日间暴露于室内过热环境对老年人自噬和细胞应激反应的影响。

James J McCormick, Robert D Meade, Kelli E King, Ashley P Akerman, Sean R Notley, Nathalie V Kirby, Ronald J Sigal, Glen P Kenny
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引用次数: 0

摘要

为了在热浪期间保护弱势群体,公共卫生机构建议将室内空气温度保持在 24-28°C 以下。虽然我们最近证明,保持室内温度≤26°C可减轻老年人高热和心血管负荷的发展,但对长时间室内热应激的细胞后果却知之甚少。因此,我们对 16 名 66-78 岁的成年人(6 名女性)在模拟 22°C (对照组)和 26°C(卫生机构建议的室内温度上限)环境条件下休息 8 小时期间的细胞应激反应进行了评估。采用 Western 印迹分析法评估暴露前后采集的外周血单核细胞中与细胞应激反应相关的蛋白质(自噬、细胞凋亡、急性炎症和热休克蛋白)的变化。暴露 8 小时后,与细胞应激反应相关的蛋白质在 26°C 和 22°C 条件下没有显著差异(全部,P≥0.056)。相比之下,与 22°C 相比,暴露于 31°C (p62:1.5 倍;P=0.003)和 36°C (LC3-II、LC3-II/I、p62;均≥2.0 倍;P≤0.002)后自噬相关蛋白升高。这些反应伴随着 31°C 和 36°C 条件下凋亡信号的升高(裂解的天冬酶-3:分别为 1.8 倍和 3.7 倍;P≤0.002)。此外,与 22°C 条件相比,36°C 条件下的 HSP90 明显减少(0.7 倍;P=0.014)。我们的研究结果表明,老年人在长时间暴露于较高的环境温度时会承受相当大的细胞压力,因此我们建议将室内温度保持在≤26°C,以防止易受热人群出现生理应激反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of daylong exposure to indoor overheating on autophagy and the cellular stress response in older adults.

To protect vulnerable populations during heat waves, public health agencies recommend maintaining indoor air temperature below ∼24-28 °C. While we recently demonstrated that maintaining indoor temperatures ≤26 °C mitigates the development of hyperthermia and cardiovascular strain in older adults, the cellular consequences of prolonged indoor heat stress are poorly understood. We therefore evaluated the cellular stress response in 16 adults (six females) aged 66-78 years during 8 h rest in ambient conditions simulating homes maintained at 22 °C (control) and 26 °C (indoor temperature upper limit proposed by health agencies), as well as non-air-conditioned domiciles during hot weather and heat waves (31 and 36 °C, respectively; all 45% relative humidity). Western blot analysis was used to assess changes in proteins associated with the cellular stress response (autophagy, apoptosis, acute inflammation, and heat shock proteins) in peripheral blood mononuclear cells harvested prior to and following exposure. Following 8 h exposure, no cellular stress response-related proteins differed significantly between the 26 and 22 °C conditions (all, P ≥ 0.056). By contrast, autophagy-related proteins were elevated following exposure to 31 °C (p62: 1.5-fold; P = 0.003) and 36 °C (LC3-II, LC3-II/I, p62; all ≥2.0-fold; P ≤ 0.002) compared to 22 °C. These responses were accompanied by elevations in apoptotic signaling in the 31 and 36 °C conditions (cleaved-caspase-3: 1.8-fold and 3.7-fold, respectively; P ≤ 0.002). Furthermore, HSP90 was significantly reduced in the 36 °C compared to 22 °C condition (0.7-fold; P = 0.014). Our findings show that older adults experience considerable cellular stress during prolonged exposure to elevated ambient temperatures and support recommendations to maintain indoor temperatures ≤26 °C to prevent physiological strain in heat-vulnerable persons.

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