Reduced Levels of Lagging Strand Polymerases Shape Stem Cell Chromatin

Author:

Snedeker Jonathan,Davis Brendon E. M.,Ranjan Rajesh,Wooten MatthewORCID,Blundon Joshua,Chen XinORCID

Abstract

AbstractStem cells display asymmetric histone inheritance while non-stem progenitor cells exhibit symmetric patterns in theDrosophilamale germline lineage. Here, we report that components involved in lagging strand synthesis, such as DNA polymerase α and δ (Polα and Polδ), have significantly reduced levels in stem cells compared to progenitor cells. Compromising Polα genetically induces the replication-coupled histone incorporation pattern in progenitor cells to be indistinguishable from that in stem cells, which can be recapitulated using a Polα inhibitor in a concentration-dependent manner. Furthermore, stem cell-derived chromatin fibers display a higher degree of old histone recycling by the leading strand compared to progenitor cell-derived chromatin fibers. However, upon reducing Polα levels in progenitor cells, the chromatin fibers now display asymmetric old histone recycling just like GSC-derived fibers. The oldversusnew histone asymmetry is comparable between stem cells and progenitor cells at both S-phase and M-phase. Together, these results indicate that developmentally programmed expression of key DNA replication components is important to shape stem cell chromatin. Furthermore, manipulating one crucial DNA replication component can induce replication-coupled histone dynamics in non-stem cells in a manner similar to that in stem cells.One Sentence SummaryDelayed lagging strand synthesis regulates asymmetric histone incorporation.

Publisher

Cold Spring Harbor Laboratory

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