三种靶向CD79b的新型嵌合抗原受体用于治疗非霍奇金淋巴瘤的临床前开发及靶抗原丢失的特征分析
Preclinical development of three novel CARs targeting CD79b for the treatment of non-Hodgkin's lymphoma and characterization of the loss of the target antigen.
作者信息
Esquinas Esperanza, Moreno-Sanz Alvaro, Sandá Victor, Stodulski-Ciesla Damian, Borregón Jennifer, Peña-Blanque Virginia, Fernández-Calles Javier, Fernandez-Fuentes Narcis, Serrano-Lopez Juana, Juan Manel, Engel Pablo, Llamas-Sillero Pilar, Solán-Blanco Laura, Martin-Antonio Beatriz
机构信息
Department of Experimental Hematology, Health Research Institute of the Jimenez Diaz Foundation, UAM, Madrid, Spain, UAM, Madrid, Spain.
Next Generation CART MAD Consortium, Madrid, Spain.
出版信息
J Immunother Cancer. 2024 Dec 18;12(12):e009485. doi: 10.1136/jitc-2024-009485.
BACKGROUND
Infusion of T cells modified with a chimeric antigen receptor (CAR) targeting CD19 has achieved exceptional responses in patients with non-Hodgkin's lymphoma (NHL), which led to the approval of CAR targeting CD19 (CART19) (Axi-cel and Liso-cel) as second line of treatment for adult patients with relapsed/refractory NHL. Unfortunately, 60% of patients still relapse after CART19 due to either a loss of expression of the target antigen (CD19) in the tumor cell, observed in 27% of relapsed patients, a limited CAR-T persistence, and additional mechanisms, including the suppression of the tumor microenvironment. Clinic strategies to prevent target antigen loss include sequential treatment with CARs directed at CD20 or CD22, which have caused loss of the second antigen, suggesting targeting other antigens less prone to disappear. CD79b, expressed in NHL, is a target in patients treated with antibody-drug conjugates (ADC). However, the limited efficacy of ADC suggests that a CAR therapy targeting CD79b might improve results.
METHODS
We designed three new CARs against CD79b termed CAR for Lymphoma (CARLY)1, 2 and 3. We compared their efficacy, phenotype, and inflammatory profiles with CART19 (ARI0001) and CARTBCMA (ARI0002h), which can treat NHL. We also analyzed the target antigen's expression loss (CD79b, CD19, and B-cell maturation antigen(BCMA)).
RESULTS
We found that CARLY2 and CARLY3 had high affinity and specificity towards CD79b on B cells. In vitro, all CAR-T cells had similar anti-NHL efficacy, which was retained in an NHL model of CD19 relapse. In vivo, CARLY3 showed the highest efficacy. Analysis of the loss of the target antigen demonstrated that CARLY cells induced CD79b and CD19 downregulation on NHL cells with concomitant trogocytosis of these antigens to T cells, being most notorious in CARLY2, which had the highest affinity towards CD79b and CD19, and supporting the selection of CARLY3 to design a new treatment for patients with NHL. Finally, we created a CAR treatment based on dual targeting of CD79b and BCMA to avoid losing the target antigen. This treatment showed the highest efficacy and did not cause loss of the target antigen.
CONCLUSIONS
Based on specificity, efficacy, and loss of the target antigen, CARLY3 represents a potential novel CAR treatment for NHL.
背景
输注靶向CD19的嵌合抗原受体(CAR)修饰的T细胞已在非霍奇金淋巴瘤(NHL)患者中取得了显著疗效,这使得靶向CD19的CAR(CART19,即阿基仑赛和利基仑赛)被批准作为复发/难治性NHL成年患者的二线治疗方案。不幸的是,60%的患者在接受CART19治疗后仍会复发,原因包括肿瘤细胞中靶抗原(CD19)表达缺失(27%的复发患者中观察到)、CAR-T细胞持久性有限以及其他机制,包括肿瘤微环境的抑制。预防靶抗原丢失的临床策略包括序贯使用靶向CD20或CD22的CAR进行治疗,但这会导致第二种抗原丢失,提示应靶向其他不易消失的抗原。在NHL中表达的CD79b是接受抗体药物偶联物(ADC)治疗患者的一个靶点。然而,ADC的疗效有限,提示靶向CD79b的CAR疗法可能会改善治疗结果。
方法
我们设计了三种针对CD79b的新型CAR,分别称为淋巴瘤CAR(CARLY)1、2和3。我们将它们的疗效、表型和炎症特征与可治疗NHL的CART19(ARI0001)和CARTBCMA(ARI0002h)进行了比较。我们还分析了靶抗原的表达缺失情况(CD79b、CD19和B细胞成熟抗原(BCMA))。
结果
我们发现CARLY2和CARLY3对B细胞上的CD79b具有高亲和力和特异性。在体外,所有CAR-T细胞具有相似的抗NHL疗效,在CD19复发的NHL模型中该疗效得以保留。在体内,CARLY3显示出最高疗效。对靶抗原丢失的分析表明,CARLY细胞可诱导NHL细胞上的CD79b和CD19下调,同时这些抗原被T细胞胞啃作用摄取,在对CD79b和CD19亲和力最高的CARLY2中最为明显,这支持选择CARLY3来设计针对NHL患者新的治疗方案。最后,我们创建了一种基于CD79b和BCMA双靶向的CAR治疗方案,以避免靶抗原丢失。该治疗方案显示出最高疗效且未导致靶抗原丢失。
结论
基于特异性、疗效和靶抗原丢失情况,CARLY3代表了一种潜在的NHL新型CAR治疗方案。
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