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在小鼠中,随着血小板计数升高,对单剂量血小板生成素的反应降低。

Responses to single-dose thrombopoietin decrease with higher platelet counts in mice.

作者信息

Kelemen E, Lehoczky D, Jakab K, Bátai A, Vargha P

机构信息

National Institute of Haematology and Immunology, Semmelweis University Medical School, Budapest, Hungary.

出版信息

Acta Haematol. 1999 Mar;101(1):41-5. doi: 10.1159/000040919.

Abstract

Since the description of human thrombopoietin (TPO) we investigated the thrombocytosis-inducing capacity of human serum samples derived from individuals with altered thrombocytopoiesis. Several times the degree of thrombocytosis developing in recipient mice differed markedly even when applying the same human material. In the last 2 years, we applied single doses of recombinant human TPO (rHuTPO) to random-bred CFLP mice, and the same observation was made. Taken together with previous information (before 1970) it was possible to select cases in which the percent increases in circulating platelet counts inversely correlated with the starting levels. It appears, however, that apart from the known absorbing role of platelets and megakaryocytes, the response to single doses of exogenous rHuTPO in mice depends, at least partially, on an unknown endogenous homeostatic mechanism. Mixing thrombopoietically active human sera with platelet-free normal serum in a 1:1 ratio remarkably reduced the thrombocytosis-inducing capacity. Repeated pharmacological doses of TPO, applied in the majority of the reported trials, however, easily obscure the physiological control mechanism.

摘要

自从对人血小板生成素(TPO)进行描述以来,我们研究了来自血小板生成改变个体的人血清样本诱导血小板增多的能力。即使使用相同的人体材料,受体小鼠中出现的血小板增多程度有时也会有显著差异。在过去两年中,我们给随机繁殖的CFLP小鼠单次注射重组人TPO(rHuTPO),也得到了相同的观察结果。结合之前(1970年之前)的信息,可以选择出循环血小板计数的百分比增加与起始水平呈负相关的病例。然而,似乎除了血小板和巨核细胞已知的吸收作用外,小鼠对外源单剂量rHuTPO的反应至少部分取决于一种未知的内源性稳态机制。将具有血小板生成活性的人血清与无血小板的正常血清按1:1比例混合,可显著降低诱导血小板增多的能力。然而,在大多数已报道的试验中应用的重复药理剂量的TPO很容易掩盖生理控制机制。

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