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Genetic and regulatory contributions of the major histocompatibility complex to the developing cytolytic T lymphocyte repertoire.

作者信息

Sherman L A

出版信息

J Immunol. 1982 Apr;128(4):1849-53.

PMID:7061852
Abstract

The specificity repertoire of H-2Kb-specific CTL derived from 10- to 14-day-old neonates was examined. Analogous to the adult repertoire, the neonatal repertoire is composed of a large number of receptor specificities, each of which is represented at a low frequency, as well as a small number of highly recurrent specificities, which thereby serve as repertoire markers. The expression of most specificities appears to be independently regulated during development, resulting in the expression of a different set of recurrent specificities for neonates and adults within the same strain. The neonatal and adult repertoires were also compared with respect to the influence of the MHC on repertoire. Unlike adults, neonates of MHC different congenic strains (B10.D2 and B10.BR) have in common approximately half their recurrent specificities. Additionally, most parental specificities are expressed codominantly in neonatal F1 hybrids. These results may be interpreted as indicating either that 1) some, but not all, receptor genes demonstrate MHC-linked polymorphism and both parental alleles are expressed in F1 neonates, or 2) T receptor genes are nonpolymorphic in MHC congenic strains and the observed MHC-related repertoire differences are attributable to a positive selection mechanism. Since adults of these same strains do not display significant repertoire similarity, it is suggested that this increased repertoire divergence may be the result of encounters with environmental antigens in association with self-MHC antigens.

摘要

相似文献

1
Genetic and regulatory contributions of the major histocompatibility complex to the developing cytolytic T lymphocyte repertoire.
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引用本文的文献

1
Cytotoxic T-cell recognition of influenza-infected target cells varies in different H-2k mouse strains.在不同的H-2k小鼠品系中,细胞毒性T细胞对流感感染靶细胞的识别存在差异。
Immunogenetics. 1983;18(2):177-81. doi: 10.1007/BF00368548.
2
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J Exp Med. 1982 Jul 1;156(1):294-9. doi: 10.1084/jem.156.1.294.
3
Recognition specificities, development and possible biological function of natural killer cells in the mouse. II. Changes in NK recognition during ontogeny and ageing, and examination of role of environment in controlling the expressed recognition repertoire.
小鼠自然杀伤细胞的识别特异性、发育及可能的生物学功能。II. 个体发育和衰老过程中自然杀伤细胞识别的变化,以及环境在控制表达的识别库中的作用研究。
Immunology. 1984 Dec;53(4):731-43.
4
T-cell clones and T-cell receptors.T细胞克隆与T细胞受体。
Microbiol Rev. 1986 Mar;50(1):50-69. doi: 10.1128/mr.50.1.50-69.1986.