非酒精性脂肪性肝病患者的端粒酶逆转录酶种系突变与肝细胞癌
Telomerase reverse transcriptase germline mutations and hepatocellular carcinoma in patients with nonalcoholic fatty liver disease.
作者信息
Donati Benedetta, Pietrelli Alessandro, Pingitore Piero, Dongiovanni Paola, Caddeo Andrea, Walker Lucy, Baselli Guido, Pelusi Serena, Rosso Chiara, Vanni Ester, Daly Ann, Mancina Rosellina Margherita, Grieco Antonio, Miele Luca, Grimaudo Stefania, Craxi Antonio, Petta Salvatore, De Luca Laura, Maier Silvia, Soardo Giorgio, Bugianesi Elisabetta, Colli Fabio, Romagnoli Renato, Anstee Quentin M, Reeves Helen L, Fracanzani Anna Ludovica, Fargion Silvia, Romeo Stefano, Valenti Luca
机构信息
Department of Pathophysiology and Transplantation, Università degli Studi di Milano, Fondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico, Milan, 20122, Italy.
Istituto Nazionale di Genetica Molecolare (INGM), Romeo ed Enrica Invernizzi, Bioinformatics Group, Milan, 20122, Italy.
出版信息
Cancer Med. 2017 Aug;6(8):1930-1940. doi: 10.1002/cam4.1078. Epub 2017 Jul 4.
In an increasing proportion of cases, hepatocellular carcinoma (HCC) develops in patients with nonalcoholic fatty liver disease (NAFLD). Mutations in telomerase reverse transcriptase (hTERT) are associated with familial liver diseases. The aim of this study was to examine telomere length and germline hTERT mutations as associated with NAFLD-HCC. In 40 patients with NAFLD-HCC, 45 with NAFLD-cirrhosis and 64 healthy controls, peripheral blood telomere length was evaluated by qRT-PCR and hTERT coding regions and intron-exon boundaries sequenced. We further analyzed 78 patients affected by primary liver cancer (NAFLD-PLC, 76 with HCC). Enrichment of rare coding mutations (allelic frequency <0.001) was evaluated by Burden test. Functional consequences were estimated in silico and by over-expressing protein variants in HEK-293 cells. We found that telomere length was reduced in individuals with NAFLD-HCC versus those with cirrhosis (P = 0.048) and healthy controls (P = 0.0006), independently of age and sex. We detected an enrichment of hTERT mutations in NAFLD-HCC, that was confirmed when we further considered a larger cohort of NAFLD-PLC, and was more marked in female patients (P = 0.03). No mutations were found in cirrhosis and local controls, and only one in 503 healthy Europeans from the 1000 Genomes Project (allelic frequency = 0.025 vs. <0.001; P = 0.0005). Mutations with predicted functional impact, including the frameshift Glu113Argfs*79 and missense Glu668Asp, cosegregated with liver disease in two families. Three patients carried missense mutations (Ala67Val in homozygosity, Pro193Leu and His296Pro in heterozygosity) in the N-terminal template-binding domain (P = 0.037 for specific enrichment). Besides Glu668Asp, the Ala67Val variant resulted in reduced intracellular protein levels. In conclusion, we detected an association between shorter telomeres in peripheral blood and rare germline hTERT mutations and NAFLD-HCC.
在越来越多的病例中,肝细胞癌(HCC)发生于非酒精性脂肪性肝病(NAFLD)患者。端粒酶逆转录酶(hTERT)突变与家族性肝病相关。本研究的目的是检测与NAFLD-HCC相关的端粒长度和种系hTERT突变。对40例NAFLD-HCC患者、45例NAFLD肝硬化患者和64例健康对照者,采用qRT-PCR评估外周血端粒长度,并对hTERT编码区及内含子-外显子边界进行测序。我们进一步分析了78例原发性肝癌患者(NAFLD-PLC,76例为HCC)。通过负荷检验评估罕见编码突变(等位基因频率<0.001)的富集情况。通过计算机模拟以及在HEK-293细胞中过表达蛋白变体来估计功能后果。我们发现,与肝硬化患者(P = 0.048)和健康对照者(P = 0.0006)相比,NAFLD-HCC患者的端粒长度缩短,且与年龄和性别无关。我们在NAFLD-HCC中检测到hTERT突变富集,在进一步纳入更大的NAFLD-PLC队列时得到证实,且在女性患者中更明显(P = 0.03)。在肝硬化患者和局部对照中未发现突变,在1000基因组计划的503名健康欧洲人中仅发现1例(等位基因频率= 0.025 vs. <0.001;P = 0.0005)。具有预测功能影响的突变,包括移码突变Glu113Argfs*79和错义突变Glu668Asp,在两个家族中与肝病共分离。3例患者在N端模板结合域携带错义突变(纯合子Ala67Val、杂合子Pro193Leu和His296Pro)(特异性富集的P = 0.037)。除Glu668Asp外,Ala67Val变体导致细胞内蛋白水平降低。总之,我们检测到外周血中端粒缩短、罕见种系hTERT突变与NAFLD-HCC之间存在关联。
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