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Allogeneic cellbased immunotherapy combined with chemotherapy and targeted therapy in advanced pancreatic cancer with metastases: A case report

机译:基于异基因细胞的免疫疗法联合化学疗法和靶向治疗在晚期胰腺癌转移中的一例报告

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Immunotherapy may be an effective and potentially less toxic treatment for cancer in addition to the traditional therapies. The current study presents a case of advanced pancreatic cancer that was treated with cellbased immunotherapy using expanded activated allogeneic lymphocytes (EAAL*) in vitro with cluster of differentiation (CD)3(+) and CD8(+) cytotoxic T lymphocytes, and CD3() and CD56(+) natural killer cells as the major effector cells, together with chemotherapy and targeted agents. A 46yearold female was diagnosed at the Chinese PLA General Hospital (Beijing, China) with stage IV pancreatic cancer with multiple metastases in October 2012. After receiving one cycle of chemotherapy plus nimotuzumab (Nimo), the patient received 14 infusions of EAAL*, which was obtained from a related donor, combined with seven cycles of chemotherapy with gemcitabine plus oxaliplatin and targeted therapy with Nimo. The patient was followed up for eight months. One day prior to the cell infusion, targeted therapy was administered and 48 h following the cell infusion, chemotherapy was administered. Following this treatment, carbohydrate antigen 19-9 levels decreased from 4,136 U/ml to within the normal ranges, along with the significant regression of the lesions. Occasionally mild upset was observed following the EAAL* transfusion. For the entire combined modality, grade II hematological and gastrointestinal toxicities plus grade I liver function damage and skin rash were identified. The present study demonstrated that combining allogeneic cellbased immunotherapy with conventional therapies is effective and safe, even in patients with endstage pancreatic cancer. Therefore, this strategy is recommended for the treatment of similar cases.
机译:除传统疗法外,免疫疗法可能是一种有效且潜在毒性较小的癌症治疗方法。当前的研究提出了一个晚期胰腺癌病例,该病例使用基于细胞的免疫疗法进行了治疗,该疗法使用了体外扩增的活化同种异体淋巴细胞(EAAL *),分化簇(CD)3(+)和CD8(+)细胞毒性T淋巴细胞以及CD3( )和CD56(+)自然杀伤细胞作为主要效应细胞,以及化学疗法和靶向药物。一名46岁的女性于2012年10月在中国人民解放军总医院(中国北京)被诊断为多发性转移的IV期胰腺癌。在接受了一个化疗周期加上尼莫妥珠单抗(Nimo)的一个周期后,该患者接受了14剂EAAL *输注从相关捐助者处获得,联合吉西他滨加奥沙利铂的七个化疗周期和尼莫的靶向治疗。对该患者进行了八个月的随访。在细胞输注前一天,进行了靶向治疗,在细胞输注后48小时,进行了化疗。治疗后,碳水化合物抗原19-9的水平从4,136 U / ml下降到正常范围,同时病灶明显消退。 EAAL *输注后偶尔观察到轻度不适。对于整个组合形式,确定了II级血液学和胃肠道毒性以及I级肝功能损害和皮疹。本研究表明,即使在患有晚期胰腺癌的患者中,将基于异基因细胞的免疫疗法与常规疗法相结合也是有效和安全的。因此,建议将该策略用于类似病例的治疗。

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