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抗体连接的细胞毒性药物在癌症治疗中的现状与未来前景

Antibody-linked cytotoxic agents in the treatment of cancer: current status and future prospects.

作者信息

Ghose T, Blair A H

出版信息

J Natl Cancer Inst. 1978 Sep;61(3):657-76.

PMID:80453
Abstract

Antibodies against tumor cell surface antigens have been used as selective carriers of anticancer drugs, which themselves lack selectivity. Although such antibodies have been demonstrated in tumor hosts, xenogeneic antitumor sera should provide larger yields of better-defined antitumor antibodies for therapeutic purposes. This review examined factors that influence the immune response to tumor-associated transplantation antigens (TATA) and the methods for rendering tumor cells more immunogenic. Consideration was also given to techniques for elimination of irrelevant immunoglobulin molecules. These could involve purification of both antitumor sera and TATA fractions for immunization, as well as tailoring of the immunization protocol. Various toxic agents that have been linked to antitumor globulins with retention of agent and antibody activity were tabulated: alkylating drugs, antibiotics, antimetabolites, cell surface agents, protein synthesis inhibitors, and unconventional anticancer agents that selectively convert nontoxic arsenicals or halides into cytocidal derivatives. The methods by which effective conjugates can be produced and their possible mode of action were described for the different types of agents. Several problems inherent in this modality of tumor therapy include: 1) the necessity of binding therapeutically effective amounts of antitumor agent, 2) ensuring of delivery of drug in active form to target sites, 3) avoidance of host reactions to foreign proteins, and 4) possible emergence of resistant tumor cell populations. Antibody-linked cytotoxic agents may find their greatest use in the eradication of small numbers of circulating tumor cells and micrometastases remaining after removal of primary tumors.

摘要

针对肿瘤细胞表面抗原的抗体已被用作抗癌药物的选择性载体,而抗癌药物本身缺乏选择性。尽管此类抗体已在肿瘤宿主中得到证实,但异种抗肿瘤血清应为治疗目的提供产量更高、定义更明确的抗肿瘤抗体。本综述研究了影响对肿瘤相关移植抗原(TATA)免疫反应的因素以及使肿瘤细胞更具免疫原性的方法。还考虑了消除无关免疫球蛋白分子的技术。这些技术可能包括纯化用于免疫的抗肿瘤血清和TATA组分,以及调整免疫方案。列出了各种与保留药物和抗体活性的抗肿瘤球蛋白相关的毒性药物:烷基化药物、抗生素、抗代谢物、细胞表面活性剂、蛋白质合成抑制剂,以及能将无毒砷化合物或卤化物选择性转化为细胞毒性衍生物的非常规抗癌药物。描述了针对不同类型药物产生有效缀合物的方法及其可能的作用方式。这种肿瘤治疗方式存在的几个固有问题包括:1)结合治疗有效量抗肿瘤药物的必要性;2)确保以活性形式将药物递送至靶位点;3)避免宿主对外源蛋白质的反应;4)可能出现耐药肿瘤细胞群体。抗体连接的细胞毒性药物可能在根除原发性肿瘤切除后残留的少量循环肿瘤细胞和微转移灶方面发挥最大作用。

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