Activity of the novel BCR kinase inhibitor IQS019 in preclinical models of B-cell non-Hodgkin lymphoma
Autor/a
Borrell Bilbao, José Ignacio
Teixidó i Closa, Jordi
Puig de la Bellacasa Cazorla, Raimon
Roué, Gaël
Balsas, P.
Esteve-Arenys, A.
Roldán, J.
Jiménez, L.
Rodríguez, V.
Valero, J. G.
Chamorro-Jorganes, A.
Matas-Céspedes, A.
Moros, A.
Martínez, A.
Campo, E.
Sáez-Borderías, A.
Pérez-Galán, P.
Colomer, D.
Otros/as autores/as
Universitat Ramon Llull. IQS
Fecha de publicación
2017-03Resumen
Background
Pharmacological inhibition of B cell receptor (BCR) signaling has recently emerged as an effective approach in a wide range of B lymphoid neoplasms. However, despite promising clinical activity of the first Bruton’s kinase (Btk) and spleen tyrosine kinase (Syk) inhibitors, a small fraction of patients tend to develop progressive disease after initial response to these agents.
Methods
We evaluated the antitumor activity of IQS019, a new BCR kinase inhibitor with increased affinity for Btk, Syk, and Lck/Yes novel tyrosine kinase (Lyn), in a set of 34 B lymphoid cell lines and primary cultures, including samples with acquired resistance to the first-in-class Btk inhibitor ibrutinib. Safety and efficacy of the compound were then evaluated in two xenograft mouse models of B cell lymphoma.
Results
IQS019 simultaneously engaged a rapid and dose-dependent de-phosphorylation of both constitutive and IgM-activated Syk, Lyn, and Btk, leading to impaired cell proliferation, reduced CXCL12-dependent cell migration, and induction of caspase-dependent apoptosis. Accordingly, B cell lymphoma-bearing mice receiving IQS019 presented a reduced tumor outgrowth characterized by a decreased mitotic index and a lower infiltration of malignant cells in the spleen, in tight correlation with downregulation of phospho-Syk, phospho-Lyn, and phospho-Btk. More interestingly, IQS019 showed improved efficacy in vitro and in vivo when compared to the first-in-class Btk inhibitor ibrutinib, and was active in cells with acquired resistance to this latest.
Conclusions
These results define IQS019 as a potential drug candidate for a variety of B lymphoid neoplasms, including cases with acquired resistance to current BCR-targeting therapies.
Tipo de documento
Artículo
Versión publicada
Lengua
English
Materias (CDU)
616 - Patología. Medicina clínica. Oncología
Palabras clave
Cèl·lules--Migració
Cèl·lules B
Limfomes
B-NHL
Btk
Lyn
Syk
Cell migration
Mouse model
Páginas
14 p.
Publicado por
BioMed Central
Publicado en
Journal of Hematology & Oncology. Vol.10, n.80 (2017)
Número del acuerdo de la subvención
info:eu-repo/grantAgreement/MINECO/PN I+D/FIS PI12/01847
info:eu-repo/grantAgreement/MINECO/PN I+D/FIS PI15/00102
info:eu-repo/grantAgreement/MINECO/PN I+D/FIS PI0110094
info:eu-repo/grantAgreement/MINECO I FEDER/PN I+D/SAF12/31242
info:eu-repo/grantAgreement/MINECO I FEDER/PN I+D/SAF11/29326
info:eu-repo/grantAgreement/MINECO I FEDER/PN I+D/SAF2010-C21617-C02
info:eu-repo/grantAgreement/MINECO i FEDER/Redes Temáticas de Investigación Cooperativa/RD12-0036-0004
info:eu-repo/grantAgreement/MINECO i FEDER/Redes Temáticas de Investigación Cooperativa/RD12-0036-0039
info:eu-repo/grantAgreement/SUR del DEC/SGR/2014-SGR-346
info:eu-repo/grantAgreement/SUR del DEC/SGR/2014-SGR-795
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