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未成熟单阳性和双阳性胸腺细胞亚群的凋亡减少导致小鼠多微生物败血症期间胸腺退化。

Apoptotic Diminution of Immature Single and Double Positive Thymocyte Subpopulations Contributes to Thymus Involution During Murine Polymicrobial Sepsis.

作者信息

Netzer Christoph, Knape Tilo, Kuchler Laura, Weigert Andreas, Zacharowski Kai, Pfeilschifter Waltraud, Sempowski Gregory, Parnham Michael J, Brüne Bernhard, von Knethen Andreas

机构信息

*Institute of Biochemistry I-Pathobiochemistry, Faculty of Medicine, Goethe-University Frankfurt, Frankfurt, Germany †Fraunhofer Institute for Molecular Biology and Applied Ecology IME, Project Group Translational Medicine and Pharmacology TMP, Frankfurt, Germany ‡Department of Anaesthesiology, Intensive Care Medicine and Pain Therapy, University Hospital Frankfurt, Frankfurt, Germany §Department of Neurology, University Hospital Frankfurt, Frankfurt, Germany ||Duke Human Vaccine Institute, Duke University School of Medicine, Durham, North Carolina.

出版信息

Shock. 2017 Aug;48(2):215-226. doi: 10.1097/SHK.0000000000000842.

Abstract

To generate and maintain functional T-cell receptor diversity, thymocyte development is tightly organized. Errors in this process may have dramatic consequences, provoking, for example, autoimmune diseases. Probably for this reason, the thymus reacts to septic stress with involution, decreasing the numbers of thymocytes. Because it is still unclear which thymocyte subpopulation contributes to thymus involution and whether thymocyte emigration is altered, we were interested to clarify this question in detail. Here, we show, using the cecal ligation and puncture (CLP) mouse model of polymicrobial sepsis, that predominantly immature thymocytes are reduced. The number of immature single positive thymocytes was most marked diminished (CLP: 6.54 × 10 ± 3.79 × 10 vs. sham: 4.54 × 10 ± 7.66 × 10 cells/thymus [24 h], CLP: 2.60 × 10 ± 2.14 × 10 vs. sham: 2.17 × 10 ± 1.90 × 10 cells/thymus [48 h]), and was consequently associated with the highest rate of apoptosis (8.4 [CLP] vs. 2.2% [sham]), the reduction in double positive thymocytes being associated with a smaller apoptotic response (number, CLP: 2.33 × 10 ± 1.38 × 10 vs. sham: 1.07 × 10 ± 2.72 × 10 cells/thymus [24 h], CLP: 2.34 × 10 ± 9.08 × 10 vs. sham: 3.5 × 10 ± 9.62 × 10 cells/thymus [48 h]; apoptosis: 2.5% [CLP] vs. 0.7% [sham]). Analysis of T-cell receptor excision circles revealed that the emigration of mature thymocytes was not inhibited. Real-time qPCR analysis revealed upregulation of pro-apoptotic Bim expression and suggested interference between Notch receptor expression on thymocytes and the respective ligands on thymic stromal cells during CLP-dependent sepsis, which might be responsible for the altered thymocyte viability in CLP-dependent sepsis.

摘要

为了产生并维持功能性T细胞受体多样性,胸腺细胞发育过程组织严密。这一过程中的错误可能会产生严重后果,例如引发自身免疫性疾病。可能正因如此,胸腺会对脓毒症应激产生反应并发生退化,导致胸腺细胞数量减少。由于目前仍不清楚哪种胸腺细胞亚群会导致胸腺退化,以及胸腺细胞的迁出是否发生改变,我们有兴趣详细阐明这个问题。在这里,我们利用多微生物脓毒症的盲肠结扎和穿刺(CLP)小鼠模型表明,主要是未成熟胸腺细胞数量减少。未成熟单阳性胸腺细胞数量减少最为显著(CLP组:6.54×10±3.79×10,假手术组:4.54×10±7.66×10个细胞/胸腺[24小时];CLP组:2.60×10±2.14×10,假手术组:2.17×10±1.90×10个细胞/胸腺[48小时]),因此其凋亡率最高(CLP组为8.4%,假手术组为2.2%),双阳性胸腺细胞数量减少与较小的凋亡反应相关(数量,CLP组:2.33×10±1.38×10,假手术组:1.07×10±2.72×10个细胞/胸腺[24小时];CLP组:2.34×10±9.08×10,假手术组:3.5×10±9.62×10个细胞/胸腺[48小时];凋亡率:CLP组为2.5%,假手术组为0.7%)。对T细胞受体切除环的分析表明,成熟胸腺细胞的迁出未受抑制。实时定量PCR分析显示促凋亡蛋白Bim表达上调,并提示在CLP依赖性脓毒症期间,胸腺细胞上的Notch受体表达与胸腺基质细胞上的相应配体之间存在相互干扰,这可能是CLP依赖性脓毒症中胸腺细胞活力改变的原因。

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