A phase 2 trial of CXCR4 antagonism and PD1 inhibition in metastatic pancreatic adenocarcinoma reveals recruitment of T cells but also immunosuppressive macrophages.

IF 6.5 2区医学 Q1 IMMUNOLOGY

Oncoimmunology Pub Date : 2025-12-01 Epub Date: 2025-08-15 DOI:10.1080/2162402X.2025.2543614

Katherine M Bever, Sarah M Shin, Jennifer N Durham, Hanfei Qi, Alexei Hernandez, Erin M Coyne, Nicole E Gross, Soren Charmsaz, Jayalaxmi Suresh Babu, Diana Carolina Vargas Carvajal, Rohan Verma, Yanyi Sun, Zhehao Zhang, Xuan Yuan, Courtney D Cannon, Sarah N Hughes, Sarah Mitchell, Madeline Figlewski, James M Leatherman, Hao Wang, Robert A Anders, Elizabeth M Jaffee, Dung T Le, Won Jin Ho

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引用次数: 0

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is characterized by dense stroma and myeloid-rich microenvironment that confer resistance to immunotherapies. Previous studies demonstrated that disrupting the immune-stroma CXCR4-CXCL12 axis facilitates T cell recruitment and mobility to collaborate with anti-PD1/PD-L1 therapy. We sought to test the clinical viability of this immunotherapeutic strategy. 21 patients with metastatic PDAC were enrolled and treated in a phase 2 trial evaluating the effects of the plerixafor/AMD3100 and cemiplimab. Primary endpoint was objective response rate. Blood and tissue biospecimens were collected for correlative analyses. Parallel mouse studies were used to determine potential mechanisms of resistance. Treatments were well-tolerated, but only two patients demonstrated a best response of stable disease. Correlative analyses confirmed significant mobilization of immune cells into circulation as well as increased immune infiltration into the tumor. High-parameter imaging revealed higher levels of CD8⁺ T cells but also granulocytes and macrophages upon treatment. Spatial analysis showed that treatment resulted in closer proximity between macrophages and T cells but not between granulocytes and T cells. Mouse studies revealed that whereas total granulocyte depletion had no effect on immunotherapeutic efficacy, macrophage-targeting yielded significant benefit. Tumor growth measurements and immune profiling of immunotherapeutic combinations incorporating macrophage-targeting showed that despite the increased T cell infiltration, CXCR4 antagonism was in fact associated with enrichment of CD206^hiIA/IE^lo macrophage subtypes and modestly dampened efficacy. Our findings validate the utility of CXCR4 antagonism as an effective immune-recruiting platform but also underscores the need for strategies that better leverage its effects.

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一项在转移性胰腺腺癌中CXCR4拮抗和PD1抑制的2期试验显示，T细胞和免疫抑制巨噬细胞的募集。

胰腺导管腺癌（PDAC）的特点是致密的间质和富含骨髓的微环境，赋予免疫治疗的抗性。先前的研究表明，破坏免疫基质CXCR4-CXCL12轴有助于T细胞的募集和迁移，从而协同抗pd1 /PD-L1治疗。我们试图测试这种免疫治疗策略的临床可行性。21例转移性PDAC患者参加了一项评估plerixafor/AMD3100和cemiplimab疗效的2期试验。主要终点为客观有效率。采集血液和组织生物标本进行相关分析。平行小鼠研究用于确定潜在的耐药机制。治疗耐受性良好，但只有两名患者表现出病情稳定的最佳反应。相关分析证实免疫细胞明显动员进入循环，免疫细胞浸润肿瘤增加。高参数成像显示治疗后CD8+ T细胞、粒细胞和巨噬细胞水平升高。空间分析显示，治疗导致巨噬细胞和T细胞之间的距离更近，而粒细胞和T细胞之间没有距离。小鼠研究表明，尽管总粒细胞消耗对免疫治疗效果没有影响，但巨噬细胞靶向却产生了显著的益处。结合巨噬细胞靶向的免疫治疗组合的肿瘤生长测量和免疫分析显示，尽管T细胞浸润增加，但CXCR4拮抗实际上与CD206hiIA/IElo巨噬细胞亚型的富集有关，并适度抑制疗效。我们的研究结果证实了CXCR4拮抗剂作为一种有效的免疫招募平台的效用，但也强调了更好地利用其效果的策略的必要性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Oncoimmunology ONCOLOGYIMMUNOLOGY-IMMUNOLOGY

CiteScore

12.50

自引率

2.80%

发文量

276

审稿时长

24 weeks

期刊介绍： OncoImmunology is a dynamic, high-profile, open access journal that comprehensively covers tumor immunology and immunotherapy. As cancer immunotherapy advances, OncoImmunology is committed to publishing top-tier research encompassing all facets of basic and applied tumor immunology. The journal covers a wide range of topics, including: -Basic and translational studies in immunology of both solid and hematological malignancies -Inflammation, innate and acquired immune responses against cancer -Mechanisms of cancer immunoediting and immune evasion -Modern immunotherapies, including immunomodulators, immune checkpoint inhibitors, T-cell, NK-cell, and macrophage engagers, and CAR T cells -Immunological effects of conventional anticancer therapies.