Cytogenotoxicological defense of retinyl palmitate in the front damage of antineoplastics

Ricardo Melo de Carvalho , Rai Pablo de Sousa Aguiar , Muhammad Torequl Islam , Marcus Vinicius Oliveira Barros de Alencar , Ana Maria Oliveira Ferreira da Mata , Antonio Lima Braga , Josemar José da Silva Júnior , Leonardo da Rocha Sousa , Rosália Maria Tôrres de Lima , Márcia Fernanda Correia Jardim Paz , João Marcelo de Castro e Sousa , Ana Amélia de Carvalho Melo-Cavalcante
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引用次数: 7

Abstract

Cancer, the multifactorial pathology and to date is the most lethal causes of death in the world. Cyclophosphamide (CPA) and doxorubicin (DOX) are the individually or combindly used two anticancer drugs. The antineoplastic drugs-mediated genetic instability can be overcome by using antioxidants. The study evaluated the cytogenotoxic modulatory potentials of retinyl palmitate (RP) caused by CPA and DOX in Swiss mice. For this, adult Mus musculus of either sex were divided equally regarding to the gender. Toxicogenetic effects were induced by the intraperitoneal (i.p.) administration of the CPA (20 mg/kg) and/or DOX (2 mg/kg), following to test for comet assay and micronucleus test in bone marrow cells after 48 h (DOX) and 7 h (CPA) of the administration of RP (100 IU/kg). Both CPA and DOX significantly (p < 0.05) increased with the index and frequency of damages, clastogenic and/or aneugenic effects with the augmenting of micronuclei, demonstrating the cytotoxicity interference on the ratio of normochromatic to polychromatic erythrocytes and bone marrow cells of mice, that were found to reduce in RP treatment groups. In conclusion, RP has a modulatory effect on CPA and DOX-mediated cytogenotoxic events. The findings may be a good indication to manage the antioneoplastic drug-induced stress mediated detrimental effects by using RP, especially as a side effect minimizer.

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棕榈酸视黄醇在抗肿瘤前损伤中的细胞基因毒理学防御
癌症是一种多因素的病理学,迄今为止是世界上最致命的死亡原因。环磷酰胺(CPA)和阿霉素(DOX)是单独或联合使用的两种抗癌药物。抗肿瘤药物介导的遗传不稳定性可以通过使用抗氧化剂来克服。该研究评估了CPA和DOX在瑞士小鼠中引起的棕榈酸视黄酯(RP)的细胞遗传学毒性调节潜力。为此,成年Mus musculus的性别被平均划分。在RP(100 IU/kg)给药48小时(DOX)和7小时(CPA)后,通过腹膜内(i.p.)给药CPA(20 mg/kg)和/或DOX(2 mg/kg)进行彗星试验和骨髓细胞微核试验,诱导毒代效应。CPA和DOX均随损伤指数和频率的增加而显著增加(p<0.05),随着微核的增加而产生致染色体断裂和/或非整倍性效应,这表明对小鼠的常染色与多色红细胞和骨髓细胞比率的细胞毒性干扰,在RP治疗组中发现这种干扰减少。总之,RP对CPA和DOX介导的细胞遗传学毒性事件具有调节作用。这些发现可能是一个很好的指示,通过使用RP来管理抗肿瘤药物诱导的应激介导的有害影响,特别是作为一种副作用最小化剂。
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来源期刊
CiteScore
2.08
自引率
0.00%
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0
审稿时长
5.3 weeks
期刊介绍: Cessation. The international multidisciplinary journal is devoted to the publication of studies covering the whole range of experimental research on disease processes and toxicology including cell biological investigations. Its aim is to support progress in the interdisciplinary cooperation of researchers working in pathobiology, toxicology, and cell biology independent of the methods applied. During the past decades increasing attention has been paid to the importance of toxic influence in the pathogenesis of human and animal diseases. This is why Experimental and Toxicologic Pathology meets the urgent need for an interdisciplinary journal felt by a wide variety of experts in medicine and biology, including pathologists, toxicologists, biologists, physicians, veterinary surgeons, pharmacists, and pharmacologists working in academic, industrial or clinical institutions.
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