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首页> 外文期刊>European journal of human genetics: EJHG >Polymorphisms in MC3R promoter and CTSZ 3'UTR are associated with tuberculosis susceptibility.
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Polymorphisms in MC3R promoter and CTSZ 3'UTR are associated with tuberculosis susceptibility.

机译:MC3R启动子和CTSZ 3'UTR的多态性与结核病易感性有关。

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摘要

We have validated the association of two genes on chromosome 20q13.31-33 with tuberculosis susceptibility. A previous genome-wide linkage study performed by Cooke et al identified the genes melanocortin-3-receptor (MC3R) and cathepsin Z (CTSZ) as possible candidates in tuberculosis susceptibility. MC3R has been implicated in obesity studies and is known to play a role in many biological systems including the regulation of energy homeostasis and fat metabolism. CTSZ has been detected in immune cells, such as macrophages and monocytes, and it is hypothesized that the protein may play a role in the immune response. In our South African population a case-control study confirmed the previously reported association with a single-nucleotide polymorphism (SNP) in CTSZ and found an association in MC3R with a SNP not previously implicated in tuberculosis susceptibility. Six SNPs in MC3R and eight in CTSZ were genotyped and haplotypes were inferred. SNP rs6127698 in the promoter region of MC3R (cases = 498; controls = 506) and rs34069356 in the 3'UTR of CTSZ (cases = 396; controls = 298) both showed significant association with tuberculosis susceptibility (P = 0.0004 and < 0.0001, respectively), indicating that pathways involving these proteins, not previously researched in this disease, could yield novel therapies for tuberculosis.
机译:我们已经验证了染色体20q13.31-33上两个基因与结核病易感性的关联。 Cooke等人先前进行的全基因组连锁研究确定,基因melanocortin-3-receptor(MC3R)和组织蛋白酶Z(CTSZ)是结核易感性的可能候选者。 MC3R与肥胖症研究有关,已知在许多生物系统中起作用,包括能量稳态和脂肪代谢的调节。 CTSZ已在免疫细胞(例如巨噬细胞和单核细胞)中检测到,据推测该蛋白可能在免疫反应中起作用。在我们的南非人群中,一项病例对照研究证实了先前报道的CTSZ与单核苷酸多态性(SNP)的关联,并发现MC3R与先前与结核病易感性无关的SNP的关联。对MC3R中的6个SNP和CTSZ中的8个SNP进行基因分型并推断出单倍型。 MC3R启动子区域的SNP rs6127698(病例= 498;对照= 506)和CTSZ 3'UTR的rs34069356(病例= 396;对照= 298)均与结核病易感性密切相关(P = 0.0004和<0.0001分别),表明涉及这些蛋白质的途径(以前未在该疾病中进行过研究)可能会产生结核病的新疗法。

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