Department of Surgery (DI.C.M.I.), Genoa University, Genoa, Italy.
J Surg Oncol. 2013 Feb;107(2):173-9. doi: 10.1002/jso.23168. Epub 2012 Jun 4.
L19-TNF is a tumor-targeting immunocytokine composed of the human L19 antibody binding to extra domain B (ED-B) of fibronectin of newly formed blood vessels, and of human TNF. This exploratory trial evaluates safety and clinical activity of L19-TNF plus melphalan-containing isolated limb perfusion (ILP) in extremity melanoma patients.
Seven and 10 patients received 325 µg and 650 µg of L19-TNF, respectively, during the ILP. Patients were studied for safety, tolerability, and clinical activity of this experimental L19-TNF ILP procedure.
Non-hematologic toxicity of L19-TNF ILP was very low, but severe myelosuppression was seen in four patients. Although L19-TNF was administered at a TNF-equivalent dose of only 3.13 and 6.25% of the approved TNF (Beromun®) dose of 4 mg, L19-TNF ILP induced objective responses in 86 and 89% of patients, respectively, including a complete response (CR) in 5/10 patients treated with L19-TNF ILP at 650 µg that was durable at 12 months in four patients. No CR was seen at 325 µg of L19-TNF.
ILP with L19-TNF had a favorable safety and a promising activity profile at a dose of 650 µg of L19-TNF, supporting the exploration of higher L19-TNF doses and a Phase II trial comparing L19-TNF ILP with standard melphalan-containing ILP.
L19-TNF 是一种肿瘤靶向免疫细胞因子,由与人纤连蛋白新形成血管的 ED-B 结合的人 L19 抗体和人 TNF 组成。这项探索性试验评估了 L19-TNF 联合包含美法仑的肢体隔离灌注(ILP)在肢体黑色素瘤患者中的安全性和临床活性。
7 名和 10 名患者分别在 ILP 中接受 325µg 和 650µg 的 L19-TNF。研究人员研究了这种实验性 L19-TNF ILP 程序的安全性、耐受性和临床活性。
L19-TNF ILP 的非血液学毒性非常低,但有 4 名患者出现严重的骨髓抑制。尽管 L19-TNF 的 TNF 等效剂量仅为批准的 TNF(Beromun®)剂量 4mg 的 3.13%和 6.25%,但 L19-TNF ILP 分别使 86%和 89%的患者产生了客观反应,包括 L19-TNF ILP 在 650µg 剂量下治疗的 10 名患者中有 5 名完全缓解(CR),4 名患者的 CR 持续 12 个月。在 325µg 的 L19-TNF 中未观察到 CR。
在 650µg 的 L19-TNF 剂量下,ILP 联合 L19-TNF 具有良好的安全性和有前途的活性特征,支持探索更高剂量的 L19-TNF 和比较 L19-TNF ILP 与标准含美法仑的 ILP 的 II 期试验。
