在老鼠中,围产期暴露于高亲和力人 PPARα 激动剂对肝癌形成的影响中,鼠与人 PPARα 之间的种属差异。
Species Differences between Mouse and Human PPARα in Modulating the Hepatocarcinogenic Effects of Perinatal Exposure to a High-Affinity Human PPARα Agonist in Mice.
机构信息
Department of Veterinary and Biomedical Sciences and Center for Molecular Toxicology and Carcinogenesis, The Pennsylvania State University, University Park, Pennsylvania 16802, USA.
Department of Environmental Sciences and Engineering, University of North Carolina, Chapel Hill, North Carolina 27599, USA.
出版信息
Toxicol Sci. 2021 Aug 30;183(1):81-92. doi: 10.1093/toxsci/kfab068.
Evidence suggests that species differences exist between rodents and humans in their biological responses to ligand activation of PPARα. Moreover, neonatal/postnatal rodents may be more sensitive to the effects of activating PPARα. Thus, the present studies examined the effects of chronic ligand activation of PPARα initiated during early neonatal development and continued into adulthood on hepatocarcinogenesis in mice. Wild-type, Ppara-null, or PPARA-humanized mice were administered a potent, high-affinity human PPARα agonist GW7647, and cohorts of mice were examined over time. Activation of PPARα with GW7647 increased expression of known PPARα target genes in liver and was associated with hepatomegaly, increased hepatic cytotoxicity and necrosis, increased expression of hepatic MYC, and a high incidence of hepatocarcinogenesis in wild-type mice. These effects did not occur or were largely diminished in Ppara-null and PPARA-humanized mice, although background levels of hepatocarcinogenesis were also noted in both Ppara-null and PPARA-humanized mice. More fatty change (steatosis) was also observed in both Ppara-null and PPARA-humanized mice independent of GW7647 administration. Results from these studies indicate that the mouse PPARα is required to mediate hepatocarcinogenesis induced by GW7647 in mice and that activation of the human PPARα with GW7647 in PPARA-humanized mice are diminished compared with wild-type mice. Ppara-null and PPARA-humanized mice are valuable tools for examining species differences in the mechanisms of PPARα-induced hepatocarcinogenesis, but background levels of liver cancer observed in aged Ppara-null and PPARA-humanized mice must be considered when interpreting results from studies that use these models. These results also demonstrate that early life exposure to a potent human PPARα agonist does not enhance sensitivity to hepatocarcinogenesis.
有证据表明,在配体激活 PPARα 后,啮齿动物和人类的生物学反应存在种属差异。此外,新生/产后啮齿动物可能对激活 PPARα 的作用更敏感。因此,本研究探讨了在新生期早期开始并持续到成年期持续激活 PPARα 对小鼠肝癌发生的影响。使用一种有效的、高亲和力的人类 PPARα 激动剂 GW7647 对野生型、Ppara 基因敲除型或 PPARA 人源化小鼠进行处理,并随时间检查小鼠的队列。GW7647 激活 PPARα 可增加肝脏中已知的 PPARα 靶基因的表达,并与肝肿大、肝毒性和坏死增加、肝 MYC 表达增加以及野生型小鼠肝癌的高发率相关。这些影响在 Ppara 基因敲除型和 PPARA 人源化小鼠中没有发生或大部分减弱,尽管在这两种小鼠中也观察到背景水平的肝癌发生。在 Ppara 基因敲除型和 PPARA 人源化小鼠中,也观察到更多的脂肪变化(脂肪变性),而与 GW7647 的给药无关。这些研究结果表明,在小鼠中,PPARα 是 GW7647 诱导肝癌所必需的,并且在 PPARA 人源化小鼠中,GW7647 激活人 PPARα 的作用与野生型小鼠相比减弱。Ppara 基因敲除型和 PPARA 人源化小鼠是研究 PPARα 诱导的肝癌发生机制中种属差异的有价值的工具,但在解释使用这些模型的研究结果时,必须考虑到在老年 Ppara 基因敲除型和 PPARA 人源化小鼠中观察到的肝癌背景水平。这些结果还表明,早期暴露于有效的人类 PPARα 激动剂不会增强对肝癌发生的敏感性。
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