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巨核细胞促进骨髓放射损伤后小鼠成骨祖细胞龛的扩增和干细胞植入。

Megakaryocytes promote murine osteoblastic HSC niche expansion and stem cell engraftment after radioablative conditioning.

机构信息

Division of Oncology, Children’s Hospital of Philadelphia, Philadelphia, PA 19104. , USA.

出版信息

Blood. 2013 Jun 27;121(26):5238-49. doi: 10.1182/blood-2012-10-463414. Epub 2013 May 10.

Abstract

Successful hematopoietic stem cell (HSC) transplantation requires donor HSC engraftment within specialized bone marrow microenvironments known as HSC niches. We have previously reported a profound remodeling of the endosteal osteoblastic HSC niche after total body irradiation (TBI), defined as relocalization of surviving megakaryocytes to the niche site and marked expansion of endosteal osteoblasts. We now demonstrate that host megakaryocytes function critically in expansion of the endosteal niche after preparative radioablation and in the engraftment of donor HSC. We show that TBI-induced migration of megakaryocytes to the endosteal niche depends on thrombopoietin signaling through the c-MPL receptor on megakaryocytes, as well as CD41 integrin-mediated adhesion. Moreover, niche osteoblast proliferation post-TBI required megakaryocyte-secreted platelet-derived growth factor-BB. Furthermore, blockade of c-MPL-dependent megakaryocyte migration and function after TBI resulted in a significant decrease in donor HSC engraftment in primary and competitive secondary transplantation assays. Finally, we administered thrombopoietin to mice beginning 5 days before marrow radioablation and ending 24 hours before transplant to enhance megakaryocyte function post-TBI, and found that this strategy significantly enhanced donor HSC engraftment, providing a rationale for improving hematopoietic recovery and perhaps overall outcome after clinical HSC transplantation.

摘要

成功的造血干细胞(HSC)移植需要供体 HSC 在内皮细胞龛等专门的骨髓微环境中植入。我们之前曾报道过全身照射(TBI)后骨内膜成骨细胞 HSC 龛位会发生深刻的重塑,表现为存活的巨核细胞向龛位的重新定位和骨内膜成骨细胞的显著扩张。现在我们证明,宿主巨核细胞在放射性消融准备后内皮龛位的扩张和供体 HSC 的植入中起着关键作用。我们发现 TBI 诱导的巨核细胞向骨内膜龛位的迁移依赖于巨核细胞上的 c-MPL 受体的血小板生成素信号,以及 CD41 整合素介导的黏附。此外,TBI 后龛位成骨细胞的增殖需要巨核细胞分泌的血小板衍生生长因子-BB。此外,TBI 后阻断 c-MPL 依赖性巨核细胞迁移和功能会导致供体 HSC 在原发性和竞争性二次移植试验中的植入明显减少。最后,我们从骨髓放射性消融前 5 天开始并在移植前 24 小时结束给小鼠施用血小板生成素,以增强 TBI 后巨核细胞的功能,发现该策略显著增强了供体 HSC 的植入,为改善造血恢复并可能改善临床 HSC 移植后的整体结果提供了依据。

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