• The Journal of urology · Dec 2020

    Review

    The Role of Opioids and Their Receptors in Urological Malignancy: A Review.

    • Patrick M Lec, Andrew T Lenis, Vishnukamal Golla, Wayne Brisbane, Brian Shuch, Isla P Garraway, Robert E Reiter, and Karim Chamie.
    • Institute of Urologic Oncology, Department of Urology, David Geffen School of Medicine at UCLA, Los Angeles, California.
    • J. Urol. 2020 Dec 1; 204 (6): 1150-1159.

    PurposeWe reviewed the literature surrounding the role of opioids and their receptors in urological malignancy. Recent studies have suggested clinically significant effects of agonism or antagonism of opioid receptors on cancer related outcomes and tumorigenesis. The focus of these efforts has centered on nonurological malignancies. However, a compelling body of evidence is growing in the fields of prostate, bladder and kidney cancer.Materials And MethodsA systematic review of English language articles published through 2020 was conducted with key phrases related to kidney, bladder or prostate cancer, and opioids or narcotics. A total of 837 unique records were identified, of which 49 were selected for full text review and 33 were included in the qualitative analysis. Eight records were identified via citation review and 1 study was recently presented at a national meeting.ResultsRetrospective reviews suggest poorer disease specific and recurrence-free survival with increased perioperative opioid administration in patients undergoing prostate or bladder cancer surgery. However, the data are controversial. Kappa opioid receptors are implicated in both proliferation and inhibition of prostate cancer cell growth across in vitro studies, with a proposed interaction with the androgen cascade. Similarly opioid growth factor receptor is highly expressed in prostate cancer cells and repressed by androgens. Prostate cancer tissue stains more intensely for the mu opioid receptor, and patients with higher expression have poorer oncologic outcomes. Opioid agonism in vitro induces urothelial cell carcinoma proliferation, migration and invasion, with possible additional influence from interactions with the bradykinin b2 receptor. Agonism of the mu, kappa and delta opioid receptors induces renal cell carcinoma tumorigenesis, possibly via upregulation of survivin. Meanwhile, opioid growth factor receptor agonism has the opposite effect in renal cell carcinoma.ConclusionsEvidence surrounding the role of opioids and their receptors in urological malignancy is provocative and should serve as an impetus for further investigation.

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