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首页> 外文期刊>British Journal of Cancer >Apparent bypass of negative selection in CD8+ tumours in CD2-myc transgenic mice
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Apparent bypass of negative selection in CD8+ tumours in CD2-myc transgenic mice

机译:CD2-myc转基因小鼠CD8 +肿瘤中负选择的明显绕过

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摘要

A role for antigen stimulation in lymphoid neoplasia has been postulated and is supported by indirect evidence that suggests that the interaction of antigen with both T cells and B cells may constitute an epigenetic event that can contribute to tumour induction or tumour progression. Using myc-bearing transgenic mice that develop mainly clonal T-cell lymphomas we have investigated the possibility that endogenous antigen-mediated clonal deletion might be overridden in tumorigenesis. CD2-myc transgenic mice were backcrossed on to a CBA/Ca background to ensure Mtv-mediated deletion of V beta 11-expressing T cells in the resultant offspring. Lymphomas arising from these mice were subsequently screened for V beta 11 expression. There was a clear correlation between the age at which mice developed neoplasia and the tumour phenotype. Mice with CD4- CD8+ tumours succumbed to thymic lymphoma at a significantly younger age than mice developing CD4+ CD8+ tumours. A small number of tumours consisted of the 'forbidden' V beta 11 phenotype, showing that cells vulnerable to transformation could escape negative selection. The majority of the V beta 11-positive tumours were CD4- CD8+ and were only observed in mice showing clinical evidence of tumour development at a relatively young age. The phenotype of these cells and the age at which tumours arose suggests that T cells escaping tolerance may be susceptible to transformation.
机译:已经假定了抗原刺激在淋巴样赘生物中的作用,并得到间接证据的支持,该间接证据表明抗原与T细胞和B细胞的相互作用可能构成表观遗传事件,可能有助于肿瘤诱导或肿瘤进展。使用主要生长克隆性T细胞淋巴瘤的带有myc的转基因小鼠,我们研究了内源性抗原介导的克隆缺失在肿瘤发生中可能被覆盖的可能性。将CD2-myc转基因小鼠回交至CBA / Ca背景,以确保在所得子代中Mtv介导的表达V beta 11的T细胞的缺失。随后筛选由这些小鼠引起的淋巴瘤的V beta 11表达。小鼠发生瘤形成的年龄与肿瘤表型之间存在明显的相关性。与患有CD4 + CD8 +肿瘤的小鼠相比,患有CD4- CD8 +肿瘤的小鼠死于胸腺淋巴瘤的年龄要小得多。少数肿瘤由“禁止的” V beta 11表型组成,表明易发生转化的细胞可以逃避阴性选择。大多数V beta 11阳性肿瘤是CD4-CD8 +,并且仅在小鼠中观察到,这些小鼠显示出相对年轻年龄的肿瘤发展的临床证据。这些细胞的表型和出现肿瘤的年龄表明逃避耐受性的T细胞可能易于转化。

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