Your search keyword '"Jin-peng Sun"' showing total 183 results

1. Structural basis of ligand recognition and activation of the histamine receptor family

Author

Xuan Zhang, Guibing Liu, Ya-Ni Zhong, Ru Zhang, Chuan-Cheng Yang, Canyang Niu, Xuanyu Pu, Jingjing Sun, Tianyao Zhang, Lejin Yang, Chao Zhang, Xiu Li, Xinyuan Shen, Peng Xiao, Jin-Peng Sun, and Weimin Gong

Subjects

Science

Abstract

Abstract Histamine is a biogenic amine that is critical in various physiological and pathophysiological processes, including but not limited to allergic reactions, wakefulness, gastric acid secretion and neurotransmission. Here, we determine 9 cryo-electron microscopy (cryo-EM) structures of the 4 histamine receptors in complex with four different G protein subtypes, with endogenous or synthetic agonists bound. Inside the ligand pocket, we identify key motifs for the recognition of histamine, the distinct binding orientations of histamine and three subpockets that facilitate the design of specific ligands. In addition, we also identify key residues responsible for the selectivity of immethridine. Moreover, we reveal distinct structural features as determinants of Gq vs. Gs or Gs vs. Gi coupling differences among the histamine receptors. Our study provides a structural framework for understanding the ligand recognition and G protein coupling of all 4 histamine receptors, which may facilitate the rational design of ligands targeting these receptors.

Published

2024

2. Molecular Determinant Underlying Selective Coupling of Primary G‐Protein by Class A GPCRs

Author

Qingya Shen, Xinyan Tang, Xin Wen, Shizhuo Cheng, Peng Xiao, Shao‐Kun Zang, Dan‐Dan Shen, Lei Jiang, Yanrong Zheng, Huibing Zhang, Haomang Xu, Chunyou Mao, Min Zhang, Weiwei Hu, Jin‐Peng Sun, Yan Zhang, and Zhong Chen

Subjects

cryo‐EM structure, G protein selectivity, GPCR, H2R, H3R, machine learning, Science

Abstract

Abstract G‐protein‐coupled receptors (GPCRs) transmit downstream signals predominantly via G‐protein pathways. However, the conformational basis of selective coupling of primary G‐protein remains elusive. Histamine receptors H2R and H3R couple with Gs‐ or Gi‐proteins respectively. Here, three cryo‐EM structures of H2R‐Gs and H3R‐Gi complexes are presented at a global resolution of 2.6‐2.7 Å. These structures reveal the unique binding pose for endogenous histamine in H3R, wherein the amino group interacts with E2065.46 of H3R instead of the conserved D1143.32 of other aminergic receptors. Furthermore, comparative analysis of the H2R‐Gs and H3R‐Gi complexes reveals that the structural geometry of TM5/TM6 determines the primary G‐protein selectivity in histamine receptors. Machine learning (ML)‐based structuromic profiling and functional analysis of class A GPCR–G‐protein complexes illustrate that TM5 length, TM5 tilt, and TM6 outward movement are key determinants of the Gs and Gi/o selectivity among the whole Class A family. Collectively, the findings uncover the common structural geometry within class A GPCRs that determines the primary Gs‐ and Gi/o‐coupling selectivity.

Published

2024

3. Medicinal chemistry strategies towards the development of non-covalent SARS-CoV-2 Mpro inhibitors

Author

Letian Song, Shenghua Gao, Bing Ye, Mianling Yang, Yusen Cheng, Dongwei Kang, Fan Yi, Jin-Peng Sun, Luis Menéndez-Arias, Johan Neyts, Xinyong Liu, and Peng Zhan

Subjects

COVID-19, SARS-CoV-2, Main protease, Non-covalent inhibitors, Medicinal chemistry strategies, Therapeutics. Pharmacology, RM1-950

Abstract

The main protease (Mpro) of SARS-CoV-2 is an attractive target in anti-COVID-19 therapy for its high conservation and major role in the virus life cycle. The covalent Mpro inhibitor nirmatrelvir (in combination with ritonavir, a pharmacokinetic enhancer) and the non-covalent inhibitor ensitrelvir have shown efficacy in clinical trials and have been approved for therapeutic use. Effective antiviral drugs are needed to fight the pandemic, while non-covalent Mpro inhibitors could be promising alternatives due to their high selectivity and favorable druggability. Numerous non-covalent Mpro inhibitors with desirable properties have been developed based on available crystal structures of Mpro. In this article, we describe medicinal chemistry strategies applied for the discovery and optimization of non-covalent Mpro inhibitors, followed by a general overview and critical analysis of the available information. Prospective viewpoints and insights into current strategies for the development of non-covalent Mpro inhibitors are also discussed.

Published

2024

4. Structural basis for ligand recognition and activation of the prostanoid receptors

Author

Xiu Li, Xuan Zhang, Xin Wen, Daolai Zhang, Changxiu Qu, Xinyi Miao, Wenkai Zhang, Ru Zhang, Guibing Liu, Peng Xiao, Jin-Peng Sun, and Weimin Gong

Subjects

CP: Molecular biology, Biology (General), QH301-705.5

Abstract

Summary: Prostaglandin F2α (PGF2α) and thromboxane A2 (TXA2) are endogenous arachidonic acid metabolites, modulating diverse physiological processes including inflammation and cardiovascular homeostasis through activating PGF2α receptor (FP) and TXA2 receptor (TP). Ligands targeting FP and TP have demonstrated efficacy in treating conditions like glaucoma and cardiovascular diseases in humans, as well as reproductive-related diseases in animals. Here, we present five cryoelectron microscopy structures illustrating FP and TP in complex with Gq and bound to PGF2α (endogenous ligand), latanoprost acid (a clinical drug), and two other synthetic agonists. Combined with mutational and functional studies, these structures reveal not only structural features for the specific recognition of endogenous ligands and attainment of receptor selectivity of FP and TP but also the common mechanisms of receptor activation and Gq protein coupling. The findings may enrich our knowledge of ligand recognition and signal transduction of the prostanoid receptor family and facilitate rational ligand design toward these two receptors.

Published

2024

5. Ligand recognition and G protein coupling of the human itch receptor MRGPRX1

Author

Lulu Guo, Yumu Zhang, Guoxing Fang, Lu Tie, Yuming Zhuang, Chenyang Xue, Qi Liu, Minghui Zhang, Kongkai Zhu, Chongzhao You, Peiyu Xu, Qingning Yuan, Chao Zhang, Lei Liu, Naikang Rong, Shengxuan Peng, Yuan Liu, Chuanzheng Wang, Xin Luo, Zongyao Lv, Dongwei Kang, Xiao Yu, Cheng Zhang, Yi Jiang, Xinzhong Dong, Jiuyao Zhou, Zhongmin Liu, Fan Yang, H. Eric Xu, and Jin-Peng Sun

Subjects

Science

Abstract

Abstract MRGPRX1, a Mas-related GPCR (MRGPR), is a key receptor for itch perception and targeting MRGPRX1 may have potential to treat both chronic itch and pain. Here we report cryo-EM structures of the MRGPRX1-Gi1 and MRGPRX1-Gq trimers in complex with two peptide ligands, BAM8-22 and CNF-Tx2. These structures reveal a shallow orthosteric pocket and its conformational plasticity for sensing multiple different peptidic itch allergens. Distinct from MRGPRX2, MRGPRX1 contains a unique pocket feature at the extracellular ends of TM3 and TM4 to accommodate the peptide C-terminal “RF/RY” motif, which could serve as key mechanisms for peptidic allergen recognition. Below the ligand binding pocket, the G6.48XP6.50F6.51G6.52X(2)F/W6.55 motif is essential for the inward tilting of the upper end of TM6 to induce receptor activation. Moreover, structural features inside the ligand pocket and on the cytoplasmic side of MRGPRX1 are identified as key elements for both Gi and Gq signaling. Collectively, our studies provide structural insights into understanding itch sensation, MRGPRX1 activation, and downstream G protein signaling.

Published

2023

6. Temporal and spatial assembly of inner ear hair cell ankle link condensate through phase separation

Author

Huang Wang, Haibo Du, Rui Ren, Tingting Du, Lin Lin, Zhe Feng, Dange Zhao, Xiaoxi Wei, Xiaoyan Zhai, Hongyang Wang, Tingting Dong, Jin-Peng Sun, Hao Wu, Zhigang Xu, and Qing Lu

Subjects

Science

Abstract

In this work, the authors demonstrate that LLPS of the quaternary USH2 protein complex initiates the formation of stereociliary ankle link condensates, providing insights into the pathogenesis of deafness.

Published

2023

7. Deafness‐Associated ADGRV1 Mutation Impairs USH2A Stability through Improper Phosphorylation of WHRN and WDSUB1 Recruitment

Author

Ying Guan, Hai‐Bo Du, Zhao Yang, Yu‐Zhu Wang, Rui Ren, Wen‐Wen Liu, Chao Zhang, Jia‐Hai Zhang, Wen‐Tao An, Na‐Na Li, Xiao‐Xue Zeng, Jie Li, Yi‐Xiao Sun, Yan‐Fei Wang, Fan Yang, Jun Yang, Wei Xiong, Xiao Yu, Ren‐Jie Chai, Xiao‐Ming Tu, Jin‐Peng Sun, and Zhi‐Gang Xu

Subjects

adhesion G protein‐coupled receptor V subfamily member 1, ankle link complex, deafness, phosphorylation, ubiquitination, Science

Abstract

Abstract The ankle‐link complex (ALC) consists of USH2A, WHRN, PDZD7, and ADGRV1 and plays an important role in hair cell development. At present, its architectural organization and signaling role remain unclear. By establishing Adgrv1 Y6236fsX1 mutant mice as a model of the deafness‐associated human Y6244fsX1 mutation, the authors show here that the Y6236fsX1 mutation disrupts the interaction between adhesion G protein‐coupled receptor V subfamily member 1 (ADGRV1) and other ALC components, resulting in stereocilia disorganization and mechanoelectrical transduction (MET) deficits. Importantly, ADGRV1 inhibits WHRN phosphorylation through regional cAMP‐PKA signaling, which in turn regulates the ubiquitination and stability of USH2A via local signaling compartmentalization, whereas ADGRV1 Y6236fsX1 does not. Yeast two‐hybrid screening identified the E3 ligase WDSUB1 that binds to WHRN and regulates the ubiquitination of USH2A in a WHRN phosphorylation‐dependent manner. Further FlAsH‐BRET assay, NMR spectrometry, and mutagenesis analysis provided insights into the architectural organization of ALC and interaction motifs at single‐residue resolution. In conclusion, the present data suggest that ALC organization and accompanying local signal transduction play important roles in regulating the stability of the ALC.

Published

2023

8. Expression of fatty acid related gene promotes astaxanthin heterologous production in Chlamydomonas reinhardtii

Author

Jin-peng Sun, Xue-hong Wei, Xiao-mei Cong, Wen-hua Zhang, Le-Xin Qiu, and Xiao-nan Zang

Subjects

Haematococcus pluvialis, Chlamydomonas reinhardtii, astaxanthin, fatty acid, gene heterologous expression, metabolic engineering, Nutrition. Foods and food supply, TX341-641

Abstract

Natural astaxanthin is a high-value ketone carotenoid mainly derived from Haematococcus pluvialis, which is an excellent antioxidant for human consumption. To study the role of lipids in accumulation of astaxanthin, the H. pluvialis-derived astaxanthin synthesis pathway genes (β-carotene ketolase gene, BKT and β-carotene hydroxylase gene, BCH) and fatty acid elongation gene (mitochondrial trans-2-enoyl-coa reductase gene, MECR) were heterologously co-expressed in C. reinhardtii. Zeaxanthin, the precursor of astaxanthin synthesis, was significantly increased after BKT and BCH were expressed. In contrast, the α-carotene that competes with astaxanthin synthesis for lycopene decreased significantly. This redistribution of carbon flow was conducive to the synthesis of astaxanthin. In addition, the transformant only expressed astaxanthin metabolism related genes (BKT, BCH) would lead to an increase in total lipid, a decrease in monounsaturated fatty acids and an increase in polyunsaturated fatty acids. On this basis, the expression of MECR gene further increased the total lipid, and the relative content of different fatty acids also changed. The astaxanthin content of algal strains transformed with BKT and BCH genes was nearly 50% higher than that of the wild type. On this basis, the astaxanthin content of transformants expressing MECR gene related to long-chain fatty acid synthesis was increased by 227.5%. In this study, an astaxanthin production model similar to H. pluvialis by combining carotenoid metabolism and fatty acid metabolism was constructed in C. reinhardtii. The results suggest that the increase in astaxanthin is indeed linked to the regulation of fatty acid metabolism, and this link may involve the type of fatty acids and the dynamics of astaxanthin ester in cells. The strategy of promoting the synthesis of fatty acids has potential to achieve efficient production of astaxanthin in C. reinhardtii.

Published

2023

9. S-nitrosylation-mediated coupling of G-protein alpha-2 with CXCR5 induces Hippo/YAP-dependent diabetes-accelerated atherosclerosis

Author

Meng-Lin Chao, Shanshan Luo, Chao Zhang, Xuechun Zhou, Miao Zhou, Junyan Wang, Chuiyu Kong, Jiyu Chen, Zhe Lin, Xin Tang, Shixiu Sun, Xinlong Tang, Hongshan Chen, Hong Wang, Dongjin Wang, Jin-Peng Sun, Yi Han, Liping Xie, and Yong Ji

Subjects

Science

Abstract

S-nitrosylation can influence many pathophysiological processes. Here the authors show that the coupling efficiency of GNAI2 with CXCR5 is enhanced by S-nitrosylation of GNAI2, leading to Hippo-YAP dysfunction in endothelium, and plays a role in diabetes-accelerated atherosclerosis.

Published

2021

10. Structural studies of phosphorylation-dependent interactions between the V2R receptor and arrestin-2

Author

Qing-Tao He, Peng Xiao, Shen-Ming Huang, Ying-Li Jia, Zhong-Liang Zhu, Jing-Yu Lin, Fan Yang, Xiao-Na Tao, Ru-Jia Zhao, Feng-Yuan Gao, Xiao-Gang Niu, Kun-Hong Xiao, Jiangyun Wang, Changwen Jin, Jin-Peng Sun, and Xiao Yu

Subjects

Science

Abstract

The interaction between a GPCR, such as the vasopressin receptor-2 (V2R), and arrestin depends on the receptors’ phosphorylation pattern. Here authors use FRET and NMR to analyze the phosphorylation patterns of the V2R-arrestin complex and show that phospho-interactions are the key determinants of selective arrestin conformational states and correlated functions.

Published

2021

11. DeSiphering receptor core-induced and ligand-dependent conformational changes in arrestin via genetic encoded trimethylsilyl 1H-NMR probe

Author

Qi Liu, Qing-tao He, Xiaoxuan Lyu, Fan Yang, Zhong-liang Zhu, Peng Xiao, Zhao Yang, Feng Zhang, Zhao-ya Yang, Xiao-yan Wang, Peng Sun, Qian-wen Wang, Chang-xiu Qu, Zheng Gong, Jing-yu Lin, Zhen Xu, Shao-le Song, Shen-ming Huang, Sheng-chao Guo, Ming-jie Han, Kong-kai Zhu, Xin Chen, Alem W. Kahsai, Kun-Hong Xiao, Wei Kong, Fa-hui Li, Ke Ruan, Zi-jian Li, Xiao Yu, Xiao-gang Niu, Chang-wen Jin, Jiangyun Wang, and Jin-peng Sun

Subjects

Science

Abstract

Characterization of dynamic conformational changes in membrane protein complexes by NMR spectroscopy remains challenging. Here authors report the site-specific incorporation of 4-trimethylsilyl phenylalanine (TMSiPhe) into proteins, which enabled the characterization of multiple conformational states of a phospho-β2 adrenergic receptor/β-arrestin-1 complex in response to different receptor ligands.

Published

2020

12. Arctigenin Attenuates Ischemia/Reperfusion Induced Ventricular Arrhythmias by Decreasing Oxidative Stress in Rats

Author

Jing Yang, Hong-shan Yin, Ya-jing Cao, Zhi-an Jiang, Yong-jun Li, Mu-chun Song, Yong-fei Wang, Zhi-hua Wang, Rong Yang, Yun-fa Jiang, Jin-peng Sun, Bo-yi Liu, and Chuan Wang

Subjects

Arctigenin, Arrhythmias, Ischemia reperfusion, Oxidative stress, Nrf2 signaling, Physiology, QP1-981, Biochemistry, QD415-436

Abstract

Background/Aims: Arctigenin (ATG) has been shown to possess anti-inflammatory, immunemodulatory, anti-viral, anti-microbial, anti-carcinogenic, vasodilatory and anti-platelet aggregation properties. However, the protective role of ATG in prevention of arrhythmias induced by myocardial ischemia/reperfusion is unknown. The aim of this study was to investigate the anti-arrhythmia effect of ATG in an ischemia/reperfusion injured rat heart model and explore the related mechanisms. Methods: Rats were randomly exposed to sham operation, myocardial ischemia/ reperfusion (MI/R) alone, ATG+ MI/R, pretreated with ATG in low (12.5 mg/kg/day), medium (50 mg/kg/day) and high dose (200 mg/kg/day), respectively. Ventricular arrhythmias were assessed. The activity of superoxide dismutase (SOD), glutathione peroxidase (GSH-Px) and the level of malondialdehyde (MDA) in myocardial tissue were determined by chemical analysis. Results: Compared to MI/R, rats pretreated with ATG in doses of 50 mg/kg/day and 200 mg/kg/day showed significantly reduced incidence and duration of ventricular fibrillation, ventricular tachycardia and ventricular ectopic beat (VEB), and decreased the arrhythmia score during the 30-min ischemia. Incidence and duration of ventricular tachycardia, infarction size and arrhythmia scores in these groups were significantly decreased during the 120-min reperfusion. No ventricular fibrillation occurred during the period of reperfusion. Rats pretreated with ATG in doses of 50 mg/kg/day and 200 mg/kg/ day markedly enhanced the activities of antioxidant enzymes SOD and GSH-Px, reduced the level of MDA. No differences were observed between the group pretreated with a low dose of ATG and the sham group. Administration of ATG significantly increased the expression of antioxidant stress protein Nrf2, Trx1 and Nox1. Conclusion: Our data suggested that ATG plays anti-arrhythmia role in ischemia/reperfusion injury, which is probably associated with attenuating oxidative stress by Nrf2 signaling pathway.

Published

2018

13. A prediction model for lymph node metastases using pathologic features in patients intraoperatively diagnosed as stage I non-small cell lung cancer

Author

Fei Zhao, Yue Zhou, Peng-Fei Ge, Chen-Jun Huang, Yue Yu, Jun Li, Yun-Gang Sun, Yang-Chun Meng, Jian-Xia Xu, Ting Jiang, Zhi-Xuan Zhang, Jin-Peng Sun, and Wei Wang

Subjects

Non-small-cell lung cancer, Lymph node, Metastasis, Multivariable logistic model, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background There is little information on which pattern should be chosen to perform lymph node dissection for stage I non-small-cell lung cancer. This study aimed to develop a model for predicting lymph node metastasis using pathologic features of patients intraoperatively diagnosed as stage I non-small-cell lung cancer. Methods We collected pathology data from 284 patients intraoperatively diagnosed as stage I non-small-cell lung cancer who underwent lobectomy with complete lymph node dissection from 2013 through 2014, assessing various factors for an association with metastasis to lymph nodes (age, gender, pathology, tumour location, tumour differentiation, tumour size, pleural invasion, bronchus invasion, multicentric invasion and angiolymphatic invasion). After analysing these variables, we developed a multivariable logistic model to estimate risk of metastasis to lymph nodes. Results Univariate logistic regression identified tumour size >2.65 cm (p 2.65 cm (p 0.80, 0.43 2 cm and ŷ ≤0.43 plus tumour size ≤2 cm yielded positive lymph node metastasis predictive values of 44%, 18%, 14% and 0%, respectively. Conclusions A non-invasive prediction model including tumour size, tumour differentiation and bronchus invasion may be useful to give thoracic surgeons recommendations on lymph node dissection for patients intraoperatively diagnosed as Stage I non-small cell lung cancer.

Published

2017

14. Arrestin-biased AT1R agonism induces acute catecholamine secretion through TRPC3 coupling

Author

Chun-Hua Liu, Zheng Gong, Zong-Lai Liang, Zhi-Xin Liu, Fan Yang, Yu-Jing Sun, Ming-Liang Ma, Yi-Jing Wang, Chao-Ran Ji, Yu-Hong Wang, Mei-Jie Wang, Fu-Ai Cui, Amy Lin, Wen-Shuai Zheng, Dong-Fang He, Chang-xiu Qu, Peng Xiao, Chuan-Yong Liu, Alex R. B. Thomsen, Thomas Joseph Cahill, Alem W. Kahsai, Fan Yi, Kun-Hong Xiao, Tian Xue, Zhuan Zhou, Xiao Yu, and Jin-Peng Sun

Subjects

Science

Abstract

Angiotensin II type 1 receptor (AT1R)-mediated acute catecholamine release is modulated by β-arrestin. Here the authors show that β-arrestin-1 recruits the Ca2+channel TRPC3 and the PLCγ to the AT1R-β-arrestin complex, triggering G protein-independent calcium influx and catecholamine secretion.

Published

2017

15. Visualization of the parathyroid hormone receptor in long-active states

Author

Zhao Yang, Jun-Yan Wang, Xiao Yu, and Jin-Peng Sun

Subjects

Pharmacy and materia medica, RS1-441

Published

2019

16. Crystal Structure and Substrate Specificity of PTPN12

Author

Hui Li, Fan Yang, Chunhua Liu, Peng Xiao, Yunfei Xu, Zonglai Liang, Chuan Liu, Hongmei Wang, Wenjun Wang, Wenshuai Zheng, Wei Zhang, Xiaoyun Ma, Dongfang He, Xiaoyuan Song, Fuai Cui, Zhigang Xu, Fan Yi, Jin-Peng Sun, and Xiao Yu

Subjects

Biology (General), QH301-705.5

Abstract

PTPN12 is an important tumor suppressor that plays critical roles in various physiological processes. However, the molecular basis underlying the substrate specificity of PTPN12 remains uncertain. Here, enzymological and crystallographic studies have enabled us to identify two distinct structural features that are crucial determinants of PTPN12 substrate specificity: the pY+1 site binding pocket and specific basic charged residues along its surface loops. Key structurally plastic regions and specific residues in PTPN12 enabled recognition of different HER2 phosphorylation sites and regulated specific PTPN12 functions. In addition, the structure of PTPN12 revealed a CDK2 phosphorylation site in a specific PTPN12 loop. Taken together, our results not only provide the working mechanisms of PTPN12 for desphosphorylation of its substrates but will also help in designing specific inhibitors of PTPN12.

Published

2016

17. Gq activity- and β-arrestin-1 scaffolding-mediated ADGRG2/CFTR coupling are required for male fertility

Author

Dao-Lai Zhang, Yu-Jing Sun, Ming-Liang Ma, Yi-jing Wang, Hui Lin, Rui-Rui Li, Zong-Lai Liang, Yuan Gao, Zhao Yang, Dong-Fang He, Amy Lin, Hui Mo, Yu-Jing Lu, Meng-Jing Li, Wei Kong, Ka Young Chung, Fan Yi, Jian-Yuan Li, Ying-Ying Qin, Jingxin Li, Alex R B Thomsen, Alem W Kahsai, Zi-Jiang Chen, Zhi-Gang Xu, Mingyao Liu, Dali Li, Xiao Yu, and Jin-Peng Sun

Subjects

GPCR, arrestin, G protein, CFTR, ADGRG2, infertility, Medicine, Science, Biology (General), QH301-705.5

Abstract

Luminal fluid reabsorption plays a fundamental role in male fertility. We demonstrated that the ubiquitous GPCR signaling proteins Gq and β-arrestin-1 are essential for fluid reabsorption because they mediate coupling between an orphan receptor ADGRG2 (GPR64) and the ion channel CFTR. A reduction in protein level or deficiency of ADGRG2, Gq or β-arrestin-1 in a mouse model led to an imbalance in pH homeostasis in the efferent ductules due to decreased constitutive CFTR currents. Efferent ductule dysfunction was rescued by the specific activation of another GPCR, AGTR2. Further mechanistic analysis revealed that β-arrestin-1 acts as a scaffold for ADGRG2/CFTR complex formation in apical membranes, whereas specific residues of ADGRG2 confer coupling specificity for different G protein subtypes, this specificity is critical for male fertility. Therefore, manipulation of the signaling components of the ADGRG2-Gq/β-arrestin-1/CFTR complex by small molecules may be an effective therapeutic strategy for male infertility.

Published

2018

18. Biochemical and functional studies of lymphoid-specific tyrosine phosphatase (Lyp) variants S201F and R266W.

Author

Jing Liu, Ming Chen, Rong Li, Fan Yang, Xuanren Shi, Lichao Zhu, Hong-Mei Wang, Wei Yao, Qiji Liu, Fan-Guo Meng, Jin-Peng Sun, Qi Pang, and Xiao Yu

Subjects

Medicine, Science

Abstract

The Lymphoid specific tyrosine phosphatase (Lyp) has elicited tremendous research interest due to the high risk of its missense mutation R620W in a wide spectrum of autoimmune diseases. While initially characterized as a gain-of-function mutant, R620W was thought to lead to autoimmune diseases through loss-of-function in T cell signaling by a recent study. Here we investigate the biochemical characters and T cell signaling functions of two uncharacterized Lyp variants S201F and R266W, together with a previously characterized Lyp variant R263Q, which had reduced risk in several autoimmune diseases, including systemic lupus erythematosus (SLE), ulcerative colitis (UC) and rheumatoid arthritis (RA). Our kinetic and functional studies of R263Q polymorphism basically reproduced previous findings that it was a loss-of-function mutant. The other variant S201F reduced Lyp phosphatase activity moderately and decreased Lyp function in T cell slightly, while R266W severely impaired phosphatase activity and was a loss-of-function variant in T cell signaling. A combined kinetic and structure analysis suggests that the R266W variant may decrease its phosphatase activity through perturbing either the Q-loop or the WPD loop of Lyp. As both R266W and R263Q significantly change their phosphatase activity and T cell functions, future work could be considered to evaluate these mutants in a broader spectrum of autoimmune diseases.

Published

2012

19. Structural basis of amine odorant perception by a mammal olfactory receptor

Author

Lulu Guo, Jie Cheng, Shuo Lian, Qun Liu, Yan Lu, Yuan Zheng, Kongkai Zhu, Minghui Zhang, Yalei Kong, Chao Zhang, Naikang Rong, Yuming Zhuang, Guoxing Fang, Jingjing Jiang, Tianyao Zhang, Xiang Han, Zili Liu, Ming Xia, Shangming Liu, Lei Zhang, Stephen D. Liberles, Xiao Yu, Yunfei Xu, Fan Yang, Qian Li, and Jin-Peng Sun

Subjects

Multidisciplinary

Published

2023

20. Structures of the ADGRG2–Gs complex in apo and ligand-bound forms

Author

Hui Lin, Peng Xiao, Rui-Qian Bu, Shengchao Guo, Zhao Yang, Daopeng Yuan, Zhong-Liang Zhu, Chuan-Xin Zhang, Qing-Tao He, Chao Zhang, Yu-Qi Ping, Ru-Jia Zhao, Chuan-Shun Ma, Chang-Hao Liu, Xiao-Ning Zhang, Dan Jiang, Shaohui Huang, Yue-Tong Xi, Dao-Lai Zhang, Chen-Yang Xue, Bai-Sheng Yang, Jian-Yuan Li, Hao-Cheng Lin, Xu-Hui Zeng, Han Zhao, Wen-Ming Xu, Fan Yi, Zhongmin Liu, Jin-Peng Sun, and Xiao Yu

Subjects

Cell Biology, Molecular Biology

Published

2022

21. Structural basis for the tethered peptide activation of adhesion GPCRs

Author

Yu-Qi Ping, Peng Xiao, Fan Yang, Ru-Jia Zhao, Sheng-Chao Guo, Xu Yan, Xiang Wu, Chao Zhang, Yan Lu, Fenghui Zhao, Fulai Zhou, Yue-Tong Xi, Wanchao Yin, Feng-Zhen Liu, Dong-Fang He, Dao-Lai Zhang, Zhong-Liang Zhu, Yi Jiang, Lutao Du, Shi-Qing Feng, Torsten Schöneberg, Ines Liebscher, H. Eric Xu, and Jin-Peng Sun

Subjects

Multidisciplinary

Published

2022

22. Tethered peptide activation mechanism of the adhesion GPCRs ADGRG2 and ADGRG4

Author

Peng Xiao, Shengchao Guo, Xin Wen, Qing-Tao He, Hui Lin, Shen-Ming Huang, Lu Gou, Chao Zhang, Zhao Yang, Ya-Ni Zhong, Chuan-Cheng Yang, Yu Li, Zheng Gong, Xiao-Na Tao, Zhi-Shuai Yang, Yan Lu, Shao-Long Li, Jun-Yan He, Chuanxin Wang, Lei Zhang, Liangliang Kong, Jin-Peng Sun, and Xiao Yu

Subjects

Multidisciplinary, Protein Domains, Cryoelectron Microscopy, Humans, Peptides, Receptors, G-Protein-Coupled

Abstract

Adhesion G protein-coupled receptors (aGPCRs) constitute an evolutionarily ancient family of receptors that often undergo autoproteolysis to produce α and β subunits

Published

2022

23. A molecular mechanism of UDCA engagement with GPBAR and subsequent G protein interaction revealed by scattered alanine scanning

Author

Ruirui, Lu, Xu, Yan, Guoxing, Fang, Yuming, Zhuang, Lulu, Guo, Chao, Zhang, Xiang, Wu, Peng, Xiao, Yiwen, Cao, Fan, Yang, Xiao, Yu, Jin-Peng, Sun, and Jiu-Yao, Zhou

Subjects

Bile Acids and Salts, Molecular Docking Simulation, Alanine, GTP-Binding Proteins, Ursodeoxycholic Acid, Biophysics, Cell Biology, Molecular Biology, Biochemistry, Receptors, G-Protein-Coupled

Abstract

As the most known therapeutic component of bear bile acids, ursodeoxycholic acid (UDCA) is an FDA-approved drug for the treatment of primary biliary cirrhosis (PBC), the dissolution of cholesterol gallstones. UDCA produces many beneficial effects on metabolism and immune responses via its interaction with the membrane G protein-coupled bile acid receptor (GPBAR); however, how UDCA interacts with GPBAR and its selective cellular effects remain elusive. In this study, we delineated the interaction of UDCA with GPBAR and activation mechanism of GPBAR by scattered alanine scanning and molecular docking. Our results indicated that transmembrane helix 2 (TM2), TM3, TM5 and TM6 of GPBAR contribute to the interaction of UDCA in GPBAR binding pocket. Moreover, we predicted that the engagement of the 3-OH of UDCA with phenolic oxygen of Y240

Published

2022

24. Substance P promotes epidural fibrosis via induction of type 2 macrophages.

Author

Feng Hua, Hao-Ran Wang, Yun-Feng Bai, Jin-Peng Sun, Wei-Shun Wang, Ying Xu, Ming-Shun Zhang, and Jun Liu

Published

2023

25. Structural basis and molecular mechanism of biased GPBAR signaling in regulating NSCLC cell growth via YAP activity

Author

Lijuan Ma, Fan Yang, Xiang Wu, Chunyou Mao, Lulu Guo, Tianshu Miao, Shao-Kun Zang, Xiaoyu Jiang, Dan-Dan Shen, Tianhui Wei, Hengxing Zhou, Qin Wei, Shiyang Li, Qiang Shu, Shiqing Feng, Changtao Jiang, Bo Chu, Lutao Du, Jin-Peng Sun, Xiao Yu, Yan Zhang, and Pengju Zhang

Subjects

Bile Acids and Salts, Multidisciplinary, Lung Neoplasms, beta-Arrestin 1, Carcinoma, Non-Small-Cell Lung, Cryoelectron Microscopy, Humans, Cell Cycle Proteins, Cholic Acids, Receptors, G-Protein-Coupled, Transcription Factors

Abstract

The G protein–coupled bile acid receptor (GPBAR) is the membrane receptor for bile acids and a driving force of the liver–bile acid–microbiota–organ axis to regulate metabolism and other pathophysiological processes. Although GPBAR is an important therapeutic target for a spectrum of metabolic and neurodegenerative diseases, its activation has also been found to be linked to carcinogenesis, leading to potential side effects. Here, via functional screening, we found that two specific GPBAR agonists, R399 and INT-777, demonstrated strikingly different regulatory effects on the growth and apoptosis of non–small cell lung cancer (NSCLC) cells both in vitro and in vivo. Further mechanistic investigation showed that R399-induced GPBAR activation displayed an obvious bias for β-arrestin 1 signaling, thus promoting YAP signaling activation to stimulate cell proliferation. Conversely, INT-777 preferentially activated GPBAR-Gs signaling, thus inactivating YAP to inhibit cell proliferation and induce apoptosis. Phosphorylation of GPBAR by GRK2 at S310/S321/S323/S324 sites contributed to R399-induced GPBAR–β-arrestin 1 association. The cryoelectron microscopy (cryo-EM) structure of the R399-bound GPBAR-Gs complex enabled us to identify key interaction residues and pivotal conformational changes in GPBAR responsible for the arrestin signaling bias and cancer cell proliferation. In summary, we demonstrate that different agonists can regulate distinct functions of cell growth and apoptosis through biased GPBAR signaling and control of YAP activity in a NSCLC cell model. The delineated mechanism and structural basis may facilitate the rational design of GPBAR-targeting drugs with both metabolic and anticancer benefits.

Published

2023

26. Structure, function and pharmacology of human itch receptor complexes

Author

Zhongliang Zhu, Peng Xiao, Jin-Peng Sun, Zijian Li, Changxiu Qu, Lulu Guo, Lei Liu, Xu Yan, Xiao Yu, Yu Li, Fan Yang, Qun Liu, Guo-Xing Fang, Xu Chen, Yunfei Xu, Chao Zhang, Ning Gao, Guopeng Wang, Jia Wang, and Jiuyao Zhou

Subjects

Transmembrane domain, Multidisciplinary, Drug development, Chemistry, Structure function, Rational design, Trimer, Computational biology, Receptor, Ligand (biochemistry), Bony fish

Abstract

In the clades of animals that diverged from the bony fish, a group of Mas-related G-protein-coupled receptors (MRGPRs) evolved that have an active role in itch and allergic signals1,2. As an MRGPR, MRGPRX2 is known to sense basic secretagogues (agents that promote secretion) and is involved in itch signals and eliciting pseudoallergic reactions3–6. MRGPRX2 has been targeted by drug development efforts to prevent the side effects induced by certain drugs or to treat allergic diseases. Here we report a set of cryo-electron microscopy structures of the MRGPRX2–Gi1 trimer in complex with polycationic compound 48/80 or with inflammatory peptides. The structures of the MRGPRX2–Gi1 complex exhibited shallow, solvent-exposed ligand-binding pockets. We identified key common structural features of MRGPRX2 and describe a consensus motif for peptidic allergens. Beneath the ligand-binding pocket, the unusual kink formation at transmembrane domain 6 (TM6) and the replacement of the general toggle switch from Trp6.48 to Gly6.48 (superscript annotations as per Ballesteros–Weinstein nomenclature) suggest a distinct activation process. We characterized the interfaces of MRGPRX2 and the Gi trimer, and mapped the residues associated with key single-nucleotide polymorphisms on both the ligand and G-protein interfaces of MRGPRX2. Collectively, our results provide a structural basis for the sensing of cationic allergens by MRGPRX2, potentially facilitating the rational design of therapies to prevent unwanted pseudoallergic reactions. Cryo-electron microscopy structures of the MRGPRX2–Gi1 trimer in complex with polycationic compound 48/80 or inflammatory peptides provide insights into the sensing of cationic allergens by MRGPRX2, potentially facilitating the design of therapies to prevent unwanted pseudoallergic reactions.

Published

2021

27. Nidogen-2 Maintains the Contractile Phenotype of Vascular Smooth Muscle Cells and Prevents Neointima Formation via Bridging Jagged1-Notch3 Signaling

Author

Qinghua Cui, Jin-Peng Sun, Yiting Jia, Yi Fu, Nan Xie, Fang Yu, Guizhen Zhao, Wei Kong, Ma Zihan, Baihui Ma, Weihao Li, Yuan Zhou, and Chenfeng Mao

Subjects

Male, 0301 basic medicine, Neointima, Vascular smooth muscle, Bridging (networking), Vascular homeostasis, 030204 cardiovascular system & hematology, Muscle, Smooth, Vascular, Extracellular matrix, Mice, 03 medical and health sciences, 0302 clinical medicine, Physiology (medical), Animals, Humans, Medicine, Receptor, Notch3, Mice, Knockout, business.industry, Calcium-Binding Proteins, Contractile phenotype, Cell biology, Phenotype, 030104 developmental biology, cardiovascular system, Nidogen-2, Cardiology and Cardiovascular Medicine, business, Cell Adhesion Molecules, Jagged-1 Protein

Abstract

Background: How the extracellular matrix (ECM) microenvironment modulates the contractile phenotype of vascular smooth muscle cells (VSMCs) and confers vascular homeostasis remains elusive. Methods: To explore the key ECM proteins in the maintenance of the contractile phenotype of VSMCs, we applied protein-protein interaction network analysis to explore novel ECM proteins associated with the VSMC phenotype. By combining in vitro and in vivo genetic mice vascular injury models, we identified nidogen-2, a basement membrane glycoprotein, as a key ECM protein for maintenance of vascular smooth muscle cell identity. Results: We collected a VSMC phenotype–related gene dataset by using Gene Ontology annotation combined with a literature search. A computational analysis of protein-protein interactions between ECM protein genes and the genes from the VSMC phenotype–related gene dataset revealed the candidate gene nidogen-2, a basement membrane glycoprotein involved in regulation of the VSMC phenotype. Indeed, nidogen-2–deficient VSMCs exhibited loss of contractile phenotype in vitro, and compared with wild-type mice, nidogen-2 –/ – mice showed aggravated post–wire injury neointima formation of carotid arteries. Further bioinformatics analysis, coimmunoprecipitation assays, and luciferase assays revealed that nidogen-2 specifically interacted with Jagged1, a conventional Notch ligand. Nidogen-2 maintained the VSMC contractile phenotype via Jagged1-Notch3 signaling but not Notch1 or Notch2 signaling. Nidogen-2 enhanced Jagged1 and Notch3 interaction and subsequent Notch3 activation. Reciprocally, Jagged1 and Notch3 interaction, signaling activation, and Jagged1-triggered VSMC differentiation were significantly repressed in nidogen-2–deficient VSMCs. In accordance, the suppressive effect of Jagged1 overexpression on neointima formation was attenuated in nidogen-2 –/– mice compared with wild-type mice. Conclusions: Nidogen-2 maintains the contractile phenotype of VSMCs through Jagged1-Notch3 signaling in vitro and in vivo. Nidogen-2 is required for Jagged1-Notch3 signaling.

Published

2021

28. Loss-of-function missense variant of AKAP4 induced male infertility through reduced interaction with QRICH2 during sperm flagella development

Author

Lanlan Meng, Jin-Peng Sun, Jiao Cheng, Guangxiu Lu, Wenming Xu, Zhiliang Ji, Huan Zhang, Juan Du, Ge Lin, Yue-Qiu Tan, Mingwei Wang, Chaofeng Tu, Guohui Zhang, and Dongyan Li

Subjects

Male, A Kinase Anchor Proteins, Motility, Flagellum, Biology, Male infertility, Andrology, Mice, Capacitation, Genetics, medicine, Animals, Humans, Missense mutation, Molecular Biology, Infertility, Male, Genetics (clinical), Sperm fibrous sheath, General Medicine, medicine.disease, Spermatozoa, Sperm, Phenotype, Sperm Maturation, Flagella, Sperm Tail, Microtubule Proteins, Sperm Motility

Abstract

Sperm fibrous sheath (FS) is closely related to sperm maturation, capacitation and motility, and A-kinase anchor protein 4 (AKAP4) is the most abundant protein in sperm FS. Previous studies found incomplete sperm FSs and abnormal flagella in Akap4 knockout mice. Meanwhile, it was reported that the partial deletion in AKAP4 is highly relevant to the dysplasia of the FS in an infertile man, and so far, there is no report about male infertility caused by hemizygous AKAP4 variant. Furthermore, the specific mechanisms of how the variant is relevant to the phenotype remain elusive. In this study, we investigated three multiple morphological abnormalities of the sperm flagella-affected men from three independent families (including one consanguine family) carried hemizygous c.C1285T variant in AKAP4. The patients carried this variant, which showed dysplastic sperm FS, and the protein expression of AKAP4 was decreased in flagella, which was further confirmed in HEK-293T cells in vitro. In addition, the co-localization and interaction between AKAP4 and glutamine-rich protein 2 (QRICH2) on the molecular level were identified by immunofluorescence and co-immunoprecipitation (CO-IP). The hemizygous c.1285C > T variant in AKAP4 induced decreased protein expression of QRICH2 in spermatozoa. These results suggested that the normal expression of AKAP4 is required for maintaining the expression of QRICH2 and the decreased protein expression of AKAP4 and QRICH2，as well as the interaction between them induced by the hemizygous variant of AKAP4 caused dysplastic fibrous sheath, which eventually led to reduced sperm motility and male infertility.

Published

2021

29. Emerging roles of olfactory receptors in glucose metabolism

Author

Zhao Yang, Jie Cheng, Pan Shang, Jin-Peng Sun, and Xiao Yu

Subjects

Cell Biology

Abstract

Olfactory receptors (ORs) are widely expressed in extra-nasal tissues, where they participate in the regulation of divergent physiological processes. An increasing body of evidence over the past decade has revealed important regulatory roles for extra-nasal ORs in glucose metabolism. Recently, nonodorant endogenous ligands of ORs with metabolic significance have been identified, implying the therapeutic potential of ORs in the treatment of metabolic diseases, such as diabetes and obesity. In this review, we summarize current understanding of the expression patterns and functions of ORs in key tissues involved in glucose metabolism modulation, describe odorant and endogenous OR ligands, explain the biased signaling downstream of ORs, and outline OR therapeutic potential.

Published

2022

30. Single-molecule FRET and conformational analysis of beta-arrestin-1 through genetic code expansion and a Se-click reaction†

Author

Zhongliang Zhu, Xiaohong Liu, Mengyi Yang, Chunlai Chen, Yirong Yao, Chao Chen, Ming-Jie Han, Changxiu Qu, Dawei Zhang, Fan Yang, Qing-tao He, Yuchuan Wang, Jin-Peng Sun, Jiangyun Wang, Cheng Hu, Xuzhen Guo, and Kong-kai Zhu

Subjects

chemistry.chemical_classification, 0303 health sciences, Conformational change, Fluorophore, Calmodulin, biology, General Chemistry, Single-molecule FRET, 010402 general chemistry, 01 natural sciences, 0104 chemical sciences, Amino acid, 03 medical and health sciences, chemistry.chemical_compound, Chemistry, Förster resonance energy transfer, chemistry, Click chemistry, Biophysics, biology.protein, 030304 developmental biology, G protein-coupled receptor

Abstract

Single-molecule Förster resonance energy transfer (smFRET) is a powerful tool for investigating the dynamic properties of biomacromolecules. However, the success of protein smFRET relies on the precise and efficient labeling of two or more fluorophores on the protein of interest (POI), which has remained highly challenging, particularly for large membrane protein complexes. Here, we demonstrate the site-selective incorporation of a novel unnatural amino acid (2-amino-3-(4-hydroselenophenyl) propanoic acid, SeF) through genetic expansion followed by a Se-click reaction to conjugate the Bodipy593 fluorophore on calmodulin (CaM) and β-arrestin-1 (βarr1). Using this strategy, we monitored the subtle but functionally important conformational change of βarr1 upon activation by the G-protein coupled receptor (GPCR) through smFRET for the first time. Our new method has broad applications for the site-specific labeling and smFRET measurement of membrane protein complexes, and the elucidation of their dynamic properties such as transducer protein selection., A facile bioconjugation reaction for site-specific protein modification was developed for smFRET measurement, which detected the subtle but important conformational change of the β-arrestin/GPCR complex for the first time.

Published

2021

31. DCA-TGR5 signaling activation alleviates inflammatory response and improves cardiac function in myocardial infarction

Author

Xianjuan Lin, Jin-Peng Sun, Xiang Wu, Changtao Jiang, Wei Gao, Jianshu Zhang, Ming Xu, Fan Yang, Jiaxing Wang, Yan Zhang, and Yupeng Wang

Subjects

Male, 0301 basic medicine, Cardiac function curve, Cell signaling, medicine.drug_class, Anti-Inflammatory Agents, Myocardial Infarction, Myocardial Ischemia, Inflammation, 030204 cardiovascular system & hematology, Pharmacology, Receptors, G-Protein-Coupled, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Animals, Humans, Myocytes, Cardiac, Myocardial infarction, Molecular Biology, Bile acid, business.industry, Deoxycholic acid, Fibroblasts, Hypoxia (medical), medicine.disease, G protein-coupled bile acid receptor, Cell Hypoxia, Mice, Inbred C57BL, 030104 developmental biology, chemistry, medicine.symptom, Reactive Oxygen Species, Cardiology and Cardiovascular Medicine, business, Deoxycholic Acid, Signal Transduction

Abstract

Aims The progression of myocardial infarction (MI) involves multiple metabolic disorders. Bile acid metabolites have been increasingly recognized as pleiotropic signaling molecules that regulate multiple cardiovascular functions. G protein-coupled bile acid receptor (TGR5) is one of the receptors sensing bile acids to mediate their biological functions. In this study, we aimed to elucidate the effects of bile acids-TGR5 signaling pathways in myocardial infarction (MI). Methods and results Blood samples of AMI patients or control subjects were collected and plasma was used for bile acid metabolism analysis. We discovered that bile acid levels were altered and deoxycholic acid (DCA) was substantially reduced in the plasma of AMI patients. Mice underwent either the LAD ligation model of MI or sham operation. Both MI and sham mice were gavaged with 10 mg/kg/d DCA or vehicle control since 3-day before the operation. Cardiac function was assessed by ultrasound echocardiography, infarct area was evaluated by TTC staining and Masson trichrome staining. Administration of DCA improved cardiac function and reduced ischemic injury at the 7th-day post-MI. The effects of DCA were dependent on binding to its receptor TGR5. Tgr5−/− mice underwent the same MI model. Cardiac function deteriorated and infarct size was increased at the 7th-day post-MI, which were not savaged by DCA administration. Moreover, DCA inhibited interleukin (IL)-1β expression in the infarcted hearts, and ameliorated IL-1β activation at 1-day post-MI. DCA inhibited NF-κB signaling and further IL-1β expression in cultured neonatal mouse cardiomyocytes under hypoxia as well as cardio-fibroblasts with the treatment of LPS. Conclusions DCA-TGR5 signaling pathway activation decreases inflammation and ameliorates heart function post-infarction. Strategies that control bile acid metabolism and TGR5 signaling to ameliorate the inflammatory responses may provide beneficial effects in patients with myocardial infarction.

Published

2021

32. Cartilage oligomeric matrix protein is an endogenous β-arrestin-2-selective allosteric modulator of AT1 receptor counteracting vascular injury

Author

Tao Zhang, Zhiqing Li, Xin Jia, Guizhen Zhao, Heng Zhang, Chanjuan Xu, Pei Gao, Zhixin Liu, Ming-Liang Ma, Tuoyi Li, Junbao Du, Yi Fu, Shengchao Guo, Wengong Wang, Chenfeng Mao, Jingang Zheng, Jianfeng Liu, Zhao Yang, Wei Guo, Li Li, Qingbo Xu, Bo Liu, Meili Wang, Ziyi Liu, Wei Kong, Chaoshu Tang, Yiwei Zhou, Xian Wang, Jin-Peng Sun, Yaqian Huang, Yufei Chen, Yiting Jia, and Bing Yu

Subjects

Allosteric modulator, Allosteric regulation, Endogeny, Cartilage Oligomeric Matrix Protein, 030204 cardiovascular system & hematology, Receptor, Angiotensin, Type 1, Mice, 03 medical and health sciences, 0302 clinical medicine, Animals, Humans, Receptor, Molecular Biology, beta-Arrestins, 030304 developmental biology, G protein-coupled receptor, Cartilage oligomeric matrix protein, 0303 health sciences, Angiotensin II receptor type 1, biology, Cell Biology, Vascular System Injuries, beta-Arrestin 2, Research Highlight, Angiotensin II, Cell biology, HEK293 Cells, cardiovascular system, biology.protein, hormones, hormone substitutes, and hormone antagonists

Abstract

Compelling evidence has revealed that biased activation of G protein-coupled receptor (GPCR) signaling, including angiotensin II (AngII) receptor type 1 (AT1) signaling, plays pivotal roles in vascular homeostasis and injury, but whether a clinically relevant endogenous biased antagonism of AT1 signaling exists under physiological and pathophysiological conditions has not been clearly elucidated. Here, we show that an extracellular matrix protein, cartilage oligomeric matrix protein (COMP), acts as an endogenous allosteric biased modulator of the AT1 receptor and its deficiency is clinically associated with abdominal aortic aneurysm (AAA) development. COMP directly interacts with the extracellular N-terminus of the AT1 via its EGF domain and inhibits AT1-β-arrestin-2 signaling, but not Gq or Gi signaling, in a selective manner through allosteric regulation of AT1 intracellular conformational states. COMP deficiency results in activation of AT1a-β-arrestin-2 signaling and subsequent exclusive AAA formation in response to AngII infusion. AAAs in COMP–/– or ApoE–/– mice are rescued by AT1a or β-arrestin-2 deficiency, or the application of a peptidomimetic mimicking the AT1-binding motif of COMP. Explorations of the endogenous biased antagonism of AT1 receptor or other GPCRs may reveal novel therapeutic strategies for cardiovascular diseases.

Published

2021

33. Structures of the glucocorticoid-bound adhesion receptor GPR97–Go complex

Author

Qingya Shen, Xiaona Tao, Ya-Ni Zhong, Zijian Li, Xin Wen, Caiping Tian, Huibing Zhang, Jin-Peng Sun, Fan Yang, Fan Yi, H. Eric Xu, Xiao Yu, Yi Jiang, Peng Xiao, Guang-Yu Wang, Yan Zhang, Wen-Tao An, Shaolong Li, Changxiu Qu, Zhao Yang, Chunyou Mao, Ru-Jia Zhao, Yu-Qi Ping, Jing Yang, and Dan-Dan Shen

Subjects

0301 basic medicine, Multidisciplinary, G protein, Chemistry, Plasma protein binding, Ligand (biochemistry), 03 medical and health sciences, Transmembrane domain, 030104 developmental biology, 0302 clinical medicine, Palmitoylation, Biophysics, Binding site, Receptor, 030217 neurology & neurosurgery, G protein-coupled receptor

Abstract

Adhesion G-protein-coupled receptors (GPCRs) are a major family of GPCRs, but limited knowledge of their ligand regulation or structure is available1-3. Here we report that glucocorticoid stress hormones activate adhesion G-protein-coupled receptor G3 (ADGRG3; also known as GPR97)4-6, a prototypical adhesion GPCR. The cryo-electron microscopy structures of GPR97-Go complexes bound to the anti-inflammatory drug beclomethasone or the steroid hormone cortisol revealed that glucocorticoids bind to a pocket within the transmembrane domain. The steroidal core of glucocorticoids is packed against the 'toggle switch' residue W6.53, which senses the binding of a ligand and induces activation of the receptor. Active GPR97 uses a quaternary core and HLY motif to fasten the seven-transmembrane bundle and to mediate G protein coupling. The cytoplasmic side of GPR97 has an open cavity, where all three intracellular loops interact with the Go protein, contributing to the high basal activity of GRP97. Palmitoylation at the cytosolic tail of the Go protein was found to be essential for efficient engagement with GPR97 but is not observed in other solved GPCR complex structures. Our work provides a structural basis for ligand binding to the seven-transmembrane domain of an adhesion GPCR and subsequent G protein coupling.

Published

2021

34. Endogenous Lipid-GPR120 Signaling Modulates Pancreatic Islet Homeostasis to Different Extents

Author

Ya-Qin Du, Xue-Ying Sha, Jie Cheng, Jin Wang, Jing-Yu Lin, Wen-Tao An, Wei Pan, Li-Jun Zhang, Xiao-Na Tao, Yun-Fei Xu, Ying-Li Jia, Zhao Yang, Peng Xiao, Ming Liu, Jin-Peng Sun, and Xiao Yu

Subjects

Mice, Inbred C57BL, Islets of Langerhans, Mice, endocrine system, Endocrinology, Diabetes and Metabolism, Fatty Acids, Diabetes Mellitus, Internal Medicine, Animals, Homeostasis, Insulin, Ligands, Receptors, G-Protein-Coupled

Abstract

Long-chain fatty acids (LCFAs) not only are energy sources but also serve as signaling molecules. GPR120, an LCFA receptor, plays key roles in maintaining metabolic homeostasis. However, whether endogenous ligand-GPR120 circuits exist and how such circuits function in pancreatic islets are unclear. Here, we found that endogenous GPR120 activity in pancreatic δ cells modulated islet functions. At least two unsaturated LCFAs, oleic acid (OA) and linoleic acid (LA), were identified as GPR120 agonists within pancreatic islets. These two LCFAs promoted insulin secretion by inhibiting somatostatin secretion, and showed bias activation of GPR120 in a model system. Compared to OA, LA exerted higher potency in promoting insulin secretion, which is dependent on β-arrestin2 function. Moreover, GPR120 signaling was impaired in the diabetic db/db model, and replenishing OA and LA improved islet function in both the db/db- and STZ-treated diabetic models. Consistently, the administration of LA improved glucose metabolism in db/db mice. Collectively, our results reveal that endogenous LCFA-GPR120 circuits exist and modulate homeostasis in pancreatic islets. The contributions of phenotype differences caused by different LCFA-GPR120 circuits within islets highlight the roles of fine-tuned ligand–receptor signaling networks in maintaining islet homeostasis.

Published

2022

35. Progesterone activates GPR126 to promote breast cancer development via the Gi pathway

Author

Wentao An, Hui Lin, Lijuan Ma, Chao Zhang, Yuan Zheng, Qiuxia Cheng, Chuanshun Ma, Xiang Wu, Zihao Zhang, Yani Zhong, Menghui Wang, Dongfang He, Zhao Yang, Lutao Du, Shiqing Feng, Chuanxin Wang, Fan Yang, Peng Xiao, Pengju Zhang, Xiao Yu, and Jin-Peng Sun

Subjects

Multidisciplinary, 17-alpha-Hydroxyprogesterone, Cell Line, Tumor, Humans, Triple Negative Breast Neoplasms, Receptors, Progesterone, Progesterone, Receptors, G-Protein-Coupled, Signal Transduction

Abstract

GPR126 is a member of the adhesion G protein-coupled receptors (aGPCRs) that is essential for the normal development of diverse tissues, and its mutations are implicated in various pathological processes. Here, through screening 34 steroid hormones and their derivatives for cAMP production, we found that progesterone (P4) and 17-hydroxyprogesterone (17OHP) could specifically activate GPR126 and trigger its downstream Gi signaling by binding to the ligand pocket in the seven-transmembrane domain of the C-terminal fragment of GPR126. A detailed mutagenesis screening according to a computational simulated structure model indicated that K1001ECL2 and F1012ECL2 are key residues that specifically recognize 17OHP but not progesterone. Finally, functional analysis revealed that progesterone-triggered GPR126 activation promoted cell growth in vitro and tumorigenesis in vivo, which involved Gi-SRC pathways in a triple-negative breast cancer model. Collectively, our work identified a membrane receptor for progesterone/17OHP and delineated the mechanisms by which GPR126 participated in potential tumor progression in triple-negative breast cancer, which will enrich our understanding of the functions and working mechanisms of both the aGPCR member GPR126 and the steroid hormone progesterone.

Published

2022

36. Function and therapeutic potential of G protein‐coupled receptors in epididymis

Author

Yanfei Wang, Hui Jiang, Zhigang Xu, Yujing Sun, Xiao Yu, Wenming Xu, Hui Lin, Yingli Jia, Daolai Zhang, Mingwei Wang, and Jin-Peng Sun

Subjects

Male, 0301 basic medicine, Infertility, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Biology, Bioinformatics, Receptors, G-Protein-Coupled, Male infertility, 03 medical and health sciences, 0302 clinical medicine, GTP-Binding Proteins, medicine, Humans, Receptor, Review Articles, Infertility, Male, G protein-coupled receptor, Epididymis, Pharmacology, SUPERFAMILY, medicine.disease, Spermatozoa, 030104 developmental biology, medicine.anatomical_structure, Female, 030217 neurology & neurosurgery, Function (biology)

Abstract

Infertility rates for both females and males have increased continuously in recent years. Currently, effective treatments for male infertility with defined mechanisms or targets are still lacking. G protein‐coupled receptors (GPCRs) are the largest class of drug targets, but their functions and the implications for the therapeutic development for male infertility largely remain elusive. Nevertheless, recent studies have shown that several members of the GPCR superfamily play crucial roles in the maintenance of ion–water homeostasis of the epididymis, development of the efferent ductules, formation of the blood–epididymal barrier and maturation of sperm. Knowledge of the functions, genetic variations and working mechanisms of such GPCRs, along with the drugs and ligands relevant to their specific functions, provide future directions and a great arsenal for new developments in the treatment of male infertility.

Published

2020

37. Identification of HN252 as a potent inhibitor of protein phosphatase PPM1B

Author

Zhenyu Li, Baobing Zhao, Peng Xiao, Yuemao Shen, Zhiyuan Lu, Yuan Zhou, Jin-Peng Sun, and Xiao Yu

Subjects

0301 basic medicine, Models, Molecular, Immunoprecipitation, Phosphatase, Molecular Conformation, AKT1, substrate, Mass Spectrometry, PPM1B, Serine, 03 medical and health sciences, Structure-Activity Relationship, 0302 clinical medicine, Drug Discovery, Humans, Threonine, Enzyme Inhibitors, Phosphorylation, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Cyclin-dependent kinase 2, protein phosphatase, Cell Biology, Original Articles, p‐terphenyl, Recombinant Proteins, inhibitor, Enzyme Activation, Protein Phosphatase 2C, 030104 developmental biology, Biochemistry, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Original Article, Protein Binding

Abstract

Protein phosphatase 1B (PPM1B), a member of metal‐dependent protein serine/threonine phosphatase family, is involved in the regulation of several signalling pathways. However, our understanding of its substrate interaction and physiological functions is still largely limited. There is no reported PPM1B inhibitor to date. In this study, we identified HN252, a p‐terphenyl derivative, as a potent PPM1B inhibitor (Ki = 0.52 ± 0.06 µM). HN252 binding to PPM1B displayed remarkable and specific inhibition of PPM1B in both in vitro and ex vivo. With the aid of this small molecular inhibitor, we identified 30 proteins’ serine/threonine phosphorylation as potential substrates of PPM1B, 5 of which were demonstrated by immunoprecipitation, including one known (CDK2) and 4 novel ones (AKT1, HSP90B, β‐catenin and BRCA1). Furthermore, GO and KEGG analysis of dramatically phosphorylated proteins by PPM1B inhibition indicated that PPM1B plays roles in the regulation of multiple cellular processes and signalling pathways, such as gene transcription, inflammatory regulation, ageing and tumorigenesis. Our work provides novel insights into further investigation of molecular mechanisms of PPM1B.

Published

2020

38. DeSiphering receptor core-induced and ligand-dependent conformational changes in arrestin via genetic encoded trimethylsilyl 1H-NMR probe

Author

Jing-Yu Lin, Changxiu Qu, Qi Liu, Changwen Jin, Peng Sun, Sheng-chao Guo, Xiaoyan Wang, Xiaogang Niu, Zhao Yang, Zhen Xu, Zijian Li, Peng Xiao, Kunhong Xiao, Zhongliang Zhu, Fahui Li, Qing-tao He, Xin Chen, Zheng Gong, Ke Ruan, Jiangyun Wang, Shao-le Song, Jin-Peng Sun, Kong-kai Zhu, Feng Zhang, Qian-wen Wang, Fan Yang, Zhao-ya Yang, Wei Kong, Xiao Yu, Xiao-xuan Lyu, Ming-Jie Han, Shen-Ming Huang, and Alem W. Kahsai

Subjects

0301 basic medicine, Science, General Physics and Astronomy, Plasma protein binding, 010402 general chemistry, 01 natural sciences, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Protein structure, Arrestin, Binding site, lcsh:Science, Multidisciplinary, biology, Chemistry, Active site, General Chemistry, Transmembrane protein, 0104 chemical sciences, 030104 developmental biology, Membrane protein, Biophysics, biology.protein, lcsh:Q, Signal transduction

Abstract

Characterization of the dynamic conformational changes in membrane protein signaling complexes by nuclear magnetic resonance (NMR) spectroscopy remains challenging. Here we report the site-specific incorporation of 4-trimethylsilyl phenylalanine (TMSiPhe) into proteins, through genetic code expansion. Crystallographic analysis revealed structural changes that reshaped the TMSiPhe-specific amino-acyl tRNA synthetase active site to selectively accommodate the trimethylsilyl (TMSi) group. The unique up-field 1H-NMR chemical shift and the highly efficient incorporation of TMSiPhe enabled the characterization of multiple conformational states of a phospho-β2 adrenergic receptor/β-arrestin-1(β-arr1) membrane protein signaling complex, using only 5 μM protein and 20 min of spectrum accumulation time. We further showed that extracellular ligands induced conformational changes located in the polar core or ERK interaction site of β-arr1 via direct receptor transmembrane core interactions. These observations provided direct delineation and key mechanism insights that multiple receptor ligands were able to induce distinct functionally relevant conformational changes of arrestin.

Published

2020

39. Structural basis of GPBAR activation and bile acid recognition

Author

Ruirui Lu, Jiuyao Zhou, Vincent C. Luca, Qianqian Ming, Qingya Shen, Kai Zhang, Linqi Zhang, Yan Zhang, Fan Yi, Shimeng Guo, Chunyou Mao, Fajun Nan, Chenlu Zhang, Fan Yang, Peng Xiao, Yuemao Shen, Shen-Ming Huang, Xin Xie, Xiaoying Liang, Changtao Jiang, Dan-Dan Shen, Jing-Yu Lin, Lulu Guo, Xiang Wu, Jin-Peng Sun, Xiao Yu, Yuqi Ping, and Cheng Ma

Subjects

0301 basic medicine, Multidisciplinary, Bile acid, Chemistry, G protein, medicine.drug_class, GTP-Binding Protein alpha Subunits, Allosteric regulation, Plasma protein binding, digestive system, G protein-coupled bile acid receptor, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Biochemistry, Amphiphile, medicine, Receptor, 030217 neurology & neurosurgery

Abstract

The G-protein-coupled bile acid receptor (GPBAR) conveys the cross-membrane signalling of a vast variety of bile acids and is a signalling hub in the liver–bile acid–microbiota–metabolism axis1–3. Here we report the cryo-electron microscopy structures of GPBAR–Gs complexes stabilized by either the high-affinity P3954 or the semisynthesized bile acid derivative INT-7771,3 at 3 A resolution. These structures revealed a large oval pocket that contains several polar groups positioned to accommodate the amphipathic cholic core of bile acids, a fingerprint of key residues to recognize diverse bile acids in the orthosteric site, a putative second bile acid-binding site with allosteric properties and structural features that contribute to bias properties. Moreover, GPBAR undertakes an atypical mode of activation and G protein coupling that features a different set of key residues connecting the ligand-binding pocket to the Gs-coupling site, and a specific interaction motif that is localized in intracellular loop 3. Overall, our study not only reveals unique structural features of GPBAR that are involved in bile acid recognition and allosteric effects, but also suggests the presence of distinct connecting mechanisms between the ligand-binding pocket and the G-protein-binding site in the G-protein-coupled receptor superfamily. Using cryo-electron microscopy, the authors report the structures of G-protein-coupled bile acid receptor–Gs complexes and reveal the structural basis of bile acid recognition.

Published

2020

40. Substance P promotes epidural fibrosis via induction of type 2 macrophages

Author

Jun Liu, Ming-Shun Zhang, Feng Hua, Hao-Ran Wang, Yun-Feng Bai, Jin-Peng Sun, Wei-Shun Wang, and Ying Xu

Subjects

Developmental Neuroscience

Published

2023

41. Activation of PTH1R alleviates epididymitis and orchitis through Gq and β-arrestin-1 pathways

Author

Zhao Yang, Shu-Hua Zhou, Ge-Lin Huang, Hui Jiang, Xiao Yu, Jian-Ning Sun, Mingwei Wang, Jin-Peng Sun, Haocheng Lin, Wenming Xu, and Xu Chen

Subjects

Lipopolysaccharides, Male, medicine.medical_specialty, Parathyroid hormone, Orchitis, Inflammation, Internal medicine, medicine, Animals, Receptor, Infertility, Male, Receptor, Parathyroid Hormone, Type 1, Epididymitis, Multidisciplinary, business.industry, Parathyroid hormone receptor, Biological Sciences, medicine.disease, Epididymis, Mice, Inbred C57BL, beta-Arrestin 1, Endocrinology, medicine.anatomical_structure, Mumps virus, GTP-Binding Protein alpha Subunits, Gq-G11, medicine.symptom, business, GNAQ

Abstract

Inflammation in the epididymis and testis contributes significantly to male infertility. Alternative therapeutic avenues treating epididymitis and orchitis are expected since current therapies using antibiotics have limitations associated to side effects and are commonly ineffective for inflammation due to nonbacterial causes. Here, we demonstrated that type 1 parathyroid hormone receptor (PTH1R) and its endogenous agonists, parathyroid hormone (PTH) and PTH-related protein (PTHrP), were mainly expressed in the Leydig cells of testis as well as epididymal epithelial cells. Screening the secretin family G protein–coupled receptor identified that PTH1R in the epididymis and testis was down-regulated in mumps virus (MuV)- or lipopolysaccharide (LPS)-induced inflammation. Remarkably, activation of PTH1R by abaloparatide (ABL), a Food and Drug Administration–approved treatment for postmenopausal osteoporosis, alleviated MuV- or LPS-induced inflammatory responses in both testis and epididymis and significantly improved sperm functions in both mouse model and human samples. The anti-inflammatory effects of ABL were shown to be regulated mainly through the Gq and β-arrestin-1 pathway downstream of PTH1R as supported by the application of ABL in Gnaq(±) and Arrb1(−/−) mouse models. Taken together, our results identified an important immunoregulatory role for PTH1R signaling in the epididymis and testis. Targeting to PTH1R might have a therapeutic effect for the treatment of epididymitis and orchitis or other inflammatory disease in the male reproductive system.

Published

2021

42. Scaffolding mechanism of arrestin-2 in the cRaf/MEK1/ERK signaling cascade

Author

Kiae Kim, Rui-Rui Li, Vsevolod V. Gurevich, Ka Young Chung, Fan Yang, Donghee Ham, Ji Young Park, Changxiu Qu, Min Woo Yun, Jin-Peng Sun, Tina M. Iverson, and Qing-Tao He

Subjects

MAPK/ERK pathway, genetic structures, Arrestins, MAP Kinase Signaling System, media_common.quotation_subject, MAP Kinase Kinase 1, Protein Serine-Threonine Kinases, environment and public health, Mass Spectrometry, Homologous desensitization, Chlorocebus aethiops, Arrestin, Fluorescence Resonance Energy Transfer, Animals, Humans, Phosphorylation, Internalization, Extracellular Signal-Regulated MAP Kinases, Nuclear Magnetic Resonance, Biomolecular, beta-Arrestins, media_common, Mitogen-Activated Protein Kinase Kinases, Multidisciplinary, MAP kinase kinase kinase, Kinase, Chemistry, Proteins, Biological Sciences, MAP Kinase Kinase Kinases, beta-Arrestin 2, eye diseases, Cell biology, Rats, beta-Arrestin 1, COS Cells, sense organs, Signal transduction, biological phenomena, cell phenomena, and immunity, Mitogen-Activated Protein Kinases, Protein Processing, Post-Translational, Protein Binding, Signal Transduction

Abstract

Arrestins were initially identified for their role in homologous desensitization and internalization of G protein-coupled receptors. Receptor-bound arrestins also initiate signaling by interacting with other signaling proteins. Arrestins scaffold MAPK signaling cascades, MAPK kinase kinase (MAP3K), MAPK kinase (MAP2K), and MAPK. In particular, arrestins facilitate ERK1/2 activation by scaffolding ERK1/2 (MAPK), MEK1 (MAP2K), and Raf (MAPK3). However, the structural mechanism underlying this scaffolding remains unknown. Here, we investigated the mechanism of arrestin-2 scaffolding of cRaf, MEK1, and ERK2 using hydrogen/deuterium exchange-mass spectrometry, tryptophan-induced bimane fluorescence quenching, and NMR. We found that basal and active arrestin-2 interacted with cRaf, while only active arrestin-2 interacted with MEK1 and ERK2. The ATP binding status of MEK1 or ERK2 affected arrestin-2 binding; ATP-bound MEK1 interacted with arrestin-2, whereas only empty ERK2 bound arrestin-2. Analysis of the binding interfaces suggested that the relative positions of cRaf, MEK1, and ERK2 on arrestin-2 likely facilitate sequential phosphorylation in the signal transduction cascade.

Published

2021

43. Structural insights into ligand recognition and activation of the melanocortin-4 receptor

Author

Antao Dai, Wenbo Feng, Yan Zhang, Dan-Dan Shen, Li-Nan Chen, Huibing Zhang, Jiao Qin, Daniel H. Scharf, Dehua Yang, Ming-Wei Wang, Chunyou Mao, Yan Zhou, Qingya Shen, Jin-Peng Sun, Shanshan Xie, Tianhua Zhou, and Tingjun Hou

Subjects

Agonist, Gs alpha subunit, medicine.drug_class, G protein, Biology, Ligands, Article, Glutamates, Heterotrimeric G protein, medicine, Humans, Myocytes, Cardiac, Amino Acid Sequence, Obesity, Heart Atria, Receptor, Molecular Biology, Cell Differentiation, Cell Biology, Ligand (biochemistry), Research Highlight, Cell biology, Melanocortin 4 receptor, THIQ, Receptor, Melanocortin, Type 4, medicine.drug

Abstract

Melanocortin-4 receptor (MC4R) plays a central role in the regulation of energy homeostasis. Its high sequence similarity to other MC receptor family members, low agonist selectivity and the lack of structural information concerning MC4R-specific activation have hampered the development of MC4R-seletive therapeutics to treat obesity. Here, we report four high-resolution structures of full-length MC4R in complex with the heterotrimeric G(s) protein stimulated by the endogenous peptide ligand α-MSH, FDA-approved drugs afamelanotide (Scenesse™) and bremelanotide (Vyleesi™), and a selective small-molecule ligand THIQ, respectively. Together with pharmacological studies, our results reveal the conserved binding mode of peptidic agonists, the distinctive molecular details of small-molecule agonist recognition underlying receptor subtype selectivity, and a distinct activation mechanism for MC4R, thereby offering new insights into G protein coupling. Our work may facilitate the discovery of selective therapeutic agents targeting MC4R.

Published

2021

44. Structural insights into ligand recognition and activation of the melanocortin-4 receptor

Author

Tingjun Hou, Wenbo Feng, Jin-Peng Sun, Tianhua Zhou, Daniel H. Scharf, Jiao Qin, Shanshan Xie, Chunyou Mao, Dan-Dan Shen, Dehua Yang, Qingya Shen, Li-Nan Chen, Yan Zhang, Yan Zhou, Ming-Wei Wang, Huibing Zhang, and Antao Dai

Subjects

Agonist, Melanocortin 4 receptor, Gs alpha subunit, Chemistry, medicine.drug_class, G protein, THIQ, Heterotrimeric G protein, medicine, Ligand (biochemistry), Receptor, medicine.drug, Cell biology

Abstract

SUMMARYMelanocortin-4 receptor (MC4R) plays a central role in the regulation of energy homeostasis. Its high sequence similarity to other MC receptor family members, low agonist selectivity and the lack of structural information concerning receptor activation have hampered the development of MC4R-seletive therapeutics to treat obesity. Here, we report four high-resolution structures of full-length MC4R in complex with the heterotrimeric Gs protein stimulated by the endogenous peptide α-MSH, FDA-approved drugs afamelanotide (Scenesse™) and bremelanotide (Vyleesi™), and selective small-molecule ligand THIQ, respectively. Together with pharmacological studies, our results reveal the conserved binding mode of peptidic agonists, the distinctive molecular details of small-molecule agonist recognition underlying receptor subtype selectivity, and distinct activation mechanism for MC4R, thereby offering new insights into G protein coupling. Our work may facilitate the discovery of selective therapeutic agents targeting MC4R.

Published

2021

45. Genetically Encoded Fluorescent Amino Acid for Monitoring Protein Interactions through FRET

Author

Fan Yang, Jiangyun Wang, Fahui Li, Jin-Peng Sun, Qi Liu, Ming-Jie Han, Wei Kong, Yingli Jia, Xiao Yu, Changxiu Qu, Shen-Ming Huang, Bai-Yang Cai, and Qing-tao He

Subjects

Binding Sites, Fluorophore, Glycine, Tryptophan, Plasma protein binding, Protein Engineering, Analytical Chemistry, Protein–protein interaction, chemistry.chemical_compound, beta-Arrestin 1, Förster resonance energy transfer, chemistry, Structural biology, Fluorescence Resonance Energy Transfer, Biophysics, Umbelliferones, Target protein, Amino Acids, Binding site, Ternary complex, Fluorescent Dyes, Protein Binding

Abstract

Forster resonance energy transfer (FRET) is a well-established method for studying macromolecular interactions and conformational changes within proteins. Such a method normally uses fluorescent proteins or chemical-labeling methods which are often only accessible to surface-exposed residues and risk-disturbing target protein structures. Here, we demonstrate that the genetic incorporation of a synthetic fluorescent amino acid, L-(7-hydroxycoumarin-4-yl) ethylglycine (Cou) and natural endogenous fluorophore Tryptophan (Trp) residues of a protein could serve as an efficient FRET pair to monitor protein interactions, using the signaling transducer β-arrestin-1 as a model system. We used this technology to record the dynamic spectra in both binding and competition experiments of β-arrestin-1, the contribution of each specific phosphate in ternary complex formation, in a rapid and efficient manner. The determined Kd value for the association between the active arrestin and Fab30 is 0.68 μM in the three-component interaction system. Moreover, we were able to determine the contributions of the site 3 phospho-site and the site 6 phospho-site binding, each contributing to the high affinity ternary complex assembly as 2.7 fold and 15.5 fold, respectively, which were never determined before. These results thus highlighted the potential usage of this new method in measurement of the allosteric-induced enhanced affinity with small amount proteins and in a fast manner and in a complex system. Collectively, our newly developed Trp:Cou FRET system based on genetic expansion technology has extended the molecular toolboxes available for biochemical and structural biology studies.

Published

2019

46. Deletion of pancreatic β‐cell adenosine kinase improves glucose homeostasis in young mice and ameliorates streptozotocin‐induced hyperglycaemia

Author

Hui Wei Feng, Chaodong Wu, Min Cui, Dongfang He, Xin Yu Chen, Makawi Ahmed Abdalhamid Osman, Jin-Peng Sun, Hui Lin, Yuqing Huo, Rui Jia Li, Jin Wang, Zhao Yang, Dong Mei Zeng, Yu Jing Sun, and Xiao Yu

Subjects

0301 basic medicine, insulin, replication, Aging, medicine.medical_specialty, Time Factors, endocrine system diseases, medicine.medical_treatment, Cell, β cell, Cell Count, Context (language use), Adenosine kinase, adenosine kinase, Carbohydrate metabolism, Streptozocin, 03 medical and health sciences, 0302 clinical medicine, Insulin-Secreting Cells, Internal medicine, medicine, Animals, Homeostasis, Glucose homeostasis, Cell Proliferation, Mice, Knockout, diabetes, biology, Insulin, Original Articles, Cell Biology, Streptozotocin, ADK, Glucose, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Hyperglycemia, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Original Article, Gene Deletion, medicine.drug

Abstract

Severe reduction in the β‐cell number (collectively known as the β‐cell mass) contributes to the development of both type 1 and type 2 diabetes. Recent pharmacological studies have suggested that increased pancreatic β‐cell proliferation could be due to specific inhibition of adenosine kinase (ADK). However, genetic evidence for the function of pancreatic β‐cell ADK under physiological conditions or in a pathological context is still lacking. In this study, we crossed mice carrying LoxP‐flanked Adk gene with Ins2‐Cre mice to acquire pancreatic β ‐cell ADK deficiency (Ins2‐Cre±Adkfl/fl) mice. Our results revealed that Ins2‐Cre+/‐Adkfl/fl mice showed improved glucose metabolism and β‐cell mass in younger mice, but showed normal activity in adult mice. Moreover, Ins2‐Cre±Adkfl/fl mice were more resistant to streptozotocin (STZ) induced hyperglycaemia and pancreatic β‐cell damage in adult mice. In conclusion, we found that ADK negatively regulates β‐cell replication in young mice as well as under pathological conditions, such as STZ induced pancreatic β‐cell damage. Our study provided genetic evidence that specific inhibition of pancreatic β‐cell ADK has potential for anti‐diabetic therapy.

Published

2019

47. Structural studies of phosphorylation-dependent interactions between the V2R receptor and arrestin-2

Author

Shen-Ming Huang, Peng Xiao, Changwen Jin, Zhongliang Zhu, Ru-Jia Zhao, Xiaogang Niu, Jing-Yu Lin, Qing-Tao He, Kunhong Xiao, Xiaona Tao, Fan Yang, Jiangyun Wang, Xiao Yu, Feng-Yuan Gao, Jin-Peng Sun, and Yingli Jia

Subjects

Phosphopeptides, Protein Conformation, alpha-Helical, 0301 basic medicine, Receptors, Vasopressin, genetic structures, Science, General Physics and Astronomy, Crystallography, X-Ray, environment and public health, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, Arrestin, Humans, Phosphorylation, Receptor, Nuclear Magnetic Resonance, Biomolecular, X-ray crystallography, G protein-coupled receptor, Multidisciplinary, Chemistry, General Chemistry, Receptor phosphorylation, Genetic code, Recombinant Proteins, eye diseases, HEK293 Cells, beta-Arrestin 1, 030104 developmental biology, Förster resonance energy transfer, Mutation, Biophysics, sense organs, Spectrum analysis, 030217 neurology & neurosurgery

Abstract

Arrestins recognize different receptor phosphorylation patterns and convert this information to selective arrestin functions to expand the functional diversity of the G protein-coupled receptor (GPCR) superfamilies. However, the principles governing arrestin-phospho-receptor interactions, as well as the contribution of each single phospho-interaction to selective arrestin structural and functional states, are undefined. Here, we determined the crystal structures of arrestin2 in complex with four different phosphopeptides derived from the vasopressin receptor-2 (V2R) C-tail. A comparison of these four crystal structures with previously solved Arrestin2 structures demonstrated that a single phospho-interaction change results in measurable conformational changes at remote sites in the complex. This conformational bias introduced by specific phosphorylation patterns was further inspected by FRET and 1H NMR spectrum analysis facilitated via genetic code expansion. Moreover, an interdependent phospho-binding mechanism of phospho-receptor-arrestin interactions between different phospho-interaction sites was unexpectedly revealed. Taken together, our results provide evidence showing that phospho-interaction changes at different arrestin sites can elicit changes in affinity and structural states at remote sites, which correlate with selective arrestin functions., The interaction between a GPCR, such as the vasopressin receptor-2 (V2R), and arrestin depends on the receptors’ phosphorylation pattern. Here authors use FRET and NMR to analyze the phosphorylation patterns of the V2R-arrestin complex and show that phospho-interactions are the key determinants of selective arrestin conformational states and correlated functions.

Published

2021

48. Whole genome sequencing revealed genetic diversity and selection of Guangxi indigenous chickens

Author

Jin-Peng Sun, Yu Huang, Wang Ran, Yang Manman, Liao Y, Wei Qiang, Zhu M, and Tao Chen

Subjects

Whole genome sequencing, education.field_of_study, Genetic diversity, Evolutionary biology, Population, Introgression, Biology, education, Selective sweep, Genome, Selection (genetic algorithm), Nucleotide diversity

Abstract

Guangxi chickens play an important role in promoting the high-quality development of the broiler industry in China, but their value and potential are yet to be discovered. To determine the genetic diversity and population structure of Guangxi indigenous chicken, we analyzed the whole genomes of 185 chicken from 8 phenotypically and geographically representative Guangxi chicken breeds, together with 12 RJFt, 12 BRA and 12 WL genomes available from previous studies. Calculation of heterozygosity (Hp), nucleotide diversity (π), and LD level indicated that Guangxi populations were characterized by higher genetic diversity and lower differentiation than RJFt and commercial breeds except HGFC. Population structure analysis also confirmed the introgression from commercial broiler breeds. Each population clustered together while the overall differentiation was small, MA has the richest genetic diversity among all varieties. Selective sweep analysis revealed BCO2, EDN3 and other candidate genes have received strong selection in local breeds, these also provided novel breeding visual and data basis for future breeding.

Published

2021

49. Ligand recognition, unconventional activation, and G protein coupling of the prostaglandin E 2 receptor EP2 subtype

Author

Ya-Ni Zhong, Xiaona Tao, Xu Yan, Jin-Peng Sun, Qingya Shen, Xiao Yu, Changxiu Qu, Dan-Dan Shen, Ying Guan, Chao Zhang, Chunyou Mao, Peng-Ju Zhang, Ru-Jia Zhao, Peng Xiao, Guige Hou, Yan Zhang, Guihua Hou, Junyan He, Fan Yang, Huibing Zhang, Renjie Chai, You-Fei Guan, and Zijian Li

Subjects

Agonist, 0303 health sciences, Multidisciplinary, G protein, Chemistry, medicine.drug_class, Prostaglandin E2 receptor, Rational design, Ligand (biochemistry), Cell biology, 03 medical and health sciences, 0302 clinical medicine, Heterotrimeric G protein, medicine, lipids (amino acids, peptides, and proteins), Receptor, 030217 neurology & neurosurgery, Endogenous agonist, 030304 developmental biology

Abstract

Selective modulation of the heterotrimeric G protein α S subunit-coupled prostaglandin E2 (PGE2) receptor EP2 subtype is a promising therapeutic strategy for osteoporosis, ocular hypertension, neurodegenerative diseases, and cardiovascular disorders. Here, we report the cryo-electron microscopy structure of the EP2-Gs complex with its endogenous agonist PGE2 and two synthesized agonists, taprenepag and evatanepag (CP-533536). These structures revealed distinct features of EP2 within the EP receptor family in terms of its unconventional receptor activation and G protein coupling mechanisms, including activation in the absence of a typical W6.48 "toggle switch" and coupling to Gs via helix 8. Moreover, inspection of the agonist-bound EP2 structures uncovered key motifs governing ligand selectivity. Our study provides important knowledge for agonist recognition and activation mechanisms of EP2 and will facilitate the rational design of drugs targeting the PGE2 signaling system.

Published

2021

50. PTP‐MEG2 regulates quantal size and fusion pore opening through two distinct structural bases and substrates

Author

Zhigang Xu, Zhong-Liang Zhu, Min Cui, Kangshuai Li, Yi-Jing Wang, Sheng Zhang, You-Chen Song, Chuan Wang, Jin-Peng Sun, Changhe Wang, Yunfei Xu, Chun-Hua Liu, Xu Chen, Zhiliang Ji, Wei-Dong Zhao, Zhao Yang, Zhong Yin Zhang, Xiao Yu, Peng Xiao, and Xiao-Zhen Yang

Subjects

animal structures, Mutant, Peptide, Protein tyrosine phosphatase, environment and public health, Biochemistry, Exocytosis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Genetics, Secretion, Phosphorylation, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, Fusion, 0303 health sciences, Vesicle, Substrate (chemistry), Tyrosine phosphorylation, Articles, Protein Tyrosine Phosphatases, Non-Receptor, enzymes and coenzymes (carbohydrates), chemistry, Biophysics, Protein Tyrosine Phosphatases, Peptides, 030217 neurology & neurosurgery

Abstract

Tyrosine phosphorylation of secretion machinery proteins is a crucial regulatory mechanism for exocytosis. However, the participation of protein tyrosine phosphatases (PTPs) in different exocytosis stages has not been defined. Here we demonstrated that PTP-MEG2 controls multiple steps of catecholamine secretion. Biochemical and crystallographic analyses revealed key residues that the interactions between govern the PTP-MEG2 and NSF-pY83 site, specify PTP-MEG2 substrate selectivity and modulate the fusion of catecholamine-containing vesicles. Unexpectedly, delineation of PTP-MEG2 mutants along with the NSF binding interface revealed that PTP-MEG2 controls the fusion pore opening through non-NSF dependent mechanisms. Utilizing bioinformatics search and biochemical and electrochemical screening approaches, we discovered that PTP-MEG2 regulates the opening and extension of the fusion pore by dephosphorylating the DYNAMIN2-pY125 and MUNC18-1-pY145 site. Further structural and biochemical analysis confirmed the interaction of PTP-MEG2 with MUNC18-1-pY145 or DYNAMIN2-pY125 through a distinct structural basis compared with that of the NSF-pY83 site. Our studies extended mechanistic insights in complex exocytosis processes.HIGHLIGHTSPTP-MEG2 regulates multiple steps of exocytosis.A crystal structure of the PTP-MEG2/phosphor-NSF-pY83 segment was obtained.Functional delineation of the PTP-MEG2/NSF interface led to the discovery of new PTP-MEG2 substrates.PTP-MEG2 regulates fusion pore opening and extension through the DYNAMIN2-pY125 site and MUNC18-1 pY145 site.The distinct structural basis of the recognition of substrates by PTP-MEG2 allows selective inhibitor design.

Published

2021