氯吡格雷抗血小板治疗可预防高血压大鼠主动脉的内皮功能障碍和血管重塑。
Anti-platelet therapy with clopidogrel prevents endothelial dysfunction and vascular remodeling in aortas from hypertensive rats.
作者信息
Giachini Fernanda R, Leite Romulo, Osmond David A, Lima Victor V, Inscho Edward W, Webb R Clinton, Tostes Rita C
机构信息
Institute of Biological Sciences and Health, Federal University of Mato Grosso, Barra do Garças, MT, Brazil.
School of Pharmacy, Federal University of Ouro Preto, Ouro Preto, MG, Brazil.
出版信息
PLoS One. 2014 Mar 17;9(3):e91890. doi: 10.1371/journal.pone.0091890. eCollection 2014.
The aim was to investigate the beneficial effects of clopidogrel in thoracic aorta function and structure and to characterize if P2Y12 receptors contribute to these effects. Male Sprague Dawley rats were infused with angiotensin II [(Ang II) 60 ng x min(-1), 14 days] or saline (control rats) and were simultaneously treated with clopidogrel (10 mg x kg(-1) x day(-1)) or vehicle. After 14 days, systolic blood pressure (mmHg) was similar in Ang II-hypertensive rats treated with clopidogrel or vehicle (199±9 vs. 190±11, respectively). Systolic blood pressure in control rats was not altered by clopidogrel treatment (128±1 vs. vehicle, 134±2). Endothelium-dependent relaxation induced by 2-MeS-ADP was decreased in aortas from vehicle-treated Ang II-hypertensive rats, compared to vehicle-treated control rats. This response was elicited via activation of P2Y1 and P2Y12 receptors. In the presence of L-NAME and indomethacin, 2-MeS-ADP induced contraction and this response was augmented in vehicle-treated Ang II-hypertensive rats, compared to vehicle-treated control rats. The contraction to 2-MeS-ADP was evoked by P2Y13 and P2Y12 receptor activation. Clopidogrel-treatment did not normalize relaxation or contractile responses induced by 2-MeS-ADP in aortas from Ang II-hypertensive rats. P2Y1 and P2Y12 protein expression was increased, whereas P2Y13 receptor expression was reduced in aorta from vehicle-treated Ang II-hypertensive rats. Endothelium-dependent relaxation upon acetylcholine-stimulation was reduced in vehicle-treated Ang II-hypertensive rats, and clopidogrel treatment was effective in improving endothelial function. Clopidogrel also prevented vascular remodeling, evidenced by augmented media thickness in aortas from Ang II-hypertensive rats. Clopidogrel has beneficial effects on the aortic endothelium of Ang II-hypertensive rats, but its effects do not seem to be directly related to the presence of P2Y12 receptors in this vessel.
本研究旨在探讨氯吡格雷对胸主动脉功能和结构的有益作用,并确定P2Y12受体是否参与这些作用。将雄性Sprague Dawley大鼠输注血管紧张素II [(Ang II)60 ng·min⁻¹,共14天]或生理盐水(对照大鼠),并同时给予氯吡格雷(10 mg·kg⁻¹·天⁻¹)或赋形剂。14天后,接受氯吡格雷或赋形剂治疗的Ang II高血压大鼠的收缩压(mmHg)相似(分别为199±9和190±11)。氯吡格雷治疗未改变对照大鼠的收缩压(赋形剂组为134±2,氯吡格雷组为128±1)。与接受赋形剂治疗的对照大鼠相比,接受赋形剂治疗的Ang II高血压大鼠主动脉中由2-MeS-ADP诱导的内皮依赖性舒张降低。这种反应是通过激活P2Y1和P2Y12受体引发的。在L-NAME和吲哚美辛存在的情况下,2-MeS-ADP诱导收缩,与接受赋形剂治疗的对照大鼠相比,接受赋形剂治疗的Ang II高血压大鼠的这种反应增强。对2-MeS-ADP的收缩是由P2Y13和P2Y12受体激活引起的。氯吡格雷治疗未能使Ang II高血压大鼠主动脉中由2-MeS-ADP诱导的舒张或收缩反应恢复正常。接受赋形剂治疗的Ang II高血压大鼠主动脉中P2Y1和P2Y12蛋白表达增加,而P2Y13受体表达减少。接受赋形剂治疗的Ang II高血压大鼠乙酰胆碱刺激后的内皮依赖性舒张降低,氯吡格雷治疗可有效改善内皮功能。氯吡格雷还可预防血管重塑,Ang II高血压大鼠主动脉中膜厚度增加证明了这一点。氯吡格雷对Ang II高血压大鼠的主动脉内皮有有益作用,但其作用似乎与该血管中P2Y12受体的存在无直接关系。
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