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低剂量七氟醚吸入后人类激动剂诱导的粒细胞-血小板聚集的延迟抑制

Delayed inhibition of agonist-induced granulocyte-platelet aggregation after low-dose sevoflurane inhalation in humans.

作者信息

Wacker Johannes, Lucchinetti Eliana, Jamnicki Marina, Aguirre José, Härter Luc, Keel Marius, Zaugg Michael

机构信息

Institute of Anesthesiology, University Hospital Zurich, University of Zurich, Zurich, Switzerland.

出版信息

Anesth Analg. 2008 Jun;106(6):1749-58. doi: 10.1213/ane.0b013e318172f9e9.

Abstract

BACKGROUND

Sevoflurane can be used as sedative-analgesic drug with endothelial protective properties. We tested whether low-dose sevoflurane inhalation provides sustained inhibition of detrimental granulocyte-platelet aggregation in humans.

METHODS

Ten healthy male volunteers were enrolled in this crossover study. Each subject inhaled sevoflurane for 1 h at 0.5-1 vol % end-tidal concentration in oxygen (50 vol %). Inhaling oxygen (50 vol %) alone served as control. Venous blood samples were collected at baseline before inhalation, immediately after inhalation, and 24 h thereafter, and were used for flow cytometry to determine platelet surface marker (CD41, CD42b, CD62P/P-selectin, and PAC-1) on platelets and granulocytes and for kaolin-induced clot formation, as assessed by thromboelastography. In flow cytometry experiments, platelets were stimulated with arachidonic acid (AA, 30 microM), adenosine diphosphate (ADP, 1 microM), and thrombin receptor agonist peptide-6 (TRAP-6, 6 microM).

RESULTS

AA, ADP, and TRAP-6 markedly increased the expression of CD62P on platelets, whereas CD42b (shedding) and PAC-1 (heterotypic conjugates) expression decreased. The amount of granulocyte-platelet aggregates increased upon agonist stimulation. Low-dose sevoflurane inhalation reduced ADP-induced CD62P expression on platelets 24 h after inhalation, and inhibited the formation of granulocyte-platelet aggregates under stimulation with AA and ADP after 1 and 24 h, and with TRAP-6 after 24 h compared with control. Inhibition of granulocyte-platelet aggregates was accompanied by reduced clot firmness 24 h after sevoflurane inhalation compared with control.

CONCLUSIONS

We demonstrated for the first time that inhaling low-dose sevoflurane (<1 vol % end-tidal) inhibits agonist-induced granulocyte-platelet interactions 24 h after administration and thus counteracts thromboinflammatory processes.

摘要

背景

七氟醚可用作具有内皮保护特性的镇静镇痛药。我们测试了低剂量吸入七氟醚是否能持续抑制人体中有害的粒细胞 - 血小板聚集。

方法

十名健康男性志愿者参与了这项交叉研究。每位受试者在氧气(50%体积分数)中以0.5 - 1%体积分数的呼气末浓度吸入七氟醚1小时。仅吸入氧气(50%体积分数)作为对照。在吸入前的基线、吸入后即刻以及此后24小时采集静脉血样本,用于流式细胞术以测定血小板和粒细胞上的血小板表面标志物(CD41、CD42b、CD62P/P - 选择素和PAC - 1),并用于高岭土诱导的血凝块形成,通过血栓弹力图进行评估。在流式细胞术实验中,用花生四烯酸(AA,30μM)、二磷酸腺苷(ADP,1μM)和凝血酶受体激动肽 - 6(TRAP - 6,6μM)刺激血小板。

结果

AA、ADP和TRAP - 6显著增加血小板上CD62P的表达,而CD42b(脱落)和PAC - 1(异型结合物)表达降低。激动剂刺激后粒细胞 - 血小板聚集体的数量增加。低剂量吸入七氟醚在吸入后24小时降低了ADP诱导的血小板上CD62P的表达,并且与对照相比,在1小时和24小时时抑制了AA和ADP刺激下以及24小时时TRAP - 6刺激下粒细胞 - 血小板聚集体的形成。与对照相比,七氟醚吸入后24小时,粒细胞 - 血小板聚集体的抑制伴随着血凝块硬度的降低。

结论

我们首次证明,吸入低剂量七氟醚(呼气末<1%体积分数)可在给药后24小时抑制激动剂诱导的粒细胞 - 血小板相互作用,从而对抗血栓炎症过程。

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