. A role for SPINK5 in OM susceptibility is further supported by lower RNA counts in variant carriers, strong SPINK5 localisation in outer ear skin, faint localisation to middle ear mucosa and eardrum and increased SPINK5 expression in human cholesteatoma., Conclusion: SPINK5 variants confer susceptibility to non-syndromic OM. These variants potentially contribute to middle ear pathology through breakdown of mucosal and epithelial barriers, immunodeficiency such as poor vaccination response, alteration of head and neck microbiota and facilitation of entry of opportunistic pathogens into the middle ear., Competing Interests: Competing interests: AR is a cofounder of, shareholder in and uncompensated consultant to Otonomy, Inc, a relationship that was approved by the University of California San Diego., (© Author(s) (or their employer(s)) 2021. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2021

19. Polygenic and multifactorial scores for pancreatic ductal adenocarcinoma risk prediction.

Author

Galeotti AA, Gentiluomo M, Rizzato C, Obazee O, Neoptolemos JP, Pasquali C, Nentwich M, Cavestro GM, Pezzilli R, Greenhalf W, Holleczek B, Schroeder C, Schöttker B, Ivanauskas A, Ginocchi L, Key TJ, Hegyi P, Archibugi L, Darvasi E, Basso D, Sperti C, Bijlsma MF, Palmieri O, Hlavac V, Talar-Wojnarowska R, Mohelnikova-Duchonova B, Hackert T, Vashist Y, Strouhal O, van Laarhoven H, Tavano F, Lovecek M, Dervenis C, Izbéki F, Padoan A, Małecka-Panas E, Maiello E, Vanella G, Capurso G, Izbicki JR, Theodoropoulos GE, Jamroziak K, Katzke V, Kaaks R, Mambrini A, Papanikolaou IS, Szmola R, Szentesi A, Kupcinskas J, Bursi S, Costello E, Boggi U, Milanetto AC, Landi S, Gazouli M, Vodickova L, Soucek P, Gioffreda D, Gemignani F, Brenner H, Strobel O, Büchler M, Vodicka P, Paiella S, Canzian F, and Campa D

Subjects

ABO Blood-Group System genetics, Alleles, Carcinoma, Pancreatic Ductal diagnosis, Carcinoma, Pancreatic Ductal genetics, Early Detection of Cancer, Female, Gene Frequency, Humans, Male, Pancreatic Neoplasms genetics, Polymorphism, Single Nucleotide, Risk Assessment, Multifactorial Inheritance

Abstract

Background: Most cases of pancreatic ductal adenocarcinoma (PDAC) are asymptomatic in early stages, and the disease is typically diagnosed in advanced phases, resulting in very high mortality. Tools to identify individuals at high risk of developing PDAC would be useful to improve chances of early detection., Objective: We generated a polygenic risk score (PRS) for PDAC risk prediction, combining the effect of known risk SNPs, and carried out an exploratory analysis of a multifactorial score., Methods: We tested the associations of the individual known risk SNPs on up to 2851 PDAC cases and 4810 controls of European origin from the PANcreatic Disease ReseArch (PANDoRA) consortium. Thirty risk SNPs were included in a PRS, which was computed on the subset of subjects that had 100% call rate, consisting of 839 cases and 2040 controls in PANDoRA and 6420 cases and 4889 controls from the previously published Pancreatic Cancer Cohort Consortium I-III and Pancreatic Cancer Case-Control Consortium genome-wide association studies. Additional exploratory multifactorial scores were constructed by complementing the genetic score with smoking and diabetes., Results: The scores were associated with increased PDAC risk and reached high statistical significance (OR=2.70, 95% CI 1.99 to 3.68, p=2.54×10 -10 highest vs lowest quintile of the weighted PRS, and OR=14.37, 95% CI 5.57 to 37.09, p=3.64×10 -8 , highest vs lowest quintile of the weighted multifactorial score)., Conclusion: We found a highly significant association between a PRS and PDAC risk, which explains more than individual SNPs and is a step forward in the direction of the construction of a tool for risk stratification in the population., Competing Interests: Competing interests: MFB has received research funding from Celgene. HvL has acted as a consultant for Celgene, and Eli Lilly and Company, Nordic Pharma Group and Philips, and has received research grants from Amgen, Bayer Schering Pharma, Celgene, Eli Lilly and Company, GlaxoSmithKline Pharmaceuticals, MSD, Nordic Pharma Group, Philips and Roche Pharmaceuticals., (© Author(s) (or their employer(s)) 2021. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2021

20. Paediatric ovarian tumours and their associated cancer susceptibility syndromes

Author

W. Glenn McCluggage, Stephanie Vairy, Leora Witkowski, William D. Foulkes, and Catherine Goudie

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, Pathology, genetic epidemiology, Granulosa cell, cancer: colon, Ovary, Biology, Small-cell carcinoma, Germline, cancer: endocrine, cancer: breast, Diagnosis, Differential, genome-wide, diagnostics tests, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Genetic predisposition, Cancer Genetics, Humans, Genetic Predisposition to Disease, genetics, Child, Position Statement, Pathological, Genetics (clinical), Ovarian Neoplasms, Complex Traits, Syndrome, genetic screening/counselling, medicine.disease, Sertoli cell, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, 030220 oncology & carcinogenesis, molecular genetics, oncology, Female, Germ cell, clinical genetics, reproductive medicine

Abstract

Background Germline pathogenic variants in SDHB/SDHC/SDHD are the most frequent causes of inherited phaeochromocytomas/paragangliomas. Insufficient information regarding penetrance and phenotypic variability hinders optimum management of mutation carriers. We estimate penetrance for symptomatic tumours and elucidate genotype–phenotype correlations in a large cohort of SDHB/SDHC/SDHD mutation carriers. Methods A retrospective survey of 1832 individuals referred for genetic testing due to a personal or family history of phaeochromocytoma/paraganglioma. 876 patients (401 previously reported) had a germline mutation in SDHB/SDHC/SDHD (n=673/43/160). Tumour risks were correlated with in silico structural prediction analyses. Results Tumour risks analysis provided novel penetrance estimates and genotype–phenotype correlations. In addition to tumour type susceptibility differences for individual genes, we confirmed that the SDHD:p.Pro81Leu mutation has a distinct phenotype and identified increased age-related tumour risks with highly destabilising SDHB missense mutations. By Kaplan-Meier analysis, the penetrance (cumulative risk of clinically apparent tumours) in SDHB and (paternally inherited) SDHD mutation-positive non-probands (n=371/67 with detailed clinical information) by age 60 years was 21.8% (95% CI 15.2% to 27.9%) and 43.2% (95% CI 25.4% to 56.7%), respectively. Risk of malignant disease at age 60 years in non-proband SDHB mutation carriers was 4.2%(95% CI 1.1% to 7.2%). With retrospective cohort analysis to adjust for ascertainment, cumulative tumour risks for SDHB mutation carriers at ages 60 years and 80 years were 23.9% (95% CI 20.9% to 27.4%) and 30.6% (95% CI 26.8% to 34.7%). Conclusions Overall risks of clinically apparent tumours for SDHB mutation carriers are substantially lower than initially estimated and will improve counselling of affected families. Specific genotype–tumour risk associations provides a basis for novel investigative strategies into succinate dehydrogenase-related mechanisms of tumourigenesis and the development of personalised management for SDHB/SDHC/SDHD mutation carriers.

Published

2017

21. Uptake of breast cancer prevention and screening trials.

Author

Evans, D Gareth, Harvie, Michelle, Bundred, Nigel, and Howell, Anthony

Abstract

Background Uptake of cancer trials and in particular prevention trials has been disappointing globally. Methods Uptake to three randomised chemotherapy breast cancer prevention trials and two dietary prevention trials in women at increased familial risk were assessed and compared with uptake of screening trials across a range of risk categories. Results Uptake of drug prevention trials remains low at 5.3–13.6%, but is significantly higher in the high (12%) compared to very high risk group (8.4%) for IBIS1 and IBIS2 combined (p=0.004). Recruitment to two dietary prevention studies via mail shot was also disappointingly low at 6.2% and 12.5%. In contrast uptake to two mammography screening trials was >90% in all risk categories. Conclusions More work must be done to improve recruitment to prevention trials if they are to be seen as viable alternatives to risk reducing surgery. Impact Trial designs and decision aids need to be developed to improve recruitment. [ABSTRACT FROM PUBLISHER]

Published

2010

22. Ovarian cancer familial relative risks by tumour subtypes and by known ovarian cancer genetic susceptibility variants

Author

Sarah Jervis, Douglas F. Easton, Ian Jacobs, Jonathan Tyrer, Andy C. H. Lee, Ed Dicks, Honglin Song, Antonis C. Antoniou, Patricia Harrington, and Paul P.D. Pharoah

Subjects

Adult, Risk, Oncology, medicine.medical_specialty, endocrine system diseases, Genes, BRCA2, Population, Genes, BRCA1, Biology, Polymorphism, Single Nucleotide, Young Adult, Breast cancer, Internal medicine, Genetics, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, Family history, education, Genetics (clinical), Aged, Ovarian Neoplasms, education.field_of_study, Middle Aged, medicine.disease, female genital diseases and pregnancy complications, Genetic epidemiology, Relative risk, Mutation, Female, Neoplasms, Cystic, Mucinous, and Serous, Ovarian cancer, Cohort study

Abstract

Background Family history is one of the most important risk factors for epithelial ovarian cancer (EOC). Little is known, however, on how EOC familial relative risks (FRRs) vary by factors such as tumour subtype or the combined effects of common EOC susceptibility alleles. In addition, no data currently exist on the FRRs associated with EOC after exclusion of BRCA1 or BRCA2 mutation carriers. Methods EOC FRRs were computed from observed EOCs in relatives of 1548 patients with EOC recruited between 1999 and 2010 from a population-based cohort study with known BRCA1 and BRCA2 mutation status and tumour subtype, compared with the number expected in the general population. Results The EOC FRR to all first-degree relatives was estimated to be 2.96 (95% CI 2.35 to 3.72) but there was no evidence of difference in the FRRs for mothers, sisters and daughters. There was significant evidence that the FRR for relatives of patients with EOC diagnosed under age 50 years is higher than that for older patients (4.72 (95% CI 3.21 to 6.95) and 2.53 (95% CI 1.91 to 3.35), p-diff=0.0052) and a suggestion that the FRR in relatives of patients with serous disease is higher than that for non-serous tumours (3.64 (95% CI 2.72 to 4.87) and 2.25 (95% CI 1.56 to 3.26), p-diff=0.0023). The FRR to relatives of cases without a deleterious mutation in BRCA1 or BRCA2 was estimated to be over twice that of the general population (2.24 (95% CI 1.71 to 2.94)). BRCA1 and BRCA2 mutations were estimated to account for about 24% of the EOC FRR to first-degree relatives. FRRs were found to increase with increasing polygenic risk score of the index patient, although the trend was not significant. Conclusions These estimates could be useful in the counselling of relatives of patients with ovarian cancer.

Published

2013

23. Confirmation of papillary thyroid cancer susceptibility loci identified by genome-wide association studies of chromosomes 14q13, 9q22, 2q35 and 8p12 in a Chinese population

Author

Shicheng Guo, Li Jin, Xiaofeng Wang, Yan Yun Ma, Shou Hao Feng, Jiucun Wang, Wen Jun Wei, Yu Wang, Duan Shu Li, Qinghai Ji, Yu-Long Wang, and Zhuo Ying Wang

Subjects

Adult, Male, China, Genotype, endocrine system diseases, Single-nucleotide polymorphism, Genome-wide association study, Biology, Polymorphism, Single Nucleotide, Papillary thyroid cancer, Asian People, Odds Ratio, Genetics, medicine, Humans, SNP, Genetic Predisposition to Disease, Thyroid Neoplasms, Thyroid cancer, Alleles, Genetics (clinical), Aged, Genetic association, Chromosomes, Human, Pair 14, Thyroid disease, Carcinoma, Computational Biology, Middle Aged, medicine.disease, Carcinoma, Papillary, Genetic epidemiology, Genetic Loci, Thyroid Cancer, Papillary, Case-Control Studies, Chromosomes, Human, Pair 2, Female, Chromosomes, Human, Pair 9, Chromosomes, Human, Pair 8, Genome-Wide Association Study

Abstract

Background Five single nucleotide polymorphisms (SNPs) were previously reported to be associated with thyroid cancer in European populations in two genome-wide association studies (GWAS): rs965513 (9q22.33), rs944289 (14q13.3), rs116909374 (14q13.3), rs966423 (2q35) and rs2439302 (8p12). Only the first two SNPs have been validated in independent populations and none were replicated in Chinese populations. Methods The above five SNPs were genotyped in 845 papillary thyroid cancer (PTC) and 503 benign thyroid tumour (BN) patients and 1005 controls in a Chinese population using the SNaPshot multiplex single nucleotide extension system. Results Significant associations were detected among PTC and rs944289 (p=8.007e-11), rs965513 (p=1.013e-4), rs966423 (p=1.688e-3) and rs2439302 (p=1.096e-4) in a dominant model, while the rs116909374 SNP was not detected in the Chinese population. The PTC risk increased with rise in accumulative numbers of risk alleles carried by individuals (p=5.929e-13). The PTC OR of carriers of six risk alleles (1.4% of the control population) was 23.587 compared with non-risk homozygotes (1.0% of the control population, with zero risk alleles). No individuals were homozygous for all the four SNPs (carriers of eight risk alleles) and only three PTC cases were carriers of seven risk alleles. A significant association between 14q13.3 SNP rs944289T and BN was also found (p=0.0014). Conclusions Four candidate loci, rs965513 (9q22.33), rs944289 (14q13.3), rs966423 (2q35) and rs2439302 (8p12), identified by GWAS for PTC risk were confirmed in a Chinese population. The PTC risk of accumulative risk allele carriers increased with the number of risk alleles.

Published

2013

24. Large-scale genotyping identifies a new locus at 22q13.2 associated with female breast size

Author

Mikael Hartman, Jajini Varghese, Keith Humphreys, Yi Li, Vessela N. Kristensen, Jianjun Liu, Nils Schoof, Per Hall, Jonine D. Figueroa, Jia Nee Foo, Deborah J. Thompson, Jingmei Li, Chiea Chuen Khor, Swee Tian Quek, Kamila Czene, Gretchen L. Gierach, Pablo Fernández-Navarro, Silje Nord, Marina Pollán, and Unión Europea

Subjects

Epidemiology, Chromosomes, Human, Pair 22, Quantitative Trait Loci, Single-nucleotide polymorphism, Genome-wide association study, Locus (genetics), Quantitative trait locus, Biology, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Genetics, medicine, breast [Cancer], Mammography, Humans, Genetic epidemiology, Genome-wide, skin and connective tissue diseases, Mammary Glands, Human, Genotyping, Genetics (clinical), 030304 developmental biology, 0303 health sciences, medicine.diagnostic_test, Organ Size, Complex traits, medicine.disease, 3. Good health, 030220 oncology & carcinogenesis, Organelle Size, Female, Chromosomes, Human, Pair 8, Genome-Wide Association Study

Abstract

BACKGROUND: Individual differences in breast size are a conspicuous feature of variation in human females and have been associated with fecundity and advantage in selection of mates. To identify common variants that are associated with breast size, we conducted a large-scale genotyping association meta-analysis in 7169 women of European descent across three independent sample collections with digital or screen film mammograms. METHODS: The samples consisted of the Swedish KARMA, LIBRO-1 and SASBAC studies genotyped on iCOGS, a custom illumina iSelect genotyping array comprising of 211 155 single nucleotide polymorphisms (SNPs) designed for replication and fine mapping of common and rare variants with relevance to breast, ovary and prostate cancer. Breast size of each subject was ascertained by measuring total breast area (mm(2)) on a mammogram. RESULTS: We confirm genome-wide significant associations at 8p11.23 (rs10086016, p=1.3×10(-14)) and report a new locus at 22q13 (rs5995871, p=3.2×10(-8)). The latter region contains the MKL1 gene, which has been shown to impact endogenous oestrogen receptor α transcriptional activity and is recruited on oestradiol sensitive genes. We also replicated previous genome-wide association study findings for breast size at four other loci. CONCLUSIONS: A new locus at 22q13 may be associated with female breast size. KARMA and LIBRO-1 were supported by Märit and Hans Rausings Initiative Against Breast Cancer. SASBAC was supported by funding from the Agency for Science, Technology and Research of Singapore (A*STAR), the US National Institute of Health (NIH) and the Susan G. Komen Breast Cancer Foundation. All three studies are genotyped as part of the Collaborative Oncological Gene-environment Study (COGS), which is supported by the European Community's Seventh Framework Programme under grant agreement 223175 (HEALTH-F2-2009-223175) (COGS). Genotyping of the iCOGS array was funded by the European Union (HEALTH-F2-2009-223175), Cancer Research UK (C1287/A10710), the Canadian Institutes of Health Research (CIHR) for the CIHR Team in Familial Risks of Breast Cancer program and the Ministry of Economic Development, Innovation and Export Trade of Quebec (grant PSR-SIIRI-701). BCAC is funded by Cancer Research UK (C1287/A10118 and C1287/A12014). Combining the GWAS data was supported in part by the US National Institutes of Health (NIH) Cancer Post-Cancer GWAS initiative grant 1 U19 CA 148065-01 (DRIVE, part of the GAME-ON initiative). KC was financed by the Swedish Cancer Society (5128-B07-01PAF). KH was supported by the Swedish Research Council (523-2006-972) and the Swedish E Science Research Centre. This work was also supported, in part, by the Intramural Research Program of the U.S. National Cancer Institute, Department of Health and Human Services, USA. We wish to thank Aki Tuuliainen, Kimberley Sio Kim Chua, Sander Canisius, Grethe I.G. Alnæs, Torben Luders and Lodewyk Wessels for their help in data collection and analysis Sí

Published

2013

25. Deletion of the 5'exons of COL4A6 is not needed for the development of diffuse leiomyomatosis in patients with Alport syndrome

Author

Fernando Neves, Guy Froyen, S. Alves, Umbelina Ramos, Maria João Nabais Sá, Márcia Rodrigues, Fernando Teixeira e Costa, Nathalie Fieremans, Adelino Carvalho, Arjan P.M. de Brouwer, Maria José Brito, Joana Felgueiras, Fernanda Carvalho, Rita de Sousa, Francisco Sousa, José Ramón Vizcaíno, Filipa Carvalho, João Paulo Oliveira, Clinical sciences, and Medical Genetics

Subjects

Adult, Collagen Type IV, Male, medicine.medical_specialty, Genotype, Nephritis, Hereditary, Biology, urologic and male genital diseases, Young Adult, Exon, Nephritis, Hereditary/genetics, Leiomyomatosis, Molecular genetics, otorhinolaryngologic diseases, Genetics, medicine, Humans, Alport syndrome, Child, Genetics (clinical), Molecular pathology, Leiomyomatosis/genetics, Exons, Middle Aged, medicine.disease, Molecular biology, Collagen Type IV/genetics, Pedigree, Genetics and epigenetic pathways of disease DCN MP - Plasticity and memory [NCMLS 6], Genetic epidemiology, Child, Preschool, Medical genetics, Female, Gene Deletion

Abstract

Background Alport syndrome (AS), a hereditary type IV collagen nephropathy, is a major cause of end-stage renal disease in young people. About 85% of the cases are X-linked (ATS), due to mutations in the COL4A5 gene. Rarely, families have a contiguous gene deletion comprising at least exon 1 of COL4A5 and the first exons of COL4A6 , associated with the development of diffuse leiomyomatosis (ATS-DL). We report three novel deletions identified in families with AS, one of which challenges the current concepts on genotype-phenotype correlations of ATS/ATS-DL. Methods In the setting of a multicentric study aiming to describe the genetic epidemiology and molecular pathology of AS in Portugal, three novel COL4A5 deletions were identified in two families with x-linked Alport syndrome (ATS) and in one family with ATS-DL. These mutations were initially detected by PCR and Multiplex Ligation-dependent Probe Amplification, and further mapped by high-resolution X chromosome-specific oligo-array and PCR. Results In the ATS-DL family, a COL4A5 deletion spanning exons 2 through 51, extending distally beyond COL4A5 but proximally not into COL4A6 , segregated with the disease phenotype. A COL4A5 deletion encompassing exons 2 through 29 was identified in one of the ATS families. In the second ATS family, a deletion of exon 13 of COL4A5 through exon 3 of COL4A6 was detected. Conclusions These observations suggest that deletion of the 5′ exons of COL4A6 and of the common promoter of the COL4A5 and COL4A6 genes is not essential for the development of leiomyomatosis in patients with ATS, and that COL4A5_COL4A6 deletions extending into COL4A6 exon 3 may not result in ATS-DL.

Published

2013

26. Disruption of RAB40AL function leads to Martin–Probst syndrome, a rare X-linked multisystem neurodevelopmental human disorder

Author

Yongsheng Bai, Amol C. Shetty, Jennifer M. Skidmore, James D. Cavalcoli, Kajari Mondal, Julie B Kaplan, Anthony Antonellis, Charles E. Schwartz, Mark A. Durham, Jun Li, Jirair K. Bedoyan, Cindy Skinner, Valerie M. Schaibley, Donna M. Martin, Michael E. Zwick, Arti Dhiraaj, Joseph A. Micucci, and Weiping Peng

Subjects

Male, DNA Mutational Analysis, Xenopus, GTPase, medicine.disease_cause, genome-wide, Mice, 0302 clinical medicine, Chlorocebus aethiops, Missense mutation, guidelines, Zebrafish, Genetics (clinical), Genetics, 0303 health sciences, Mutation, Massive parallel sequencing, Developmental Defects, Genetic Diseases, X-Linked, Syndrome, Pedigree, Organ Specificity, COS Cells, Female, medicine.symptom, microarray, Adult, Primates, genetic epidemiology, Blotting, Western, Green Fluorescent Proteins, Molecular Sequence Data, Mutation, Missense, Biology, Short stature, Mitochondrial Proteins, complex traits, 03 medical and health sciences, Fetus, copy-number, medicine, Animals, Humans, developmental, chromosomal, Gene, 030304 developmental biology, Base Sequence, epigenetics, academic medicine, Sequence Analysis, DNA, biology.organism_classification, Spectrometry, Fluorescence, molecular genetics, ras Proteins, clinical genetics, 030217 neurology & neurosurgery

Abstract

Background and aim Martin–Probst syndrome (MPS) is a rare X-linked disorder characterised by deafness, cognitive impairment, short stature and distinct craniofacial dysmorphisms, among other features. The authors sought to identify the causative mutation for MPS. Methods and results Massively parallel sequencing in two affected, related male subjects with MPS identified a RAB40AL (also called RLGP ) missense mutation (chrX:102,079,078-102,079,079AC → GA p.D59G; hg18). RAB40AL encodes a small Ras-like GTPase protein with one suppressor of cytokine signalling box. The p.D59G variant is located in a highly conserved region of the GTPase domain between β-2 and β-3 strands. Using RT-PCR, the authors show that RAB40AL is expressed in human fetal and adult brain and kidney, and adult lung, heart, liver and skeletal muscle. RAB40AL appears to be a primate innovation, with no orthologues found in mouse, Xenopus or zebrafish. Western analysis and fluorescence microscopy of GFP-tagged RAB40AL constructs from transiently transfected COS7 cells show that the D59G missense change renders RAB40AL unstable and disrupts its cytoplasmic localisation. Conclusions This is the first study to show that mutation of RAB40AL is associated with a human disorder. Identification of RAB40AL as the gene mutated in MPS allows for further investigations into the molecular mechanism(s) of RAB40AL and its roles in diverse processes such as cognition, hearing and skeletal development.

Published

2012

27. A multi-centre clinico-genetic analysis of the VPS35 gene in Parkinson disease indicates reduced penetrance for disease-associated variants

Author

Peter Lichtner, Ryan J. Uitti, George D. Mellick, Georgios M. Hadjigeorgiou, Carles Vilariño-Güell, Kuo Chu Yueh, Georg Auburger, Peter A. Silburn, Andrew A. Hicks, Suzana Gispert, Y. Zhao, Gaëtan Garraux, Timothy Lynch, Harumi S. Yomono, Maria Barcikowska, Miho Murata, Suzanne Lesage, Eng-King Tan, Joanne D. Stockton, Lars Bertram, Owen A. Ross, Sung Sup Park, Alexander Zimprich, Barbara Jasinska-Myga, Thomas Gasser, Karin Wirdefeldt, Alexis Brice, Rejko Krüger, Beomseok Jeon, Christina M. Lill, Vincent Mok, Wataru Satake, Hiroyuki Tomiyama, Tim M. Strom, Matthew J. Farrer, Cecile Libioulle, Grzegorz Opala, Peter P. Pramstaller, Irene Pichler, Grazia Annesi, Demetrius M. Maraganore, Jessie Theuns, Jan O. Aasly, Maria Bozi, Anna Krygowska-Wajs, John P. A. Ioannidis, Zbigniew K. Wszolek, Carl E Clarke, Karen E. Morrison, Nobutaka Hattori, Zygmunt Jamrozik, Maurizio F. Facheris, Manu Sharma, Thomas Meitnger, Tatsushi Toda, Aldo Quattrone, Christine Van Broeckhoven, Ekaterina Rogaeva, Leonidas Stefanis, Georgia Xiromerisiou, David Crosiers, Juei-Jueng Lin, Anthony E. Lang, and GEOPD Consortium

Subjects

Male, Parkinson's disease, Population, Vesicular Transport Proteins, Locus (genetics), Disease, Biology, VPS35 protein, human, Bioinformatics, genetics [Vesicular Transport Proteins], genetics [Parkinson Disease], Risk Factors, medicine, metabolism [Vesicular Transport Proteins], Genetics, Missense mutation, VPS35 Gene, Humans, Genetic epidemiology, Genetic Predisposition to Disease, ddc:610, Genome-wide, education, Genetics (clinical), Genetic Association Studies, Vacuolar protein sorting, education.field_of_study, Genotype-Phenotype Correlations, Parkinson Disease, Complex traits, medicine.disease, Penetrance, ddc, Mutation, Female, Human medicine, Parkinson-s disease

Abstract

Background Two recent studies identified a mutation (p.Asp620Asn) in the vacuolar protein sorting 35 gene as a cause for an autosomal dominant form of Parkinson disease. Although additional missense variants were described, their pathogenic role yet remains inconclusive. Methods and results We performed the largest multi-center study to ascertain the frequency and pathogenicity of the reported vacuolar protein sorting 35 gene variants in more than 15,000 individuals worldwide. p.Asp620Asn was detected in 5 familial and 2 sporadic PD cases and not in healthy controls, p.Leu774Met in 6 cases and 1 control, p.Gly51Ser in 3 cases and 2 controls. Overall analyses did not reveal any significant increased risk for p.Leu774Met and p.Gly51Ser in our cohort. Conclusions Our study apart from identifying the p. Asp620Asn variant in familial cases also identified it in idiopathic Parkinson disease cases, and thus provides genetic evidence for a role of p.Asp620Asn in Parkinson disease in different populations worldwide.

Published

2012

28. MEIS1 and BTBD9: genetic association with restless leg syndrome in end stage renal disease

Author

Andreas Ströhle, Darina Czamara, Ioannis Stefanidis, Efthimios Dardiotis, Maria Kaffe, Georgios M. Hadjigeorgiou, George K. Sakkas, Thomas Meitinger, Walter Samtleben, Christian Gieger, Konrad Oexle, Juliane Winkelmann, Nadine Gross, Barbara Schormair, Bertram Müller-Myhsok, Jens Plag, Uwe Heemann, Peter Lichtner, and Andreas Vainas

Subjects

Male, medicine.medical_specialty, genetic epidemiology, renal medicine, genetic association studies, 030232 urology & nephrology, Nerve Tissue Proteins, Polymorphism, Single Nucleotide, End stage renal disease, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Internal medicine, Germany, Restless Legs Syndrome, mental disorders, Genetics, Genetic predisposition, Medicine, Humans, Restless legs syndrome, Myeloid Ecotropic Viral Integration Site 1 Protein, Genetics (clinical), Alleles, Genetic association, Aged, Homeodomain Proteins, end-stage renal disease, Greece, business.industry, Complex Traits, Case-control study, Middle Aged, medicine.disease, Comorbidity, ddc, Neoplasm Proteins, BTBD9, Endocrinology, Genetic epidemiology, movement disorders (other than Parkinson's), Case-Control Studies, Kidney Failure, Chronic, Female, business, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Background Restless legs syndrome (RLS) is a sleep related movement disorder that occurs both in an idiopathic form and in symptomatic varieties. RLS is a frequent and distressing comorbidity in end stage renal disease (ESRD). For idiopathic RLS (iRLS), genetic risk factors have been identified, but their role in RLS in ESRD has not been investigated yet. Therefore, a caseecontrol association study of these variants in ESRD patients was performed. Methods The study genotyped 10 iRLS associated variants at four loci encompassing the genes MEIS1, BTBD9, MAP2K5/SKOR1, and PTPRD, in two independent caseecontrol samples from Germany and Greece using multiplex PCR and MALDI-TOF (matrix assisted laser desorption/ionisation time-of-flight) mass spectrometry. Statistical analysis was performed as logistic regression with age and gender as covariates. For the combined analysis a CochraneManteleHaenszel test was applied. Results The study included 200 RLS-positive and 443 RLS-negative ESRD patients in the German sample, and 141 and 393 patients, respectively, in the Greek sample. In the German sample, variants in MEIS1 and BTBD9 were associated with RLS in ESRD (Pnom#0.004, ORs 1.52 and 1.55), whereas, in the Greek sample, there was a trend for association to MAP2K5/SKOR1 and BTBD9 (Pnom#0.08, ORs 1.41 and 1.33). In the combined analysis including all samples, BTBD9 was associated after correction for multiple testing (Pcorrected¼0.0013, OR 1.47). Conclusions This is the first demonstration of a genetic influence on RLS in ESRD patients with BTBD9 being significantly associated. The extent of the genetic predisposition could vary between different subgroups of RLS in ESRD.

Published

2011

29. CDKN2BAS is associated with periodontitis in different European populations is activated by bacterial infection

Author

Markus Reinartz, Barbara Noack, Stefan Schreiber, Gesa M. Richter, Marja L. Laine, Michael Nothnagel, Henrik Dommisch, Bruno G. Loos, Birte Groessner-Schreiber, Arne S. Schaefer, Mathias Folwaczny, Søren Jepsen, Periodontology, Preventive Dentistry, Parodontologie (OII, ACTA), and Preventieve tandheelkunde (OII, ACTA)

Subjects

Male, Gingiva, Linkage Disequilibrium, 0302 clinical medicine, Gene Frequency, Aggressive periodontitis, Genetics (clinical), 0303 health sciences, education.field_of_study, biology, Bacterial Infections, 3. Good health, Up-Regulation, Aggressive Periodontitis, Female, Porphyromonas gingivalis, Adult, Population, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, White People, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Genetics, medicine, Humans, Genetic Predisposition to Disease, RNA, Antisense, RNA, Messenger, education, Periodontitis, Cyclin-Dependent Kinase Inhibitor p16, Genetic Association Studies, 030304 developmental biology, Cyclin-Dependent Kinase Inhibitor p15, CDKN2BAS, Cyclin-Dependent Kinase 4, Epithelial Cells, 030206 dentistry, Fibroblasts, medicine.disease, biology.organism_classification, Chronic periodontitis, Genetic epidemiology, Streptococcus gordonii, Immunology, Chronic Periodontitis

Abstract

Epidemiological studies have indicated a relationship between coronary heart disease (CHD) and periodontitis. Recently, CDKN2BAS was reported as a shared genetic risk factor of CHD and aggressive periodontitis (AgP), but the causative variant has remained unknown. To identify and validate risk variants in different European populations, we first explored 150 kb of the genetic region of CDKN2BAS including the adjacent genes CDKN2A and CDKN2B, covering 51 tagging single nucleotide polymorphisms (tagSNPs) in AgP and chronic periodontitis (CP) in individuals of Dutch origin (n=313). In a second step, we tested the significant SNP associations in an independent AgP and CP population of German origin (n=1264). For the tagSNPs rs1360590, rs3217992, and rs518394, we could validate the associations with AgP before and after adjustment for the covariates smoking, gender and diabetes, with SNP rs3217992 being the most significant (OR 1.48, 95% CI 1.19 to 1.85; p=0.0004). We further showed in vivo gene expression of CDKN2BAS, CDKN2A, CDKN2B, and CDK4 in healthy and inflamed gingival epithelium (GE) and connective tissue (CT), and detected a significantly higher expression of CDKN2BAS in healthy CT compared to GE (p=0.004). After 24 h of stimulation with Porphyromonas gingivalis in Streptococcus gordonii pre-treated gingival fibroblast (HGF) and cultured gingival epithelial cells (GECs), we observed a 25-fold and fourfold increase of CDKN2BAS gene expression in HGFs (p=0.003) and GECs (p=0.004), respectively. Considering the global importance of CDKN2BAS in the disease risk of CHD, this observation supports the theory of inflammatory components in the disease physiology of CHD.

Published

2011

30. Understanding polygenic models, their development and the potential application of polygenic scores in healthcare.

Author

Babb de Villiers C, Kroese M, and Moorthie S

Subjects

Delivery of Health Care, Genomics trends, Humans, Polymorphism, Single Nucleotide genetics, Genetic Predisposition to Disease, Genome-Wide Association Study, Multifactorial Inheritance genetics

Abstract

The use of genomic information to better understand and prevent common complex diseases has been an ongoing goal of genetic research. Over the past few years, research in this area has proliferated with several proposed methods of generating polygenic scores. This has been driven by the availability of larger data sets, primarily from genome-wide association studies and concomitant developments in statistical methodologies. Here we provide an overview of the methodological aspects of polygenic model construction. In addition, we consider the state of the field and implications for potential applications of polygenic scores for risk estimation within healthcare., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2020

31. Association between genetic polymorphisms and endometrial cancer risk: a systematic review.

Author

Bafligil C, Thompson DJ, Lophatananon A, Smith MJ, Ryan NA, Naqvi A, Evans DG, and Crosbie EJ

Subjects

Aromatase genetics, Endometrial Neoplasms epidemiology, Endometrial Neoplasms pathology, Female, Hepatocyte Nuclear Factor 1-beta genetics, Humans, Kruppel-Like Transcription Factors genetics, Polymorphism, Single Nucleotide genetics, Prospective Studies, Proto-Oncogene Proteins c-mdm2 genetics, Proto-Oncogene Proteins c-myc genetics, Risk Factors, SOXC Transcription Factors genetics, eIF-2 Kinase genetics, Endometrial Neoplasms genetics, Genetic Predisposition to Disease, Genome-Wide Association Study

Abstract

Introduction: Endometrial cancer is one of the most commonly diagnosed cancers in women. Although there is a hereditary component to endometrial cancer, most cases are thought to be sporadic and lifestyle related. The aim of this study was to systematically review prospective and retrospective case-control studies, meta-analyses and genome-wide association studies to identify genomic variants that may be associated with endometrial cancer risk., Methods: We searched MEDLINE, Embase and CINAHL from 2007 to 2019 without restrictions. We followed PRISMA 2009 guidelines. The search yielded 3015 hits in total. Following duplicate exclusion, 2674 abstracts were screened and 453 full-texts evaluated based on our pre-defined screening criteria. 149 articles were eligible for inclusion., Results: We found that single nucleotide polymorphisms (SNPs) in HNF1B , KLF , EIF2AK , CYP19A1 , SOX4 and MYC were strongly associated with incident endometrial cancer. Nineteen variants were reported with genome-wide significance and a further five with suggestive significance. No convincing evidence was found for the widely studied MDM2 variant rs2279744. Publication bias and false discovery rates were noted throughout the literature., Conclusion: Endometrial cancer risk may be influenced by SNPs in genes involved in cell survival, oestrogen metabolism and transcriptional control. Larger cohorts are needed to identify more variants with genome-wide significance., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY. Published by BMJ.)

Published

2020

32. Risk of metastatic pheochromocytoma and paraganglioma in SDHx mutation carriers: a systematic review and updated meta-analysis.

Author

Lee H, Jeong S, Yu Y, Kang J, Sun H, Rhee JK, and Kim YH

Subjects

Adrenal Gland Neoplasms genetics, Adrenal Gland Neoplasms pathology, Germ-Line Mutation genetics, Heterozygote, Humans, Mitochondrial Proteins genetics, Neoplasm Metastasis, Paraganglioma pathology, Pheochromocytoma pathology, Electron Transport Complex II genetics, Membrane Proteins genetics, Paraganglioma genetics, Pheochromocytoma genetics, Succinate Dehydrogenase genetics

Abstract

Background: Pheochromocytoma and paraganglioma (PPGL) are tumours that arise from chromaffin cells. Some genetic mutations influence PPGL, among which, those in genes encoding subunits of succinate dehydrogenase (SDHA, SDHB, SDHC and SDHD) and assembly factor (SDHAF2) are the most relevant. However, the risk of metastasis posed by these mutations is not reported except for SDHB and SDHD mutations. This study aimed to update the metastatic risks, considering prevalence and incidence of each SDHx mutation, which were dealt formerly all together., Methods: We searched EMBASE and MEDLINE and selected 27 articles. The patients included in the studies were divided into three groups depending on the presence of PPGL. We checked the heterogeneity between studies and performed a meta-analysis using Hartung-Knapp-Sidik-Jonkman method based on a random effect model., Results: The highest PPGL prevalence was for SDHB mutation, ranging from 23% to 31%, and for SDHC mutation (23%), followed by that for SDHA mutation (16%). The lowest prevalence was for SDHD mutation, ranging from 6% to 8%. SDHAF2 mutation showed no metastatic events. The PPGL incidence showed a tendency similar to that of its prevalence with the highest risk of metastasis posed by SDHB mutation (12%-41%) and the lowest risk by SDHD mutation (~4%)., Conclusion: There was no integrated evidence of how SDHx mutations are related to metastatic PPGL. However, these findings suggest that SDHA, SDHB and SDHC mutations are highly associated and should be tested as indicators of metastasis in patients with PPGL., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2020. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2020

33. Natural course of Fabry disease: changing pattern of causes of death in FOS - Fabry Outcome Survey

Author

Mathias Beck, Atul Mehta, Roberto Giugliani, Aleš Linhart, Perry M. Elliott, Gere Sunder-Plassmann, Jtr Clarke, Royal Free Hospital, London, Hospital for Sick Children, Toronto, Hospital de Clínicas de Porto Alegre (HCPA), The Heart Hospital [London], University College of London [London] (UCL), Charles University [Prague] (CU), University of Mainz, Johannes Gutenberg - Universität Mainz (JGU), and Medizinische Universität Wien = Medical University of Vienna

Subjects

Adult, Male, medicine.medical_specialty, Metabolic disorders, Cardiomyopathy, Disease, 030204 cardiovascular system & hematology, Cohort Studies, 03 medical and health sciences, Sex Factors, 0302 clinical medicine, Cause of Death, Internal medicine, Genetics, medicine, Humans, Lipid disorders, Genetic epidemiology, Child, Genetics (clinical), Cause of death, Chi-Square Distribution, Vascular disease, business.industry, Data Collection, Enzyme replacement therapy, medicine.disease, Fabry disease, 3. Good health, Cohort, Fabry Disease, Female, Kidney Diseases, business, 030217 neurology & neurosurgery, Cohort study

Abstract

Background: Fabry disease is a rare X-linked lysosomal storage disorder characterised by severe multisystemic involvement that leads to major organ failure and premature death in affected men and women. Over the past 7 years, the Fabry Outcome Survey (FOS) has collected data on the natural history of Fabry disease, and the long-term efficacy and safety of enzyme-replacement therapy. This paper provides an update on the first analysis of FOS data. Design: Baseline data on clinical manifestations and causes of death in a cohort of 1453 patients (699 male, 754 female) from 19 countries worldwide were analysed. Causes of death of affected relatives were analysed separately. Results: The most frequently reported signs and symptoms of Fabry disease were neurological. Cardiac, ocular, gastrointestinal, dermatological, auditory and renal manifestations were also common. The principal causes of death among 181 affected relatives of patients in FOS (most of whom had died before 2001) were renal failure in males (42%) and cerebrovascular disease in females (25%). In contrast, of the 42 patients enrolled in FOS whose deaths were reported between 2001 and 2007, cardiac disease was the main cause of death in both male (34%) and female (57%) patients. Conclusion: These data suggest that the importance of renal disease as a cause of death in patients with Fabry disease is decreasing while the importance of cardiac disease is increasing. This pattern probably reflects improvements in the management of renal disease in patients with Fabry disease.

Published

2009

34. Case-only exome sequencing and complex disease susceptibility gene discovery: study design considerations

Author

Hu Li, Hugues Sicotte, Eric D. Wieben, Daniel J. Schaid, Lang Wu, and Gloria M. Petersen

Subjects

Genetics, medicine.medical_specialty, Clinical study design, Complex disease, Susceptibility gene, Sequence Analysis, DNA, Biology, Article, Phenotype, Genetic epidemiology, Research Design, Molecular genetics, Susceptibility locus, medicine, Humans, Exome, Genetic Predisposition to Disease, Genetics (clinical), Exome sequencing, Genetic Association Studies

Abstract

Whole exome sequencing (WES) provides an unprecedented opportunity to identify the potential aetiological role of rare functional variants in human complex diseases. Large-scale collaborations have generated germline WES data on patients with a number of diseases, especially cancer, but less often on healthy controls under the same sequencing procedures. These data can be a valuable resource for identifying new disease susceptibility loci if study designs are appropriately applied. This review describes suggested strategies and technical considerations when focusing on case-only study designs that use WES data in complex disease scenarios. These include variant filtering based on frequency and functionality, gene prioritisation, interrogation of different data types and targeted sequencing validation. We propose that if case-only WES designs were applied in an appropriate manner, new susceptibility genes containing rare variants for human complex diseases can be detected.

Published

2014

35. High risk of tobacco-related cancers in CDKN2A mutation-positive melanoma families

Author

Göran Jönsson, Johan Hansson, Hildur Helgadottir, Christian Ingvar, Rainer Tuominen, Håkan Olsson, Åke Borg, and Veronica Höiom

Subjects

Adult, Male, Risk, Oncology, medicine.medical_specialty, Cancer: head and neck, Adolescent, Genetic screening/counselling, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, CDKN2A, Neoplasms, Internal medicine, Pancreatic cancer, Cancer Genetics, Genetics, medicine, Humans, Genetic epidemiology, Genetic Predisposition to Disease, Prospective Studies, Cancer: lung, First-degree relatives, Child, Prospective cohort study, Cyclin-Dependent Kinase Inhibitor p16, Genetics (clinical), Aged, 030304 developmental biology, Aged, 80 and over, 0303 health sciences, business.industry, Smoking, Cancer, Odds ratio, Middle Aged, medicine.disease, Cancer: dermatological, 3. Good health, Cancer registry, Child, Preschool, 030220 oncology & carcinogenesis, Mutation, Immunology, Female, business

Abstract

Background Germline mutations in the tumour suppressor gene CDKN2A occur in 5–20% of familial melanoma cases. A single founder mutation, p.Arg112dup, accounts for the majority of CDKN2A mutations in Swedish carriers. In a national program, carriers of p.Arg112dup mutation have been identified. The aim of this study was to assess cancer risks in p.Arg112dup carriers and their first degree relatives (FDRs) and second degree relatives (SDRs). Methods In this prospective cohort study, cancer diagnoses in carriers (n=120), non-carriers (n=111), carriers’ FDRs (n=275) and SDRs (n=321) and controls (n=3976) were obtained from the Swedish Cancer Registry. Relative risks (RRs) for cancers were calculated (number of cancers/person years). Two-sided 95% CIs were calculated for all RRs. Results In carriers prospective RR for non-melanoma cancers was 5.0 (95% CI 3.7 to 7.3), for pancreatic cancer 43.8 (95% CI 13.8 to 139.0), for cancers in upper digestive tissues 17.1 (95% CI 6.3 to 46.5), and in respiratory tissues 15.6 (5.4 to 46.0). In FDRs and SDRs RRs were significantly elevated for cancers in pancreas, respiratory and upper digestive tissues. In ever-smoking carriers compared with never-smoking carriers, the odds ratio (OR) of cancers in pancreas, respiratory or upper digestive tissues was 9.3 (95% CI 1.9 to 44.7). Conclusions CDKN2A p.Arg112dup mutation carriers from melanoma-prone families and their FDRs and SDRs have elevated risk for pancreatic, lung, head and neck and gastro-oesophageal carcinomas. These cancers were mainly seen in ever-smoking carriers. Germline CDKN2A mutations may confer an increased sensitivity to carcinogens in tobacco smoke. CDKN2A mutation carriers should be counselled to abstain from smoking.

Published

2014

36. Haplotypes of the inducible nitric oxide synthase gene are strongly associated with exhaled nitric oxide levels in adults: a population-based study

Author

Åsa Torinsson Naluai, Santosh Dahgam, Anna-Carin Olin, Fredrik Nyberg, and Lars Modig

Subjects

Adult, Male, Nitric Oxide Synthase Type II, Single-nucleotide polymorphism, Nitric Oxide, Polymorphism, Single Nucleotide, Linkage Disequilibrium, parasitic diseases, Genetics, Humans, Gene, Genetics (clinical), Genetic Association Studies, Genetic association, Aged, biology, Haplotype, Middle Aged, Molecular biology, Asthma, Nitric oxide synthase, Population based study, Genetic epidemiology, Haplotypes, Exhalation, Immunology, Exhaled nitric oxide, biology.protein

Abstract

Previous genetic association studies have reported evidence for association of single-nucleotide polymorphisms (SNPs) in the NOS2 gene, encoding inducible nitric oxide synthase (iNOS), to variation in levels of fractional exhaled nitric oxide (FENO) in children and adults. In this study, we evaluated 10 SNPs in the region of chromosome 17 from 26.07 Mb to 26.13 Mb to further understand the contribution of NOS2 to variation in levels of FENO.In a cohort of 5912 adults 25-75 years of age, we investigated the relationship between NOS2 haplotypes and FENO, and effect modification by asthma.Seven common (frequency ≥5%) haplotypes (H1-H7) were inferred from all possible haplotype combinations. One haplotype (H3) was significantly associated with lower levels of FENO: -5.8% (95% CI -9.8 to -1.7; p=0.006) compared with the most common baseline haplotype H1. Two haplotypes (H5 and H6) were significantly associated with higher levels of FENO: +10.7% (95% CI 5.0 to 16.7; p=0.0002) and +14.9% (95% CI 10.6 to 19.3; p=7.8×10(-13)), respectively. The effect of haplotype H3 was mainly seen in subjects with asthma (-21.6% (95% CI -33.5 to -5.9)) and was not significant in subjects without asthma (-4.2% (95% CI -8.4 to 0.2)). The p value for interaction between H3 and asthma status was 0.004.Our findings suggest that several common haplotypes in the NOS2 gene contribute to variation in FENO in adults. We also saw some evidence of effect modification by asthma status on haplotype H3.

Published

2014

37. A genome-wide association study suggests that a locus within the ataxin 2 binding protein 1 gene is associated with hand osteoarthritis: the Treat-OA consortium

Author

M. Kloppenburg, Deborah J. Hart, Michael Inouye, Bernet S. Kato, Feng Zhang, Eline Slagboom, Tim D. Spector, Ingrid Meulenbelt, Guangju Zhai, André G. Uitterlinden, Panagiotis Deloukas, Gregory Livshits, Ana M. Valdes, J. B. Richards, J.B. van Meurs, Nicole Soranzo, Frances M K Williams, Department of Twin Research & Genetic Epidemiology, King's College London, Erasmus University Medical Center [Rotterdam] (Erasmus MC), Tel Aviv University [Tel Aviv], Section Molecular Epidemiology, Leiden University Medical Center (LUMC), The Wellcome Trust Sanger Institute [Cambridge], and Department of Rheumatology and Clinical Epidemiology, Leiden University Medical Center (LUMC)

Subjects

Male, Short Report, Single-nucleotide polymorphism, Genome-wide association study, Locus (genetics), Biology, Polymorphism, Single Nucleotide, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Osteoarthritis, Genetics, Humans, SNP, Genetic Predisposition to Disease, Genetic epidemiology, Prospective Studies, Allele, Prospective cohort study, Gene, Genetics (clinical), 030304 developmental biology, 030203 arthritis & rheumatology, 0303 health sciences, RNA-Binding Proteins, Hand, 3. Good health, Female, RNA Splicing Factors, Genome-Wide Association Study

Abstract

To identify the susceptibility gene in hand osteoarthritis (OA) the authors used a two-stage approach genomewide association study using two discovery samples (the TwinsUK cohort and the Rotterdam discovery subset; a total of 1804 subjects) and four replication samples (the Chingford Study, the Chuvasha Skeletal Aging Study, the Rotterdam replication subset and the Genetics, Arthrosis, and Progression (GARP) Study; a total of 3266 people). Five single-nucleotide polymorphisms (SNPs) had a likelihood of association with hand OA in the discovery stage and one of them (rs716508), was successfully confirmed in the replication stage (meta-analysis p = 1.81×10 -5). The C allele conferred a reduced risk of 33% to 41% using a case-control definition. The SNP is located in intron 1 of the A2BP1 gene. This study also found that the same allele of the SNP significantly reduced bone density at both the hip and spine (p

Published

2009

38. Genetic characteristics of retinitis pigmentosa in 1204 Japanese patients.

Author

Koyanagi Y, Akiyama M, Nishiguchi KM, Momozawa Y, Kamatani Y, Takata S, Inai C, Iwasaki Y, Kumano M, Murakami Y, Omodaka K, Abe T, Komori S, Gao D, Hirakata T, Kurata K, Hosono K, Ueno S, Hotta Y, Murakami A, Terasaki H, Wada Y, Nakazawa T, Ishibashi T, Ikeda Y, Kubo M, and Sonoda KH

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Female, Gene Frequency, Genetic Variation, High-Throughput Nucleotide Sequencing, Humans, Japan, Male, Middle Aged, Mutation, Retinitis Pigmentosa diagnosis, Sequence Analysis, DNA, Usher Syndromes diagnosis, Young Adult, Asian People genetics, Retinitis Pigmentosa genetics, Usher Syndromes genetics

Abstract

Background: The genetic profile of retinitis pigmentosa (RP) in East Asian populations has not been well characterised. Therefore, we conducted a large-scale sequencing study to investigate the genes and variants causing RP in a Japanese population., Methods: A total of 1209 Japanese patients diagnosed with typical RP were enrolled. We performed deep resequencing of 83 known causative genes of RP using next-generation sequencing. We defined pathogenic variants as those that were putatively deleterious or registered as pathogenic in the Human Gene Mutation Database or ClinVar database and had a minor allele frequency in any ethnic population of ≤0.5% for recessive genes or ≤0.01% for dominant genes as determined using population-based databases., Results: We successfully sequenced 1204 patients with RP and determined 200 pathogenic variants in 38 genes as the cause of RP in 356 patients (29.6%). Variants in six genes ( EYS , USH2A , RP1L1 , RHO , RP1 and RPGR ) caused RP in 65.4% (233/356) of those patients. Among autosomal recessive genes, two known founder variants in EYS [p.(Ser1653fs) and p.(Tyr2935*)] and four East Asian-specific variants [p.(Gly2752Arg) in USH2A , p.(Arg658*) in RP1L1 , p.(Gly2186Glu) in EYS and p.(Ile535Asn) in PDE6B ] and p.(Cys934Trp) in USH2A were found in ≥10 patients. Among autosomal dominant genes, four pathogenic variants [p.(Pro347Leu) in RHO , p.(Arg872fs) in RP1 , p.(Arg41Trp) in CRX and p.(Gly381fs) in PRPF31 ] were found in ≥4 patients, while these variants were unreported or extremely rare in both East Asian and non-East Asian population-based databases., Conclusions: East Asian-specific variants in causative genes were the major causes of RP in the Japanese population., Competing Interests: Competing interests: SU reports personal fees from Nidek, Chuo Sangio, Santen and Alcon outside the submitted work. AM reports grants from Pfizer Japan, Abbott Japan, Otsuka Pharmaceutical, Eisai, Alcon Japan, Novartis Pharma KK, SEED and Santen Pharmaceutical, and personal fees from Lion Japan outside the submitted work. In addition, AM has a patent hydrogel contact lens for gene treatment licensed. HT reports personal fees from Rohto Pharmaceutical, Takeda Pharmaceutical, Mitsubishi Tanabe, AbbVie, Daiichi Sankyo, Chuo Sangio, Sanofi, Nihon Tenganyaku, Alcon Pharma, Bayer and Graybug Vision, grants and personal fees from Nidek, Otsuka, Pfizer, Santen, Alcon, Novartis, Senju, Kowa and Wakamoto, grants from HOYA and Allergan Japan, and personal fees and non-financial support from Carl Zeiss Meditec outside the submitted work. In addition, HT has a patent pending with Nidek., (© Author(s) (or their employer(s)) 2019. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2019

39. Addition of a 161-SNP polygenic risk score to family history-based risk prediction: impact on clinical management in non- BRCA1/2 breast cancer families.

Author

Lakeman IMM, Hilbers FS, Rodríguez-Girondo M, Lee A, Vreeswijk MPG, Hollestelle A, Seynaeve C, Meijers-Heijboer H, Oosterwijk JC, Hoogerbrugge N, Olah E, Vasen HFA, van Asperen CJ, and Devilee P

Subjects

Adult, Aged, Aged, 80 and over, Alleles, Breast Neoplasms mortality, Breast Neoplasms therapy, Case-Control Studies, Clinical Decision-Making, Disease Management, Genotype, Humans, Middle Aged, Pedigree, Prognosis, Proportional Hazards Models, Risk Assessment, Young Adult, Biomarkers, Tumor, Breast Neoplasms diagnosis, Breast Neoplasms genetics, Genetic Association Studies, Genetic Predisposition to Disease, Polymorphism, Single Nucleotide

Abstract

Background: The currently known breast cancer-associated single nucleotide polymorphisms (SNPs) are presently not used to guide clinical management. We explored whether a genetic test that incorporates a SNP-based polygenic risk score (PRS) is clinically meaningful in non- BRCA1/2 high-risk breast cancer families., Methods: 101 non- BRCA1/2 high-risk breast cancer families were included; 323 cases and 262 unaffected female relatives were genotyped. The 161-SNP PRS was calculated and standardised to 327 population controls (sPRS). Association analysis was performed using a Cox-type random effect regression model adjusted by family history. Updated individualised breast cancer lifetime risk scores were derived by combining the Breast and Ovarian Analysis of Disease Incidence and Carrier Estimation Algorithm breast cancer lifetime risk with the effect of the sPRS., Results: The mean sPRS for cases and their unaffected relatives was 0.70 (SD=0.9) and 0.53 (SD=0.9), respectively. A significant association was found between sPRS and breast cancer, HR=1.16, 95% CI 1.03 to 1.28, p=0.026. Addition of the sPRS to risk prediction based on family history alone changed screening recommendations in 11.5%, 14.7% and 19.8 % of the women according to breast screening guidelines from the USA (National Comprehensive Cancer Network), UK (National Institute for Health and Care Excellence and the Netherlands (Netherlands Comprehensive Cancer Organisation), respectively., Conclusion: Our results support the application of the PRS in risk prediction and clinical management of women from genetically unexplained breast cancer families., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2019. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2019

40. Genetic variants in CHI3L1 influencing YKL-40 levels: resequencing 900 individuals and genotyping 9000 individuals from the general population

Author

Julia S. Johansen, Alisa D. Kjaergaard, Stig E. Bojesen, and Børge G. Nordestgaard

Subjects

musculoskeletal diseases, medicine.medical_specialty, Linkage disequilibrium, Denmark, Population, DNA Mutational Analysis, Single-nucleotide polymorphism, Biology, Linkage Disequilibrium, White People, Adipokines, Molecular genetics, Lectins, Genetics, medicine, SNP, Humans, Chitinase-3-Like Protein 1, Prospective Studies, education, Genotyping, Genetics (clinical), education.field_of_study, Minor allele frequency, Genetic epidemiology

Abstract

Background Despite its important role in many serious diseases, the genetic background for plasma YKL-40 has still not been systematically catalogued. Therefore, we aimed at identifying genetic variants in CHI3L1 influencing plasma YKL-40 levels in the general population. Methods We resequenced the promoter, all 10 exons and exon-flanking intron segments of CHI3L1 in 904 individuals from the Danish general population (n=8899) with extreme plasma YKL-40 levels, adjusted for age. To potentially identify clinically important genetic variants with elevated plasma YKL-40 levels, we included twice as many individuals with the highest plasma YKL-40 levels (n=603) compared with the lowest plasma YKL-40 levels (n=301). Next, we mapped linkage disequilibrium for all variants with a minor allele frequency (MAF)>0.005. Finally, all participants were genotyped for eight variants that had divergent MAFs in the two extreme plasma YKL-40 groups. Results We identified 59 genetic variants in CHI3L1 . Fifteen of the genetic variants were associated with plasma YKL-40 levels. Three promoter SNPs, 1 non-synonymous SNP, and four intronic SNPs in C HI3L1 were associated with plasma YKL-40 levels at or below genome-wide association significance levels (unadjusted p for trend: from 4 × 10 −8 to 6 × 10 −243 ; age adjusted percentiles p for trend: from 3 × 10 −12 to 2 × 10 −304 ). Conclusions In a systematic search to identify genetic variants influencing plasma YKL-40 levels, we identified eight SNPs associated with plasma YKL-40 levels in the general population.

Published

2013

41. Delineating the genetic heterogeneity of ALS using targeted high-throughput sequencing

Author

Colette Donaghy, Mark Heverin, Marwa Elamin, Daniel G. Bradley, Russell L. McLaughlin, Derek W. Morris, Paul Cormican, Kevin P. Kenna, Elaine Kenny, Orla Hardiman, and Susan Byrne

Subjects

Genetic Markers, Male, medicine.medical_specialty, Motor Neurone Disease, Penetrance, Biology, TARDBP, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, C9orf72, Molecular genetics, Genetics, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, Amyotrophic lateral sclerosis, Genetics (clinical), 030304 developmental biology, Aged, 0303 health sciences, Genetic heterogeneity, Amyotrophic Lateral Sclerosis, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Middle Aged, medicine.disease, 3. Good health, Phenotype, Genetic epidemiology, Genetic Epidemiology, Screening, Female, Ireland, 030217 neurology & neurosurgery

Abstract

Background Over 100 genes have been implicated in the aetiology of amyotrophic lateral sclerosis (ALS). A detailed understanding of their independent and cumulative contributions to disease burden may help guide various clinical and research efforts. Methods Using targeted high-throughput sequencing, we characterised the variation of 10 Mendelian and 23 low penetrance/tentative ALS genes within a population-based cohort of 444 Irish ALS cases (50 fALS, 394 sALS) and 311 age-matched and geographically matched controls. Results Known or potential high-penetrance ALS variants were identified within 17.1% of patients (38% of fALS, 14.5% of sALS). 12.8% carried variants of Mendelian disease genes (C9orf72 8.78%; SETX 2.48%; ALS2 1.58%; FUS 0.45%; TARDBP 0.45%; OPTN 0.23%; VCP 0.23%. ANG, SOD1, VAPB 0%), 4.7% carried variants of low penetrance/tentative ALS genes and 9.7% (30% of fALS, 7.1% of sALS) carried previously described ALS variants (C9orf72 8.78%; FUS 0.45%; TARDBP 0.45%). 1.6% of patients carried multiple known/potential disease variants, including all identified carriers of an established ALS variant (pA(p.[G287S]) (n=2/2 sALS). Comparison of our results with those from studies of other European populations revealed significant differences in the spectrum of disease variation (p=1.7×10−4). Conclusions Up to 17% of Irish ALS cases may carry high-penetrance variants within the investigated genes. However, the precise nature of genetic susceptibility differs significantly from that reported within other European populations. Certain variants may not cause disease in isolation and concomitant analysis of disease genes may prove highly important.

Published

2013

42. Genetic epidemiology of early onset breast cancer

Author

Diana Eccles, G Royle, Andrew Collins, Newton E. Morton, and Angela J. Marlow

Subjects

Adult, Proband, Oncology, medicine.medical_specialty, Genotype, Genetic counseling, Breast Neoplasms, Biology, Breast cancer, Risk Factors, Internal medicine, Genetics, medicine, Humans, Age of Onset, Genetics (clinical), Aged, Aged, 80 and over, Complex segregation analysis, Middle Aged, medicine.disease, Penetrance, United Kingdom, Pedigree, Genetic epidemiology, Female, Age of onset, Research Article

Abstract

Risks for breast cancer when there is a family history of the disease are usually calculated using data from segregation analyses which favour a single dominant gene with high penetrance. There are, however, at least three loci known to be associated with familial breast cancer (p53, BRCA1, and an as yet unpublished locus) and the frequencies and penetrances of these genes are not likely to be the same. We have attempted to address the problem of which genetic parameters should be used to calculate risks for different patterns of familial breast cancer. Data from 384 nuclear families ascertained through a proband selected for early onset breast cancer were subjected to complex segregation analysis, correcting for ascertainment bias resulting from selection for severe phenotype. Age of onset of breast cancer, incorporated as severity, provides additional information to the segregation model over and above that given by assigning liability classes on the basis of age at observation. The use of this additional parameter in the analysis is described. There is fair agreement between estimates from this sample and previous predictions from consecutive probands and consultands. The differences suggest more than one rare dominant gene for susceptibility to breast cancer, with different penetrances. Although refinements of segregation analysis will help to delineate these different genes, perfect resolution will require identification of the mutant alleles. Methods to estimate genetic parameters under genotype specific mortality need to be developed. Meanwhile, we suggest that high and low estimates of penetrance be used in risk estimation for genetic counselling, and as a guide to candidates for entry into clinical trials of screening and chemoprevention in breast cancer.

Published

1994

43. A genome-wide association study of men with symptoms of testicular dysgenesis syndrome and its network biology interpretation

Author

Jorma Toppari, John E Nielsen, Gabriella Cohn-Cedermark, Marlene D. Dalgaard, Daniel Edsgärd, Gedske Daugaard, Jeremy D. Silver, Thomas Skøt Jensen, Ewa Rajpert-De Meyts, Yvonne Lundberg Giwercman, Tune H. Pers, Søren Brunak, Helena E. Virtanen, Thomas A. Gerds, Aleksander Giwercman, Henrik Leffers, Niels E Skakkebk, Niels Jørgensen, Nils Weinhold, Ramneek Gupta, and Anders Juul

Subjects

Male, Bone Morphogenetic Protein 7, Gonadal dysgenesis, Gene Expression, Genome-wide association study, Bioinformatics, Gonadal Dysgenesis, Linkage Disequilibrium, Male infertility, Cohort Studies, genome-wide, 0302 clinical medicine, Testis, GWAS, genetics, Protein Interaction Maps, Genetics (clinical), Genetics, 0303 health sciences, Stem Cell Factor, diabetes, systems biology, Neoplasms, Germ Cell and Embryonal, 3. Good health, 030220 oncology & carcinogenesis, oncology, Medical genetics, Proteoglycans, epidemiology, infertility, SNP array, reproductive medicine, Adult, Genetic Markers, medicine.medical_specialty, genetic epidemiology, Genotype, testis cancer, Biology, cancer: urological, Polymorphism, Single Nucleotide, 03 medical and health sciences, endocrinology, SDG 3 - Good Health and Well-being, Testicular Neoplasms, medicine, Humans, developmental, Genetic Predisposition to Disease, chromosomal, Testicular cancer, TDS, 030304 developmental biology, Complex Traits, Case-control study, Cancer, medicine.disease, Case-Control Studies, Receptors, Transforming Growth Factor beta, Genome-Wide Association Study

Abstract

Background Testicular dysgenesis syndrome (TDS) is a common disease that links testicular germ cell cancer, cryptorchidism and some cases of hypospadias and male infertility with impaired development of the testis. The incidence of these disorders has increased over the last few decades, and testicular cancer now affects 1% of the Danish and Norwegian male population. Methods To identify genetic variants that span the four TDS phenotypes, the authors performed a genome-wide association study (GWAS) using Affymetrix Human SNP Array 6.0 to screen 488 patients with symptoms of TDS and 439 selected controls with excellent reproductive health. Furthermore, they developed a novel integrative method that combines GWAS data with other TDS-relevant data types and identified additional TDS markers. The most significant findings were replicated in an independent cohort of 671 Nordic men. Results Markers located in the region of TGFBR3 and BMP7 showed association with all TDS phenotypes in both the discovery and replication cohorts. An immunohistochemistry investigation confirmed the presence of transforming growth factor beta receptor type III (TGFBR3) in peritubular and Leydig cells, in both fetal and adult testis. Single-nucleotide polymorphisms in the KITLG gene showed significant associations, but only with testicular cancer. Conclusions The association of single-nucleotide polymorphisms in the TGFBR3 and BMP7 genes, which belong to the transforming growth factor b signalling pathway, suggests a role for this pathway in the pathogenesis of TDS. Integrating data from multiple layers can highlight findings in GWAS that are biologically relevant despite having border significance at currently accepted statistical levels.

Published

2011

44. Genetic architecture of open angle glaucoma and related determinants

Author

Nomdo M. Jansonius, Ben A. Oostra, André G. Uitterlinden, Johannes R. Vingerling, Albert Hofman, Cornelia M. van Duijn, Roger C. W. Wolfs, Caroline C W Klaver, Wishal D. Ramdas, Ayse Demirkan, Fernando Rivadeneira, Yurii S. Aulchenko, A. Cecile J.W. Janssens, Leonieke M E van Koolwijk, Hans G Lemij, Paulus T. V. M. de Jong, Najaf Amin, Netherlands Institute for Neuroscience (NIN), Ophthalmology, Faculteit der Geneeskunde, Epidemiology, Internal Medicine, Clinical Genetics, and Neurosciences

Subjects

Male, Intraocular pressure, genetic structures, Glaucoma, Genome-wide association study, INTRAOCULAR-PRESSURE, Cohort Studies, Rotterdam Study, 0302 clinical medicine, Risk Factors, Prospective Studies, Genetics (clinical), POPULATION, Phylogeny, Aged, 80 and over, 0303 health sciences, education.field_of_study, HERITABILITY, ASSOCIATION, Middle Aged, Explained variation, DISEASES, Female, Glaucoma, Open-Angle, Adult, medicine.medical_specialty, Adolescent, Population, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, 03 medical and health sciences, Young Adult, Age Distribution, Ophthalmology, Genetics, medicine, Humans, Sex Distribution, education, CENTRAL CORNEAL THICKNESS, Intraocular Pressure, 030304 developmental biology, Aged, business.industry, medicine.disease, ROTTERDAM, Cross-Sectional Studies, Genetic epidemiology, 030221 ophthalmology & optometry, business, Genome-Wide Association Study

Abstract

Background Although the vertical cup-disc ratio (VCDR) and intraocular pressure (IOP) are important determinants of open angle glaucoma (OAG), it is unclear to what extent the genetic origin of these traits overlap with those of OAG. We evaluated whether the same genes that determine VCDR and IOP also predict OAG.Methods Genetic risk scores were constructed from single nucleotide polymorphisms (SNPs) using genome wide association data of 9326 participants from the Rotterdam Study cohorts (mean +/- SD age: 64.6 +/- 9.1 years). These risk scores were used to calculate the explained variance of VCDR and IOP in an independent cohort (Erasmus Rucphen Family study) consisting of 1646 participants (mean +/- SD age: 46.8 +/- 14.1 years) and the OAG risk in a subset of the Rotterdam Study cohorts. To evaluate false positive findings, we generated two new variables containing randomly sampled values to serve as a negative control.Results The explained variance of VCDR increased when increasing the number of SNPs included in the risk score, suggesting a polygenic model. We found no clear evidence for a similar model for IOP, suggesting that a small number of SNPs determine the susceptibility to IOP. The SNPs related to IOP in terms of p values contributed little to VCDR. The risk scores associated with VCDR were also associated significantly with OAG. This suggests a common polygenic background for VCDR and OAGConclusions We found evidence for a polygenic model underlying one of the major traits of OAG, VCDR, and OAG itself. The IOP did not show any evidence for such a model.

Published

2010

45. Ancestry informative markers for fine-scale individual assignment to worldwide populations

Author

Asif Javed, Petros Drineas, Jamey Lewis, and Peristera Paschou

Subjects

Genetic Markers, Internationality, Genetic genealogy, Population, Population genetics, Ancestry-informative marker, Human genetic variation, Computational biology, Biology, Genetic variation, Databases, Genetic, Genetics, Humans, International HapMap Project, education, Genetics (clinical), Oligonucleotide Array Sequence Analysis, education.field_of_study, Principal Component Analysis, Genome, Human, Decision Trees, Genetic Variation, Reproducibility of Results, Genetics, Population, Genetic epidemiology, Haplotypes, Genealogy and Heraldry

Abstract

Background and aims The analysis of large-scale genetic data from thousands of individuals has revealed the fact that subtle population genetic structure can be detected at levels that were previously unimaginable. Using the Human Genome Diversity Panel as reference (51 populations - 650,000 SNPs), this works describes a systematic evaluation of the resolution that can be achieved for the inference of genetic ancestry, even when small panels of genetic markers are used. Methods and results A comprehensive investigation of human population structure around the world is undertaken by leveraging the power of Principal Components Analysis (PCA). The problem is dissected into hierarchical steps and a decision tree for the prediction of individual ancestry is proposed. A complete leave-one-out validation experiment demonstrates that, using all available SNPs, assignment of individuals to their self-reported populations of origin is essentially perfect. Ancestry informative genetic markers are selected using two different metrics (In and correlation with PCA scores). A thorough cross-validation experiment indicates that, in most cases here, the number of SNPs needed for ancestry inference can be successfully reduced to less than 0.1% of the original 650,000 while retaining close to 100% accuracy. This reduction can be achieved using a novel clustering-based redundancy removal algorithm that is also introduced here. Finally, the applicability of our suggested SNP panels is tested on HapMap Phase 3 populations. Conclusion The proposed methods and ancestry informative marker panels, in combination with the increasingly more comprehensive databases of human genetic variation, open new horizons in a variety of fields, ranging from the study of human evolution and population history, to medical genetics and forensics.

Published

2010

46. Tumour risks and genotype-phenotype correlations associated with germline variants in succinate dehydrogenase subunit genes SDHB , SDHC and SDHD .

Author

Andrews KA, Ascher DB, Pires DEV, Barnes DR, Vialard L, Casey RT, Bradshaw N, Adlard J, Aylwin S, Brennan P, Brewer C, Cole T, Cook JA, Davidson R, Donaldson A, Fryer A, Greenhalgh L, Hodgson SV, Irving R, Lalloo F, McConachie M, McConnell VPM, Morrison PJ, Murday V, Park SM, Simpson HL, Snape K, Stewart S, Tomkins SE, Wallis Y, Izatt L, Goudie D, Lindsay RS, Perry CG, Woodward ER, Antoniou AC, and Maher ER

Subjects

Adrenal Gland Neoplasms pathology, Age Factors, Aged, Aged, 80 and over, Female, Genetic Association Studies, Genotype, Germ-Line Mutation genetics, Heterozygote, Humans, Kaplan-Meier Estimate, Male, Middle Aged, Mutation, Missense genetics, Paraganglioma pathology, Pheochromocytoma pathology, Risk Factors, Sex Characteristics, Adrenal Gland Neoplasms genetics, Membrane Proteins genetics, Paraganglioma genetics, Pheochromocytoma genetics, Succinate Dehydrogenase genetics

Abstract

Background: Germline pathogenic variants in SDHB/SDHC / SDHD are the most frequent causes of inherited phaeochromocytomas/paragangliomas. Insufficient information regarding penetrance and phenotypic variability hinders optimum management of mutation carriers. We estimate penetrance for symptomatic tumours and elucidate genotype-phenotype correlations in a large cohort of SDHB/SDHC / SDHD mutation carriers., Methods: A retrospective survey of 1832 individuals referred for genetic testing due to a personal or family history of phaeochromocytoma/paraganglioma. 876 patients (401 previously reported) had a germline mutation in SDHB/SDHC / SDHD (n=673/43/160). Tumour risks were correlated with in silico structural prediction analyses., Results: Tumour risks analysis provided novel penetrance estimates and genotype-phenotype correlations. In addition to tumour type susceptibility differences for individual genes, we confirmed that the SDHD: p.Pro81Leu mutation has a distinct phenotype and identified increased age-related tumour risks with highly destabilising SDHB missense mutations. By Kaplan-Meier analysis, the penetrance (cumulative risk of clinically apparent tumours) in SDHB and (paternally inherited) SDHD mutation-positive non-probands (n=371/67 with detailed clinical information) by age 60 years was 21.8% (95% CI 15.2% to 27.9%) and 43.2% (95% CI 25.4% to 56.7%), respectively. Risk of malignant disease at age 60 years in non-proband SDHB mutation carriers was 4.2%(95% CI 1.1% to 7.2%). With retrospective cohort analysis to adjust for ascertainment, cumulative tumour risks for SDHB mutation carriers at ages 60 years and 80 years were 23.9% (95% CI 20.9% to 27.4%) and 30.6% (95% CI 26.8% to 34.7%)., Conclusions: Overall risks of clinically apparent tumours for SDHB mutation carriers are substantially lower than initially estimated and will improve counselling of affected families. Specific genotype-tumour risk associations provides a basis for novel investigative strategies into succinate dehydrogenase-related mechanisms of tumourigenesis and the development of personalised management for SDHB/SDHC / SDHD mutation carriers., Competing Interests: Competing interests: None declared., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2018. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2018

47. A protein truncating BRCA1 allele with a low penetrance of breast cancer

Author

Steven A. Narod, Janusz Menkiszak, Bohdan Górski, Jacek Gronwald, and Jakub Lubiński

Subjects

Adult, medicine.medical_specialty, endocrine system diseases, Population, Genes, BRCA1, Breast Neoplasms, Penetrance, Biology, medicine.disease_cause, Breast cancer, Risk Factors, Molecular genetics, Genetics, medicine, Humans, Genetic Predisposition to Disease, Allele, skin and connective tissue diseases, education, Genetics (clinical), Alleles, Aged, Aged, 80 and over, Ovarian Neoplasms, education.field_of_study, Mutation, Cancer, Middle Aged, medicine.disease, Peptide Fragments, Genetic epidemiology, Female, Poland, Online Mutation Report, Gene Deletion

Abstract

In the 10 years since the identification of the BRCA1 gene, many cancer families have been tested throughout the world, and there is ongoing interest in estimating the cancer risks for women with mutations in this gene. There is some evidence that families with mutations in the central part of BRCA1 (nucleotides 2401 to 4190) have a higher than expected ratio of ovarian to breast cancers, due to a lower than average risk of breast cancer.1 The absolute and relative risks of breast and ovarian cancers associated with different mutations have been difficult to quantify, in part because of the large number of different mutations in the gene, the rarity of mutations in the general population, and the expense of testing. The majority of established BRCA1 mutations are protein truncating, although a number of deleterious missense mutations have also been identified.2 Poland is ideally suited to the study of the genetic epidemiology of BRCAl mutations because the country is ethnically homogeneous, and because three common BRCA1 mutations comprise 91% of all BRCA1 mutations found in the population.3 Since 1999, we have tested large numbers of …

Published

2004

48. Risk of breast cancer in male BRCA2 carriers

Author

John Dawson, Eamonn R. Maher, Emma R. Woodward, D G R Evans, F Lalloo, and I Susnerwala

Subjects

Adult, Male, Oncology, medicine.medical_specialty, Genetic counseling, Genes, BRCA2, Kaplan-Meier Estimate, Risk Assessment, Breast Neoplasms, Male, Prospective analysis, Breast cancer, Internal medicine, Genetics, Humans, Medicine, Family, Genetic Predisposition to Disease, Prospective Studies, Risk factor, skin and connective tissue diseases, Genetics (clinical), Aged, Retrospective Studies, BRCA2 Protein, business.industry, Age Factors, Cancer, Retrospective cohort study, Middle Aged, medicine.disease, Pedigree, Endocrinology, England, Genetic epidemiology, Mutation, Female, Breast disease, business

Abstract

The risk of breast cancer for unaffected men who test positive for a BRCA2 mutation is based on very few retrospective studies. We have used both retrospective and prospective analysis in 321 families with pathogenic BRCA2 mutations. Three breast cancers occurred in male first-degree relatives after family ascertainment in 4140 years of follow-up suggesting a risk of breast cancer to 80 years of 8.9%. A second analysis excluding index cases identified 16 breast cancers in 905 first-degree male relatives on which Kaplan–Meier analysis was performed after assigning carrier status. This analysis confirmed that breast cancer risk in men was 7.1% (SE 5.2–8.6%) by age 70 years and 8.4% (SE 6.2–10.6%) by age 80 years.

Published

2010

49. Familial clear cell renal cell carcinoma (FCRC): clinical features and mutation analysis of the VHL, MET, and CUL2 candidate genes

Author

Nabeel A. Affara, Emma R. Woodward, Steven C. Clifford, Dewi Astuti, and Eamonn R. Maher

Subjects

Adult, Male, Candidate gene, medicine.medical_specialty, Genetic Linkage, Ubiquitin-Protein Ligases, Cell Cycle Proteins, Biology, urologic and male genital diseases, Proto-Oncogene Mas, Ligases, Germline mutation, Molecular genetics, Genetics, medicine, Genetic predisposition, Humans, Carcinoma, Renal Cell, Genetics (clinical), Polymorphism, Single-Stranded Conformational, Aged, Genetic heterogeneity, Tumor Suppressor Proteins, Proteins, Original Articles, Middle Aged, Proto-Oncogene Proteins c-met, medicine.disease, Cullin Proteins, female genital diseases and pregnancy complications, Kidney Neoplasms, Clear cell renal cell carcinoma, Genetic epidemiology, Von Hippel-Lindau Tumor Suppressor Protein, Clear cell carcinoma, Cancer research, Female, Chromosomes, Human, Pair 3, Carrier Proteins, Chromosomes, Human, Pair 7

Abstract

Familial renal cell carcinoma (RCC) is genetically heterogeneous. Genetic predisposition to clear cell RCC (CCRCC) is a major feature of von Hippel-Lindau (VHL) disease (MIM 193300) and has rarely been associated with chromosome 3 translocations. In addition, familial papillary (non-clear cell) RCC may result from germline mutations in the MET proto-oncogene (MIM 164860). However, rare kindreds with familial CCRCC (FCRC) not linked to the VHL tumour suppressor gene have been described suggesting that further familial RCC susceptibility genes exist. To investigate the genetic epidemiology of FCRC, we undertook a clinical and molecular study of FCRC in nine kindreds with two or more cases of CCRCC in first degree relatives. FCRC was characterised by an earlier age at onset (mean 47.1 years, 52% of cases

Published

2000

50. Association of the CBLB gene with multiple sclerosis: new evidence from a replication study in an Italian population.

Author

Corrado, Lucia, Bergamaschi, Laura, Barizzone, Nadia, Fasano, Maria Edvige, Guerini, Franca R, Salvetti, Marco, Galimberti, Daniela, Benedetti, Maria Donata, Leone, Maurizio, and D'Alfonso, Sandra

Abstract

Background The T allele of rs9657904 within the gene was recently found to be significantly associated with multiple sclerosis (MS) in a genome-wide association study in Sardinia. Objective To replicate this association in an independent population with a different genetic background. Methods The rs9657904 variant was typed in a sample of 1435 cases and 1466 controls from the Italian mainland. Results It was found that in this sample also, the common allele T of rs9657904 is significantly positively associated (one-tailed p=7.35×10) and with a comparable effect size with MS (OR=1.31, 95% CI 1.14 to 1.52). Conclusion These data provide further evidence of the association of MS disease with variation within [ABSTRACT FROM PUBLISHER]

Published

2011