Dual-targeting CD33/CD123 NANOBODY T-cell engager with potent anti-AML activity and good safety profile.
Zhihong ZengAnnelies RoobrouckGeert DeschampsHelene BonnevauxStephane GuerifVeronique De BrabandereCéline AmaraEline DejonckheereAngela Virone-OddosMarielle ChironMarina Y KonoplevaMelissa DullaersPublished in: Blood advances (2024)
Novel therapies are needed for effective treatment of acute myeloid leukemia (AML). Relapse is common and salvage treatment with cytotoxic chemotherapy is rarely curative. CD123 and CD33, 2 clinically validated targets in AML, are jointly expressed on blasts and leukemic stem cells in >95% of patients with AML. However, their expression is heterogenous between subclones and between patients, which may affect the efficacy of single-targeting agents in certain patient populations. We present here a dual-targeting CD33/CD123 NANOBODY T-cell engager (CD33/CD123-TCE) that was designed to decrease the risk of relapse from possible single antigen-negative clones and to increase coverage within and across patients. CD33/CD123-TCE killed AML tumor cells expressing 1 or both antigens in vitro. Compared with single-targeting control compounds, CD33/CD123-TCE conferred equal or better ex vivo killing of AML blasts in most primary AML samples tested, suggesting a broader effectiveness across patients. In a disseminated cell-line-derived xenograft mouse model of AML, CD33/CD123-TCE cleared cancer cells in long bones and in soft tissues. As cytokine release syndrome is a well-documented adverse effect of TCE, the compound was tested in a cytokine release assay and shown to induce less cytokines compared to a CD123 single-targeting control. In an exploratory single-dose nonhuman primate study, CD33/CD123-TCE revealed a favorable PK profile. Depletion of CD123 and CD33 expressing cells was observed, but there were neither signs of cytokine release syndrome nor clinical signs of toxicity. Taken together, the CD33/CD123 dual-targeting NANOBODY TCE exhibits potent and safe anti-AML activity and promises a broad patient coverage.
Keyphrases
- acute myeloid leukemia
- allogeneic hematopoietic stem cell transplantation
- stem cells
- end stage renal disease
- ejection fraction
- newly diagnosed
- cancer therapy
- prognostic factors
- randomized controlled trial
- oxidative stress
- gene expression
- systematic review
- acute lymphoblastic leukemia
- poor prognosis
- cell proliferation
- patient reported outcomes
- signaling pathway
- dendritic cells
- long non coding rna
- patient reported
- high throughput
- smoking cessation
- binding protein