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首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >Platelets in nonresponders to epinephrine stimulation showed reduced response to ADP.
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Platelets in nonresponders to epinephrine stimulation showed reduced response to ADP.

机译:对肾上腺素刺激无反应的血小板显示对ADP的反应降低。

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It has been reported that platelets from some healthy donors did not respond to epinephrine (Epi). To identify the cause for the lack of response, we examined the alpha(2) adrenoceptor in the platelets and their signal transduction pathways. No differences in the genomic (-2076 to 1526 bp) and coding region of alpha(2A) adrenoceptor complementary DNA (cDNA) were found between the responders (R) and nonresponders (NR). No expression of alpha(2B) or alpha(2C) adrenoceptor was detected in platelets. When UK14,304 was used to induce platelet aggregation, similar effect to Epi was observed between R and NR, and any involvement of the alpha(1) and beta adrenoceptor was ruled out. Radioligand binding assay showed similar number of alpha(2) binding sites between the two groups (139+/-25/platelet vs. 145+/-37/platelets). However, platelets from NR showed a weaker response to adenosine diphosphate (ADP, 52.3+/-17.8% vs. 80.5+/-8.7% from R, P<.01). In the presence of P2Y(1) antagonist adenosine 3',5'-diphosphosulfate (A3P5PS), ADP failed to induce platelet aggregation in NR (7.8+/-4.7% vs. 64.7+/-11.2% in R, P<.01). Addition of SQ22,536 to inhibit adenylyl cyclase did not convert NR to R. These observations demonstrate that there is an impaired platelet responsiveness to ADP as well as to Epi in NR, due to a difference in downstream of the signal transduction pathway but independent of adenylyl cyclase inhibition.
机译:据报道,一些健康供体的血小板对肾上腺素(Epi)无反应。为了确定缺乏反应的原因,我们检查了血小板中的α(2)肾上腺素能受体及其信号转导途径。在响应者(R)和非响应者(NR)之间未发现基因组(-2076至1526 bp)和α(2A)肾上腺素受体互补DNA(cDNA)编码区的差异。在血小板中未检测到α(2B)或α(2C)肾上腺素能受体的表达。当UK14,304用于诱导血小板聚集时,在R和NR之间观察到与Epi相似的作用,并且排除了alpha(1)和β肾上腺素能受体的任何参与。放射性配体结合测定显示两组之间相似数量的alpha(2)结合位点(139 +/- 25 /血小板与145 +/- 37 /血小板)。然而,来自NR的血小板显示出对二磷酸腺苷的较弱的响应(ADP,52.3 +/- 17.8%,而来自R的血小板为80.5 +/- 8.7%,P <0.01)。在存在P2Y(1)拮抗剂腺苷3',5'-二磷酸硫酸盐(A3P5PS)的情况下,ADP无法诱导NR中的血小板凝集(7.8 +/- 4.7%,R中为64.7 +/- 11.2%,P <。 01)。加入SQ22,536抑制腺苷酸环化酶并不能将NR转化为R。这些观察结果表明,由于信号转导途径下游的差异,但与信号转导途径的差异,血小板对NR中的ADP和Epi的反应性受损。腺苷酸环化酶抑制作用。

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