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Protective effects of Eugenia jambolana extract versus N‐acetyl cysteine against cisplatin‐induced damage in rat testis
Author(s) -
Anand H.,
Misro M. M.,
Sharma S. B.,
Prakash S.
Publication year - 2015
Publication title -
andrologia
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.633
H-Index - 59
eISSN - 1439-0272
pISSN - 0303-4569
DOI - 10.1111/and.12247
Subject(s) - glutathione , antioxidant , oxidative stress , testosterone (patch) , catalase , apoptosis , glutathione reductase , cisplatin , medicine , endocrinology , pharmacology , chemistry , andrology , biology , biochemistry , enzyme , glutathione peroxidase , chemotherapy
Summary To assess the protective effects of Eugenia jambolana extract ( EJE ) or N‐acetyl cysteine ( NAC ) on testis, cisplatin ( CIS , 5 mg kg −1 bw, single dose) was administered either alone or along with EJE (25 mg kg −1 bw, alternate day) or NAC (150 mg kg −1 bw, Day 1 and 4) for 7 days. Significant alterations in serum LH, FSH and testosterone were observed in CIS group which were effectively modulated by EJE or NAC supplementation. Upregulation of 3β‐HSD gene indicated the rise in functional Leydig cells. This was further confirmed from the identical improvement in hCG ‐stimulated testosterone production in isolated Leydig cells. Reduction in oxidative stress was associated with restoration of total antioxidant capacity and glutathione levels, and activation of antioxidant enzymes, SOD , catalase, glutathione s‐transferase ( GST ) and glutathione reductase ( GR ). CIS‐induced apoptosis of germ and Leydig cells was contained by both NAC and EJE intervention by effective modulation of apoptotic markers in the extrinsic, intrinsic and other pathways of metazoan apoptosis. Taken together, the study findings establish the potential of EJE as a therapeutically better antioxidant than NAC for use in curtailing the adverse effects of anticancer drugs on testicular function.