Biochemistry and Pharmacology - Research Publications

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2020 - 2023 724
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Start date: 2020 × Type: Journal Article × End date: 2023 ×

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    Unravelling the mechanism of neurotensin recognition by neurotensin receptor 1
    Asadollahi, K ; Rajput, S ; de Zhang, LA ; Ang, C-S ; Nie, S ; Williamson, NA ; Griffin, MDW ; Bathgate, RAD ; Scott, DJ ; Weikl, TR ; Jameson, GNL ; Gooley, PR (NATURE PORTFOLIO, 2023-12-09)
    The conformational ensembles of G protein-coupled receptors (GPCRs) include inactive and active states. Spectroscopy techniques, including NMR, show that agonists, antagonists and other ligands shift the ensemble toward specific states depending on the pharmacological efficacy of the ligand. How receptors recognize ligands and the kinetic mechanism underlying this population shift is poorly understood. Here, we investigate the kinetic mechanism of neurotensin recognition by neurotensin receptor 1 (NTS1) using 19F-NMR, hydrogen-deuterium exchange mass spectrometry and stopped-flow fluorescence spectroscopy. Our results indicate slow-exchanging conformational heterogeneity on the extracellular surface of ligand-bound NTS1. Numerical analysis of the kinetic data of neurotensin binding to NTS1 shows that ligand recognition follows an induced-fit mechanism, in which conformational changes occur after neurotensin binding. This approach is applicable to other GPCRs to provide insight into the kinetic regulation of ligand recognition by GPCRs.
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    Structures of the interleukin 11 signalling complex reveal gp130 dynamics and the inhibitory mechanism of a cytokine variant
    Metcalfe, RD ; Hanssen, E ; Fung, KY ; Aizel, K ; Kosasih, CC ; Zlatic, CO ; Doughty, L ; Morton, CJ ; Leis, AP ; Parker, MW ; Gooley, PR ; Putoczki, TL ; Griffin, MDW (NATURE PORTFOLIO, 2023-11-20)
    Interleukin (IL-)11, an IL-6 family cytokine, has pivotal roles in autoimmune diseases, fibrotic complications, and solid cancers. Despite intense therapeutic targeting efforts, structural understanding of IL-11 signalling and mechanistic insights into current inhibitors are lacking. Here we present cryo-EM and crystal structures of the human IL-11 signalling complex, including the complex containing the complete extracellular domains of the shared IL-6 family β-receptor, gp130. We show that complex formation requires conformational reorganisation of IL-11 and that the membrane-proximal domains of gp130 are dynamic. We demonstrate that the cytokine mutant, IL-11 Mutein, competitively inhibits signalling in human cell lines. Structural shifts in IL-11 Mutein underlie inhibition by altering cytokine binding interactions at all three receptor-engaging sites and abrogating the final gp130 binding step. Our results reveal the structural basis of IL-11 signalling, define the molecular mechanisms of an inhibitor, and advance understanding of gp130-containing receptor complexes, with potential applications in therapeutic development.
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    Mtfp1 ablation enhances mitochondrial respiration and protects against hepatic steatosis
    Patitucci, C ; Hernandez-Camacho, JD ; Vimont, E ; Yde, S ; Cokelaer, T ; Chaze, T ; Gianetto, QG ; Matondo, M ; Gazi, A ; Nemazanyy, I ; Stroud, DA ; Hock, DH ; Donnarumma, E ; Wai, T (NATURE PORTFOLIO, 2023-12-20)
    Hepatic steatosis is the result of imbalanced nutrient delivery and metabolism in the liver and is the first hallmark of Metabolic dysfunction-associated steatotic liver disease (MASLD). MASLD is the most common chronic liver disease and involves the accumulation of excess lipids in hepatocytes, inflammation, and cancer. Mitochondria play central roles in liver metabolism yet the specific mitochondrial functions causally linked to MASLD remain unclear. Here, we identify Mitochondrial Fission Process 1 protein (MTFP1) as a key regulator of mitochondrial and metabolic activity in the liver. Deletion of Mtfp1 in hepatocytes is physiologically benign in mice yet leads to the upregulation of oxidative phosphorylation (OXPHOS) activity and mitochondrial respiration, independently of mitochondrial biogenesis. Consequently, liver-specific knockout mice are protected against high fat diet-induced steatosis and metabolic dysregulation. Additionally, Mtfp1 deletion inhibits mitochondrial permeability transition pore opening in hepatocytes, conferring protection against apoptotic liver damage in vivo and ex vivo. Our work uncovers additional functions of MTFP1 in the liver, positioning this gene as an unexpected regulator of OXPHOS and a therapeutic candidate for MASLD.
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    The broccoli-derived antioxidant sulforaphane changes the growth of gastrointestinal microbiota, allowing for the production of anti-inflammatory metabolites
    Marshall, SA ; Young, RB ; Lewis, JM ; Rutten, EL ; Gould, J ; Barlow, CK ; Giogha, C ; Marcelino, VR ; Fields, N ; Schittenhelm, RB ; Hartland, EL ; Scott, NE ; Forster, SC ; Gulliver, EL (ELSEVIER, 2023-08)
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    Vasculature is getting Hip(po): Hippo in vascular development and disease
    Kobayashi, S ; Cox, AG ; Harvey, KF ; Hogan, BM (CELL PRESS, 2023-12-04)
    The Hippo signaling pathway regulates developmental organ growth, regeneration, and cell fate decisions. Although the role of the Hippo pathway, and its transcriptional effectors YAP and TAZ, has been well documented in many cell types and species, only recently have the roles for this pathway come to light in vascular development and disease. Experiments in mice, zebrafish, and in vitro have uncovered roles for the Hippo pathway, YAP, and TAZ in vasculogenesis, angiogenesis, and lymphangiogenesis. In addition, the Hippo pathway has been implicated in vascular cancers and cardiovascular diseases, thus identifying it as a potential therapeutic target for the treatment of these conditions. However, despite recent advances, Hippo's role in the vasculature is still underappreciated compared with its role in epithelial tissues. In this review, we appraise our current understanding of the Hippo pathway in blood and lymphatic vessel development and highlight the current knowledge gaps and opportunities for further research.
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    Next Generation Cell Culture Tools Featuring Micro‐ and Nanotopographies for Biological Screening (Adv. Funct. Mater. 3/2022)
    Carthew, J ; Abdelmaksoud, HH ; Cowley, KJ ; Hodgson‐Garms, M ; Elnathan, R ; Spatz, JP ; Brugger, J ; Thissen, H ; Simpson, KJ ; Voelcker, NH ; Frith, JE ; Cadarso, VJ (Wiley, 2022-01)
    In article number 2100881, Nicolas H. Voelcker, Jessica E. Frith, Victor J. Cadarso, and co-workers demonstrate a novel approach to imprint micro and nanoscaled topographical features into conventional cell cultureware, facilitating its compatibility with standard biological techniques. This enables high-throughput screening to integrate the effects of surface topographies into unique cell specific responses and fate determination.
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    Extracellular vesicular lipids as biomarkers for the diagnosis of Alzheimer’s disease
    Su, H ; Rustam, YH ; Masters, CL ; Makalic, E ; McLean, C ; Hill, AF ; Barnham, KJ ; Reid, GE ; Vella, LJ (Wiley, 2021-12-31)
    An increasing number of studies have revealed that dysregulated lipid homeostasis is associated with the pathological processes that lead to Alzheimer’s disease (AD). If changes in key lipid species could be detected in the periphery, it would advance our understanding of the disease and facilitate biomarker discovery. Global lipidomic profiling of sera/blood however has proved challenging with limited disease or tissue specificity. Small extracellular vesicles (EV) in the central nervous system, can pass the blood-brain barrier and enter the periphery, carrying a subset of lipids that could reflect lipid homeostasis in brain. This makes EVs uniquely suited for peripheral biomarker exploration.
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    The Concise Guide to PHARMACOLOGY 2023/24: G protein-coupled receptors
    Alexander, SPH ; Christopoulos, A ; Davenport, AP ; Kelly, E ; Mathie, AA ; Peters, JA ; Veale, EL ; Armstrong, JF ; Faccenda, E ; Harding, SD ; Davies, JA ; Abbracchio, MP ; Abraham, G ; Agoulnik, A ; Alexander, W ; Al-hosaini, K ; Back, M ; Baker, JG ; Barnes, NM ; Bathgate, R ; Beaulieu, J-M ; Beck-Sickinger, AG ; Behrens, M ; Bernstein, KE ; Bettler, B ; Birdsall, NJM ; Blaho, V ; Boulay, F ; Bousquet, C ; Brauner-Osborne, H ; Burnstock, G ; Calo, G ; Castano, JP ; Catt, KJ ; Ceruti, S ; Chazot, P ; Chiang, N ; Chini, B ; Chun, J ; Cianciulli, A ; Civelli, O ; Clapp, LH ; Couture, R ; Cox, HM ; Csaba, Z ; Dahlgren, C ; Dent, G ; Douglas, SD ; Dournaud, P ; Eguchi, S ; Escher, E ; Filardo, EJ ; Fong, T ; Fumagalli, M ; Gainetdinov, RR ; Garelja, ML ; de Gasparo, M ; Gerard, C ; Gershengorn, M ; Gobeil, F ; Goodfriend, TL ; Goudet, C ; Gratz, L ; Gregory, KJ ; Gundlach, AL ; Hamann, J ; Hanson, J ; Hauger, RL ; Hay, DL ; Heinemann, A ; Herr, D ; Hollenberg, MD ; Holliday, ND ; Horiuchi, M ; Hoyer, D ; Hunyady, L ; Husain, A ; Ijzerman, AP ; Inagami, T ; Jacobson, KA ; Jensen, RT ; Jockers, R ; Jonnalagadda, D ; Karnik, S ; Kaupmann, K ; Kemp, J ; Kennedy, C ; Kihara, Y ; Kitazawa, T ; Kozielewicz, P ; Kreienkamp, H-J ; Kukkonen, JP ; Langenhan, T ; Larhammar, D ; Leach, K ; Lecca, D ; Lee, JD ; Leeman, SE ; Leprince, J ; Li, XX ; Lolait, SJ ; Lupp, A ; Macrae, R ; Maguire, J ; Malfacini, D ; Mazella, J ; McArdle, CA ; Melmed, S ; Michel, MC ; Miller, LJ ; Mitolo, V ; Mouillac, B ; Mueller, CE ; Murphy, PM ; Nahon, J-L ; Ngo, T ; Norel, X ; Nyimanu, D ; O'Carroll, A-M ; Offermanns, S ; Panaro, MA ; Parmentier, M ; Pertwee, RG ; Pin, J-P ; Prossnitz, ER ; Quinn, M ; Ramachandran, R ; Ray, M ; Reinscheid, RK ; Rondard, P ; Rovati, GE ; Ruzza, C ; Sanger, GJ ; Schoeneberg, T ; Schulte, G ; Schulz, S ; Segaloff, DL ; Serhan, CN ; Singh, KD ; Smith, CM ; Stoddart, LA ; Sugimoto, Y ; Summers, R ; Tan, VP ; Thal, D ; Thomas, WW ; Timmermans, PBMWM ; Tirupula, K ; Toll, L ; Tulipano, G ; Unal, H ; Unger, T ; Valant, C ; Vanderheyden, P ; Vaudry, D ; Vaudry, H ; Vilardaga, J-P ; Walker, CS ; Wang, JM ; Ward, DT ; Wester, H-J ; Willars, GB ; Williams, TL ; Woodruff, TM ; Yao, C ; Ye, RD (WILEY, 2023-10)
    The Concise Guide to PHARMACOLOGY 2023/24 is the sixth in this series of biennial publications. The Concise Guide provides concise overviews, mostly in tabular format, of the key properties of approximately 1800 drug targets, and about 6000 interactions with about 3900 ligands. There is an emphasis on selective pharmacology (where available), plus links to the open access knowledgebase source of drug targets and their ligands (https://www.guidetopharmacology.org), which provides more detailed views of target and ligand properties. Although the Concise Guide constitutes almost 500 pages, the material presented is substantially reduced compared to information and links presented on the website. It provides a permanent, citable, point-in-time record that will survive database updates. The full contents of this section can be found at http://onlinelibrary.wiley.com/doi/bph.16177. G protein-coupled receptors are one of the six major pharmacological targets into which the Guide is divided, with the others being: ion channels, nuclear hormone receptors, catalytic receptors, enzymes and transporters. These are presented with nomenclature guidance and summary information on the best available pharmacological tools, alongside key references and suggestions for further reading. The landscape format of the Concise Guide is designed to facilitate comparison of related targets from material contemporary to mid-2023, and supersedes data presented in the 2021/22, 2019/20, 2017/18, 2015/16 and 2013/14 Concise Guides and previous Guides to Receptors and Channels. It is produced in close conjunction with the Nomenclature and Standards Committee of the International Union of Basic and Clinical Pharmacology (NC-IUPHAR), therefore, providing official IUPHAR classification and nomenclature for human drug targets, where appropriate.
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    Integrated Transcriptomic and Metabolomic Mapping Reveals the Mechanism of Action of Ceftazidime/Avibactam against Pan-Drug-Resistant Klebsiella pneumoniae
    Hussein, M ; Allobawi, R ; Zhao, J ; Yu, H ; Neville, SL ; Wilksch, J ; Wong, LJM ; Baker, M ; McDevitt, CA ; Rao, GG ; Li, J ; Velkov, T (AMER CHEMICAL SOC, 2023-10-25)
    Here, we employed an integrated metabolomics and transcriptomics approach to investigate the molecular mechanism(s) of action of ceftazidime/avibactam against a pan-drug-resistant K. pneumoniae clinical isolate from a patient with urinary tract infection. Ceftazidime/avibactam induced time-dependent perturbations in the metabolome and transcriptome of the bacterium, mainly at 6 h, with minimal effects at 1 and 3 h. Metabolomics analysis revealed a notable reduction in essential lipids involved in outer membrane glycerolipid biogenesis. This disruption effect extended to peptidoglycan and lipopolysaccharide biosynthetic pathways, including lipid A and O-antigen assembly. Importantly, ceftazidime/avibactam not only affected the final steps of peptidoglycan biosynthesis in the periplasm, a common mechanism of ceftazidime action, but also influenced the synthesis of lipid-linked intermediates and early stages of cytoplasmic peptidoglycan synthesis. Furthermore, ceftazidime/avibactam substantially inhibited central carbon metabolism (e.g., the pentose phosphate pathway and tricarboxylic acid cycle). Consistently, the dysregulation of genes governing these metabolic pathways aligned with the metabolomics findings. Certain metabolomics and transcriptomics signatures associated with ceftazidime resistance were also perturbed. Consistent with the primary target of antibiotic activity, biochemical assays also confirmed the direct impact of ceftazidime/avibactam on peptidoglycan production. This study explored the intricate interactions of ceftazidime and avibactam within bacterial cells, including their impact on cell envelope biogenesis and central carbon metabolism. Our findings revealed the complexities of how ceftazidime/avibactam operates, such as hindering peptidoglycan formation in different cellular compartments. In summary, this study confirms the existing hypotheses about the antibacterial and resistance mechanisms of ceftazidime/avibactam while uncovering novel insights, including its impact on lipopolysaccharide formation.
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    Selective transduction and photoinhibition of pre-Bötzinger complex neurons that project to the facial nucleus in rats affects nasofacial activity
    Melo, MR ; Wykes, AD ; Connelly, AA ; Bassi, JK ; Cheung, SD ; McDougall, SJ ; Menuet, C ; Bathgate, RAD ; Allen, AM (eLife Sciences Publications Ltd, 2023-09-29)
    The pre-Bötzinger complex (preBötC), a key primary generator of the inspiratory breathing rhythm, contains neurons that project directly to facial nucleus (7n) motoneurons to coordinate orofacial and nasofacial activity. To further understand the identity of 7n-projecting preBötC neurons, we used a combination of optogenetic viral transgenic approaches to demonstrate that selective photoinhibition of these neurons affects mystacial pad activity, with minimal effects on breathing. These effects are altered by the type of anesthetic employed and also between anesthetized and conscious states. The population of 7n-projecting preBötC neurons we transduced consisted of both excitatory and inhibitory neurons that also send collaterals to multiple brainstem nuclei involved with the regulation of autonomic activity. We show that modulation of subgroups of preBötC neurons, based on their axonal projections, is a useful strategy to improve our understanding of the mechanisms that coordinate and integrate breathing with different motor and physiological behaviors. This is of fundamental importance, given that abnormal respiratory modulation of autonomic activity and orofacial behaviors have been associated with the development and progression of diseases.