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蓖麻毒素A链-单克隆抗体791T/36免疫毒素的生物分布及肝阻断剂的影响

Biodistribution of ricin toxin A chain-monoclonal antibody 791T/36 immunotoxin and influence of hepatic blocking agents.

作者信息

Byers V S, Pimm M V, Pawluczyk I Z, Lee H M, Scannon P J, Baldwin R W

机构信息

Cancer Research Campaign Laboratories, University of Nottingham, United Kingdom.

出版信息

Cancer Res. 1987 Oct 15;47(20):5277-83.

PMID:3498532
Abstract

Immunotoxin constructed by conjugating ricin A chain to monoclonal antibody 791T/36 has a markedly altered biodistribution when compared to unconjugated antibody. This is principally manifest as hepatic uptake of immunotoxin which appears to be controlled by the ricin A chain (RTA) moiety. This was established by comparing the blood survival and organ distribution of immunotoxin with that of ricin A chain and free antibody using preparations in which either the RTA or antibody, alone or as components of the immunotoxin, was radiolabeled. Gel filtration chromatography of sera from immunotoxin treated animals demonstrated a preferential blood clearance of immunotoxin with high RTA-antibody ratio. Hepatic uptake is dependent upon Kupffer cell recognition of mannose-containing oligosaccharide structures on the RTA moiety of immunotoxin. Mannose-containing blocking agents given with immunotoxin were shown to prolong circulation time of the immunotoxin in blood including those species with higher RTA-monoclonal antibody ratios and reduce liver uptake. Effective blocking agents include ovalbumin, ovomucoid, and mannosyl-lysine (Man3Ly2). These studies demonstrate that agents specifically inhibiting hepatic uptake of immunotoxin significantly alter biodistribution and may improve their therapeutic efficacy.

摘要

与未偶联的抗体相比,将蓖麻毒素A链与单克隆抗体791T/36偶联构建的免疫毒素的生物分布有显著改变。这主要表现为免疫毒素的肝脏摄取,这似乎受蓖麻毒素A链(RTA)部分控制。通过使用RTA或抗体单独或作为免疫毒素成分被放射性标记的制剂,比较免疫毒素与蓖麻毒素A链和游离抗体的血液存留时间和器官分布,证实了这一点。对免疫毒素处理动物的血清进行凝胶过滤层析显示,高RTA-抗体比例的免疫毒素优先从血液中清除。肝脏摄取取决于库普弗细胞对免疫毒素RTA部分上含甘露糖的寡糖结构的识别。与免疫毒素一起给予含甘露糖的阻断剂可延长免疫毒素在血液中的循环时间,包括那些RTA-单克隆抗体比例较高的物种,并减少肝脏摄取。有效的阻断剂包括卵清蛋白、卵类粘蛋白和甘露糖基赖氨酸(Man3Ly2)。这些研究表明,特异性抑制免疫毒素肝脏摄取的试剂可显著改变生物分布,并可能提高其治疗效果。

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