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辅助细胞可使纯化的胎儿肝脏干细胞在异基因受体中实现植入。

Facilitating cells enable engraftment of purified fetal liver stem cells in allogeneic recipients.

作者信息

Gaines B A, Colson Y L, Kaufman C L, Ildstad S

机构信息

Division of Cellular Therapeutics, Department of Surgery, University of Pittsburgh, PA 15261, USA.

出版信息

Exp Hematol. 1996 Jul;24(8):902-13.

PMID:8690049
Abstract

It has been reported that while stem cells purified from adult bone marrow engraft in syngeneic recipients, they fail to engraft in allogeneic recipients. We have recently shown that the addition of as few as 30,000 facilitating cells (CD8+/CD3+/CD45R+/Thy 1.2+/TCR-), a unique bone marrow-derived population that does not possess stem cell properties, results in the permanent engraftment of stem cells in a major histocompatibility complex (MHC)-disparate allogeneic host. It has been suggested that fetal hematopoietic tissue may be a source of stem cells with enhanced proliferative and self-renewal properties compared with adult bone marrow. We were interested, therefore, in whether fetal stem cells demonstrated a superior capacity to engraft in allogeneic recipients. In this study, we have examined the engraftment properties of mouse fetal liver cells in syngeneic and allogeneic recipients. Transplantation of unmodified fetal liver cells into allogeneic recipients results in stable multilineage chimerism with donor-specific tolerance, indicating that the pluripotent hematopoietic stem cell is present in fetal liver and is capable of engraftment in allogeneic adult recipients. Similarly, 2000 to 3000 sorted fetal liver stem cells (Sca+/c-kit+/Lin-) successfully reconstituted lethally irradiated syngeneic adults and adults differing only in minor histocompatibility antigens. Two thousand to 10,000 fetal stem cells failed to rescue lethally irradiated allogeneic recipients, but the addition of 30,000 MHC-matched purified facilitating cells to the fetal stem cell inoculum resulted in sustained engraftment with multilineage production. These results, which parallel our earlier work with stem cells derived from adult bone marrow, indicate that the pluripotent fetal stem cell behaves in a fashion similar to that of adult stem cells with regard to allogeneic transplantation.

摘要

据报道,从成年骨髓中纯化的干细胞能在同基因受体中植入,但在异基因受体中却无法植入。我们最近发现,添加低至30000个辅助细胞(CD8+/CD3+/CD45R+/Thy 1.2+/TCR-),这是一种独特的源自骨髓的细胞群体,不具备干细胞特性,却能使干细胞在主要组织相容性复合体(MHC)不相合的异基因宿主体内永久植入。有人提出,与成年骨髓相比,胎儿造血组织可能是具有更强增殖和自我更新特性的干细胞来源。因此,我们感兴趣的是胎儿干细胞在异基因受体中的植入能力是否更强。在本研究中,我们检测了小鼠胎儿肝细胞在同基因和异基因受体中的植入特性。将未修饰的胎儿肝细胞移植到异基因受体中会导致稳定的多谱系嵌合体形成,并产生供体特异性耐受,这表明多能造血干细胞存在于胎儿肝脏中,并且能够在异基因成年受体中植入。同样,2000至3000个分选的胎儿肝脏干细胞(Sca+/c-kit+/Lin-)成功地重建了经致死性照射的同基因成年小鼠以及仅在次要组织相容性抗原上不同的成年小鼠。2000至10000个胎儿干细胞未能挽救经致死性照射的异基因受体,但在胎儿干细胞接种物中添加30000个MHC匹配的纯化辅助细胞会导致多谱系产生的持续植入。这些结果与我们早期对成年骨髓来源干细胞的研究结果相似,表明在异基因移植方面,多能胎儿干细胞的行为方式与成年干细胞相似。

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