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题名

Inhibition of LSD1 promotes the differentiation of human induced pluripotent stem cells into insulin-producing cells

作者
通讯作者Li,Fu Rong
发表日期
2020-05-19
DOI
发表期刊
ISSN
1757-6512
EISSN
1757-6512
卷号11期号:1
摘要

Background: Human induced pluripotent stem cells (hiPSCs) represent a potentially unlimited source of pancreatic endocrine lineage cells. Although insulin-producing β cells derived from hiPSCs have been successfully induced, much work remains to be done to achieve mature β cells. Lysine-specific demethylase 1 (LSD1) plays an important role in the regulation of hiPSC self-renewal and differentiation. We propose a new strategy to acquire insulin-producing cells (IPCs) from hiPSCs by knocking down LSD1. Methods: Knockdown of LSD1 in hiPSCs with five shRNA. Assessment of the effects of shRNA on hiPSC proliferation, cell cycle, and apoptosis. Using knockdown hiPSCs with 31.33% LSD1 activity, we achieved a four-step differentiation into IPCs and test its differentiation efficiency, morphology, and marker genes and proteins. We implanted the IPCs into the renal subcapsular of SCID-Beige diabetic mice to evaluate the hypoglycemic effect in vivo. We tested LSD1 and HDAC1 whether they are present in the CoREST complex through IP-WB, and analyzed LSD1, CoREST, HDAC1, H3K4me2/me3, and H3K27me3 protein expression before and after knockdown of LSD1. Results: Differentiated hiPSCs were 38.32% ± 3.54% insulin-positive cells and released insulin/C-peptide in response to glucose stimulus in a manner comparable to adult human islets. Most of the IPCs co-expressed mature β cell-specific markers. When transplanted under the left renal capsule of SCID-Beige diabetic mice, these IPCs reversed hyperglycemia, leading to a significant increase in the definitive endoderm cells. IP-WB results showed that LSD1, HDAC1, and CoREST formed a complex in hiPSCs. Chip-PCR results showed that LSD1, HDAC1, and CoREST were enriched in the same district during the SOX17 and FOXA2 promoter region. Inhibition of LSD1 would not affect the level of CoREST but decreased the HDAC1 expressions. The H3K4me2/me3 and H3K9act level of SOX17 and FOXA2 promoter region increased after inhibited of LSD1, and promoted transcriptional activation. The H3K4me2/me3 and H3K9act level of OCT4 and SOX2 promoter region decreased with the transcriptional repressed. Conclusions: LSD1 regulated histone methylation and acetylation in promoter regions of pluripotent or endodermal genes. Our results suggest a highly efficient approach to producing IPCs from hiPSCs.

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相关链接[Scopus记录]
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语种
英语
学校署名
其他
资助项目
National Natural Science Foundation of China[81670702][81700683] ; Natural Science Foundation of Guangdong[2017A030310646] ; Science and Technology Project of Shenzhen[GJHZ20180413181702008][JCYJ20170307100 154602][JCYJ2016031115823245]
WOS研究方向
Cell Biology ; Research & Experimental Medicine
WOS类目
Cell & Tissue Engineering ; Cell Biology ; Medicine, Research & Experimental
WOS记录号
WOS:000536674900006
出版者
Scopus记录号
2-s2.0-85084965180
来源库
Scopus
引用统计
被引频次[WOS]:4
成果类型期刊论文
条目标识符http://sustech.caswiz.com/handle/2SGJ60CL/138145
专题生命科学学院_生物系
生命科学学院
作者单位
1.Translational Medicine Collaborative Innovation Center,Second Clinical Medical College,Shenzhen People's Hospital,Ji'Nan University,Shenzhen,1017 Dongmen North Road,518020,China
2.Guangdong Engineering Technology Research Center of Stem Cell and Cell Therapy,Shenzhen,518020,China
3.Shenzhen Cell Therapy Public Service Platform,Shenzhen,518020,China
4.Department of Biology,Southern University of Science and Technology,Shenzhen,518055,China
推荐引用方式
GB/T 7714
Yang,Xiao Fei,Zhou,Shu Yan,Wang,Ce,et al. Inhibition of LSD1 promotes the differentiation of human induced pluripotent stem cells into insulin-producing cells[J]. Stem Cell Research & Therapy,2020,11(1).
APA
Yang,Xiao Fei.,Zhou,Shu Yan.,Wang,Ce.,Huang,Wei.,Li,Ning.,...&Li,Fu Rong.(2020).Inhibition of LSD1 promotes the differentiation of human induced pluripotent stem cells into insulin-producing cells.Stem Cell Research & Therapy,11(1).
MLA
Yang,Xiao Fei,et al."Inhibition of LSD1 promotes the differentiation of human induced pluripotent stem cells into insulin-producing cells".Stem Cell Research & Therapy 11.1(2020).
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