c 型凝集素受体 clec2d 的基因消减会增加腹膜炎的死亡率、炎症和生理机能,但不会减轻器官损伤。

IF 2.7 3区 医学 Q2 CRITICAL CARE MEDICINE
SHOCK Pub Date : 2024-09-01 Epub Date: 2024-06-11 DOI:10.1097/SHK.0000000000002413
Allan E Stolarski, Jiann-Jyh Lai, Jiyoun Kim, Kenneth L Rock, Daniel Remick
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引用次数: 0

摘要

背景:败血症造成了大量的发病率和死亡率,促使研究人员继续寻找驱动该疾病发病机制的途径和分子。本研究探讨了新型 C 型凝集素受体(CLR)Clec2d 是否在败血症发病机制中发挥重要作用:方法:将Clec2d基因敲除(KO)小鼠完全回交到C57/BL6背景上。腹腔注射脂多糖(LPS)诱导急性内毒素血症。在两种不同的模型(盲肠结扎和穿刺(CLP)和铜绿假单胞菌肺炎)中诱导败血症。两种模型均使用抗生素和液体复苏治疗。在败血症模型中,通过采集少量外周血样本,在24小时后测量生理和血液学指标。对死亡率进行了 14 天的跟踪观察:共研究了 197 只小鼠,其中 LPS 模型中 58 只野生型(WT)小鼠和 54 只基因敲除(KO)小鼠;CLP 模型中 27 只野生型小鼠和 21 只基因敲除(KO)小鼠;肺炎模型中 22 只 WT 小鼠和 15 只基因敲除(KO)小鼠。在 LPS 和 CLP 研究中,Clec2d KO 小鼠的死亡率较高,但在肺炎模型中,Clec2d KO 小鼠的死亡率并不高。在败血症后 24 小时测定的多个参数中,死亡小鼠与存活小鼠之间存在显著差异。与之前的报告一致,在 CLP 模型中,濒死小鼠体内 IL-6 浓度更高,外周血淋巴细胞数量增加,肾损伤加重。相反,在肺炎模型中,存活小鼠的 IL-6 水平较高,但肺炎模型中的 IL-6 水平(0.6 ± 0.3 纳克/毫升,平均值 ± SEM)不到 CLP 模型中死亡小鼠 IL-6 水平(41 ± 9 纳克/毫升,平均值 ± SEM)的 2%。在肺炎模型中,存活小鼠和死亡小鼠的淋巴细胞计数或肾损伤没有差异。在两种败血症模型中,垂死小鼠的心率、呼吸频率和体温都较低。在CLP中,KO小鼠的这些数值也低于WT小鼠,但KO肺炎小鼠的呼吸频率和体温都有所升高:结论:C型凝集素受体Clec2d在败血症的发病机制中起着复杂的作用,其作用因感染源而异,这在用于研究该疾病的模型中得到了证实。这些数据突显了脓毒症反应的异质性,并进一步证明驱动脓毒症器官损伤和死亡的单一共同途径可能并不存在。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
GENETIC ABLATION OF THE C-TYPE LECTIN RECEPTOR CLEC2D INCREASES PERITONITIS MORTALITY, INFLAMMATION, AND PHYSIOLOGY WITHOUT DIMINISHING ORGAN INJURY.

Abstract: Background: Sepsis accounts for substantial morbidity and mortality motivating investigators to continue the search for pathways and molecules driving the pathogenesis of the disease. The current study examined if the novel C-type lectin receptor (CLR), Clec2d, plays a significant role in the pathogenesis of sepsis. Methods: Clec2d knockout (KO) mice were fully backcrossed onto the C57/BL6 background. Acute endotoxemia was induced with an intraperitoneal injection of lipopolysaccharide (LPS). Sepsis was induced in two different models, cecal ligation and puncture (CLP) and Pseudomonas aeruginosa pneumonia. Both models were treated with antibiotics and fluid resuscitation. In the sepsis models, physiologic and hematologic measurements were measured at 24 h by collecting a small sample of peripheral blood. Mortality was followed for 14 days. Results : A total of 197 mice were studied, 58 wild type (WT) and 54 knock-out (KO) in the LPS model; 27 wild type and 21 KO mice in the CLP model; and 22 WT and 15 KO mice in the pneumonia model. Clec2d KO mice had greater mortality in the LPS and CLP studies but not the pneumonia model. There were significant differences in multiple parameters determined 24 h post sepsis between mice who subsequently died and those lived. Consistent with previous reports in the CLP model, higher concentrations of IL-6, increased numbers of peripheral blood lymphocytes and greater renal injury were found in the dying mice. In contrast, in the pneumonia model, IL-6 was higher in the surviving mice; however, the IL-6 levels in the pneumonia model (0.6 ± 0.3 ng/mL mean ± SEM) were less than 2% of the IL-6 levels of mice that died in the CLP model (41 ± 9 ng/mL, mean ± SEM). There were no differences in the lymphocyte count or renal injury between living and dying mice in the pneumonia model. In both sepsis models, dying mice had lower heart rates, respiratory rates, and body temperatures. These values were also lower in the KO mice compared to the WT in CLP, but the breath rate and body temperature were increased in the KO pneumonia mice. Conclusion: The C-type lectin receptor Clec2d plays a complicated role in the pathogenesis of sepsis, which varies with source of infection as demonstrated in the models used to study the disease. These data highlight the heterogeneity of the responses to sepsis and provide further evidence that a single common pathway driving sepsis organ injury and death likely does not exist.

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来源期刊
SHOCK
SHOCK 医学-外科
CiteScore
6.20
自引率
3.20%
发文量
199
审稿时长
1 months
期刊介绍: SHOCK®: Injury, Inflammation, and Sepsis: Laboratory and Clinical Approaches includes studies of novel therapeutic approaches, such as immunomodulation, gene therapy, nutrition, and others. The mission of the Journal is to foster and promote multidisciplinary studies, both experimental and clinical in nature, that critically examine the etiology, mechanisms and novel therapeutics of shock-related pathophysiological conditions. Its purpose is to excel as a vehicle for timely publication in the areas of basic and clinical studies of shock, trauma, sepsis, inflammation, ischemia, and related pathobiological states, with particular emphasis on the biologic mechanisms that determine the response to such injury. Making such information available will ultimately facilitate improved care of the traumatized or septic individual.
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