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Query: UMLS:C0311368 (
Idiopathic eosinophilia
)
2
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Primary (nonreactive)
eosinophilia
is operationally classified as either a "clonal" or an "idiopathic" process. Clonal
eosinophilia
stipulates the presence of cytogenetic, molecular, or bone marrow histologic evidence of acute leukemia or a chronic myeloid disorder.
Idiopathic eosinophilia
is a diagnosis of exclusion that is made after ruling out both "secondary" (reactive) and clonal
eosinophilia
. Hypereosinophilic syndrome is a subclass of idiopathic
eosinophilia
that requires the documentation of both sustained
eosinophilia
(> or = 1500/microL for at least 6 months) and target-organ damage. A series of novel observations in the last 5 years have warranted a refined approach to the diagnosis as well as the treatment of clonal eosinophilic disorders, including systemic mastocytosis. At the center of these new developments are mutations involving the platelet-derived growth factor receptor genes (PDGFRA and PDGFRB), which have been pathogenetically linked to clonal
eosinophilia
, and their presence predicts complete as well as durable treatment responses to imatinib mesylate. The bone marrow histologic phenotype of these imatinib-sensitive eosinophilic disorders includes systemic mastocytosis, chronic eosinophilic leukemia, chronic myelomonocytic leukemia, and atypical chronic myeloproliferative disorder.
...
PMID:Imatinib therapy in clonal eosinophilic disorders, including systemic mastocytosis. 1523 93
Acquired blood
eosinophilia
is considered either a primary or a secondary phenomenon. Causes of secondary (ie, reactive)
eosinophilia
include tissue-invasive parasitosis, allergic or inflammatory conditions, and malignancies in which eosinophils are not considered part of the neoplastic process. Primary
eosinophilia
is classified operationally into 2 categories: clonal and idiopathic. Clonal
eosinophilia
stipulates the presence of either cytogenetic evidence or bone marrow histological evidence of an otherwise classified hematologic malignancy such as acute leukemia or a chronic myeloid disorder.
Idiopathic eosinophilia
is a diagnosis of exclusion (ie, not secondary or clonal). Hypereosinophilic syndrome is a subcategory of idiopathic
eosinophilia
; diagnosis requires documentation of both sustained
eosinophilia
(absolute eosinophil count > or = 1500 cells/microL for at least 6 months) and target organ damage (eg, involvement of the heart, lung, skin, or nerve tissue). Genetic mutations involving the platelet-derived growth factor receptor genes (PDGFR-alpha and PDGFR-beta) have been pathogenetically linked to clonal
eosinophilia
, and their presence predicts treatment response to imatinib. Accordingly, cytogenetic and/or molecular investigations for the presence of an imatinib-sensitive molecular target should accompany current evaluation for primary
eosinophilia
. In the absence of such a drug target, specific treatment is dictated by the underlying hematologic malignancy in cases of clonal
eosinophilia
; however, the initial treatment of choice for symptomatic patients with hypereosinophilic syndrome is prednisone and/or interferon alfa.
...
PMID:Blood eosinophilia: a new paradigm in disease classification, diagnosis, and treatment. 1566 33
