Molecular Cancer (Dec 2023)

Safety and efficacy of a novel anti-CD19 chimeric antigen receptor T cell product targeting a membrane-proximal domain of CD19 with fast on- and off-rates against non-Hodgkin lymphoma: a first-in-human study

  • Yunlin Zhang,
  • Ruchi P. Patel,
  • Ki Hyun Kim,
  • Hyungwoo Cho,
  • Jae-Cheol Jo,
  • Seong Hyun Jeong,
  • Sung Yong Oh,
  • Yoon Seok Choi,
  • Sung Hyun Kim,
  • Ji Hyun Lee,
  • Mathew Angelos,
  • Puneeth Guruprasad,
  • Ivan Cohen,
  • Ositadimma Ugwuanyi,
  • Yong Gu Lee,
  • Raymone Pajarillo,
  • Jong Hyun Cho,
  • Alberto Carturan,
  • Luca Paruzzo,
  • Guido Ghilardi,
  • Michael Wang,
  • Soohwan Kim,
  • Sung-Min Kim,
  • Hyun-Jong Lee,
  • Ji-Ho Park,
  • Leiguang Cui,
  • Tae Bum Lee,
  • In-Sik Hwang,
  • Young-Ha Lee,
  • Yong-Jun Lee,
  • Patrizia Porazzi,
  • Dongfang Liu,
  • Yoon Lee,
  • Jong-Hoon Kim,
  • Jong-Seo Lee,
  • Dok Hyun Yoon,
  • Junho Chung,
  • Marco Ruella

DOI
https://doi.org/10.1186/s12943-023-01886-9
Journal volume & issue
Vol. 22, no. 1
pp. 1 – 23

Abstract

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Abstract Background Commercial anti-CD19 chimeric antigen receptor T-cell therapies (CART19) are efficacious against advanced B-cell non-Hodgkin lymphoma (NHL); however, most patients ultimately relapse. Several mechanisms contribute to this failure, including CD19-negative escape and CAR T dysfunction. All four commercial CART19 products utilize the FMC63 single-chain variable fragment (scFv) specific to a CD19 membrane-distal epitope and characterized by slow association (on) and dissociation (off) rates. We hypothesized that a novel anti-CD19 scFv that engages an alternative CD19 membrane-proximal epitope independent of FMC63 and that is characterized by faster on- and off-rates could mitigate CART19 failure and improve clinical efficacy. Methods We developed an autologous CART19 product with 4-1BB co-stimulation using a novel humanized chicken antibody (h1218). This antibody is specific to a membrane-proximal CD19 epitope and harbors faster on/off rates compared to FMC63. We tested h1218-CART19 in vitro and in vivo using FMC63-CART19-resistant models. We conducted a first-in-human multi-center phase I clinical trial to test AT101 (clinical-grade h1218-CART19) in patients with relapsed or refractory (r/r) NHL. Results Preclinically, h1218- but not FMC63-CART19 were able to effectively eradicate lymphomas expressing CD19 point mutations (L174V and R163L) or co-expressing FMC63-CAR19 as found in patients relapsing after FMC63-CART19. Furthermore, h1218-CART19 exhibited enhanced killing of B-cell malignancies in vitro and in vivo compared with FMC63-CART19. Mechanistically, we found that h1218-CART19 had reduced activation-induced cell death (AICD) and enhanced expansion compared to FMC63-CART19 owing to faster on- and off-rates. Based on these preclinical results, we performed a phase I dose-escalation trial, testing three dose levels (DL) of AT101 (the GMP version of h1218) using a 3 + 3 design. In 12 treated patients (7 DLBCL, 3 FL, 1 MCL, and 1 MZL), AT101 showed a promising safety profile with 8.3% grade 3 CRS (n = 1) and 8.3% grade 4 ICANS (n = 1). In the whole cohort, the overall response rate was 91.7%, with a complete response rate of 75.0%, which improved to 100% in DL-2 and -3. AT101 expansion correlates with CR and B-cell aplasia. Conclusions We developed a novel, safe, and potent CART19 product that recognizes a membrane-proximal domain of CD19 with fast on- and off-rates and showed significant efficacy and promising safety in patients with relapsed B-cell NHL. Trial registration NCT05338931; Date: 2022–04-01.

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