Daratumumab induces cell-mediated cytotoxicity of primary effusion lymphoma and is active against refractory disease.

IF 7.2 2区 医学
Prabha Shrestha, Yana Astter, David A Davis, Ting Zhou, Constance M Yuan, Ramya Ramaswami, Hao-Wei Wang, Kathryn Lurain, Robert Yarchoan
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引用次数: 1

Abstract

Primary effusion lymphoma (PEL), an aggressive non-Hodgkin lymphoma caused by Kaposi sarcoma-associated herpesvirus (KSHV), lacks standard therapy and has a median survival of 10-22 months with combination chemotherapy. PEL is a tumor of plasmablast-like B cells generally expressing CD38, the target of daratumumab (Dara). Initially, we assessed PEL cells from eight patients and established that each expressed high levels of CD38 by flow cytometry. PEL cell lines were also evaluated and most had high CD38 expression. We then assessed Dara's effects on complement-dependent cytotoxicity (CDC) and antibody-dependent cell-mediated cytotoxicity (ADCC) of PEL cell lines as well as its clinical benefits on two patients with PEL. Despite high CD38 expression, Dara did not induce CDC of PEL cell lines, due in part to high levels of the complement-inhibitory proteins, CD55 and CD59. However, Dara induced significant and dose-dependent increases in ADCC, particularly in those lines with high CD38 levels. Two FDA-approved drugs, all trans-retinoic acid (ATRA) and pomalidomide (Pom), significantly increased surface CD38 levels in low-CD38 expressing PEL cell lines, resulting in increased Dara-induced ADCC. Two patients with refractory PEL were treated with Dara alone or in combination with Pom. One patient with leptomeningeal PEL had a complete response to Dara and Pom combination treatment. Others had improvement in performance status and resolution of malignant ascites with Dara alone. Together, these data support the use of Dara monotherapy or in combination with ATRA or Pom as a potential therapeutic option for PEL.

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达拉单抗诱导细胞介导的原发性积液性淋巴瘤的细胞毒性,并对难治性疾病有效。
原发性积液性淋巴瘤(PEL)是一种由卡波西肉瘤相关疱疹病毒(KSHV)引起的侵袭性非霍奇金淋巴瘤,缺乏标准治疗,联合化疗的中位生存期为10-22个月。PEL是一种通常表达CD38的质母细胞样B细胞肿瘤,CD38是达拉单抗(Dara)的靶点。最初,我们评估了来自8名患者的PEL细胞,并通过流式细胞术确定每个细胞都表达高水平的CD38。对PEL细胞系也进行了评估,大多数细胞系CD38表达水平较高。然后,我们评估了Dara对补体依赖性细胞毒性(CDC)和抗体依赖性细胞介导的细胞毒性(ADCC)的影响,以及它对两名PEL患者的临床益处。尽管CD38高表达,但Dara并未诱导PEL细胞系的CDC,部分原因是补体抑制蛋白CD55和CD59的高水平。然而,Dara诱导ADCC显著且剂量依赖性增加,特别是在那些CD38水平高的细胞系中。fda批准的两种药物,全反式维甲酸(ATRA)和pomalidomide (Pom),在低CD38表达的PEL细胞系中显著增加表面CD38水平,导致dara诱导的ADCC增加。2例难治性PEL患者单独或联合Pom治疗。1例脑膜轻脑膜PEL患者对Dara和Pom联合治疗有完全反应。另一些患者单独应用Dara治疗后,表现改善,恶性腹水消退。总之,这些数据支持使用Dara单一疗法或与ATRA或Pom联合作为PEL的潜在治疗选择。
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
Oncoimmunology ONCOLOGY-IMMUNOLOGY
CiteScore
12.80
自引率
2.80%
发文量
276
期刊介绍: Tumor immunology explores the natural and therapy-induced recognition of cancers, along with the complex interplay between oncogenesis, inflammation, and immunosurveillance. In response to recent advancements, a new journal, OncoImmunology, is being launched to specifically address tumor immunology. The field has seen significant progress with the clinical demonstration and FDA approval of anticancer immunotherapies. There's also growing evidence suggesting that many current chemotherapeutic agents rely on immune effectors for their efficacy. While oncologists have historically utilized chemotherapeutic and radiotherapeutic regimens successfully, they may have unwittingly leveraged the immune system's ability to recognize tumor-specific antigens and control cancer growth. Consequently, immunological biomarkers are increasingly crucial for cancer prognosis and predicting chemotherapy efficacy. There's strong support for combining conventional anticancer therapies with immunotherapies. OncoImmunology will welcome high-profile submissions spanning fundamental, translational, and clinical aspects of tumor immunology, including solid and hematological cancers, inflammation, and both innate and acquired immune responses.
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