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Genetic control of the circulating concentration of transforming growth factor type beta1.

机译:遗传控制的转化生长因子类型β1的循环浓度。

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摘要

The concentration of transforming growth factor beta (TGF-beta) in plasma has been correlated with the development of several diseases, including atherosclerosis and certain forms of cancer. However, the mechanisms that control the concentration of TGF-beta in plasma are poorly understood. In a study of 170 pairs of female twins (average age 57.7 years) we show that the concentration of active plus acid-activatable latent TGF-beta1 [(a+l) TGF-beta therefore is predominantly under genetic control (heritability estimate 0.54). Single strand conformation polymorphism (SSCP) mapping of the TGF-beta1 gene promoter has identified two single base substitution polymorphisms. The two polymorphisms (G-->A at position -800 bp and C-->T at position -509 bp) are in linkage disequilibrium (correlation coefficient Delta = 0.215, P < 0.01). The C-509T polymorphism is significantly associated with the plasma concentration of (a+l) TGF-beta1, explaining 8.2% of the additive genetic variance of (a+l) TGF-beta1 concentration. It is therefore possible that predisposition to atherosclerosis, bone diseases or various forms of cancer may be correlated with the presence of particular alleles at the TGFB1 locus.
机译:血浆中转化生长因子β(TGF-β)的浓度与多种疾病的发展相关,包括动脉粥样硬化和某些形式的癌症。但是,人们对控制血浆中TGF-β浓度的机制了解甚少。在一项对170对女性双胞胎(平均年龄57.7岁)的研究中,我们发现活性加酸可活化的潜在TGF-beta1 [(a + 1)TGF-beta的浓度主要受遗传控制(遗传估计0.54) 。 TGF-beta1基因启动子的单链构象多态性(SSCP)映射已确定两个单碱基取代多态性。两种多态性(-800 bp处的G-> A和-509 bp处的C-> T)处于连锁不平衡状态(相关系数Delta = 0.215,P <0.01)。 C-509T多态性与(a + 1)TGF-beta1的血浆浓度显着相关,解释了(a + 1)TGF-beta1浓度的累加遗传变异的8.2%。因此,动脉粥样硬化,骨骼疾病或各种形式的癌症的易感性可能与TGFB1基因座处特定等位基因的存在有关。

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