AI Article Synopsis
- Androgens play a key role in regulating vascular function and structure, affecting the release of vasoactive factors like thromboxane A (TXA).
- Prostate cancer patients undergoing androgen deprivation therapies (ADTs) have higher TXA levels and increased cardiovascular mortality risk, as studied in the context of oxidative and inflammatory markers.
- Research finds that TXA negatively impacts the aortic function in male rats, leading to reduced vasodilation and increased vasoconstriction, highlighting the potential cardiovascular risks associated with increased TXA levels in PCa patients on ADT.
Article Abstract
Androgens have been described as important players in the regulation of vascular function/structure through their action on the release and effect of vasoactive factors, such as prostanoids. Patients with prostate cancer (PCa) under androgen deprivation therapies (ADTs) present increased risk of cardiovascular mortality. Since thromboxane A (TXA) is one of the most studied prostanoids and its involvement in different cardiovascular diseases has been described, the aim of this study was to investigate: (i) the effect of ADT on the serum levels of TXA in PCa patients and its possible link to the redox status and (ii) the effect of the non-hydrolyzable TXA analog U-46619 on the function of the aorta of male rats. The levels of TXA and total antioxidant status in 50 healthy subjects, 54 PCa patients, and 57 PCa under ADT were evaluated. These determinations were accompanied by levels of testosterone and C-reactive protein as an inflammation marker. In aortic segments from male rats, the U46619-induced effects on: (i) the vasomotor responses to acetylcholine (ACh), to the NO donor sodium nitroprusside (SNP), to the carbon monoxide-releasing molecule-3 (CORM-3), and to noradrenaline (NA) and (ii) the expression of cyclooxygenase-2 (COX-2), heme oxygenase-1 (HO-1), and phosphorylated ERK1/2 were analyzed. The serum level of TXA in patients with PCa was increased with respect to healthy subjects, which was further increased by ADT. There was no modification in the total antioxidant status among the three experimental groups. In aortic segments from male rats, the TXA analog decreased the endothelium-dependent relaxation and the sensitivity of smooth muscle cells to NO, while it increased the vasoconstriction induced by NA; the expression of COX-2, HO-1, and pERK1/2 was also increased. ADT increased, along with other inflammatory/oxidative markers, the serum levels of TXA. The fact that TXA negatively impacts the vascular function of the aorta of healthy male rats suggests that inhibition of TXA-mediated events could be considered a potential strategy to protect the cardiovascular system.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8076684 | PMC |
| http://dx.doi.org/10.3389/fcvm.2021.653126 | DOI Listing |
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