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C6O4 对血小板聚集途径的干扰:新一代全氟烷基物质的线索。

Interference of C6O4 on platelet aggregation pathways: Cues on the new-generation of perfluoro-alkyl substance.

机构信息

Department of Medicine, Section of Internal Medicine C, University of Verona, Verona, Italy.

Department of Medicine and Unit of Andrology and Reproduction Medicine, University of Padova, Padova, Italy.

出版信息

Environ Int. 2021 Sep;154:106584. doi: 10.1016/j.envint.2021.106584. Epub 2021 Apr 23.

Abstract

BACKGROUND

Health concerns associated with the exposure to legacy perfluoro-alkyl substances (PFAS) led to the development of new-generation PFAS, such as C6O4. Here we investigated the possible effects of C6O4 on the platelet's activation profile, by incubating human platelets from healthy donors with C6O4 at different concentrations and evaluating the effects on activation, production and phenotype of platelets micro-particles (MPV) and aggregation under-flow. Based on the eventual platelet pro-aggregation profile detected, the preventive effect of acetylsalicylic acid (ASA) was also explored.

METHODS

Adhesion-induced platelet aggregation of platelet rich plasma (PRP) under flow was evaluated on collagen-coated microchip at a shear stress of 10 Dyne. The turbidimetric method was used to investigate platelet aggregation. Finally, the in vitro generation of pro-coagulant MPV in PRP was evaluated by flow cytometry, as characterized by CD41 and annexin V positive events, under resting conditions and after stimulation with agonists at low shear stress.

RESULTS

The generation of platelet aggregates under flow was significantly increased by the pretreatment of PRP with 100-200 ng/mL C6O4, compared to both the control condition and the experiment performed in presence of ASA. Arachidonic acid (AA), ADP and collagen induced an higher maximal aggregation, at turbidimetric evaluation, when PRP was pretreated with 100-500 ng/mL C6O4. In addition, PRP stimulated with AA also showed a steeper slope of the aggregation curve. The aggregation induced by the tested agonists was almost abolished by ASA. Finally, pretreatment with C6O4 increased the number of MPV in resting conditions and in presence of ADP and TRAP. ASA tended to reduce MPV generation.

CONCLUSIONS

Exposure to C6O4 associates with an increased platelet response to agonists, translating into a possible increased risk of cardiovascular events. Pending a further clarification on the toxicokinetics of this compound, our results claim the possible prophylactic use of ASA.

摘要

背景

与接触传统全氟烷基物质 (PFAS) 相关的健康问题促使人们开发了新一代 PFAS,如 C6O4。在这里,我们研究了 C6O4 对血小板激活谱的可能影响,方法是将来自健康供体的人血小板与不同浓度的 C6O4 孵育,并评估其对血小板微颗粒 (MPV) 的激活、产生和表型以及在低切应力下的聚集的影响。基于检测到的最终血小板促聚集谱,还探索了乙酰水杨酸 (ASA) 的预防作用。

方法

在 10 达因的切应力下,在胶原涂层微芯片上评估富含血小板的血浆 (PRP) 的诱导性血小板聚集。采用比浊法研究血小板聚集。最后,通过流式细胞术评估 PRP 中在低切应力下刺激激动剂时 pro-coagulant MPV 的体外生成,特征为 CD41 和膜联蛋白 V 阳性事件。

结果

与对照条件和存在 ASA 时的实验相比,PRP 用 100-200ng/mL C6O4 预处理后,在流动下血小板聚集体的生成显著增加。在用 100-500ng/mL C6O4 预处理后,PRP 在比浊评价中用 AA、ADP 和胶原诱导的最大聚集更高。此外,用 AA 刺激的 PRP 也显示出聚集曲线更陡峭的斜率。在测试的激动剂诱导的聚集几乎被 ASA 完全抑制。最后,C6O4 的预处理增加了静息状态和 ADP 和 TRAP 存在下的 MPV 数量。ASA 倾向于减少 MPV 的产生。

结论

暴露于 C6O4 与血小板对激动剂的反应增加有关,这可能转化为心血管事件风险的增加。在进一步阐明该化合物的毒代动力学之前,我们的结果表明可能需要预防性使用 ASA。

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