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MHC class I and class I-like gene product expression by malignant T cells: relationships between CD1a HLA-ABC and beta 2-microglobulin.

机译:恶性T细胞表达MHC I类和I类类基因产物:CD1aHLA-ABC和β2微球蛋白之间的关系。

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摘要

Beta 2-microglobulin (beta 2m) forms the invariant light chain of the MHC-encoded HLA-ABC and the non-MHC-encoded CD1 molecules. While HLA-ABC (MHC Class I) molecules are virtually ubiquitous in tissue distribution, CD1 determinants by contrast are more restricted. We have assessed, by indirect immunoenzymeassay, the relative membrane densities of these molecules on malignant thymic and post-thymic T cells. It was found that the T cells of mature post-thymic proliferations expressed significantly more beta 2m-associated protein, predominantly HLA-ABC in nature, than thymic-ALL blasts. This parallels the situation found in normal peripheral T cells and thymocytes. In contrast to post-thymic T cells, thymic-ALL blasts showed considerable case to case variation with respect to non-HLA-associated beta 2m and, of particular interest, not all of this excess beta 2m could be accounted for by CD1a. We therefore conclude that other beta 2m-containing molecules may be expressed on thymic-ALL blasts and possibly also on post-thymic leukaemic T cells. In addition, it was found that T cells from CD4+ cases of post-thymic proliferations expressed more beta 2m-associated determinants than other T cells, whether of either normal or malignant origin, and that certain post-thymic malignancies express significantly increased levels of beta 2m-associated protein relative to normal peripheral T-cells. This is in direct contrast to the situation seen in many solid malignancies.
机译:Beta 2微球蛋白(beta 2m)形成了MHC编码的HLA-ABC和非MHC编码的CD1分子的不变轻链。虽然HLA-ABC(I类MHC)分子在组织分布中实际上无处不在,但CD1决定簇却受到更大的限制。我们已经通过间接免疫酶法评估了这些分子在恶性胸腺和胸腺后T细胞上的相对膜密度。已发现,成熟的胸腺后增殖的T细胞表达的β2m相关蛋白明显多于胸腺ALL细胞,本质上主要是HLA-ABC。这与正常外周T细胞和胸腺细胞中发现的情况相似。与胸腺后T细胞相反,胸腺ALL胚细胞与非HLA相关的beta 2m表现出明显的个体差异,特别令人感兴趣的是,CD1a不能解释所有这些过量的beta 2m。因此,我们得出结论,其他含β2m的分子可能在胸腺ALL细胞上表达,也可能在胸腺后白血病T细胞上表达。另外,发现胸腺后增殖的CD4 +病例中的T细胞比其他T细胞表达更多的β2m相关决定簇,无论是正常来源还是恶性起源,而且某些胸腺后恶性肿瘤表达的β水平明显升高。相对于正常外周T细胞为2m相关蛋白。这与许多实体恶性肿瘤中看到的情况形成直接对比。

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