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由Ld限制的肿瘤肽特异性细胞毒性T淋巴细胞克隆产生的偏向性T细胞受体使用情况。

Biased T cell receptor usage by Ld-restricted, tum- peptide-specific cytotoxic T lymphocyte clones.

作者信息

Solheim J C, Alexander-Miller M A, Martinko J M, Connolly J M

机构信息

Department of Microbiology, Southern Illinois University, Carbondale 62901.

出版信息

J Immunol. 1993 Feb 1;150(3):800-11.

PMID:8380825
Abstract

We have investigated the TCR gene usage in a panel of H-2Ld-restricted, tum- peptide-specific CTL clones. These clones possess identical MHC restriction and peptide specificity, yet they vary dramatically in the amount of peptide required to sensitize targets for recognition. We previously demonstrated a precise quantitative correlation between the determinant density requirement of a given clone and the CD8 dependency. In this study we sequenced polymerase chain reaction copies of the TCR mRNA used by these clones, not only to correlate TCR structure with recognition of a specific class I/peptide complex, but also to determine if the functional affinity differences between these clones is reflected in the TCR gene products used. The number of TCR V beta, V alpha, and J alpha region gene segments expressed by these clones is very limited. Twelve of 17 clones express V beta 8 at comparable levels on the cell surface. Using PCR amplification of cDNA templates, cloning, and dideoxy sequencing, we have obtained the nucleotide sequence of the TCR V-(D)-J regions in seven of the V beta 8+ clones. Two of the clones use V beta 8.2 and identical J alpha gene segments. Three of the five V beta 8.3+ clones express identical V alpha and J alpha gene products and the other two use similar V alpha chains and J alpha chains with a shared motif in the predicted CDR3 region. Although no clear correlation between TCR gene usage and CD8 dependency was seen, the range of TCR gene usage in the tum- peptide-specific, Ld-restricted immune response is strikingly narrow and suggests a coselection of the alpha- and beta- chains for recognition of the class I/peptide complex.

摘要

我们研究了一组受H-2Ld限制、肿瘤肽特异性CTL克隆中的TCR基因使用情况。这些克隆具有相同的MHC限制性和肽特异性,但在使靶细胞被识别所需的肽量上有显著差异。我们之前证明了给定克隆的决定簇密度需求与CD8依赖性之间存在精确的定量相关性。在本研究中,我们对这些克隆所使用的TCR mRNA的聚合酶链反应拷贝进行了测序,不仅是为了将TCR结构与特定I类/肽复合物的识别相关联,也是为了确定这些克隆之间的功能亲和力差异是否反映在所使用的TCR基因产物中。这些克隆表达的TCR Vβ、Vα和Jα区域基因片段数量非常有限。17个克隆中有12个在细胞表面以相当的水平表达Vβ8。通过对cDNA模板进行PCR扩增、克隆和双脱氧测序,我们获得了7个Vβ8+克隆中TCR V-(D)-J区域的核苷酸序列。其中两个克隆使用Vβ8.2和相同的Jα基因片段。五个Vβ8.3+克隆中的三个表达相同的Vα和Jα基因产物,另外两个使用相似的Vα链和Jα链,在预测的CDR3区域有共同基序。虽然未观察到TCR基因使用与CD8依赖性之间有明确的相关性,但在肿瘤肽特异性、Ld限制的免疫反应中TCR基因使用的范围非常狭窄,这表明α链和β链在识别I类/肽复合物时存在共同选择。

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