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高剂量的纯化干细胞可使同基因和异基因宿主的造血功能早期恢复。

High doses of purified stem cells cause early hematopoietic recovery in syngeneic and allogeneic hosts.

作者信息

Uchida N, Tsukamoto A, He D, Friera A M, Scollay R, Weissman I L

机构信息

SyStemix, Incorporated, Palo Alto, California 94304, USA.

出版信息

J Clin Invest. 1998 Mar 1;101(5):961-6. doi: 10.1172/JCI1681.

Abstract

In humans, autologous transplants derived from bone marrow (BM) usually engraft more slowly than transplants derived from mobilized peripheral blood. Allogeneic BM transplants show a further delay in engraftment and have an apparent requirement for donor T cells to facilitate engraftment. In mice, Thy-1.1(lo)Lin-/loSca-1+ hematopoietic stem cells (HSCs) are the principal population in BM which is responsible for engraftment in syngeneic hosts at radioprotective doses, and higher doses of HSCs can radioprotect an allogeneic host in the absence of donor T cells. Using the mouse as a preclinical model, we wished to test to what extent engraftment kinetics was a function of HSC content, and whether at high doses of c-Kit+Thy-1.1(lo)Lin-/loSca-1+ (KTLS) cells rapid allogeneic engraftment could also be achieved. Here we demonstrate that engraftment kinetics varied greatly over the range of KTLS doses tested (100-10,000 cells), with the most rapid engraftment being obtained with a dose of 5,000 or more syngeneic cells. Mobilized splenic KTLS cells and the rhodamine 123(lo) subset of KTLS cells were also able to engraft rapidly. Higher doses of allogeneic cells were needed to produce equivalent engraftment kinetics. This suggests that in mice even fully allogeneic barriers can be traversed with high doses of HSCs, and that in humans it may be possible to obtain rapid engraftment in an allogeneic context with clinically achievable doses of purified HSCs.

摘要

在人类中,源自骨髓(BM)的自体移植通常比源自动员外周血的移植植入速度更慢。同种异体BM移植的植入会进一步延迟,并且明显需要供体T细胞来促进植入。在小鼠中,Thy-1.1(lo)Lin-/loSca-1+造血干细胞(HSCs)是BM中的主要细胞群,在辐射防护剂量下负责同基因宿主中的植入,更高剂量的HSCs在没有供体T细胞的情况下可以对同种异体宿主起到辐射防护作用。以小鼠作为临床前模型,我们希望测试植入动力学在多大程度上是HSC含量的函数,以及在高剂量的c-Kit+Thy-1.1(lo)Lin-/loSca-1+(KTLS)细胞时是否也能实现快速的同种异体植入。在这里,我们证明在所测试的KTLS剂量范围(100 - 10,000个细胞)内,植入动力学有很大差异,使用5000个或更多同基因细胞的剂量可获得最快的植入速度。动员的脾KTLS细胞和KTLS细胞的罗丹明123(lo)亚群也能够快速植入。需要更高剂量的同种异体细胞才能产生等效的植入动力学。这表明在小鼠中,即使是完全同种异体的屏障,高剂量的HSCs也可以跨越,并且在人类中,使用临床可实现剂量的纯化HSCs在同种异体情况下可能获得快速植入。

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