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首页> 外文期刊>The Journal of molecular diagnostics: JMD >Microsatellite analysis of hereditary nonpolyposis colorectal cancer-associated colorectal adenomas by laser-assisted microdissection: correlation with mismatch repair protein expression provides new insights in early steps of tumorigenesis.
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Microsatellite analysis of hereditary nonpolyposis colorectal cancer-associated colorectal adenomas by laser-assisted microdissection: correlation with mismatch repair protein expression provides new insights in early steps of tumorigenesis.

机译:激光辅助显微切割对遗传性非息肉性大肠直肠癌相关大肠腺瘤的微卫星分析:与错配修复蛋白表达的相关性为肿瘤发生的早期提供了新的见识。

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摘要

Although microsatellite instability (MSI) testing is a useful tool for molecular screening of hereditary nonpolyposis colorectal cancer (HNPCC) carcinomas, conflicting results have been obtained in colorectal adenomas. This might result from different techniques of tissue sampling and MSI analysis. Alternatively, some HNPCC-associated adenomas may follow a molecular route that differs from the MSI pathway. In the present study we examined the MSI status of 18 adenomas from 17 HNPCC patients by comparing manual adenoma dissection under gross visual control with laser microdissection of single adenoma crypts. After manual gross dissection, 50% (9 of 18) and 11.1% (2 of 18) of the adenomas displayed high-level (MSI-H) and low-level (MSI-L) MSI, respectively. The same set of adenomas split into 83.3% (15 of 18) MSI-H and 5.6% (1 of 18) MSI-L after laser microdissection. The expression pattern of mismatch repair (MMR) proteins showed a higher concordance rate with the MSI status in laser-dissected (94%) than gross-dissected (47%) adenomas. Whereas two adenomas remained microsatellite stable (MSS) and MMR proficient even after laser-assisted dissection, two MSI-H cases showed either rare instabilities at coding microsatellites or intratumoral heterogeneity of MSI with and without MSH2 expression. This suggests that in some adenomas development of MMR dysfunction occurs stepwise with MSI, arising before complete loss of MMR gene expression, whereas other HNPCC-associated adenomas might develop independently of MMR deficiency.
机译:尽管微卫星不稳定性(MSI)测试是用于遗传性非息肉病性结直肠癌(HNPCC)癌分子筛查的有用工具,但在结直肠腺瘤中却获得了矛盾的结果。这可能是由于组织采样和MSI分析的不同技术导致的。或者,某些与HNPCC相关的腺瘤可能遵循不同于MSI途径的分子途径。在本研究中,我们通过比较肉眼视觉控制下的手动腺瘤切除术与单个腺瘤隐窝的激光显微解剖,检查了来自17名HNPCC患者的18例腺瘤的MSI状态。人工大体解剖后,分别有50%(18个中的9个)和11.1%(18个中的2个)腺瘤表现为高水平(MSI-H)和低水平(MSI-L)。激光显微切割后,同一组腺瘤分成83.3%(18个中的15个)MSI-H和5.6%(18个中的1个)MSI-L。错配修复(MMR)蛋白的表达模式与激光切割(94%)的MSI状态相比,与总切割(47%)的腺瘤具有更高的一致性。尽管两个腺瘤即使在激光辅助解剖后仍保持微卫星稳定(MSS)和MMR熟练水平,但是两个MSI-H病例在编码微卫星时表现出罕见的不稳定性,或者在有和没有MSH2表达的情况下,MSI的瘤内异质性。这表明在一些腺瘤中,MMI会逐步发生MMR功能障碍,这是在MMR基因表达完全丧失之前发生的,而其他HNPCC相关的腺瘤可能独立于MMR缺乏而发展。

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