Literature DB >> 17295306

Assessing human germ-cell mutagenesis in the Postgenome Era: a celebration of the legacy of William Lawson (Bill) Russell.

Andrew J Wyrobek1, John J Mulvihill, John S Wassom, Heinrich V Malling, Michael D Shelby, Susan E Lewis, Kristine L Witt, R Julian Preston, Sally D Perreault, James W Allen, David M Demarini, Richard P Woychik, Jack B Bishop.   

Abstract

Birth defects, de novo genetic diseases, and chromosomal abnormality syndromes occur in approximately 5% of all live births, and affected children suffer from a broad range of lifelong health consequences. Despite the social and medical impact of these defects, and the 8 decades of research in animal systems that have identified numerous germ-cell mutagens, no human germ-cell mutagen has been confirmed to date. There is now a growing consensus that the inability to detect human germ-cell mutagens is due to technological limitations in the detection of random mutations rather than biological differences between animal and human susceptibility. A multidisciplinary workshop responding to this challenge convened at The Jackson Laboratory in Bar Harbor, Maine. The purpose of the workshop was to assess the applicability of an emerging repertoire of genomic technologies to studies of human germ-cell mutagenesis. Workshop participants recommended large-scale human germ-cell mutation studies be conducted using samples from donors with high-dose exposures, such as cancer survivors. Within this high-risk cohort, parents and children could be evaluated for heritable changes in (a) DNA sequence and chromosomal structure, (b) repeat sequences and minisatellites, and (c) global gene expression profiles and pathways. Participants also advocated the establishment of a bio-bank of human tissue samples from donors with well-characterized exposure, including medical and reproductive histories. This mutational resource could support large-scale, multiple-endpoint studies. Additional studies could involve the examination of transgenerational effects associated with changes in imprinting and methylation patterns, nucleotide repeats, and mitochondrial DNA mutations. The further development of animal models and the integration of these with human studies are necessary to provide molecular insights into the mechanisms of germ-cell mutations and to identify prevention strategies. Furthermore, scientific specialty groups should be convened to review and prioritize the evidence for germ-cell mutagenicity from common environmental, occupational, medical, and lifestyle exposures. Workshop attendees agreed on the need for a full-scale assault to address key fundamental questions in human germ-cell environmental mutagenesis. These include, but are not limited to, the following: Do human germ-cell mutagens exist? What are the risks to future generations? Are some parents at higher risk than others for acquiring and transmitting germ-cell mutations? Obtaining answers to these, and other critical questions, will require strong support from relevant funding agencies, in addition to the engagement of scientists outside the fields of genomics and germ-cell mutagenesis.

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Year:  2007        PMID: 17295306      PMCID: PMC2071946          DOI: 10.1002/em.20284

Source DB:  PubMed          Journal:  Environ Mol Mutagen        ISSN: 0893-6692            Impact factor:   3.216


  101 in total

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Review 5.  Ionizing radiation and genetic risks XIV. Potential research directions in the post-genome era based on knowledge of repair of radiation-induced DNA double-strand breaks in mammalian somatic cells and the origin of deletions associated with human genomic disorders.

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Review 6.  Relative susceptibilities of male germ cells to genetic defects induced by cancer chemotherapies.

Authors:  Andrew J Wyrobek; Thomas E Schmid; Francesco Marchetti
Journal:  J Natl Cancer Inst Monogr       Date:  2005

7.  Advancing age has differential effects on DNA damage, chromatin integrity, gene mutations, and aneuploidies in sperm.

Authors:  A J Wyrobek; B Eskenazi; S Young; N Arnheim; I Tiemann-Boege; E W Jabs; R L Glaser; F S Pearson; D Evenson
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8.  Genetic disease in offspring of long-term survivors of childhood and adolescent cancer.

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9.  Comparison of germ cell mutagenicity in male CYP2E1-null and wild-type mice treated with acrylamide: evidence supporting a glycidamide-mediated effect.

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10.  Somatic cell gene mutations in humans: biomarkers for genotoxicity.

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Journal:  Environ Health Perspect       Date:  1993-10       Impact factor: 9.031

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Journal:  Int J Cancer       Date:  2011-05-15       Impact factor: 7.396

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4.  Comparison of germ line minisatellite mutation detection at the CEB1 locus by Southern blotting and PCR amplification.

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6.  James V. Neel and Yuri E. Dubrova: Cold War debates and the genetic effects of low-dose radiation.

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7.  Stillbirth and neonatal death in relation to radiation exposure before conception: a retrospective cohort study.

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9.  Parental nutrient intake and risk of retinoblastoma resulting from new germline RB1 mutation.

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10.  Cancer in the offspring of female radiation workers: a record linkage study.

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