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辐射诱导胸腺淋巴瘤发生中早期起始事件的分析。

Analysis of early initiating event(s) in radiation-induced thymic lymphomagenesis.

作者信息

Muto M, Chen Y, Kubo E, Mita K

机构信息

Division of Biology and Oncology, National Institute of Radiological Sciences, Chiba.

出版信息

Jpn J Cancer Res. 1996 Mar;87(3):247-57. doi: 10.1111/j.1349-7006.1996.tb00213.x.

Abstract

Since the T cell receptor rearrangement is a sequential process and unique to the progeny of each clone, we investigated the early initiating events in radiation-induced thymic lymphomagenesis by comparing the oncogenic alterations with the pattern of gamma T cell receptor (TCR) rearrangements. We reported previously that after leukemogenic irradiation, preneoplastic cells developed, albeit infrequently, from thymic leukemia antigen-2+ (TL-2+) thymocytes. Limited numbers of TL-2+ cells from individual irradiated B10.Thy 1.1 mice were injected into B10.Thy 1.2 mice intrathymically, and the common genetic changes among the donor-type T cell lymphomas were investigated with regard to p53 gene and chromosome aberrations. The results indicated that some mutations in the p53 gene had taken place in these lymphomas, but there was no common mutation among the donor-type lymphomas from individual irradiated mice, suggesting that these mutations were late-occurring events in the process of oncogenesis. On the other hand, there were common chromosome aberrations or translocations such as trisomy 15, t(7F;10C), t(1A;13D) or t(6A;XB) among the donor-type lymphomas derived from half of the individual irradiated mice. This indicated that the aberrations/translocations, which occurred in single progenitor cells at the early T cell differentiation either just before or after gamma T cell receptor rearrangements, might be important candidates for initiating events. In the donor-type lymphomas from the other half of the individual irradiated mice, microgenetic changes were suggested to be initial events and also might take place in single progenitor cells just before or right after gamma TCR rearrangements.

摘要

由于T细胞受体重排是一个连续的过程,且每个克隆的子代都具有独特性,因此我们通过比较致癌改变与γT细胞受体(TCR)重排模式,研究了辐射诱导胸腺淋巴瘤发生过程中的早期起始事件。我们之前报道过,致癌性照射后,尽管频率不高,但胸腺白血病抗原2+(TL-2+)胸腺细胞会发育成肿瘤前细胞。将来自个体受照射的B10.Thy 1.1小鼠的有限数量的TL-2+细胞胸腺内注射到B10.Thy 1.2小鼠中,并就p53基因和染色体畸变研究供体型T细胞淋巴瘤之间的常见遗传变化。结果表明,这些淋巴瘤中发生了一些p53基因的突变,但来自个体受照射小鼠的供体型淋巴瘤之间没有共同的突变,这表明这些突变是肿瘤发生过程中的晚期事件。另一方面,在一半个体受照射小鼠来源的供体型淋巴瘤中存在常见的染色体畸变或易位,如三体15、t(7F;10C)、t(1A;13D)或t(6A;XB)。这表明,在γT细胞受体重排之前或之后的早期T细胞分化阶段发生在单个祖细胞中的畸变/易位,可能是起始事件的重要候选因素。在另一半个体受照射小鼠来源的供体型淋巴瘤中,微基因变化被认为是起始事件,也可能发生在γTCR重排之前或之后的单个祖细胞中。

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