Centre de Recherche des Cordeliers, Université Paris Cité, Sorbonne Université, Equipe labellisée par la Ligue contre le cancer, Inserm U1138, Paris, France.
Metabolomics and Cell Biology Platforms, Gustave Roussy Institut, Villejuif, France.
Mol Cancer. 2024 Sep 6;23(1):187. doi: 10.1186/s12943-024-02098-5.
The plasma concentrations of acyl coenzyme A binding protein (ACBP, also known as diazepam-binding inhibitor, DBI, or 'endozepine') increase with age and obesity, two parameters that are also amongst the most important risk factors for cancer.
We measured ACBP/DBI in the plasma from cancer-free individuals, high-risk patients like the carriers of TP53 or BRCA1/2 mutations, and non-syndromic healthy subjects who later developed cancer. In mice, the neutralization of ACBP/DBI was used in models of non-small cell lung cancer (NSCLC) and breast cancer development and as a combination treatment with chemoimmunotherapy (chemotherapy + PD-1 blockade) in the context of NSCLC and sarcomas. The anticancer T cell response upon ACBP/DBI neutralization was characterized by flow cytometry and single-cell RNA sequencing.
Circulating levels of ACBP/DBI were higher in patients with genetic cancer predisposition (BRCA1/2 or TP53 germline mutations) than in matched controls. In non-syndromic cases, high ACBP/DBI levels were predictive of future cancer development, and especially elevated in patients who later developed lung cancer. In preclinical models, ACBP/DBI neutralization slowed down breast cancer and NSCLC development and enhanced the efficacy of chemoimmunotherapy in NSCLC and sarcoma models. When combined with chemoimmunotherapy, the neutralizing monoclonal antibody against ACBP/DBI reduced the frequency of regulatory T cells in the tumor bed, modulated the immune checkpoint profile, and increased activation markers.
These findings suggest that ACBP/DBI acts as an endogenous immune suppressor. We conclude that elevation of ACBP/DBI constitutes a risk factor for the development of cancer and that ACBP/DBI is an actionable target for improving cancer immunosurveillance.
酰基辅酶 A 结合蛋白(ACBP,也称为地西泮结合抑制剂、DBI 或“内源性安定”)的血浆浓度随着年龄和肥胖而增加,这两个参数也是癌症最重要的危险因素之一。
我们测量了无癌症个体、携带 TP53 或 BRCA1/2 突变等高危患者以及后来发生癌症的非综合征健康受试者的血浆中的 ACBP/DBI。在小鼠中,使用 ACBP/DBI 的中和作用在非小细胞肺癌(NSCLC)和乳腺癌发展模型中以及 NSCLC 和肉瘤的化疗免疫治疗(化疗+PD-1 阻断)联合治疗中进行了研究。ACBP/DBI 中和作用后的抗癌 T 细胞反应通过流式细胞术和单细胞 RNA 测序进行了表征。
具有遗传癌症易感性(BRCA1/2 或 TP53 种系突变)的患者的循环 ACBP/DBI 水平高于匹配对照。在非综合征病例中,高 ACBP/DBI 水平预示着未来癌症的发展,尤其是在后来发生肺癌的患者中升高。在临床前模型中,ACBP/DBI 的中和作用减缓了乳腺癌和 NSCLC 的发展,并增强了 NSCLC 和肉瘤模型中化疗免疫治疗的疗效。当与化疗免疫治疗联合使用时,针对 ACBP/DBI 的中和单克隆抗体减少了肿瘤床中的调节性 T 细胞频率,调节了免疫检查点谱,并增加了激活标志物。
这些发现表明 ACBP/DBI 作为一种内源性免疫抑制剂发挥作用。我们得出结论,ACBP/DBI 的升高构成了癌症发展的危险因素,并且 ACBP/DBI 是改善癌症免疫监测的可行靶点。
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