Endometrial cancer has been generally categorized into two broad groups of tumors, type I (TI) and type II (TII), with distinct epidemiological/clinical features and genetic alterations. Because telomere attrition appears to trigger genomic instability in certain cancers, we explored the role of telomere dysfunction in endometrial cancer by analyzing telomeres and other markers of telomere status in both tumor types. We describe a new method, telomere chromogenic in situ hybridization, which permitted us to detect cells with short telomeres relative to control (stromal) cells within the same tissue section. Using this method, we found that both types of tumor cells had short telomeres. However, only TII tumors were significantly associated with critical telomere shortening in adjacent, morphologically normal epithelium, suggesting that telomere shortening contributes to the initiation of TII but not TI tumors. To explore this hypothesis, we analyzed mice with critically short telomeres and documented distinctive endometrial lesions that histologically resembled the in situ precursor of TII serous carcinomas; these lesions have not been observed previously in TI mouse models of endometrial cancer. Based on this and previous studies, we propose a model in which telomere attrition contributes to the initiation of TII and progression of TI endometrial cancers.
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机译:子宫内膜癌通常分为两大类肿瘤,即 I 型 (TI) 和 II 型 (TII),具有不同的流行病学/临床特征和遗传改变。由于端粒损耗似乎会引发某些癌症的基因组不稳定,因此我们通过分析端粒和两种肿瘤类型中端粒状态的其他标志物来探索端粒功能障碍在子宫内膜癌中的作用。我们描述了一种新方法,端粒显色原位杂交,它使我们能够检测同一组织切片中相对于对照(基质)细胞端粒较短的细胞。使用这种方法,我们发现两种类型的肿瘤细胞都具有短端粒。然而,在相邻的形态学正常的上皮细胞中,只有 TII 肿瘤与关键端粒缩短显着相关,这表明端粒缩短有助于 TII 的发生,但不有助于 TI 肿瘤的发生。为了探索这一假设,我们分析了端粒极短的小鼠,并记录了独特的子宫内膜病变,这些病变在组织学上类似于 TII 浆液性癌的原位前体;这些病变以前在子宫内膜癌的TI小鼠模型中未观察到。基于这项研究和以前的研究,我们提出了一个模型,其中端粒磨损有助于 TII 的发生和 TI 子宫内膜癌的进展。
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