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新诊断慢性髓性白血病患者血小板功能相关变量的前瞻性评估。

Prospective evaluation of variables affecting platelet function in patients with newly diagnosed chronic myeloid leukemia.

机构信息

Department of Haematology, Vardhman Mahavir Medical College and Safdarjung Hospital, New Delhi, India.

出版信息

Blood Coagul Fibrinolysis. 2020 Dec;31(8):562-568. doi: 10.1097/MBC.0000000000000965.

Abstract

: Platelet function in chronic myeloid leukemia (CML) could be affected by either hyperleucocytosis, clonal megakaryopoiesis, or tyrosine kinase inhibitors. However, these variables have never been prospectively evaluated. We conducted a prospective study over a period of 1.5 years in a tertiary care center of north India. Patients with CML in chronic phase, more than 18 years, and treated with imatinib were enrolled (n = 32). Age, and sex-matched controls were also included. Platelet function test was performed using two-channel Chrono-Log aggregometer 490 at four time-points: first, at diagnosis; second, after leucoreduction (total leucocyte count, <10 × 10/l) achieved with hydroxycarbamide; third, on-imatinib at BCR-ABL less than 1%; and fourth, in an independent cohort (off-imatinib) at deep molecular response (DMR) (BCR-ABL < 0.01%). Statistical analysis was performed using IBM SPSS statistics (version 22.0). Median age of patients was 42 years (15-65), and M : F ratio was 1 : 1. At diagnosis, platelet function correlated negatively with total leucocyte count, but not with platelet count. As compared with baseline, platelet aggregation with ADP (2.5 μl), and collagen (2.5 μl) improved significantly after leucoreduction (P = 0.05 and 0.009, respectively). Imatinib further caused significant impairment of aggregation with ADP (2.5 μl), collagen (2.5 μl), and collagen (1 μl) (P = 0.04, 0.008, and 0.02, respectively). Patients in DMR also demonstrated a significant impairment of platelet aggregation with all the agonists as compared with controls. While leucoreduction alone can improve the baseline platelet function derangement in CML, imatinib further impairs it. Residual CML stem cells, or effect of imatinib on normal common myeloid progenitors might account for platelet function derangement at DMR.

摘要

: 慢性髓性白血病(CML)患者的血小板功能可能受到白细胞增多、克隆性巨核细胞增生或酪氨酸激酶抑制剂的影响。然而,这些变量从未被前瞻性评估过。我们在印度北部的一家三级护理中心进行了一项为期 1.5 年的前瞻性研究。纳入了接受伊马替尼治疗的 CML 慢性期、年龄超过 18 岁的患者(n=32)。还纳入了年龄和性别匹配的对照组。在四个时间点使用双通道 Chrono-Log 聚集仪 490 进行血小板功能测试:第一次是在诊断时;第二次是在羟基脲使白细胞计数(总白细胞计数,<10×10/l)降低后;第三次是在 BCR-ABL 小于 1%时使用伊马替尼;第四次是在独立队列(停用伊马替尼)中在深度分子反应(DMR)(BCR-ABL<0.01%)时。使用 IBM SPSS statistics(版本 22.0)进行统计分析。患者的中位年龄为 42 岁(15-65 岁),男女比例为 1:1。在诊断时,血小板功能与总白细胞计数呈负相关,但与血小板计数无关。与基线相比,白细胞减少后 ADP(2.5μl)和胶原(2.5μl)诱导的血小板聚集显著改善(P=0.05 和 0.009)。伊马替尼进一步导致 ADP(2.5μl)、胶原(2.5μl)和胶原(1μl)诱导的聚集显著受损(P=0.04、0.008 和 0.02)。与对照组相比,DMR 患者所有激动剂诱导的血小板聚集也明显受损。白细胞减少单独可以改善 CML 中血小板功能障碍的基线水平,而伊马替尼进一步损害了它。残留的 CML 干细胞,或伊马替尼对正常共同髓系祖细胞的影响可能是 DMR 时血小板功能障碍的原因。

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