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骨肿瘤患者前列环素活性稳定性降低。

Decreased stabilization of prostacyclin activity in patients with bone tumors.

作者信息

Mehta P, Ostrowski N, Brigmon L

出版信息

Cancer Res. 1984 Jul;44(7):3132-4.

PMID:6373003
Abstract

Tumor metastasis is mediated in part by platelet activation. Since prostacyclin regulates platelet activity, we examined stabilization of bioactivity of exogenous prostacyclin in plasma of patients with malignant bone tumors. Bioactivity of prostacyclin (platelet aggregation inhibition) incubated in patient plasma was found to be significantly less compared to that in normal plasma. In addition, the duration of bioactivity of prostacyclin was considerably less in plasma of patients with bone tumors. These preliminary data indicate decreased prostacyclin activity in plasma of patients with malignant bone tumors, which may be a mechanism of platelet-tumor cell aggregate formation and subsequent evolution of metastasis.

摘要

肿瘤转移部分是由血小板激活介导的。由于前列环素调节血小板活性,我们检测了恶性骨肿瘤患者血浆中外源性前列环素生物活性的稳定性。与正常血浆相比,在患者血浆中孵育的前列环素(抑制血小板聚集)的生物活性显著降低。此外,骨肿瘤患者血浆中前列环素生物活性的持续时间也明显缩短。这些初步数据表明,恶性骨肿瘤患者血浆中前列环素活性降低,这可能是血小板 - 肿瘤细胞聚集体形成及随后转移进展的一种机制。

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