AlprostadilvsPT-141

Alprostadil is synthetic prostaglandin E1 (PGE1), a 20-carbon oxygenated fatty acid derived from dihomo-gamma-linolenic acid (DGLA) through the cyclooxygenase pathway. It acts locally on penile vascular and trabecular smooth muscle through two prostaglandin E receptor subtypes: EP2 and EP4, both of which are Gs-coupled GPCRs that increase intracellular cAMP upon activation.

Elevated cAMP activates protein kinase A (PKA), which phosphorylates multiple targets in smooth muscle cells to produce relaxation. PKA phosphorylates myosin light chain kinase (MLCK), reducing its affinity for the calcium-calmodulin complex and decreasing its ability to phosphorylate myosin light chains — the final step in smooth muscle contraction. PKA also activates calcium-ATPase pumps and opens potassium channels, reducing intracellular calcium concentration. The net effect is relaxation of both the helicine arterioles (which supply blood to the corpora cavernosa) and the trabecular smooth muscle (which forms the spongy erectile tissue). As these relax, blood flows into the sinusoidal spaces of the corpora cavernosa, expanding the tissue against the tunica albuginea and compressing the subtunical veins — trapping blood and producing an erection.

The critical distinction of alprostadil's mechanism is its direct, local action independent of central sexual arousal pathways and independent of nitric oxide. PDE5 inhibitors (sildenafil, etc.) work by preventing cGMP breakdown downstream of nitric oxide release, which requires sexual arousal to generate the initial NO signal. Alprostadil generates its own second messenger (cAMP) at the injection site regardless of arousal state, which is why it produces erections reliably even in patients with neurogenic erectile dysfunction (spinal cord injury, radical prostatectomy) where the nerve-mediated NO pathway is damaged. The extremely rapid pulmonary metabolism (80% cleared in a single pass through the lungs) ensures that systemic effects are minimal when administered locally.

PT-141 (bremelanotide) is a cyclic heptapeptide derived from Melanotan II through targeted structural modification to shift receptor selectivity toward MC4R and away from MC1R. It was developed specifically to capture the sexual arousal effects observed with MT-II while minimizing the unwanted tanning (MC1R-mediated) effects. The result is a peptide that acts primarily on the central nervous system rather than peripheral vasculature.

PT-141 activates melanocortin 4 receptors (MC4R) in key brain regions involved in sexual function, particularly the medial preoptic area, the paraventricular nucleus of the hypothalamus, and descending autonomic pathways. MC4R is a Gs-coupled GPCR that increases intracellular cAMP, activating neural circuits that regulate sexual desire, arousal, and physiological sexual response. This central mechanism is fundamentally different from PDE5 inhibitors (sildenafil, tadalafil), which work peripherally by enhancing nitric oxide-mediated vasodilation in penile and clitoral erectile tissue. PDE5 inhibitors improve the mechanical response to arousal but do not affect desire; PT-141 acts upstream, enhancing the desire and arousal signals that originate in the brain.

In women with hypoactive sexual desire disorder (HSDD), PT-141 activates these hypothalamic sexual arousal circuits to increase desire, sexual arousal, and genital response. The nausea experienced by approximately 40% of users is attributed to MC4R activation in the area postrema (the vomiting center in the brainstem), which lies outside the blood-brain barrier and is therefore accessible to circulating peptides. The transient blood pressure elevation results from sympathetic nervous system activation downstream of hypothalamic MC4R signaling. PT-141 retains some residual MC1R activity, which can produce mild facial flushing, but at therapeutic doses the tanning effect is minimal compared to MT-II.