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全基因组搜索重复了循环血管紧张素I转换酶(ACE)数量性状基因座的证据,该基因座与ACE基因不连锁。

A genome-wide search replicates evidence of a quantitative trait locus for circulating angiotensin I-converting enzyme (ACE) unlinked to the ACE gene.

作者信息

McKenzie Colin A, Zhu Xiaofeng, Forrester Terrence E, Luke Amy, Adeyemo Adebowale A, Bouzekri Nourdine, Cooper Richard S

机构信息

Tropical Metabolism Research Unit, University of the West Indies, Kingston, Jamaica.

出版信息

BMC Med Genomics. 2008 Jun 10;1:23. doi: 10.1186/1755-8794-1-23.

Abstract

BACKGROUND

Angiotensin I-converting enzyme (ACE) plays an important role in cardiovascular homeostasis. There is evidence from different ethnic groups that circulating ACE levels are influenced by a quantitative trait locus (QTL) at the ACE gene on chromosome 17. The finding of significant residual familial correlations in different ethnic groups, after accounting for this QTL, and the finding of support for linkage to a locus on chromosome 4 in Mexican-American families strongly suggest that there may well be QTLs for ACE unlinked to the ACE gene.

METHODS

A genome-wide panel of microsatellite markers, and a panel of biallelic polymorphisms in the ACE gene were typed in Nigerian families. Single locus models with fixed parameters were used to test for linkage to circulating ACE with and without adjustment for the effects of the ACE gene polymorphisms.

RESULTS

Strong evidence was found for D17S2193 (Zmax = 3.5); other nearby markers on chromosome 17 also showed modest support. After adjustment for the effects of the ACE gene locus, evidence of "suggestive linkage" to circulating ACE was found for D4S1629 (Zmax = 2.2); this marker is very close to a locus previously shown to be linked to circulating ACE levels in Mexican-American families.

CONCLUSION

In this report we have provided further support for the notion that there are QTLs for ACE unlinked to the ACE gene; our findings for chromosome 4, which appear to replicate the findings of a previous independent study, should be considered strong grounds for a more detailed examination of this region in the search for genes/variants which influence ACE levels.The poor yields, thus far, in defining the genetic determinants of hypertension risk suggest a need to look beyond simple relationships between genotypes and the ultimate phenotype. In addition to incorporating information on important environmental exposures, a better understanding of the factors which influence the building blocks of the blood pressure homeostatic network is also required. Detailed studies of the genetic determinants of ACE, an important component of the renin-angiotensin system, have the potential to contribute to this strategic objective.

摘要

背景

血管紧张素I转换酶(ACE)在心血管稳态中起重要作用。来自不同种族群体的证据表明,循环ACE水平受17号染色体上ACE基因的一个数量性状位点(QTL)影响。在考虑该QTL后,不同种族群体中仍存在显著的残余家族相关性,以及墨西哥裔美国家庭中与4号染色体上一个位点连锁的证据,强烈提示可能存在与ACE基因不连锁的ACE的QTL。

方法

在尼日利亚家庭中对一组全基因组微卫星标记以及ACE基因中的一组双等位基因多态性进行分型。使用具有固定参数的单基因座模型来测试与循环ACE的连锁,同时调整或不调整ACE基因多态性的影响。

结果

发现D17S2193存在有力的连锁证据(Zmax = 3.5);17号染色体上其他附近的标记也显示出一定的支持。在调整ACE基因座的影响后,发现D4S1629与循环ACE存在“提示性连锁”的证据(Zmax = 2.2);该标记非常接近先前在墨西哥裔美国家庭中显示与循环ACE水平连锁的一个位点。

结论

在本报告中,我们进一步支持了存在与ACE基因不连锁的ACE的QTL这一观点;我们在4号染色体上的发现似乎重复了先前一项独立研究的结果,应被视为在寻找影响ACE水平的基因/变异时更详细检查该区域的有力依据。迄今为止,在确定高血压风险的遗传决定因素方面收获不佳,这表明需要超越基因型与最终表型之间的简单关系去探寻。除了纳入重要环境暴露的信息外,还需要更好地理解影响血压稳态网络组成部分的因素。对肾素 - 血管紧张素系统的重要组成部分ACE的遗传决定因素进行详细研究,有可能有助于实现这一战略目标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/52af/2442613/0cc18f9fa6fc/1755-8794-1-23-1.jpg

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