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An evolutionary genomic approach to identify genes involved in human birth timing
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نویسنده
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plunkett j. ,doniger s. ,orabona g. ,morgan t. ,haataja r. ,hallman m. ,puttonen h. ,menon r. ,kuczynski e. ,norwitz e. ,snegovskikh v. ,palotie a. ,peltonen l. ,fellman v. ,defranco e.a. ,chaudhari b.p. ,mcgregor t.l. ,mcelroy j.j. ,oetjens m.t. ,teramo k. ,borecki i. ,fay j. ,muglia l.
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منبع
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plos genetics - 2011 - دوره : 7 - شماره : 4
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چکیده
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Coordination of fetal maturation with birth timing is essential for mammalian reproduction. in humans,preterm birth is a disorder of profound global health significance. the signals initiating parturition in humans have remained elusive,due to divergence in physiological mechanisms between humans and model organisms typically studied. because of relatively large human head size and narrow birth canal cross-sectional area compared to other primates,we hypothesized that genes involved in parturition would display accelerated evolution along the human and/or higher primate phylogenetic lineages to decrease the length of gestation and promote delivery of a smaller fetus that transits the birth canal more readily. further,we tested whether current variation in such accelerated genes contributes to preterm birth risk. evidence from allometric scaling of gestational age suggests human gestation has been shortened relative to other primates. consistent with our hypothesis,many genes involved in reproduction show human acceleration in their coding or adjacent noncoding regions. we screened >8,400 snps in 150 human accelerated genes in 165 finnish preterm and 163 control mothers for association with preterm birth. in this cohort,the most significant association was in fshr,and 8 of the 10 most significant snps were in this gene. further evidence for association of a linkage disequilibrium block of snps in fshr,rs11686474,rs11680730,rs12473870,and rs1247381 was found in african americans. by considering human acceleration,we identified a novel gene that may be associated with preterm birth,fshr. we anticipate other human accelerated genes will similarly be associated with preterm birth risk and elucidate essential pathways for human parturition. © 2011 plunkett et al.
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آدرس
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department of pediatrics,vanderbilt university school of medicine,monroe carell jr. children's hospital at vanderbilt,nashville,tn,united states,human and statistic genetics program,washington university school of medicine,st. louis,mo, United States, computational biology program,washington university school of medicine,st. louis,mo, United States, department of pediatrics,vanderbilt university school of medicine,monroe carell jr. children's hospital at vanderbilt,nashville,tn,united states,center for human genetics research,vanderbilt university school of medicine,nashville,tn, United States, department of pediatrics,vanderbilt university school of medicine,monroe carell jr. children's hospital at vanderbilt,nashville,tn,united states,center for human genetics research,vanderbilt university school of medicine,nashville,tn, United States, institute of clinical medicine,department of pediatrics,university of oulu,oulu, Finland, institute of clinical medicine,department of pediatrics,university of oulu,oulu, Finland, departments of obstetrics and gynecology,university of helsinki,helsinki, Finland, the perinatal research center,nashville,tn,united states,department of epidemiology,rollins school of public health,emory university,atlanta,ga, United States, department of obstetrics,gynecology,and reproductive sciences,yale university school of medicine,new haven,ct, United States, department of obstetrics,gynecology,and reproductive sciences,yale university school of medicine,new haven,ct, United States, department of obstetrics,gynecology,and reproductive sciences,yale university school of medicine,new haven,ct, United States, finnish institute of molecular medicine,university of helsinki,helsinki,finland,the broad institute of mit and harvard,cambridge,ma,united states,wellcome trust sanger institute,cambridge, United Kingdom, finnish institute of molecular medicine,university of helsinki,helsinki,finland,the broad institute of mit and harvard,cambridge,ma,united states,wellcome trust sanger institute,cambridge, United Kingdom, department of pediatrics,lund university,lund,sweden,department of pediatrics,university of helsinki,helsinki, Finland, department of obstetrics and gynecology,university of cincinnati college of medicine,cincinnati,oh, United States, department of pediatrics,washington university school of medicine,st. louis,mo, United States, department of pediatrics,vanderbilt university school of medicine,monroe carell jr. children's hospital at vanderbilt,nashville,tn, United States, department of pediatrics,vanderbilt university school of medicine,monroe carell jr. children's hospital at vanderbilt,nashville,tn,united states,center for human genetics research,vanderbilt university school of medicine,nashville,tn, United States, center for human genetics research,vanderbilt university school of medicine,nashville,tn, United States, departments of obstetrics and gynecology,university of helsinki,helsinki, Finland, division of statistical genomics,washington university school of medicine,st. louis,mo, United States, department of genetics and center for genome sciences,washington university school of medicine,st. louis,mo, United States, department of pediatrics,vanderbilt university school of medicine,monroe carell jr. children's hospital at vanderbilt,nashville,tn,united states,department of molecular physiology and biophysics,vanderbilt university school of medicine,nashville,tn,united states,vanderbilt kennedy center for human development,vanderbilt university,nashville,tn, United States
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Authors
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