Phosphodiesterases Mediate The Augmentation of Myogenic Constriction by Inhibitory G Protein Signaling And Is Negatively Modulated by The Dual Action of RGS2 And 5

Function Pub Date : 2024-01-19 DOI:10.1093/function/zqae003
Bo Sun, Nia Smith, Alethia J. Dixon, Patrick Osei-Owusu
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Abstract

G protein regulation by regulators of G protein signaling (RGS) proteins of the R4/B family plays a key role in vascular tone maintenance; However, the regulatory mechanisms are poorly understood. Previous studies showed that the loss of Gi/o and Gq/11 regulation by RGS2 and RGS5 is involved in augmented vascular tone and decreased uterine blood flow in mice. RGS2 and 5 are structurally and functionally closely related and are co-expressed in the resistance vasculature, including the uterine vascular bed. However, whether and how RGS2 and 5 coordinate their regulatory activities to finetune G protein signaling and regulate vascular tone are unclear. Here, we tested the hypothesis that the integrated activity of RGS2 and 5 modulates vascular tone by negatively regulating Gi/o signaling to promote cAMP-dependent attenuation of uterine artery (UA) myogenic tone (MT). Using pressure myography, we examined MT of UA segments isolated from non-pregnant wild type (WT), Rgs2−/−, Rgs5−/−, and Rgs2/5 dbKO mice in the absence and presence of exogenous cAMP or chemical inhibition of Gi/o signaling, while nitric oxide tone was continuously suppressed with the eNOS inhibitor, L-NAME. We found that MT was reduced in Rgs5−/− relative to WT or Rgs2−/− UA in the absence or presence of L-NAME. Activating Gi/o with dopamine increased, whereas exogenous cAMP decreased MT in Rgs5−/− UA to similar levels in WT UA. Dual deletion of Rgs2 and 5 abolished the reduction of MT due to the absence of only Rgs5 and enhanced dopamine-induced Gi/o effects in Rgs2/5 dbKO UA. Conversely, and as in WT UA, Gi/o inhibition with pertussis toxin or the application of exogenous cAMP decreased MT in Rgs2/5 dbKO to similar levels in Rgs5−/− UA. Application of the pan-phosphodiesterase (PDE) inhibitor, IBMX, concentration dependently decreased and normalized MT in all genotypes, and blocked dopamine-mediated MT augmentation in Rgs2−/−, Rgs5−/−, and Rgs2/5 dbKO UA. These results indicate that activated Gi/o augments MT by promoting PDE-mediated inhibition of cAMP-dependent vasodilatation; and while both RGS2 and 5 negatively regulate this novel Gi/o-PDE-cAMP signaling pathway, RGS5 dampens the inhibitory efficacy of RGS2 towards Gi/o in uterine arteries.
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磷酸二酯酶介导抑制性 G 蛋白信号对生肌收缩的增强作用,并受到 RGS2 和 5 的双重作用的负向调节
R4/B家族的G蛋白信号调节蛋白(RGS)对G蛋白的调节在维持血管张力中起着关键作用;然而,人们对其调节机制还知之甚少。先前的研究表明,RGS2 和 RGS5 失去对 Gi/o 和 Gq/11 的调控参与了小鼠血管张力增强和子宫血流量减少的过程。RGS2 和 RGS5 在结构上和功能上密切相关,并在包括子宫血管床在内的阻力血管中共同表达。然而,RGS2 和 5 是否以及如何协调它们的调节活动以微调 G 蛋白信号并调节血管张力尚不清楚。在这里,我们测试了一个假设,即 RGS2 和 5 的综合活性通过负向调节 Gi/o 信号来调节血管张力,从而促进 cAMP 依赖性的子宫动脉(UA)肌张力(MT)衰减。利用压力肌电图,我们检测了在没有和有外源 cAMP 或化学抑制 Gi/o 信号传导的情况下,从未孕野生型(WT)、Rgs2-/-、Rgs5-/- 和 Rgs2/5 dbKO 小鼠分离的 UA 节段的 MT,同时用 eNOS 抑制剂 L-NAME 持续抑制一氧化氮张力。我们发现,在没有或有L-NAME的情况下,Rgs5-/- UA的MT相对于WT或Rgs2-/- UA有所降低。用多巴胺激活Gi/o可使Rgs5-/-UA的MT增加,而外源性cAMP则可使Rgs5-/-UA的MT降低到与WT UA相似的水平。在 Rgs2/5 dbKO UA 中,Rgs2 和 5 的双重缺失消除了因仅缺失 Rgs5 而导致的 MT 减少,并增强了多巴胺诱导的 Gi/o 效应。相反,与在 WT UA 中一样,用百日咳毒素抑制 Gi/o 或应用外源 cAMP 会使 Rgs2/5 dbKO 中的 MT 下降到与 Rgs5-/- UA 中相似的水平。应用泛磷酸二酯酶(PDE)抑制剂 IBMX 可使所有基因型的 MT 浓度下降并恢复正常,并阻断 Rgs2-/-、Rgs5-/- 和 Rgs2/5 dbKO UA 中多巴胺介导的 MT 增量。这些结果表明,活化的 Gi/o 通过促进 PDE 介导的 cAMP 依赖性血管舒张抑制作用来增强 MT;虽然 RGS2 和 5 对这一新型 Gi/o-PDE-cAMP 信号通路有负向调节作用,但 RGS5 可抑制 RGS2 对子宫动脉中 Gi/o 的抑制作用。
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