Three BTK-Specific Inhibitors, in Contrast to Ibrutinib, Do Not Antagonize Rituximab-Dependent NK-Cell Mediated Cytotoxicity

Rajasekaran, Narendiran; Sadaram, Mohith; Hebb, Jonathan; Sagiv-Barfi, Idit; Ambulkar, Siddhant; Rajapaksa, Amanda; Chang, Serena; Chester, Cariad; Waller, Erin; Wang, Lai; Lannutti, Brian J.; Johnson, David R.; Levy, Ronald; Kohrt, Holbrook E.

doi:10.1182/blood.v124.21.3118.3118

Cited by 20 publications

(18 citation statements)

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“…Ibrutinib resulted in decreased phosphorylation at tyrosine 180 (Y180) of ITK, confirming ITK as a known target of ibrutinib (Fig C) (Dubovsky et al , ). These data are consistent with previous reports indicating that ibrutinib antagonized rituximab‐dependent NK cell‐mediated cytotoxicity (Kohrt et al , ; Rajasekaran et al , ; Roit et al , ), however one group has demonstrated that ibrutinib increased NK cell‐mediated activity of mouse NK cells (Kuo et al , ).…”

Section: Resultssupporting

confidence: 92%

Activity of lenalidomide in mantle cell lymphoma can be explained by NK cell‐mediated cytotoxicity

Hagner¹,

Chiu²,

Ortiz³

et al. 2017

Br J Haematol

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Lenalidomide is an immunomodulatory agent that has demonstrated clinical benefit for patients with relapsed or refractory mantle cell lymphoma (MCL); however, despite this observed clinical activity, the mechanism of action (MOA) of lenalidomide has not been characterized in this setting. We investigated the MOA of lenalidomide in clinical samples from patients enrolled in the CC-5013-MCL-002 trial (NCT00875667) comparing single-agent lenalidomide versus investigator's choice single-agent therapy and validated our findings in pre-clinical models of MCL. Our results revealed a significant increase in natural killer (NK) cells relative to total lymphocytes in lenalidomide responders compared to non-responders that was associated with a trend towards prolonged progression-free survival and overall survival. Clinical response to lenalidomide was independent of baseline tumour microenvironment expression of its molecular target, cereblon, as well as genetic mutations reported to impact clinical response to the Bruton tyrosine kinase inhibitor ibrutinib. Preclinical experiments revealed lenalidomide enhanced NK cell-mediated cytotoxicity against MCL cells via increased lytic immunological synapse formation and secretion of granzyme B. In contrast, lenalidomide exhibited minimal direct cytotoxic effects against MCL cells. Taken together, these data provide the first insight into the clinical activity of lenalidomide against MCL, revealing a predominately immune-mediated MOA.

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Section: Resultssupporting

confidence: 92%

Activity of lenalidomide in mantle cell lymphoma can be explained by NK cell‐mediated cytotoxicity

Hagner¹,

Chiu²,

Ortiz³

et al. 2017

Br J Haematol

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“…ITK is also expressed in natural killer (NK) cells (Khurana et al, 2007), and inhibition thereof has been reported to decrease the antibody-dependent cellular cytotoxicity function of NK cells (Kohrt et al, 2014). It was reported that ibrutinib inhibited both rituximab-and trastuzumab-induced NK cell cytokine secretion and lysis in vitro in a dose-dependent manner (0.1 and 1 mM), whereas acalabrutinib did not show any effects at 1 mM (Rajasekaran et al, 2014). This indicates that acalabrutinib is associated with a reduced risk of affecting antibody-dependent cellular cytotoxicity-mediated therapies.…”

Section: Discussionmentioning

confidence: 99%

Acalabrutinib (ACP-196): A Covalent Bruton Tyrosine Kinase Inhibitor with a Differentiated Selectivity and In Vivo Potency Profile

Barf¹,

Covey²,

Izumi³

et al. 2017

J Pharmacol Exp Ther

323

343

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Several small-molecule Bruton tyrosine kinase (BTK) inhibitors are in development for B cell malignancies and autoimmune disorders, each characterized by distinct potency and selectivity patterns. Herein we describe the pharmacologic characterization of BTK inhibitor acalabrutinib [compound 1, ACP-196 (4-[8-amino-3-[(2)-1-but-2-ynoylpyrrolidin-2-yl]imidazo[1,5-]pyrazin-1-yl]--(2-pyridyl)benzamide)]. Acalabrutinib possesses a reactive butynamide group that binds covalently to Cys481 in BTK. Relative to the other BTK inhibitors described here, the reduced intrinsic reactivity of acalabrutinib helps to limit inhibition of off-target kinases having cysteine-mediated covalent binding potential. Acalabrutinib demonstrated higher biochemical and cellular selectivity than ibrutinib and spebrutinib (compounds 2 and 3, respectively). Importantly, off-target kinases, such as epidermal growth factor receptor (EGFR) and interleukin 2-inducible T cell kinase (ITK), were not inhibited. Determination of the inhibitory potential of anti-immunoglobulin M-induced CD69 expression in human peripheral blood mononuclear cells and whole blood demonstrated that acalabrutinib is a potent functional BTK inhibitor. In vivo evaluation in mice revealed that acalabrutinib is more potent than ibrutinib and spebrutinib. Preclinical and clinical studies showed that the level and duration of BTK occupancy correlates with in vivo efficacy. Evaluation of the pharmacokinetic properties of acalabrutinib in healthy adult volunteers demonstrated rapid absorption and fast elimination. In these healthy individuals, a single oral dose of 100 mg showed approximately 99% median target coverage at 3 and 12 hours and around 90% at 24 hours in peripheral B cells. In conclusion, acalabrutinib is a BTK inhibitor with key pharmacologic differentiators versus ibrutinib and spebrutinib and is currently being evaluated in clinical trials.

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“…The emergence of ibrutinib-resistant disease and subsequent studies have uncovered potential contributors to ibrutinib resistance in MCL, including acquired BTK mutations that interfere with ibrutinib binding or aberrant upregulation of PI3K (12,13). Assessment of novel BTK inhibitors therefore provides a valuable platform to study BTK as a rational therapeutic target and to probe the role of BTK in ibrutinib resistance.…”

Section: Introductionmentioning

confidence: 99%

Pleiotropic Action of Novel Bruton's Tyrosine Kinase Inhibitor BGB-3111 in Mantle Cell Lymphoma

Jiang

Liu

et al. 2019

Molecular Cancer Therapeutics

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Bruton's tyrosine kinase (BTK) is a key mediator of BCRdependent cell growth signaling and a clinically effective therapeutic target in mantle cell lymphoma (MCL). The molecular impact of BTK inhibition remains unclear particularly in hematopoietic malignancies. We analyzed the molecular mechanisms of BTK inhibition with the novel inhibitor BGB-3111 (zanubrutinib) in MCL models. The efficacy of BGB-3111 was investigated using growth proliferation/cell viability and apoptosis assays in MCL cell lines and patientderived xenograft (PDX) MCL cells. The activity and mechanisms of BGB-3111 were further confirmed using a cell line xenograft model, an MCL PDX mouse model, and a human phosphokinase profiler array and reverse phase protein array. Finally, the mechanisms related to resistance to BTK inhibition were analyzed by creating cell lines with low levels of BTK using CRISPR/Cas 9 genome editing. We found that inhibition of BTK leads to suppression of tumor growth, which was mediated via potent suppression of AKT/mTOR, apoptosis, and metabolic stress. Moreover, targeted disruption of the BTK gene in MCL cells resulted in resistance to BTK inhibition and the emergence of novel survival mechanisms. Our studies suggest a general efficacy of BTK inhibition in MCL and potential drug resistance mechanism via alternative signaling pathways.

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Three BTK-Specific Inhibitors, in Contrast to Ibrutinib, Do Not Antagonize Rituximab-Dependent NK-Cell Mediated Cytotoxicity

Cited by 20 publications

References 0 publications

Activity of lenalidomide in mantle cell lymphoma can be explained by NK cell‐mediated cytotoxicity

Activity of lenalidomide in mantle cell lymphoma can be explained by NK cell‐mediated cytotoxicity

Acalabrutinib (ACP-196): A Covalent Bruton Tyrosine Kinase Inhibitor with a Differentiated Selectivity and In Vivo Potency Profile

Pleiotropic Action of Novel Bruton's Tyrosine Kinase Inhibitor BGB-3111 in Mantle Cell Lymphoma

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