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热射病后组织和循环中白细胞介素-1 家族成员的表达。

Tissue and circulating expression of IL-1 family members following heat stroke.

机构信息

United States Army Research Institute of Environmental Medicine, Thermal and Mountain Medicine Division, Natick, Massachusetts 01760, USA.

出版信息

Physiol Genomics. 2011 Oct 6;43(19):1096-104. doi: 10.1152/physiolgenomics.00076.2011. Epub 2011 Aug 9.

Abstract

Interleukin-1 (IL-1) is thought to have a significant role in the pathophysiology of heat stroke (HS), although little is known regarding the actions or expression patterns of the IL-1 family. This study tested the hypotheses that following HS IL-1 family gene expression is dynamic, while loss of IL-1 signaling enhances recovery. IL-1 family expression was determined in plasma, spleen, and liver from C57BL/6J mice (n=24 control, n=20 HS) at maximum core temperature (Tc,Max), hypothermia, and 24 h post-HS (24 h). Soluble IL-1 receptor subtype I (sIL-1RI) protein expression peaked at 24 h (14,659.01±2,016.28 pg/ml, P<0.05), while sIL-1RII peaked at hypothermia (19,099.30±1,177.07 pg/ml). IL-1α gene expression in the spleen (ninefold) and liver (fourfold) along with IL-1RI (threefold spleen and fivefold liver) were maximal at hypothermia. Spleen IL-1β gene expression peaked at Tc,Max (fourfold) but at hypothermia (fourfold) in liver. Gene expression of the IL-1 family member IL-18 peaked (2.5-fold) at Tc,Max but was similar at all other time points. Subsequent studies revealed that despite accruing a greater heating area (298±16 vs. 247±13°C·min, P<0.05), IL-1RI knockout (KO) mice (n=14) showed an attenuated hypothermia depth (28.5±0.2 vs. 27.3±0.5°C, P<0.05) and duration (675±82 vs. 1,283±390 min, P<0.05) with a higher 24 h Tc (36.9 vs. 34.1°C, P<0.05) compared with C57BL/6J mice (n=8). The current results demonstrate that following HS IL-1 family gene expression is altered and IL-1RI KO mice display Tc responses consistent with a more rapid recovery.

摘要

白细胞介素-1(IL-1)被认为在中暑(HS)的病理生理学中具有重要作用,尽管对于 IL-1 家族的作用或表达模式知之甚少。本研究检验了以下假设:在中暑后,IL-1 家族基因表达是动态的,而丧失 IL-1 信号会促进恢复。在最大核心温度(Tc,Max)、低温和中暑后 24 小时(24 h)时,从 C57BL/6J 小鼠的血浆、脾脏和肝脏中确定了 IL-1 家族的表达(n=24 个对照组,n=20 个中暑组)。可溶性白细胞介素-1 受体亚型 I(sIL-1RI)蛋白表达在 24 小时时达到峰值(14659.01±2016.28 pg/ml,P<0.05),而 sIL-1RII 在低温时达到峰值(19099.30±1177.07 pg/ml)。脾脏和肝脏中 IL-1α 基因表达(脾脏九倍,肝脏四倍)以及 IL-1RI(脾脏三倍,肝脏五倍)在低温时达到最大。脾脏 IL-1β 基因表达在 Tc,Max 时达到峰值(四倍),但在肝脏中在低温时达到峰值(四倍)。IL-1 家族成员 IL-18 的基因表达在 Tc,Max 时达到峰值(2.5 倍),但在所有其他时间点都相似。随后的研究表明,尽管积累了更大的加热面积(298±16 与 247±13°C·min,P<0.05),但 IL-1RI 敲除(KO)小鼠(n=14)的低温深度(28.5±0.2 与 27.3±0.5°C,P<0.05)和持续时间(675±82 与 1283±390 min,P<0.05)更短,24 小时 Tc 更高(36.9 与 34.1°C,P<0.05)与 C57BL/6J 小鼠(n=8)相比。目前的结果表明,中暑后 IL-1 家族基因表达发生改变,IL-1RI KO 小鼠的 Tc 反应与更快的恢复一致。

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