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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Basophilic blast phase of chronic myelogenous Leukemia
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Basophilic blast phase of chronic myelogenous Leukemia

机译:慢性髓性白血病的嗜碱性强碱

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A 29-year-old man with an 8-year history of chronic myeloid leukemia (CML) was referred to our institution for marked leukocytosis and 3% blasts (white blood cells [WBC], 338.7 X 109/L; neutrophils, 159.2 X 109/L; myelocytes, 88.1 X 109/L; basophils, 47.4 X 109/L) (panel A). Cytogenetic studies showed t(9;22)(q34;q11.2), and the diagnosis of CML, chronic phase, was confirmed. The treatment history included imatinib (Gleevec) (not well tolerated), followed by dasatinib and hydroxyurea (Hydrea). Treatment with dasatinib failed due to poor compliance. Molecular studies identified a T315I mutation, and the patient was started on ponatinib. Ten months later, he presented with fevers.and leukocytosis (WBC, 109.7 X 109/L), with >20% blasts. The blasts were moderate in size and had fine chromatin and a moderate amount of granular cytoplasm (panel B). In addition, both the peripheral blood and bone marrow showed absolute basophilia (98.7 X 109/L), including numerous basophilic precursors such as myelocytes and metamyelocytes. These cells comprised ~90% of the white cells by flow cytometry and expressed CD7, CD 13, CD25, CD33, CD38, CD117, CD123, and CD 203c markers, confirming their basophilic differentiation. Cytogenetic studies revealed additional abnormalities [50,XY,+8, + 8, t(9;22), +17, and +19]. Taken together, these findings support the diagnosis of basophilic blast phase of CML, a very rare manifestation of myeloid blast crisis.
机译:一名29岁的男子患有8年的慢性骨髓白血病历史(CML)被提交给我们标记白细胞增多症和3%爆炸的机构(白细胞[WBC],338.7 x 109 / L;中性粒细胞,159.2 x 109 / L; myelocytes,88.1 x 109 / L;嗜碱性粒细胞,47.4 x 109 / L)(图A)。细胞遗传学研究显示T(9; 22)(Q34; Q11.2),确认CML慢性阶段的诊断。治疗史包括伊马替尼(Gleevec)(不良好耐受),其次是Dasatinib和羟基脲(Hydrea)。由于遵守性差,达斯卡内韦治疗失败。分子研究确定了T315i突变,患者在Ponatinib上开始。十个月后,他介绍了Fevers.and白细胞增多症(WBC,109.7 x 109 / L),爆炸> 20%。爆炸的大小适中,具有细染色质和中等量的粒状细胞质(面板B)。此外,外周血和骨髓都显示出绝对的嗜碱性嗜碱性(98.7×10 9升),包括许多嗜碱性前体如骨髓细胞和元素细胞。这些细胞通过流式细胞术包含〜90%的白色细胞,表达CD7,CD13,CD25,CD33,CD38,CD117,CD123和CD 203C标记,证实了它们的嗜碱性分化。细胞遗传学研究揭示了另外的异常[50,XY,+ 8,+ 8,T(9; 22),+17和+19]。总之,这些发现支持CML的嗜碱性强度癌症诊断,这是一种非常罕见的骨髓爆炸危机的表现。

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