Leuk Lymphoma. 2006 Nov;47(11):2289-300.

Ten years and counting: so what do we know about t(4;14)(p16;q32) multiple myeloma.

Keats JJ, Reiman T, Belch AR, Pilarski LM.

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Department of Oncology, University of Alberta & Cross Cancer Institute, Edmonton, Canada. keats.jonathan@mayo.edu

Abstract

Multiple myeloma is a genetically heterogenous disease with a wide variety of characterized genetic aberrations. Until recently, the impact of these aberrations on patient outcome was not known. However, in the last 5-10 years, several genetic markers have been linked to patient outcome. One of the strongest predictors of outcome identified to date is t(4;14)(p16;q32). Although this translocation is tightly linked to chromosome 13 deletions, another poor prognosis marker, it is becoming apparent that the translocation and not the deletion of 13 is the important factor. Unfortunately, despite the known association with outcome, an understanding of the mechanism(s) whereby the translocation contributes to developing and maintaining this aggressive form of myeloma remains elusive.

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Leuk Lymphoma. 2006 Nov ;47(11):2289-300.

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