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PDGFD switches on stem cell endothelial commitment

Weisi Lu, Peipei Xu, Boxiong Deng, Jianing Zhang, Ying Zhan, Xianchai Lin, Xiangzhong Xu, Zhaoxia Xia, Xiaoxi Yang, Xiaoling Zeng, Lijuan Huang, Bingbing Xie, Chenghu Wang, Shasha Wang, Haiqing Kuang, Xianjing Han, Antonio Mora, Yihai Cao, Qin Jiang, Xuri Li

2022Angiogenesis10 citationsDOIOpen Access PDF

Abstract

The critical factors regulating stem cell endothelial commitment and renewal remain not well understood. Here, using loss- and gain-of-function assays together with bioinformatic analysis and multiple model systems, we show that PDGFD is an essential factor that switches on endothelial commitment of embryonic stem cells (ESCs). PDGFD genetic deletion or knockdown inhibits ESC differentiation into EC lineage and increases ESC self-renewal, and PDGFD overexpression activates ESC differentiation towards ECs. RNA sequencing reveals a critical requirement of PDGFD for the expression of vascular-differentiation related genes in ESCs. Importantly, PDGFD genetic deletion or knockdown increases ESC self-renewal and decreases blood vessel densities in both embryonic and neonatal mice and in teratomas. Mechanistically, we reveal that PDGFD fulfills this function via the MAPK/ERK pathway. Our findings provide new insight of PDGFD as a novel regulator of ESC fate determination, and suggest therapeutic implications of modulating PDGFD activity in stem cell therapy.

Topics & Concepts

Gene knockdownEmbryonic stem cellCell biologyBiologyEndothelial stem cellStem cellMAPK/ERK pathwayAngiogenesisRegulatorCellular differentiationCell fate determinationCancer researchGeneSignal transductionGeneticsTranscription factorIn vitroSingle-cell and spatial transcriptomicsCancer Genomics and DiagnosticsEpigenetics and DNA Methylation
PDGFD switches on stem cell endothelial commitment | Litcius