Angiotensin-Converting Enzyme in Systemic Sclerosis

:  The main pathologic hallmark of systemic sclerosis (SSc) is endothelial derangement; the pathologic alterations of the vessel wall in SSc are strikingly similar to the modification detected in the atherosclerotic lesions, and it is now evident that SSc is also characterized by accelerated macrova...

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Bibliographic Details
Published in:Annals of the New York Academy of Sciences 2006-06, Vol.1069 (1), p.10-19
Main Authors: GUIDUCCI, SERENA, FATINI, CINZIA, ROGAI, VERONICA, CINELLI, MARINA, STICCHI, ELENA, ABBATE, ROSANNA, CERINIC, MARCO MATUCCI
Format: Article
Language:English
Subjects:
ACE
angiotensin
angiotensin-converting enzyme
atherosclerosis
macrovascular disease
polymorphism
renin-angiotensin system
systemic sclerosis
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Summary::  The main pathologic hallmark of systemic sclerosis (SSc) is endothelial derangement; the pathologic alterations of the vessel wall in SSc are strikingly similar to the modification detected in the atherosclerotic lesions, and it is now evident that SSc is also characterized by accelerated macrovascular disease. Peptides related to angiotensin II, the final product of the renin–angiotensin system (RAS), play a role as regulators of endothelial cell function. Angiotensin‐converting enzyme (ACE), the key enzyme in the RAS, is the predominant pathway of angiotensin II formation in blood and tissues. In intron 16 of the gene encoding for ACE an insertion/deletion (I/D) polymorphism, consisting of the presence or absence of a 287–base pair Alu sequence, has been identified. This polymorphism has been related to ACE enzyme levels, and data from experimental studies reported a functional role for this polymorphism in modulating the angiotensin II levels. We previously documented a high ACE D allele frequency in SSc patients and its role in increasing the risk of SSc, thus suggesting that the I/D polymorphism might be a useful genetic marker to identify SSc patients at risk to develop a severe vascular disease, frequently leading to gangrene. Moreover, our preliminary data, besides supporting the role of ACE I/D polymorphism as a predisposing factor to SSc, demonstrated its involvement in accelerated macrovascular disease by increasing the intima media thickness. Therefore, in SSc, not only endothelial dysfunction, but also vascular damage, linked to ACE I/D polymorphism, may significantly contribute to accelerated macrovascular disease, as the ACE D allele, by regulating both the production of angiotensin II and the degradation of bradykinin, contributes to mechanisms involved in the induction and maintenance of vessel wall modification.
ISSN:0077-8923
1749-6632
DOI:10.1196/annals.1351.002