Erectile dysfunction in cardiovascular patients: A prospective study of the eNOS gene T‐786C, G894T, and INTRON variable number of the tandem repeat functional interaction

Author:

Segura Ana1,Muriel Javier2,Miró Pau3,Agulló Laura2,Arrarte Vicente4,Carracedo Patricia5,Zandonai Thomas26,Peiró Ana M27

Affiliation:

1. Urology Department, Andrology Unit Dr. Balmis General University Hospital Alicante Spain

2. Clinical Pharmacology Department Pharmacogenetic Unit Dr. Balmis General University Hospital, Alicante Institute for Health and Biomedical Research (ISABIAL) Alicante Spain

3. Department of Applied Statistics and Operational Research, and Quality Universitat Politecnica de València, Campus of Alcoi Plaza Ferrandiz y Carbonell s/n Alcoy Spain

4. Cardiology Department Dr. Balmis General University Hospital Alicante Spain

5. Department of Statistics and Applied Operational Research and Quality Universitat Politècnica de València Valencia Spain

6. Department of Psychology of Developmental and Socialization Processes “Sapienza” University of Rome Rome Italy

7. Clinical Pharmacology, Toxicology and Chemical Safety Unit Institute of Bioengineering Miguel Hernández University Avda. de la Universidad s/n Elche Spain

Abstract

AbstractBackgroundCardiovascular disease induces erectile dysfunction modulated by endothelial nitric oxide synthase enzyme and an impaired ejection fraction that restricts penis vascular congestion. However, the mechanisms regulating endothelial dysfunction are not understood.ObjectivesExploring the functional impact of endothelial nitric oxide synthase genetic polymorphisms on erectile dysfunction and drug therapy optimization in high‐risk cardiovascular disease patients.Materials and methodsPatients with erectile dysfunction symptoms and candidates for andrology therapy were included (n = 112). Clinical data and endothelial nitric oxide synthase rs1799983 (G894T) and rs2070744 (T‐786C), genotyped by fluorescence polarization assays, were registered. The 27‐bp variable number of the tandem repeat polymorphism in intron 4 (intron4b/a) was analyzed by polymerase chain reaction‐restriction fragment length polymorphism. Association analyses were run with the R‐3.2.0 software.ResultsA significant association between endothelial nitric oxide synthase 786‐TT (p = 0.005) and the aa/ac of intron 4 variable number of the tandem repeat (p = 0.02) with higher erectile dysfunction susceptibility was observed in cardiovascular disease patients (60 ± 9 years, 66% severe erectile dysfunction, 56% ejection fraction). After 3‐months of phosphodiesterase type 5 inhibitors, erectile dysfunction (International Index of Erectile Function, 50 ± 16 scores, the International Index of Erectile Function‐Erectile Function 21 ± 10 scores, p < 0.001) and sexual quality of life (modified Sexual Life Quality Questionnaire 55 ± 23 scores, p < 0.001) had significantly improved. The cardiovascular ejection fraction was influenced positively with better sexual quality of life (0.1941), and also in the endothelial nitric oxide synthase G894‐T allele (p = 0.076) carriers, which could merit future analyses. Erectile dysfunction was present as the primary clinical manifestation in 62% of cases, with cardiovascular disease occurring concurrently. Only former smokers and obese subjects debuted prior to cardiovascular disease than to erectile dysfunction.ConclusionsOur study provides comprehensive insights into the functional interaction linking endothelial nitric oxide synthase gene polymorphisms, erectile function, and ejection fraction in high‐risk cardiovascular disease patients. Future therapeutic strategies could target endothelial nitric oxide synthase activity by including lifestyle changes and epigenetic modulations.

Publisher

Wiley

Reference57 articles.

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