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胸腺细胞可能在没有骨髓祖细胞任何输入的情况下持续分化。

Thymocytes may persist and differentiate without any input from bone marrow progenitors.

机构信息

Institut National de la Santé et de la Recherche Médicale, Unit 1020, 75015 Paris, France.

出版信息

J Exp Med. 2012 Jul 30;209(8):1401-8. doi: 10.1084/jem.20120845. Epub 2012 Jul 9.

Abstract

Thymus transplants can correct deficiencies of the thymus epithelium caused by the complete DiGeorge syndrome or FOXN1 mutations. However, thymus transplants were never used to correct T cell-intrinsic deficiencies because it is generally believed that thymocytes have short intrinsic lifespans. This notion is based on thymus transplantation experiments where it was shown that thymus-resident cells were rapidly replaced by progenitors originating in the bone marrow. In contrast, here we show that neonatal thymi transplanted into interleukin 7 receptor-deficient hosts harbor populations with extensive capacity to self-renew, and maintain continuous thymocyte generation and export. These thymus transplants reconstitute the full diversity of peripheral T cell repertoires one month after surgery, which is the earliest time point studied. Moreover, transplantation experiments performed across major histocompatibility barriers show that allogeneic transplanted thymi are not rejected, and allogeneic cells do not induce graft-versus-host disease; transplants induced partial or total protection to infection. These results challenge the current dogma that thymocytes cannot self-renew, and indicate a potential use of neonatal thymus transplants to correct T cell-intrinsic deficiencies. Finally, as found with mature T cells, they show that thymocyte survival is determined by the competition between incoming progenitors and resident cells.

摘要

胸腺移植可以纠正由于完全 DiGeorge 综合征或 FOXN1 突变引起的胸腺上皮细胞的缺陷。然而,胸腺移植从未用于纠正 T 细胞内在缺陷,因为人们普遍认为胸腺细胞的固有寿命很短。这种观点基于胸腺移植实验,该实验表明,胸腺驻留细胞被起源于骨髓的祖细胞迅速取代。相比之下,在这里我们表明,移植到白细胞介素 7 受体缺陷宿主中的新生胸腺含有具有广泛自我更新能力的群体,并维持持续的胸腺细胞生成和输出。这些胸腺移植在手术后一个月重建了外周 T 细胞库的全部多样性,这是研究的最早时间点。此外,在主要组织相容性屏障上进行的移植实验表明,同种异体移植的胸腺不会被排斥,同种异体细胞不会引起移植物抗宿主病;移植诱导了部分或完全对感染的保护。这些结果挑战了胸腺细胞不能自我更新的现行教条,并表明新生儿胸腺移植有潜力纠正 T 细胞内在缺陷。最后,与成熟 T 细胞一样,它们表明胸腺细胞的存活取决于进入的祖细胞和驻留细胞之间的竞争。

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