Macrophage Ontogeny: Implications for Host Defence, T-lymphocyte Differentiation, and the Acquisition of Self-tolerance

CHRISTOPHER Y. LU, EMIL R. UNANUE
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引用次数: 8

Abstract

It has become increasingly more apparent that la-bearing accessory cells are important in regulating the function of mature T lymphocytes as well as the maturation of immature T lymphocytes in the thymus. The experiments reviewed here have focused on the ontogeny of la-bearing macrophages in the peritoneal cavity, spleen, and thymus. In the former two sites, la-bearing macrophages appear late in ontogeny. This makes the neonate and fetus vulnerable to infection, but may also offer the immune system a critical mechanism for inducing self-tolerance. The delayed ontogenesis of la-bearing macrophages at these two sites is regulated by high concentrations of PGE2 as well as alpha-fetoprotein. On the other hand, la-bearing thymic macrophages are present early in ontogeny and may contribute to the expansion and maturation of appropriate T lymphocyte clones early in development.

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巨噬细胞个体发生:宿主防御、t淋巴细胞分化和获得自我耐受的意义
承载la的辅助细胞在调节胸腺成熟T淋巴细胞的功能以及未成熟T淋巴细胞的成熟中起着重要的作用,这一点越来越明显。本文综述的实验主要集中在腹腔、脾脏和胸腺中携带la的巨噬细胞的个体发生。在前两个部位,巨噬细胞在个体发育中出现较晚。这使得新生儿和胎儿容易受到感染,但也可能为免疫系统提供一个诱导自我耐受的关键机制。在这两个部位携带la的巨噬细胞的延迟个体形成是由高浓度的PGE2和甲胎蛋白调节的。另一方面,携带la的胸腺巨噬细胞在个体发育早期就存在,可能有助于发育早期适当T淋巴细胞克隆的扩张和成熟。
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