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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Evaluation of the effects of RP5063, a novel, multimodal, serotonin receptor modulator, as single-agent therapy and co-administrated with sildenafil, bosentan, and treprostinil in a monocrotaline-induced pulmonary arterial hypertension rat model
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Evaluation of the effects of RP5063, a novel, multimodal, serotonin receptor modulator, as single-agent therapy and co-administrated with sildenafil, bosentan, and treprostinil in a monocrotaline-induced pulmonary arterial hypertension rat model

机译:RP5063,一种新型,多式联运,血清素受体调节剂的效果评价,作为单症治疗和共同促进西地那非,波丝沙坦和赤裸蛋白酶,在一角质碱诱导的肺动脉高压大鼠模型中

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摘要

Pulmonary arterial hypertension (PAH), a condition that is defined by pulmonary vasculature constriction and remodeling, involves dysfunctional signaling of the serotonin (5-HT) receptors, 5-HT2A/2B/7. In a rat model of monocrotaline (MCT)-induced PAH, the effectiveness of RP5063 (RP), a dopamine and 5-HT receptor modulator, was evaluated as monotherapy and as an adjunct to standard PAH treatments. After a single 60 mg/kg dose of MCT, rats received vehicle (MCT+Veh; gavage twice-daily [b.i.d.]), RP (10 mg/kg; gavage b.i.d.), bosentan (B; 100 mg/kg; gavage BID), sildenafil (S; 50 mg/kg; gavage, BID), treprostinil (T; 100 ng/kg/min over 24 h intravenous), RP+B, RP+S, and RP+T for 28 days. Single-agent RP limited the functional and structural effects of PAH seen in the MCT+Veh group, with significant improvements in pulmonary hemodynamics, right ventricular (RV) hypertrophy, SO2, and pulmonary blood vessel structural changes. These effects appeared comparable with those associated with B, S, and T. Adjunctive RP treatment resulted in significantly lower mean pulmonary arterial pressures, RV systolic pressure. It also improved SO2 measurements, as compared with MCT+Veh (P0.05), and diastolic pulmonary artery pressure (P0.05), as compared with single-agent B and S therapy (Bonferroni method adjusting for multiplicity). RP+S appeared to show the most consistent and extensive effects on pulmonary hemodynamics, respiratory parameters, and histopathologic changes. These results corroborate earlier preclinical findings supporting the efficacy of single-agent RP in PAH. RP, as mono and adjunctive therapy compared with induced-control, mitigated the functional and structural effects of MCT-induced PAH.
机译:肺动脉高血压(PAH),由肺脉管系统收缩和重塑定义的条件涉及血清素(5-HT)受体,5-HT2A / 2B / 7的功能障碍信号传导。在偏菌碱(MCT)诱导的PAH的大鼠模型中,RP5063(RP),多巴胺和5-HT受体调节剂的有效性被评为单疗法,作为标准PAH治疗的辅助。在单次60mg / kg剂量的MCT后,大鼠接受了载体(MCT + VEL;饲养疗法两次 - 每日[BID]),RP(10mg / kg; Gavage BID),Bosentan(B; 100 mg / kg; Gavage出价),西地那非(S; 50毫克/千克;灌胃,BID),曲前列素(T; 100纳克/千克/ min,历经24小时静脉内),RP + B,RP + S和RP + T 28天。单药RP限制了MCT + VOL组中PAH的功能和结构效果,具有显着改善的肺血流动力学,右心室(RV)肥大,SO2和肺血管结构变化。这些效果出现与与B,S和T相关的效果相当。辅助RP处理导致显着较低的平均肺动脉压力,RV收缩压。与单体剂B和S治疗相比,它还改善了SO2测量,与MCT +载体(P <0.05)和舒张肺动脉压(P <0.05)相比(对多种子量调节的Bonferroni方法)相比。 RP + S似乎对肺血流动力学,呼吸道参数和组织病理学变化显示出最一致和广泛的影响。这些结果证实了初期的临床前调查结果支持单药RP在PAH中的疗效。 RP,作为单声道和辅助治疗与诱导控制相比,减轻了MCT诱导的PAH的功能和结构效应。

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