西罗莫司联合ganetespib治疗难治性肉瘤和恶性外周神经鞘瘤的I/II期研究（SARC023）

Targeting Refractory Sarcomas and Malignant Peripheral Nerve Sheath Tumors in a Phase I/II Study of Sirolimus in Combination with Ganetespib (SARC023).

作者信息

Kim AeRang, Lu Yao, Okuno Scott H, Reinke Denise, Maertens Ophélia, Perentesis John, Basu Mitali, Wolters Pamela L, De Raedt Thomas, Chawla Sant, Chugh Rashmi, Van Tine Brian A, O'Sullivan Geraldine, Chen Alice, Cichowski Karen, Widemann Brigitte C

机构信息

Children's National Medical Center, 111 Michigan Ave., NW, Washington, DC 20010, USA.

SARC Statistics, Weill Cornell Medicine Healthcare and Policy Research, 602 East 67 Street, New York, NY 10065, USA.

出版信息

Sarcoma. 2020 Jan 30;2020:5784876. doi: 10.1155/2020/5784876. eCollection 2020.

DOI:10.1155/2020/5784876

PMID:32089640

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7013290/

Abstract

PURPOSE

Malignant peripheral nerve sheath tumors (MPNSTs) are aggressive soft tissue sarcomas. Combining Hsp90 inhibitors to enhance endoplasmic reticulum stress with mTOR inhibition results in dramatic MPNST shrinkage in a genetically engineered MPNST mouse model. Ganetespib is an injectable potent small molecule inhibitor of Hsp90. Sirolimus is an oral mTOR inhibitor. We sought to determine the safety, tolerability, and recommended dose of ganetespib and sirolimus in patients with refractory sarcomas and assess clinical benefits in patients with unresectable/refractory MPNSTs. . In this multi-institutional, open-label, phase 1/2 study of ganetespib and sirolimus, patients ≥16 years with histologically confirmed refractory sarcoma (phase 1) or MPNST (phase 2) were eligible. A conventional 3 + 3 dose escalation design was used for phase 1. Pharmacokinetic and pharmacodynamic measures were evaluated. Primary objectives of phase 2 were to determine the clinical benefit rate (CBR) of this combination in MPNSTs. Patient-reported outcomes assessed pain.

RESULTS

Twenty patients were enrolled (10 per phase). Toxicities were manageable; most frequent non-DLTs were diarrhea, elevated liver transaminases, and fatigue. The recommended dose of ganetespib was 200 mg/m intravenously on days 1, 8, and 15 with sirolimus 4 mg orally once daily with day 1 loading dose of 12 mg. In phase 1, one patient with leiomyosarcoma achieved a sustained partial response. In phase 2, no responses were observed. The median number of cycles treated was 2 (1-4). Patients did not meet the criteria for clinical benefit as defined per protocol. Pain ratings decreased or were stable.

CONCLUSION

Despite promising preclinical rationale and tolerability of the combination therapy, no responses were observed, and the study did not meet parameters for further evaluation in MPNSTs. This trial was registered with (NCT02008877).

摘要

目的

恶性外周神经鞘瘤（MPNSTs）是侵袭性软组织肉瘤。在基因工程MPNST小鼠模型中，联合使用热休克蛋白90（Hsp90）抑制剂增强内质网应激与雷帕霉素靶蛋白（mTOR）抑制可导致MPNST显著缩小。ganetespib是一种可注射的强效Hsp90小分子抑制剂。西罗莫司是一种口服mTOR抑制剂。我们试图确定ganetespib和西罗莫司在难治性肉瘤患者中的安全性、耐受性和推荐剂量，并评估不可切除/难治性MPNST患者的临床获益情况。在这项关于ganetespib和西罗莫司的多机构、开放标签的1/2期研究中，年龄≥16岁、组织学确诊为难治性肉瘤（1期）或MPNST（2期）的患者符合条件。1期采用传统的3+3剂量递增设计。评估了药代动力学和药效学指标。2期的主要目标是确定该联合方案在MPNST中的临床获益率（CBR）。患者报告的结局评估了疼痛情况。

结果

共纳入20例患者（每期10例）。毒性反应可控；最常见的非剂量限制性毒性是腹泻、肝转氨酶升高和疲劳。ganetespib的推荐剂量为在第1、8和15天静脉注射200mg/m²，西罗莫司为每日口服4mg，第1天负荷剂量为12mg。在1期，1例平滑肌肉瘤患者获得持续部分缓解。在2期，未观察到缓解。治疗的中位周期数为2（1-4）。患者未达到方案定义的临床获益标准。疼痛评分降低或稳定。

结论

尽管联合治疗有前景良好的临床前理论依据和耐受性，但未观察到缓解，该研究未达到MPNST进一步评估的参数标准。本试验已在（NCT02008877）注册。

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西罗莫司联合ganetespib治疗难治性肉瘤和恶性外周神经鞘瘤的I/II期研究（SARC023）

Targeting Refractory Sarcomas and Malignant Peripheral Nerve Sheath Tumors in a Phase I/II Study of Sirolimus in Combination with Ganetespib (SARC023).

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