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Regulation of MLL/COMPASS stability through its proteolytic cleavage by taspase1 as a possible approach for clinical therapy of leukemia.

Genes Dev.. 2019-01; 
ZhaoZibo, WangLu, VolkAndrew G, BirchNoah W, StoltzKristen L, BartomElizabeth T, MarshallStacy A, RendlemanEmily J, NestlerCarson M, ShilatiJoseph, SchiltzGary E, CrispinoJohn D, Shilatifar
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摘要

Chromosomal translocations of the Mixed-lineage leukemia 1 () gene generate MLL chimeras that drive the pathogenesis of acute myeloid and lymphoid leukemia. The untranslocated MLL1 is a substrate for proteolytic cleavage by the endopeptidase threonine aspartase 1 (taspase1); however, the biological significance of MLL1 cleavage by this endopeptidase remains unclear. Here, we demonstrate that taspase1-dependent cleavage of MLL1 results in the destabilization of MLL. Upon loss of taspase1, MLL1 association with chromatin is markedly increased due to the stabilization of its unprocessed version, and this stabilization of the uncleaved MLL1 can result in the displacement of MLL chimeras from chromatin in le... More

关键词

CKII,CX-4945,KMT2A,MLL1,TASP1,protein stability,regulation of gene expression,tasp