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评估多拉韦林诱导幼年大鼠发育性免疫毒性的理论风险。

Assessing a theoretical risk of dolutegravir-induced developmental immunotoxicity in juvenile rats.

机构信息

GlaxoSmithKline, Research Triangle Park, North Carolina 27709-3398, USA.

出版信息

Toxicol Sci. 2012 Nov;130(1):70-81. doi: 10.1093/toxsci/kfs220. Epub 2012 Jul 12.

DOI:10.1093/toxsci/kfs220
PMID:22790968
Abstract

HIV-1 integrase inhibitors (INIs) are a promising class of antiretrovirals for the treatment of HIV in adults; there is interest in expanding their use into pediatric populations. A theoretical concern for developmental immunotoxicity was raised after a publication suggested that two HIV INI tool compounds inhibited in vitro cleavage activity of recombination activating genes 1 and 2 (RAG1/2) through the inhibition of their binding to recombination signal sequences. RAG1/2 are required for the development of mature B and T lymphocyte populations. The potential effects of the investigational INI dolutegravir on RAG1/2 were addressed by developing assays in juvenile rats to measure T cell receptor (TCR) Vβ usage by flow cytometry as an indicator of TCR repertoire diversity and a T cell dependent antibody response (TDAR) as an indicator of immunosuppression. These endpoints were incorporated into a juvenile rat toxicity study, along with immunophenotyping, hematology, and histopathology of immunologic organs. Dose levels of 0, 0.5, 2, or 75mg/kg/day dolutegravir were given via oral gavage from postnatal day 4 through 66. At the highest dose, there was decreased body weight gain and two preweanling deaths; however, there were no treatment-related effects on developmental parameters. There were no effects on immunologic competence, as measured by TDAR, and no effects on lymphocyte subsets or CD4 and CD8 TCR Vβ usage in peripheral blood. Histopathology of immunologic organs (spleen, thymus, lymph nodes) and hematology evaluation revealed no effects. The no observed adverse effect level for immunotoxicity endpoints was 75mg/kg/day.

摘要

HIV-1 整合酶抑制剂(INIs)是治疗成人 HIV 的一类有前途的抗逆转录病毒药物;人们有兴趣将其应用扩展到儿科人群。在一篇出版物表明两种 HIV INI 工具化合物通过抑制其与重组信号序列的结合来抑制重组激活基因 1 和 2(RAG1/2)的体外切割活性后,人们对发育免疫毒性提出了理论上的担忧。RAG1/2 是成熟 B 和 T 淋巴细胞群体发育所必需的。通过在幼年大鼠中开发测定法来测量 T 细胞受体(TCR)Vβ 的使用,以作为 TCR 库多样性的指标,并作为免疫抑制的指标来测量 T 细胞依赖性抗体反应(TDAR),从而研究了研究性 INI 地达格鲁韦对 RAG1/2 的潜在影响。这些终点与免疫表型,免疫器官的血液学和组织病理学一起纳入了幼年大鼠毒性研究。通过口服灌胃,从出生后第 4 天到 66 天,给予 0、0.5、2 或 75mg/kg/天的地达格鲁韦。在最高剂量下,体重增加减少,有两只新生期死亡;但是,发育参数没有治疗相关的影响。TDAR 测量的免疫能力没有受到影响,外周血中淋巴细胞亚群或 CD4 和 CD8 TCR Vβ 的使用也没有受到影响。免疫器官(脾脏,胸腺,淋巴结)的组织病理学和血液学评估未发现任何影响。免疫毒性终点的无观察到不良效应水平为 75mg/kg/天。

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