Maciocia, Nicola; Hoekx, Malika; Acuna, Ciaran; Wade, Brandon; Burley, Amy; Ramanayake, Saumya; Nannini, Francesco; ... Maciocia, Paul; + view all Maciocia, Nicola; Hoekx, Malika; Acuna, Ciaran; Wade, Brandon; Burley, Amy; Ramanayake, Saumya; Nannini, Francesco; Wawrzyniecka, Patrycja A; Karpanasamy, Thaneswari; Schuldt, Maria; Ng, Stephanie; Ferrari, Mathieu; Marafioti, Teresa; Gritti, Giuseppe; Onuoha, Shimobi; O’Connor, David; Lee, Lydia; Mansour, Marc; Khwaja, Asim; Pule, Martin; Maciocia, Paul; - view fewer (2025) Preclinical development of anti-CD21 chimeric antigen receptor T cells to treat T cell acute lymphoblastic leukemia. Science Translational Medicine , 17 (794) , Article eadr1476. 10.1126/scitranslmed.adr1476.

Preview	Text (Article) Maciocia_250318adr1476_ArticleContent_accepted_NM.pdf - Accepted Version Download (433kB) | Preview
Preview	Text (Supplementary Information) Maciocia_250303SM_NMrevised.pdf - Accepted Version Download (6MB) | Preview
Preview	Image (Figures) Maciocia_Figure1.pdf Download (268kB) | Preview
Preview	Image (Figures) Maciocia_Figure2.pdf Download (309kB) | Preview
Preview	Image (Figures) Maciocia_Figure3.pdf Download (250kB) | Preview
Preview	Image (Figures) Maciocia_Figure4.pdf Download (274kB) | Preview
Preview	Image (Figures) Maciocia_Figure5.pdf Download (157kB) | Preview
Preview	Image (Figures) Maciocia_Figure6.pdf Download (360kB) | Preview

Abstract

Patients with relapsed/refractory (r/r) T cell acute lymphoblastic leukemia (T-ALL) have a dismal prognosis, highlighting the urgent need for effective therapies. Chimeric antigen receptor (CAR)–T cell approaches targeting pan–T cell antigens may be limited by T cell aplasia and fratricide, necessitating “rescue” allogeneic hematopoietic stem cell transplantation. In this study, we identify CD21, a pan–B cell marker, as a promising target for T-ALL immunotherapy. CD21 is expressed in 50% of T-ALL cases at diagnosis but in fewer than 10% of mature T cells. We observed that CAR-T cells targeting membrane-distal CD21 epitopes were ineffective, likely because of the bulky, glycosylated nature of the antigen. However, when we engineered CAR-T cells to target membrane-proximal CD21 epitopes using an antigen-binding fragment (Fab)–CAR design, we demonstrated robust activity against T-ALL cell lines, primary tumors, and patient-derived xenografts in both in vitro and in vivo models. The enhanced efficacy of this Fab-CAR design was driven by its high stability and reduced surface expression, addressing limitations of traditional CAR constructs. In addition, pharmacological inhibition of the phosphatidylinositol 3-kinase axis up-regulated CD21 expression in T-ALL, further enhancing the potency of anti-CD21 CAR-T cells in vitro and in a patient-derived xenograft in vivo model. This study establishes CD21 as a viable CAR-T target and highlights advances in CAR design for bulky antigens, as well as the potential for pharmacological strategies to augment target expression. Anti-CD21 CAR-T cells represent a promising therapeutic option for improving outcomes for patients with T-ALL.

Download activity - last month

Export as JSONCSVXML

Download activity - last 12 months

Export as CSVXMLJSON

Downloads by country - last 12 months

Export as XMLCSVJSON

Archive Staff Only

View Item