Database Commons
Database Commons

a catalog of worldwide biological databases

Database Profile

AVP-Phos

General information

URL: https://esbl.nhlbi.nih.gov/Databases/AVP-Phos
Full name: Vasopressin-Regulated Phosphorylation Sites in Collecting Duct
Description: Vasopressin regulates renal water excretion through control of the aquaporin-2 water channel in collecting duct cells. Studies of vasopressin-induced protein phosphorylation have focused mainly on the phosphorylation of aquaporin-2. This study describes 44 phosphoproteins other than aquaporin-2 that undergo vasopressin-mediated phosphorylation changes and summarizes potential physiological roles of each.
Year founded: 2023
Last update: 2021-11-29
Version: 1.0
Accessibility:
Accessible
Country/Region: United States

Classification & Tag

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Contact information

University/Institution: National Institutes of Health
Address: Epithelial Systems Biology Laboratory, Systems Biology Center, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, Maryland
City:
Province/State:
Country/Region: United States
Contact name (PI/Team): Mark A Knepper
Contact email (PI/Helpdesk): knep@helix.nih.gov

Publications

36264882
Data resource: vasopressin-regulated protein phosphorylation sites in the collecting duct. [PMID: 36264882]
Euijung Park, Chin-Rang Yang, Viswanathan Raghuram, Venkatesh Deshpande, Arnab Datta, Brian G Poll, Kirby T Leo, Hiroaki Kikuchi, Lihe Chen, Chung-Lin Chou, Mark A Knepper

Vasopressin controls renal water excretion through actions to regulate aquaporin-2 (AQP2) trafficking, transcription, and degradation. These actions are in part dependent on vasopressin-induced phosphorylation changes in collecting duct cells. Although most efforts have focused on the phosphorylation of AQP2 itself, phosphoproteomic studies have identified many vasopressin-regulated phosphorylation sites in proteins other than AQP2. The goal of this bioinformatics-based review is to create a compendium of vasopressin-regulated phosphorylation sites with a focus on those that are seen in both native rat inner medullary collecting ducts and cultured collecting duct cells from the mouse (mpkCCD), arguing that these sites are the best candidates for roles in AQP2 regulation. This analysis identified 51 vasopressin-regulated phosphorylation sites in 45 proteins. We provide resource web pages at https://esbl.nhlbi.nih.gov/Databases/AVP-Phos/ and https://esbl.nhlbi.nih.gov/AVP-Network/, listing the phosphorylation sites and describing annotated functions of each of the vasopressin-targeted phosphoproteins. Among these sites are 23 consensus protein kinase A (PKA) sites that are increased in response to vasopressin, consistent with a central role for PKA in vasopressin signaling. The remaining sites are predicted to be phosphorylated by other kinases, most notably ERK1/2, which accounts for decreased phosphorylation at sites with a X-p(S/T)-P-X motif. Additional protein kinases that undergo vasopressin-induced changes in phosphorylation are Camkk2, Cdk18, Erbb3, Mink1, and Src, which also may be activated directly or indirectly by PKA. The regulated phosphoproteins are mapped to processes that hypothetically can account for vasopressin-mediated control of AQP2 trafficking, cytoskeletal alterations, and gene expression, providing grist for future studies. Vasopressin regulates renal water excretion through control of the aquaporin-2 water channel in collecting duct cells. Studies of vasopressin-induced protein phosphorylation have focused mainly on the phosphorylation of aquaporin-2. This study describes 44 phosphoproteins other than aquaporin-2 that undergo vasopressin-mediated phosphorylation changes and summarizes potential physiological roles of each.

Am J Physiol Renal Physiol. 2023:324(1) | 12 Citations (from Europe PMC, 2026-03-28)

Ranking

All databases:
2740/6932 (60.488%)
Gene genome and annotation:
849/2039 (58.411%)
Genotype phenotype and variation:
398/1012 (60.771%)
2740
Total Rank
11
Citations
3.667
z-index

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Record metadata

Created on: 2023-08-23
Curated by:
Xinyu Zhou [2023-09-12]
Yue Qi [2023-09-04]
Yuanyuan Cheng [2023-08-23]