Angiotensin-Converting Enzyme in Systemic Sclerosis: From Endothelial Injury to a Genetic Polymorphism

doi:10.1196/annals.1351.002

The main pathologic hallmark of systemic sclerosis (SSc) isendothelial derangement; the pathologic alterations of the vesselwall in SSc are strikingly similar to the modification detectedin the atherosclerotic lesions, and it is now evident that SScis also characterized by accelerated macrovascular disease.Peptides related to angiotensin II, the final product of therenin–angiotensin system (RAS), play a role as regulatorsof endothelial cell function. Angiotensin-converting enzyme(ACE), the key enzyme in the RAS, is the predominant pathwayof angiotensin II formation in blood and tissues. In intron16 of the gene encoding for ACE an insertion/deletion (I/D)polymorphism, consisting of the presence or absence of a 287–basepair Alu sequence, has been identified. This polymorphism hasbeen related to ACE enzyme levels, and data from experimentalstudies reported a functional role for this polymorphism inmodulating the angiotensin II levels. We previously documenteda high ACE D allele frequency in SSc patients and its role inincreasing the risk of SSc, thus suggesting that the I/D polymorphismmight be a useful genetic marker to identify SSc patients atrisk to develop a severe vascular disease, frequently leadingto gangrene. Moreover, our preliminary data, besides supportingthe role of ACE I/D polymorphism as a predisposing factor toSSc, demonstrated its involvement in accelerated macrovasculardisease by increasing the intima media thickness. Therefore,in SSc, not only endothelial dysfunction, but also vasculardamage, linked to ACE I/D polymorphism, may significantly contributeto accelerated macrovascular disease, as the ACE D allele, byregulating both the production of angiotensin II and the degradationof bradykinin, contributes to mechanisms involved in the inductionand maintenance of vessel wall modification.