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Titlebook: Chronic Myeloid Neoplasias and Clonal Overlap Syndromes; Epidemiology, Pathop Richard Greil,Lisa Pleyer,Daniel Neureiter Book 2010 Springer

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,Introduction to “Classic” Chronic Myeloproliferative Disorders (CMPDs) — Molecular and Cellular BioPDs and non-clonal benign and malignant hematopoietic disorders on the other hand. (2) The initial lack of clonal molecular diagnostic markers in the pre-JAK2 era, as well as the previous lack of clear-cut diagnostic criteria and an adequate classification system, has often led to misclassification of chronic myeloproliferative disorders.
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Chronic myelogenous leukemia (CML),anagement of treatment failure, surveys results with approved second generation Abl kinase inhibitors after imatinib failure, and finally gives an outlook for promising treatment strategies examined in current and future clinical trials.
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ent.Well illustrated with clinical photos, clear graphics anIntroduction The understanding of the genetic, epigenetic, immuno- well as for practicing hematologists or oncologists. logical and biological causes of myeloproliferative dis- Each chapter follows a similar architecture and leads orders ha
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https://doi.org/10.1057/978-1-137-54642-5s one extreme end of this spectrum, characterized by maximal clonal/oligoclonal T-cell proliferation, as LGL-like immunodominant cytotoxic lymphocyte (CTL) clonotypes are found within the whole spectrum of this continuum of overlap syndromes [.].
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Primary Myelofibrosis (PMF) [Previously Chronic Idiopathic Myelofibrosid (CIMF), Myelofibrosis withse disease (PMF-BP, post-PV/ET MF in blast phase). However, the recent change in nomenclature from chronic idiopathic myelofibrosis to primary myelofibrosis [.] is of questionable benefit at best, as well as inexact and confusing, considering that biologically, there is no such thing as “primary” myelofibrosis [.].
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Chronic Myelomonocytic Leukemia (CMML),urse of their disease and ultimately progress to CMML [.]. Approximately one-fifth of patients with MDS present with a monocyte count of above 10% in the peripheral blood without fulfilling the FAB/WHO criteria for the diagnosis of CMML. A high incidence of disease progression to CMML has been reported for this subgroup [.] (see .).
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Clonal Bone Marrow Failure Overlap Syndromes,s one extreme end of this spectrum, characterized by maximal clonal/oligoclonal T-cell proliferation, as LGL-like immunodominant cytotoxic lymphocyte (CTL) clonotypes are found within the whole spectrum of this continuum of overlap syndromes [.].
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