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百岁老人血管紧张素I转换酶的血浆浓度、动力学常数及基因多态性

Plasma concentration, kinetic constants, and gene polymorphism of angiotensin I-converting enzyme in centenarians.

作者信息

Faure-Delanef L, Baudin B, Bénéteau-Burnat B, Beaudoin J C, Giboudeau J, Cohen D

机构信息

Fondation Jean Dausset CEPH, Paris, France.

出版信息

Clin Chem. 1998 Oct;44(10):2083-7.

PMID:9761238
Abstract

We have determined serum activity and kinetic constants of angiotensin I-converting enzyme (ACE), parallel to an insertion/deletion (I/D) polymorphism in its gene, in French centenarians and controls 20-70 years of age because this enzyme could have an impact on cardiovascular risk, and thus on longevity. Both the ACE D allele and ACE D/D genotype were more frequent in centenarians in comparison with controls, without sex-related differences nor significant correlation with a cardiovascular pathology. In centenarians, I/D polymorphism was correlated with circulating ACE activity (D/D genotype, 89.0 +/- 36.8 U/L; I/D genotype, 63.5 +/- 26.0 U/L; and I/I genotype, 55.1 +/- 39.4 U/L). The Michaelis constants for two substrates were identical whatever the genotype and were not different between centenarians and controls, i.e., 0.30 +/- 0.03 mmol/L for furylacryloyl-phenylalanyl-glycyl-glycine and 1.35 +/- 0.05 mmol/L for hippuryl-histidyl-leucine; for the latter, the optimal pH and activating concentration of chloride did not depend on I/D polymorphism. The maximal velocities with both substrates reflected the distribution of serum ACE activity as a function of the genotypes, in centenarians and in controls. In conclusion, plasma ACE activity is subject to a similar genotypic influence in centenarians as in adults 20-70 years of age; however, ACE itself appears to be functionally similar for each genotype. Furthermore, the D allele as well as the higher serum ACE activities associated with the D/D genotype cannot discriminate individuals at high risk for cardiovascular diseases, major causes of mortality before the age of 100 years.

摘要

我们测定了法国百岁老人和20至70岁对照组人群中血管紧张素I转换酶(ACE)的血清活性及动力学常数,并同时研究了该酶基因中的插入/缺失(I/D)多态性,因为这种酶可能会影响心血管风险,进而影响寿命。与对照组相比,百岁老人中ACE D等位基因和ACE D/D基因型更为常见,且无性别差异,也与心血管疾病无显著相关性。在百岁老人中,I/D多态性与循环ACE活性相关(D/D基因型,89.0±36.8 U/L;I/D基因型,63.5±26.0 U/L;I/I基因型,55.1±39.4 U/L)。无论基因型如何,两种底物的米氏常数相同,百岁老人和对照组之间也无差异,即对于呋喃丙烯酰 - 苯丙氨酰 - 甘氨酰 - 甘氨酸为0.30±0.03 mmol/L,对于马尿酸 - 组氨酰 - 亮氨酸为1.35±0.05 mmol/L;对于后者,最佳pH值和氯化物激活浓度不依赖于I/D多态性。两种底物的最大反应速度反映了百岁老人和对照组中血清ACE活性随基因型的分布情况。总之,百岁老人血浆ACE活性受基因型影响与20至70岁成年人相似;然而,ACE本身在各基因型中功能似乎相似。此外,D等位基因以及与D/D基因型相关的较高血清ACE活性并不能区分心血管疾病高危个体,而心血管疾病是100岁前主要的死亡原因。

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