Editorial


Distinct benefit from crizotinib in lung cancer patients carrying distinct ALK translocations: is fluorescent hybridization in situ testing still sufficient to guide clinical decisions?

Natalia V. Mitiushkina, Evgeny N. Imyanitov

Abstract

ALK rearrangements in lung cancer (LC) were discovered in the year 2007 upon the systematic search for novel LC-associated oncogenes (1,2). Fortunately, an experimental MET inhibitor, PF-2341066 (crizotinib), was by then known to have a concurrent ALK-inhibiting activity and its clinical profile was already under phase I evaluation (3-6). It was quickly revealed that the status of ALK, but not MET, is a primary determinant of tumor sensitivity to crizotinib (5), and a number of subsequent studies heralded a real breakthrough in the treatment of ALK-rearranged cancers (6-9).

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