Genetic and reproductive toxicity of lamivudine, tenofovir disoproxil fumarate, efavirenz and their combination in the bone marrow and testicular cells of male mice

A. Bakare, K. M. Akinseye, Bayonle Aminu, Francis C. Ofoegbu, Saheed O. Anifowose, Stork Abruda, Opeoluwa M. Fadoju, Olusegun I. Ogunsuyi, I. Oyeyemi, O. Alabi, O. M. Adetona, C. Alimba
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引用次数: 3

Abstract

Abstract The combination of antiretroviral (ARV) drugs: lamivudine, tenofovir disoproxil fumarate (TDF) and efavirenz is among the preferred first-line regimens for adolescents and adults infected with HIV. However, knowledge on in vivo genetic and reproductive toxicity of each of these drugs and their combination is limited. We evaluated the genotoxicity of lamivudine, TDF, efavirenz and their combination utilizing the mouse micronucleus (MN) and sperm morphology tests. Histopathological analysis of the testes of exposed mice was also carried out. 0.016, 0.032, 0.064 and 0.129 mg/kg bwt of lamivudine, TDF and the combination; and 0.032, 0.064, 0.129 and 0.259 mg/kg bwt of efavirenz corresponding to 0.125, 0.250, 0.500 and 1.000 x the human therapeutic daily dose (HTD) of each of the ARVs and their combinations were administered to mice for 5 consecutive days. Data on MN showed a significant increase (p < 0.05) across the tested doses of TDF, efavirenz and the combination, with the combination inducing lower frequency of MN than TDF and efavirenz. Lamivudine did not evoke significant induction of MN. Significant increase in frequency of abnormal sperm cells were observed in the tested samples, however, the combination induced the highest number of abnormal spermatozoa. The ARVs and their combination induced pathological lesions such as vacuolation and necrosis in mice testes. These findings suggest that the individual ARVs and their combination are potentially capable of activating genetic alterations in the bone marrow and germ cells of male mice thereby raising concern for long term use by HIV patients.
拉米夫定、富马酸替诺福韦二氧吡酯、依非韦伦及其联合用药对雄性小鼠骨髓和睾丸细胞的遗传和生殖毒性
抗逆转录病毒(ARV)药物:拉米夫定、富马酸替诺福韦二吡酯(TDF)和依非韦伦联合治疗是青少年和成人感染HIV的首选一线治疗方案之一。然而,关于每一种药物及其联合使用的体内遗传和生殖毒性的知识是有限的。我们利用小鼠微核(MN)和精子形态试验评估了拉米夫定、TDF、依非韦伦及其联合用药的遗传毒性。对暴露小鼠的睾丸进行了组织病理学分析。拉米夫定、TDF及联合用药0.016、0.032、0.064、0.129 mg/kg bwt;小鼠连续5天给予0.032、0.064、0.129和0.259 mg/kg bwt的依非韦伦,分别相当于每一种抗逆转录病毒药物及其联合药物的人治疗日剂量(HTD)的0.125、0.250、0.500和1.000倍。MN的数据显示,TDF、依非韦伦和联合用药剂量的MN显著增加(p < 0.05),其中联合用药诱导MN的频率低于TDF和依非韦伦。拉米夫定没有引起明显的MN诱导。在测试样本中观察到异常精子细胞的频率显著增加,然而,该组合诱导的异常精子数量最多。ARVs及其联合用药可引起小鼠睾丸空泡化、坏死等病理病变。这些发现表明,单个抗逆转录病毒药物及其组合可能能够激活雄性小鼠骨髓和生殖细胞中的遗传改变,从而引起对艾滋病毒患者长期使用的担忧。
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