北京大学学报(医学版) ›› 2023, Vol. 55 ›› Issue (2): 254-261. doi: 10.19723/j.issn.1671-167X.2023.02.008
Li LIANG,Xin LI,Lin NONG,Ying DONG,Ji-xin ZHANG,Dong LI,Ting LI*()
摘要:
目的: 对比结直肠癌(colorectal cancer, CRC), 评估子宫内膜癌(endometrial cancer, EMC)微卫星不稳定性(microsatellite instability, MSI)改变的特点。方法: 收集228例EMC和770例CRC进行对比分析。采用免疫组织化学(immunohistochemistry, IHC)方法检测错配修复缺陷(deficient mismatch repair, dMMR)蛋白表达缺失, 采用PCR及毛细管电泳片段分析法检测MSI(MSI-PCR), MSI-PCR采用5个单核苷酸位点(BAT-25、BAT-26、NR-21、NR-24和MONO-27)。结果: EMC中, 27.19%(62/228例)为dMMR, 显著高于CRC(7.79%, 60/770例), 且4例dMMR-EMC和2例dMMR-CRC呈错配修复(mismatch repair, MMR)蛋白亚克隆表达。MSI-PCR检测依据显著微卫星变换判读标准, EMC的结果显示: 16.23%(37/228例)为高度MSI, 2.63%(6/228例)为低度MSI, 81.14%(185/228例)为微卫星稳定型, MMR-IHC与MSI-PCR两种评估方法的不一致率为11.84%(27/228例); CRC的结果显示: 8.05%(62/770例)为高度MSI, 0.13%(1/770例)为低度MSI, 91.82%(707/770例)为微卫星稳定型, 两种评估方法的不一致率仅为0.52%(4/770例)。而依据微小微卫星变换结果判读, 12例EMC发现微小微卫星变换(8例dMMR/微卫星稳定型和4例dMMR/低度MSI), 被评估为dMMR/高度MSI, 因此, 高度MSI型EMC为21.49%(49/228例), 两种方法的不一致率降至6.58%(15/228例)。CRC中未见微小微卫星变换。与显著微卫星变换EMC组相比, 微小微卫星变换EMC组的患者年龄偏小, 肿瘤分化更好, 国际妇产科联盟(International Fede-ration of Gyne-cology and Obstetrics, FIGO)分期更早。两组间组织学类型及FIGO分期的差异有统计学意义(P < 0.001, P=0.006)。结论: EMC易发生微小微卫星变换, MSI-PCR检测结果的判读不应忽视微小微卫星变换, MMR-IHC和MSI-PCR互补联合检测是捕获dMMR肿瘤最敏感和特异的方法。
中图分类号:
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