Kosmas C, Snook D, Gooden C S, Courtenay-Luck N S, McCall M J, Meares C F, Epenetos A A
Department of Clinical Oncology, Royal Postgraduate Medical School, Hammersmith Hospital, London, United Kingdom.
Cancer Res. 1992 Feb 15;52(4):904-11.
The development of stable immunoconjugates by the advent of macrocyclic metal chelating agents (DOTA) has enabled us to study the ability of 111In-DOTA-labeled monoclonal antibodies to detect tumor lesions in a pilot radioimmunolocalization study, as well as to evaluate the kinetics, toxicity, and efficacy of i.p. administered 90Y-DOTA-labeled murine monoclonal antibody in a Phase I/II clinical trial of advanced ovarian cancer. The development of serum sickness-like reactions in three of six treated patients, in the absence of previous monoclonal antibody administration, led us to study the potential immunogenicity of the new chelate. Six patients with ovarian cancer received 25 mg of HMFG1 monoclonal antibody coupled with 90Y-DOTA (doses of radioactivity, 15 to 25 mCi), administered i.p. Eight patients with various malignant tumors received low doses (220 micrograms to 1 mg) of monoclonal antibodies, labeled with 111In-DOTA, i.v. for imaging studies. Using a solid-phase enzyme-linked immunosorbent assay method, the immunogenicity of DOTA was evaluated. Serial dilutions of patients' sera, before and after imaging or therapy with DOTA-coupled monoclonal antibodies, as well as sera from patients who did not receive DOTA-coupled antibody, were screened on enzyme-linked immunosorbent assay plates coated with human serum albumin (HSA), HSA-2-iminothiolane, and HSA-2-iminothiolane-benzyl-DOTA. All patients treated with i.p. monoclonal antibody developed anti-DOTA antibodies. Four of eight patients who received i.v. "imaging" doses of DOTA-coupled monoclonal antibody developed antibodies against DOTA. The levels of anti-DOTA response correlated with the amount of injected radioimmunoconjugate (r = 0.889, P less than 0.001). None of the patients who received DOTA-coupled antibody had detectable antibodies against the macrocycle before immunoconjugate administration. We then addressed further the restriction of the immune response against the macrocycle. We found that there was no or very low response against the aromatic ring attached to DOTA. Most, if not all, of the immune response is directed against the DOTA ring structure. Affinity purification of anti-DOTA antibody from serum enabled quantitation of these antibodies in the serum of patients. An inverse, statistically significant correlation was observed between the percentage of binding inhibition of a patient's serum to DOTA, by HSA-2-iminothiolane-DOTA (100 micrograms/ml) and the level of anti-DOTA immunoglobulin in the serum.(ABSTRACT TRUNCATED AT 400 WORDS)
大环金属螯合剂(DOTA)的出现促使稳定免疫缀合物得以发展,这使我们能够在一项初步放射免疫定位研究中,研究111In-DOTA标记的单克隆抗体检测肿瘤病灶的能力,以及在晚期卵巢癌的I/II期临床试验中,评估腹腔注射90Y-DOTA标记的鼠单克隆抗体的动力学、毒性和疗效。在6名接受治疗的患者中有3名出现血清病样反应,且此前未给予单克隆抗体,这促使我们研究这种新型螯合物的潜在免疫原性。6名卵巢癌患者腹腔注射了25 mg与90Y-DOTA偶联的HMFG1单克隆抗体(放射性剂量为15至25 mCi)。8名患有各种恶性肿瘤的患者静脉注射低剂量(220微克至1毫克)的111In-DOTA标记的单克隆抗体用于成像研究。使用固相酶联免疫吸附测定法评估DOTA的免疫原性。在包被有人血清白蛋白(HSA)、HSA-2-亚氨基硫醇和HSA-2-亚氨基硫醇-苄基-DOTA的酶联免疫吸附测定板上,筛选患者在接受DOTA偶联单克隆抗体成像或治疗前后血清的系列稀释液,以及未接受DOTA偶联抗体患者的血清。所有接受腹腔注射单克隆抗体治疗的患者均产生了抗DOTA抗体。8名接受静脉注射“成像”剂量DOTA偶联单克隆抗体的患者中有4名产生了抗DOTA抗体。抗DOTA反应水平与注射的放射免疫缀合物量相关(r = 0.889,P < 0.001)。在给予免疫缀合物之前,接受DOTA偶联抗体的患者中没有检测到针对大环的抗体。然后我们进一步研究了针对大环的免疫反应的限制。我们发现,对连接在DOTA上的芳香环没有或只有非常低的反应。大部分(如果不是全部)免疫反应是针对DOTA环结构的。从血清中亲和纯化抗DOTA抗体能够定量患者血清中的这些抗体。观察到患者血清与DOTA的结合抑制百分比(由HSA-2-亚氨基硫醇-DOTA(100微克/毫升)引起)与血清中抗DOTA免疫球蛋白水平之间存在反向的、具有统计学意义的相关性。(摘要截短于400字)
