在商业嵌合抗原受体 T 细胞疗法治疗复发或难治性侵袭性 B 细胞淋巴瘤之前桥接放射治疗。
Bridging Radiation Therapy Before Commercial Chimeric Antigen Receptor T-Cell Therapy for Relapsed or Refractory Aggressive B-Cell Lymphoma.
机构信息
Department of Radiation Oncology, University of Pennsylvania, Philadelphia, Pennsylvania.
Department of Radiation Oncology, University of Pennsylvania, Philadelphia, Pennsylvania.
出版信息
Int J Radiat Oncol Biol Phys. 2020 Sep 1;108(1):178-188. doi: 10.1016/j.ijrobp.2020.05.014. Epub 2020 May 22.
PURPOSE
CD19-targeting chimeric antigen receptor T-cell (CART) therapy has emerged as a promising treatment for relapsed/refractory aggressive B-cell lymphoma (r/rABL), culminating in 2 US Food and Drug Administration-approved therapies: tisagenlecleucel (tisa-cel) and axicabtagene ciloleucel (axi-cel). Following leukapheresis and in preparation for CART infusion, contemporary bridging and lymphodepletion regimens rely mostly on cytotoxic chemotherapy. Here, in a cohort of patients treated with commercial tisa-cel and axi-cel, we show that bridging-RT may offer a supplemental approach.
METHODS AND MATERIALS
Thirty-one patients receiving commercial tisa-cel (n = 13) or axi-cel (n = 18) between August 2018 and February 2019 for r/rABL were retrospectively reviewed. Patients were categorized into 2 groups: (1) bridging-RT within 30 days of CART infusion or (2) nonbridging-RT (NBRT), in which patients received either remote RT greater than 30 days before CART infusion or no prior RT.
RESULTS
Five patients received bridging-RT within 30 days of CART infusion. Median bridging-RT dose was 37.5 Gy and was completed a median of 13 days before infusion. No grade 3 (G3) or higher RT-toxicities occurred. No patients in the bridging-RT group experienced G3 or higher CART-related toxicities (CRS or neurotoxicity), and 23% (n = 6) and 15% (n = 4) experienced G3-5 CRS and G3-5 neurotoxicity in the NBRT group, respectively. Overall treatment response in the bridging-RT and NBRT groups was 80% and 64%, respectively. The axi-cel CART product was associated with CRS (odds ratio [OR] = 26.67, P = .001) and CRS correlated with neurotoxicity (OR = 12.22, P = .028). There was a trend toward an association for CRS with metabolic tumor volume (OR = 1.06/mL, P = .141) and TLG (OR = 1.01/mL x standard uptake value, P = .099).
CONCLUSIONS
Bridging-RT before commercial CART does not appear to increase the risk for CART-related toxicities or negatively affect outcomes in r/rABL patients. No G3 or higher RT-toxicities occurred in this series. Pretreatment metabolic tumor burden may be associated with CART-associated CRS; however, larger patient numbers are required to elucidate significant associations. Future work to prospectively assess the value of bridging-RT is warranted.
目的
CD19 靶向嵌合抗原受体 T 细胞(CART)疗法已成为治疗复发/难治性侵袭性 B 细胞淋巴瘤(r/rABL)的一种有前途的方法,最终有 2 种美国食品和药物管理局批准的疗法:tisagenlecleucel(tisa-cel)和 axicabtagene ciloleucel(axi-cel)。在白细胞分离术之后并为 CART 输注做准备时,当代桥接和淋巴耗竭方案主要依赖细胞毒性化学疗法。在这里,在接受商业 tisa-cel 和 axi-cel 治疗的患者队列中,我们表明桥接-RT 可能是一种补充方法。
方法和材料
2018 年 8 月至 2019 年 2 月期间,31 例接受商业 tisa-cel(n = 13)或 axi-cel(n = 18)治疗 r/rABL 的患者进行了回顾性分析。患者分为 2 组:(1)CART 输注前 30 天内进行桥接-RT;或(2)非桥接-RT(NBRT),其中患者接受 CART 输注前大于 30 天的远程 RT 或无先前 RT。
结果
5 例患者在 CART 输注前 30 天内接受桥接-RT。中位桥接-RT 剂量为 37.5Gy,输注前中位完成时间为 13 天。没有发生 3 级(G3)或更高的 RT 毒性。桥接-RT 组无患者发生 G3 或更高级别的 CART 相关毒性(细胞因子释放综合征(CRS)或神经毒性),NBRT 组分别有 23%(n = 6)和 15%(n = 4)发生 G3-5 CRS 和 G3-5 神经毒性。桥接-RT 组和 NBRT 组的总体治疗反应率分别为 80%和 64%。axi-cel CART 产品与 CRS 相关(比值比 [OR] = 26.67,P =.001),CRS 与神经毒性相关(OR = 12.22,P =.028)。CRS 与代谢肿瘤体积(OR = 1.06/mL,P =.141)和 TLG(OR = 1.01/mL x 标准摄取值,P =.099)之间存在关联的趋势。
结论
在商业 CART 之前进行桥接-RT 似乎不会增加 CART 相关毒性的风险,也不会对 r/rABL 患者的结局产生负面影响。本系列中未发生 G3 或更高的 RT 毒性。治疗前代谢肿瘤负荷可能与 CART 相关的 CRS 相关;然而,需要更大的患者数量来阐明显著的相关性。有必要进行前瞻性评估桥接-RT 价值的未来工作。
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