Evaluation and clinical relevance of patient immune responses to intravenous therapy with murine monoclonal antibodies conjugated to adriamycin.

Molecular biotherapy Pub Date : 1991-03-01
B Avner, L Swindell, E Sharp, S K Liao, J R Ogden, B P Avner, R K Oldham
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Abstract

A retrospective study was performed in order to examine the clinical relevance of human anti-murine antibodies (HAMA) to concurrent clinical events in 21 patients receiving intravenous therapy with cocktails of murine monoclonal antibodies conjugated to Adriamycin. In vivo tumor localization of the murine antibodies was also evaluated. Serum levels of HAMA, human-murine immune complexes (HMIC), and murine antibodies were measured using an automated fluorescence immunoassay. Immunohistochemical staining was performed on frozen sections of tumor biopsies from eight of the patients to examine the in vivo binding of the murine antibodies. The patients were divided into low, intermediate, and high antibody dose groups. The incidence of allergic symptoms (80%) and HAMA correlation (75%) were highest in the low dose group. Specific IgM HAMA was the most highly correlated with allergic reactions, being present in 61.5% of the allergic patients. Thirteen of the 21 patients studied (61.9%) developed allergic symptoms after one or more doses of the murine monoclonal antibody conjugates. The percentages of total antibody doses in the patients' sera at varying intervals post-infusion varied widely from patient to patient for any given time point and dose, suggesting complex factors in the distribution and clearance of the murine antibodies. All eight of the patients biopsied during or post-therapy exhibited tumor localization of the murine monoclonal antibodies. Six of the eight had concurrent HAMA in their sera. Thus, the presence of HAMA did not prevent in vivo localization of the murine antibodies in the target tumors.(ABSTRACT TRUNCATED AT 250 WORDS)

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阿霉素偶联小鼠单克隆抗体静脉治疗对患者免疫反应的评价及其临床意义。
为了检查21例接受阿霉素偶联小鼠单克隆抗体鸡尾酒静脉治疗的患者的人抗小鼠抗体(HAMA)与并发临床事件的临床相关性,进行了回顾性研究。小鼠抗体的体内肿瘤定位也进行了评估。采用自动荧光免疫分析法测定血清HAMA、人鼠免疫复合物(HMIC)和小鼠抗体水平。对其中8例患者的冷冻肿瘤切片进行免疫组化染色,以检测小鼠抗体的体内结合。将患者分为低、中、高抗体剂量组。低剂量组过敏症状发生率(80%)和HAMA相关性(75%)最高。特异性IgM HAMA与过敏反应的相关性最高,61.5%的过敏患者存在特异性IgM HAMA。21例患者中有13例(61.9%)在服用一次或多次小鼠单克隆抗体偶联物后出现过敏症状。在任何给定的时间点和剂量下,注射后不同时间间隔患者血清中总抗体剂量的百分比在患者之间差异很大,表明小鼠抗体的分布和清除中存在复杂的因素。在治疗期间或治疗后活检的所有8例患者均显示小鼠单克隆抗体的肿瘤定位。8人中有6人血清中同时存在HAMA。因此,HAMA的存在并不能阻止小鼠抗体在靶肿瘤中的体内定位。(摘要删节250字)
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