The dynamics of early intestinal tumour proliferation: to be or not to be.

Cancer surveys Pub Date : 1998-01-01
D Shibata
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Abstract

New data and approaches bring novel perspectives and possibilities to old problems. The speculation of this chapter attempts to merge the puzzling MS data observed in human tumours (Figs. 3 and 4B) within a multistep tumour progression model. Clearly the current models are gross simplifications and other, more sophisticated models may better account for the distribution of MS alleles found in human tumours. The findings and the data are also limited to MMR deficient tumours, and studies in non-mutator phenotype tumours may be more difficult since fewer polymorphisms will arise during progression. The current model, however, precisely defines proliferation and clearly delineates two very distinct patterns. Further studies using MS loci in MMR deficient tumours will allow fairer tests of alternative pathways (Fig. 4C) to cancer. Evolution proceeding in occult progenitor populations allows mutations to accumulate throughout life and not just in the last decades after polyps appear.

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早期肠道肿瘤增殖动力学:生存还是毁灭。
新的数据和方法为老问题带来新的视角和可能性。本章的推测试图在一个多步骤肿瘤进展模型中合并在人类肿瘤中观察到的令人困惑的MS数据(图3和4B)。显然,目前的模型是粗略的简化,其他更复杂的模型可能更好地解释在人类肿瘤中发现的多发性硬化症等位基因的分布。研究结果和数据也仅限于MMR缺陷肿瘤,非突变表型肿瘤的研究可能更加困难,因为在进展过程中会出现较少的多态性。然而,目前的模型精确地定义了扩散,并清楚地描绘了两种截然不同的模式。在MMR缺陷肿瘤中使用MS基因座的进一步研究将允许对癌症的替代途径进行更公平的测试(图4C)。在隐蔽的祖先群体中进行的进化允许突变在整个生命中积累,而不仅仅是在息肉出现后的最后几十年。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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