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注射抗CD3单克隆抗体后细胞因子相关综合征:体内T细胞短暂激活的进一步证据

Cytokine-related syndrome following injection of anti-CD3 monoclonal antibody: further evidence for transient in vivo T cell activation.

作者信息

Ferran C, Sheehan K, Dy M, Schreiber R, Merite S, Landais P, Noel L H, Grau G, Bluestone J, Bach J F

机构信息

INSERM U 25, CNRS UA 122, Hôpital Necker, Paris, France.

出版信息

Eur J Immunol. 1990 Mar;20(3):509-15. doi: 10.1002/eji.1830200308.

Abstract

In vivo injection of the hamster anti-murine CD3 monoclonal antibody 145 2C11 into BALB/c mice induces a massive systemic release of several cytokines. Very high circulating levels of tumor necrosis factor are detected both by enzyme-linked immunosorbent assay and L-929 bioassay 90 min following a single injection of 10 micrograms/mouse 145 2C11. Peak circulating levels of exclusively T cell-derived products such as interferon-gamma, interleukin 2 and interleukin 3 are also detected 90 min to 8 h post-injection. Importantly, this cytokine release is transient since none of these cytokines are still present 12 to 24 h post-injection. In parallel to cytokine release, 145 2C11-treated mice (10 micrograms/mouse) exhibit somnolence, hypomotility (quantified by actimetry), hypothermia, diarrhea and piloerection. At this dosage, the physical reaction is not lethal and reverses in all mice by 48 h post-injection. Severe but again reversible anatomopathological changes are also observed: massive cellular depletion, necrosis and edema of lymphoid organs, leakage syndrome and inflammatory cell infiltrates of the lung, cell vacuolization, necrosis and vascular congestion of the liver. All these data are similar to the clinical and immunological manifestations of the OKT3-induced reaction in patients and, thus, provide an invaluable experimental tool to study its mechanisms and explore its prevention.

摘要

向BALB/c小鼠体内注射仓鼠抗小鼠CD3单克隆抗体145 2C11会诱导多种细胞因子大量释放到全身。单次注射10微克/小鼠的145 2C11后90分钟,通过酶联免疫吸附测定和L-929生物测定法均可检测到循环中肿瘤坏死因子的水平非常高。在注射后90分钟至8小时,还可检测到仅由T细胞衍生的产物如干扰素-γ、白细胞介素2和白细胞介素3的循环峰值水平。重要的是,这种细胞因子释放是短暂的,因为在注射后12至24小时这些细胞因子均不再存在。与细胞因子释放同时,用145 2C11处理的小鼠(10微克/小鼠)表现出嗜睡、活动减少(通过活动量测定法量化)、体温过低、腹泻和竖毛。在此剂量下,身体反应不会致命,所有小鼠在注射后48小时均可恢复。还观察到严重但同样可逆的解剖病理学变化:淋巴器官大量细胞耗竭、坏死和水肿、渗漏综合征以及肺部炎性细胞浸润、肝细胞空泡化、坏死和血管充血。所有这些数据与患者中OKT3诱导反应的临床和免疫学表现相似,因此为研究其机制和探索预防方法提供了宝贵的实验工具。

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