Antineoplastic efficacy profiles of avapritinib and nintedanib in KIT D816V+ systemic mastocytosis: a preclinical study

Lina Degenfeld-Schonburg; Susanne Gamperl; Gabriele Stefanzl; Anna-Katharina Schruef; Irina Sadovnik; Karin Bauer; Dubravka Smiljkovic; Gregor Eisenwort; Barbara Peter; Georg Greiner; Emir Hadzijusufovic; Juliana Schwaab; Wolfgang R Sperr; Gregor Hoermann; Sonja Kopanja; Zsolt Szépfalusi; Konrad Hoetzenecker; Peter Jaksch; Andreas Reiter; Michel Arock; Peter Valent

Antineoplastic efficacy profiles of avapritinib and nintedanib in KIT D816V⁺ systemic mastocytosis: a preclinical study

Am J Cancer Res. 2023 Feb 15;13(2):355-378. eCollection 2023.

Authors

Lina Degenfeld-Schonburg¹, Susanne Gamperl¹, Gabriele Stefanzl^{1

2}, Anna-Katharina Schruef¹, Irina Sadovnik², Karin Bauer², Dubravka Smiljkovic², Gregor Eisenwort^{1

2}, Barbara Peter^{1

2}, Georg Greiner^{2

3}, Emir Hadzijusufovic^{1

2

4}, Juliana Schwaab⁵, Wolfgang R Sperr^{1

2}, Gregor Hoermann^{2

6}, Sonja Kopanja⁷, Zsolt Szépfalusi⁷, Konrad Hoetzenecker⁸, Peter Jaksch⁸, Andreas Reiter⁵, Michel Arock⁹, Peter Valent^{1

2}

Affiliations

¹ Department of Internal Medicine I, Division of Hematology and Hemostaseology, Medical University of Vienna Austria.
² Ludwig Boltzmann Institute for Hematology and Oncology, Medical University of Vienna Austria.
³ Ihr Labor, Medical Diagnostic Laboratories Vienna, Austria.
⁴ Department/Hospital for Companion Animals and Horses, University Hospital for Small Animals, Internal Medicine Small Animals, University of Veterinary Medicine Vienna Austria.
⁵ Department of Hematology and Oncology, University Medical Centre Mannheim and Medical Faculty Mannheim, Heidelberg University Germany.
⁶ MLL Munich Leukemia Laboratory Munich, Germany.
⁷ Department of Pediatrics and Adolescent Medicine, Division of Pediatric Pulmonology, Allergy and Endocrinology, Medical University of Vienna Austria.
⁸ Department of Surgery, Division of Thoracic Surgery, Medical University of Vienna Austria.
⁹ Department of Hematological Biology, Pitié-Salpêtrière Hospital, Pierre et Marie Curie University (UPMC) Paris, France.

PMID: 36895976
PMCID: PMC9989615

Abstract

Systemic mastocytosis (SM) is a hematopoietic neoplasm with a complex pathology and a variable clinical course. Clinical symptoms result from organ infiltration by mast cells (MC) and the effects of pro-inflammatory mediators released during MC activation. In SM, growth and survival of MC are triggered by various oncogenic mutant-forms of the tyrosine kinase KIT. The most prevalent variant, D816V, confers resistance against various KIT-targeting drugs, including imatinib. We examined the effects of two novel promising KIT D816V-targeting drugs, avapritinib and nintedanib, on growth, survival, and activation of neoplastic MC and compared their activity profiles with that of midostaurin. Avapritinib was found to suppress growth of HMC-1.1 cells (KIT V560G) and HMC-1.2 cells (KIT V560G + KIT D816V) with comparable IC₅₀ values (0.1-0.25 µM). In addition, avapritinib was found to inhibit the proliferation of ROSA^{KIT WT} cells, (IC₅₀: 0.1-0.25 µM), ROSA^{KIT D816V} cells (IC₅₀: 1-5 µM), and ROSA^{KIT K509I} cells (IC₅₀: 0.1-0.25 µM). Nintedanib exerted even stronger growth-inhibitory effects in these cells (IC₅₀ in HMC-1.1: 0.001-0.01 µM; HMC-1.2: 0.25-0.5 µM; ROSA^{KIT WT}: 0.01-0.1 µM; ROSA^{KIT D816V}: 0.5-1 µM; ROSA^{KIT K509I}: 0.01-0.1 µM). Avapritinib and nintedanib also suppressed the growth of primary neoplastic cells in most patients with SM examined (avapritinib IC₅₀: 0.5-5 µM; nintedanib IC₅₀: 0.1-5 µM). Growth-inhibitory effects of avapritinib and nintedanib were accompanied by signs of apoptosis and decreased surface expression of the transferrin receptor CD71 in neoplastic MC. Finally, we were able to show that avapritinib counteracts IgE-dependent histamine secretion in basophils and MC in patients with SM. These effects of avapritinib may explain the rapid clinical improvement seen during treatment with this KIT inhibitor in patients with SM. In conclusion, avapritinib and nintedanib are new potent inhibitors of growth and survival of neoplastic MC expressing various KIT mutant forms, including D816V, V560G, and K509I, which favors the clinical development and application of these new drugs in advanced SM. Avapritinib is of particular interest as it also blocks mediator secretion in neoplastic MC.

Keywords: KIT; Mast cells; mastocytosis; targeted therapy; tyrosine kinase inhibitors.