Dual targeting of CD19 and CD22 against B-ALL using a novel high-sensitivity aCD22 CAR

利用新型高灵敏度 aCD22 CAR 双重靶向 CD19 和 CD22 治疗 B 细胞急性淋巴细胞白血病 (B-ALL)。

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作者:Evangelia Kokalaki ,Biao Ma ,Mathieu Ferrari ,Thomas Grothier ,Warren Hazelton ,Somayya Manzoor ,Eren Costu ,Julia Taylor ,Anna Bulek ,Saket Srivastava ,Isaac Gannon ,Ram Jha ,Rosalind Gealy ,Lukas Stanczuk ,Tatiana Rizou ,Mathew Robson ,Mohamed El-Kholy ,Vania Baldan ,Matteo Righi ,James Sillibourne ,Simon Thomas ,Shimobi Onuoha ,Shaun Cordoba ,Martin Pule

Abstract

CAR T cells recognizing CD19 effectively treat relapsed and refractory B-ALL and DLBCL. However, CD19 loss is a frequent cause of relapse. Simultaneously targeting a second antigen, CD22, may decrease antigen escape, but is challenging: its density is approximately 10-fold less than CD19, and its large structure may hamper immune synapse formation. The characteristics of the optimal CD22 CAR are underexplored. We generated 12 distinct CD22 antibodies and tested CARs derived from them to identify a CAR based on the novel 9A8 antibody, which was sensitive to low CD22 density and lacked tonic signaling. We found no correlation between affinity or membrane proximity of recognition epitope within Ig domains 3-6 of CD22 with CART function. The optimal strategy for CD19/CD22 CART co-targeting is undetermined. Co-administration of CD19 and CD22 CARs is costly; single CARs targeting CD19 and CD22 are challenging to construct. The co-expression of two CARs has previously been achieved using bicistronic vectors. Here, we generated a dual CART product by co-transduction with 9A8-41BBζ and CAT-41BBζ (obe-cel), the previously described CD19 CAR. CAT/9A8 CART eliminated single- and double-positive target cells in vitro and eliminated CD19- tumors in vivo. CAT/9A8 CART is being tested in a phase I clinical study (NCT02443831).

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