首页> 外文期刊>Journal of hepato-biliary-pancreatic surgery >Genome-wide microsatellite analysis of focal nodular hyperplasia: a strong tool for the differential diagnosis of non-neoplastic liver nodule from hepatocellular carcinoma.
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Genome-wide microsatellite analysis of focal nodular hyperplasia: a strong tool for the differential diagnosis of non-neoplastic liver nodule from hepatocellular carcinoma.

机译:全基因组微卫星分析局灶性结节性增生:一个强有力的工具来鉴别诊断肝细胞癌非肿瘤性肝结节。

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摘要

Allelic imbalance (AI), which represents certain chromosomal gains or losses, has been described in hepatocellular carcinoma (HCC), but the significance of AI analysis in focal nodular hyperplasia (FNH) has not been fully clarified. We hypothesized, therefore, that comprehensive allelotyping of FNH could be a useful tool for differentiating FNH from HCC. A 27-year-old man was admitted to the hospital because of general fatigue. A computed tomography (CT) scan disclosed a hepatic nodule 8 cm in diameter. No definite diagnosis was made after imaging or by biopsy before surgery. Macroscopically and microscopically, the surgical specimen showed typical features of FNH. Comprehensive microsatellite analysis was carried out with 382 microsatellite markers distributed throughout all chromosomes. To detect AI effectively, the cutoff value of the AI index was set at 0.70. Among the 382 microsatellite markers, 212 loci were informative, but no AI was detected. The absence of gross chromosomal alterations strongly suggested that the large nodule was FNH rather than HCC, in terms of its genetic background. The patient's subsequent clinical course revealed the nodule to be benign. The results suggest that this genome-wide microsatellite analysis is a useful tool for the differential diagnosis of non-neoplastic liver nodules from HCC.
机译:肝细胞癌(HCC)中已描述了代表某些染色体得失的等位基因失衡(AI),但尚未充分阐明AI分析在局灶性结节性增生(FNH)中的意义。因此,我们假设,对FNH进行全面的定型分析可能是区分FNH与HCC的有用工具。一名27岁的男子因全身疲倦而入院。计算机断层扫描(CT)扫描显示直径为8厘米的肝结节。影像学检查后或手术前活检未明确诊断。宏观和微观上,手术标本显示了FNH的典型特征。使用分布在所有染色体上的382个微卫星标记进行了全面的微卫星分析。为了有效地检测AI,将AI指数的临界值设置为0.70。在382个微卫星标记中,有212个基因座提供了信息,但未检测到AI。缺乏总的染色体改变强烈地表明,就其遗传背景而言,大的结节是FNH而不是HCC。患者随后的临床过程显示结节是良性的。结果表明,这种全基因组微卫星分析是从HCC鉴别诊断非肿瘤性肝结节的有用工具。

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