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ISB 2001 三特异性 T 细胞衔接器显示出强大的肿瘤细胞毒性,并克服了多发性骨髓瘤细胞的免疫逃逸机制。

ISB 2001 trispecific T cell engager shows strong tumor cytotoxicity and overcomes immune escape mechanisms of multiple myeloma cells.

机构信息

Ichnos Glenmark Innovation, New York, NY, USA.

Certara UK Limited, Canterbury Innovation Centre, University Road, Canterbury, United Kingdom.

出版信息

Nat Cancer. 2024 Oct;5(10):1494-1514. doi: 10.1038/s43018-024-00821-1. Epub 2024 Sep 11.

DOI:10.1038/s43018-024-00821-1
PMID:39261676
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11505469/
Abstract

Despite recent advances in immunotherapies targeting single tumor-associated antigens, patients with multiple myeloma eventually relapse. ISB 2001 is a CD3 T cell engager (TCE) co-targeting BCMA and CD38 designed to improve cytotoxicity against multiple myeloma. Targeting of two tumor-associated antigens by a single TCE resulted in superior cytotoxic potency across a variable range of BCMA and CD38 tumor expression profiles mimicking natural tumor heterogeneity, improved resistance to competing soluble factors and exhibited superior cytotoxic potency on patient-derived samples and in mouse models. Despite the broad expression of CD38 across human tissues, ISB 2001 demonstrated a reduced T cell activation profile in the absence of tumor cells when compared to TCEs targeting CD38 only. To determine an optimal first-in-human dose for the ongoing clinical trial ( NCT05862012 ), we developed an innovative quantitative systems pharmacology model leveraging preclinical data, using a minimum pharmacologically active dose approach, therefore reducing patient exposure to subefficacious doses of therapies.

摘要

尽管针对单一肿瘤相关抗原的免疫疗法最近取得了进展,但多发性骨髓瘤患者最终仍会复发。ISB 2001 是一种靶向 BCMA 和 CD38 的 CD3 T 细胞衔接器(TCE),旨在提高对多发性骨髓瘤的细胞毒性。通过单个 TCE 靶向两个肿瘤相关抗原,可提高对模拟自然肿瘤异质性的不同 BCMA 和 CD38 肿瘤表达谱的细胞毒性效力,增强对竞争可溶性因子的抵抗力,并在患者来源的样本和小鼠模型中表现出更高的细胞毒性效力。尽管 CD38 在人类组织中广泛表达,但与仅靶向 CD38 的 TCE 相比,当不存在肿瘤细胞时,ISB 2001 显示出降低的 T 细胞激活谱。为了确定正在进行的临床试验(NCT05862012)的最佳首次人体剂量,我们开发了一种利用临床前数据的创新定量系统药理学模型,采用最低药效剂量方法,从而减少患者暴露于亚有效剂量的治疗药物。

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