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First-in-man Study of Western Reserve Strain Oncolytic Vaccinia Virus: Safety, Systemic Spread, and Antitumor Activity

机译:西方储备菌株溶瘤痘苗病毒的首次人体研究:安全性,系统性传播和抗肿瘤活性

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Oncolytic viral therapy utilizes a tumor-selective replicating virus which preferentially infects and destroys cancer cells and triggers antitumor immunity. The Western Reserve strain of vaccinia virus (VV) is the most virulent strain of VV in animal models and has been engineered for tumor selectivity through two targeted gene deletions (vvDD). We performed the first-in-human phase 1, intratumoral dose escalation clinical trial of vvDD in 16 patients with advanced solid tumors. In addition to safety, we evaluated signs of vvDD replication and spread to distant tumors, pharmacokinetics and pharmacodynamics, clinical and immune responses to vvDD. Dose escalation proceeded without dose-limiting toxicities to a maximum feasible dose of 3 x 10(9) pfu. vvDD replication in tumors was reproducible. vvDD genomes and/or infectious particles were recovered from injected (n = 5 patients) and noninjected (n = 2 patients) tumors. At the two highest doses, vvDD genomes were detected acutely in blood in all patients while delayed re-emergence of vvDD genomes in blood was detected in two patients. Fifteen of 16 patients exhibited late symptoms, consistent with ongoing vvDD replication. In summary, intratumoral injection of the oncolytic vaccinia vvDD was well-tolerated in patients and resulted in selective infection of injected and noninjected tumors and antitumor activity.
机译:溶瘤病毒疗法利用肿瘤选择性复制病毒,该病毒优先感染并破坏癌细胞并触发抗肿瘤免疫力。牛痘病毒(VV)的Western Reserve株是动物模型中最具毒性的VV株,经过两个靶向基因缺失(vvDD)的工程改造,具有一定的肿瘤选择性。我们在16例晚期实体瘤患者中进行了vvDD的人类首次1期体内肿瘤剂量递增临床试验。除了安全性,我们还评估了vvDD复制的迹象并传播到远处的肿瘤,药代动力学和药效学,对vvDD的临床和免疫反应。剂量逐步升高,没有毒性限制,最大可行剂量为3 x 10(9)pfu。 vvDD在肿瘤中的复制是可重现的。从已注射(n = 5例)和未注射(n = 2例)的肿瘤中回收了vvDD基因组和/或感染性颗粒。在两个最高剂量下,在所有患者的血液中均急性检测到vvDD基因组,而在两名患者的血液中检测到vvDD基因组的延迟再生。 16名患者中有15名表现出晚期症状,与正在进行的vvDD复制一致。总之,肿瘤内注射溶瘤牛痘vvDD在患者中具有良好的耐受性,并导致注射和未注射肿瘤的选择性感染和抗肿瘤活性。

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