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针对免疫显性次要组织相容性抗原肽的优先细胞溶解性T淋巴细胞反应。

The preferential cytolytic T lymphocyte response to immunodominant minor histocompatibility antigen peptides.

作者信息

Nevala W K, Wettstein P J

机构信息

Department of Surgery, The Mayo Foundation, Rochester, Minnesota 55905, USA.

出版信息

Transplantation. 1996 Jul 27;62(2):283-91. doi: 10.1097/00007890-199607270-00022.

Abstract

C57BL/6 mice preferentially generate cytolytic T lymphocytes (CTL) to a limited number of immunodominant minor antigens and associated immunogenic peptides when primed with H2-matched Balb.B spleen cells despite multiple minor histocompatibility (H) antigen differences. We have examined the complexity of dominant H antigens recognized by these CTLs to estimate the number of peptides associated with single antigens. Peptides eluted from Kb molecules of lymphoblasts from Balb.B and CXB recombinant inbred (RI) strains were tested for sensitization of RMA-S cells for lysis by short-term C57BL/6 CTL lines specific for Balb.B and CXB strains. Anti-Balb.B CTLs recognized four Kb-bound peptides; subsets of these peptides were recognized by anti-CXB CTLs when tested with peptides from the respective CXB strains. Single peptides segregated independently among the CXB strains, confirming that single peptides were encoded by independently segregating alleles. These peptides were expressed in diverse inbred mouse strains and were recognized preferentially by C57BL/6 CTLs stimulated by different inbred mouse strains. This set of peptides was subclassified by their capacity to sensitize targets when presented in unfractionated mixtures of Kb-bound peptides. The peptide associated with the previously classified dominant CTT-2 antigen was the only peptide to strongly sensitize RMA-S cells for lysis under these conditions. These results suggest that dominant peptides have a wide strain distribution and may have a distinct advantage over dominated peptides in binding to class I molecules and/or in presentation to CTLs.

摘要

当用H2匹配的Balb.B脾细胞对C57BL/6小鼠进行初次免疫时,尽管存在多种次要组织相容性(H)抗原差异,但它们优先针对有限数量的免疫显性次要抗原和相关免疫原性肽产生细胞毒性T淋巴细胞(CTL)。我们已经研究了这些CTL识别的显性H抗原的复杂性,以估计与单一抗原相关的肽的数量。对从Balb.B和CXB重组近交(RI)品系的淋巴母细胞的Kb分子上洗脱的肽进行测试,以检测RMA-S细胞被针对Balb.B和CXB品系的短期C57BL/6 CTL系裂解的致敏情况。抗Balb.B CTL识别四种Kb结合肽;当用来自各自CXB品系的肽进行测试时,这些肽的亚群被抗CXB CTL识别。单一肽在CXB品系中独立分离,证实单一肽由独立分离的等位基因编码。这些肽在多种近交小鼠品系中表达,并被不同近交小鼠品系刺激的C57BL/6 CTL优先识别。当以Kb结合肽的未分级混合物形式呈现时,根据它们使靶细胞致敏的能力对这组肽进行了亚分类。在这些条件下,与先前分类的显性CTT-2抗原相关的肽是唯一能强烈使RMA-S细胞致敏以进行裂解的肽。这些结果表明,显性肽具有广泛的品系分布,并且在与I类分子结合和/或呈递给CTL方面可能比被主导的肽具有明显优势。

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