CLL B Cells Develop Resistance to Ibrutinib By Reinvigorating the IL-4R-IL-4 Axis Blocked By Bruton's Tyrosine Kinase Inhibitors Including Acalabrutinib and Zanubrutinib

Shih-Shih Chen; Constantine S Tam; Alan G Ramsay; Priyadarshini Ravichandran; Natalia C Couto-Francisco; Michael Ibrahim; Gerardo Ferrer; Jonathan E Kolitz; Steven L Allen; He Zhou; Jacqueline C Barrientos; Kanti R Rai; Nicholas Chiorazzi

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CLL B Cells Develop Resistance to Ibrutinib By Reinvigorating the IL-4R-IL-4 Axis Blocked By Bruton's Tyrosine Kinase Inhibitors Including Acalabrutinib and Zanubrutinib

Shih-Shih Chen, Constantine S Tam, Alan G Ramsay, Priyadarshini Ravichandran, Natalia C Couto-Francisco, Michael Ibrahim, Gerardo Ferrer, Jonathan E Kolitz, Steven L Allen, He Zhou, Jacqueline C Barrientos, Kanti R Rai, Nicholas Chiorazzi

BLOOD | AMER SOC HEMATOLOGY | Published : 2019

DOI: 10.1182/blood-2019-127255

Abstract

Bruton's tyrosine kinases inhibitors (BTKis) represent major advances in CLL therapy. However resistance to this form of therapy is emerging, and such patients often progress more rapidly. Hence there is an important need for therapies that address resistance. Microenvironmental input like IL-4 is critical for CLL disease progression. Compared with normal B cells, CLL cells exhibit significantly higher levels of surface membrane (sm) IL-4 receptor (IL4-R) and contain increased amounts of pSTAT6, a downstream mediator of IL-4R signaling. IL-4 stimulation of CLL B cells suppresses smCXCR4 and increases smIgM, thus promotes CLL cell retention and expansion. In this study, we aime..

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CLL B Cells Develop Resistance to Ibrutinib By Reinvigorating the IL-4R-IL-4 Axis Blocked By Bruton's Tyrosine Kinase Inhibitors Including Acalabrutinib and Zanubrutinib

Abstract

University of Melbourne Researchers

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