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Nat Genet:科学家发现与肝纤维化有关的蛋白

2017-05-26 Flora 生物探索

近期,来自于悉尼Westmead医学研究所的研究团队在Nature子刊《Nature Genetics》发表文章,揭示了引发肝脏组织损伤的罪魁祸首,为肝病治疗带来新的启示。他们首次发现,干扰素λ3(INLF3)蛋白突变会导致肝纤维化。由Jacob George教授和Mohammed Eslam博士领导的国际研究小组之前已经证实,与肝纤维化有关联的常见基因变异位于染色体9号上的IFNL3和IFNL4

近期,来自于悉尼Westmead医学研究所的研究团队在Nature子刊《Nature Genetics》发表文章,揭示了引发肝脏组织损伤的罪魁祸首,为肝病治疗带来新的启示。他们首次发现,干扰素λ3(INLF3)蛋白突变会导致肝纤维化。

由Jacob George教授和Mohammed Eslam博士领导的国际研究小组之前已经证实,与肝纤维化有关联的常见基因变异位于染色体9号上的IFNL3和IFNL4基因之间。但是,IFNL3、IFNL4蛋白谁会引发肝纤维化一直未有答案。

现在,在这一篇最新文章中,研究团队招募2000名丙肝患者进行相关研究,借助先进的基因测序和功能分析技术,第一次明确与肝纤维化相关的蛋白是IFNL3。

结果发现,受伤后,从血液中迁移至肝脏组织的炎症细胞会变多,且IFNL3蛋白表达量会增加,导致肝脏损伤。而且,这一系列反应很大程度上由基因决定。

Jacob George教授认为,这一成果很重要,它可以作为预测个体发生肝脏疾病风险的关键指标,从而及早干预以及改变不良生活方式。

目前,研究团队已经设计出一款基于最新发现的诊断工具,用于预测患者发生肝纤维化的风险。它可以依赖于基因信息,预测一个人发生纤维化风险的程度是否很高,以及评估患者肝病发展的速度。

Mohammed Eslam教授相信,未来这一发现将在预控肝病医疗负担中发挥重要作用。目前,我们依然没有治疗晚期肝纤维化的药物,肝移植是治疗肝脏衰竭的唯一方法。“现在,我们知道,IFNL3蛋白是导致肝脏瘢痕的原因。所以,我们可以开发针对这一突变位点的新疗法和药物。” Eslam教授表示。

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    2017-12-15 cy0324
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    2017-10-07 canlab
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    2018-03-21 liye789132251
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    2017-05-26 jaysppr

    感谢分享!!!!!

    0

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