Gap Junction Regulation of Vascular Tone: Implications of Modulatory Intercellular Communication During Gestation

Ampey, Bryan C.; Morschauser, Timothy J.; Lampe, Paul D.; Magness, Ronald R.

doi:10.1007/978-1-4939-1031-1_11

Cited by 20 publications

(22 citation statements)

References 139 publications

(215 reference statements)

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“…Elevations in these endothelial vasodilators are responsible for proportional inductions of the respective elevated levels of cAMP 8,13,19 and cGMP 8,13,19 . Signaling of cyclic nucleotides are further implicated in the formation and assembly of GJs through posttranslational modifications of Cx43 22 . Thus this signaling process involves a feedforward loop between ATP, cyclic nucleotides, and Cx43-mediated GJIC to establish this pregnancy specific vasodilatory phenotype.…”

Section: Discussionmentioning

confidence: 99%

Domain-Specific Partitioning of Uterine Artery Endothelial Connexin43 and Caveolin-1

et al. 2016

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Uterine vascular adaptations facilitate rises in uterine blood flow (UBF) during pregnancy, which are associated with gap junction connexin (Cx) proteins and eNOS. In uterine artery endothelial cells (UAECs) ATP activates eNOS in a pregnancy (P) specific manner that is dependent on Cx43 function. Caveolar subcellular domain partitioning plays key roles in ATP-induced eNOS activation and NO production. Little is known regarding the partitioning of Cx proteins to caveolar domains or their dynamics upon ATP treatment. We observed that Cx43-mediated gap junction function upon ATP stimulation is associated with Cx43 re-partitioning between the non-caveolar and caveolar domains. Compared to UAECs from nonpregnant (NP) ewes, levels of ATP, PGI2, cAMP, NOx, and cGMP were 2-fold higher (P<0.05) in P-UAECs. In P-UAECs ATP increased lucifer yellow dye transfer, a response abrogated by Gap27, but not Gap 26 indicating involvement of Cx43 but not Cx37. Confocal microscopy revealed domain partitioning of Cx43 and Cav-1. In P-UAECs LC/MS/MS analysis revealed only Cx43 in the caveolar domain. In contrast, Cx37 was located only in the non-caveolar pool. Western analysis revealed that ATP increased Cx43 distribution (1.7-fold;P=0.013) to the caveolar domain, but had no effect on Cx37. These data demonstrate rapid ATP-stimulated repartitioning of Cx43 to the caveolae, where eNOS resides and plays an important role in NO-mediated increasing UBF during pregnancy.

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Section: Discussionmentioning

confidence: 99%

Domain-Specific Partitioning of Uterine Artery Endothelial Connexin43 and Caveolin-1

et al. 2016

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“…prostacyclin and nitric oxide) (Ampey et al . ). The role of intercellular communication in uterine vascular adaptations to pregnancy has been primarily addressed in the context of endothelial‐to‐endothelial cell and endothelial‐to‐vascular smooth muscle cell interactions (Ampey et al .…”

Section: Introductionmentioning

confidence: 97%

Uterine perivascular adipose tissue is a novel mediator of uterine artery blood flow and reactivity in rat pregnancy

Osikoya

Ahmed

Panahi

et al. 2019

The Journal of Physiology

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Key pointsr In vivo, uterine perivascular adipose tissue (PVAT) potentiates uterine artery blood flow in pregnant rats, although not in non-pregnant rats.r In isolated preparations, uterine PVAT has pro-contractile and anti-dilatory effects on uterine arteries.r Pregnancy induces changes in uterine arteries that makes them responsive to uterine PVAT signalling.Abstract An increase in uterine artery blood flow (UtBF) is a common and necessary feature of a healthy pregnancy. In the present study, we tested the hypothesis that adipose tissue surrounding uterine arteries (uterine perivascular adipose tissue; PVAT) is a novel local mediator of UtBF and uterine artery tone during pregnancy. In vivo experiments in anaesthetized Sprague-Dawley rats showed that pregnant animals (gestational day 16, term = 22--23 days) had a three-fold higher UtBF compared to non-pregnant animals. Surgical removal of uterine PVAT reduced UtBF only in pregnant rats. In a series of ex vivo bioassays, we demonstrated that uterine PVAT had pro-contractile and anti-dilatory effects on rat uterine arteries. In the presence of PVAT-conditioned media, isolated uterine arteries from both pregnant and non-pregnant rats had reduced vasodilatory responses. In non-pregnant rats, these responses were mediated at the level of uterine vascular smooth muscle, whereas, in pregnant rats, PVAT-media reduced endothelium-dependent relaxation. Pregnancy increased adipocyte size in ovarian adipose tissue but had no effect on uterine PVAT adipocyte morphology. In addition, pregnancy down-regulated the gene expression of metabolic adipokines in uterine but not in aortic PVAT. In conclusion, this is the first study to demonstrate that uterine PVAT plays a regulatory role in UtBF, at least in part, as a result of its actions on uterine artery tone. We propose that the interaction between the

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“…Few other important EC functions were tested [20]. To help advance efforts to therapeutically rebuild the GCX in a functional manner, we assessed the efficacy of HS regeneration by probing gap junctions, which are of great interest due to their complexity and mediation of many vasculoprotective EC functions [31–33]. Gap junctions in EC are formed by connexin (Cx) proteins of various isoforms.…”

Section: Introductionmentioning

confidence: 99%

Regeneration of glycocalyx by heparan sulfate and sphingosine 1-phosphate restores inter-endothelial communication

et al. 2017

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Vasculoprotective endothelium glycocalyx (GCX) shedding plays a critical role in vascular disease. Previous work demonstrated that GCX degradation disrupts endothelial cell (EC) gap junction connexin (Cx) proteins, likely blocking interendothelial molecular transport that maintains EC and vascular tissue homeostasis to resist disease. Here, we focused on GCX regeneration and tested the hypothesis that vasculoprotective EC function can be stimulated via replacement of GCX when it is shed. We used EC with [i] intact heparan sulfate (HS), the most abundant GCX component; [ii] degraded HS; or [iii] HS that was restored after enzyme degradation, by cellular self-recovery or artificially. Artificial HS restoration was achieved via treatment with exogenous HS, with or without the GCX regenerator and protector sphingosine 1- phosphate (S1P). In these cells we immunocytochemically examined expression of Cx isotype 43 (Cx43) at EC borders and characterized Cx-containing gap junction activity by measuring interendothelial spread of gap junction permeable Lucifer Yellow dye. With intact HS, 60% of EC borders expressed Cx43 and dye spread to 2.88 ± 0.09 neighboring cells. HS degradation decreased Cx43 expression to 30% and reduced dye spread to 1.87± 0.06 cells. Cellular self-recovery of HS restored baseline levels of Cx43 and dye transfer. Artificial HS recovery with exogenous HS partially restored Cx43 expression to 46% and yielded dye spread to only 1.03 ± 0.07 cells. Treatment with both HS and S1P, recovered HS and restored Cx43 to 56% with significant dye transfer to 3.96 ± 0.23 cells. This is the first evidence of GCX regeneration in a manner that effectively restores vasculoprotective EC communication.

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Gap Junction Regulation of Vascular Tone: Implications of Modulatory Intercellular Communication During Gestation

Cited by 20 publications

References 139 publications

Domain-Specific Partitioning of Uterine Artery Endothelial Connexin43 and Caveolin-1

Domain-Specific Partitioning of Uterine Artery Endothelial Connexin43 and Caveolin-1

Uterine perivascular adipose tissue is a novel mediator of uterine artery blood flow and reactivity in rat pregnancy

Regeneration of glycocalyx by heparan sulfate and sphingosine 1-phosphate restores inter-endothelial communication

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