通过长期抑制 mTOR,延长 Apc Min/+ FAP 小鼠的寿命。

Aging pathobiology and therapeutics Pub Date : 2020-01-01 Epub Date: 2020-12-31 DOI:10.31491/apt.2020.12.039
Manish Parihar, Sherry G Dodds, Marty Javors, Randy Strong, Paul Hasty, Zelton Dave Sharp
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引用次数: 0

摘要

背景:Apc Min/+ 小鼠是家族性腺瘤性息肉病(FAP)的模型,这种疾病会导致大量结肠息肉,进而引发结肠直肠癌。我们以前的研究表明,用抗衰老药物雷帕霉素长期治疗 Apc Min/+ 雌性小鼠,可通过减少息肉病和预防贫血恢复正常寿命。野生型 UM-HET3 小鼠长期服用雷帕霉素后寿命的延长与性别有关,其中雌性小鼠获益最大。Apc Min/+ 小鼠对慢性 mTOR 抑制是否也有类似的性别依赖性反应尚不清楚:为了填补这一知识空白并深入了解慢性 mTOR 抑制如何预防肠息肉病,我们比较了雌雄 Apc Min/+ 小鼠对含雷帕霉素饮食的慢性治疗反应。给动物喂食含有 42 ppm 微胶囊雷帕霉素或空胶囊的食物,其中一组用于测定寿命,另一组在 16 周龄时接受类似处理,进行横断面研究:我们发现,在这种情况下,雄性的存活率高于雌性(P < 0.0197)。为了探索这种差异的潜在基础,我们分析了受慢性雷帕霉素影响的因素。免疫印迹检测显示,以核糖体蛋白 S6(rpS6)磷酸化作为间接测量指标,雄性和雌性的 mTORC1 抑制水平大致相同。rpS6磷酸化的免疫组化检测显示,雷帕霉素对mTORC1活性的抑制程度相同,最显著的差异是在雌雄两性的肠隐窝Paneth细胞中。慢性雷帕霉素还减少了雄性和雌性 Apc Min/+ 小鼠的隐窝深度(P < 0.0001),这与隐窝上皮细胞增殖减少一致。最后,慢性雷帕霉素对雄性和雌性小鼠贫血的预防作用相同:在雄性和雌性小鼠中,这些发现将雷帕霉素介导的肠息肉病预防与Paneth细胞中的mTORC1抑制和上皮细胞增殖减少联系起来。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Sex-dependent lifespan extension of Apc Min/+ FAP mice by chronic mTOR inhibition.

Background: Apc Min/+ mice model familial adenomatous polyposis (FAP), a disease that causes numerous colon polyps leading to colorectal cancer. We previously showed that chronic treatment of Apc Min/+ females with the anti-aging drug, rapamycin, restored a normal lifespan through reduced polyposis and anemia prevention. Lifespan extension by chronic rapamycin in wildtype UM-HET3 mice is sex-dependent with females gaining the most benefit. Whether Apc Min/+ mice have a similar sex-dependent response to chronic mTOR inhibition is not known.

Methods: To address this knowledge gap and gain deeper insight into how chronic mTOR inhibition prevents intestinal polyposis, we compared male and female Apc Min/+ mice responses to chronic treatment with a rapamycin-containing diet. Animals were fed a diet containing either 42 ppm microencapsulate rapamycin or empty capsules, one group was used to determine lifespan and a second group with similar treatment was harvested at 16 weeks of age for cross-sectional studies.

Results: We found that the survival of males is greater than females in this setting (P < 0.0197). To explore the potential basis for this difference we analyzed factors affected by chronic rapamycin. Immunoblot assays showed that males and females exhibited approximately the same level of mTORC1 inhibition using phosphorylation of ribosomal protein S6 (rpS6) as an indirect measure. Immunohistochemistry assays of rpS6 phosphorylation showed that rapamycin reduction of mTORC1 activity was on the same level, with the most prominent difference being in intestinal crypt Paneth cells in both sexes. Chronic rapamycin also reduced crypt depths in both male and female Apc Min/+ mice (P < 0.0001), consistent with reduced crypt epithelial cell proliferation. Finally, chronic rapamycin prevented anemia equally in males and females.

Conclusions: In males and females, these findings link rapamycin-mediated intestinal polyposis prevention with mTORC1 inhibition in Paneth cells and concomitant reduced epithelial cell proliferation.

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