Differential regulation of vacuolar H<sup>+</sup>‐ATPase subunits by transforming growth factor‐β1 in salivary ducts

Kluge, Milena; Namkoong, Eun; Khakipoor, Shokoufeh; Park, Kyungpyo; Roussa, Eleni

doi:10.1002/jcp.28147

Cited by 2 publications

(2 citation statements)

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“…During CNS development—although both TGF-β2 and TGF-β3 isoforms are expressed in neural progenitor cells, in radial glia cells and in differentiating neurons—TGF-β2 has been considered relatively more relevant compared to TGF-β3 [ 28 ]. Interestingly, several transport proteins have been identified as targets of TGF-β signaling within and outside the CNS, including CFTR, ENaC, distinct V-ATPase subunits in epithelia and NBCe1 in astrocytes [ 29 , 30 , 31 , 32 ]. We have previously shown that TGF-β signaling regulates trafficking of KCC2 to the plasma membrane in differentiating and mature mouse hippocampal neurons via TGF-β/CREB/Rab11b pathway [ 33 ].…”

Section: Introductionmentioning

confidence: 99%

TGF-β2 Regulates Transcription of the K+/Cl− Cotransporter 2 (KCC2) in Immature Neurons and Its Phosphorylation at T1007 in Differentiated Neurons

Rigkou

Magyar

Speer

et al. 2022

Cells

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KCC2 mediates extrusion of K+ and Cl− and assuresthe developmental “switch” in GABA function during neuronal maturation. However, the molecular mechanisms underlying KCC2 regulation are not fully elucidated. We investigated the impact of transforming growth factor beta 2 (TGF-β2) on KCC2 during neuronal maturation using quantitative RT-PCR, immunoblotting, immunofluorescence and chromatin immunoprecipitation in primary mouse hippocampal neurons and brain tissue from Tgf-β2-deficient mice. Inhibition of TGF-β/activin signaling downregulates Kcc2 transcript in immature neurons. In the forebrain of Tgf-β2−/− mice, expression of Kcc2, transcription factor Ap2β and KCC2 protein is downregulated. AP2β binds to Kcc2 promoter, a binding absent in Tgf-β2−/−. In hindbrain/brainstem tissue of Tgf-β2−/− mice, KCC2 phosphorylation at T1007 is increased and approximately half of pre-Bötzinger-complex neurons lack membrane KCC2phenotypes rescued through exogenous TGF-β2. These results demonstrate that TGF-β2 regulates KCC2 transcription in immature neurons, possibly acting upstream of AP2β, and contributes to the developmental dephosphorylation of KCC2 at T1007. The present work suggests multiple and divergent roles for TGF-β2 on KCC2 during neuronal maturation and provides novel mechanistic insights for TGF-β2-mediated regulation of KCC2 gene expression, posttranslational modification and surface expression. We propose TGF-β2 as a major regulator of KCC2 with putative implications for pathophysiological conditions.

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Section: Introductionmentioning

confidence: 99%

TGF-β2 Regulates Transcription of the K+/Cl− Cotransporter 2 (KCC2) in Immature Neurons and Its Phosphorylation at T1007 in Differentiated Neurons

Rigkou

Magyar

Speer

et al. 2022

Cells

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“…The cAMP pathway-elicited β3-AR stimulation might activate CREB signaling and transcription. Indeed, Kluge et al (2019) described CREB binding sequences in the promoter regions of the human B1 subunit of the V1 domain of H + -ATPase (ATP6V1B1) in the human submandibular cell line. This aspect deserves further investigation.…”

Section: Discussionmentioning

confidence: 99%

β3-Adrenoceptor as a new player in the sympathetic regulation of the renal acid–base homeostasis

Milano,

Saponara,

Gerbino

et al. 2024

Front. Physiol.

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Efferent sympathetic nerve fibers regulate several renal functions activating norepinephrine receptors on tubular epithelial cells. Of the beta-adrenoceptors (β-ARs), we previously demonstrated the renal expression of β3-AR in the thick ascending limb (TAL), the distal convoluted tubule (DCT), and the collecting duct (CD), where it participates in salt and water reabsorption. Here, for the first time, we reported β3-AR expression in the CD intercalated cells (ICCs), where it regulates acid–base homeostasis. Co-localization of β3-AR with either proton pump H+-ATPase or Cl−/HCO3− exchanger pendrin revealed β3-AR expression in type A, type B, non-A, and non-B ICCs in the mouse kidney. We aimed to unveil the possible regulatory role of β3-AR in renal acid–base homeostasis, in particular in modulating the expression, subcellular localization, and activity of the renal H+-ATPase, a key player in this process. The abundance of H+-ATPase was significantly decreased in the kidneys of β3-AR−/− compared with those of β3-AR+/+ mice. In particular, H+-ATPase reduction was observed not only in the CD but also in the TAL and DCT, which contribute to acid–base transport in the kidney. Interestingly, we found that in in vivo, the absence of β3-AR reduced the kidneys’ ability to excrete excess proton in the urine during an acid challenge. Using ex vivo stimulation of mouse kidney slices, we proved that the β3-AR activation promoted H+-ATPase apical expression in the epithelial cells of β3-AR-expressing nephron segments, and this was prevented by β3-AR antagonism or PKA inhibition. Moreover, we assessed the effect of β3-AR stimulation on H+-ATPase activity by measuring the intracellular pH recovery after an acid load in β3-AR-expressing mouse renal cells. Importantly, β3-AR agonism induced a 2.5-fold increase in H+-ATPase activity, and this effect was effectively prevented by β3-AR antagonism or by inhibiting either H+-ATPase or PKA. Of note, in urine samples from patients treated with a β3-AR agonist, we found that β3-AR stimulation increased the urinary excretion of H+-ATPase, likely indicating its apical accumulation in tubular cells. These findings demonstrate that β3-AR activity positively regulates the expression, plasma membrane localization, and activity of H+-ATPase, elucidating a novel physiological role of β3-AR in the sympathetic control of renal acid–base homeostasis.

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Differential regulation of vacuolar H⁺‐ATPase subunits by transforming growth factor‐β1 in salivary ducts

Cited by 2 publications

References 46 publications

TGF-β2 Regulates Transcription of the K+/Cl− Cotransporter 2 (KCC2) in Immature Neurons and Its Phosphorylation at T1007 in Differentiated Neurons

TGF-β2 Regulates Transcription of the K+/Cl− Cotransporter 2 (KCC2) in Immature Neurons and Its Phosphorylation at T1007 in Differentiated Neurons

β3-Adrenoceptor as a new player in the sympathetic regulation of the renal acid–base homeostasis

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Differential regulation of vacuolar H+‐ATPase subunits by transforming growth factor‐β1 in salivary ducts

Cited by 2 publications

References 46 publications

TGF-β2 Regulates Transcription of the K+/Cl− Cotransporter 2 (KCC2) in Immature Neurons and Its Phosphorylation at T1007 in Differentiated Neurons

TGF-β2 Regulates Transcription of the K+/Cl− Cotransporter 2 (KCC2) in Immature Neurons and Its Phosphorylation at T1007 in Differentiated Neurons

β3-Adrenoceptor as a new player in the sympathetic regulation of the renal acid–base homeostasis

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Differential regulation of vacuolar H⁺‐ATPase subunits by transforming growth factor‐β1 in salivary ducts