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The functional polymorphism rs73598374:GA (p.Asp8Asn) of the ADA gene is associated with telomerase activity and leukocyte telomere length

机译:ADA基因的功能性多态性rs73598374:G A(p.Asp8Asn)与端粒酶活性和白细胞端粒长度有关

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摘要

Recent evidence demonstrated a relevant role of adenosine deaminase (ADA) in replicative senescence of T cells through its capacity to modulate telomerase activity (TA). Herein, we tested the impact of the functional polymorphism ADA rs73598374:G>A (c.22G>A, p.Asp8Asn) on telomere biology, by measuring TA and leukocyte telomere length (LTL) in healthy subjects selected according to rs73598374 genotype. rs73598374-A carriers showed lower TA (P=0.019) and shorter LTL (P=0.003), respectively, compared to G/G carriers. rs73598374-A carriers showed a stronger cross-sectional age reduction of LTL (r=−0.314, P=0.005) compared to G/G carriers (r=−0.243, P=0.022). The reduced ADA activity associated to rs73598374-A variant predisposes those carriers to display higher levels of adenosine compared to G/G carriers. Consequently, it may lead to an accelerated process of replicative senescence, causing a stronger reduction of TA and in turn shorter LTL. In conclusion, the crucial role played by replicative senescence of the immune system in several human diseases and in the aging process underscores the relevance of the present findings and also spurs interest into the possible involvement of rs73598374 in shaping the susceptibility to several age-related diseases.
机译:最近的证据表明,腺苷脱氨酶(ADA)通过调节端粒酶活性(TA)的能力在T细胞复制性衰老中具有相关作用。本文中,我们通过测量根据rs73598374基因型选择的健康受试者的TA和白细胞端粒长度(LTL),测试了功能性多态性ADA rs73598374:G> A(c.22G> A,p.Asp8Asn)对端粒生物学的影响。与G / G载波相比,rs73598374-A载波分别显示出较低的TA(P = 0.019)和较短的LTL(P = 0.003)。与G / G载体(r = -0.243,P = 0.022)相比,rs73598374-A载体的LTL横截面年龄减小更强(r = -0.314,P = 0.005)。与rs73598374-A变体相关的ADA活性降低,使这些载体比G / G载体表现出更高水平的腺苷。因此,它可能导致复制衰老的加速过程,导致TA的降低更强,而LTL则更短。总之,免疫系统复制性衰老在几种人类疾病和衰老过程中所起的关键作用突显了本研究结果的相关性,也激发了人们对rs73598374可能参与形成对几种与年龄有关的疾病的易感性的兴趣。 。

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