Angiotensin-converting enzyme (ACE) haplotypes and cyclosporine A (CsA) response: a model of the complex relationship between ACE quantitative trait locus and pathological phenotypes

doi:10.1093/hmg/ddi238

Human Molecular Genetics Advance Access originally published online on July 7, 2005
Human Molecular Genetics 2005 14(16):2357-2367; doi:10.1093/hmg/ddi238

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Angiotensin-converting enzyme (ACE) haplotypes and cyclosporine A (CsA) response: a model of the complex relationship between ACE quantitative trait locus and pathological phenotypes

Paolo Catarsi²^,*, Roberto Ravazzolo³^,7, Francesco Emma⁴, Doriana Fruci⁵, Livio Finos⁶, Andrea Frau², Giacomo Morreale², Alba Carrea² and Gian Marco Ghiggeri¹^,2

¹Department of Nephrology, ²Laboratory of Pathophysiology of Uremia and ³Laboratory of Molecular Genetics, G. Gaslini Institute, Genova, ⁴Division of Nephrology and Dialysis and ⁵Laboratory of Cell Biology, Bambin Gesù Hospital, Roma and ⁶Faculty of Medicine, D.S.B.T.A. Section of Human Physiology, University of Ferrara, Ferrara, ⁷Department of Pediatrics and CEBR, University of Genova, Italy

^* To whom correspondence should be addressed at: Laboratory of Pathophysiology of Uremia, G. Gaslini Institute, Largo Gaslini 5, 16147 Genova, Italy. Tel: +39 010 5636 419; Fax: +39 010 395214; Email: pcatarsi{at}libero.it

Received May 6, 2005; Accepted June 29, 2005

It is highly controversial to define the role of angiotensin-convertingenzyme (ACE) polymorphisms in essential hypertension. We studieda group of patients in whom hypertension was the major sideeffect of treatment by cyclosporine A (CsA). This study groupcomprised 227 Italian patients with nephrotic syndrome, 103of which were treated with CsA and had different outcome. Forty-ninepatients developed serious hypertension that was reversed afterwithdrawal of drug. ACE haplotypes were determined by a combinationof molecular and statistical methods after verifying genotypesof six intragenic single nucleotide polymorphisms in 304 Italianblood donors and assembling them in clades (A, B, C) that include95% of observed haplotypes. The association between ACE cladecombinations and serum enzymatic levels confirmed the previousresults about a role of an unidentified genetic variant at the5' of the intragenic recombination site located near intron7. ACE clades were then determined in patients, and regressionmethods were used to analyze variables associated with CsA responsivityand progression to renal failure. ACE genotype and responsivenessto CsA were strictly associated, because homozygosis for ACEB clade was able to influence CsA sensitivity. This highlightsthe role of 5' variants, which differentiate clades B and C.Other genetic markers were tested to search for possible additiveeffects. We found that PAI-1 4G allele was associated with progressionto renal failure in the group of CsA-treated patients. Our resultsare in agreement with the hypothesis, raised after experimentalresults obtained in mouse models, that the effect of ACE polymorphismson blood pressure is detectable once environmental factors,like CsA treatment in our case, overcome physiological homeostaticmechanisms.

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