Small molecule compound induces chromatin de-condensation and facilitates induced pluripotent stern cell generation

Small molecule compound induces chromatin de-condensation and facilitates induced pluripotent stern cell generation

The revolutionary induced pturipotent stem celt (iPSC) technoLogy provides a new means for celt replacement therapies and drug screening. Small molecule compounds have been found extremely useful to improve the generation of iPSCs and understand the repro- gramming mechanism. Here we report the iden...

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Veröffentlicht in:分子细胞生物学报:英文版 2014 (5), p.409-420
1. Verfasser: Xiaoyuan Wei Yueting Chen Yongyu Xu YangZhan Ru Zhang Min Wang Qiuhong Hua Haifeng Gu Fajun Nan Xin Xie
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Sprache:eng
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凝聚
凯尔特人
多能干细胞
小分子化合物
异染色质
染色质结构
船尾
诱导
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container_title 分子细胞生物学报:英文版
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creator Xiaoyuan Wei Yueting Chen Yongyu Xu YangZhan Ru Zhang Min Wang Qiuhong Hua Haifeng Gu Fajun Nan Xin Xie
description The revolutionary induced pturipotent stem celt (iPSC) technoLogy provides a new means for celt replacement therapies and drug screening. Small molecule compounds have been found extremely useful to improve the generation of iPSCs and understand the repro- gramming mechanism. Here we report the identification of a novel chemical, CYT296, which improves OSKM-mediated induction of iPSCs for 〉10 folds and enables efficient reprogramming with only Oct4 in combination with other small molecules. The derived iPSCs are genuinely pluripotent and support the development oftwo 'All-iPSC' mice by tetraploid complementation. CYT296 profoundly impacts heterochromatin formation without affecting celt viability. MEFs treated with CYT296 exhibit de-condensed chromatin structure with markedly reduced loci containing heterochromatin protein 1α (HPIoL) and H3K9me3, which is very similar to the chromatin configuration in embryonic stem cells (ESCs). Given that an open chromatin structure serves as a hallmark of pLuripotency and has to be acquired to fulfill reprogramming, we propose that CYT296 might facilitate this process by disrupting condensed chromatin, thereby creating a more favorable environment for reprogramming. In agreement of this idea, shRNA targeting HP1α also promotes the generation of iPSCs. Thus current findings not only provide a novel chemical for efficient iPSC induction, but also suggest a new approach to regulate somatic cell reprogramming by targeting chromatin de-condensation with small molecules.
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subjects 凝聚
凯尔特人
多能干细胞
小分子化合物
异染色质
染色质结构
船尾
诱导
title Small molecule compound induces chromatin de-condensation and facilitates induced pluripotent stern cell generation
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