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Immunomodulation of Proton-activated G Protein-coupled Receptors in Inflammation
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作者 Min-shan LI Xiang-hong WANG Heng WANG 《Current Medical Science》 SCIE CAS 2024年第3期475-484,共10页
Proton-activated G protein-coupled receptors(GPCRs),initially discovered by Ludwig in 2003,are widely distributed in various tissues.These receptors have been found to modulate the immune system in several inflammator... Proton-activated G protein-coupled receptors(GPCRs),initially discovered by Ludwig in 2003,are widely distributed in various tissues.These receptors have been found to modulate the immune system in several inflammatory diseases,including inflammatory bowel disease,atopic dermatitis,and asthma.Proton-activated GPCRs belong to the G protein-coupled receptor family and can detect alternations in extracellular pH.This detection triggers downstream signaling pathways within the cells,ultimately influencing the function of immune cells.In this review,we specifically focused on investigating the immune response of proton-activated GPCRs under inflammatory conditions. 展开更多
关键词 proton-activated g protein-coupled receptors INFLAMMATION IMMUNOMODULATION DISEASE
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肝星状细胞特异性Grk2基因敲除小鼠模型的制备及鉴定
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作者 王语涵 许雅萍 +6 位作者 李南 陈婷婷 李玲 高萍萍 王华 魏伟 孙妩弋 《中国药理学通报》 CAS CSCD 北大核心 2024年第1期189-194,共6页
目的利用Cre-loxP基因敲除技术建立肝星状细胞特异性G蛋白偶联受体激酶2(G protein-coupled receptor kinase 2,GRK2)基因敲除小鼠模型,为研究GRK2在肝星状细胞中的生物学功能提供动物模型基础。方法将loxP标记的Grk2基因小鼠(Grk2^(fl/... 目的利用Cre-loxP基因敲除技术建立肝星状细胞特异性G蛋白偶联受体激酶2(G protein-coupled receptor kinase 2,GRK2)基因敲除小鼠模型,为研究GRK2在肝星状细胞中的生物学功能提供动物模型基础。方法将loxP标记的Grk2基因小鼠(Grk2^(fl/fl))和Lrat-Cre工具鼠进行多次繁殖,建立肝星状细胞特异性Grk2基因敲除(Grk2^(ΔHSC))小鼠模型。观察和分析小鼠的生长繁殖情况;通过PCR反应鉴定flox和Cre基因型;免疫荧光双染检测肝星状细胞中GRK2表达;Western blot检测小鼠肝星状细胞及肺、脾、肾脏、心脏组织中GRK2蛋白表达;HE染色观察肝脏及肺、脾、心脏、肾脏组织学形态。结果成功鉴定Grk2^(ΔHSC)小鼠基因型;两组小鼠体质量、繁殖能力无明显差异;免疫荧光双染及Western blot结果表明,Grk2^(ΔHSC)小鼠的肝星状细胞中GRK2蛋白水平明显低于对照组小鼠,Grk2^(ΔHSC)小鼠肺、脾、肾脏和心脏组织中GRK2蛋白表达与对照组相比无明显变化;HE染色结果显示,Grk2^(ΔHSC)小鼠肝脏及主要组织结构与Grk2^(fl/fl)相比差异无显著性,可用于后续研究。结论本研究应用Cre-loxP技术成功构建了肝星状细胞特异性Grk2基因敲除小鼠,为进一步研究GRK2在肝脏中的作用提供了优良工具。 展开更多
关键词 g蛋白偶联受体激酶2 Cre-loxP重组酶系统 细胞特异性敲除 肝星状细胞 基因鉴定 繁育
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Mogroside IIE,an in vivo metabolite of sweet agent,alleviates acute lung injury via Pla2g2a-EGFR inhibition
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作者 Weichao Lü Guoqing Ren +2 位作者 Kuniyoshi Shimizu Renshi Li Chaofeng Zhang 《Food Science and Human Wellness》 SCIE CSCD 2024年第1期299-312,共14页
In the face of increasingly serious environmental pollution,the health of human lung tissues is also facing serious threats.Mogroside IIE(M2E)is the main metabolite of sweetening agents mogrosides from the anti-tussiv... In the face of increasingly serious environmental pollution,the health of human lung tissues is also facing serious threats.Mogroside IIE(M2E)is the main metabolite of sweetening agents mogrosides from the anti-tussive Chinese herbal Siraitia grosvenori.The study elucidated the anti-inflammatory action and molecular mechanism of M2E against acute lung injury(ALI).A lipopolysaccharide(LPS)-induced ALI model was established in mice and MH-S cells were employed to explore the protective mechanism of M2E through the western blotting,co-immunoprecipitation,and quantitative real time-PCR analysis.The results indicated that M2E alleviated LPS-induced lung injury through restraining the activation of secreted phospholipase A2 type IIA(Pla2g2a)-epidermal growth factor receptor(EGFR).The interaction of Pla2g2a and EGFR was identified by co-immunoprecipitation.In addition,M2E protected ALI induced with LPS against inflammatory and damage which were significantly dependent upon the downregulation of AKT and m TOR via the inhibition of Pla2g2a-EGFR.Pla2g2a may represent a potential target for M2E in the improvement of LPS-induced lung injury,which may represent a promising strategy to treat ALI. 展开更多
关键词 Mogroside IIE Acute lung injury Secreted phospholipase A2 type IIA(Pla2g2a) Epidermal growth factor receptor(EgFR)
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Adrenal G protein-coupled receptor kinase-2 in regulation of sympathetic nervous system activity in heart failure 被引量:4
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作者 Katie A Mc Crink Ava Brill Anastasios Lymperopoulos 《World Journal of Cardiology》 CAS 2015年第9期539-543,共5页
Heart failure(HF), the number one cause of death in the western world, is caused by the insufficient performance of the heart leading to tissue underperfusion in response to an injury or insult. It comprises complex i... Heart failure(HF), the number one cause of death in the western world, is caused by the insufficient performance of the heart leading to tissue underperfusion in response to an injury or insult. It comprises complex interactions between important neurohormonal mechanisms that try but ultimately fail to sustain cardiac output. The most prominent such mechanism is the sympathetic(adrenergic) nervous system(SNS), whose activity and outflow are greatly elevated in HF. SNS hyperactivity confers significant toxicity to the failing heart and markedly increases HF morbidity and mortality via excessive activation of adrenergic receptors, which are G protein-coupled receptors. Thus, ligand binding induces their coupling to heterotrimeric G proteins that transduce intracellular signals. G protein signaling is turned-off by the agonist-bound receptor phosphorylation courtesy of G protein-coupled receptor kinases(GRKs), followed by βarrestin binding, which prevents the GRK-phosphorylated receptor from further interaction with the G proteins and simultaneously leads it inside the cell(receptor sequestration). Recent evidence indicates that adrenal GRK2 and βarrestins can regulate adrenal catecholamine secretion, thereby modulating SNS activity in HF. The present review gives an account of all these studies on adrenal GRKs and βarrestins in HF and discusses the exciting new therapeutic possibilities for chronic HF offered by targeting these proteins pharmacologically. 展开更多
关键词 g protein-coupled receptor g protein-coupled recep
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Therapeutic strategies targeting the epidermal growth factor receptor signaling pathway in metastatic colorectal cancer
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作者 Yi Zhou Shuang Wu Fan-Jie Qu 《World Journal of Gastrointestinal Oncology》 SCIE 2024年第6期2362-2379,共18页
More than 1.9 million new colorectal cancer(CRC)cases and 935000 deaths were estimated to occur worldwide in 2020,representing about one in ten cancer cases and deaths.Overall,colorectal ranks third in incidence,but s... More than 1.9 million new colorectal cancer(CRC)cases and 935000 deaths were estimated to occur worldwide in 2020,representing about one in ten cancer cases and deaths.Overall,colorectal ranks third in incidence,but second in mortality.More than half of the patients are in advanced stages at diagnosis.Treatment options are complex because of the heterogeneity of the patient population,including different molecular subtypes.Treatments have included conventional fluorouracil-based chemotherapy,targeted therapy,immunotherapy,etc.In recent years,with the development of genetic testing technology,more and more targeted drugs have been applied to the treatment of CRC,which has further prolonged the survival of metastatic CRC patients. 展开更多
关键词 Metastatic colorectal cancer Epidermal growth factor receptor B-type RAF mutation Kirsten rat sarcoma viral oncogene wild type Kirsten rat sarcoma viral oncogene g12C mutation Human epidermal growth factor receptor 2 overexpression/amplification
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Leucine-rich repeat-containing G protein-coupled receptor 5 marks different cancer stem cell compartments in human Caco-2 and LoVo colon cancer lines 被引量:4
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作者 Samah Abdulaali Alharbi Dmitry A Ovchinnikov Ernst Wolvetang 《World Journal of Gastroenterology》 SCIE CAS 2021年第15期1578-1594,共17页
BACKGROUND Colon cancer cell lines are widely used for research and for the screening of drugs that specifically target the stem cell compartment of colon cancers.It was reported that colon cancer carcinoma specimens ... BACKGROUND Colon cancer cell lines are widely used for research and for the screening of drugs that specifically target the stem cell compartment of colon cancers.It was reported that colon cancer carcinoma specimens contain a subset of leucine-rich repeatcontaining G protein-coupled receptor 5(LGR5)-expressing stem cells,these socalled“tumour-initiating”cells,reminiscent in their properties of the normal intestinal stem cells(ISCs),may explain the apparent heterogeneity of colon cancer cell lines.Also,colon cancer is initiated by aberrant Wnt signaling in ISCs known to express high levels of LGR5.Furthermore,in vivo reports demonstrate the clonal expansion of intestinal adenomas from a single LGR5-expressing cell.AIM To investigate whether colon cancer cell lines contain cancer stem cells and to characterize these putative cancer stem cells.METHODS A portable fluorescent reporter construct based on a conserved fragment of the LGR5 promoter was used to isolate the cell compartments expressing different levels of LGR5 in two widely used colon cancer cell lines(Caco-2 and LoVo).These cells were then characterized according to their proliferation capacity,gene expression signatures of ISC markers,and their tumorigenic properties in vivo and in vitro.RESULTS The data revealed that the LGR5 reporter can be used to identify and isolate a classical intestinal crypt stem cell-like population from the Caco-2,but not from the LoVo,cell lines,in which the cancer stem cell population is more akin to B lymphoma Moloney murine leukemia virus insertion region 1 homolog(+4 crypt)stem cells.This sub-population within Caco-2 cells exhibits an intestinal cancer stem cell gene expression signature and can both self-renew and generate differentiated LGR5 negative progeny.Our data also show that cells expressing high levels of LGR5/enhanced yellow fluorescent protein(EYFP)from this cell line exhibit tumorigenic-like properties in vivo and in vitro.In contrast,cell compartments of LoVo that are expressing high levels of LGR5/EYFP did not show these stem cell-like properties.Thus,cells that exhibit high levels of LGR5/EYFP expression represent the cancer stem cell compartment of Caco-2 colon cancer cells,but not LoVo cells.CONCLUSION Our findings highlight the presence of a spectrum of different ISC-like compartments in different colon cancer cell lines.Their existence is an important consideration for their screening applications and should be taken into account when interpreting drug screening data.We have generated a portable LGR5-reporter that serves as a valuable tool for the identification and isolation of different colon cancer stem cell populations in colon cancer lines. 展开更多
关键词 Colorectal cancer Colon cancer cell lines Intestinal stem cell Cancer stem cell Leucine-rich repeat-containing g protein-coupled receptor 5 Heterogenicity
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肺癌患者GASP-1、LCN2和TPX2的表达水平及其与TNM分期和预后的相关性分析
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作者 黄彦泽 文英娟 《海军医学杂志》 2024年第2期176-179,共4页
目的探究肺癌患者血清G蛋白偶联受体相关分选蛋白1(GASP-1)、脂质运载蛋白-2(LCN2)、Xklp2靶蛋白(TPX2)表达水平及其与TNM分期和预后的相关性。方法选取2019年4月至2022年5月在南部战区总医院接受诊疗的92例肺癌患者作为观察组,同期选... 目的探究肺癌患者血清G蛋白偶联受体相关分选蛋白1(GASP-1)、脂质运载蛋白-2(LCN2)、Xklp2靶蛋白(TPX2)表达水平及其与TNM分期和预后的相关性。方法选取2019年4月至2022年5月在南部战区总医院接受诊疗的92例肺癌患者作为观察组,同期选取92例健康体检者作为对照组。采集所有研究对象的外周静脉血样,检测血清GASP-1、LCN2、TPX2表达水平。将观察组按预后情况分为预后良好组和预后不佳组,比较2组患者血清GASP-1、LCN2、TPX2表达水平。分析肺癌患者血清GASP-1、LCN2、TPX2表达水平与TNM分期和预后的相关性。结果观察组血清GASP-1、LCN2、TPX2表达水平高于对照组(P<0.05);观察组TNM分期为Ⅲ、Ⅳ期的肺癌患者血清GASP-1、LCN2、TPX2表达水平高于TNM分期为Ⅰ、Ⅱ期的肺癌患者(P<0.05),TNM分期为Ⅳ期的患者血清GASP-1、LCN2、TPX2表达水平均高于TNM分期为Ⅲ期的患者(P<0.05)。预后良好组血清GASP-1、LCN2、TPX2水平均低于预后不佳组(P<0.05);观察组治疗前血清GASP-1、LCN2、TPX2表达水平均与TNM分期呈正相关(P<0.05),治疗后血清GASP-1、LCN2、TPX2表达水平均与预后呈负相关(P<0.05)。结论血清GASP-1、LCN2、TPX2表达水平与肺癌患者的TNM分期相关,在对症治疗后检测上述血清指标,可在一定程度上反映患者预后情况,为临床提供参考。 展开更多
关键词 肺癌 g蛋白偶联受体相关分选蛋白1 人脂质运载蛋白-2 Xklp2靶蛋白 TNM分期
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The Role of GPER in Sepsis-Induced Myocardial Cell Damage and 28-Day Mortality Risk
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作者 Jiangfeng Tang Jiangqin Liu 《Yangtze Medicine》 2024年第3期57-71,共15页
Purpose: The role of GPER in sepsis-induced myocardial cell injury and its potential impact on the risk of death within 28 days in sepsis. Methods: An in vitro experiment was conducted to establish a sepsis-induced my... Purpose: The role of GPER in sepsis-induced myocardial cell injury and its potential impact on the risk of death within 28 days in sepsis. Methods: An in vitro experiment was conducted to establish a sepsis-induced myocardial cell model. H9C2 myocardial cells were treated with 10 μg/ml lipopolysaccharide (LPS) for 24 hours. The effects of different concentrations of the GPER agonist G1 (1, 3, and 10 μmol/L) on cell viability, expression of inflammatory markers, cell apoptosis, and the NF-κB pathway were evaluated. A Mendelian randomization analysis was conducted using Single Nucleotide Polymorphism (SNPs) related to the GPER gene as instrumental variables to investigate the causal relationship between the GPER gene variations and sepsis (28-day death). Results: The results indicate that the group treated with LPS showed a significant decrease in myocardial cell viability, an increase in concentrations of tumor necrosis factor-alpha (TNF-α) and interleukin-6 (IL-6), higher apoptosis rates, and increased phosphorylation levels of NF-κB p65 (p-P65/P65) and IκB-α (p-IκB-α/IκB-α) compared to the control group (P κB pathway. However, genetic evidence did not show a causal relationship between GPER gene variations and sepsis (28-day death) (P κB pathway. However, genetic evidence did not show a causal relationship between GPER gene variations and sepsis (28-day death). 展开更多
关键词 g protein-coupled Estrogen receptor Sepsis-Induced Cardiomyopathy Inflammation and Apoptosis Sepsis (28-Day death) Mendelian Randomization
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Functionally diverse ligands modulate different activation states of the formyl peptide receptor 2,a G protein-coupled receptor
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作者 Shuo ZHANG Hao GONG Richard Dequan YE 《中国药理学与毒理学杂志》 CSCD 北大核心 2017年第10期981-982,共2页
OBJECTIVE To identify the mechanisms by which the formyl peptide receptor 2(FPR2)mediates both inflammatory and anti-inflammatory signaling in an agonist-dependent manner.METHODS Cells expressing FPR2 were incubated w... OBJECTIVE To identify the mechanisms by which the formyl peptide receptor 2(FPR2)mediates both inflammatory and anti-inflammatory signaling in an agonist-dependent manner.METHODS Cells expressing FPR2 were incubated with weak agonists,Aβ42 and Ac2-26,before stimulation with a strong agonist,WKYMVm.Calcium mobilization,c AMP inhibition and MAP kinase activation were measured.Intramolecular FRET were determined using FPR2 constructs with an ECFP attached to the C-terminus and a Fl As H binding motif embedded in the first or third intracellular loop(IL1 or IL3,respectively).RESULTS Aβ42 did not induce significant Ca^(2+) mobilization,but positively modulated WKYMVm-induced Ca^(2+) mobilization and c AMP reduction in a dose-variable manner within a narrow range of ligand concentrations.Treating FPR2-expressing cells with Ac2-26,a peptide with anti-inflammatory activity,negatively modulated WKYMVm-induced Ca^(2+) mobilization and c AMP reduction.Intramolecular FRET assay showed that stimulation of the receptor constructs with Aβ42 brought the C-terminal domain closer to IL1 but away from IL3.An opposite conformational change was induced by Ac2-26.The FPR2 conformation induced by Aβ42 corresponded to enhanced ERK phosphorylation and attenuated p38 MAPK phosphorylation,whereas Ac2-26 induced FPR2 conformational change corresponding to elevated p38 MAPK phosphorylation and reduced ERK phosphorylation.CONCLUSION Aβ42 and Ac2-26 induce different conformational changes in FPR2.These findings provide a structural basis for FPR2 mediation of inflammatory vs anti-inflammatory functions and identify a type of receptor modulation that differs from the classic positive and negative allosteric modulation. 展开更多
关键词 g protein-coupled receptors allosteric modulation fluorescent resonance energy transfer formyl peptide receptor 2 conformational changes
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G protein-coupled estrogen receptor in colon function, immune regulation and carcinogenesis 被引量:6
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作者 Damian Jacenik Ellen J Beswick +1 位作者 Wanda M Krajewska Eric R Prossnitz 《World Journal of Gastroenterology》 SCIE CAS 2019年第30期4092-4104,共13页
Estrogens play important roles in the development and progression of multiple tumor types.Accumulating evidence points to the significance of estrogen action not only in tumors of hormonally regulated tissues such as ... Estrogens play important roles in the development and progression of multiple tumor types.Accumulating evidence points to the significance of estrogen action not only in tumors of hormonally regulated tissues such as the breast,endometrium and ovary,but also in the development of colorectal cancer(CRC).The effects of estrogens in physiological and pathophysiological conditions are mediated by the nuclear estrogen receptorsαandβ,as well as the membranebound G protein-coupled estrogen receptor(GPER).The roles of GPER in CRC development and progression,however,remain poorly understood.Studies on the functions of GPER in the colon have shown that this estrogen receptor regulates colonic motility as well as immune responses in CRC-associated diseases,such as Crohn’s disease and ulcerative colitis.GPER is also involved in cell cycle regulation,endoplasmic reticulum stress,proliferation,apoptosis,vascularization,cell migration,and the regulation of fatty acid and estrogen metabolism in CRC cells.Thus,multiple lines of evidence suggest that GPER may play an important role in colorectal carcinogenesis.In this review,we present the current state of knowledge regarding the contribution of GPER to colon function and CRC. 展开更多
关键词 g protein-coupled ESTROgEN receptor Colorectal cancer Proliferation Migration COLONIC MOTILITY Inflammatory BOWEL disease
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Roles of G protein-coupled receptors in inflammatory bowel disease 被引量:7
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作者 Zhen Zeng Arjudeb Mukherjee +3 位作者 Adwin Pidiyath Varghese Xiao-Li Yang Sha Chen Hu Zhang 《World Journal of Gastroenterology》 SCIE CAS 2020年第12期1242-1261,共20页
Inflammatory bowel disease(IBD)is a complex disease with multiple pathogenic factors.Although the pathogenesis of IBD is still unclear,a current hypothesis suggests that genetic susceptibility,environmental factors,a ... Inflammatory bowel disease(IBD)is a complex disease with multiple pathogenic factors.Although the pathogenesis of IBD is still unclear,a current hypothesis suggests that genetic susceptibility,environmental factors,a dysfunctional immune system,the microbiome,and the interactions of these factors substantially contribute to the occurrence and development of IBD.Although existing and emerging drugs have been proven to be effective in treating IBD,none can cure IBD permanently.G protein-coupled receptors(GPCRs)are critical signaling molecules implicated in the immune response,cell proliferation,inflammation regulation and intestinal barrier maintenance.Breakthroughs in the understanding of the structures and functions of GPCRs have provided a driving force for exploring the roles of GPCRs in the pathogenesis of diseases,thereby leading to the development of GPCR-targeted medication.To date,a number of GPCRs have been shown to be associated with IBD,significantly advancing the drug discovery process for IBD.The associations between GPCRs and disease activity,disease severity,and disease phenotypes have also paved new avenues for the precise management of patients with IBD.In this review,we mainly focus on the roles of the most studied proton-sensing GPCRs,cannabinoid receptors,and estrogen-related GPCRs in the pathogenesis of IBD and their potential clinical values in IBD and some other diseases. 展开更多
关键词 g protein-coupled receptorS INFLAMMATORY BOWEL disease PATHOgENESIS Signaling pathway Drug discovery
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Takeda G protein-coupled receptor 5 modu⁃lates depression-like behaviors via hippocam⁃pal CA3 pyramidal neurons afferent to dorso⁃lateral septum 被引量:4
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作者 WANG Hao TAN Yuan-zhi +6 位作者 MU Rong-hao TANG Su-su LIU Xiao XING Shu-yun LONG Yan YUAN Dan-hua HONG Hao 《中国药理学与毒理学杂志》 CAS 北大核心 2021年第9期689-690,共2页
OBJECTIVE Takeda G protein-coupled receptor 5(TGR5)is recognized as a promising target for type 2 diabetes and metabolic syndrome;its expression has been demonstrat⁃ed in the brain and is thought to be neuroprotec⁃tiv... OBJECTIVE Takeda G protein-coupled receptor 5(TGR5)is recognized as a promising target for type 2 diabetes and metabolic syndrome;its expression has been demonstrat⁃ed in the brain and is thought to be neuroprotec⁃tive.Here,we hypothesize that dysfunction of central TGR5 may contribute to the pathogene⁃sis of depression.METHODS In well-established chronic social defeat stress(CSDS)and chronic restraint stress(CRS)models of depression,we investigated the functional roles of TGR5 in CA3 pyramidal neurons(PyNs)and underlying mech⁃anisms of the neuronal circuit in depression(for in vivo studies,n=10;for in vitro studies,n=5-10)using fiber photometry;optogenetic,chemoge⁃netic,pharmacological,and molecular profiling techniques;and behavioral tests.RESULTS Both CSDS and CRS most significantly reduced TGR5 expression of hippocampal CA3 PyNs.Genetic overexpression of TGR5 in CA3 PyNs or intra-CA3 infusion of INT-777,a specific agonist,protected against CSDS and CRS,exerting sig⁃nificant antidepressant-like effects that were mediated via CA3 PyN activation.Conversely,genetic knockout or TGR5 knockdown in CA3 facilitated stress-induced depression-like behav⁃iors.Re-expression of TGR5 in CA3 PyNs rather than infusion of INT-777 significantly improved depression-like behaviors in Tgr5 knockout mice exposed to CSDS or CRS.Silencing and stimula⁃tion of CA3 PyNs→somatostatin-GABAergic(gamma-aminobutyric acidergic)neurons of the dorsolateral septum circuit bidirectionally regulat⁃ed depression-like behaviors,and blockade of this circuit abrogated the antidepressant-like effects from TGR5 activation of CA3 PyNs.CON⁃CLUSION TGR5 can regulate depression via CA3 PyNs→somatostatin-GABAergic neurons of dorsolateral septum transmission,suggesting that TGR5 could be a novel target for developing antidepressants. 展开更多
关键词 DEPRESSION dorsolateral septum gABAergic neuron HIPPOCAMPUS pyramidal neuron takeda g protein-coupled receptor 5
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G protein-coupled receptors as potential targets for nonalcoholic fatty liver disease treatment 被引量:3
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作者 Ming Yang Chun-Ye Zhang 《World Journal of Gastroenterology》 SCIE CAS 2021年第8期677-691,共15页
Nonalcoholic fatty liver disease(NAFLD)is a broad-spectrum disease,ranging from simple hepatic steatosis to nonalcoholic steatohepatitis,which can progress to cirrhosis and liver cancer.Abnormal hepatic lipid accumula... Nonalcoholic fatty liver disease(NAFLD)is a broad-spectrum disease,ranging from simple hepatic steatosis to nonalcoholic steatohepatitis,which can progress to cirrhosis and liver cancer.Abnormal hepatic lipid accumulation is the major manifestation of this disease,and lipotoxicity promotes NAFLD progression.In addition,intermediate metabolites such as succinate can stimulate the activation of hepatic stellate cells to produce extracellular matrix proteins,resulting in progression of NAFLD to fibrosis and even cirrhosis.G protein-coupled receptors(GPCRs)have been shown to play essential roles in metabolic disorders,such as NAFLD and obesity,through their function as receptors for bile acids and free fatty acids.In addition,GPCRs link gut microbiota-mediated connections in a variety of diseases,such as intestinal diseases,hepatic steatosis,diabetes,and cardiovascular diseases.The latest findings show that gut microbiota-derived acetate contributes to liver lipogenesis by converting dietary fructose into hepatic acetyl-CoA and fatty acids.GPCR agonists,including peptides and natural products like docosahexaenoic acid,have been applied to investigate their role in liver diseases.Therapies such as probiotics and GPCR agonists may be applied to modulate GPCR function to ameliorate liver metabolism syndrome.This review summarizes the current findings regarding the role of GPCRs in the development and progression of NAFLD and describes some preclinical and clinical studies of GPCR-mediated treatment.Overall,understanding GPCR-mediated signaling in liver disease may provide new therapeutic options for NAFLD. 展开更多
关键词 Nonalcoholic fatty liver disease g protein-coupled receptors METABOLISM Bile acids Short-chain fatty acids gut microbiota
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Desensitization of G-protein-coupled receptors induces vascular hypocontractility in response to norepinephrine in the mesenteric arteries of cirrhotic patients and rats 被引量:1
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作者 Wei Chen Jiang-Yong Sang +4 位作者 De-Jun Liu Jun Qin Yan-Miao Huo Jia Xu Zhi-Yong Wu 《Hepatobiliary & Pancreatic Diseases International》 SCIE CAS 2013年第3期295-304,共10页
BACKGROUND: The increased β-arrestin-2 and its combination with G-protein-coupled receptors (GPCRs) lead to GPCRs desensitization. The latter may be responsible for decreased contractile reactivity in the mesenteric ... BACKGROUND: The increased β-arrestin-2 and its combination with G-protein-coupled receptors (GPCRs) lead to GPCRs desensitization. The latter may be responsible for decreased contractile reactivity in the mesenteric arteries of cirrhotic patients and rats. The present study is to investigate the machinery changes of α-adrenergic receptors and G proteins and their roles in the contractility of mesenteric arteries of cirrhotic patients and animal models. METHODS: Patients with cirrhosis due to hepatitis B and cirrhotic rats induced by CCl 4 were studied. Mesenteric artery contractility in response to norepinephrine was determined by a vessel perfusion system. The contractile effect of G protein-coupled receptor kinase-2 (GRK-2) inhibitor on the mesenteric artery was evaluated. The protein expression of the α 1 adrenergic receptor, G proteins, β-arrestin-2, GRK-2 as well as the activity of Rho associated coiled-coil forming protein kinase-1 (ROCK-1) were measured by Western blot. In addition, the interaction of α 1 adrenergic receptor with β-arrestin-2 was assessed by co-immunoprecipitation. RESULTS: The portal vein pressure of cirrhotic patients and rats was significantly higher than that of controls. The doseresponse curve to norepinephrine in mesenteric arteriole was shifted to the right, and EC 50 was significantly increased in cirrhotic patients and rats. There were no significant differences in the expressions of the α 1 adrenergic receptor and G proteins in the cirrhotic group compared with the controls. However, the protein expressions of GRK-2 and β-arrestin-2 were significantly elevated in cirrhotic patients and rats compared with those of the controls. The interaction of the α 1 adrenergic receptor and β-arrestin-2 was significantly aggravated. This interaction was significantly reversed by GRK-2 inhibitor. Both the protein expression and activity of ROCK-1 were significantly decreased in the mesenteric artery in patients with cirrhosis compared with those of the controls, and this phenomenon was not shown in the cirrhotic rats. Norepinephrine significantly increased the activity of ROCK-1 in normal rats but not in cirrhotic ones. Norepinephrine significantly increased ROCK-1 activity in cirrhotic rats when GRK-2 inhibitor was used. CONCLUSIONS: β-arrestin-2 expression and its interaction with GPCRs are significantly upregulated in the mesenteric arteries in patients and rats with cirrhosis. These upregulations result in GPCR desensitization, G-protein dysfunction and ROCK inhibition. These may explain the decreased contractility of the mesenteric artery in response to vasoconstrictors. 展开更多
关键词 portal hypertension DESENSITIZATION g-protein-coupled receptors β-arrestin-2 Rho associated coiled-coil forming protein kinase
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黏附性G蛋白偶联受体F1在胰腺导管腺癌中的表达及其促进癌症进展的机制研究 被引量:1
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作者 陈溯源 木司塔巴·木台力甫 +1 位作者 李冬雪 张志刚 《上海交通大学学报(医学版)》 CAS CSCD 北大核心 2024年第1期23-34,共12页
目的·分析黏附性G蛋白偶联受体F1(adhesion G protein-coupled receptor F1,ADGRF1)在胰腺导管腺癌(pancreatic ductal adenocarcinoma,PDAC)发生及发展过程中的表达变化,探究ADGRF1对PDAC细胞增殖的影响以及促进PDAC进展的潜在分... 目的·分析黏附性G蛋白偶联受体F1(adhesion G protein-coupled receptor F1,ADGRF1)在胰腺导管腺癌(pancreatic ductal adenocarcinoma,PDAC)发生及发展过程中的表达变化,探究ADGRF1对PDAC细胞增殖的影响以及促进PDAC进展的潜在分子机制。方法·基于癌症基因组图谱(The Cancer Genome Atlas,TCGA)数据库和基因表达综合(Gene Expression Omnibus,GEO)数据库分析ADGRF1在正常胰腺组织及PDAC组织中的mRNA水平表达。利用实时荧光定量PCR(quantitative real-time PCR,qPCR)和蛋白质印迹法(Western blotting)检测ADGRF1在正常胰腺导管上皮细胞hTERT-HPNE及多种PDAC细胞中的表达情况。利用免疫组织化学染色(immunohistochemistry staining,IHC)检测PDAC患者的癌组织及癌旁组织中ADGRF1的表达差异。转染小干扰RNA(small interfering RNA,siRNA)敲低ADGRF1后,通过CCK8和平板克隆形成实验检测PDAC细胞AsPC-1、SW1990增殖能力的变化。构建稳定过表达ADGRF1的Patu8988细胞,通过CCK8实验检测过表达ADGRF1引起的PDAC细胞增殖变化。利用RNA测序(RNA-sequence,RNA-seq)、基因集富集分析(gene set enrichment analysis,GSEA)和免疫浸润分析预测与ADGRF1促进PDAC癌症进展相关的信号通路。结果·TCGA数据库和GEO数据库的分析结果显示ADGRF1 mRNA在PDAC组织中的表达高于正常胰腺组织(均P=0.000)。qPCR和Western blotting结果显示,与hTERT-HPNE细胞相比,多种PDAC细胞中ADGRF1的mRNA和蛋白水平均有所上调(均P<0.05)。IHC结果显示ADGRF1在PDAC患者癌组织中的表达也高于癌旁组织。此外,下调ADGRF1能够抑制PDAC细胞AsPC-1、SW1990的增殖能力;而过表达ADGRF1则促进Patu8988细胞的增殖能力(均P<0.05)。RNAseq、GSEA富集分析和免疫浸润的结果显示,ADGRF1的表达与干扰素α(interferon-α,IFN-α)、肿瘤坏死因子α(tumor necrosis factor-α,TNF-α)和核因子κB(nuclear factorκB,NF-κB)等信号通路有关。结论·ADGRF1在PDAC细胞和组织中高表达,促进PDAC细胞的增殖,其机制可能与多个免疫相关信号通路有关。 展开更多
关键词 胰腺导管腺癌 黏附性g蛋白偶联受体F1 免疫 促癌作用
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Overexpression of G protein-coupled receptor 31 as a poor prognosticator in human colorectal cancer
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作者 Yu-Ming Rong Xiao-Ming Huang +7 位作者 De-Jun Fan Xu-Tao Lin Feng Zhang Jian-Cong Hu Ying-Xin Tan Xi Chen Yi-Feng Zou Ping Lan 《World Journal of Gastroenterology》 SCIE CAS 2018年第41期4679-4690,共12页
AIM To investigate the expression of G protein-coupled receptor 31 (GPR31) and its clinical significance in human colorectal cancer (CRC).METHODS To determine the association between the GPR31 expression and the progn... AIM To investigate the expression of G protein-coupled receptor 31 (GPR31) and its clinical significance in human colorectal cancer (CRC).METHODS To determine the association between the GPR31 expression and the prognosis of patients, we obtained paraffin-embedded pathological specimens from 466 CRC patients who underwent initial resection. A total of 321 patients from the First Affiliated Hospital of Sun Yat-sen University from January 1996 to December 2008 were included as a training cohort, whereas 145 patients from the Sixth Affiliated Hospital of Sun Yat-sen University from January 2007 to November 2008 were included as a validation cohort. We examined GPR31 expression levels in CRC tissues from two independent cohorts via immunohistochemical staining. All patients were categorized into either a GPR31 low expression group or a GPR31 high expression group. The clinicopathological factors and the prognosis of patients in the GPR31 low expression group and GPR31 high expression group were compared.RESULTS We compared the clinicopathological factors and the prognosis of patients in the GPR31 low expression group and GPR31 high expression group. Significant differences were observed in the number of patients in pM classification between patients in the GPR31 low expression group and GPR31 high expression group (P = 0.007). The five-year survival and tumor-free survival rates of patients were 84.3% and 82.2% in the GPR31 low expression group, respectively, and both rates were 59.7% in the GPR31 high expression group (P < 0.05). Results of the Cox proportional hazard regression model revealed that GPR31 upregulation was associated with shorter overall survival and tumor-free survival of patients with CRC (P < 0.05). Multivariate analysis identified GPR31 expression in colorectal cancer as an independent predictive factor of CRC patient survival (P < 0.05).CONCLUSION High GPR31 expression levels were found to be correlated with pM classification of CRC and to serve as an independent predictive factor of poor survival of CRC patients. 展开更多
关键词 g protein-coupled receptor 31 COLORECTAL cancer Predictive factor METASTASIS Clinical SIgNIFICANCE
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G protein-coupled receptor 37(GPR37) emerges as an important modulator of adenosinergic transmission in the striatum
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作者 Xavier Morato Rodrigo A. Cunha Francisco Ciruela 《Neural Regeneration Research》 SCIE CAS CSCD 2019年第11期1912-1914,共3页
G protein-coupled receptor 37 (GPR37), also known as parkin associated endothelin-like (Pael) receptor, is an orphan G protein- coupled receptor, which suffers a defective parking ubiquitination in autosomal recessive... G protein-coupled receptor 37 (GPR37), also known as parkin associated endothelin-like (Pael) receptor, is an orphan G protein- coupled receptor, which suffers a defective parking ubiquitination in autosomal recessive Parkinson’s disease promoting its endoplasmic reticulum aggregation and stress, neurotoxicity and neuronal death (Takahashi and Imai, 2003). Interestingly, we have demonstrated previously that GPR37 heteromerizes with adenosine A2A receptor (A2AR) in the striatum (Morato et al., 2017;Sokolina et al., 2017). 展开更多
关键词 g protein-coupled receptor 37(gPR37) important MODULATOR adenosinergic TRANSMISSION
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人工智能加速GPCR配体的发现 被引量:2
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作者 Wei Chen Chi Song +2 位作者 Liang Leng Sanyin Zhang Shilin Chen 《Engineering》 SCIE EI CAS CSCD 2024年第1期18-28,共11页
G protein-coupled receptors(GPCRs)are crucial players in various physiological processes,making them attractive candidates for drug discovery.However,traditional approaches to GPCR ligand discovery are time-consuming ... G protein-coupled receptors(GPCRs)are crucial players in various physiological processes,making them attractive candidates for drug discovery.However,traditional approaches to GPCR ligand discovery are time-consuming and resource-intensive.The emergence of artificial intelligence(AI)methods has revolutionized the field of GPCR ligand discovery and has provided valuable tools for accelerating the identification and optimization of GPCR ligands.In this study,we provide guidelines for effectively utilizing AI methods for GPCR ligand discovery,including data collation and representation,model selection,and specific applications.First,the online resources that are instrumental in GPCR ligand discovery were summarized,including databases and repositories that contain valuable GPCR-related information and ligand data.Next,GPCR and ligand representation schemes that can convert data into computer-readable formats were introduced.Subsequently,the key applications of AI methods in the different stages of GPCR drug discovery were discussed,ranging from GPCR function prediction to ligand design and agonist identification.Furthermore,an AI-driven multi-omics integration strategy for GPCR ligand discovery that combines information from various omics disciplines was proposed.Finally,the challenges and future directions of the application of AI in GPCR research were deliberated.In conclusion,continued advancements in AI techniques coupled with interdisciplina ry collaborations will offer great potential for improving the efficiency of GPCR ligand discovery. 展开更多
关键词 g protein-coupled receptor LIgAND Artificial intelligence Multi-omics Drug discovery
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Milk fat globule membrane supplementation protects againstβ-lactoglobul-ininduced food allergy in mice via upregulation of regulatory T cells and enhancement of intestinal barrier in a microbiota-derived short-chain fatty acids manner 被引量:1
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作者 Han Gong Tiange Li +3 位作者 Dong Liang Jingxin Gao Xiaohan Liu Xueying Mao 《Food Science and Human Wellness》 SCIE CSCD 2024年第1期124-136,共13页
Milk fat globule membrane(MFGM),which contains abundant glycoproteins and phospholipids,exerts beneficial effects on intestinal health and immunomodulation.The aim of this study was to evaluate the protective effects ... Milk fat globule membrane(MFGM),which contains abundant glycoproteins and phospholipids,exerts beneficial effects on intestinal health and immunomodulation.The aim of this study was to evaluate the protective effects and possible underlying mechanisms of MFGM on cow’s milk allergy(CMA)in aβ-lactoglobulin(BLG)-induced allergic mice model.MFGM was supplemented to allergic mice induced by BLG at a dose of 400 mg/kg body weight.Results demonstrated that MFGM alleviated food allergy symptoms,decreased serum levels of lipopolysaccharide,pro-inflammatory cytokines,immunoglobulin(Ig)E,Ig G1,and Th2 cytokines including interleukin(IL)-4,while increased serum levels of Th1 cytokines including interferon-γand regulatory T cells(Tregs)cytokines including IL-10 and transforming growth factor-β.MFGM modulated gut microbiota and enhanced intestinal barrier of BLG-allergic mice,as evidenced by decreased relative abundance of Desulfobacterota,Rikenellaceae,Lachnospiraceae,and Desulfovibrionaceae,while increased relative abundance of Bacteroidetes,Lactobacillaceae and Muribaculaceae,and enhanced expressions of tight junction proteins including Occludin,Claudin-1 and zonula occludens-1.Furthermore,MFGM increased fecal short-chain fatty acids(SCFAs)levels,which elevated G protein-coupled receptor(GPR)43 and GPR109A expressions.The increased expressions of GPR43 and GPR109A induced CD103+dendritic cells accumulation and promoted Tregs differentiation in mesenteric lymph node to a certain extent.In summary,MFGM alleviated CMA in a BLG-induced allergic mice model through enhancing intestinal barrier and promoting Tregs differentiation,which may be correlated with SCFAs-mediated activation of GPRs.These findings suggest that MFGM may be useful as a promising functional ingredient against CMA. 展开更多
关键词 Cow’s milk allergy Milk fat globule membrane gut microbiota Short-chain fatty acid g protein-coupled receptor Regulatory T cell
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人源GRK2的真核表达、纯化及活性检测 被引量:1
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作者 蒋励萍 陈露颖 +6 位作者 蒯佳婕 王凤玲 李浩 关艳玲 马旸 韩陈陈 魏伟 《安徽医科大学学报》 CAS 北大核心 2023年第2期179-184,共6页
目的构建人源G蛋白偶联受体激酶2(GRK2)真核表达系统。方法设计引物,以pIRES-EGFP-GRK2(全长)基因为模板,PCR扩增His-GRK2目的基因,将His-GRK2目的基因连接在pcDNA3.1-EGFP真核表达载体上;将pcDNA3.1-EGFP-His-GRK2质粒转染至HEK 293T细... 目的构建人源G蛋白偶联受体激酶2(GRK2)真核表达系统。方法设计引物,以pIRES-EGFP-GRK2(全长)基因为模板,PCR扩增His-GRK2目的基因,将His-GRK2目的基因连接在pcDNA3.1-EGFP真核表达载体上;将pcDNA3.1-EGFP-His-GRK2质粒转染至HEK 293T细胞,48 h后采用Western blot法检测GRK2蛋白表达,通过镍螯合的磁珠法纯化GRK2蛋白,考马斯亮蓝染色和Western blot法检测GRK2蛋白纯化,His pull down检测GRK2蛋白活性。结果双酶切和测序鉴定结果表明,pcDNA3.1-EGFP-His-GRK2真核表达质粒成功构建;Western blot法检测结果表明,GRK2蛋白的分子量约为80 ku,提示GRK2蛋白在HEK 293T细胞中成功表达(t=6.433,P=0.003);通过镍螯合的磁珠纯化得到GRK2蛋白,His pull down实验结果表明GRK2与前列腺素E2受体4亚型(EP4)结合,提示GRK2蛋白具有生物学活性(t=13.5,P=0.0002)。结论pcDNA3.1-EGFP-His-GRK2真核表达质粒的序列测序正确,成功构建GRK2重组质粒,GRK2重组质粒在真核细胞HEK 293T的细胞中成功表达且表达的蛋白具有生物学活性。 展开更多
关键词 g蛋白偶联受体激酶2 HEK 293T细胞 真核表达 蛋白纯化 活性鉴定
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