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胶原锚定白细胞介素-2 和白细胞介素-12 安全重塑犬软组织肉瘤的肿瘤微环境。

Collagen-Anchored Interleukin-2 and Interleukin-12 Safely Reprogram the Tumor Microenvironment in Canine Soft-Tissue Sarcomas.

机构信息

Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, Massachusetts.

Department of Biological Engineering, Massachusetts Institute of Technology, Cambridge, Massachusetts.

出版信息

Clin Cancer Res. 2023 Jun 1;29(11):2110-2122. doi: 10.1158/1078-0432.CCR-23-0006.

Abstract

PURPOSE

Cytokine therapies such as IL2 and IL12 suffer from impractically small therapeutic windows driven by their on-target, off-tumor activity, limiting their clinical potential despite potent antitumor effects. We previously engineered cytokines that bind and anchor to tumor collagen following intratumoral injection, and sought to test their safety and biomarker activity in spontaneous canine soft-tissue sarcomas (STS).

EXPERIMENTAL DESIGN

Collagen-binding cytokines were canine-ized to minimize immunogenicity and were used in a rapid dose-escalation study in healthy beagles to identify a maximum tolerated dose. Ten client-owned pet dogs with STS were then enrolled into trial, receiving cytokines at different intervals prior to surgical tumor excision. Tumor tissue was analyzed through IHC and NanoString RNA profiling for dynamic changes within treated tumors. Archived, untreated STS samples were analyzed in parallel as controls.

RESULTS

Intratumorally administered collagen-binding IL2 and IL12 were well tolerated by STS-bearing dogs, with only Grade 1/2 adverse events observed (mild fever, thrombocytopenia, neutropenia). IHC revealed enhanced T-cell infiltrates, corroborated by an enhancement in gene expression associated with cytotoxic immune function. We found concordant increases in expression of counter-regulatory genes that we hypothesize would contribute to a transient antitumor effect, and confirmed in mouse models that combination therapy to inhibit this counter-regulation can improve responses to cytokine therapy.

CONCLUSIONS

These results support the safety and activity of intratumorally delivered, collagen-anchoring cytokines for inflammatory polarization of the canine STS tumor microenvironment. We are further evaluating the efficacy of this approach in additional canine cancers, including oral malignant melanoma.

摘要

目的

细胞因子疗法,如 IL2 和 IL12,由于其在目标肿瘤外的活性,治疗窗口非常小,限制了其临床应用潜力,尽管它们具有强大的抗肿瘤作用。我们之前设计了可以与肿瘤胶原结合并锚定的细胞因子,旨在测试其在自发性犬软组织肉瘤(STS)中的安全性和生物标志物活性。

实验设计

胶原结合细胞因子被犬源化以最大程度降低免疫原性,并在健康比格犬中进行快速剂量递增研究,以确定最大耐受剂量。然后,将 10 只患有 STS 的宠物犬纳入试验,在手术切除肿瘤前,以不同的间隔接受细胞因子治疗。通过免疫组化(IHC)和 NanoString RNA 谱分析,研究肿瘤组织内的动态变化。同时分析存档的、未经治疗的 STS 样本作为对照。

结果

STS 犬对瘤内给予的胶原结合 IL2 和 IL12 具有良好的耐受性,仅观察到 1/2 级不良事件(轻度发热、血小板减少、中性粒细胞减少)。IHC 显示增强的 T 细胞浸润,这与与细胞毒性免疫功能相关的基因表达增强一致。我们发现,与负调节相关的基因表达也呈一致性增加,我们假设这些基因会促进短暂的抗肿瘤效应,并在小鼠模型中证实,联合抑制这种负调节可以改善细胞因子治疗的反应。

结论

这些结果支持瘤内给予胶原锚定细胞因子的安全性和活性,用于犬 STS 肿瘤微环境的炎症极化。我们正在进一步评估这种方法在其他犬类癌症中的疗效,包括口腔恶性黑色素瘤。

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Intratumorally anchored cytokine therapy.瘤内锚定细胞因子疗法。
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