Nicod L P, Isler P, Chicheportiche R, Songeon F, Dayer J M
Respiratory Division, University Hospital, Geneva, Switzerland.
Eur Cytokine Netw. 1996 Dec;7(4):757-63.
TNF-alpha and lymphotoxin alpha (TNF-beta) are pleiotropic cytokines with regulatory functions in inflammatory reactions and T cell activation. Natural TNF inhibitors such as soluble TNF-binding proteins, i.e. TNFsR55 and TNFsR75, are shed from white blood cells and probably other cells. These naturally occurring inhibitors of TNF are shown to be 10 times less effective than the bivalent antagonist of TNF, recombinant soluble TNF receptor p55-human gamma 3 fusion protein (rsTNFR-p55h gamma 3), in controlling the release of prostaglandin E2 (PGE2) and collagenase by fibroblasts, as well as in controlling T cell proliferation. In order to block the action of rhTNF-alpha added to fibroblasts, a fivefold excess of rsTNFR-p55h gamma 3 was sufficient, but concentrations of a hundred to a thousand times higher were required to obtain a significant inhibition of T cell activation. This concentration appears to be required to block membrane-bound TNF-alpha on peripheral blood mononuclear cells as shown by Scatchard analysis. We additionally show that rsTNFR-p55h gamma 3 at high concentrations also blocks T cell activation by dendritic cells. In conclusion rsTNFR-p55h gamma 3 has a much higher anti-inflammatory effect than immunosuppressive effect.
肿瘤坏死因子-α(TNF-α)和淋巴毒素-α(TNF-β,即TNF-β)是多效性细胞因子,在炎症反应和T细胞活化中具有调节功能。天然TNF抑制剂,如可溶性TNF结合蛋白,即TNFR55和TNFR75,是从白细胞以及可能的其他细胞中脱落产生的。这些天然存在的TNF抑制剂在控制成纤维细胞释放前列腺素E2(PGE2)和胶原酶以及控制T细胞增殖方面,其效果比TNF的二价拮抗剂重组可溶性TNF受体p55-人γ3融合蛋白(rsTNFR-p55hγ3)低10倍。为了阻断添加到成纤维细胞中的重组人TNF-α(rhTNF-α)的作用,五倍过量的rsTNFR-p55hγ3就足够了,但需要高出一百到一千倍的浓度才能显著抑制T细胞活化。如Scatchard分析所示,该浓度似乎是阻断外周血单个核细胞上膜结合的TNF-α所必需的。我们还表明,高浓度的rsTNFR-p55hγ3也能阻断树突状细胞对T细胞的活化作用。总之,rsTNFR-p55hγ3的抗炎作用远高于免疫抑制作用。
