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Contrary to Total Therapy (TT) 2 for multiple myeloma patients, FGFR3- translocation bore no adverse effects on outcome in TT3 with added bortezomib. Del TP53, another poor-risk feature in TT2 and present in 10% of 441 patients treated, was examined for its prognostic consequences in TT3. Not affecting rate or duration of complete response, TP53 haplo-insufficiency also did not compromise, in the 83% with genomically defined low-risk myeloma, survival or event-free survival. FGFR3+ and FGFR3- molecular subgroups fared worse in the presence of del TP53 when applying TT2 but not TT3. Thus, the prognostic implications of del TP53 were protocol-, genome-defined risk- and molecular subgroup-dependent.
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John D. Shaughnessy
Winthrop Rockefeller Foundation
Yiming Zhou
Kunming University of Science and Technology
Jeff Haessler
University of Copenhagen
British Journal of Haematology
University of Arkansas for Medical Sciences
Cancer Research And Biostatistics
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Shaughnessy et al. (Fri,) studied this question.
synapsesocial.com/papers/6a19d5f9a2165c1276df1905 — DOI: https://doi.org/10.1111/j.1365-2141.2009.07864.x
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