Canevari S, Stoter G, Arienti F, Bolis G, Colnaghi M I, Di Re E M, Eggermont A M, Goey S H, Gratama J W, Lamers C H
Division of Experimental Oncology, Istituto Nazionale per lo Studio e la Cura dei Tumori, Milan, Italy.
J Natl Cancer Inst. 1995 Oct 4;87(19):1463-9. doi: 10.1093/jnci/87.19.1463.
The high frequency of relapse after induction chemotherapy of advanced ovarian carcinoma calls for new therapeutic approaches. Lysis of ovarian carcinoma cells can be achieved by retargeting of T lymphocytes using F(ab')2 fragments of the bispecific monoclonal antibody (MAb) OC/TR, which is directed to the CD3 molecule on T lymphocytes and to the folate receptor on ovarian carcinoma cells.
Our purpose was to assess in ovarian carcinoma patients the antitumor activity of in vitro-activated autologous peripheral blood T lymphocytes retargeted with OC/TR.
Patients with epithelial ovarian cancer (International Federation of Gynecology and Obstetrics stages III and IV) meeting specific criteria were eligible to enter a phase II immunotherapy trial. Before immunotherapy, the 28 patients who entered the trial underwent laparotomy to reduce their tumor load and to allow measurement of all indicator lesions. They then received two cycles of five daily intraperitoneal infusions of autologous in vitro activated peripheral blood T lymphocytes retargeted with OC/TR plus recombinant interleukin 2 (IL-2) with (n = 11) or without (n = 17) a second daily infusion of OC/TR F(ab')2 and IL-2. Response to treatment could be assessed in 26 patients following explorative laparotomy; time to progression could be assessed in 27 patients.
Seven patients had clinical evidence of progressive disease after treatment and therefore did not undergo laparotomy. Of the 19 patients evaluated by surgery and histology, three showed complete response, one showed complete intraperitoneal response with progressive disease in retroperitoneal lymph nodes, three showed partial response, seven had stable disease, and five had progressive disease. The overall intraperitoneal response rate was 27% (95% confidence interval [CI] = 10%-44%). The complete responses seen in three patients lasted 26 months in one patient, 23 months in the second, and 18 months in the third. Two patients were not assessable for response. One of these patients had bowel perforation during catheter removal, which precluded further evaluation. The second patient was positive only by cytologic examination before immunotherapy, was tumor free at laparotomy after immunotherapy, and remained so for the entire 21 months of follow-up, as determined by cytologic examination of random biopsy specimens. The median time to disease progression in the 15 assessable patients plus those who had stable disease was 11 months (95% CI = 6-18 months). Immunotherapy-related toxic effects included mild to moderate fever, nausea, emesis, and fatigue. Anti-mouse antibodies were detectable by the end of the treatment in 21 of 25 patients tested.
Locoregional immunotherapy of ovarian cancer with bispecific MAb-retargeted T lymphocytes can result in tumor regression. Toxicity was mild to moderate and only transient.
Improvement in systemic antitumor responses is needed before this approach can prove useful as adjunctive treatment following induction chemotherapy in patients with minimal residual disease.
晚期卵巢癌诱导化疗后复发率高,需要新的治疗方法。使用双特异性单克隆抗体(MAb)OC/TR的F(ab')2片段重新靶向T淋巴细胞,可实现卵巢癌细胞的裂解,该双特异性单克隆抗体针对T淋巴细胞上的CD3分子和卵巢癌细胞上的叶酸受体。
我们的目的是评估用OC/TR重新靶向的体外激活的自体外周血T淋巴细胞在卵巢癌患者中的抗肿瘤活性。
符合特定标准的上皮性卵巢癌(国际妇产科联盟III期和IV期)患者有资格进入II期免疫治疗试验。在免疫治疗前,进入试验的28例患者接受剖腹手术以减轻肿瘤负荷并允许测量所有指标性病变。然后,他们接受两个周期的治疗,每天进行5次腹腔内输注用OC/TR重新靶向的自体体外激活的外周血T淋巴细胞加重组白细胞介素2(IL-2),其中11例患者每日还输注OC/TR F(ab')2和IL-2,另外17例患者则不输注。在 exploratory剖腹手术后,可对26例患者的治疗反应进行评估;可对27例患者的疾病进展时间进行评估。
7例患者治疗后有疾病进展的临床证据,因此未接受剖腹手术。在通过手术和组织学评估的19例患者中,3例显示完全缓解,1例显示腹腔内完全缓解但腹膜后淋巴结有疾病进展,3例显示部分缓解,7例疾病稳定,5例疾病进展。总体腹腔内反应率为27%(95%置信区间[CI]=10%-44%)。3例患者出现的完全缓解分别持续26个月(1例患者)、23个月(第2例患者)和18个月(第3例患者)。2例患者无法评估反应。其中1例患者在拔除导管期间出现肠穿孔,无法进行进一步评估。第2例患者在免疫治疗前仅细胞学检查呈阳性,免疫治疗后剖腹手术时无肿瘤,随机活检标本的细胞学检查确定在整个21个月的随访期间均如此。15例可评估患者加上疾病稳定的患者的疾病进展中位时间为11个月(95%CI=6-18个月)。免疫治疗相关的毒性作用包括轻度至中度发热、恶心、呕吐和疲劳。在接受检测的25例患者中,21例在治疗结束时可检测到抗小鼠抗体。
用双特异性单克隆抗体重新靶向的T淋巴细胞对卵巢癌进行局部区域免疫治疗可导致肿瘤消退。毒性为轻度至中度且仅为短暂性。
在这种方法可被证明对微小残留病患者诱导化疗后作为辅助治疗有用之前,需要改善全身抗肿瘤反应。
