Hypoimmunogenic human pluripotent stem cells are valid cell sources for cell therapeutics with normal self-renewal and multilineage differentiation capacity

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作者
Yifan Chen
Yanjie Zhou
Zhongshu Zhou
Yujiang Fang
Lin Ma
Xiaoqing Zhang
Jie Xiong
Ling Liu
机构
[1] Tongji University,Translational Medical Center for Stem Cell Therapy, Shanghai East Hospital, School of Medicine
[2] Orthopaedic Department of Tongji Hospital,Key Laboratory of Spine and Spinal Cord Injury Repair and Regeneration of Ministry of Education
[3] Shanghai Institute of Stem Cell Research and Clinical Translation,Key Laboratory of Neuroregeneration of Shanghai Universities, School of Medicine
[4] Tongji University,Clinical Center for Brain and Spinal Cord Research
[5] Tongji University,Tsingtao Advanced Research Institute
[6] Tongji University,undefined
来源
Stem Cell Research & Therapy | / 14卷
关键词
Hypoimmunogenic hPSCs; Self-renewal; Multilineage differentiation; Functional maturity;
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摘要
Hypoimmunogenic human pluripotent stem cells (hPSCs) are expected to serve as an unlimited cell source for generating universally compatible “off-the-shelf” cell grafts. However, whether the engineered hypoimmunogenic hPSCs still preserve their advantages of unlimited self-renewal and multilineage differentiation to yield functional tissue cells remains unclear. Here, we systematically studied the self-renewal and differentiation potency of three types of hypoimmunogenic hPSCs, established through the biallelic lesion of B2M gene to remove all surface expression of classical and nonclassical HLA class I molecules (B2Mnull), biallelic homologous recombination of nonclassical HLA-G1 to the B2M loci to knockout B2M while expressing membrane-bound β2m-HLA-G1 fusion proteins (B2MmHLAG), and ectopic expression of soluble and secreted β2m-HLA-G5 fusion proteins in B2MmHLAG hPSCs (B2Mm/sHLAG) in the most widely used WA09 human embryonic stem cells. Our results showed that hypoimmunogenic hPSCs with variable expression patterns of HLA molecules and immune compromising spectrums retained their normal self-renewal capacity and three-germ-layer differentiation potency. More importantly, as exemplified by neurons, cardiomyocytes and hepatocytes, hypoimmunogenic hPSC-derived tissue cells were fully functional as of their morphology, electrophysiological properties, macromolecule transportation and metabolic regulation. Our findings thus indicate that engineered hypoimmunogenic hPSCs hold great promise of serving as an unlimited universal cell source for cell therapeutics.
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