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Size Matters: Sequential Mutations in Tumorigenesis May Reflect the Stochastic Effect of Mutagen Target Sizes

机译:大小问题:肿瘤发生中的顺序突变可能反映了诱变目标大小的随机效应

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摘要

We tallied the number of possible mutant amino acids in proteins thought to be inactivated early in tumorigenesis and in proteins thought to be inactivated late in tumorigenesis, respectively. Proteins thought to be inactivated early in tumorigenesis, on average, have a greater number of alternative, mutant possibilities, which raises the possibility that the sequential order of mutations associated with cancer development reflects the random chance, throughout life, of a mutagen inactivating a larger versus a smaller target. The hypothesis that the temporal order of genetic changes in cancer reflects mutagen target sizes leads to novel considerations of 1) the mechanisms of the acquisition of cancer hallmarks and 2) cancer screening strategies.
机译:我们分别计算了在肿瘤发生早期被认为失活的蛋白质和在肿瘤发生晚期被认为失活的蛋白质中可能的突变氨基酸的数量。平均而言,被认为在肿瘤发生早期被灭活的蛋白质具有更多的替代突变可能性,这增加了与癌症发展相关的突变顺序顺序反映出一生中诱变剂灭活的随机机会的可能性。与较小的目标相比。癌症中遗传变化的时间顺序反映了诱变靶标大小的假说导致了以下新考虑:1)获得癌症标志的机制和2)癌症筛查策略。

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