LAIR-1 agonism as a therapy for acute myeloid leukemia
Rustin R. Lovewell, … , Dallas B. Flies, Tae Kon Kim
Rustin R. Lovewell, … , Dallas B. Flies, Tae Kon Kim
Published November 15, 2023
Citation Information: J Clin Invest. 2023;133(22):e169519. https://doi.org/10.1172/JCI169519.
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Research Article Oncology

LAIR-1 agonism as a therapy for acute myeloid leukemia

Abstract

Effective eradication of leukemic stem cells (LSCs) remains the greatest challenge in treating acute myeloid leukemia (AML). The immune receptor LAIR-1 has been shown to regulate LSC survival; however, the therapeutic potential of this pathway remains unexplored. We developed a therapeutic LAIR-1 agonist antibody, NC525, that induced cell death of LSCs, but not healthy hematopoietic stem cells in vitro, and killed LSCs and AML blasts in both cell- and patient-derived xenograft models. We showed that LAIR-1 agonism drives a unique apoptotic signaling program in leukemic cells that was enhanced in the presence of collagen. NC525 also significantly improved the activity of azacitidine and venetoclax to establish LAIR-1 targeting as a therapeutic strategy for AML that may synergize with standard-of-care therapies.

Authors

Rustin R. Lovewell, Junshik Hong, Subhadip Kundu, Carly M. Fielder, Qianni Hu, Kwang Woon Kim, Haley E. Ramsey, Agnieszka E. Gorska, Londa S. Fuller, Linjie Tian, Priyanka Kothari, Ana Paucarmayta, Emily F. Mason, Ingrid Meza, Yanira Manzanarez, Jason Bosiacki, Karla Maloveste, Ngan Mitchell, Emilia A. Barbu, Aaron Morawski, Sebastien Maloveste, Zac Cusumano, Shashank J. Patel, Michael R. Savona, Solomon Langermann, Han Myint, Dallas B. Flies, Tae Kon Kim

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Figure 2

LAIR-1 agonist mAb NC525 inhibits colony formation in LSCs but not healthy stem cells.

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LAIR-1 agonist mAb NC525 inhibits colony formation in LSCs but not healt...
(A) Representative images of ex vivo colony formation of LSCs from AML patient 19-0029 when plated at the indicated cell number and treated with 5 μg /mL of NC525 or isotype control. (B) Colony-forming units (CFUs) formed by ex vivo plating of (left to right) 50,000, 20,000, or 12,000 LSCs per well from the indicated AML patient during titrated treatment with anti–LAIR-1 agonist mAb NC525. n = 3 technical replicates per group. P values determined by 1-way ANOVA with multiple comparisons. (C) CFU formation from healthy donor BM or AML patient BM treated with 5 μg /mL NC525. Values normalized to isotype control. n = 14 AML biological replicates or 5 healthy biological replicates. P value determined by Student’s t test.