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当血小板减少症是由于巨核细胞缺乏所致时,人体血小板生成素水平较高;而当血小板减少症是由于血小板破坏增加所致时,人体血小板生成素水平较低。

Human thrombopoietin levels are high when thrombocytopenia is due to megakaryocyte deficiency and low when due to increased platelet destruction.

作者信息

Emmons R V, Reid D M, Cohen R L, Meng G, Young N S, Dunbar C E, Shulman N R

机构信息

Hematology Branch, NHLBI, NIH, Bethesda, MD 20892, USA.

出版信息

Blood. 1996 May 15;87(10):4068-71.

PMID:8639762
Abstract

Thrombopoietin (TPO), the ligand for c-mpl, stimulates proliferation of committed megakaryocytic progenitors and induces maturation of megakaryocytes. To better understand factors regulating TPO levels, we measured blood levels of TPO in patients with impaired platelet production due to aplastic anemia (AA) and with platelet destructive disorders, including idiopathic thrombocytopenic purpura (ITP), posttransfusion purpura (PTP), drug purpura (DP), and X-linked thrombocytopenia (XLTP). The TPO receptor capture enzyme immunoassay (EIA) used had a detection limit of integral of approximately-150 to 200 pg/mL. TPO was undetectable in 88 of 89 normal individuals. Eighteen of 19 patients with AA and a mean platelet count (MPC) of 18,000/microliters (2,000 to 61,000/microliters) had markedly elevated TPO levels (mean, 1,467 pg/mL; range, 597 to 3,834 pg/mL). Eight AA patients who responded to immunosuppressive therapy with their MPC increasing to 140,000/microliters (92,000 to 175,000/microliters) had substantial decreases in TPO (mean, 440 pg/mL; range, 193 to 771 pg/mL). Initial TPO levels did not differ significantly between responders and nonresponders. In contrast, all 21 patients with ITP and an MPC of 16,000/microliters (1,000 to 51,000 /microliters) had undetectable TPO levels, as did 6 patients with acute PTP or DP and 2 patients with XLTP. Megakaryocyte mass, reflected in the rate of platelet production, appears to be the major determinant of TPO levels in thrombocytopenic patients rather than circulating platelet levels per se. Measurement of serum TPO may be useful in differentiating thrombocytopenias due to peripheral destruction from those due to thrombopoietic failure.

摘要

血小板生成素(TPO)是c-mpl的配体,可刺激定向巨核细胞祖细胞的增殖并诱导巨核细胞成熟。为了更好地了解调节TPO水平的因素,我们检测了再生障碍性贫血(AA)导致血小板生成受损的患者以及患有血小板破坏性疾病(包括特发性血小板减少性紫癜(ITP)、输血后紫癜(PTP)、药物性紫癜(DP)和X连锁血小板减少症(XLTP))患者的血液中TPO水平。所使用的TPO受体捕获酶免疫测定法(EIA)的检测限约为-150至200 pg/mL。89名正常个体中有88名检测不到TPO。19名AA患者中,平均血小板计数(MPC)为18,000/微升(2,000至61,000/微升)的18名患者TPO水平显著升高(平均为1,467 pg/mL;范围为597至3,834 pg/mL)。8名对免疫抑制治疗有反应且MPC增加至140,000/微升(92,000至175,000/微升)的AA患者TPO大幅下降(平均为440 pg/mL;范围为193至771 pg/mL)。初始TPO水平在有反应者和无反应者之间无显著差异。相比之下,所有21名ITP患者(MPC为16,000/微升(1,000至51,000/微升))、6名急性PTP或DP患者以及2名XLTP患者的TPO水平均检测不到。反映在血小板生成速率上的巨核细胞量似乎是血小板减少患者TPO水平的主要决定因素,而非循环血小板水平本身。检测血清TPO可能有助于区分因外周破坏导致的血小板减少症和因血小板生成衰竭导致的血小板减少症。

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Human thrombopoietin levels are high when thrombocytopenia is due to megakaryocyte deficiency and low when due to increased platelet destruction.当血小板减少症是由于巨核细胞缺乏所致时,人体血小板生成素水平较高;而当血小板减少症是由于血小板破坏增加所致时,人体血小板生成素水平较低。
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