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一种含重组人肿瘤坏死因子的抗黑色素瘤免疫毒素:在异种移植模型中的组织分布、药代动力学及治疗研究

An antimelanoma immunotoxin containing recombinant human tumor necrosis factor: tissue disposition, pharmacokinetic, and therapeutic studies in xenograft models.

作者信息

Rosenblum M G, Cheung L, Mujoo K, Murray J L

机构信息

Department of Clinical Immunology and Biological Therapy, M. D. Anderson Cancer Center, Houston 77030, USA.

出版信息

Cancer Immunol Immunother. 1995 May;40(5):322-8. doi: 10.1007/BF01519633.

Abstract

The ability of monoclonal antibody conjugates to re-direct plant or bacterial toxins, chemotherapeutic agents and radionuclides to selected target cells has been well-documented. Recombinant human tumor necrosis factor (TNF) is a macrophage-derived, non-glycosylated (17 kDa) peptide with a broad range of biological and immunological effects including antiviral activity, cytotoxic and cytostatic effects. A conjugate of the antimelanoma antibody ZME-018 and TNF in previous studies has shown melanoma-selective cytotoxic effects in vitro. Pharmacokinetic studies of the ZME-TNF immunotoxin showed that the agent cleared from plasma biphasically with alpha- and beta-phase half-lives similar to that of ZME itself (72 min and 36 h compared to 84 min and 41 h respectively). In contrast, TNF itself was cleared rapidly from plasma with a terminal-phase half-life of only 2.7 h. The clearance rate of ZME-TNF from plasma (Clp) was almost tenfold more rapid than for ZME (1.1 versus 0.16 ml/kg x min) but was threefold slower than the clearance for TNF itself (3.4 ml/kg x min). Tissue distribution studies in nude mice bearing human melanoma xenografts showed similar tumor localization of the immunotoxin compared to the free antibody and slightly higher concentrations in liver and kidney compared to ZME itself. Treatment of nude mice bearing well-developed A375 tumors with the immunotoxin resulted in a statistically significant (P < 0.002) suppression in tumor growth rate (fivefold increase) compared to saline-treated controls, which increased 20-fold over the same period. These studies demonstrate the feasibility of this approach and suggest that TNF may represent a non-antigenic alternative to immunotoxins containing plant and bacterial toxins.

摘要

单克隆抗体偶联物将植物或细菌毒素、化疗药物及放射性核素重新导向特定靶细胞的能力已得到充分证明。重组人肿瘤坏死因子(TNF)是一种巨噬细胞衍生的非糖基化(17 kDa)肽,具有广泛的生物学和免疫学效应,包括抗病毒活性、细胞毒性和细胞生长抑制作用。在先前的研究中,抗黑色素瘤抗体ZME - 018与TNF的偶联物在体外显示出对黑色素瘤的选择性细胞毒性作用。ZME - TNF免疫毒素的药代动力学研究表明,该药物从血浆中呈双相清除,α相和β相半衰期与ZME本身相似(分别为72分钟和36小时,而ZME本身为84分钟和41小时)。相比之下,TNF本身从血浆中迅速清除,终末相半衰期仅为2.7小时。ZME - TNF从血浆中的清除率(Clp)几乎比ZME快十倍(分别为1.1和0.16 ml/kg·min),但比TNF本身的清除率慢三倍(3.4 ml/kg·min)。在携带人黑色素瘤异种移植瘤的裸鼠中的组织分布研究表明,与游离抗体相比,免疫毒素在肿瘤中的定位相似,与ZME本身相比,在肝脏和肾脏中的浓度略高。用免疫毒素治疗携带成熟A375肿瘤的裸鼠,与盐水处理的对照组相比,肿瘤生长速率有统计学意义的显著抑制(P < 0.002)(增加了五倍),而对照组在同一时期增加了20倍。这些研究证明了这种方法的可行性,并表明TNF可能是含有植物和细菌毒素的免疫毒素的一种非抗原性替代物。

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