The roles of aberrant expression of constitutively active ALK chimeric proteins in the pathogenesis of anaplastic large-cell lymphoma (ALCL) have been well defined; nevertheless, the notion that ALK is a molecular target for the therapeutic modulation of ALK ؉ ALCL has not been validated thus far. Select fused pyrrolocarbazole (FP)-derived small molecules with ALK inhibitory activity were used as pharmacologic tools to evaluate whether functional ALK is essential for the prolifera-
IntroductionChromosomal translocations occur frequently in a select group of human cancers, including most lymphomas, leukemias, and sarcomas. Individual translocations have shown a high degree of specificity for particular cancer types and the presence of a particular translocation often correlates well with clinical behavior and outcome for specific types of cancer. 1 Consequently, therapies directed at molecular targets dysregulated by tumor-specific genetic aberrations will potentially provide more effective and less toxic therapies than conventional chemotherapy. 1,2 Anaplastic large-cell lymphomas (ALCLs) comprise a group of non-Hodgkin lymphomas (NHLs) that are usually of T-cell origin and often present with extranodal disease, especially the skin, and are characterized by the expression of the CD30/Ki-1 antigen. Roughly 2500 to 3000 new cases of ALCLs are diagnosed in the United States each year and 50% to 60% of these ALCLs are associated with a specific t(2;5) (p23;q35) chromosome translocation. 4,5 The genes altered in the t(2;5) translocation contain the N-terminal portion of nucleophosmin (NPM) gene, a nuclear phosphoprotein, fused to the catalytic domain of anaplastic lymphoma kinase (ALK) gene. ALK is a cell-membrane-spanning receptor tyrosine kinase and a member of the insulin receptor superfamily. Although the precise physiologic function and regulation of ALK have not been well defined, the NPM-ALK fusion gene encodes for an 80-kDa NPM-ALK chimeric oncoprotein with constitutively active ALK tyrosine kinase activity, which plays a key role in lymphomagenesis by the aberrant phosphorylation of multiple intracellular substrates downstream of NPM-ALK. 4,5 Subsequently, other fusion partners of ALK were also reported in ALCL, and dysregulated expression and constitutive activation of the ALK protein was demonstrated in approximately 60% to 70% of ALCLs, termed ALK ϩ lymphomas. 4,[6][7][8] Preclinical experimental data have demonstrated that the aberrant expression of constitutively active ALK is directly implicated in the pathogenesis of ALCL and that ALK down-regulation or inhibition of ALK-mediated pathways can markedly impair the growth of ALK ϩ lymphoma cells. 9-15 Currently there is no optimal therapeutic regimen for ALK ϩ ALCL. Doxorubicin-based combination chemotherapy has limited effectiveness, resulting in a substantial number of patients with ALK ϩ ALCL with a poor outcome, either failing to enter remission or relapsing within a few months from the start of treatment. 3 Thus, optimal and more effective therapeu...
There are numerous published studies establishing a link between reactive metabolite formation and toxicity of various drugs. Although the correlation between idiosyncratic reactions and reactive metabolite formation is not 1:1, the association between the two is such that many pharmaceutical companies now monitor for reactive metabolites as a standard part of drug candidate testing and selection. The most common method involves in vitro human microsomal incubations in the presence of a thiol trapping agent, such as glutathione (GSH), followed by LC/MS analysis. In this study, we describe several 2,7-disubstituted-pyrrolotriazine analogues that are extremely potent reactive metabolite precursors. Utilizing a UPLC/UV/MS method, unprecedented levels of GSH adducts were measured that are 5-10 times higher than previously reported for high reactive metabolite-forming compounds such as clozapine and troglitazone.
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