Van Zee K J, Kohno T, Fischer E, Rock C S, Moldawer L L, Lowry S F
Laboratory of Surgical Metabolism, New York Hospital-Cornell University Medical Center, NY 10021.
Proc Natl Acad Sci U S A. 1992 Jun 1;89(11):4845-9. doi: 10.1073/pnas.89.11.4845.
Tumor necrosis factor alpha (TNF alpha), a primary mediator of systemic responses to sepsis and infection, can be injurious to the organism when present in excessive quantities. Here we report that two types of naturally occurring soluble TNF receptors (sTNFR-I and sTNFR-II) circulate in human experimental endotoxemia and in critically ill patients and demonstrate that they neutralize TNF alpha-induced cytotoxicity and immunoreactivity in vitro. Utilizing immunoassays that discriminate between total sTNFR-I and sTNFR-I not bound to TNF alpha, we show that sTNFR-I-TNF alpha complexes may circulate even in the absence of detectable free TNF alpha. To investigate the therapeutic possibilities of sTNFR-I, recombinant protein was administered to nonhuman primates with lethal bacteremia and found to attenuate hemodynamic collapse and cytokine induction. We conclude that soluble receptors for TNF alpha are inducible in inflammation and circulate at levels sufficient to block the in vitro cytotoxicity associated with TNF alpha levels observed in nonlethal infection. Administration of sTNFR-I can prevent the adverse pathologic sequelae caused by the exaggerated TNF alpha production observed in lethal sepsis.
肿瘤坏死因子α(TNFα)是机体对脓毒症和感染产生全身反应的主要介质,当其过量存在时会对机体造成损害。我们在此报告,两种天然存在的可溶性TNF受体(sTNFR - I和sTNFR - II)在人类实验性内毒素血症及重症患者体内循环,且在体外可中和TNFα诱导的细胞毒性和免疫反应性。利用能区分总sTNFR - I和未与TNFα结合的sTNFR - I的免疫测定方法,我们发现即使在未检测到游离TNFα的情况下,sTNFR - I - TNFα复合物也可能在循环中存在。为研究sTNFR - I的治疗潜力,将重组蛋白给予患有致死性菌血症的非人灵长类动物,发现其可减轻血流动力学崩溃和细胞因子诱导。我们得出结论,TNFα的可溶性受体在炎症中可被诱导,且以足以阻断与非致死性感染中观察到的TNFα水平相关的体外细胞毒性的水平循环。给予sTNFR - I可预防致死性脓毒症中因TNFα过度产生而导致的不良病理后果。
