Aggarwal Charu, Cohen Roger B, Morrow Matthew P, Kraynyak Kimberly A, Sylvester Albert J, Cheung Jocelyn, Dickerson Kelsie, Schulten Veronique, Knoblock Dawson, Gillespie Elisabeth, Bauml Joshua M, Yan Jian, Diehl Malissa, Boyer Jean, Dallas Michael, Kim J Joseph, Weiner David B, Skolnik Jeffrey M
Division of Hematology Oncology, University of Pennsylvania, Philadelphia, PA 19104, USA.
Inovio Pharmaceuticals, Inc., Plymouth Meeting, PA 19462, USA.
Vaccines (Basel). 2020 Jan 29;8(1):56. doi: 10.3390/vaccines8010056.
Background: Recurrent respiratory papillomatosis (RRP) is a rare disorder characterized by the generation of papillomas of the aerodigestive tract, usually associated with human papilloma virus (HPV) subtypes 6, 11. INO-3106 is a DNA plasmid-based immunotherapy targeting E6 and E7 proteins of HPV6, in order to create a robust immune T cell response.
Testing of INO-3016 in animal models confirmed immunogenicity of the DNA-based therapy. A single-site open-label Phase 1 study was initiated for patients with HPV6-positive RRP. Patients were dosed with INO-3106 with or without INO-9012, a DNA plasmid immunotherapy that encodes IL-12, delivered intramuscularly (IM) in combination with electroporation (EP) with the CELLECTRA device. Patients received an escalating dose of INO-3106, 3 mg once and then 6 mg for three additional doses, each dose three weeks apart, with the third and fourth doses co-administered with INO-9012. The primary objective of the study was to evaluate the safety and tolerability of INO-3106 with and without INO-9012. The secondary objective was to determine cellular immune responses to INO-3106 with and without INO-9012. Exploratory objectives included preliminary clinical efficacy to the therapy.
Three patients were enrolled in this study, of which two had RRP. Study therapy was well-tolerated, with no related serious adverse events and all related adverse events (AEs) were low-grade. Injection site pain was the most common related AE reported. Immunogenicity was evidenced by multiple immune assays showing engagement and expansion of an HPV6-specific cellular response, including cytotoxic T cells. Preliminary efficacy was demonstrated in patients with RRP in the form of reduction in need for surgical intervention for papilloma growth. Prior to intervention, both patients required surgical intervention approximately every 180 days. One patient demonstrated a greater than three-fold increase in surgery avoidance (584 days) and the other patient remains completely surgery-free as of the last contact at 915 days, a greater than 5-fold increase in surgery interval.
INO-3106 with and without INO-9012 was well tolerated, immunogenic and demonstrated preliminary efficacy in patients with HPV6-associated RRP aerodigestive lesions. Further clinical study is indicated.
背景:复发性呼吸道乳头状瘤病(RRP)是一种罕见疾病,其特征为在气道消化道产生乳头状瘤,通常与人乳头瘤病毒(HPV)6型、11型相关。INO-3106是一种基于DNA质粒的免疫疗法,靶向HPV6的E6和E7蛋白,以产生强大的免疫T细胞应答。
在动物模型中对INO-3016进行的测试证实了这种基于DNA的疗法具有免疫原性。针对HPV6阳性RRP患者启动了一项单中心开放标签1期研究。患者接受INO-3106治疗,联合或不联合INO-9012(一种编码IL-12的DNA质粒免疫疗法),通过CELLECTRA设备经肌肉注射(IM)并结合电穿孔(EP)给药。患者接受递增剂量的INO-3106,一次3mg,然后再额外注射3次6mg,每次剂量间隔3周,第三和第四剂与INO-9012联合给药。该研究的主要目的是评估联合或不联合INO-9012时INO-3106的安全性和耐受性。次要目的是确定联合或不联合INO-9012时对INO-3106的细胞免疫应答。探索性目的包括该疗法的初步临床疗效。
该研究共纳入3例患者,其中2例患有RRP。研究治疗耐受性良好,未出现相关严重不良事件,所有相关不良事件(AE)均为低级别。注射部位疼痛是报告的最常见相关AE。多种免疫测定证明了免疫原性,显示HPV6特异性细胞应答(包括细胞毒性T细胞)的参与和扩增。RRP患者表现出初步疗效,表现为乳头状瘤生长所需手术干预减少。在干预前,两名患者大约每180天需要进行一次手术干预。一名患者避免手术的时间增加了三倍多(584天),另一名患者截至最后一次随访915天时仍完全无需手术,手术间隔增加了五倍多。
联合或不联合INO-9012时,INO-3106耐受性良好,具有免疫原性,并在HPV6相关RRP气道消化道病变患者中显示出初步疗效。需要进一步进行临床研究。
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