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51. A genome-wide association study identifies only two ancestry specific variants associated with spontaneous preterm birth

Author

Xiaobin Wang, Jeffrey B. Gould, Ronald J. Wong, Marina Sirota, Jason A. Reuter, John Oehlert, Nikolaos A. Patsopoulos, Scott Huntsman, Jonathan Toung, Christopher R. Gignoux, Louis J. Muglia, Gary L. Darmstadt, Dale L. Bodian, Esteban G. Burchard, Michael Snyder, Carlos Bustamante, Nadav Rappoport, Gary M. Shaw, Xiumei Hong, John E. Niederhuber, Weronika Sikora-Wohfeld, Sam S. Oh, Kazumichi Fujioka, David K. Stevenson, Dexter Hadley, Laura L. Jelliffe-Pawlowski, Atul J. Butte, Donglei Hu, Hui Wang, Celeste Eng, Hugh O'Brodovich, Charles Abbott, Ge Zhang, and Elad Ziv

Subjects
0301 basic medicine, Male, lcsh:Medicine, Genome-wide association study, Reproductive health and childbirth, Low Birth Weight and Health of the Newborn, 0302 clinical medicine, Polymorphism (computer science), Infant Mortality, 2.1 Biological and endogenous factors, 030212 general & internal medicine, Aetiology, lcsh:Science, Pediatric, Genetics, education.field_of_study, Multidisciplinary, Continental Population Groups, Incidence (epidemiology), Single Nucleotide, Middle Aged, 3. Good health, Chromosomes, Human, Pair 1, Premature birth, Pair 1, Pair 8, Premature Birth, Female, Chromosomes, Human, Pair 8, Human, Adult, Population, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Article, Chromosomes, 03 medical and health sciences, Preterm, Clinical Research, medicine, Humans, Polymorphism, education, lcsh:R, Racial Groups, Human Genome, Infant, Newborn, Infant, Perinatal Period - Conditions Originating in Perinatal Period, medicine.disease, Newborn, Twin study, Good Health and Well Being, 030104 developmental biology, lcsh:Q, Gene polymorphism
Abstract

Preterm birth (PTB), or the delivery prior to 37 weeks of gestation, is a significant cause of infant morbidity and mortality. Although twin studies estimate that maternal genetic contributions account for approximately 30% of the incidence of PTB, and other studies reported fetal gene polymorphism association, to date no consistent associations have been identified. In this study, we performed the largest reported genome-wide association study analysis on 1,349 cases of PTB and 12,595 ancestry-matched controls from the focusing on genomic fetal signals. We tested over 2 million single nucleotide polymorphisms (SNPs) for associations with PTB across five subpopulations: African (AFR), the Americas (AMR), European, South Asian, and East Asian. We identified only two intergenic loci associated with PTB at a genome-wide level of significance: rs17591250 (P = 4.55E-09) on chromosome 1 in the AFR population and rs1979081 (P = 3.72E-08) on chromosome 8 in the AMR group. We have queried several existing replication cohorts and found no support of these associations. We conclude that the fetal genetic contribution to PTB is unlikely due to single common genetic variant, but could be explained by interactions of multiple common variants, or of rare variants affected by environmental influences, all not detectable using a GWAS alone.

Published
2018

52. GWAS in childhood acute lymphoblastic leukemia reveals novel genetic associations at chromosomes 17q12 and 8q24.21

Author

Semira Gonseth, Xiaorong Xiao, Rong Wang, Josephine Hoh, Adam J. de Smith, Herbert Yu, Andrew T. DeWan, Catherine Metayer, Xiaomei Ma, Ivan Smirnov, Helen M. Hansen, Juhi Ojha, Kyle M. Walsh, Lisa F. Barcellos, Libby M. Morimoto, Stephen S. Francis, Joseph L. Wiemels, and Roberta McKean-Cowdin

Subjects
0301 basic medicine, Oncology, Male, General Physics and Astronomy, Genome-wide association study, California, Gene Frequency, Risk Factors, hemic and lymphatic diseases, 2.1 Biological and endogenous factors, Aetiology, lcsh:Science, Child, Cancer, Pediatric, Multidisciplinary, Single Nucleotide, Hispanic or Latino, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, IKZF3, 3. Good health, Child, Preschool, Cohort, Pair 8, Female, Hispanic Americans, Chromosomes, Human, Pair 8, Human, medicine.medical_specialty, Childhood leukemia, Adolescent, Pediatric Cancer, Childhood Leukemia, Science, Locus (genetics), Biology, Polymorphism, Single Nucleotide, Article, General Biochemistry, Genetics and Molecular Biology, Chromosomes, 03 medical and health sciences, Rare Diseases, Clinical Research, Internal medicine, medicine, Genetics, Humans, Genetic Predisposition to Disease, Polymorphism, Preschool, Allele frequency, Childhood Acute Lymphoblastic Leukemia, Pair 17, Human Genome, Infant, Newborn, Infant, General Chemistry, medicine.disease, Newborn, 030104 developmental biology, Genetic epidemiology, lcsh:Q, Chromosomes, Human, Pair 17, Genome-Wide Association Study
Abstract

Childhood acute lymphoblastic leukemia (ALL) (age 0–14 years) is 20% more common in Latino Americans than non-Latino whites. We conduct a genome-wide association study in a large sample of 3263 Californian children with ALL (including 1949 of Latino heritage) and 3506 controls matched on month and year of birth, sex, and ethnicity, and an additional 12,471 controls from the Kaiser Resource for Genetic Epidemiology Research on Aging Cohort. Replication of the strongest genetic associations is performed in two independent datasets from the Children’s Oncology Group and the California Childhood Leukemia Study. Here we identify new risk loci on 17q12 near IKZF3/ZPBP2/GSDMB/ORMDL3, a locus encompassing a transcription factor important for lymphocyte development (IKZF3), and at an 8q24 region known for structural contacts with the MYC oncogene. These new risk loci may impact gene expression via local (four 17q12 genes) or long-range (8q24) interactions, affecting function of well-characterized hematopoietic and growth-regulation pathways., Childhood acute lymphoblastic leukemia is common in Latino Americans. Here, the authors conduct a genome-wide association study in a Californian cohort containing children of Latino heritage, and identify loci on 17q12 and 8q24 which may affect hematopoietic and growth-regulation pathways.

Published
2018

53. Inherited variant on chromosome 11q23 increases susceptibility to IDH-mutated but not IDH-normal gliomas regardless of grade or histology

Author

Matthew L. Kosel, Helen M. Hansen, Caterina Giannini, Lucie McCoy, Alexander R. Pico, Jesse S. Voss, Brooke L. Fridley, Joseph S. Patoka, Hugues Sicotte, Terri Rice, Jeanette E. Eckel-Passow, Joseph L. Wiemels, George Hsuang, Thomas M. Kollmeyer, Margaret Wrensch, Tarik Tihan, Amanda L. Rynearson, Brian P. O'Neill, Paige M. Bracci, John K. Wiencke, Ivan Smirnov, Yuanyuan Xiao, Daniel H. Lachance, Shichun Zheng, Stephanie R. Fink, Alissa Caron, Michael D. Prados, Susan M. Chang, Paul A. Decker, Kyle M. Walsh, Mitchel S. Berger, and Robert B. Jenkins

Subjects
Male, Cancer Research, Pathology, rs55705857, adult glioma, Chromosomes, Human, 2.1 Biological and endogenous factors, Oligodendroglial Tumor, Pair 11, Aetiology, Cancer, Tumor, Brain Neoplasms, Glioma, Single Nucleotide, Middle Aged, single-nucleotide polymorphism, Prognosis, Isocitrate Dehydrogenase, Editorial, Isocitrate dehydrogenase, Oncology, Basic and Translational Investigations, DNA methylation, rs498872, Pair 8, Female, Chromosomes, Human, Pair 8, Human, Adult, medicine.medical_specialty, IDH1 and IDH2 mutation, Oncology and Carcinogenesis, Locus (genetics), Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Chromosomes, Rare Diseases, Clinical Research, Biomarkers, Tumor, Genetics, medicine, Humans, Genetic Predisposition to Disease, Oncology & Carcinogenesis, Polymorphism, Allele, neoplasms, Neoplasm Staging, Chromosomes, Human, Pair 11, Neurosciences, Case-control study, medicine.disease, Brain Disorders, nervous system diseases, Brain Cancer, Case-Control Studies, Mutation, Cancer research, Neurology (clinical), Neoplasm Grading, Biomarkers
Abstract

We and others first reported several inherited variants that increase glioma risk in 2009.1,2 Additional confirmation and new risk loci have been identified since then.3–8 We9 and Simon et al.10 showed that the glioma risk loci in 8q24 and 11q23 first identified by Shete et al.1 were associated with risk of lower grade infiltrating gliomas but not with glioblastomas. It is now well established that mutation in the isocitrate dehydrogenase (IDH) 1 and 2 genes leads to genome-wide histone and DNA methylation changes that result in abnormal gene expression and gliomagenesis, defining a distinct subclass of gliomas.11,12 IDH mutations occur in ∼50%–80% of grade II-III gliomas and secondary glioblastomas but in fewer than 10% of primary glioblastomas.13–17 Tumor IDH mutations are associated with younger age of onset and better overall survival among patients with gliomas of all grades and histologies18,19 and are also associated with other somatic, genetic, and epigenetic alterations.17,20 Given these observations, we hypothesized that the 8q24 and 11q23 glioma risk loci might be specific to IDH-mutated, but not to IDH-wild-type gliomas. In a separate recent publication,21 we showed that the 8q24 locus is specifically associated with risk for oligodendroglial tumors and IDH-mutated astrocytomas of all grades. Here, we report that the 11q23 glioma risk variant rs498872 T allele is associated with risk of IDH-mutated gliomas but not with risk of IDH-wild-type gliomas, regardless of grade or histology.

Published
2013

54. Co-operative leukemogenesis in acute myeloid leukemia and acute promyelocytic leukemia reveals C/EBPα as a common target of TRIB1 and PML/RARA

Author

Nader Omidvar, Pauline Vieugué, Takuro Nakamura, Loveena Rishi, Shahzya Chaudhury, Lu Liang, Elaine Garcia, Scott C. Kogan, Karen Keeshan, and Coline Gaillard

Subjects
Myeloid, Oncogene Proteins, Fusion, Chromosomal translocation, Trisomy, Cardiorespiratory Medicine and Haematology, Trisomy 8, Mice, Leukemia, Promyelocytic, Acute, hemic and lymphatic diseases, 2.1 Biological and endogenous factors, Aetiology, Cancer, Promyelocytic, Oncogene Proteins, Pediatric, Leukemia, Intracellular Signaling Peptides and Proteins, Myeloid leukemia, Articles, Hematology, Protein-Serine-Threonine Kinases, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Pair 8, Chromosomes, Human, Pair 8, Human, Biotechnology, Acute promyelocytic leukemia, Pediatric Cancer, Childhood Leukemia, Immunology, Context (language use), Biology, Acute, Protein Serine-Threonine Kinases, Chromosomes, Proto-Oncogene Proteins c-myc, Promyelocytic leukemia protein, Rare Diseases, medicine, Genetics, Animals, Humans, Fusion, medicine.disease, Cancer research, biology.protein, CCAAT-Enhancer-Binding Proteins, Bone marrow
Abstract

The PML/RARA fusion protein occurs as a result of the t(15;17) translocation in the acute promyelocytic leukaemia subtype of human acute myeloid leukaemia. Gain of chromosome 8 is the most common chromosomal gain in human acute myeloid leukaemia, including acute promyelocytic leukaemia. We previously demonstrated that gain of chromosome 8-containing MYC is of central importance in trisomy 8, but the role of the nearby TRIB1 gene has not been experimentally addressed in this context. We have now tested the hypothesis that both MYC and TRIB1 have functional roles underlying leukaemogenesis of trisomy 8 by using retroviral vectors to express MYC and TRIB1 in wild-type bone marrow and in marrow that expressed a PML/RARA transgene. Interestingly, although MYC and TRIB1 readily cooperated in leukaemogenesis for wild-type bone marrow, TRIB1 provided no selective advantage to cells expressing PML/RARA. We hypothesized that this lack of cooperation between PML/RARA and TRIB1 reflected a common pathway for their effect: both proteins targeting the myeloid transcription factor C/EBPα. In support of this idea, TRIB1 expression abrogated the All Trans-Retinoic Acid response of acute promyelocytic leukaemia cells in vitro and in vivo. Our data delineate the common and redundant inhibitory effects of TRIB1 and PML/RARA on C/EBPα providing a potential explanation for the lack of selection of TRIB1 in human acute promyelocytic leukaemia, and highlighting the key role of C/EBPs in acute promyelocytic leukaemia pathogenesis and therapeutic response. In addition, the cooperativity we observed between MYC and TRIB1 in the absence of PML/RARA show that, outside of acute promyelocytic leukaemia, gain of both genes may drive selection for trisomy 8.

Published
2016

55. Prostate Cancer Susceptibility in Men of African Ancestry at 8q24

Author

Fredrick R. Schumacher, Dennis J. Hazelett, Anslem J.M. Hennis, Suh Yuh Wu, Xin Sheng, David V. Conti, Dominique Quinque, Brian E. Henderson, Sara S. Strom, Sue A. Ingles, Yao Tettey, Richard B. Biritwum, Bogdan Pasaniuc, Graham Casey, Lisa B. Signorello, Edward D. Yeboah, Shelley Niwa, Anand P. Chokkalingam, Sonja I. Berndt, John D. Carpten, Michael G. Rosenfeld, Stephen J. Chanock, Phyllis J. Goodman, Ying Han, Wei Zheng, Alex Lubwama, M. Cristina Leske, Dimple Notani, Ann W. Hsing, Andrew A. Adjei, Susan M. Gapstur, William J. Blot, Janet L. Stanford, Stephen Watya, Evelyn Tay, Michael B. Cook, Loreall Pooler, Christopher A. Haiman, Victoria L. Stevens, Benjamin A. Rybicki, Lisa Chu, Barbara Nemesure, Ann Truelove, Nadin Rohland, Christine Neslund-Dudas, William B. Isaacs, John S. Witte, Alex Allen, Adam B. Murphy, Suzanne Kolb, Swapan Mallick, David Reich, Rick A. Kittles, Esther M. John, Jianfeng Xu, S. Lilly Zheng, Ranveer Singh Jayani, Gerhard A. Coetzee, Zhaoming Wang, Arti Tandon, Eric A. Klein, Kristin A. Rand, Daniel O. Stram, and Curtis A. Pettaway

Subjects
0301 basic medicine, Oncology, Male, Cancer Research, Aging, Prostate cancer, Prostate, 80 and over, 2.1 Biological and endogenous factors, Aetiology, Cancer, Aged, 80 and over, Prostate Cancer, PROSTATE CANCER SUSCEPTIBILITY, Single Nucleotide, Middle Aged, Control subjects, medicine.anatomical_structure, Pair 8, RNA, Long Noncoding, Long Noncoding, Chromosomes, Human, Pair 8, Human, Urologic Diseases, medicine.medical_specialty, Oncology and Carcinogenesis, Brief Communication, Polymorphism, Single Nucleotide, Chromosomes, 03 medical and health sciences, Clinical Research, Internal medicine, medicine, Genetics, Humans, Genetic Predisposition to Disease, Oncology & Carcinogenesis, Polymorphism, Aged, business.industry, Prevention, Human Genome, Case-control study, Prostatic Neoplasms, Odds ratio, medicine.disease, Confidence interval, United States, Black or African American, 030104 developmental biology, Case-Control Studies, Risk allele, RNA, business
Abstract

The 8q24 region harbors multiple risk variants for distinct cancers, including >8 for prostate cancer. In this study, we conducted fine mapping of the 8q24 risk region (127.8-128.8Mb) in search of novel associations with common and rare variation in 4853 prostate cancer case patients and 4678 control subjects of African ancestry. All statistical tests were two-sided. We identified three independent associations at P values of less than 5.00×10(-8), all of which were replicated in studies from Ghana and Uganda (combined sample = 5869 case patients, 5615 control subjects; rs114798100: risk allele frequency [RAF] = 0.04, per-allele odds ratio [OR] = 2.31, 95% confidence interval [CI] = 2.04 to 2.61, P = 2.38×10(-40); rs72725879: RAF = 0.33, OR = 1.37, 95% CI = 1.30 to 1.45, P = 3.04×10(-27); and rs111906932: RAF = 0.03, OR = 1.79, 95% CI = 1.53 to 2.08, P = 1.39×10(-13)). Risk variants rs114798100 and rs111906923 are only found in men of African ancestry, with rs111906923 representing a novel association signal. The three variants are located within or near a number of prostate cancer-associated long noncoding RNAs (lncRNAs), including PRNCR1, PCAT1, and PCAT2. These findings highlight ancestry-specific risk variation and implicate prostate-specific lncRNAs at the 8q24 prostate cancer susceptibility region.

Published
2016

56. Squalene epoxidase is a bona fide oncogene by amplification with clinical relevance in breast cancer

Author

Irene Caffa, Gabriele Zoppoli, Daniela Piras, Saverio Alberti, Alessio Nencioni, Gabriella Cirmena, Maurizio Gallo, Alberto Ballestrero, David N Brown, and Anna Garuti

Subjects
0301 basic medicine, Transcription, Genetic, Receptor, ErbB-2, Squalene monooxygenase, Gene Dosage, Genes, myc, Gene Expression, Cell Transformation, ErbB-2, 0302 clinical medicine, Transcription (biology), Gene expression, Ovarian Neoplasms, Genetics, Tumor, Multidisciplinary, myc, Prognosis, 3. Good health, Cell Transformation, Neoplastic, 030220 oncology & carcinogenesis, Disease Progression, Pair 8, Female, Transcription, Human, Receptor, Chromosomes, Human, Pair 8, DNA Copy Number Variations, Cell Survival, Copy number alterations, Cholesterol-synthesis, Molecular portraits, Expression analyses, Inhibition, Fungal, Metabolism, NB-598, Genes, Monooxygenase, Breast Neoplasms, Gene dosage, Chromosomes, Article, Cell Line, 03 medical and health sciences, Breast cancer, Genetic, Phénomènes atmosphériques, Cell Line, Tumor, Biomarkers, Tumor, medicine, Humans, Gene silencing, Gene Silencing, Gene, Proportional Hazards Models, Neoplastic, Oncogene, business.industry, Oncogenes, Genetic Loci, Neoplasm Grading, Patient Outcome Assessment, Squalene Monooxygenase, medicine.disease, 030104 developmental biology, Genes, Cancer research, business, Biomarkers
Abstract

SQLE encodes squalene epoxidase, a key enzyme in cholesterol synthesis. SQLE has sporadically been reported among copy-number driven transcripts in multi-omics cancer projects. Yet, its functional relevance has never been subjected to systematic analyses. Here, we assessed the correlation of SQLE copy number (CN) and gene expression (GE) across multiple cancer types, focusing on the clinico-pathological associations in breast cancer (BC). We then investigated whether any biological effect of SQLE inhibition could be observed in BC cell line models. Breast, ovarian, and colorectal cancers showed the highest CN driven GE among 8,783 cases from 22 cancer types, with BC presenting the strongest one. SQLE overexpression was more prevalent in aggressive BC, and was an independent prognostic factor of unfavorable outcome. Through SQLE pharmacological inhibition and silencing in a panel of BC cell lines portraying the diversity of SQLE CN and GE, we demonstrated that SQLE inhibition resulted in a copy-dosage correlated decrease in cell viability, and in a noticeable increase in replication time, only in lines with detectable SQLE transcript. Altogether, our results pinpoint SQLE as a bona fide metabolic oncogene by amplification, and as a therapeutic target in BC. These findings could have implications in other cancer types., SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2016

57. Leukemia-related chromosomal loss detected in hematopoietic progenitor cells of benzene-exposed workers

Author

Zhiying Ji, Qing Lan, Alan Hubbard, Stephen M. Rappaport, Min Shen, Nathaniel Rothman, Roel Vermeulen, Martyn T. Smith, Richard B. Hayes, Luoping Zhang, Guilan Li, Songnian Yin, Martha S. Linet, Cliona M. McHale, and Weihong Guo

Subjects
Myeloid, Male, Cancer Research, Aneuploidy, Trisomy 8, 0302 clinical medicine, Monosomy, In Situ Hybridization, In Situ Hybridization, Fluorescence, 0303 health sciences, Leukemia, leukemia, Myeloid leukemia, Hematology, Prognosis, Haematopoiesis, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Pair 8, Pair 7, Female, Chromosome Deletion, Chromosomes, Human, Pair 7, Human, Chromosomes, Human, Pair 8, Adult, Acute, Biology, Chromosomes, Fluorescence, Article, Colony-Forming Units Assay, 03 medical and health sciences, Occupational Exposure, medicine, Humans, Progenitor cell, 030304 developmental biology, hematopoietic progenitor, Benzene, medicine.disease, Molecular biology, Cross-Sectional Studies, Case-Control Studies, Follow-Up Studies
Abstract

Benzene exposure causes acute myeloid leukemia and hematotoxicity, shown as suppression of mature blood and myeloid progenitor cell numbers. As the leukemia-related aneuploidies monosomy 7 and trisomy 8 previously had been detected in the mature peripheral blood cells of exposed workers, we hypothesized that benzene could cause leukemia through the induction of these aneuploidies in hematopoietic stem and progenitor cells. We measured loss and gain of chromosomes 7 and 8 by fluorescence in situ hybridization in interphase colony-forming unit-granulocyte-macrophage (CFU-GM) cells cultured from otherwise healthy benzene-exposed (n=28) and unexposed (n=14) workers. CFU-GM monosomy 7 and 8 levels (but not trisomy) were significantly increased in subjects exposed to benzene overall, compared with levels in the control subjects (P=0.0055 and P=0.0034, respectively). Levels of monosomy 7 and 8 were significantly increased in subjects exposed to

Published
2012

58. PTEN loss and chromosome 8 alterations in Gleason grade 3 prostate cancer cores predicts the presence of un-sampled grade 4 tumor: implications for active surveillance

Author

Jonathan W. Said, Beatrice S. Knudsen, Tamara L. Lotan, Helen Fedor, H. Ballentine Carter, Bruce J. Trock, Bora Gurel, Robert B. Jenkins, Angelo M. De Marzo, and Samson W. Fine

Subjects
Male, Pathology, medicine.medical_specialty, PTEN, 030232 urology & nephrology, Adenocarcinoma, urologic and male genital diseases, Medical and Health Sciences, Gleason Score 6, Chromosomes, Article, Pathology and Forensic Medicine, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Prostate, Biopsy, medicine, Humans, Gleason grade 3, Chromosome Aberrations, Prostatectomy, Tissue microarray, biology, medicine.diagnostic_test, active surveillance, PTEN Phosphohydrolase, Prostatic Neoplasms, Odds ratio, Middle Aged, medicine.disease, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Pair 8, LPL/8p, Chromosome Deletion, Neoplasm Grading, MYC/8q, Human, Chromosomes, Human, Pair 8
Abstract

Men who enter active surveillance because their biopsy exhibits only Gleason grade 3 (G3) frequently have higher grade tumor missed by biopsy. Thus, biomarkers are needed that, when measured on G3 tissue, can predict the presence of higher grade tumor in the whole prostate. We evaluated whether PTEN loss, chromosome 8q gain (MYC) and/or 8p loss (LPL) measured only on G3 cores is associated with un-sampled G4 tumor. A tissue microarray was constructed of prostatectomy tissue from patients whose prostates exhibited only Gleason score 3+3, only 3+4, or only 4+3 tumor (n=50 per group). Cores sampled only from areas of G3 were evaluated for PTEN loss by immunohistochemistry, and PTEN deletion, LPL/8p loss, and MYC/8q gain by fluorescence in situ hybridization (FISH). Biomarker results were compared between Gleason score 6 vs. 7 tumors using conditional logistic regression. PTEN protein loss, odds ratio=4.99, p=.033, MYC/8q gain, odds ratio=5.36, p=.010, and LPL/8p loss, odds ratio=3.96, p=.003 were significantly more common in G3 cores derived from Gleason 7 vs. Gleason 6 tumors. PTEN gene deletion was not statistically significant. Associations were stronger comparing Gleason 4+3 vs. 6 than for Gleason 3+4 vs. 6. MYC/8q gain, LPL/8p loss, and PTEN protein loss measured in G3 tissue microarray cores strongly differentiate whether the core comes from a Gleason 6 or Gleason 7 tumor. If validated to predict upgrading from G3 biopsy to prostatectomy these biomarkers could reduce the likelihood of enrolling high risk men and facilitate safe patient selection for active surveillance.

Published
2015

59. Autosomal dominant cortical tremor, myoclonus and epilepsy: many syndromes, one phenotype

Author

Pasquale Striano, Federico Zara, Salvatore Striano, Striano, P, Zara, F, and Striano, Salvatore

Subjects
Adult, Male, Benign adult familial myoclonic epilepsy, Adolescent, Genetic Linkage, genetics/physiopathology, Pedigree chart, Locus (genetics), Neurological disorder, Epilepsies, Biology, Chromosomes, Electrocardiography, Epilepsy, Japan, Genetic linkage, Tremor, medicine, Humans, genetics, Genetic Predisposition to Disease, Adolescent, Adult, Aged, Child, Chromosomes, Human, Pair 2, genetics, Chromosomes, Pair 8, genetics, Electrocardiography, Epilepsies, Myoclonic, genetics/physiopathology, Female, Genetic Linkage, Genetic Predisposition to Disease, Humans, Italy, Japan, Male, Middle Aged, Pedigree, Phenotype, Retrospective Studies, Syndrome, Tremor, Child, Aged, Retrospective Studies, Genetic heterogeneity, Syndrome, General Medicine, Middle Aged, medicine.disease, Pedigree, nervous system diseases, Phenotype, Italy, Neurology, Female, Neurology (clinical), medicine.symptom, Neuroscience, Myoclonus
Abstract

The association of cortical tremor, myoclonus and epileptic seizures has been reported in many Japanese and European families with different acronyms. We reviewed the familial cases presenting the clinical picture of autosomal dominant cortical tremor, myoclonus and epilepsy and analysed the phenotypic differences between the pedigrees, according to the recent genetic acquisitions. We concluded that BAFME, FAME, FEME, FCTE and ADCME are the same clinical entity even if genetically heterogeneous, with Japanese families linked to 8q24 and Italian ones to 2p11.1-q12. A third locus could also be involved. Further studies should better clarify the electrophysiological features of this condition and identify the underlying molecular defects.

Published
2005

60. 8p11 myeloproliferative syndrome with a novel t(7;8) translocation leading to fusion of theFGFR1 andTIF1 genes

Author

Bruno Martino, Patrizia Gasparini, Cinzia Tapinassi, Maurizio Trubia, Francesco Lo-Coco, Elena Belloni, Pier Giuseppe Pelicci, Carla Micucci, Paolo Nuciforo, Pier Paolo Di Fiore, and Stefano Confalonieri

Subjects
leukocyte count, fusion, Cancer Research, Oncogene Proteins, Fusion, Oncogene Proteins, pair 7, correlation analysis, pair 8, receptor, myeloproliferative disorder, translocation, Apoptosis, Chromosomal translocation, 8p11 myeloproliferative syndrome, Translocation, Genetic, Receptor tyrosine kinase, oncogene proteins, Genetics, biology, fibroblast growth factor receptor 1, gene product, adult, article, Nuclear Proteins, Syndrome, Middle Aged, symptom, Phenotype, unclassified drug, enzyme activity, type 1, priority journal, chromosome 8p, Female, Chromosomes, Human, Pair 7, Chromosomes, Human, Pair 8, chromosomes, Genotype, Molecular Sequence Data, gene rearrangement, hybrid protein, protein tif1, case report, chromosome translocation 7, clinical feature, female, genotype, human, nucleotide sequence, phenotype, reverse transcription polymerase chain reaction, RNA translation, apoptosis, base sequence, carrier proteins, chromosomes, human, pair 7, humans, middle aged, molecular sequence data, myeloproliferative disorders, myosin heavy chains, oncogene proteins, fusion, receptor protein-tyrosine kinases, receptor, fibroblast growth factor, syndrome, fibroblast growth factor, Settore MED/05 - Patologia Clinica, Humans, Receptor, Fibroblast Growth Factor, Type 1, Kinase activity, Gene, Myeloproliferative Disorders, Base Sequence, Myosin Heavy Chains, Fibroblast growth factor receptor 1, Receptor Protein-Tyrosine Kinases, Receptors, Fibroblast Growth Factor, Fusion protein, stomatognathic diseases, biology.protein, Apoptosis Regulatory Proteins, Carrier Proteins
Abstract

8p11 myeloproliferative syndrome (EMS) is a clinical-pathologic entity characterized by rearrangements involving the FGFR1 gene, which encodes a receptor tyrosine kinase. These rearrangements invariably lead to aberrant fusion proteins in which the kinase activity is constitutively turned on, with resulting oncogenic properties. In this article, we describe a new translocation in EMS, t(7;8)(q34;p11), in which the FGFR1 gene is fused to a previously unidentified partner, the TIF1 gene. We show that both the TIF1-FGFR1 and FGFR1-TIF1 fusion proteins have the potential to be translated as a result of the translocation. Thus, our data extend the involvement of FGFR1 in EMS and lend support to the concept that there is a precise correlation between genotype and phenotype in this disease.

Published
2005

61. Discrepancy Between Fluorescence In Situ Hybridization and Multiplex Ligation-Dependent Probe Amplification in Orbital Recurrence of Uveal Melanoma 26 Years After Enucleation

Author

Suresh Sagili, Sarah E. Coupland, Cornelius Rene, Bertil Damato, and Andrea Russo

Subjects
Male, Uveal Neoplasms, Pathology, Fatal Outcome, Medicine, Multiplex, Melanoma, In Situ Hybridization, Fluorescence, In Situ Hybridization, Tumor, medicine.diagnostic_test, Liver Neoplasms, S100 Proteins, DNA, Neoplasm, General Medicine, Local, Recurrent Melanoma, Pair 3, Pair 8, Chromosomes, Human, Pair 6, Chromosomes, Human, Pair 3, Pair 6, Melanoma-Specific Antigens, Chromosomes, Human, Pair 8, gp100 Melanoma Antigen, Human, medicine.medical_specialty, Enucleation, Chromosomes, Eye Enucleation, Fluorescence, MART-1 Antigen, Late Recurrence, Biomarkers, Tumor, Humans, Multiplex ligation-dependent probe amplification, Aged, Neoplasm Recurrence, Local, Orbital Neoplasms, Multiplex Polymerase Chain Reaction, business.industry, DNA, medicine.disease, Ophthalmology, Neoplasm Recurrence, Chromosome 3, Neoplasm, Surgery, business, Biomarkers, Fluorescence in situ hybridization
Abstract

Cytogenetic analysis has transformed the management of uveal melanoma in recent years and allows categorization of such tumors into low-grade tumors with a favorable prognosis and high-grade tumors that metastasize with a fatal outcome. The authors report the case of a 73-year-old man who presented with recurrent melanoma in his left socket, 26 years after enucleation for uveal melanoma. Chromosomal analysis by multiplex ligation-dependent probe amplification revealed partial loss of chromosome 3 and gains in chromosomes 6 and 8, which were missed with fluorescence in situ hybridization. The patient developed multiple liver metastases 14 months after orbital exenteration and died 8 months later. To the best of authors' knowledge, this is the first report of late recurrence of uveal melanoma after enucleation, in which multiplex ligation-dependent probe amplification chromosomal analysis has been used. The case also highlights the limitations of fluorescence in situ hybridization and the benefits of multiplex ligation-dependent probe amplification, which is more reliable at predicting survival.

Published
2012

62. Unbiased analysis of potential targets of breast cancer susceptibility loci by Capture Hi-C

Author

Steven W. Wingett, Nicola H. Dryden, Takashi Nagano, Stefan Schoenfelder, Nichola Johnson, Maryou B K Lambros, Peter Fraser, Nick Orr, Eleni Perrakis, Frank Dudbridge, Rachael Natrajan, Ioannis Assiotis, Simon Andrews, Sarah Maguire, Kerry Fenwick, Iwanka Kozarewa, Laura Broome, James Campbell, Alan Ashworth, and Olivia Fletcher

Subjects
Method, Genome-wide association study, Regulatory Sequences, Nucleic Acid, Genome, Medical and Health Sciences, Protein Interaction Mapping, 2.1 Biological and endogenous factors, Aetiology, Genetics (clinical), Oligonucleotide Array Sequence Analysis, Cancer, Genetics, Tumor, Research Support, Non-U.S. Gov't, Chromosome Mapping, Single Nucleotide, Biological Sciences, PVT1, Regulatory sequence, Chromosomes, Human, Pair 2, Pair 2, MCF-7 Cells, Pair 8, RNA, Long Noncoding, Long Noncoding, Chromosomes, Human, Pair 9, Sequence Analysis, Chromosomes, Human, Pair 8, Human, Pair 9, Protein Binding, Biotechnology, Hepatocyte Nuclear Factor 3-alpha, Chromatin Immunoprecipitation, Sequence analysis, Bioinformatics, Single-nucleotide polymorphism, Breast Neoplasms, Biology, Real-Time Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Chromosomes, Cell Line, Kruppel-Like Factor 4, Cell Line, Tumor, Breast Cancer, Journal Article, Humans, Genetic Predisposition to Disease, Polymorphism, Gene, Homeodomain Proteins, Nucleic Acid, Genome, Human, Human Genome, Reproducibility of Results, Sequence Analysis, DNA, DNA, RNA, Human genome, Regulatory Sequences, Genome-Wide Association Study
Abstract

Genome-wide association studies have identified more than 70 common variants that are associated with breast cancer risk. Most of these variants map to non-protein-coding regions and several map to gene deserts, regions of several hundred kilobases lacking protein-coding genes. We hypothesized that gene deserts harbor long-range regulatory elements that can physically interact with target genes to influence their expression. To test this, we developed Capture Hi-C (CHi-C), which, by incorporating a sequence capture step into a Hi-C protocol, allows high-resolution analysis of targeted regions of the genome. We used CHi-C to investigate long-range interactions at three breast cancer gene deserts mapping to 2q35, 8q24.21, and 9q31.2. We identified interaction peaks between putative regulatory elements (“bait fragments”) within the captured regions and “targets” that included both protein-coding genes and long noncoding (lnc) RNAs over distances of 6.6 kb to 2.6 Mb. Target protein-coding genes were IGFBP5, KLF4, NSMCE2, and MYC; and target lncRNAs included DIRC3, PVT1, and CCDC26. For one gene desert, we were able to define two SNPs (rs12613955 and rs4442975) that were highly correlated with the published risk variant and that mapped within the bait end of an interaction peak. In vivo ChIP-qPCR data show that one of these, rs4442975, affects the binding of FOXA1 and implicate this SNP as a putative functional variant.

Published
2014

63. Two Functional Lupus-Associated BLK Promoter Variants Control Cell-Type- and Developmental-Stage-Specific Transcription

Author

Joan T. Merrill, R. Hal Scofield, Anne M. Stevens, Diane L. Kamen, Nan Shen, Jennifer A. Kelly, Michelle Petri, Gary S. Gilkeson, Edward K. Wakeland, Carl D. Langefeld, Hye Soon Lee, Kenneth M. Kaufman, Chaim O. Jacob, Robert P. Kimberly, Carol F. Webb, Graham B. Wiley, Xana Kim-Howard, Joel M. Guthridge, Swapan K. Nath, Kathy L. Sivils, Jeffery Edberg, Betty P. Tsao, Harry Sun, Robert R. Graham, Susan A. Boackle, John B. Harley, Elizabeth E. Brown, Xiaoxia Qian, Marta E. Alarcón-Riquelme, Rosalind Ramsey-Goldman, Timothy J. Vyse, Lindsey A. Criswell, Luis M. Vilá, Isaac T.W. Harley, Beth L. Cobb, Judith A. James, John D. Reveille, Timothy W. Behrens, Young Bin Joo, Susan R. Macwana, Celi Sun, Patrick M. Gaffney, So Young Bang, Christopher J. Lessard, Timothy B. Niewold, Jiyoung Choi, Barry I. Freedman, Nicolas Dominguez, Adam Adler, Sang Cheol Bae, and Rufei Lu

Subjects
Male, Transcription, Genetic, Electrophoretic Mobility Shift Assay, Medical and Health Sciences, Transcription (biology), 2.1 Biological and endogenous factors, Lupus Erythematosus, Systemic, Genetics(clinical), Aetiology, Promoter Regions, Genetic, Genetics (clinical), Genetics, Genetics & Heredity, Systemic lupus erythematosus, Single Nucleotide, Biological Sciences, src-Family Kinases, Pair 8, Female, Transcription, Human, Chromosomes, Human, Pair 8, Lupus, Locus (genetics), Biology, Autoimmune Disease, Polymorphism, Single Nucleotide, Chromosomes, Article, Promoter Regions, Genetic, Clinical Research, medicine, Humans, Electrophoretic mobility shift assay, Genetic Predisposition to Disease, Allele, Progenitor cell, Polymorphism, Alleles, Lupus erythematosus, Lupus Erythematosus, Inflammatory and immune system, Haplotype, Systemic, medicine.disease, Stem Cell Research, Molecular biology, Haplotypes
Abstract

Efforts to identify lupus-associated causal variants in the FAM167A/BLK locus on 8p21 are hampered by highly associated noncausal variants. In this report, we used a trans-population mapping and sequencing strategy to identify a common variant (rs922483) in the proximal BLK promoter and a tri-allelic variant (rs1382568) in the upstream alternative BLK promoter as putative causal variants for association with systemic lupus erythematosus. The risk allele (T) at rs922483 reduced proximal promoter activity and modulated alternative promoter usage. Allelic differences at rs1382568 resulted in altered promoter activity in B progenitor cell lines. Thus, our results demonstrated that both lupus-associated functional variants contribute to the autoimmune disease association by modulating transcription of BLK in B cells and thus potentially altering immune responses.

Published
2014

64. RUNX1-ETO induces a type I interferon response which negatively effects t(8;21)-induced increased self-renewal and leukemia development

Author

Joseph R. Biggs, Benjamin Lewin, Stephanie Weng, Russell Dekelver, Ming Yan, and Dong-Er Zhang

Subjects
Cancer Research, Oncogene Proteins, Fusion, Chromosomes, Human, Pair 21, Chromosomal translocation, Receptor, Interferon alpha-beta, Cell Transformation, Translocation, Genetic, Interferon alpha-beta, chemistry.chemical_compound, Mice, RUNX1 Translocation Partner 1 Protein, Interferon, hemic and lymphatic diseases, 2.1 Biological and endogenous factors, Cancer, Mice, Knockout, Oncogene Proteins, Leukemic, Pediatric, Tumor, Leukemia, Gene Expression Regulation, Leukemic, Myeloid leukemia, U937 Cells, interferon, Hematology, Cell Transformation, Neoplastic, Oncology, RUNX1, Interferon Type I, Core Binding Factor Alpha 2 Subunit, Pair 8, medicine.drug, Chromosomes, Human, Pair 8, Human, Receptor, Pediatric Cancer, Childhood Leukemia, Knockout, 21), Immunology, Clinical Sciences, Translocation, Biology, acute myeloid leukemia, Article, Chromosomes, Cell Line, Rare Diseases, Genetic, Cell Line, Tumor, Proto-Oncogene Proteins, medicine, Genetics, Animals, Humans, Fusion, Neoplastic, Animal, medicine.disease, Fusion protein, Disease Models, Animal, chemistry, Gene Expression Regulation, RUNX1-ETO, Disease Models, Cancer research, Pair 21, Interferon type I, t(8, Transcription Factors
Abstract

The 8;21 translocation is the most common chromosomal aberration occurring in acute myeloid leukemia (AML). This translocation causes expression of the RUNX1-ETO (AML1-ETO) fusion protein, which cooperates with additional mutations in leukemia development. We report here that interferons (IFNs) and IFN-stimulated genes are a group of genes consistently up-regulated by RUNX1-ETO in both human and murine models. RUNX1-ETO-induced up-regulation of IFN-stimulated genes occurs primarily via type I IFN signaling with a requirement for the IFNAR complex. Addition of exogenous IFN in vitro significantly reduces the increase in self-renewal potential induced by both RUNX1-ETO and its leukemogenic splicing isoform RUNX1-ETO9a. Finally, loss of type I IFN signaling via knockout of Ifnar1 significantly accelerates leukemogenesis in a t(8;21) murine model. This demonstrates the role of increased IFN signaling as an important factor inhibiting t(8;21) fusion protein function and leukemia development and supports the use of type I IFNs in the treatment of AML.

Published
2014

65. Genetic variation at 8q24, family history of cancer, and upper gastrointestinal cancers in a Chinese population

Author

Hua Wang, Lina Mu, Heather P. Tarleton, Shun-Zhang Yu, Qingwu Jiang, Shehnaz K. Hussain, Sungshim L. Park, Jianyu Rao, Nai-Chieh Y. You, Shen-Chih Chang, Na He, Jinkou Zhao, Lin Cai, Zuo-Feng Zhang, and Bao-Guo Ding

Subjects
Oncology, Male, Cancer Research, Esophageal Neoplasms, Esophageal cancer, Gastroenterology, Oral and gastrointestinal, Odds Ratio, 2.1 Biological and endogenous factors, Family history, Aetiology, Stomach cancer, Genetics (clinical), Gastrointestinal Neoplasms, Cancer, education.field_of_study, Liver Disease, Liver Neoplasms, Single Nucleotide, Middle Aged, Hepatitis B, Asians, Population study, Pair 8, Female, Liver cancer, Chromosomes, Human, Pair 8, Human, medicine.medical_specialty, Population, Oncology and Carcinogenesis, Polymorphism, Single Nucleotide, Article, Chromosomes, Rare Diseases, Asian People, Clinical Research, Internal medicine, medicine, Genetics, Humans, Genetic Predisposition to Disease, Family, Oncology & Carcinogenesis, Polymorphism, education, Aged, business.industry, Prevention, Human Genome, Genetic Variation, Odds ratio, medicine.disease, Good Health and Well Being, Case-Control Studies, 8q24 SNPs, Family history of cancer, business, Digestive Diseases
Abstract

Genetic variation at 8q24 is associated with prostate, bladder, breast, colorectal, thyroid, lung, ovarian, UADT, liver and stomach cancers. However, a role for variation at 8q24 in familial clustering of upper gastrointestinal cancers has not been studied. In order to explore potential inherited susceptibility, we analyzed epidemiologic data from a population-based case-control study of upper gastrointestinal cancers from Taixing, China. The study population includes 204 liver, 206 stomach, and 218 esophageal cancer cases and 415 controls. Associations between 8q24 rs1447295, rs16901979, rs6983267 and these cancers were stratified by family history of cancer. Odds ratios and 95% confidence intervals were adjusted for potential confounders: age, sex, education, tobacco smoking, alcohol consumption, and BMI at interview. We also adjusted for hepatitis B and aflatoxin (liver cancer) and Helicobacter pylori (stomach cancer). In a dominant model, among those with a family history of cancer, rs1447295 was positively associated with liver cancer (OR(adj) 2.80; 95% CI 1.15-6.80). Heterogeneity was observed (P(heterogeneity) = 0.029) with rs6983267 and liver cancer, with positive association in the dominant model among those with a family history of cancer and positive association in the recessive model among those without a family history of cancer. When considered in a genetic risk score model, each additional 8q24 risk genotype increased the odds of liver cancer by two-fold among those with a family history of cancer (OR(adj) 2.00; 95% CI 1.15-3.47). These findings suggest that inherited susceptibility to liver cancer may exist in the Taixing population and that variation at 8q24 might be a genetic component of that inherited susceptibility.

Published
2014

66. Copy number variation of the beta defensin gene cluster on chromosome 8p influences the bacterial microbiota within the nasopharynx of otitis-prone children

Author

Lauren O. Bakaletz, Edward J. Hollox, Anchasa Kananurak, Eric A. Jones, Charles L. Bevins, and Harder, Jürgen

Subjects
beta-Defensins, Gene Dosage, lcsh:Medicine, Pediatrics, 0302 clinical medicine, Risk Factors, Nasopharynx, Gene cluster, Medicine and Health Sciences, 2.1 Biological and endogenous factors, 030212 general & internal medicine, Copy-number variation, Aetiology, lcsh:Science, Child, Defensin, Pediatric, 0303 health sciences, Innate Immune System, Multidisciplinary, Microbiota, 3. Good health, Bacterial Pathogens, Infectious Diseases, Medical Microbiology, Child, Preschool, Multigene Family, Pediatric Otolaryngology, Pair 8, medicine.symptom, Human, Chromosomes, Human, Pair 8, Research Article, General Science & Technology, Immunology, Biology, Gene dosage, Microbiology, Chromosomes, 03 medical and health sciences, Clinical Research, Genetic variation, medicine, Genetics, Humans, Preschool, Microbial Pathogens, 030304 developmental biology, Retrospective Studies, Bacteria, lcsh:R, Case-control study, Immunity, Infant, Biology and Life Sciences, Otitis Media, Beta defensin, Otitis, Good Health and Well Being, Otorhinolaryngology, Case-Control Studies, Immune System, lcsh:Q
Abstract

As there is increasing evidence that aberrant defensin expression is related to susceptibility for infectious disease and inflammatory disorders, we sought to determine if copy number of the beta-defensin gene cluster located on chromosome 8p23.1 (DEFB107, 106, 105, 104, 103, DEFB4 and SPAG11), that shows copy number variation as a block, was associated with susceptibility to otitis media (OM). The gene DEFB103 within this complex encodes human beta defensin-3 (hBD-3), an antimicrobial peptide (AP) expressed by epithelial cells that line the mammalian airway, important for defense of mucosal surfaces and previously shown to have bactericidal activity in vitro against multiple human pathogens, including the three that predominate in OM. To this end, we conducted a retrospective case-control study of 113 OM prone children and 267 controls aged five to sixty months. We identified the copy number of the above defined beta-defensin gene cluster (DEFB-CN) in each study subject by paralogue ratio assays. The mean DEFB-CN was indistinguishable between subjects classified as OM prone based on a recent history of multiple episodes of OM and control subjects who had no history of OM (4.4 ± 0.96 versus 4.4 ± 1.08, respectively: Odds Ratio [OR]: 1.16 (95% CI: 0.61, 2.20). Despite a lack of direct association, we observed a statistically significant correlation between DEFB-CN and nasopharyngeal bacterial colonization patterns. Collectively, our findings suggested that susceptibility to OM might be mediated by genetic variation among individuals, wherein a DEFB-CN less than 4 exerts a marked influence on the microbiota of the nasopharynx, specifically with regard to colonization by the three predominant bacterial pathogens of OM.

Published
2014

67. Amerindian-specific regions under positive selection harbour new lipid variants in Latinos

Author

Päivi Pajukanta, Niina Matikainen, Alejandra Rodriguez, Carlos A. Aguilar-Salinas, Johan G. Eriksson, Laura Riba, Marja-Riitta Taskinen, Matti Jauhiainen, Daphna Weissglas-Volkov, Olli T. Raitakari, Veikko Salomaa, Ivette Cruz Bautista, Rosario Rodríguez-Guillén, Janet S. Sinsheimer, Maribel Rodríguez-Torres, Robert Brown, Antti Jula, Rita M. Cantor, Marcus Alvarez, Elina Nikkola, Terho Lehtimäki, Markus Perola, Bogdan Pasaniuc, Prasad M. V. Linga Reddy, Olimpia Arellano-Campos, Teresa Tusie-Luna, Jaakko Kaprio, Kirk E. Lohmueller, Arthur Ko, Linda L. Muñoz-Hernández, and Markku Heliövaara

Subjects
Male, General Physics and Astronomy, Genome-wide association study, Disease, 030204 cardiovascular system & hematology, Cardiovascular, Bioinformatics, 0302 clinical medicine, Indians, Group F, 2.1 Biological and endogenous factors, Aetiology, Pair 11, Hypertriglyceridemia, 2. Zero hunger, Genetics, 0303 health sciences, Multidisciplinary, Nuclear Receptor Subfamily 1, Group F, Member 1, Single Nucleotide, Middle Aged, Pair 8, Female, North American, Chromosomes, Human, Pair 8, Human, Adult, Member 1, Genotype, Nuclear Receptor Subfamily 1, Hypercholesterolemia, European Continental Ancestry Group, Locus (genetics), Biology, Polymorphism, Single Nucleotide, White People, Article, Chromosomes, General Biochemistry, Genetics and Molecular Biology, Young Adult, 03 medical and health sciences, Clinical Research, medicine, Humans, Genetic Predisposition to Disease, Obesity, Polymorphism, Allele, Mexico, Apolipoproteins A, Nutrition, Dyslipidemias, 030304 developmental biology, Prevention, Chromosomes, Human, Pair 11, Human Genome, Haplotype, General Chemistry, ta3121, Atherosclerosis, medicine.disease, Genetic architecture, Lipoprotein Lipase, Logistic Models, Haplotypes, Apolipoprotein A-V, Case-Control Studies, Indians, North American, Protein Kinases, Dyslipidemia, Genome-Wide Association Study
Abstract

Dyslipidemia and obesity are especially prevalent in populations with Amerindian backgrounds, such as Mexican–Americans, which predispose these populations to cardiovascular disease. Here we design an approach, known as the cross-population allele screen (CPAS), which we conduct prior to a genome-wide association study (GWAS) in 19,273 Europeans and Mexicans, in order to identify Amerindian risk genes in Mexicans. Utilizing CPAS to restrict the GWAS input variants to only those differing in frequency between the two populations, we identify novel Amerindian lipid genes, receptor-related orphan receptor alpha (RORA) and salt-inducible kinase 3 (SIK3), and three loci previously unassociated with dyslipidemia or obesity. We also detect lipoprotein lipase (LPL) and apolipoprotein A5 (APOA5) harbouring specific Amerindian signatures of risk variants and haplotypes. Notably, we observe that SIK3 and one novel lipid locus underwent positive selection in Mexicans. Furthermore, after a high-fat meal, the SIK3 risk variant carriers display high triglyceride levels. These findings suggest that Amerindian-specific genetic architecture leads to a higher incidence of dyslipidemia and obesity in modern Mexicans., Dyslipidemia and obesity have a high prevalence in populations with Amerindian backgrounds, such as Mexican–Americans. Here, the authors design an approach to identify Amerindian risk genes in Mexicans and identify five genomic loci, which include RORA and SIK3 that may contribute to the risk of dyslipidemia and obesity in Amerindian populations.

Published
2014

68. Prognostic gene mutations and distinct gene- and microRNA-expression signatures in acute myeloid leukemia with a sole trisomy 8

Author

Michael D. Radmacher, Sebastian Schwind, Krzysztof Mrózek, Michael A. Caligiuri, Bayard L. Powell, Yue-Zhong Wu, Susan P. Whitman, Kati Maharry, Peter Paschka, Meir Wetzler, Maria R. Baer, Guido Marcucci, Deedra Nicolet, Klaus H. Metzeler, Heiko Becker, Stefano Volinia, Jonathan E. Kolitz, Jessica Kohlschmidt, Ann-Kathrin Eisfeld, Clara D. Bloomfield, Jason H. Mendler, Thomas H. Carter, Andrew J. Carroll, and Richard Stone

Subjects
Adult, Myeloid, Male, Cancer Research, Adolescent, Trisomy, Gene mutation, Biology, Acute, Trisomy 8, medicine.disease_cause, Article, Disease-Free Survival, Chromosomes, Dioxygenases, NO, hemic and lymphatic diseases, Proto-Oncogene Proteins, medicine, 80 and over, Humans, Aged, Aged, 80 and over, Genetics, Mutation, Leukemia, Myeloid leukemia, Hematology, Middle Aged, medicine.disease, Prognosis, DNA-Binding Proteins, Female, Leukemia, Myeloid, Acute, MicroRNAs, fms-Like Tyrosine Kinase 3, Chromosomes, Human, Pair 8, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Oncology, Fms-Like Tyrosine Kinase 3, Pair 8, Human
Abstract

Prognostic gene mutations and distinct gene- and microRNA-expression signatures in acute myeloid leukemia with a sole trisomy 8

Published
2014

69. Genetic variation at 8q24, family history of cancer, and upper gastrointestinal cancers in a Chinese population.

Author

Tarleton, Heather, Tarleton, Heather, Chang, Shen-Chih, Park, Sungshim, Cai, Lin, Ding, Baoguo, He, Na, Hussain, Shehnaz, Jiang, Qingwu, Mu, Li-Na, Rao, Jian, Wang, Hua, You, Nai-Chieh, Yu, Shun-Zhang, Zhao, Jin-Kou, Zhang, Zuo-Feng, Tarleton, Heather, Tarleton, Heather, Chang, Shen-Chih, Park, Sungshim, Cai, Lin, Ding, Baoguo, He, Na, Hussain, Shehnaz, Jiang, Qingwu, Mu, Li-Na, Rao, Jian, Wang, Hua, You, Nai-Chieh, Yu, Shun-Zhang, Zhao, Jin-Kou, and Zhang, Zuo-Feng

Abstract

Genetic variation at 8q24 is associated with prostate, bladder, breast, colorectal, thyroid, lung, ovarian, UADT, liver and stomach cancers. However, a role for variation at 8q24 in familial clustering of upper gastrointestinal cancers has not been studied. In order to explore potential inherited susceptibility, we analyzed epidemiologic data from a population-based case-control study of upper gastrointestinal cancers from Taixing, China. The study population includes 204 liver, 206 stomach, and 218 esophageal cancer cases and 415 controls. Associations between 8q24 rs1447295, rs16901979, rs6983267 and these cancers were stratified by family history of cancer. Odds ratios and 95% confidence intervals were adjusted for potential confounders: age, sex, education, tobacco smoking, alcohol consumption, and BMI at interview. We also adjusted for hepatitis B and aflatoxin (liver cancer) and Helicobacter pylori (stomach cancer). In a dominant model, among those with a family history of cancer, rs1447295 was positively associated with liver cancer (OR(adj) 2.80; 95% CI 1.15-6.80). Heterogeneity was observed (P(heterogeneity) = 0.029) with rs6983267 and liver cancer, with positive association in the dominant model among those with a family history of cancer and positive association in the recessive model among those without a family history of cancer. When considered in a genetic risk score model, each additional 8q24 risk genotype increased the odds of liver cancer by two-fold among those with a family history of cancer (OR(adj) 2.00; 95% CI 1.15-3.47). These findings suggest that inherited susceptibility to liver cancer may exist in the Taixing population and that variation at 8q24 might be a genetic component of that inherited susceptibility.

Published
2014

70. A colorectal cancer genome-wide association study in a Spanish cohort identifies two variants associated with colorectal cancer risk at 1p33 and 8p12

Author

Rosa M. Xicola, Xavier Bessa, Xavier Llor, Juan Clofent, Luis G. Carvajal-Carmona, Angel Carracedo, Claire Palles, Rodrigo Jover, Montserrat Andreu, Ceres Fernandez-Rozadilla, Ian Tomlinson, Montserrat Baiget, Antoni Castells, Sergi Castellví-Bel, Jean-Baptiste Cazier, María Jesús Lamas, Dolors Gonzalez, Luis A. López-Fernández, Victor Moreno, Alejandro Brea-Fernández, Luis Bujanda, Clara Ruiz-Ponte, Anna Abulí, and Universitat de Barcelona

Subjects
Male, Genome-wide association study, GENETICS AND HEREDITY, Medical and Health Sciences, Cohort Studies, 0302 clinical medicine, Missing heritability problem, Risk Factors, Genotype, Odds Ratio, 80 and over, 2.1 Biological and endogenous factors, GWAS, Aetiology, Cancer, Aged, 80 and over, Genetics, 0303 health sciences, Principal Component Analysis, Genome, Statistics, Single Nucleotide, Middle Aged, Biological Sciences, 3. Good health, Colo-Rectal Cancer, Chromosomes, Human, Pair 1, 030220 oncology & carcinogenesis, Cohort, Pair 1, Pair 8, Dual-Specificity Phosphatases, Female, Colorectal Neoplasms, Research Article, Chromosomes, Human, Pair 8, Cohort study, Biotechnology, Human, SNPs, neoplasias colorrectales, Bioinformatics, European Continental Ancestry Group, genoma humano, Single-nucleotide polymorphism, BIOTECHNOLOGY AND APPLIED MICROBIOLOGY, and over, Biology, Genetic polymorphisms, Polymorphism, Single Nucleotide, Chromosomes, White People, 8p12, 03 medical and health sciences, Estadístiques, Càncer colorectal, Information and Computing Sciences, Humans, Polymorphism, 030304 developmental biology, Genetic association, Aged, 1p33, Genome, Human, Polimorfisme genètic, Prevention, Human Genome, Odds ratio, Colorectal cancer, Spain, Genetic Loci, Spanish cohort, Mitogen-Activated Protein Kinase Phosphatases, EPICOLON Consortium, Digestive Diseases, Genome-Wide Association Study
Abstract

Background: Colorectal cancer (CRC) is a disease of complex aetiology, with much of the expected inherited risk being due to several common low risk variants. Genome-Wide Association Studies (GWAS) have identified 20 CRC risk variants. Nevertheless, these have only been able to explain part of the missing heritability. Moreover, these signals have only been inspected in populations of Northern European origin. Results: Thus, we followed the same approach in a Spanish cohort of 881 cases and 667 controls. Sixty-four variants at 24 loci were found to be associated with CRC at p-values

Published
2013

71. Mapping of genes predisposing to idiopathic generalized epilepsy

Author

Federico Zara, Massimo Pandolfo, Giuliano Avanzini, Barbara Castellotti, S. Di Donato, A Bianchi, and Pragna Patel

Subjects
Male, Genetic Linkage, Locus (genetics), Biology, Chromosomes, Idiopathic generalized epilepsy, Epilepsy, Chromosome 15, Gene mapping, Genetic linkage, Genetics, medicine, Humans, Generalized epilepsy, Molecular Biology, Chromosomes, Human, Pair 6, Chromosomes, Human, Pair 8, Disease Susceptibility, Epilepsy, Generalized, Family Health, Female, Pedigree, Chromosome Mapping, Genetics (clinical), Generalized, General Medicine, medicine.disease, Pair 8, Pair 6, Juvenile myoclonic epilepsy, Human
Abstract

Idiopathic generalized epilepsy (IGE) is characterized by recurring generalized seizures in the absence of detectable brain lesions and/or metabolic abnormalities. Twin and family studies suggest that genetic factors play a key part in IGE. A multilocus model appears to best fit the observed inheritance patterns. Mapping of IGE-related genes has been previously attempted using parametric methods, with conflicting results. In particular, recent evidence argues both for and against a chromosome 6p locus (EJM1) for juvenile myoclonic epilepsy, a subtype of IGE. We have approached the problem of mapping IGE loci using non-parametric methods, which have recently been successful for other complex diseases. No evidence for linkage to chromosome 6p was obtained. However, we obtained evidence for involvement of a locus at chromosome 8q24, close to the marker D8S256. The same 8q24 region was previously implicated in families with benign neonatal familial convulsions (BNFC), a generalized epilepsy syndrome that is inherited as a simple dominant mendelian trait. There is an apparent conserved syntenic group of genes in human 8q24 and a region of mouse chromosome 15, which harbors the stargazer (stg) locus. Homozygous mutant mice at the stg locus show a form of generalized epilepsy that resembles human absence epilepsy. Our findings may have implications for a locus on 8q24 predisposing to IGE.

Published
1995

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

Author

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

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

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

Published
2012

73. Common Variants at 9p21 and 8q22 Are Associated with Increased Susceptibility to Optic Nerve Degeneration in Glaucoma

Author

Brian L. Yaspan, Robert N. Weinreb, Douglas E. Gaasterland, Stephanie Loomis, Kristy Crooks, Tomohiro Masuda, David S. Friedman, Daniel B. Mirel, Jason Ernst, Joel S. Schuman, Kathleen M. Scott, Joshua D. Stein, Wael Abdrabou, Sayoko E. Moroi, Cathy C. Laurie, Paul R. Lichter, Margaret A. Pericak-Vance, Catherine A. McCarty, Gadi Wollstein, Anthony Realini, Felipe A. Medeiros, Richard K. Lee, Jae H. Kang, Louis R. Pasquale, Sachiko Yoneyama, Frank W. Rozsa, R. Rand Allingham, Kuldev Singh, Yutao Liu, Julia E. Richards, E. DelBono, Wendy Brodeur, David C. Musch, Manolis Kellis, Baojian Fan, Donald L. Budenz, Edward H. Trager, Jonathan L. Haines, Kang Zhang, Donald J. Zack, Janey L. Wiggs, Dan Y. Wang, Kimberly F. Doheny, Joseph Caprioli, Andrew Crenshaw, Paul C. VanVeldhuisen, Terry Gaasterland, Douglas Vollrath, Michael A. Hauser, Lana M. Olson, Massachusetts Institute of Technology. Computer Science and Artificial Intelligence Laboratory, Massachusetts Institute of Technology. Department of Electrical Engineering and Computer Science, Kellis, Manolis, Ernst, Jason, and Barsh, Gregory S

Subjects
Aging, Cancer Research, Intraocular pressure, RNA, Untranslated, genetic structures, Glaucoma, Genome-wide association study, Neurodegenerative, QH426-470, Eye, Exfoliation Syndrome, 0302 clinical medicine, Transforming Growth Factor beta, 2.1 Biological and endogenous factors, Aetiology, Genetics (clinical), Genetics, 0303 health sciences, Untranslated, Single Nucleotide, 3. Good health, Open-Angle, Optic nerve, Medicine, Pair 8, RNA, Long Noncoding, Long Noncoding, Chromosomes, Human, Pair 9, Glaucoma, Open-Angle, Research Article, Chromosomes, Human, Pair 8, Human, Pair 9, medicine.medical_specialty, Open angle glaucoma, Biology, Polymorphism, Single Nucleotide, Chromosomes, 03 medical and health sciences, Clinical Research, Ophthalmology, medicine, Humans, Inherited Eye Disorders, Allele, Polymorphism, Eye Disease and Disorders of Vision, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Alleles, 030304 developmental biology, Genetic association, Homeodomain Proteins, Human Genome, CDKN2BAS, Neurosciences, Optic Nerve, medicine.disease, eye diseases, Nerve Degeneration, 030221 ophthalmology & optometry, RNA, sense organs, Genome-Wide Association Study, Developmental Biology
Abstract

Optic nerve degeneration caused by glaucoma is a leading cause of blindness worldwide. Patients affected by the normal-pressure form of glaucoma are more likely to harbor risk alleles for glaucoma-related optic nerve disease. We have performed a meta-analysis of two independent genome-wide association studies for primary open angle glaucoma (POAG) followed by a normal-pressure glaucoma (NPG, defined by intraocular pressure (IOP) less than 22 mmHg) subgroup analysis. The single-nucleotide polymorphisms that showed the most significant associations were tested for association with a second form of glaucoma, exfoliation-syndrome glaucoma. The overall meta-analysis of the GLAUGEN and NEIGHBOR dataset results (3,146 cases and 3,487 controls) identified significant associations between two loci and POAG: the CDKN2BAS region on 9p21 (rs2157719 [G], OR = 0.69 [95%CI 0.63–0.75], p = 1.86×10−18), and the SIX1/SIX6 region on chromosome 14q23 (rs10483727 [A], OR = 1.32 [95%CI 1.21–1.43], p = 3.87×10−11). In sub-group analysis two loci were significantly associated with NPG: 9p21 containing the CDKN2BAS gene (rs2157719 [G], OR = 0.58 [95% CI 0.50–0.67], p = 1.17×10−12) and a probable regulatory region on 8q22 (rs284489 [G], OR = 0.62 [95% CI 0.53–0.72], p = 8.88×10−10). Both NPG loci were also nominally associated with a second type of glaucoma, exfoliation syndrome glaucoma (rs2157719 [G], OR = 0.59 [95% CI 0.41–0.87], p = 0.004 and rs284489 [G], OR = 0.76 [95% CI 0.54–1.06], p = 0.021), suggesting that these loci might contribute more generally to optic nerve degeneration in glaucoma. Because both loci influence transforming growth factor beta (TGF-beta) signaling, we performed a genomic pathway analysis that showed an association between the TGF-beta pathway and NPG (permuted p = 0.009). These results suggest that neuro-protective therapies targeting TGF-beta signaling could be effective for multiple forms of glaucoma., Author Summary Loss of vision from glaucoma, a common cause of blindness worldwide, is due to irreversible damage to the optic nerve. Current therapies cannot prevent glaucoma-related optic nerve disease and very little is known about the underlying responsible molecular events. Glaucoma patients affected by the “normal-pressure” subtype of glaucoma (NPG) have increased susceptibility to optic nerve degeneration. Although NPG has a high heritability, common predisposing genetic variants have not been identified. Therefore, we performed a meta-analysis of two independent genome-wide association studies for a common form of glaucoma, primary open angle glaucoma (POAG), followed by NPG subgroup analysis. We found that SNPs in the CDKN2BAS gene region on 9p21 and a highly conserved region with a probable regulatory function on 8q22 were associated with NPG and with optic nerve disease in a second type of glaucoma, exfoliation glaucoma. Both genomic regions are predicted to influence TGF-beta activity, and using whole-genome data we showed that the TGF-beta signaling pathway overall is associated with NPG. These results reveal new insights into the molecular pathogenesis of optic nerve disease in glaucoma and are an important step toward the development of preventative and protective therapies.

Published
2012

74. Receptor tyrosine kinase pathway analysis sheds light on similarities between clear-cell sarcoma and metastatic melanoma

Author

Piero Picci, Marco Alberghini, Alessandro Gronchi, Silvana Pilotti, Valentina Mauro, Silvia Brich, Giuseppina F. Dusio, Marta Orsenigo, Marco A. Pierotti, Fabio Bozzi, Silvia Stacchiotti, Elena Conca, Giuseppe Pelosi, Tiziana Negri, Paolo G. Casali, Negri, Tiziana, Brich, Silvia, Conca, Elena, Bozzi, Fabio, Orsenigo, Marta, Stacchiotti, Silvia, Alberghini, Marco, Mauro, Valentina, Gronchi, Alessandro, Dusio, Giuseppina F., Pelosi, Giuseppe, Picci, Piero, Casali, Paolo G., Pierotti, Marco A, and Pilotti, Silvana

Subjects
Neuroblastoma RAS viral oncogene homolog, Male, Cancer Research, Chromosomes, Human, Pair 22, Gene Expression, Trisomy, RNA-Binding Protein, medicine.disease_cause, Receptor tyrosine kinase, Clear Cell, Chromosome Duplication, 80 and over, Phosphorylation, Melanoma, Genetics, Aged, 80 and over, Tumor, RNA-Binding Proteins, Sarcoma, Middle Aged, Receptor Protein-Tyrosine Kinase, Lymphatic Metastasis, Adult, Aged, Base Sequence, Biomarkers, Tumor, Calmodulin-Binding Proteins, Chromosomes, Human, Pair 8, Female, Humans, Receptor Protein-Tyrosine Kinases, Sarcoma, Clear Cell, Sequence Analysis, DNA, Young Adult, Pair 8, KRAS, Sequence Analysis, Human, PDGFRB, Biology, Chromosomes, Genetic, medicine, Protein kinase B, PI3K/AKT/mTOR pathway, Calmodulin-Binding Protein, fungi, Lymphatic Metastasi, DNA, medicine.disease, Cancer research, biology.protein, Pair 22, RNA-Binding Protein EWS, Biomarkers, V600E
Abstract

To highlight possible similarities and differences in receptor tyrosine kinase (RTK) and downstream signalling activation profiles between clear-cell sarcomas (CCS) and metastatic melanomas (MM), frozen, and paired-matched fixed samples of six CCS with EWSR1 rearrangement (EWSR1+), five CCS without EWSR1 rearrangement (EWSR1-), and seven MM were investigated by means of biochemical, immunohistochemical, FISH, molecular analyses, and immunofluorescence confocal microscopy. Fixed samples of a further 10 CCS and 14 MM were investigated by means of sequencing for BRAF, NRAS, and KRAS mutations and FISH analyses for the gain of chromosomes 22 and 8. RTK analysis of all CCS/MM samples showed activation of short-form (sf) recepteur d'origine nantais (RON) RTK and of PDGFRB, MET, and HER3. Analysis of downstream signaling revealed consistent phosphorylation patterns of PI3K/AKT, RSK, and the mTOR targets S6 and 4EBP1. Analysis of frozen and fixed material from 21 CCS and 21 MM showed the presence of the V600E BRAF mutation in 2/12 EWSR1+ and 3/9 EWSR1- CCS and 9/21 MM and demonstrated a significant (P < 0.001) correlation between the gain of chromosomes 22 and 8 and EWSR1- CCS. Our results show that BRAF mutation can also be present in CCS and support the proposed aberration of chromosomes 22 and 8 as a possibly useful nonrandom hallmark of EWSR1- CCS. Besides, they broaden the spectrum of the similarities of RTK pathway activation between CCS and MM, thus suggesting that new drugs found to be active in melanoma and RON inhibitors could have a role in CCS treatment. © 2011 Wiley Periodicals, Inc.

Published
2012

75. Who is in the driver's seat in 8p12 amplifications? ZNF703 in luminal B breast tumors

Author

Paul Yaswen and Alexey V. Bazarov

Subjects
Cellular differentiation, 1.1 Normal biological development and functioning, Oncology and Carcinogenesis, Breast Neoplasms, Chromosomes, Metastasis, Cell Line, Mice, Viewpoint, Transforming Growth Factor beta, Underpinning research, Cell Line, Tumor, Breast Cancer, medicine, Cell Adhesion, Genetics, Animals, Humans, Oncology & Carcinogenesis, Progenitor cell, Neoplasm Metastasis, Cell adhesion, Cell Proliferation, Cancer, Tumor, biology, Oncogene, Cell growth, Gene Amplification, Cell Differentiation, Transforming growth factor beta, medicine.disease, Stem Cell Research, Cancer research, biology.protein, Neoplastic Stem Cells, Pair 8, Female, Stem Cell Research - Nonembryonic - Non-Human, Stem cell, Carrier Proteins, Chromosomes, Human, Pair 8, Human, Transcription Factors, Signal Transduction
Abstract

© 2011 BioMed Central Ltd. Two recent reports identify ZNF703 as an oncogene driving selection of frequent chromosome 8p12 amplifications in luminal B breast tumors. The estrogen-responsive ZNF703 gene encodes a transcriptional cofactor that, when overexpressed, induces cell proliferation and interferes with transforming growth factor beta signaling. In MCF7 cells, increased ZNF703 expression results in activation of genes involved in stem cell self-renewal - while in primary human mammary epithelial cells, ZNF703 increases the ratio of luminal to basal progenitors. Expression of the murine homolog of ZNF703 reduces cell adhesion and promotes metastasis. ZNF703 overexpression thus alters regulation of proliferation and differentiation in luminal B tumors.

Published
2011

76. FGF17, a gene involved in cerebellar development, is downregulated in a patient with Dandy-Walker malformation carrying a de novo 8p deletion

Author

Letizia Da Sacco, Enrico Bertini, Antonio Novelli, Ginevra Zanni, Sabina Barresi, Stefano Cianfarani, Bruno Dallapiccola, Laura Bernardini, Massimiliano Valeriani, Enza Maria Valente, Eugenio Mercuri, Teresa Rizza, Alessandro Ferraris, Maria Cristina Digilio, and Lorena Travaglini

Subjects
Cerebellum, Fibroblast Growth Factor 8, Down-Regulation, Biology, Fibroblast growth factor, Chromosomes, 03 medical and health sciences, Cellular and Molecular Neuroscience, Settore MED/39 - NEUROPSICHIATRIA INFANTILE, 0302 clinical medicine, FGF8, Dandy–Walker syndrome, Gene expression, Genetics, medicine, Humans, Child, Preschool, Genetics (clinical), 030304 developmental biology, Settore MED/38 - Pediatria Generale e Specialistica, 0303 health sciences, Comparative Genomic Hybridization, Gene Expression Profiling, medicine.disease, Cell biology, Gene expression profiling, medicine.anatomical_structure, Spatiotemporal gene expression, Child, Preschool, Cerebellar vermis, Pair 8, Female, Chromosome Deletion, Dandy-Walker Syndrome, Chromosomes, Human, Pair 8, 030217 neurology & neurosurgery, Human
Abstract

Fibroblast growth factors (FGFs) are important signaling molecules which act during early vertebrate central nervous system development. FGF17, together with FGF8, is a key factor in the patterning of the mid-hindbrain region with a complex picture of spatiotemporal gene expression during the various stages of cerebellar development. Disruption or reduced expression of fgf17 in mice has been associated with cerebellar vermis abnormalities. We have identified a de novo 2.3-Mb deletion of chromosome 8p21.2-p21.3 in a girl with severe growth retardation, seizures, and classical Dandy-Walker malformation. Analysis of gene expression in blood lymphocytes and skin fibroblasts revealed markedly reduced levels of FGF17, which is located 1 Mb from the proximal deletion breakpoint. This is the first report of a human cerebellar malformation associated with transcriptional downregulation of the FGF17 gene.

Published
2011

77. Whole-genome linkage scan for epilepsy-related photosensitivity: A mega-analysis

Author

Auli Siren, Hiltrud Muhle, Gabrielle Rudolf, D. G Kasteleijn Nolst Trenité, Costin Leu, Ingrid E. Scheffer, Dalila Pinto, Pasquale Striano, C. G. F. de Kovel, Petra M.C. Callenbach, Thomas Sander, Bobby P. C. Koeleman, Ulrich Stephani, Dick Lindhout, S. Lorenz, Anne Hempelmann, Samuel F. Berkovic, Betül Baykan, Ulrike Tauer, and Bernd A. Neubauer

Subjects
Male, Genetic Linkage, LOCI, Genome, Photoparoxysmal response, Epilepsy, 0302 clinical medicine, Idiopathic generalised epilepsy, Photosensitivity, genetics, Genetics, Genome-wide linkage, 0303 health sciences, Chromosome Mapping, Phenotype, GENETIC DISSECTION, Neurology, TWINS, Geographic origin, Chromosomes, Human, Pair 5, Pair 8, Female, Mega analysis, Pair 5, Chromosomes, Human, Pair 8, Human, Mega-analysis, Locus (genetics), Biology, IDIOPATHIC GENERALIZED EPILEPSIES, Epilepsy, Reflex, Chromosomes, 7Q32, methods, 03 medical and health sciences, Genetic linkage, Reflex, medicine, Humans, methods, Chromosomes, Pair 16, genetics, Chromosomes, genetics, Epilepsy, genetics, Female, Genetic Linkage, genetics, Genetic Predisposition to Disease, Genome, genetics, Humans, Male, Genetic Predisposition to Disease, 030304 developmental biology, Genome, Human, medicine.disease, SEIZURES, Neurology (clinical), Chromosomes, Human, Pair 16, 030217 neurology & neurosurgery, 16P13
Abstract

Photoparoxysmal response (PPR) is considered to be a risk factor for idiopathic generalised epilepsy (IGE) and it has a strong genetic basis. Two genome-wide linkage studies have been published before and they identified loci for PPR at 6p21, 7q32, 13q13, 13q31 and 16p13. Here we combine these studies, augmented with additional families, in a mega-analysis of 100 families. Non-parametric linkage analysis identified three suggestive peaks for photosensitivity, two of which are novel (5q35.3 and 8q21.13) and one has been found before (16p13.3). We found no evidence for linkage at four previously detected loci (6p21, 7q32, 13q13 and 13q31).Our results suggest that the different family data sets are not linked to a shared locus. Detailed analysis showed that the peak at 16p13 was mainly supported by a single subset of families, while the peaks at 5q35 and 8q21 had weak support from multiple subsets.Family studies clearly support the role of PPR as a risk factor for IGE. This mega-analysis shows that distinct loci seem to be linked to subsets of PPR-positive families that may differ in subtle clinical phenotypes or geographic origin. Further linkage studies of PPR should therefore include in-depth phenotyping to make appropriate subsets and increase genetic homogeneity. (C) 2010 Elsevier B.V. All rights reserved.

Published
2010

78. Update on the Genetics of Stroke and Cerebrovascular Disease 2008

Author

Robert A. Hegele and Martin Dichgans

Subjects
Risk, Candidate gene, Genotype, Genome-wide association study, Single-nucleotide polymorphism, Locus (genetics), Chromosomes, Brain Ischemia, Medicine, Humans, Genotyping, Advanced and Specialized Nursing, Genetics, Framingham Risk Score, business.industry, Stem Cells, Intracranial Aneurysm, Odds ratio, Stroke, Cerebrovascular Disorders, Pharmacogenetics, Chromosomal region, Pair 8, Neurology (clinical), Cardiology and Cardiovascular Medicine, business, Chromosomes, Human, Pair 9, Medical Genetics, Human, Pair 9, Genome-Wide Association Study, Chromosomes, Human, Pair 8
Abstract

2008 has brought us the first fruits from genomewide association studies (GWASs), an unbiased and comprehensive approach to identify common risk alleles for complex diseases of adulthood. By genotyping >310 000 single nucleotide polymorphisms (SNPs) in over 1700 intracranial aneurysm (IA) cases and 7400 controls from Finland and the Netherlands, a multinational team of investigators recently identified several common SNPs that showed significant association with IA.1 SNPs on chromosomes 2q, 8q and 9p were found to replicate in an independent sample from Japan with similar odds ratios (OR) in all 3 samples. Pooled OR were between 1.24 and 1.36, and analyses of the combined effects suggested a significant linear relationship with risk score in each cohort, with a more than 3-fold increase from the lowest to highest strata. Collectively, the 3 loci were calculated to account for 38% to 46% of the population–attributable fraction of IA, which is substantial. Although additional work in other ethnic groups is required, the consistency emphasizes the robustness of the findings. The critical genetic intervals on chromosomes 8q and 9p both harbor genes that are implicated in the regulation of stem (progenitor) cell populations and expressed in the adult vasculature. SOX17 , the main candidate gene on 8q, is required for both endothelial formation and maintenance—an interesting aspect when considering the predominant location of IA at arterial branch points and sites of endothelial shear stress. The association between common variants at 9p and IA had already been reported in another study earlier last year.2 The 9p21.3 region was originally identified as a major risk locus for coronary artery disease and myocardial infarction.3 Subsequent analyses revealed that the same chromosomal region is also implicated in the risk of IA and abdominal aortic aneurysms. The estimated risk for IA conferred by the main risk …

Published
2009

79. Unusual 8p Inverted Duplication Deletion with Telomere Capture from 8q

Author

Geert Mortier, Karen Buysse, Björn Menten, Ulrike Fränkel, Francesca Antonacci, Frank Speleman, Bart Loeys, Bert Callewaert, and Victoria Mok Siu

Subjects
Medical Biochemistry, Biology, Pediatrics, Chromosomes, Gene mapping, Gene Duplication, Gene duplication, Genetics, medicine, Humans, Gene, Genetics (clinical), Chromosomal inversion, Chromosome Aberrations, Olfactory receptor, Chromosome, Infant, General Medicine, Telomere, Molecular biology, medicine.anatomical_structure, Chromosome Inversion, Cytogenetic Analysis, Pair 8, Chromosome Deletion, Homologous recombination, Human, Chromosomes, Human, Pair 8
Abstract

Inverted 8p duplication deletions are recurrent chromosomal rearrangements that are mediated through non-allelic homologous recombination (NAHR) between olfactory receptor (OR) gene clusters at 8p23.1. These rearrangements result in a proximal inverted duplication of various extent, a single copy region between the OR gene clusters and a terminal 8p deletion. The terminal deletions are stabilized by direct addition of telomeric repeats, so called telomere healing. Here, we report a patient with an unusual inverted duplication deletion of 8p. Stabilization of the broken chromosome end was achieved by telomere capture instead of telomere healing, resulting in an additional duplication of 8q24.13-->qter on the short arm of chromosome 8. Moreover, the inverted duplication was only 3.4 Mb in size (restricted to band 8p22) and thus cytogenetically undetectable. To the best of our knowledge this is the smallest inverted duplication reported hitherto. We describe the molecular characterization by FISH and array CGH of this unusual inv dup del (8p) and a previously reported patient with a similar 8q duplication and review the literature on cases associated with telomere capture.

Published
2009

80. Heterogeneity of breast cancer associations with five susceptibility loci by clinical and pathological characteristics

Author

Montserrat Garcia-Closas, Per Hall, Heli Nevanlinna, Karen Pooley, Jonathan Morrison, Douglas A Richesson, Stig E Bojesen, Børge G Nordestgaard, Christen K Axelsson, Jose I Arias, Roger L Milne, Gloria Ribas, Anna González-Neira, Javier Benítez, Pilar Zamora, Hiltrud Brauch, Christina Justenhoven, Ute Hamann, Yon-Dschun Ko, Thomas Bruening, Susanne Haas, Thilo Dörk, Peter Schürmann, Peter Hillemanns, Natalia Bogdanova, Michael Bremer, Johann Hinrich Karstens, Rainer Fagerholm, Kirsimari Aaltonen, Kristiina Aittomäki, Karl von Smitten, Carl Blomqvist, Arto Mannermaa, Matti Uusitupa, Matti Eskelinen, Maria Tengström, Veli-Matti Kosma, Vesa Kataja, Georgia Chenevix-Trench, Amanda B Spurdle, Jonathan Beesley, Xiaoqing Chen, Australian Ovarian Cancer Management Group, Kathleen Cuningham Foundation Consortium for Research into Familial Breast Cancer, Peter Devilee, Christi J van Asperen, Catharina E Jacobi, Rob A E M Tollenaar, Petra E A Huijts, Jan G M Klijn, Jenny Chang-Claude, Silke Kropp, Tracy Slanger, Dieter Flesch-Janys, Elke Mutschelknauss, Ramona Salazar, Shan Wang-Gohrke, Fergus Couch, Ellen L Goode, Janet E Olson, Celine Vachon, Zachary S Fredericksen, Graham G Giles, Laura Baglietto, Gianluca Severi, John L Hopper, Dallas R English, Melissa C Southey, Christopher A Haiman, Brian E Henderson, Laurence N Kolonel, Loic Le Marchand, Daniel O Stram, David J Hunter, Susan E Hankinson, David G Cox, Rulla Tamimi, Peter Kraft, Mark E Sherman, Stephen J Chanock, Jolanta Lissowska, Louise A Brinton, Beata Peplonska, Maartje J Hooning, Han Meijers-Heijboer, J Margriet Collee, Ans van den Ouweland, Andre G Uitterlinden, Jianjun Liu, Low Yen Lin, Li Yuqing, Keith Humphreys, Kamila Czene, Angela Cox, Sabapathy P Balasubramanian, Simon S Cross, Malcolm W R Reed, Fiona Blows, Kristy Driver, Alison Dunning, Jonathan Tyrer, Bruce A J Ponder, Suleeporn Sangrajrang, Paul Brennan, James McKay, Fabrice Odefrey, Valerie Gabrieau, Alice Sigurdson, Michele Doody, Jeffrey P Struewing, Bruce Alexander, Douglas F Easton, Paul D Pharoah, Human genetics, CCA - Disease profiling, Human Genetics, Medical Oncology, Psychiatry, Clinical Genetics, and Internal Medicine

Subjects
Oncology, Cancer Research, Linkage disequilibrium, Fibroblast Growth Factor, Colorectal cancer, Genome-wide association study, QH426-470, Bioinformatics, Linkage Disequilibrium, 0302 clinical medicine, Trinucleotide Repeats, Receptors, Odds Ratio, Genetics and Genomics/Genetics of Disease, Progesterone, Genetics (clinical), 0303 health sciences, Ecology, Microfilament Proteins, High Mobility Group Proteins, Single Nucleotide, Middle Aged, 3. Good health, Oncology/Breast Cancer, 030220 oncology & carcinogenesis, Pair 8, Female, Receptors, Progesterone, Type 2, Research Article, Chromosomes, Human, Pair 8, Human, Receptor, medicine.medical_specialty, Evolution, MAP Kinase Kinase Kinase 1, Breast Neoplasms, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Chromosomes, 03 medical and health sciences, Breast cancer, Behavior and Systematics, SDG 3 - Good Health and Well-being, Internal medicine, Genetics, medicine, Humans, Genetic Predisposition to Disease, Receptor, Fibroblast Growth Factor, Type 2, Polymorphism, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Case-Control Studies, Case-control study, Odds ratio, medicine.disease, TOX3, Trans-Activators, Apoptosis Regulatory Proteins
Abstract

A three-stage genome-wide association study recently identified single nucleotide polymorphisms (SNPs) in five loci (fibroblast growth receptor 2 (FGFR2), trinucleotide repeat containing 9 (TNRC9), mitogen-activated protein kinase 3 K1 (MAP3K1), 8q24, and lymphocyte-specific protein 1 (LSP1)) associated with breast cancer risk. We investigated whether the associations between these SNPs and breast cancer risk varied by clinically important tumor characteristics in up to 23,039 invasive breast cancer cases and 26,273 controls from 20 studies. We also evaluated their influence on overall survival in 13,527 cases from 13 studies. All participants were of European or Asian origin. rs2981582 in FGFR2 was more strongly related to ER-positive (per-allele OR (95%CI) = 1.31 (1.27–1.36)) than ER-negative (1.08 (1.03–1.14)) disease (P for heterogeneity = 10−13). This SNP was also more strongly related to PR-positive, low grade and node positive tumors (P = 10−5, 10−8, 0.013, respectively). The association for rs13281615 in 8q24 was stronger for ER-positive, PR-positive, and low grade tumors (P = 0.001, 0.011 and 10−4, respectively). The differences in the associations between SNPs in FGFR2 and 8q24 and risk by ER and grade remained significant after permutation adjustment for multiple comparisons and after adjustment for other tumor characteristics. Three SNPs (rs2981582, rs3803662, and rs889312) showed weak but significant associations with ER-negative disease, the strongest association being for rs3803662 in TNRC9 (1.14 (1.09–1.21)). rs13281615 in 8q24 was associated with an improvement in survival after diagnosis (per-allele HR = 0.90 (0.83–0.97). The association was attenuated and non-significant after adjusting for known prognostic factors. Our findings show that common genetic variants influence the pathological subtype of breast cancer and provide further support for the hypothesis that ER-positive and ER-negative disease are biologically distinct. Understanding the etiologic heterogeneity of breast cancer may ultimately result in improvements in prevention, early detection, and treatment., Author Summary This report from the Breast Cancer Association Consortium evaluates whether common variants in five recently identified breast cancer susceptibility loci (FGFR2, TNRC9, MAP3K1, 8q24, and LSP1) influence the clinical presentation of breast cancer and survival after diagnosis. We studied these susceptibility loci in relation to clinically important tumor characteristics in up to 23,039 invasive breast cancer cases and 26,273 controls of European or Asian origin from 20 studies. The association, with overall survival, was evaluated in 13,527 cases from 13 studies. The most notable findings were that the genetic variants in the fibroblast growth factor receptor 2 (FGFR2) gene and the 8q24 region were more strongly related to ER-positive than ER-negative disease, and to low rather than high grade tumors. The loci did not significantly influence survival after accounting for known prognostic factors. Analyses indicated that common genetic variants influence the pathological subtype of breast cancer and provide further support for the hypothesis that ER-positive and ER-negative diseases are biologically distinct tumors. Understanding the etiologic heterogeneity of breast cancer may ultimately result in improvements in prevention, early detection, and treatment.

Published
2008

81. A low-frequency variant at 8q24.21 is strongly associated with risk of oligodendroglial tumors and astrocytomas with IDH1 or IDH2 mutation.

Author

Jenkins, Robert, Jenkins, Robert, Xiao, Yuanyuan, Sicotte, Hugues, Decker, Paul, Kollmeyer, Thomas, Hansen, Helen, Kosel, Matthew, Zheng, Shichun, Rice, Terri, Bracci, Paige, McCoy, Lucie, Smirnov, Ivan, Patoka, Joseph, Hsuang, George, Caron, Alissa, Fink, Stephanie, Halder, Chandralekha, Rynearson, Amanda, Fridley, Brooke, Buckner, Jan, ONeill, Brian, Giannini, Caterina, Lachance, Daniel, Pico, Alexander, Eckel-Passow, Jeanette, Prados, Michael, Berger, Mitchel, Wiemels, Joseph, Chang, Susan, Walsh, Kyle, Tihan, Tarik, Wiencke, John, Wrensch, Margaret, Jenkins, Robert, Jenkins, Robert, Xiao, Yuanyuan, Sicotte, Hugues, Decker, Paul, Kollmeyer, Thomas, Hansen, Helen, Kosel, Matthew, Zheng, Shichun, Rice, Terri, Bracci, Paige, McCoy, Lucie, Smirnov, Ivan, Patoka, Joseph, Hsuang, George, Caron, Alissa, Fink, Stephanie, Halder, Chandralekha, Rynearson, Amanda, Fridley, Brooke, Buckner, Jan, ONeill, Brian, Giannini, Caterina, Lachance, Daniel, Pico, Alexander, Eckel-Passow, Jeanette, Prados, Michael, Berger, Mitchel, Wiemels, Joseph, Chang, Susan, Walsh, Kyle, Tihan, Tarik, Wiencke, John, and Wrensch, Margaret

Abstract

Variants at 8q24.21 have been shown to be associated with glioma development. By means of tag SNP genotyping and imputation, pooled next-generation sequencing using long-range PCR and subsequent validation SNP genotyping, we identified seven low-frequency SNPs at 8q24.21 that were strongly associated with glioma risk (P=1×10(-25) to 1×10(-14)). The most strongly associated SNP, rs55705857, remained highly significant after individual adjustment for the other top six SNPs and two previously published SNPs. After stratifying by histological and tumor genetic subtype, the most significant associations of rs55705857 were with oligodendroglial tumors and gliomas with mutant IDH1 or IDH2 (odds ratio (OR)=5.1, P=1.1×10(-31) and OR=4.8, P=6.6×10(-22), respectively). Strong associations were observed for astrocytomas with mutated IDH1 or IDH2 (grades 2-4) (OR=5.16-6.66, P=4.7×10(-12) to 2.2×10(-8)) but not for astrocytomas with wild-type IDH1 and IDH2 (smallest P=0.26). The conserved sequence block that includes rs55705857 is consistently modeled as a microRNA.

Published
2012

82. Trisomy 8 in chronic lymphocytic leukaemia: a report of two cases

Author

Donatella Raspadori, Daniela Tozzuoli, Alessandro Gozzetti, Mariapia Lenoci, Francesco Zaja, Maristella Tassi, Simona Calabrese, Rosaria Crupi, Francesco Lauria, Gozzetti, A, Calabrese, S, Crupi, R, Zaja, Francesco, Tozzuoli, D, Tassi, M, Raspadori, D, Lenoci, M, and Lauria, F.

Subjects
Male, Cancer Research, Pathology, medicine.medical_specialty, Leukemia, Chronic lymphocytic leukemia, B-Cell, Trisomy, Biology, medicine.disease, Trisomy 8, Chromosomes, Lymphocytic, Genetics, medicine, Pair 8, Humans, Female, Chronic, Molecular Biology, Aged, Chromosomes, Human, Pair 8, Leukemia, Lymphocytic, Chronic, B-Cell, Human
Published
2007

83. Positive Selection on Loci Associated with Drug and Alcohol Dependence

Author

Andrew Brooks, John I. Nurnberger, Marc A. Schuckit, John Kramer, Brooke Sadler, Howard J. Edenberg, Gabe Haller, Alison Goate, Jay A. Tischfield, and Lin, Zhicheng Carl

Subjects
Male, lcsh:Medicine, Receptors, Nicotinic, Nicotinic, Drug Abuse, Nicotine, Receptors, lcsh:Science, Genetics, Multidisciplinary, Natural selection, biology, CHRNA5, Substance Abuse, Wechsler Adult Intelligence Scale, Single Nucleotide, Alcoholism, Multigene Family, Pair 8, Female, Mental health, Databases, Nucleic Acid, Chromosomes, Human, Pair 8, Research Article, Human, medicine.drug, Adult, Drug Abuse (NIDA Only), General Science & Technology, Nerve Tissue Proteins, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Chromosomes, Cocaine-Related Disorders, Databases, Tobacco, medicine, Humans, Polymorphism, 1000 Genomes Project, Selection (genetic algorithm), Chromosomes, Human, Pair 15, Nucleic Acid, Tobacco Smoke and Health, Prevention, lcsh:R, Human Genome, Haplotype, Pair 15, Brain Disorders, Genetic Loci, biology.protein, lcsh:Q
Abstract

Much of the evolution of human behavior remains a mystery, including how certain disadvantageous behaviors are so prevalent. Nicotine addiction is one such phenotype. Several loci have been implicated in nicotine related phenotypes including the nicotinic receptor gene clusters (CHRNs) on chromosomes 8 and 15. Here we use 1000 Genomes sequence data from 3 populations (Africans, Asians and Europeans) to examine whether natural selection has occurred at these loci. We used Tajima's D and the integrated haplotype score (iHS) to test for evidence of natural selection. Our results provide evidence for strong selection in the nicotinic receptor gene cluster on chromosome 8, previously found to be significantly associated with both nicotine and cocaine dependence, as well as evidence selection acting on the region containing the CHRNA5 nicotinic receptor gene on chromosome 15, that is genome wide significant for risk for nicotine dependence. To examine the possibility that this selection is related to memory and learning, we utilized genetic data from the Collaborative Studies on the Genetics of Alcoholism (COGA) to test variants within these regions with three tests of memory and learning, the Wechsler Adult Intelligence Scale (WAIS) Block Design, WAIS Digit Symbol and WAIS Information tests. Of the 17 SNPs genotyped in COGA in this region, we find one significantly associated with WAIS digit symbol test results. This test captures aspects of reaction time and memory, suggesting that a phenotype relating to memory and learning may have been the driving force behind selection at these loci. This study could begin to explain why these seemingly deleterious SNPs are present at their current frequencies.

Published
2015

84. Overlapping morphologic and immunophenotypic profiles in small B-cell lymphoma. A report of two cases

Author

Stefano Lazzi, Alberto Fabbri, Ioannis Kostopoulos, Alessandro D'Amuri, Lorenzo Leoncini, Mario Cocco, Francesco Forconi, Chiara Ginanneschi, and Maria Margherita De Santi

Subjects
Male, Pathology, Follicular lymphoma, genetics/metabolism, Chromosomal translocation, Translocation, Genetic, Aged, B-Lymphocytes, metabolism/pathology, Chromosomes, Human, Pair 11, genetics, Chromosomes, Pair 14, Pair 18, Pair 8, genetics, Cyclin D1, genetics/metabolism, Female, Humans, Immunophenotyping, methods, In Situ Hybridization, Fluorescence, Leukemia, Lymphocytic, Chronic, B-Cell, genetics/metabolism/pathology, Lymph Nodes, metabolism/pathology, Male, Middle Aged, Translocation, Genetic, Tumor Markers, Biological, metabolism, genetics/metabolism/pathology, immune system diseases, hemic and lymphatic diseases, genetics, Cyclin D1, B-cell lymphoma, Tumor Markers, In Situ Hybridization, Fluorescence, In Situ Hybridization, B-Lymphocytes, Leukemia, medicine.diagnostic_test, General Medicine, Middle Aged, BCL6, Female, Chromosomes, Human, Pair 8, metabolism/pathology, medicine.medical_specialty, Translocation, Biology, Chromosome aberration, Chromosomes, Fluorescence, Pathology and Forensic Medicine, Immunophenotyping, methods, Genetic, medicine, Biomarkers, Tumor, Humans, Molecular Biology, Aged, Chromosomes, Human, Pair 14, Chromosomes, Human, Pair 11, Cell Biology, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, Lymphoma, Lymph Nodes, Chromosomes, Human, Pair 18, Fluorescence in situ hybridization
Abstract

We present two cases of small B-cell lymphomas of particular diagnostic interest because the histological patterns were at variance with their immunophenotype. One of these lymphomas, involving the gallbladder and duodenum, showed a marginal zone lymphoma-like (MALT type) pattern of cellular infiltration with CD5 negativity but (unexpectedly) Cyclin D1 positivity. Fluorescence in situ hybridization analysis of this case was performed because of the aberrant expression of Cyclin D1, and was clearly positive for the Cyclin D1 gene translocation. The second case, occurring in a lymph node, showed the typical growth pattern of a follicular lymphoma but it had an atypical immunophenotype, namely, expression of Cyclin D1, CD10, and Bcl2 and focally Bcl6, accompanied by a lack of CD5 and CD23. The Cyclin D1 gene translocation was detected by fluorescence in situ hybridisation (FISH), whereas c-myc and Bcl2 genes translocation were absent. Numerical chromosomal changes, which were visualized for chromosomes 8, 11, and 18 could be correlated to the aberrant immunoprofile. In this context, we discuss the diagnostic value of Cyclin D1, CD5, CD23, CD10, Bcl6 markers revealed by immunohistochemistry, as well as the significance of detection by FISH of chromosomal translocations such as t(11;14) and t(14;18). The question still remains as to whether such cases should be designated as specific lymphoma entities or reported as unclassifiable and the chromosome aberration reported.

Published
2006

85. Common variants in LSP1, 2q35 and 8q24 and breast cancer risk for BRCA1 and BRCA2 mutation carriers

Author

Antoniou, A. C., Sinilnikova, O. M., McGuffog, L., Healey, S., Nevanlinna, H., Heikkinen, T., Simard, J., Spurdle, A. B., Beesley, J., Chen, X., Neuhausen, S. L., Ding, Y. C., Couch, F. J., Wang, X., Fredericksen, Z., Peterlongo, P., Peissel, B., Bonanni, B., Viel, A., Bernard, L., Radice, P., Szabo, C. I., Foretova, L., Zikan, M., Claes, K., Greene, M. H., Mai, P. L., Rennert, G., Lejbkowicz, F., Andrulis, I. L., Ozcelik, H., Glendon, G., Gerdes, A. -M, Thomassen, M., Sunde, L., Caligo, M. A., Laitman, Y., Kontorovich, T., Cohen, S., Kaufman, B., Dagan, E., Baruch, R. G., Friedman, E., Harbst, K., Barbany-Bustinza, G., Rantala, J., Ehrencrona, H., Karlsson, P., Domchek, S. M., Nathanson, K. L., Osorio, A., Blanco, I., Lasa, A., Benítez, J., Hamann, U., Hogervorst, F. B. L., Rookus, M. A., Collee, J. M., Devilee, P., Ligtenberg, M. J., van der Luijt, R. B., Aalfs, C. M., Waisfisz, Q., Wijnen, J., van Roozendaal, C. E. P., Peock, S., Cook, M., Frost, D., Oliver, C., Platte, R., Evans, D. G., Lalloo, F., Eeles, R., Izatt, L., Davidson, R., Chu, C., Eccles, D., Cole, T., Hodgson, S., Godwin, A. K., Stoppa-Lyonnet, D., Buecher, B., Léoné, M., Bressac-de Paillerets, B., Remenieras, A., Caron, O., Lenoir, G. M., Sevenet, N., Longy, M., Ferrer, S. F., Prieur, F., Goldgar, D., Miron, A., John, E. M., Buys, S. S., Daly, M. B., Hopper, J. L., Terry, M. B., Yassin, Y., Singer, C., Gschwantler-Kaulich, D., Staudigl, C., Hansen, T. V. O., Barkardottir, R. B., Kirchhoff, T., Pal, P., Kosarin, K., Offit, K., Piedmonte, M., Rodriguez, G. C., Wakeley, K., Boggess, J. F., Basil, J., Schwartz, P. E., Blank, S. V., Toland, A. E., Montagna, M., Casella, C., Imyanitov, E. N., Allavena, A., Schmutzler, R. K., Versmold, B., Engel, C., Meindl, A., Ditsch, N., Arnold, N., Niederacher, D., Deißler, H., Fiebig, B., Suttner, C., Schönbuchner, I., Gadzicki, D., Caldes, T., de la Hoya, M., Pooley, K. A., Easton, D. F., Chenevix-Trench, G., Antoniou, A. C., Sinilnikova, O. M., McGuffog, L., Healey, S., Nevanlinna, H., Heikkinen, T., Simard, J., Spurdle, A. B., Beesley, J., Chen, X., Neuhausen, S. L., Ding, Y. C., Couch, F. J., Wang, X., Fredericksen, Z., Peterlongo, P., Peissel, B., Bonanni, B., Viel, A., Bernard, L., Radice, P., Szabo, C. I., Foretova, L., Zikan, M., Claes, K., Greene, M. H., Mai, P. L., Rennert, G., Lejbkowicz, F., Andrulis, I. L., Ozcelik, H., Glendon, G., Gerdes, A. -M, Thomassen, M., Sunde, L., Caligo, M. A., Laitman, Y., Kontorovich, T., Cohen, S., Kaufman, B., Dagan, E., Baruch, R. G., Friedman, E., Harbst, K., Barbany-Bustinza, G., Rantala, J., Ehrencrona, H., Karlsson, P., Domchek, S. M., Nathanson, K. L., Osorio, A., Blanco, I., Lasa, A., Benítez, J., Hamann, U., Hogervorst, F. B. L., Rookus, M. A., Collee, J. M., Devilee, P., Ligtenberg, M. J., van der Luijt, R. B., Aalfs, C. M., Waisfisz, Q., Wijnen, J., van Roozendaal, C. E. P., Peock, S., Cook, M., Frost, D., Oliver, C., Platte, R., Evans, D. G., Lalloo, F., Eeles, R., Izatt, L., Davidson, R., Chu, C., Eccles, D., Cole, T., Hodgson, S., Godwin, A. K., Stoppa-Lyonnet, D., Buecher, B., Léoné, M., Bressac-de Paillerets, B., Remenieras, A., Caron, O., Lenoir, G. M., Sevenet, N., Longy, M., Ferrer, S. F., Prieur, F., Goldgar, D., Miron, A., John, E. M., Buys, S. S., Daly, M. B., Hopper, J. L., Terry, M. B., Yassin, Y., Singer, C., Gschwantler-Kaulich, D., Staudigl, C., Hansen, T. V. O., Barkardottir, R. B., Kirchhoff, T., Pal, P., Kosarin, K., Offit, K., Piedmonte, M., Rodriguez, G. C., Wakeley, K., Boggess, J. F., Basil, J., Schwartz, P. E., Blank, S. V., Toland, A. E., Montagna, M., Casella, C., Imyanitov, E. N., Allavena, A., Schmutzler, R. K., Versmold, B., Engel, C., Meindl, A., Ditsch, N., Arnold, N., Niederacher, D., Deißler, H., Fiebig, B., Suttner, C., Schönbuchner, I., Gadzicki, D., Caldes, T., de la Hoya, M., Pooley, K. A., Easton, D. F., and Chenevix-Trench, G.

Abstract

Genome-wide association studies of breast cancer have identified multiple single nucleotide polymorphisms (SNPs) that are associated with increased breast cancer risks in the general population. In a previous study, we demonstrated that the minor alleles at three of these SNPs, in FGFR2, TNRC9 and MAP3K1, also confer increased risks of breast cancer for BRCA1 or BRCA2 mutation carriers. Three additional SNPs rs3817198 at LSP1, rs13387042 at 2q35 and rs13281615 at 8q24 have since been reported to be associated with breast cancer in the general population, and in this study we evaluated their association with breast cancer risk in 9442 BRCA1 and 5665 BRCA2 mutation carriers from 33 study centres. The minor allele of rs3817198 was associated with increased breast cancer risk only for BRCA2 mutation carriers [hazard ratio (HR) = 1.16, 95% CI: 1.07-1.25, P-trend = 2.8 × 10-4]. The best fit for the association of SNP rs13387042 at 2q35 with breast cancer risk was a dominant model for both BRCA1 and BRCA2 mutation carriers (BRCA1: HR = 1.14, 95% CI: 1.04-1.25, P = 0.0047; BRCA2: HR = 1.18 95% CI: 1.04-1.33, P = 0.0079). SNP rs13281615 at 8q24 was not associated with breast cancer for either BRCA1 or BRCA2 mutation carriers, but the estimated association for BRCA2 mutation carriers (per-allele HR = 1.06, 95% CI: 0.98-1.14) was consistent with odds ratio estimates derived from population-based case-control studies. The LSP1 and 2q35 SNPs appear to interact multiplicatively on breast cancer risk for BRCA2 mutation carriers. There was no evidence that the associations vary by mutation type depending on whether the mutated protein is predicted to be stable or not., The Swedish BRCA1 and BRCA2 Study (SWE-BRCA) SWE-BRCA collaborators: P.K., Margareta Nordling, Annika Bergman and Zakaria Einbeigi, Gothenburg, Sahlgrenska University Hospital; Marie Stenmark-Askmalm and Sigrun Liedgren, Linkoping University Hospital; Ake Borg, Niklas Loman, Hakan Olsson, Ulf Kristoffersson, Helena Jernstrom, K.H. and Karin Henrisson, Lund University Hospital; Annika Lindblom, Brita Arver, Anna von Wachenfeldt, Annelie Liljegren, G.B.-B. and J.R., Stockholm, Karolinska. University Hospital; Beatrice Malmer, Eva-Lena Stattin and Monica Emanuelsson, Umea University Hospital; H.E., Richard Rosenquist Brandell and Niklas Dahl, Uppsala University Hospital.

Published
2009
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86. A reanalysis of 409 European-Ancestry and African American schizophrenia pedigrees reveals significant linkage to 8p23.3 with evidence of locus heterogeneity

Author

Holliday, Elizabeth, Mowry, Bryan, Nyholt, Dale, Holliday, Elizabeth, Mowry, Bryan, and Nyholt, Dale

Abstract

The detection and replication of schizophrenia risk loci can require substantial sample sizes, which has prompted various collaborative efforts for combining multiple samples. However, pooled samples may comprise sub-samples with substantial population genetic differences, including allele frequency differences. We investigated the impact of population differences via linkage reanalysis of Molecular Genetics of Schizophrenia 1 (MGS1) affected sibling-pair data, comprising two samples of distinct ancestral origin: European (EA: 263 pedigrees) and African-American (AA: 146 pedigrees). To exploit the linkage information contained within these distinct continental samples, we performed separate analyses of the individual samples, allowing for within-sample locus heterogeneity, and the pooled sample, allowing for both within-sample and between-sample heterogeneity. Significance levels, corrected for the multiple tests, were determined empirically. For all suggestive peaks, stronger linkage evidence was obtained in either the EA or AA sample than the combined sample, regardless of how heterogeneity was modeled for the latter. Notably, we report genomewide significant linkage of schizophrenia to 8p23.3 and evidence for a second, independent susceptibility locus, reaching suggestive linkage, 29 cM away on 8p21.3. We also detected suggestive linkage on chromosomes 5p13.3 and 7q36.2. Many regions showed pronounced differences in the extent of linkage between the EA and AA samples. This reanalysis highlights the potential impact of population differences upon linkage evidence in pooled data and demonstrates a useful approach for the analysis of samples drawn from distinct continental groups.

Published
2008

87. Narrowing of the critical region in autosomal recessive spastic paraplegia linked to the SPG5 locus

Author

Maria Muglia, Chiara Criscuolo, Francesca Luisa Conforti, Paola Valentino, Alessandro Filla, Angela Magariello, Alessandra Patitucci, A. Epifanio, G. De Michele, Teresa Sprovieri, V. Scarano, P. La Spina, Rosalucia Mazzei, A. L. Gabriele, G. Ambrosio, Pio D'Adamo, Aldo Quattrone, Letterio Morgante, Paolo Gasparini, M., Muglia, C., Criscuolo, A., Magariello, Michele, G., V., Scarano, D'Adamo, ADAMO PIO, G., Ambrosio, a. L., Gabriele, A., Patitucci, R., Mazzei, F. L., Conforti, T., Sprovieri, L., Morgante, A., Epifanio, Spina, P., P., Valentino, Gasparini, Paolo, A., Filla, A., Quattrone, Muglia, M., Criscuolo, C., Magariello, A., DE MICHELE, Giuseppe, Scarano, V., D'Adamo, P., Ambrosio, G., Gabriele, A. L., Patitucci, A., Mazzei, R., Conforti, F. L., Sprovieri, T., Morgante, L., Epifanio, A., La Spina, P., Valentino, P., Gasparini, P., Filla, Alessandro, and Quattrone, A.

Subjects
Male, Candidate gene, Hereditary spastic paraplegia, Genetic analysis, Gene, Genetic Marker, Spastic, Genetics (clinical), Genetics, SPG5 locu, Linkage, General Neuroscience, Middle Aged, musculoskeletal system, Pedigree, Italy, Progressive spasticity, Microsatellite, Pair 8, genetic [Paraplegia], Female, Paraplegia, SPG5 locus, Chromosomes, Human, Pair 8, Human, Genetic Markers, Adult, Locus (genetics), Genes, Recessive, Biology, Chromosome, Chromosomes, Candidate genes, Association, Cellular and Molecular Neuroscience, Paraplegia: genetics, medicine, Humans, Recessive, Family Health, Neuroscience (all), Haplotype, medicine.disease, nervous system diseases, Autosomal recessive spastic paraplegia, Genes, Genetic marker, Lod Score, Neurology (clinical)
Abstract

Hereditary spastic paraplegias are neurodegenerative disorders characterized clinically by progressive spasticity of the lower limbs; they are inherited as autosomal dominant, autosomal recessive and X-linked traits. We have analyzed four autosomal recessive HSP families gathered from southern Italy. We performed genetic analysis using microsatellite markers associated with SPG5, SPG7, SPG11 and SPG14. Positive lod scores were obtained with markers located on chromosome 8. The lod scores for the four combined families were significantly higher than 3 for D8S509, D8S1102, D8S1723 and D8S260 with a maximum two-point lod score at θ = 0 of 3.99 for the marker D8S260. In one of the examined families, the haplotype analysis suggests two key recombination events demonstrating that the gene is localized in the 11 cM region flanked by markers D8S285 and D8S544, refining the ARHSP region by approximately 22 cm. We also analyzed five candidate genes localized within the HSP region: TOX, syndecan-binding-protein (SDCBP), RAB2, CA8 and PENK, but we did not find disease causing mutations.

Published
2004

88. Exploration of a putative susceptibility locus for idiopathic generalized epilepsy on chromosome 8p12

Author

Sander, Thomas, Windemuth, Christine, Schulz, Herbert, Saar, Kathrin, Gennaro, Elena, Riggio, Concetta, Bianchi, Amedeo, Zara, Federico, Rudolf, Gabrielle, Picard, Fabienne, Bulteau, Christine, Kaminska, Anna, Cieuta, Cécile, Prud'homme, Jean-François, Dulac, Olivier, Bate, Louise, Robinson, Robert, Gardiner, R Mark, Covanis, Athanasios, de Haan, Gerrit-Jan, Janssen, Guus A M A J, van Erp, M Gerard, Boezeman, Eduard H J F, Lindhout, Dick, Heils, Armin, Nürnberg, Peter, Janz, Diéter, and European Consortium on the Genetics of Idiopathic Generalized Epilepsy

Subjects
Proband, Male, Idiopathic generalized epilepsy, Juvenile, Gene Frequency, Models, Epilepsy, Generalized / genetics, Child, Dinucleotide Repeats, Genetics, Linkage, Myoclonic Epilepsy, Juvenile, Epilepsy, Absence / genetics, Chromosome Mapping, Syndrome, Genetic Predisposition to Disease / classification, Europe, Absence, Phenotype, Neurology, Myoclonic Epilepsy, Chromosomal region, Microsatellite, Pair 8, Epilepsy, Generalized, Female, Human, Chromosomes, Human, Pair 8, Adult, Genetic Markers, Gene Frequency / genetics, Myoclonic Epilepsy, Juvenile / genetics, Genotype, Locus (genetics), Epilepsy, Tonic-Clonic / genetics, Biology, Chromosomes, Genetic, Genetic model, medicine, Humans, Genetic Predisposition to Disease, Allele, Polymorphism, Alleles, Chromosome 8, Epilepsy, Absence, Epilepsy, Tonic-Clonic, Lod Score, Models, Genetic, Polymorphism, Genetic, Genetic Markers / genetics, Epilepsy, Generalized, Tonic-Clonic, medicine.disease, ddc:616.8, Myoclonic epilepsy, Neurology (clinical)
Abstract

Purpose: A recent genome-wide scan revealed a major susceptibility locus for idiopathic generalized epilepsies (IGEs) in the chromosomal region 8p12 in 32 IGE families without members with juvenile myoclonic epilepsy (JME). This study explored the presence of an IGE locus in the chromosomal region 8p12.Methods: Our study included 176 multiplex families of probands with common IGE syndromes. Parametric and nonparametric multipoint linkage analyses were carried out between the IGE trait and six microsatellite polymorphisms encompassing the putative susceptibility locus. To explore the associated phenotype-genotype relation, two distinct subgroups of families were selected by the presence (n = 64) or absence (n = 112) of a family member with JME. To adjust the phenotypic spectrum toward adolescent-onset IGEs, a third subgroup of 28 families without JME was chosen through an IGE proband with seizure onset at age 10-20 years.Results: Parametric and nonparametric multipoint linkage analyses provided no evidence for linkage between IGE and markers encompassing the putative IGE locus in the chromosomal region 8p12. Furthermore, we found no hint of linkage along the candidate region in any of the three family subgroups.Conclusions: We failed to provide evidence for a major IGE locus in the chromosomal region 8p12. On the contrary, these parametric linkage results provide strong evidence against linkage across the candidate region under a broad range of genetic models. If there is a susceptibility locus for IGE in the chromosomal region 8p12, then the size of the effect or the proportion of linked families is too small to detect linkage in the investigated family sample.

Published
2003

89. A genome-wide search for linkage-disequilibrium with type 1 diabetes in a recent genetically isolated population from the Netherlands

Author

Vaessen, N. (Norbert), Houwing-Duistermaat, J.J. (Jeanine), Rademaker, T.A.M. (Tessa), Testers, L., Batstra, M.R. (Manou), Sandkuijl, L.A. (Lodewijk), Duijn, C.M. (Cornelia) van, Oostra, B.A. (Ben), Snijders, P.J.L.M. (Pieter), Heutink, P. (Peter), Vaessen, N. (Norbert), Houwing-Duistermaat, J.J. (Jeanine), Rademaker, T.A.M. (Tessa), Testers, L., Batstra, M.R. (Manou), Sandkuijl, L.A. (Lodewijk), Duijn, C.M. (Cornelia) van, Oostra, B.A. (Ben), Snijders, P.J.L.M. (Pieter), and Heutink, P. (Peter)

Abstract

Type 1 diabetes has a substantial genetic component, with consistent evidence for a susceptibility locus in the HLA-DR/DQ region (chromosome 6p) and the insulin gene region (chromosome 11p). Genome scans have identified >18 other genomic regions that may harbor putative type 1 diabetes genes. However, evidence for most regions varies in different data sets. Given the genetic heterogeneity of type 1 diabetes, studies in homogeneous genetically isolated populations may be more successful in mapping susceptibility loci than in complex outbred populations. We describe a genome-wide search in a recently Dutch isolated population. We identified 43 patients that could be traced back to a common ancestor within 15 generations and performed a genome-wide scan using a combined linkage- and association-based approach. In addition to the HLA locus, evidence for type 1 diabetes loci was observed on chromosome 8q24 (marker D8S1128) and on chromosome 17q24 (marker D17S2059). Both the 8q and 17q localization are supported by allele-sharing at adjacent markers in affected individuals. Statistical evidence for a conserved ancestral haplotype was found for chromosome 8q24.

Published
2002

90. Further evidence for linkage of Gilles de la Tourette syndrome (GTS) susceptibility loci on chromosomes 2p11, 8q22 and 11q23-24 in South African Afrikaners

Author

Simonic, I., Nyholt, D.R., Gericke, G. S., Gordon, D., Matsumoto, N., Ledbetter, D. H., Ott, J., Weber, J. L., Simonic, I., Nyholt, D.R., Gericke, G. S., Gordon, D., Matsumoto, N., Ledbetter, D. H., Ott, J., and Weber, J. L.

Abstract

Utilizing DNA samples from 91 Afrikaner nuclear families with one or more affected children, five genomic regions on chromosomes 2p, 8q, 11q, 20q, and 21q that gave evidence for association with GTS in previous case-control association studies were investigated for linkage and association with GTS. Highly polymorphic markers with mean heterozygosity of 0.77 were typed and resulting genotypes evaluated using single marker transmission disequilibrium (TDT), single marker haplotype relative risk (HRR), and multi-marker "extended" TDT and HRR methods. Single marker TDT analysis showed evidence for linkage or association, with p-values near 0.05, for markers D2S139, GATA28F12, and D11S1377 on chromosomes 2p11, 8q22 and 11q23-24, respectively. Extended, two-locus TDT and HRR analysis provided further evidence for linkage or association on chromosome 2 with p-values of 0.007 and 0.025, and chromosome 8 with p-values of 0.059 and 0.013, respectively. These results provide important additional evidence for the location of GTS susceptibility loci.

Published
2001

91. An unbalanced submicroscopic translocation t(8;16)(q24.3;p13.3)pat associated with tuberous sclerosis complex, adult polycystic kidney disease, and hypomelanosis of Ito

Author

Eussen, H.J.F.M.M. (Bert), Verhoef, S., Fois, A., Halley, D.J.J. (Dicky), Bartalini, G. (Gabriella), Bakker, L. (Lida), Balestri, P. (Paolo), Lucca, C. di, Hemel, J.O. van, Dauwerse, H., Ouweland, A.M.W. (Ans) van den, Ris-Stalpers, C. (Carolyn), Eussen, H.J.F.M.M. (Bert), Verhoef, S., Fois, A., Halley, D.J.J. (Dicky), Bartalini, G. (Gabriella), Bakker, L. (Lida), Balestri, P. (Paolo), Lucca, C. di, Hemel, J.O. van, Dauwerse, H., Ouweland, A.M.W. (Ans) van den, and Ris-Stalpers, C. (Carolyn)

Abstract

We report on a familial submicroscopic translocation involving chromosomes 8 and 16. The proband of the family had a clinical picture suggestive of a large deletion in the chromosome 16p13.3 area, as he was affected with tuberous sclerosis complex (TSC) and had alpha thalassaemia trait, and his half brother, who also had TSC, may have suffered additionally from polycystic kidney disease (PKD). FISH studies provided evidence for a familial translocation t(8;16)(q24.3;p13.3) with an unbalanced form in the proband and a balanced form in the father and in a paternal aunt. The unbalanced translocation caused the index patient to be deleted for the chromosome 16p13.3-pter region, with the most proximal breakpoint described to date for terminal 16p deletions. In addition, FISH analysis showed a duplication for the distal 8q region. Since the index patient also had hypomelanosis of Ito (HI), either of the chromosomal areas involved in the translocation may be a candidate region for an HI determining gene. Furthermore, it is noteworthy that both carriers of the balanced translocation showed a nodular goitre, while the proband has hypothyroidism.

Published
2000

92. A new case of Ambras syndrome associated with a paracentric inversion (8) (q12; q22)

Author

B. Tedeschi, Stefano Cianfarani, Rubén A. Toscano, R. Balducci, Vincenzo Toscano, Brunetto Boscherini, A. Mangiantini, and Cinzia Galasso

Subjects
Hypertrichosis, medicine.drug_class, Biology, Chromosomes, Genetics, medicine, Humans, Genetics (clinical), Testosterone, Chromosomal inversion, Settore MED/38 - Pediatria Generale e Specialistica, Inversion (evolutionary biology), Chromosome, Karyotype, Anatomy, Syndrome, medicine.disease, Androgen, Dihydrotestosterone, Chromosome Inversion, Female, Chromosomes, Human, Pair 8, Pair 8, Human, medicine.drug
Abstract

Ambras syndrome (AS) is a special form of congenital universal hypertrichosis described for the first time by Baumeister et al. (1). This form differs from other forms of congenital hypertrichosis in the pattern of hair distribution and its associated anomalies. The molecular-genetic cause of AS is unknown; the association of AS with a pericentric inversion (8) (p11.2; q22) described in the case of Baumeister so far has been unique in the literature. This report is the tenth with clinical signs of AS so far described in the literature and the second with an inversion in chromosome 8 and the first with evaluation of peripheral androgens. The new-born girl presented with abundant and dark hair on the face and ears, on the shoulders and on the arms; the other parts of the body were covered with fine, lightly pigmented hair. The face showed many dysmorphic features. Chromosome analysis showed a paracentric inversion of one chromosome 8. The breakpoints were localised at q12 and q22. The parental karyotypes were normal. Laboratory investigation showed normal plasma levels of testosterone, androstenedione (A), 17-hydroxyprogesterone, dehydroepiandrosterone-sulphate (DHA-S), free testosterone (FT), dihydrotestosterone (DHT) and 3alpha-androstanediol-glucuronide (3AG). Here we report a chromosomal inversion similar to that found previously not associated with alterations in androgen plasma levels.

Published
1998

93. Hereditary auditory, vestibular, motor, and sensory neuropathy in a Slovenian Roma (Gypsy) kindred.

Author

Butinar, D, Butinar, D, Zidar, J, Leonardis, L, Popovic, M, Kalaydjieva, L, Angelicheva, D, Sininger, Y, Keats, B, Starr, A, Butinar, D, Butinar, D, Zidar, J, Leonardis, L, Popovic, M, Kalaydjieva, L, Angelicheva, D, Sininger, Y, Keats, B, and Starr, A

Abstract

Members of a Roma (Gypsy) family with hereditary motor and sensory peripheral neuropathy (HMSN) and concomitant auditory and vestibular cranial neuropathies were identified in Kocevje, Slovenia. The illness begins in childhood with a severe and progressive motor disability and the deafness is delayed until the second decade. There are no symptoms of vestibular dysfunction. The family structure is consistent with an autosomal recessive pattern of inheritance and the genetic locus for the disorder is linked to the same region of chromosome 8q24 as other Roma families with HMSN and deafness from Lom, Bulgaria (HMSN-Lom). The present study shows that the deafness is caused by a neuropathy of the auditory nerve with preserved measures of cochlear outer hair cell function (otoacoustic emissions and cochlear microphonics) but absent neural components of auditory brainstem potentials. The hearing loss affects speech comprehension out of proportion to the pure tone loss. Vestibular testing showed absence of caloric responses. Physiological and neuropathological studies of peripheral nerves were compatible with the nerve disorder contemporaneously affecting Schwann cells and axons resulting in both slowed nerve conduction and axonal loss. Genetic linkage studies suggest a refinement of the 8q24 critical region containing the HMSN-Lom locus that affects peripheral motor and sensory nerves as well as the cranial auditory and vestibular nerves.

Published
1999

94. Constitutional trisomy 8 and myelodysplasia: report of a case and review of the literature

Author

G. Neri, Assunta Tornesello, Maurizio Genuardi, Marcella Zollino, Giuseppe Zampino, Stefano Mastrangelo, Jolanta Bajer, and R. Mastrangelo

Subjects
Male, Cancer Research, Pediatrics, medicine.medical_specialty, Pathology, Adolescent, Aneuploidy, Trisomy, Trisomy 8, Chromosomes, medicine, Humans, Warkany syndrome, business.industry, Myelodysplastic syndromes, Hematology, medicine.disease, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Oncology, Myelodysplastic Syndromes, Pair 8, Congenital disease, business, Human, Chromosomes, Human, Pair 8
Abstract

A diagnosis of myelodysplastic syndrome was made in an 18-year-old patient with Warkany syndrome due to constitutional trisomy 8 mosaicism. The possible causal role of this particular chromosome constitution with respect to myelodysplasia and embryonal childhood tumors is discussed.

Published
1995

95. Polyclonal haemopoieses associated with long-term persistence of the AML1-ETO transcript in patients with FAB M2 acute myeloid leukaemia in continous clinical remission

Author

F. Lo Coco, Luigi Resegotti, C. Rosso, G. Saglio, Bernardino Allione, Giovanni Martinelli, M. Pampinella, Angelo Guerrasio, A. Santoro, and Carlo Lanza

Subjects
Myeloid, Male, Neoplasm, Residual, Oncogene Proteins, Fusion, Chromosomes, Human, Pair 21, Chromosomal translocation, Translocation, Genetic, Pathogenesis, RUNX1 Translocation Partner 1 Protein, hemic and lymphatic diseases, 80 and over, X chromosome, Aged, 80 and over, Oncogene Proteins, Leukemia, biology, Adult, Aged, Base Sequence, Chromosomes, Human, Pair 8, Core Binding Factor Alpha 2 Subunit, DNA-Binding Proteins, Female, Hematopoiesis, Humans, Leukemia, Myeloid, Acute, Middle Aged, Molecular Sequence Data, Neoplasm Proteins, Transcription Factors, Proto-Oncogene Proteins, Hematology, Haematopoiesis, medicine.anatomical_structure, Residual, Pair 8, Human, Translocation, Acute, Chromosomes, Genetic, medicine, Fusion, Minimal residual disease, Fusion transcript, Polyclonal antibodies, Immunology, biology.protein, Neoplasm, Bone marrow, Pair 21, Settore MED/15 - Malattie del Sangue
Abstract

The t(8;21) (q22;q22) translocation is a recurring chromosomal abnormality observed in about 20-40% of AML patients with subtype FAB M2 (AML-M2). The molecular facet of this translocation is represented by the formation of a new hybrid gene, the AML1-ETO, which is regularly transcribed in a chimaeric mRNA and translated into a new fusion protein believed to have a key role in the pathogenesis of this type of leukaemia. We looked for the presence of AML1-ETO transcripts, by RT-PCR, in 49 unselected patients affected by AML-M2 diagnosed at various Italian Institutions. A hybrid transcript was detected in 11 cases (23%). Minimal residual disease status was investigated in three patients in continuous complete remission (CCR) after a median follow-up of 44 months; at least one sample from each subject was found positive for the AML1-ETO transcript suggesting a long-term persistence of t(8;21) leukaemic cells. In two female patients in CCR a 'clonality' analysis was performed on peripheral blood DNA by exploiting the X chromosome inactivation pattern of the human androgen-receptor gene (HUMARA); in both cases the results were consistent with the presence of a polyclonal haemopoiesis. Our data confirm that the persistence of residual cells expressing the AML1-ETO transcripts is a frequent occurrence even in patients with long-term remission; on the other hand, clonality assays indicate that in t(8;21) leukaemias long-term remission haemopoiesis is sustained by a polyclonal bone marrow reconstitution.

Published
1995

96. p53 gene inactivation in acute lymphoblastic leukemia of B cell lineage associates with chromosomal breakpoints at 11q23 and 8q24

Author

Lanza C, Gaidano G, Cimino G, Lo Coco F, Basso G, Sainati L, Pastore C, Josep Nomdedeu, Volpe G, and Parvis G

Subjects
p53, Base Sequence, Bone Marrow, Burkitt Lymphoma, Chromosome Mapping, DNA, Neoplasm, DNA-Binding Proteins, Exons, Fusion Proteins, bcr-abl, Gene Rearrangement, Genes, myc, Genes, ras, Histone-Lysine N-Methyltransferase, Humans, Molecular Sequence Data, Myeloid-Lymphoid Leukemia Protein, Polymerase Chain Reaction, Translocation, Genetic, Chromosome Aberrations, Chromosome Disorders, Chromosomes, Human, Pair 11, Chromosomes, Human, Pair 8, Genes, p53, Mutation, Proto-Oncogenes, Transcription Factors, bcr-abl, Translocation, Chromosomes, Genetic, Pair 11, ras, Fusion Proteins, DNA, myc, Genes, Neoplasm, Pair 8, Settore MED/15 - Malattie del Sangue, Human
Abstract

The clinical heterogeneity of acute lymphoblastic leukemia (ALL) of B cell lineage reflects the presence of distinct molecular pathways leading to well-defined ALL molecular subtypes. These molecular pathways include the formation of the fusion transcripts BCR/ABL and E2A/PBX1, due to t(9;22) and t(1;19), respectively, as well as rearrangements of the MLL gene at 11q23 and of c-MYC at 8q24. Hyperdiploid ALL in the absence of chromosomal structural abnormalities is an additional ALL molecular subtype. Mutations of the RAS family genes and of the p53 tumor suppressor gene represent additional genetic lesions detected in a fraction (10-20%) of ALL cases. RAS activation in ALL may be detected in all molecular subtypes of ALL and denotes poor prognosis. Conversely, little is known regarding the clinical and biological features of ALL cases carrying p53 mutations. In order to help clarify the role of p53 inactivation in ALL development, we have determined the frequency of p53 mutations throughout the molecular spectrum of B cell lineage ALL. We report that p53 inactivation in ALL of B cell lineage is restricted to cases carrying a rearrangement of MLL or c-MYC, whereas it is consistently negative in other molecular subgroups. These data underline the molecular heterogeneity of ALL of B cell lineage and indicate that at least some of the molecular pathways involved in ALL pathogenesis require more than one genetic lesion.

Published
1995

97. Heterogeneity of lineage involvement by trisomy 8 in myelodysplastic syndrome. A multiparameter analysis combining conventional cytogenetics, DNA in situ hybridization, and bone marrow culture studies

Author

F, Fagioli, A, Cuneo, A, Bardi, M G, Carli, R, Bigoni, R, Balsamo, R, Previati, I, Pazzi, G, Roberti, and G M, Rigolin

Subjects
Male, Cultured, Cells, Trisomy, DNA, Fluorescence, Chromosomes, Immunophenotyping, Genetic Heterogeneity, Bone Marrow, Myelodysplastic Syndromes, Humans, Pair 8, Cells, Cultured, In Situ Hybridization, Fluorescence, Aged, Chromosomes, Human, Pair 8, In Situ Hybridization, Human
Abstract

To better understand the role of trisomy 8 in myelodysplastic syndrome (MDS), we performed a multiparameter analysis combining conventional chromosome studies (CCS), fluorescence in situ hybridization (FISH), and bone marrow (BM) culture studies in two patients with MDS evolving into acute myeloid leukemia (AML). A mosaicism of a cytogenetically normal clone and a clone with trisomy 8 was detected in both patients throughout the course of the disease, a finding confirmed by FISH on BM cells. The relative size of the trisomic clone increased from 52% to 71% (p0.0001) and from 53% to 69% (p = 0.001) of all BM cells at the time of the leukemic switch in patients 1 and 2, respectively. Combined FISH and immunophenotyping of BM cells showed involvement of the granulomonocytic lineage in patient 1 and involvement of erythroid cells as well as of the granulomonocytic lineage in patient 2. Only disomic lymphocytes were detected in both patients. FISH on single hemopoietic colonies grown in semisolid media detected trisomic CFU-GM and disomic BFU-E in patient 1, whereas a proportion of CFU-GM and BFU-E deriving from the trisomic clone was detected in patient 2. However, the percent of trisomic colonies was lower than the percent of involved granulomonocyte precursors and involved erythroblasts, as detected by combined FISH and immunophenotyping on fresh BM samples. We have thus shown heterogeneity of lineage involvement by trisomy 8 in MDS undergoing transformation into AML. Although preferential growth of disomic clones may occur in vitro, the finding of an increased size of the trisomic clone at the time of leukemic switch suggests that these cells had proliferative advantage in vivo over cells without trisomy 8.

Published
1995

98. Human beta defensin 1 gene: six new variants

Author

Sergio Crovella, Doroti Pirulli, Anna Belgrano, Antonio Amoroso, Michele Boniotto, Elena Bevilacqua, Serena Vatta, S., Vatta, M., Boniotto, E., Bevilacqua, A., Belgrano, D., Pirulli, Crovella, Sergio, and A., Amoroso

Subjects
3' Untranslated Region, Mutation, Missense, Computational biology, Biology, Chromosome, Polymerase Chain Reaction, Chromosomes, Defensins, Restriction Fragm, Blood Protein, Genetics, Humans, 3' Untranslated Regions, Blood Proteins, Human, Pair 8, Genetic Variation, Mutation, Missense, Polymorphism, Proteins, ent Length, Gene, Genetics (clinical), Protein, Beta-defensin 1, Defensin, Polymorphism, Restriction Fragment Length, Chromosomes, Human, Pair 8
Abstract

Mutation and Polymorphism Report

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