Immortalization of Erythroblasts by c-MYC and BCL-XL Enables Large-Scale Erythrocyte Production from Human Pluripotent Stem Cells

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• 作者：Sho-ichi Hirose ; Naoya Takayama ; Sou Nakamura ; Kazumichi Nagasawa ; Kiyosumi Ochi ; Shinji Hirata ; Satoshi Yamazaki ; Tomoyuki Yamaguchi ; Makoto Otsu ; Shinya Sano ; Nobuyasu Takahashi ; Akira Sawaguchi ; Mamoru Ito ; Takashi Kato ; Hiromitsu Nakauchi ; Koji Eto
• 刊名：Stem Cell Reports
• 出版年：17 December, 2013
• 年：2013
• 卷：1
• 期：6
• 页码：499-508
• 全文大小：2759 K

文摘

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Summary

The lack of knowledge about the mechanism of erythrocyte biogenesis through self-replication makes the in聽vitro generation of large quantities of cells difficult. We show that transduction of c-MYC and BCL-XL into multipotent hematopoietic progenitor cells derived from pluripotent stem cells and gene overexpression enable sustained exponential self-replication of glycophorin A⁺ erythroblasts, which we term immortalized erythrocyte progenitor cells (imERYPCs). In an inducible expression system, turning off the overexpression of c-MYC and BCL-XL enabled imERYPCs to mature with chromatin condensation and reduced cell size, hemoglobin synthesis, downregulation of GCN5, upregulation of GATA1, and endogenous BCL-XL and RAF1, all of which appeared to recapitulate normal erythropoiesis. imERYPCs mostly displayed fetal-type hemoglobin and normal oxygen dissociation in聽vitro and circulation in immunodeficient mice following transfusion. Using critical factors to induce imERYPCs provides a model of erythrocyte biogenesis that could potentially contribute to a stable supply of erythrocytes for donor-independent transfusion.