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   Human Oocyte-Derived Methylation Differences Persist in the Placenta Revealing Widespread Transient Imprinting  
   
نویسنده sanchez-delgado m. ,court f. ,vidal e. ,medrano j. ,monteagudo-sánchez a. ,martin-trujillo a. ,tayama c. ,iglesias-platas i. ,kondova i. ,bontrop r. ,poo-llanillo m.e. ,marques-bonet t. ,nakabayashi k. ,simón c. ,monk d.
منبع plos genetics - 2016 - دوره : 12 - شماره : 11
چکیده    Thousands of regions in gametes have opposing methylation profiles that are largely resolved during the post-fertilization epigenetic reprogramming. however some specific sequences associated with imprinted loci survive this demethylation process. here we present the data describing the fate of germline-derived methylation in humans. with the exception of a few known paternally methylated germline differentially methylated regions (dmrs) associated with known imprinted domains,we demonstrate that sperm-derived methylation is reprogrammed by the blastocyst stage of development. in contrast a large number of oocyte-derived methylation differences survive to the blastocyst stage and uniquely persist as transiently methylated dmrs only in the placenta. furthermore,we demonstrate that this phenomenon is exclusive to primates,since no placenta-specific maternal methylation was observed in mouse. utilizing single cell rna-seq datasets from human preimplantation embryos we show that following embryonic genome activation the maternally methylated transient dmrs can orchestrate imprinted expression. however despite showing widespread imprinted expression of genes in placenta,allele-specific transcriptional profiling revealed that not all placenta-specific dmrs coordinate imprinted expression and that this maternal methylation may be absent in a minority of samples,suggestive of polymorphic imprinted methylation. © 2016 sanchez-delgado et al.
آدرس imprinting and cancer group,cancer epigenetic and biology program,institut d’investigació biomedica de bellvitge,hospital duran i reynals,barcelona, Spain, laboratoire gred,cnrs,umr6293,clermont-ferrand, France, centre for genomic regulation (crg),the barcelona institute of science and technology,dr.barcelona,universitat pompeu fabra (upf),aiguader 88,barcelona, Spain, fundación ivi-instituto universitario ivi- incliva,department of obs/gyn,valenica university,valencia, Spain, imprinting and cancer group,cancer epigenetic and biology program,institut d’investigació biomedica de bellvitge,hospital duran i reynals,barcelona, Spain, imprinting and cancer group,cancer epigenetic and biology program,institut d’investigació biomedica de bellvitge,hospital duran i reynals,barcelona, Spain, department of maternal-fetal biology,national research institute for child health and development,tokyo, Japan, neonatal service,hospital sant joan de déu,bcnatal hospital sant joan de déu i clínic,universitat de barcelona,barcelona, Spain, biomedical primate research center (bprc),rijswijk, Netherlands, biomedical primate research center (bprc),rijswijk, Netherlands, fundación ivi-instituto universitario ivi- incliva,department of obs/gyn,valenica university,valencia, Spain, institute of evolutionary biology (upf-csic),prbb,barcelona,spain,catalan institute of research and advanced studies,(icrea),passeig de lluís companys,barcelona,spain,centro nacional de analisis genomico (crg-cnag),barcelona, Spain, department of maternal-fetal biology,national research institute for child health and development,tokyo, Japan, fundación ivi-instituto universitario ivi- incliva,department of obs/gyn,valenica university,valencia, Spain, imprinting and cancer group,cancer epigenetic and biology program,institut d’investigació biomedica de bellvitge,hospital duran i reynals,barcelona, Spain
 
     
   
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