Dual loss of regulator of G protein signaling 2 and 5 exacerbates ventricular myocyte arrhythmias and disrupts the fine-tuning of Gi/o signaling

Dahlen, Shelby; Bernadyn, Tyler F.; Dixon, Alethia J.; Sun, Bo; Xia, Jingsheng; Owens, Elizabeth A.; Osei‐Owusu, Patrick

doi:10.1016/j.yjmcc.2022.05.009

Cited by 1 publication

(3 citation statements)

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“… 62 In ventricular myocytes, the loss of only RGS2 or both RGS2 and 5 but not RGS5 alone leads to ventricular myocyte arrhythmias associated with decreased cAMP generation that is reversible by chemical inactivation of G i/o with PTX. 40 The results in this study also indicate that in the absence of NOS-generated nitric oxide, the modulation of G i/o activity by RGS2 and 5 to promote cAMP signaling is critical to preventing excessive myogenic response to changes in intraluminal pressure in the uterine vascular bed. And, besides the regulation of the canonical inhibition of cAMP generation by G i/o , we found a novel mechanism by which RGS2 and 5 promote cAMP signaling to modulate UA myogenic tone.…”

Section: Discussionmentioning

confidence: 52%

“…Others and we have reported that this effector antagonism between multiple RGS proteins is present in ventricular myocytes and the central nervous system. 40 , 62 In a previous study by Garzon and colleagues, it was reported that effector antagonism by RG-R7 is involved in the delayed tolerance associated with repeated morphine administration. That is, RGS-R7 proteins were found to bind G i/o/z proteins and sequester them, thereby preventing the acceleration of GTP hydrolysis necessary to restrict the amplitude of opioid analgesia by the more efficient RGS-R4 and RGS-Rz.…”

Section: Discussionmentioning

confidence: 99%

“… 38 , 39 Rgs2/5 dbKO mice were generated from crosses between Rgs2 −/− and Rgs5 −/− mice, as previously described. 40 All experiments were performed in accordance with the protocols approved by the Institutional Animal Care and Use Committee at Case Western Reserve University School of Medicine, in accordance with the National Institutes of Health Guidance for the Care and Use of Laboratory Animals.…”

Section: Methodsmentioning

confidence: 99%

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Phosphodiesterases Mediate the Augmentation of Myogenic Constriction by Inhibitory G Protein Signaling and is Negatively Modulated by the Dual Action of RGS2 and 5

Sun,

Smith,

Dixon

et al. 2024

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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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Section: Discussionmentioning

confidence: 52%

Section: Discussionmentioning

confidence: 99%