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Frequency analysis of cytotoxic T lymphocyte precursors in chimeric mice. Evidence for intrathymic maturation of clonally distinct self- major histocompatibility complex- and allo-major histocompatiblilty complex-restricted virus-specific T cells

机译:嵌合小鼠中细胞毒性T淋巴细胞前体的频率分析。克隆不同的自体主要组织相容性复合物和同种异体主要组织相容性复合物限制的病毒特异性T细胞胸腺内成熟的证据

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摘要

To study whether the thymic major histocompatibility complex (MHC) imposes a constraint on the receptor repertoire of maturating cytotoxic T lymphocyte (CTL) precursors, the restriction phenotypes of virus- specific CTL of MHC-compatible and of MHC-incompatible thymus- and bone marrow-grafted (A X B)F1 chimeric mice were compared. Dependent on the mode of in vitro sensitization, thymocytes or splenocytes of both types of chimeric mice generated Sendai virus-specific, self-MHC-or allo-MHC- restricted CTL. By applying the limiting-dilution technique, the CTL- precursor (CTL-P) frequencies of self-MHC-restricted and allo-MHC- restricted virus-specific T cells as well as of alloreactive T cells were determined. The data obtained revealed that independent of MHC differences between thymus and bone marrow, the frequencies of self-MHC- restricted and allo-MHC-restricted CTL-P were comparable, and in the same older of magnitude as those previously determined in conventionally reared mice. Self-MHC-restricted, virus-specific CTL-P were in a three- to fivefold excess over allo-MHC-restricted CTL-P. A segregation analysis revealed that clonally distinct CTL-P give rise to either self-restricted or allo-MHC-restricted, virus-specific CTL. Both sets were found not only in the spleen, but also in the thymus of chimeric mice, formally demonstrating the intrathymic differentiation pathway of self-MHC as well of allo-MHC-restricted CTL-P. These data reveal no major constraint of the thymic MHC on the capacity of T cells to recognize viral antigens either in the context of self-MHC or of allogeneic MHC products.
机译:若要研究胸腺主要组织相容性复合物(MHC)是否对成熟的细胞毒性T淋巴细胞(CTL)前体的受体组成部分施加限制,MHC兼容和MHC不兼容的胸腺和骨髓的病毒特异性CTL的限制性表型比较了移植的(AXB)F1嵌合小鼠。取决于体外致敏模式,两种嵌合小鼠的胸腺细胞或脾细胞均产生仙台病毒特异性,自身MHC或同种MHC限制的CTL。通过应用限制性稀释技术,确定了自身MHC限制性和同种MHC限制性病毒特异性T细胞以及同种反应性T细胞的CTL前体(CTL-P)频率。获得的数据表明,与胸腺和骨髓之间的MHC差异无关,自我MHC限制和异源MHC限制的CTL-P的频率是可比的,并且与以前在常规饲养的小鼠中确定的频率相同。自我MHC限制的,病毒特异性的CTL-P比异源MHC限制的CTL-P高出三到五倍。分离分析显示,克隆不同的CTL-P产生了自我限制或同种MHC限制的病毒特异性CTL。两组均不仅在脾脏中发现,而且在嵌合小鼠的胸腺中发现,这正式证明了自我MHC以及异源MHC限制的CTL-P的胸腺内分化途径。这些数据显示,在自身MHC或同种异体MHC产物的情况下,胸腺MHC对T细胞识别病毒抗原的能力没有重大限制。

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