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Breanna Perreault and Xiao Liu D145 Presentation Background : Primordial Germ Cells - PGCs: cells that give rise to gametes - Genome-wide DNA methylation reprogramming occurs in mouse PGCs What is Epigenetics? Changes in gene expression caused by mechanisms other than changes in the DNA sequence WHY is it important? Epigenetic Terminology - CpG Islands - Cytosine that is methylated and is almost always located next to a guanine nucleotide - promoter Epigenetic Terminology - Imprinting - epigenetic process that involves DNA methylation and histone methylation - transgenerational sex-dependent inheritance pattern - From dad -> reprogrammed in female offsprings-> to maternal pattern - From mom -> reprogrammed in male offsprings-> to paternal pattern Main Method Used -Bisulfite Sequencing (BS seq)Protection treatment: methylated cytosine do not get converted to uracil - Steps: 1. DNA sonicated (300-500bp) 2. DNA adaptor ligated 3. DNA treated with sodium bisulfite 4. Amplify DNA (PCR) 5. Size selection: gel extraction for 200-250bp DNA Main findings 1. 2 main phases of demethylation in PGCs 2. Combination of passive + active maintenance of methylation during global demethylation 3. Global erasure does not mean indiscriminate transcription- some other mechanism controls this 4. VECs- potential carrier of short term transgenerational epigenetic inheritance by sustained methylation 5. Primordial germ cell development and methylation linked with pluripotency Timeline of demethylation in PGCs -E6.5: ~40 PGCs arise in the epiblast -E9.5: ~200 PGCs migrate through hindgut endoderm to reach the gonads by E10.5-11.5 -E13.5 and E16.5 males and females were profiled separately 2 main phases of demethylation: 1. Early phase (Global): E6.5 --networks related to pluripotency are activated -affect promoters, CpG islands (CGIs), introns, exons, intergenic sequences -retrotransposons (LINEs, SINEs) Temporal Heatmap of Methylation 2. Late phase: E10.5 -DMR of imprinted genes -CpG Islands found on X chromosomes -CpG Islands associated with germline specific genes DMRs of Imprinted Genes Imprinting not propagated by CpG methylation CpG Islands on X chromosome Suggested Association with X-Chromosome Inactivation CpGs associated with Germline Specific Genes Reprogramming the Transcriptional Landscape of PGCs - RNA Seq -figures -analysis Methylated Regions IAPs- (Intracisternal A-Particles) -retrotransposons -can interrupt or enhance gene expression VECs- (Variably Erased CpGIs) - occurs in male and female - not related to imprinted - Act as short term transgenerational carriers Temporal Heatmap of Methylation CGI Containing Promoter Intergenic Region Non-CGI Promoter IAP Non-Promoter CGI LINE1 Exon Maternal DMR Intron Paternal DMR IAP vs LINE Methylation Level CPGI Methylation Decreases with IAP Proximity DETAIL Whole Genome GCI Promoter Demethylation Note Male and Female Difference in VECs (13.5) Global Demethylation mechanism Passive: DNA methyltransferases Dnmt1+ Np95 Active: DNA demethylase Tet1 Hairpin Bisulfite Seq Alignable sequence data Active and Passive Demethylation Performed on LINEs, however this is global demethylation trend Predominantly Passive Stagnant Transcriptional Profile Comparison LINE transcription Conclusions: 1. Global DNA methylation- passive + active demethylation 2. 2 main phases of demethylation in PGCs 3. DMR 4. X chromosome 5. Germline specific 6. Global erasure does not mean indiscriminate transcription 7. Lines and transcription 8. Pluripotency and Meiosis 9. IAP 10. VECs- carrier of short term transgenerational epigenetic inheritance Critiques Couldn’t tell exactly mechanism of Global Demethylation Too much detail to make a coherent point out of the study when not an expert in the field Mentioned differences between male and female, but did not investigate why Recommended Readings http://www.nature.com/nrg/journal/v17/n10/pdf/nrg.2016.88.pdf https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3183171/ Questions?