Abstract
Penile erection is a neurovascular event and neurologic or vascular disturbances are major causes of erectile dysfunction (ED). Radical prostatectomy for prostate cancer not only induces cavernous nerve injury (CNI) but also results in cavernous angiopathy, which is responsible for poor responsiveness to oral phosphodiesterase-5 inhibitors. Dickkopf2 (DKK2) is known as a Wnt signaling antagonist and is reported to promote mature and stable blood vessel formation. Here, we demonstrated in CNI mice that overexpression of DKK2 by administering DKK2 protein or by using DKK2-Tg mice successfully restored erectile function: this recovery was accompanied by enhanced neural regeneration through the secretion of neurotrophic factors, and restoration of cavernous endothelial cell and pericyte content. DKK2 protein also promoted neurite outgrowth in an ex vivo major pelvic ganglion culture experiment and enhanced tube formation in primary cultured mouse cavernous endothelial cells and pericytes co-culture system in vitro. In light of critical role of neuropathy and angiopathy in the pathogenesis of radical prostatectomy-induced ED, reprogramming of damaged erectile tissue toward neurovascular repair by use of a DKK2 therapeutic protein may represent viable treatment option for this condition.
Highlights
Penile erection is a neurovascular event and neurologic or vascular disturbances are major causes of erectile dysfunction (ED)
Functional and structural impairments of neuronal cells, endothelial cells, and pericytes are involved in the pathogenesis of erectile dysfunction (ED)[1,2], a condition defined as an inability to attain or maintain penile erection sufficient for satisfactory sexual intercourse[3]
New treatment strategies that correct cavernous nerve damage as well as vascular dysfunction are necessary for patients with radical prostatectomy-induced ED to overcome the limitation of PDE5 inhibitors
Summary
Penile erection is a neurovascular event and neurologic or vascular disturbances are major causes of erectile dysfunction (ED). Dickkopf[2] (DKK2) is known as a Wnt signaling antagonist and is reported to promote mature and stable blood vessel formation. We demonstrated in CNI mice that overexpression of DKK2 by administering DKK2 protein or by using DKK2-Tg mice successfully restored erectile function: this recovery was accompanied by enhanced neural regeneration through the secretion of neurotrophic factors, and restoration of cavernous endothelial cell and pericyte content. Immunophilin ligands have been shown to induce recovery of erectile function at the preclinical level[13], a clinical trial in men radical prostatectomy-induced ED failed to show the recovery of erectile function[14] This finding may imply that functional and structural derangements in erectile tissue, such as endothelial cell apoptosis and fibrosis, www.nature.com/scientificreports/. The effect of DKK2 on nervous system and erectile function has not yet been explored
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