Last update 01 Nov 2024

PKG

Last update 01 Nov 2024

Basic Info

Synonyms

cGK 1, cGK1, cGKI

+ [11]

Introduction

Serine/threonine protein kinase that acts as key mediator of the nitric oxide (NO)/cGMP signaling pathway. GMP binding activates PRKG1, which phosphorylates serines and threonines on many cellular proteins. Numerous protein targets for PRKG1 phosphorylation are implicated in modulating cellular calcium, but the contribution of each of these targets may vary substantially among cell types. Proteins that are phosphorylated by PRKG1 regulate platelet activation and adhesion, smooth muscle contraction, cardiac function, gene expression, feedback of the NO-signaling pathway, and other processes involved in several aspects of the CNS like axon guidance, hippocampal and cerebellar learning, circadian rhythm and nociception. Smooth muscle relaxation is mediated through lowering of intracellular free calcium, by desensitization of contractile proteins to calcium, and by decrease in the contractile state of smooth muscle or in platelet activation. Regulates intracellular calcium levels via several pathways: phosphorylates IRAG1 and inhibits IP3-induced Ca(2+) release from intracellular stores, phosphorylation of KCNMA1 (BKCa) channels decreases intracellular Ca(2+) levels, which leads to increased opening of this channel. PRKG1 phosphorylates the canonical transient receptor potential channel (TRPC) family which inactivates the associated inward calcium current. Another mode of action of NO/cGMP/PKGI signaling involves PKGI-mediated inactivation of the Ras homolog gene family member A (RhoA). Phosphorylation of RHOA by PRKG1 blocks the action of this protein in myriad processes: regulation of RHOA translocation; decreasing contraction; controlling vesicle trafficking, reduction of myosin light chain phosphorylation resulting in vasorelaxation. Activation of PRKG1 by NO signaling alters also gene expression in a number of tissues. In smooth muscle cells, increased cGMP and PRKG1 activity influence expression of smooth muscle-specific contractile proteins, levels of proteins in the NO/cGMP signaling pathway, down-regulation of the matrix proteins osteopontin and thrombospondin-1 to limit smooth muscle cell migration and phenotype. Regulates vasodilator-stimulated phosphoprotein (VASP) functions in platelets and smooth muscle.

Drugs associated with PKG

CN238

Target

PKG

Mechanism

PKG modulators

Active Org.

Eberhard Karls Universität Tübingen

Originator Org.

Eberhard Karls Universität Tübingen

Active Indication

Neurodegenerative Diseases [+1]

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

PKG activators(Merck)

Target

PKG

Mechanism

PKG activators

Active Org.

Merck & Co., Inc.

Originator Org.

Merck & Co., Inc.

Active Indication

Cardiovascular Diseases

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

100 Clinical Results associated with PKG

100 Translational Medicine associated with PKG

0 Patents (Medical) associated with PKG

4,354

Literatures (Medical) associated with PKG

01 Jan 2025·Journal of Ethnopharmacology

Improvement effect and mechanism of XuanFuDaiZhe tang on rats with diarrheal irritable bowel syndrome induced by colorectal dilation

Article

Author: Zhang, Kuo ; Wu, Chunfu ; Li, Shile ; Gu, Guanliang ; Cong, Huan ; Wang, Shasha ; Pang, Jie ; Jing, Weiliang ; Yang, Jingyu

ETHNOPHARMACOLOGICAL RELEVANCEXuanFuDaiZhe Tang (XFDZT) is used in traditional Chinese medicine (TCM) to treat diarrhoea-predominant irritable bowel syndrome (IBS-D). Our laboratory has demonstrated that XFDZT remarkably improves various gastrointestinal motility disorders in animal models. However, previous studies have only focused on one or several protein targets without systematically investigating dynamic changes and protein interrelations.AIM OF THE STUDYTo explore the mechanisms underlying the therapeutic action of XFDZT in IBS-D using a network pharmacology approach and in vivo experiments.MATERIALS AND METHODSThe active compounds of XFDZT were selected from TCM Systems Pharmacology and TCM Integrated databases, and potential targets were identified using the Swiss Target Prediction databases. Targets related to IBS-D were mined from the DisGeNet, Drug Bank, and Therapeutic Target databases. The intersecting protein-protein interactions (PPIs) of the drug-disease crossover genes were analysed, and a central PPI network was constructed using the STRING database and Cytoscape 3.7.2. Following Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway analyses, a gene pathway network was constructed to identify key target genes and pathways. Using haematoxylin and eosin staining and western blotting, we validated how XFDZT controls water expression in the body to treat IBS-D infection.RESULTSFirst, the results showed that XFDZT contained 1037 active ingredients and 1458 corresponding targets. After intersecting the 252 IBS targets, 108 targets were identified. The main targets of XFDZT were albumin, aquaporins such as AQP1 and AQP3, calmodulin, and the cellular enzyme CYP2C9. GO and KEGG enrichment predicted that the action pathways were the neuroactive ligand-receptor interaction, calcium signalling pathway, serotonergic synapse signalling pathway, cGMP-PKG signalling pathway, cAMP signalling pathway, and MLCK-MLC signalling pathway. Second, an IBS-D rat model was constructed using colorectal dilation (CRD). CRD can significantly induce IBS-D symptoms such as diarrhoea, abdominal pain, and anxiety and depression-like behaviour in rats. XFDZT (10, 20, and 40 g/kg) administered for 14, 21, and 28 days significantly reversed these changes in IBS-D rats in a time- and dose-dependent manner, suggesting that XFDZT significantly improved IBS-D. Finally, the mechanism by which XFDZT improves IBS-D was explored from the perspective of AQPs, tight junction proteins, and motility-related proteins in colon tissue. Compared with the control group, the protein expression of AQP1, AQP3, and AQP8 in the colon tissue of IBS-D rats was significantly downregulated, whereas the protein expression of AQP7 was significantly upregulated. The expression of tight junction-related proteins claudin-1, occludin, and ZO-1 in colon tissue was significantly downregulated, whereas the expression of motility-related proteins p-MLC, MLC, MLCK, and CaM in colon tissue was significantly upregulated, suggesting that IBS-D rats had AQP disorders, epithelial intercellular connections, and motility in colon tissue. The above changes were significantly reversed by XFDZT administration (5, 10, and 20 g/kg) for 14 days.CONCLUSIONXFDZT significantly improved diarrhoea, abdominal pain, anxiety, and depression in IBS-D rats, and its mechanism of action may be related to the regulation of AQPs, tight junction proteins, and the MLCK-MLC pathway. This study provided a pharmacological experimental basis for the development of XFDZT as a novel drug for the treatment of IBS-D.

01 Jan 2025·Journal of Pharmaceutical and Biomedical Analysis

Study on the mechanism of Xinmailong injection against chronic heart failure based on transcriptomics and proteomics

Article

Author: Wu, Dingyu ; Jin, Lu ; Peng, Fang ; Lv, Changling ; Xue, Yanni ; Tan, Di

Xinmailong (XML), a traditional Chinese medicine derived from Periplaneta americana, is commonly used in China to treat chronic heart failure (CHF). However, its pharmacological mechanism remains unclear. In our research, we employed Doxorubicin (Dox) to create a CHF animal model and administered XML treatment to investigate the pharmacological effects of XML on CHF rats by combining transcriptomic and proteomic analyses. XML improved dox-induced CHF and improved cardiac function, and a joint multi-omics analysis demonstrated that it reduced cardiomyocyte fibrosis during CHF. There is further evidence that XML may alleviate cardiomyocyte fibrosis through its effects on the cGMP-PKG signaling pathway or by reducing the expression levels of COL1A1, COL3A1, MMP9, and CXCR2. In this study, the effects of XML on rats with CHF are examined at the transcriptional and protein levels, as well as its mechanism and mode of action in treating CHF. There may be novel therapeutic targets or clinical indications for XML-based CHF therapy resulting from the study's identification of significant differential genes and signaling pathways.

01 Jan 2025·Gene

Downregulation of glucose-energy metabolism via AMPK signaling pathway in granulosa cells of diminished ovarian reserve patients

Article

Author: He, Ruifen ; Li, Yi ; Liang, Xiaolei ; Qin, Xue ; Du, Junhong ; Ma, Hao ; Zhu, Qinying

Glucose metabolism plays a crucial role in the function of granulosa cells (GCs) and the development of follicles. In cases of diminished ovarian reserve (DOR), alterations in these processes can impact female fertility. This study aims to investigate changes in glucose-energy metabolism in GCs of young DOR patients aged 20 to 35 years and their correlation with the onset and progression of DOR. 72 DOR cases and 75 women with normal ovarian reserve (NOR) as controls were included based on the POSEIDON and Bologna criteria. Samples of GCs and follicular fluid (FF) were collected for a comprehensive analysis involving transcriptomics, metabolomics, RT-qPCR, JC-1 staining, and flow cytometry. The study identified differentially expressed genes and metabolites in GCs of DOR and NOR groups, revealing 7 common pathways related to glucose-energy metabolism, along with 11 downregulated genes and 14 metabolites. Key substances in the glucose-energy metabolism pathway, such as succinate, lactate, NADP, ATP, and ADP, showed decreased levels, with the DOR group exhibiting a reduced ADP/ATP ratio. Downregulation of genes involved in glycolysis (HK, PGK, LDH1), the TCA cycle (CS), and gluconeogenesis (PCK) was observed, along with reduced glucose content and expression of glucose transporter genes (GLUT1 and GLUT3) in DOR GCs. Additionally, decreased AMPK pathway activity and impaired mitochondrial function in DOR suggest a connection between mitochondrial dysfunction and disrupted energy metabolism. Above all, the decline in glucose-energy metabolism in DOR is closely associated with its onset and progression. Reduced glucose uptake and impaired mitochondrial function in DOR GCs lead to internal energy imbalances, hindering the AMPK signaling pathway, limiting energy production and supply, and ultimately impacting follicle development and maturation.

News (Medical) associated with PKG

10 Jun 2022

·www.prnewswire.com

LRA Announces Inaugural Awards Promoting Diversity in Lupus Research

NEW YORK, June 10, 2022 /PRNewswire/ -- The Lupus Research Alliance (LRA), the world's leading private funder of lupus research, today announced inaugural recipients of Career Development and Postdoctoral Awards to Promote Diversity in Lupus Research. The Diversity in Lupus Research Award funding mechanisms aim to address underrepresentation of minorities in the scientific research profession. Lupus is an autoimmune disease that disproportionally affects underrepresented minorities in both prevalence and disease severity. To encourage the development of talented underrepresented minority early-career scientists and postdoctoral fellows, the LRA launched two new award mechanisms. This year, three outstanding early-career underrepresented minority scientists will receive the Career Development Award to Promote Diversity in Lupus Research, which provides up to $600,000 over four years. The recipients are Ashira Blazer, MD, MSCI, Hospital for Special Surgery (HSS); Andrea Knight, MD, MSCE, The Hospital for Sick Children (SickKids); and Erika Moore, PhD, University of Florida. Two promising postdoctoral research fellows, Ruth Fernandez Ruiz, MD, from Hospital for Special Surgery and Vanessa Wacleche, PhD, from Brigham and Women's Hospital, are the recipients of the Postdoctoral Award to Promote Diversity in Lupus Research. This award provides fellows with $170,000 over two years to support projects and the generation of data needed to become an independent lupus researcher. Career Development Award to Promote Diversity in Lupus Research Recipients: Ashira Blazer, MD, MSCI, Hospital for Special Surgery Dr. Blazer will build upon her preliminary research, which successfully separated lupus nephritis patients from non-lupus nephritis patients through the analysis of the sediment found in the lupus patient urine. The potential clinical use of the non-invasive, urine-based test will be confirmed using a larger multi-national SLE patient group with African ancestry, which will provide a new opportunity to learn more about lupus nephritis in a high-risk and understudied patient group. Andrea Knight, MD, MSCE, The Hospital for Sick Children (SickKids) Dr. Knight is studying ways to detect brain changes in high-risk adolescent patients with childhood-onset lupus by comparing inflammation markers, brain MRIs, and cognitive function tests from healthy adolescents and lupus patients. Since little is known about which adolescents with lupus are most at risk for the structural brain changes that affect cognition, this research aims to find ways to detect these brain changes early and identify potential new treatments. Erika Moore, PhD, University of Florida Dr. Moore will look at monocytes from women of African and European ancestry, with and without lupus, to determine how monocytes promote lupus-related blood vessel inflammation (vasculitis). Understanding how lupus and ancestry affect monocyte functions will help the lupus medical community learn how ancestry influences lupus-related blood vessel inflammation and identify treatments for patients at higher risk of developing lupus-induced cardiovascular disease. Postdoctoral Award to Promote Diversity in Lupus Research Recipients: Ruth Fernandez Ruiz, MD, Hospital for Special Surgery Dr. Fernandez Ruiz will investigate how permanent changes in our genetic makeup, called gene variants, influence lupus development and progression. By studying how genetic variants in the PRKG1 gene affect lupus, the research team may identify new biological pathways that could be targeted to reduce the inflammation in lupus patients caused by high levels of interferon alpha. Vanessa Wacleche, PhD, Brigham and Women's Hospital Dr. Wacleche will study how T peripheral helper (Tph) cells misdirect the immune response seen in systemic lupus erythematosus via an inflammatory molecule CXCL13, which may lead to the production of organ-damaging autoantibodies. The new findings generated by this research could suggest strategies to control CXCL13 production that may eventually lead to the development of novel treatments for lupus patients. Teodora Staeva, PhD, LRA Chief Scientific Officer said, "We congratulate the inaugural recipients of our Diversity in Lupus Research Awards and look forward to seeing how their research findings advance our understanding of lupus and result in the development of new treatment options for lupus patients. The Career Development and Postdoctoral Awards to Promote Diversity in Lupus Research funding mechanisms are our most recent initiatives to alleviate the disparities that are prevalent in both autoimmune diseases and biomedical research." About Lupus Lupus is a chronic, complex autoimmune disease that affects millions of people worldwide. More than 90 percent of people with lupus are women; lupus most often strikes during the childbearing years of 15-45. Ancestrally African, South and Central American, and Native Americans have two to three times higher risk of developing lupus than Americans with European ancestry. In lupus, the immune system, which is designed to protect against infection, creates antibodies that can attack any part of the body including the kidneys, brain, heart, lungs, blood, skin, and joints. About the Lupus Research Alliance The Lupus Research Alliance is the largest non-governmental, non-profit funder of lupus research worldwide. The organization aims to transform treatment by funding the most innovative lupus research, fostering diverse scientific talent, and driving discovery toward better diagnostics, improved treatments and ultimately a cure for lupus. Because the Lupus Research Alliance's Board of Directors funds all administrative and fundraising costs, 100% of all donations goes to support lupus research programs. SOURCE Lupus Research Alliance

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