Endogenous testosterone increases L-type Ca2+ channel expression in porcine coronary smooth muscle

Abstract

Evidence indicates that gender and sex hormonal status influence cardiovascular physiology and pathophysiology. We recently demonstrated increased L-type voltage-gated Ca²⁺ current ( I_Ca,L) in coronary arterial smooth muscle (CASM) of male compared with female swine. The promoter region of the L-type voltage-gated Ca²⁺ channel (VGCC) (Ca_v1.2) gene contains a hormone response element that is activated by testosterone. Thus the purpose of the present study was to determine whether endogenous testosterone regulates CASM I_Ca,L through regulation of VGCC expression and activity. Sexually mature male and female Yucatan swine (7–8 mo; 35–45 kg) were obtained from the breeder. Males were left intact (IM, n = 8), castrated (CM, n = 8), or castrated with testosterone replacement (CMT, n = 8; 10 mg/day Androgel). Females remained gonad intact ( n = 8). In right coronary arteries, both Ca_v1.2 mRNA and protein were greater in IM compared with intact females. Ca_v1.2 mRNA and protein were reduced in CM compared with IM and restored in CMT. In isolated CASM, both peak and steady-state I_Ca were reduced in CM compared with IM and restored in CMT. In males, a linear relationship was found between serum testosterone levels and I_Ca. In vitro, both testosterone and the nonaromatizable androgen, dihydrotestosterone, increased Ca_v1.2 expression. Furthermore, this effect was blocked by the androgen receptor antagonist cyproterone. We conclude that endogenous testosterone is a primary regulator of Ca_v1.2 expression and activity in coronary arteries of males.