Abstract
<div>Abstract<p><b>Purpose:</b> Classical Hodgkin lymphoma (cHL) and primary mediastinal large B-cell lymphoma (MLBCL) share similar histologic, clinical, and genetic features. In recent studies, we found that disease-specific chromosome 9p24.1/<i>JAK2</i> amplification increased JAK2 expression and activity in both cHL and MLBCL. This prompted us to assess the activity of a clinical grade JAK2 selective inhibitor, fedratinib (SAR302503/TG101348), in <i>in vitro</i> and <i>in vivo</i> model systems of cHL and MLBCL with defined <i>JAK2</i> copy numbers.</p><p><b>Experimental Design:</b> We used functional and immunohistochemical analyses to investigate the preclinical activity of fedratinib and associated biomarkers in cell lines and murine xenograft models of cHL and MLBCL with known 9p24.1/<i>JAK2</i> copy number.</p><p><b>Results:</b> Chemical JAK2 inhibition decreased the cellular proliferation of cHL and MLBCL cell lines and induced their apoptosis. There was an inverse correlation between 9p24.1/<i>JAK2</i> copy number and the EC<sub>50</sub> of fedratinib. Chemical JAK2 inhibition decreased phosphorylation of JAK2, STAT1, STAT3, and STAT6 and reduced the expression of additional downstream targets, including PD-L1, in a copy number–dependent manner. In murine xenograft models of cHL and MLBCL with 9p24.1/<i>JAK2</i> amplification, chemical JAK2 inhibition significantly decreased JAK2/STAT signaling and tumor growth and prolonged survival. In <i>in vitro</i> and <i>in vivo</i> studies, pSTAT3 was an excellent biomarker of baseline JAK2 activity and the efficacy of chemical JAK2 inhibition.</p><p><b>Conclusions:</b> In <i>in vitro</i> and <i>in vivo</i> analyses, cHL and MLBCL with 9p24.1/<i>JAK2</i> copy gain are sensitive to chemical JAK2 inhibition suggesting that clinical evaluation of JAK2 blockade is warranted. <i>Clin Cancer Res; 20(10); 2674–83. ©2014 AACR</i>.</p></div>
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