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一种组织蛋白酶靶向猝灭活性的探针可增强肿瘤切除过程中的人肿瘤检测。

A Cathepsin-Targeted Quenched Activity-Based Probe Facilitates Enhanced Detection of Human Tumors during Resection.

机构信息

Department of Surgery, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania.

Department of Clinical Sciences and Advanced Medicine, University of Pennsylvania School of Veterinary Medicine, Philadelphia, Pennsylvania.

出版信息

Clin Cancer Res. 2022 Sep 1;28(17):3729-3741. doi: 10.1158/1078-0432.CCR-22-1215.

Abstract

PURPOSE

Fluorescence-guided surgery using tumor-targeted contrast agents has been developed to improve the completeness of oncologic resections. Quenched activity-based probes that fluoresce after covalently binding to tumor-specific enzymes have been proposed to improve specificity, but none have been tested in humans. Here, we report the successful clinical translation of a cathepsin activity-based probe (VGT-309) for fluorescence-guided surgery.

EXPERIMENTAL DESIGN

We optimized the specificity, dosing, and timing of VGT-309 in preclinical models of lung cancer. To evaluate clinical feasibility, we conducted a canine study of VGT-309 during pulmonary tumor resection. We then conducted a randomized, double-blind, dose-escalation study in healthy human volunteers receiving VGT-309 to evaluate safety. Finally, we tested VGT-309 in humans undergoing lung cancer surgery.

RESULTS

In preclinical models, we found highly specific tumor cell labeling that was blocked by a broad spectrum cathepsin inhibitor. When evaluating VGT-309 for guidance during resection of canine tumors, we found that the probe selectively labeled tumors and demonstrated high tumor-to-background ratio (TBR; range: 2.15-3.71). In the Phase I human study, we found that VGT-309 was safe at all doses studied. In the ongoing Phase II trial, we report two cases in which VGT-309 localized visually occult, non-palpable tumors (TBRs = 2.83 and 7.18) in real time to illustrate its successful clinical translation and potential to improve surgical management.

CONCLUSIONS

This first-in-human study demonstrates the safety and feasibility of VGT-309 to label human pulmonary tumors during resection. These results may be generalizable to other cancers due to cathepsin overexpression in many solid tumors.

摘要

目的

荧光引导手术使用肿瘤靶向对比剂已被开发出来,以提高肿瘤切除的完整性。已经提出了荧光后共价结合到肿瘤特异性酶的淬灭活性探针以提高特异性,但没有在人体中进行测试。在这里,我们报告了一种组织蛋白酶活性探针(VGT-309)成功的临床转化,用于荧光引导手术。

实验设计

我们在肺癌的临床前模型中优化了 VGT-309 的特异性、剂量和时间。为了评估临床可行性,我们在肺肿瘤切除过程中对 VGT-309 进行了犬研究。然后,我们在健康的人类志愿者中进行了一项随机、双盲、剂量递增研究,以评估 VGT-309 的安全性。最后,我们在接受肺癌手术的患者中测试了 VGT-309。

结果

在临床前模型中,我们发现了具有高度特异性的肿瘤细胞标记,该标记被广谱组织蛋白酶抑制剂阻断。当评估 VGT-309 用于指导犬肿瘤切除时,我们发现该探针选择性地标记肿瘤,并表现出高肿瘤与背景比(TBR;范围:2.15-3.71)。在 1 期人体研究中,我们发现 VGT-309 在所有研究剂量下均安全。在正在进行的 2 期试验中,我们报告了两例 VGT-309 实时定位视觉隐匿、不可触及肿瘤(TBR 分别为 2.83 和 7.18)的病例,以说明其成功的临床转化及其改善手术管理的潜力。

结论

这项人体首次研究证明了 VGT-309 在切除过程中标记人类肺部肿瘤的安全性和可行性。由于许多实体瘤中组织蛋白酶过表达,这些结果可能适用于其他癌症。

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