10月24日、31日,学术期刊《自然—遗传》接连在线发表了我国科学家发现麻风和精神分裂症易感基因的两项重要科研成果。这两项成果的完成,主要依托安徽医科大学*皮肤病重点实验室的全基因组关联研究(GWAS)平台和生物信息分析技术。
麻风病为麻风杆菌感染后侵犯皮肤和周围神经而导致肢体致残和畸形的严重复杂疾病。2009年,安徽医科大学教授张学军与山东省医学*研究员张福仁合作,利用全基因组关联研究发现麻风病7个易感基因,并发现其致病基因作用通路,是世界上*传染病全基因组关联研究,研究成果证明麻风病具有遗传易感性,成果发表在《新英格兰医学杂志》(New England Journal of Medicine)上。
在此基础上,张福仁继续加大样本量,与张学军、刘建军教授紧密合作,今年再次发现麻风病2个新的易感基因(IL23R和RAB32),这是目前上规模zui大的麻风全基因组关联研究,对麻风的预防和治疗将具有重大意义,标志着我国麻风易感基因研究继续居于世界水平。
而精神分裂症是以基本个性、思维、情感、行为的分裂,精神活动与环境的不协调为主要特征的一类zui常见的精神病,是精神病里zui严重的一种。北京大学精神卫生研究所教授张岱和国家人类基因组南方研究中心教授黄薇的研究团队,与张学军团队共同开展了对精神分裂症易感基因的研究。
该研究通过对近1.2万例患者和正常对照的全基因组关联研究,在11号染色体上发现了一个新的精神分裂症易感基因TSPAN18,同时验证出了既往国外已有报道的位于6号染色体上的易感基因,标志着我国精神分裂症易感基因研究跻身*行列。
据悉,这是安徽医大皮肤病重点实验室第九次在《自然—遗传》上发表疾病基因研究论文。此前,该实验室先后研究发现了银屑病、白癜风、红斑狼疮、特异性皮炎等复杂皮肤病易感基因。(生物谷 )
doi:10.1038/ng.973
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Identification of two new loci at IL23R and RAB32 that influence susceptibility to leprosy
Furen Zhang, Hong Liu, Shumin Chen, Huiqi Low, Liangdan Sun, Yong Cui, Tongsheng Chu, Yi Li, Xi'an Fu, Yongxiang Yu, Gongqi Yu, Benqing Shi, Hongqing Tian, Dianchang Liu, Xiulu Yu, Jinghui Li, Nan Lu, Fangfang Bao, Chunying Yuan, Jian Liu, Huaxu Liu, Lin Zhang, Yonghu Sun, Mingfei Chen, Qing Yang et al.
We performed a genome-wide association study with 706 individuals with leprosy and 5,581 control individuals and replicated the top 24 SNPs in three independent replication samples, including a total of 3,301 individuals with leprosy and 5,299 control individuals from China. Two loci not previously associated with the disease were identified with genome-wide significance: rs2275606 (combined P = 3.94 × 10−14, OR = 1.30) on 6q24.3 and rs3762318 (combined P = 3.27 × 10−11, OR = 0.69) on 1p31.3. These associations implicate IL23R and RAB32 as new susceptibility genes for leprosy. Furthermore, we identified evidence of interaction between the NOD2 and RIPK2 loci, which is consistent with the biological association of the proteins encoded by these genes (NOD2-RIPK2 complex) in activating the NF-κB pathway as a part of the host defense response to infection. Our findings have expanded the biological functions of IL23R by uncovering its involvement in infectious disease susceptibility and suggest a potential involvement of autophagocytosis in leprosy pathogenesis. The IL23R association supports previous observations of the marked overlap of susceptibility genes for leprosy and Crohn's disease, implying common pathogenesis mechanisms.
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