International working group-myeloproliferative neoplasms research and treatment (IWG-MRT) & European competence network on mastocytosis (ECNM) consensus …

J Gotlib, A Pardanani, C Akin, A Reiter… - Blood, The Journal …, 2013 - ashpublications.org
J Gotlib, A Pardanani, C Akin, A Reiter, T George, O Hermine, H Kluin-Nelemans…
Blood, The Journal of the American Society of Hematology, 2013ashpublications.org
Systemic mastocytosis (SM) is characterized by accumulation of neoplastic mast cells and is
classified into indolent and aggressive forms. The latter include aggressive SM (ASM), mast
cell leukemia (MCL), and SM associated with a myeloid neoplasm wherein 1 or both
disease compartments exhibit advanced features. These variants, henceforth collectively
referred to as advanced SM for the purposes of this report, are typically characterized by
organ damage and shortened survival duration. In contrast to indolent SM, in which …
Abstract
Systemic mastocytosis (SM) is characterized by accumulation of neoplastic mast cells and is classified into indolent and aggressive forms. The latter include aggressive SM (ASM), mast cell leukemia (MCL), and SM associated with a myeloid neoplasm wherein 1 or both disease compartments exhibit advanced features. These variants, henceforth collectively referred to as advanced SM for the purposes of this report, are typically characterized by organ damage and shortened survival duration. In contrast to indolent SM, in which symptoms are usually managed by noncytotoxic antimediator therapy, cytoreduction is usually necessary for disease control in advanced SM. Unfortunately, current drug treatment of these patients rarely results in complete clinical and histopathologic remissions or improved survival time. Previously defined response criteria were adapted to the heterogeneous presentations of advanced SM and the limited effects of available drugs. However, recent advances in understanding the molecular pathogenesis of SM and the corresponding prospect in targeted therapy make it a priority to modify these criteria. Our current study is the product of an international group of experts and summarizes the challenges in accomplishing this task and forwards a new proposal for response criteria, which builds on prior proposals and should facilitate response evaluation in clinical trials.
ashpublications.org
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