超稀释/动态化多柔比星可降低多柔比星对卵巢组织中的猪前卵泡体外培养产生的毒性。

IF 3.3 4区 医学 Q2 REPRODUCTIVE BIOLOGY
Ramyres Diego Lima de Andrade , Gaby Judith Quispe Palomino , Isabor Sales Marinho de Queiroz , Ana Flávia Bezerra da Silva , Anna Clara Accioly Ferreira , Bênner Geraldo Alves , Selene Maia de Morais , Ana Paula Ribeiro Rodrigues , Laritza Ferreira de Lima , José Ricardo de Figueiredo
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引用次数: 0

摘要

本研究探讨了在没有或有多柔比星(0.3µg/ml)诱导的化学应激的情况下,加入异体多柔比星(DOX 0.3µg/ml)、超稀释/动态化多柔比星的载体(0.2%乙醇)、不同动态化的超稀释/动态化多柔比星(DOX 6CH、DOX 12CH和DOX 30CH)对卵泡存活和活化、培养基抗氧化能力、过氧化氢酶活性(CAT)、活性蛋白硫醇的产生、I型和III型胶原纤维的维持以及I型和III型胶原蛋白硫醇的产生的影响。3µg/ml 对体外培养 48 小时的猪卵巢组织中的卵泡存活和活化、培养基的抗氧化能力、过氧化氢酶活性(CAT)、活性蛋白硫醇的产生、I 型和 III 型胶原纤维的维持以及脂褐素的积累有什么影响?为此,一部分卵巢组织片段被固定为未培养的对照组,其余的在以下条件下培养:MEM(培养对照组)、MEM(培养对照组)、MEM(培养对照组)、MEM(培养对照组):MEM(培养对照)、DOX 0.3µg/ml、乙醇、DOX 6CH、DOX 12CH、DOX 30CH、DOX(0.3µg/ml)+ DOX 6CH、DOX(0.3µg/ml)+ DOX 12CH、DOX(0.3µg/ml)+ DOX 30CH处理。结果表明,一般来说,超稀释/动态化多柔比星(DOX 6CH、DOX 12CH和DOX 30CH)可减轻对抗疗法多柔比星(0.3µg/ml)对前卵泡形态、I型和III型胶原纤维含量以及组织中脂褐素生成的毒性作用。然而,只有 DOX(0.3µg/ml)+ DOX 6CH 能减轻 DOX(0.3µg/ml)诱导的氧化应激,保持足够的 CAT 活性,与未培养的对照组相似。此外,当考虑到三种分离的超稀释/动态化多柔比星时,与未培养的对照组和 MEM 相比,只有 DOX 12CH 提高了还原型硫醇水平。总之,在体外培养封闭在卵巢组织中的猪前卵泡时,用超稀释/动态化 DOX(DOX 6CH、DOX 12CH 和 DOX 30CH)补充培养基可减轻异种多柔比星引起的毒性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Ultra-diluted/dynamized doxorubicin reduces the toxicity caused by doxorubicin during the in vitro culture of pig preantral follicles enclosed in ovarian tissue

The present study investigated the effect of adding allopathic doxorubicin (DOX 0.3 µg/mL), the vehicle of ultradiluted/dynamized doxorubicin (0.2 % ethanol), different dynamizations of ultradiluted/dynamized doxorubicin (DOX 6CH, DOX 12CH and DOX 30CH), both in the absence or presence of chemical stress induced by doxorubicin at 0.3 µg/mL on follicular survival and activation, antioxidant capacity of the medium, Catalase activity (CAT), production of reactive protein thiol, maintenance of type I and III collagen fibers and accumulation of lipofuscin in porcine ovarian tissue cultured in vitro for 48 hours. To do this, part of the ovarian tissue fragments was fixed for the uncultured control and the rest were cultured in: MEM (cultured control), DOX 0.3 µg/mL, Ethanol, DOX 6CH, DOX 12CH, DOX 30CH, DOX (0.3 µg/mL) + DOX 6CH, DOX (0.3 µg/mL) + DOX 12CH, DOX (0.3 µg/mL) + DOX 30CH treatments. The results showed that, in general, ultradiluted/dynamized doxorubicin (DOX 6CH, DOX 12CH and DOX 30CH) mitigated the toxic effect of allopathic doxorubicin (0.3 µg/mL) on the morphology of preantral follicles, the content of type I and III collagen fibers, and the production of lipofuscin in the tissue. However, only DOX (0.3 µg/mL) + DOX 6CH attenuated the oxidative stress induced by DOX (0.3 µg/mL), maintaining adequate CAT activity that was similar to the uncultured control. Additionally, when the three isolated ultradiluted/dynamized doxorubicin were considered, only DOX 12CH increased the reduced thiol levels compared to the uncultured control and MEM. In conclusion, supplementing the culture medium with ultradiluted/dynamized DOX (DOX 6CH, DOX 12CH and DOX 30CH) attenuated the toxicity induced by allopathic doxorubicin during the in vitro culture of pig preantral follicles enclosed in ovarian tissue.

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来源期刊
Reproductive toxicology
Reproductive toxicology 生物-毒理学
CiteScore
6.50
自引率
3.00%
发文量
131
审稿时长
45 days
期刊介绍: Drawing from a large number of disciplines, Reproductive Toxicology publishes timely, original research on the influence of chemical and physical agents on reproduction. Written by and for obstetricians, pediatricians, embryologists, teratologists, geneticists, toxicologists, andrologists, and others interested in detecting potential reproductive hazards, the journal is a forum for communication among researchers and practitioners. Articles focus on the application of in vitro, animal and clinical research to the practice of clinical medicine. All aspects of reproduction are within the scope of Reproductive Toxicology, including the formation and maturation of male and female gametes, sexual function, the events surrounding the fusion of gametes and the development of the fertilized ovum, nourishment and transport of the conceptus within the genital tract, implantation, embryogenesis, intrauterine growth, placentation and placental function, parturition, lactation and neonatal survival. Adverse reproductive effects in males will be considered as significant as adverse effects occurring in females. To provide a balanced presentation of approaches, equal emphasis will be given to clinical and animal or in vitro work. Typical end points that will be studied by contributors include infertility, sexual dysfunction, spontaneous abortion, malformations, abnormal histogenesis, stillbirth, intrauterine growth retardation, prematurity, behavioral abnormalities, and perinatal mortality.
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