Histomorphometric effects of Kigelia africana (Bignoniaceae) fruit extract on the testis following short-term treatment with cisplatin in male Sprague–Dawley rats

O.O. Azu; F.I.O. Duru; A.A. Osinubi; A.A. Oremosu; C.C. Noronha; S.O. Elesha; A.O. Okanlawon

doi:10.1016/j.mefs.2010.07.001

Middle East Fertility Society Journal (Jul 2010)

Histomorphometric effects of Kigelia africana (Bignoniaceae) fruit extract on the testis following short-term treatment with cisplatin in male Sprague–Dawley rats

O.O. Azu,
F.I.O. Duru,
A.A. Osinubi,
A.A. Oremosu,
C.C. Noronha,
S.O. Elesha,
A.O. Okanlawon

Affiliations

O.O. Azu: Department of Anatomy, College of Medicine, P.M.B. 12003, Idi-araba, Lagos, Nigeria
F.I.O. Duru: Department of Anatomy, College of Medicine, P.M.B. 12003, Idi-araba, Lagos, Nigeria
A.A. Osinubi: Department of Anatomy, College of Medicine, P.M.B. 12003, Idi-araba, Lagos, Nigeria
A.A. Oremosu: Department of Anatomy, College of Medicine, P.M.B. 12003, Idi-araba, Lagos, Nigeria
C.C. Noronha: Department of Anatomy, College of Medicine, P.M.B. 12003, Idi-araba, Lagos, Nigeria
S.O. Elesha: Department of Morbid Anatomy, College of Medicine of the University of Lagos, Nigeria
A.O. Okanlawon: Department of Anatomy, College of Medicine, P.M.B. 12003, Idi-araba, Lagos, Nigeria

DOI: https://doi.org/10.1016/j.mefs.2010.07.001
Journal volume & issue: Vol. 15, no. 3
pp. 200 – 208

Abstract

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Objective: To investigate the short-term effects of Kigelia africana fruit extract (KAFE) on cisplatin-induced testicular histo-morphometric changes in Sprague–Dawley (SD) rats. Design: This is an experimental animal study. Materials and methods: Fifty-seven male SD rats were acclamatized and grouped into 10 of five rats per group. Each rat was administered either KAFE in 100 and 500mg/kg doses orally or cisplatin 10mg/kg i.p. or normal saline to controls. Experiment was terminated after 28days by i.p. injection of ketamin 50mg/kg. Testicular tissue was processed for histological and morphometric analyses while catalase enzyme activity, lipid peroxidation and glutathione levels were assayed accordingly. Sperm count/motility was also assessed. Results: Cisplatin treatment caused over 37.5% mortality of SD rats. Qualitative histological assessment showed no deleterious changes following treatment with KAFE alone or as a pre-treatment with cisplatin. KAFE post-treatment resulted in focal vacuolar changes in the seminiferous tubules (ST) of the SD rats. Cisplatin-treatment negatively affected the histoarchitecture of the seminiferous tubules with massive loss of spermatogenic cells. There was also a significant reduction in testicular weight/volume, ST diameter and cross-sectional areas (P<0.001) but KAFE positively improved these parameters. KAFE alone and as prophylaxis significantly increased body weight, serum testosterone and follicle-stimulating hormone (P<0.001). It showed a significant elevation in catalase activity, decline in malondialdehyde and up-regulated glutathione levels (P<0.001). These parameters were negatively affected by cisplatin treatment. Conclusion: The cytoprotection against cisplatin-induced testicular damage by KAFE is likely via an antioxidant modulatory pathway. Also, it is possible that KAFE possesses an androgen-stimulating property.

Published in Middle East Fertility Society Journal

ISSN: 1110-5690 (Print); 2090-3251 (Online)
Publisher: SpringerOpen
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General); Science: Biology (General): Reproduction
Website: https://mefj.springeropen.com

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