Synthesis of Novel Androstane-N-Cyclohexyl-17-Carboxamides, and Their Effect on the 5α-Reductase Isoform 2, the Androgen Receptor, and Androgen-Dependent Glands

Juan C. Lopez-Lezama; Marisa Cabeza; Yvonne Heuze; Araceli Sánchez; José L. Rojas; Norma A. Valencia-Islas

doi:10.34172/PS.2021.74

Pharmaceutical Sciences (Jul 2022)

Synthesis of Novel Androstane-N-Cyclohexyl-17-Carboxamides, and Their Effect on the 5α-Reductase Isoform 2, the Androgen Receptor, and Androgen-Dependent Glands

Juan C. Lopez-Lezama,
Marisa Cabeza,
Yvonne Heuze,
Araceli Sánchez,
José L. Rojas,
Norma A. Valencia-Islas

Affiliations

Juan C. Lopez-Lezama: Universidad Nacional de Colombia, Sede Bogotá, Facultad de Ciencias, Departamento de Farmacia. Cra. 30 No. 45-03, Bogotá, Colombia.
Marisa Cabeza: Departamento de Sistemas Biológicos, Universidad Autónoma Metropolitana-Xochimilco, Calzada del Hueso #1100. Colonia Villa Quietud, CP 04960, Ciudad de México, México.
Yvonne Heuze: Departamento de Producción Agrícola y Animal, Universidad Autónoma Metropolitana-Xochimilco, Calzada del Hueso 1100. Col. Villa Quietud, 04960 Ciudad de México, México.
Araceli Sánchez: Departamento de Sistemas Biológicos, Universidad Autónoma Metropolitana-Xochimilco, Calzada del Hueso #1100. Colonia Villa Quietud, CP 04960, Ciudad de México, México.
José L. Rojas: Universidad Nacional de Colombia, Sede Bogotá, Facultad de Ciencias, Departamento de Química. Cra. 30 No. 45-03, Bogotá, Colombia.
Norma A. Valencia-Islas: Universidad Nacional de Colombia, Sede Bogotá, Facultad de Ciencias, Departamento de Farmacia. Cra. 30 No. 45-03, Bogotá, Colombia.

DOI: https://doi.org/10.34172/PS.2021.74
Journal volume & issue: Vol. 28, no. 3
pp. 433 – 442

Abstract

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Background: Benign Prostatic Hyperplasia (BPH), and Prostate Cancer (PCa) are androgen-dependent diseases. PPCa is associated with excessive signalling of the androgen receptor (AR) due to the binding of 5α-dihydrotestosterone (5α-DHT) and testosterone (T). BPH is related to high levels of 5α-DHT, biosynthesized from T by 5α-reductase (5RD5A). The inhibition of 5RD5A and the blockage of AR are targets for their treatment. In this study, the synthesis and determination of biological activity of the new N-cyclohexyl-3β-hydroxyandrosta-5,16- diene-17-carboxamide (6), N-cyclohexyl-3-oxoandrosta-4,6,16-triene-17-carboxamide (7), and N-cyclohexyl-3-oxoandrosta-4,16-diene-17-carboxamide (8) were carried out to find new drugs to improve these afflictions. Methods: The synthesis of 6 to 8 was confirmed by spectroscopic and spectrometric analyses. Competitive binding assays determined the affinity of 6 to 8 to the AR. The inhibitory activity of 5RD5A isoform 2 (5RD5A2) (IC50) was established by the conversion of [3 H]-T to [3 H]-5α-DHT and it was compared with finasteride (FIN). The pharmacological effect of 6 to 8 was determined on the weight of the prostate and seminal vesicles glands of castrated hamsters treated with T, and on the diameter size of their flank organs. Results: Compounds 7 and 8 bound lightly (ca. 15 %) to AR. Comparing to FIN (IC50 = 8.5 nM), 6 to 8 (IC50 = 0.169, 0.105 and 0.155 nM, respectively) showed higher potency as inhibitors of 5RD5A2. Compound 6 decreased the prostate and seminal vesicles weight, as well as the hamsters’ diameter flank organs. However, 7 only decreased the diameter of flank organs. Surprisingly, 8 increased these pharmacological parameters. Conclusion: Androstane-17-caboxamide 6 is a 5RD5A2 inhibitor that reduces the weight of androgen-dependent glands such as the prostate, suggesting it could be a lead for new drugs to treat BPH and PCa.

Published in Pharmaceutical Sciences

ISSN: 2383-2886 (Online)
Publisher: Tabriz University of Medical Sciences
Country of publisher: Iran, Islamic Republic of
LCC subjects: Medicine: Pharmacy and materia medica
Website: https://ps.tbzmed.ac.ir/

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