Author:
Bamgbose Gbolahan,Bordet Guillaume,Lodhi Niraj,Tulin Alexei
Abstract
ABSTRACTPARP-1 is central to transcriptional regulation under both normal and stress conditions, with the governing mechanisms yet to be fully understood. Our biochemical and ChIP-seq-based analyses showed that PARP-1 binds specifically to active histone marks, particularly H4K20me1. We found that H4K20me1 plays a critical role in facilitating PARP-1 binding and the regulation of PARP-1-depenednt loci during both development and heat shock stress. Here we report that the sole H4K20 mono-methylase,pr-set7, andparp-1 Drosophilamutants undergo developmental arrest. RNA-seq analysis showed an absolute correlation between PR-SET7- and PARP-1-dependent loci expression, confirming co-regulation during developmental phases. PARP-1 and PR-SET7 are both essential for activatinghsp70and other heat shock genes during heat stress, with a notable increase of H4K20me1 at their gene body. Mutatingpr-set7disrupts monometylation of H4K20 along heat shock loci and abolish PARP-1 binding there. These data strongly suggest that H4 monometylation is a key triggering point in PARP-1 dependent processes in chromatin.
Publisher
Cold Spring Harbor Laboratory