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宫内造血细胞移植后免疫屏障的证据。

Evidence for an immune barrier after in utero hematopoietic-cell transplantation.

作者信息

Peranteau William H, Endo Masayuki, Adibe Obinna O, Flake Alan W

机构信息

Center for Fetal Research, Children's Hospital of Philadelphia, PA 19104, USA.

出版信息

Blood. 2007 Feb 1;109(3):1331-3. doi: 10.1182/blood-2006-04-018606. Epub 2006 Oct 5.

Abstract

The competence of the immune system of the developing fetus to act as a barrier to in utero hematopoietic-cell transplantation (IUHCT) has been a source of debate. Until now, comparisons of allogeneic and congenic engraftment have been inconclusive due to methodologic limitations resulting in minimal and inefficient engraftment. In this study, E14 fetal mice received transplants of either allogeneic or congenic bone marrow using a new intravascular technique that allows definitive administration of much higher doses of donor cells. Our results demonstrate that 100% of surviving recipients demonstrate engraftment at 1 week of age, but that 70% of allogeneic recipients lose engraftment by 1 month of age, and 80% ultimately fail to sustain long-term chimerism. In contrast, all congenic recipients maintain stable, long-term, multilineage chimerism. These results strongly support an immune barrier to allogeneic engraftment after IUHCT.

摘要

发育中的胎儿免疫系统作为子宫内造血细胞移植(IUHCT)屏障的能力一直是争论的焦点。到目前为止,由于方法学上的局限性导致植入极少且效率低下,同种异体和同基因植入的比较尚无定论。在本研究中,E14胎鼠采用一种新的血管内技术接受同种异体或同基因骨髓移植,该技术可确切给予更高剂量的供体细胞。我们的结果表明,100%存活的受体在1周龄时出现植入,但70%的同种异体受体在1月龄时失去植入,80%最终无法维持长期嵌合状态。相比之下,所有同基因受体均维持稳定的长期多谱系嵌合状态。这些结果有力地支持了IUHCT后同种异体植入存在免疫屏障。

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