胆囊癌中微卫星不稳定性和脆弱组氨酸三联体缺失

Niraj Kumari, Vinay K. Kapoor, Narendra Krishnani, Kamlesh Kumar, Dinesh Kumar Baitha, Anu Behari
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引用次数: 1

摘要

背景与目的:微卫星不稳定性和脆弱组氨酸三联体(FHIT)丢失被认为与胆囊癌的发生有关。我们使用针对MLH1、MSH2和MSH6蛋白的抗体,通过免疫组化研究了错配修复(MMR)蛋白的表达缺失和FHIT蛋白在胆囊癌中的表达缺失。方法:回顾性收集连续102例胆囊癌患者,观察MLH1、MSH2、MSH6及FHIT蛋白的表达情况。表达模式与各种临床病理参数和生存率相关。结果:52.9%的胆囊癌患者存在MMR蛋白表达缺失,45%的胆囊癌患者存在FHIT蛋白表达缺失。FHIT表达缺失见于12%的与癌相关的发育不良患者。MMR蛋白的表达缺失在16%与慢性胆囊炎相关的发育不良和32.6%与癌症相关的发育不良中发现。MMR蛋白表达缺失与肿瘤分期呈显著正相关,与完整表达患者相比,其生存期更差。FHIT表达缺失与肿瘤分级和分期均有显著相关性。结论:MMR蛋白表达缺失和FHIT表达缺失的频率从非典型增生到癌增加,提示这两种异常在胆囊癌的发病过程中都有作用,并发生在早期。53%的MMR蛋白表达缺失的胆囊癌也显示FHIT表达缺失,并且在晚期疾病中很常见,这表明FHIT表达减少可能与免疫组织化学上MMR蛋白的表达缺失有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Microsatellite instability and loss of fragile histidine triad in gallbladder carcinoma

Background and aim: Microsatellite instability and fragile histidine triad (FHIT) loss have been seen to be involved in gallbladder carcinogenesis. We studied expression loss of mismatch repair (MMR) proteins and loss of FHIT expression in gallbladder cancer by immunohistochemistry using antibodies against MLH1, MSH2 and MSH6 proteins. Methods: One hundred and two consecutive cases of gallbladder cancer were retrospectively collected and expression of MLH1, MSH2 and MSH6 and FHIT protein was studied. The expression pattern was correlated with various clinicopathologic parameters and survival. Results: Expression loss of MMR proteins was found in 52.9% and loss of FHIT expression was found in 45% cases of gallbladder cancer. Loss of FHIT expression was seen in 12% of dysplasia associated with carcinoma. Expression loss of MMR proteins was found in 16% of dysplasia associated with chronic cholecystitis and 32.6% of dysplasia associated with carcinoma. Expression loss of MMR proteins had significant positive correlation with tumor stage and had worse survival compared with patients with intact expression. Loss of FHIT expression was significantly correlated with both tumor grade and stage. Conclusions: Frequency of expression loss of MMR proteins and loss of FHIT expression increased from dysplasia to carcinoma suggesting that both these abnormalities have a role in pathogenesis and occur at an early stage in carcinogenesis of gallbladder. Fifty three percent of gallbladder cancer with expression loss of MMR proteins also showed loss of FHIT expression and were frequent in advanced stage disease suggesting that reduced FHIT expression may be correlated with expression loss of MMR proteins on immunohistochemistry.

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