Nick Holliday

Contact

• workRoom CS6 The Medical School, Floor C
  Queen's Medical Centre
  Nottingham
  NG7 2UH
  UK
• work0115 82 30084
• fax0115 82 30081
• nicholas.holliday@nottingham.ac.uk

Biography

Following undergraduate studies at the University of Cambridge (BA St John's College, 1994), Nick Holliday obtained his PhD from King's College London (1998), supported by an AJ Clark PhD studentship from the British Pharmacological Society. During subsequent postdoctoral work in London, his interests in peptide messengers regulating appetite and metabolism became focused on molecular mechanisms underlying the signalling and regulation of their receptors. Nick was awarded a independent RCUK fellowship at the University of Nottingham in 2006, followed by Lecturer (2011) and Associate Professor (2013) positions. While at Nottingham, Nick's group has been funded by the MRC, charity, the Brazilian CAPES drug discovery program and industrial collaborations, and in 2011 he was awarded the Bill Bowman travelling lectureship from the British Pharmacological Society. He has also been actively involved in public engagement, including an arts crossover project to explain the use of imaging in pharmacology ("Hijacking Natural Systems"), funded by the Wellcome Trust.

Expertise Summary

GPCRs for peptides such as neuropeptide Y, gastrin releasing peptide and ghrelin, and nutrients such as free fatty acids, are implicated in the control of appetite, body weight and insulin secretion. They provide new drug targets to treat diabetes and obesity, and as such an understanding of the cellular mechanisms that regulate receptor function is crucial when considering long-term treatment of these conditions

Our group focuses on understanding the mechanisms underlying the signalling and intracellular trafficking of these GPCRs, and developing methods to assess ligand pharmacology for these processes. We have particular expertise in high content imaging and fluorescence / luminescence complementation approaches to develop GPCR protein-protein interaction assays, with the aim to study pharmacology at the level of individual signalling complexes and so better understand the effects of GPCR dimers and ligands which are signalling biased. Recently (in collaboration with Tom Bellamy), we are developing light (optogenetic) and "designer drug" activated receptors to explore spatiotemporal signalling in both model cell systems and astrocytes.

Group members:

CAPES Drug Discovery program: Dr Corado Pedebos

PhD students: Rachel Richardson, Laura Humphrys, Jess Carpenter, Saori Mukaida, Aaron Horsey, Matt Gibbs, Nicola Dijon, Desi Nesheva

Research Interests

Signalling bias in peptide and dopamine receptors

Mechanisms of GPCR internalisation and intracellular trafficking defined through high content imaging

Allosteric interactions in peptide receptor homo and heterodimers

Optogenetic and chemogenetic stimulation of GPCR signalling

Research Expertise

GPCR pharmacology (binding and signalling assays)

High content confocal imaging and analysis

Fluorescence and luminescence complementation to detect protein interactions

Optogenetic and designer G protein coupled receptors

Teaching Summary

Main responsibilities:

Module Convenor

B31ESP - Essential Skills for Phamacists (Year 1, MPharm 40 credit)

C12PBT - Pharmacological Basis of Therapeutics (year 2, BSc, 20 credit)

A13GPD - GPCR polymorphisms, disease and personalised medicine (Year 3, BMedSci)

B33PPM - GPCR based personalised medicine (Year 3, MPharm)

Key Contributor

B34FME - Future Medicines (MPharm year 4)

Senior Tutor for the MPharm degree

Selected Publications

• SYKES DA, MOORE H, STOTT LA, HOLLIDAY ND, JAVITCH JA, LANE JR and CHARLTON SJ, 2017. Extrapyramidal side effects of antipsychotics are linked to their association kinetics at dopamine D2 receptors Nature Communications. (In Press.)
• KILPATRICK LE, HUMPHRYS LJ and HOLLIDAY ND, 2015. A G protein-coupled receptor dimer imaging assay reveals selectively modified pharmacology of neuropeptide Y Y1/Y5 receptor heterodimers. Molecular pharmacology. 87(4), 718-32
• WONG, KELVIN, BRIDDON, STEPHEN J., HOLLIDAY, NICHOLAS D. and KERR, IAN D., 2016. Plasma membrane dynamics and tetrameric organisation of ABCG2 transporters in mammalian cells revealed by single particle imaging techniques BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR CELL RESEARCH. 1863(1), 19-29
• LIU M, MOUNTFORD SJ, RICHARDSON RR, GROENEN M, , HOLLIDAY ND and THOMPSON PE, 2016. Optically pure, structural and fluorescent analogues of a dimeric Y4 receptor agonist derived by an olefin metathesis approach. J Med Chem. 59(13), 6059-6069

• View all publications

• FREITAS ACN, PEIGNEUR S, MACEDO FHP, MENEZES-FILHO JE, MILLNS P, MEDEIROS LF, ARRUDA MA, CRUZ J, HOLLIDAY ND, TYTGAT J, HATHWAY G and DE LIMA ME, 2018. The Peptide PnPP-19, a Spider Toxin Derivative, Activates μ-Opioid Receptors and Modulates Calcium Channels. Toxins. 10(1),
• SYKES DA, MOORE H, STOTT LA, HOLLIDAY ND, JAVITCH JA, LANE JR and CHARLTON SJ, 2017. Extrapyramidal side effects of antipsychotics are linked to their association kinetics at dopamine D2 receptors Nature Communications. (In Press.)
• WONG, KELVIN, BRIDDON, STEPHEN J., HOLLIDAY, NICHOLAS D. and KERR, IAN D., 2016. Plasma membrane dynamics and tetrameric organisation of ABCG2 transporters in mammalian cells revealed by single particle imaging techniques BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR CELL RESEARCH. 1863(1), 19-29
• STOTT, LISA A., HALL, DAVID A. and HOLLIDAY, NICHOLAS D., 2016. Unravelling intrinsic efficacy and ligand bias at G protein coupled receptors: A practical guide to assessing functional data BIOCHEMICAL PHARMACOLOGY. 101, 1-12
• LIU M, MOUNTFORD SJ, RICHARDSON RR, GROENEN M, , HOLLIDAY ND and THOMPSON PE, 2016. Optically pure, structural and fluorescent analogues of a dimeric Y4 receptor agonist derived by an olefin metathesis approach. J Med Chem. 59(13), 6059-6069
• LIU, MENGJIE, RICHARDSON, RACHEL R., MOUNTFORD, SIMON J., ZHANG, LEI, TEMPONE, MATHEUS H., HERZOG, HERBERT, HOLLIDAY, NICHOLAS D. and THOMPSON, PHILIP E., 2016. Identification of a Cyanine-Dye Labeled Peptidic Ligand for Y1R and Y4R, Based upon the Neuropeptide Y C-Terminal Analogue, BVD-15 BIOCONJUGATE CHEMISTRY. 27(9), 2166-2175
• NORTHFIELD, SUSAN E., MOUNTFORD, SIMON J., WIELENS, JEROME, LIU, MENGJIE, ZHANG, LEI, HERZOG, HERBERT, HOLLIDAY, NICHOLAS D., SCANLON, MARTIN J., PARKER, MICHAEL W., CHALMERS, DAVID K. and THOMPSON, PHILIP E., 2015. Propargyloxyproline Regio- and Stereoisomers for Click-Conjugation of Peptides: Synthesis and Application in Linear and Cyclic Peptides AUSTRALIAN JOURNAL OF CHEMISTRY. 68(9), 1365-1372
• KILPATRICK LE, HUMPHRYS LJ and HOLLIDAY ND, 2015. A G protein-coupled receptor dimer imaging assay reveals selectively modified pharmacology of neuropeptide Y Y1/Y5 receptor heterodimers. Molecular pharmacology. 87(4), 718-32
• VALENTIN-HANSEN L, FRIMURER TM, MOKROSINSKI J, HOLLIDAY ND and SCHWARTZ TW, 2015. Biased Gs versus Gq proteins and β-arrestin signaling in the NK1 receptor determined by interactions in the water hydrogen bond network. The Journal of biological chemistry. 290(40), 24495-508
• ALQAHTANI F, MAHDAVI J, WHELDON LM, VASSEY M, PIRINCCIOGLU N, ROYER P, QARANI SM, MORROLL S, STOOF J, HOLLIDAY ND, TEO SY, OLDFIELD NJ, WOOLDRIDGE KG and ALA'ALDEEN DAA, 2014. Deciphering the complex three-way interaction between the non-integrin laminin receptor, galectin-3 and Neisseria meningitidis. Open biology. 4(10),
• MOUNTFORD SJ, LIU M, ZHANG L, GROENEN M, HERZOG H, HOLLIDAY ND and THOMPSON PE, 2014. Synthetic routes to the Neuropeptide Y Y1 receptor antagonist 1229U91 and related analogues for SAR studies and cell-based imaging. Organic & biomolecular chemistry. 12(20), 3271-81
• ENGELSTOFT MS, NORN C, HAUGE M, HOLLIDAY ND, ELSTER L, LEHMANN J, JONES RM, FRIMURER TM and SCHWARTZ TW, 2014. Structural basis for constitutive activity and agonist-induced activation of the enteroendocrine fat sensor GPR119. British journal of pharmacology. 171(24), 5774-89
• SIVERTSEN, B., HOLLIDAY, N., MADSEN, A. N. and HOLST, B., 2013. Functionally biased signalling properties of 7TM receptors - opportunities for drug development for the ghrelin receptor BRITISH JOURNAL OF PHARMACOLOGY. 170(7), 1349-1362
• HOLLIDAY ND, WATSON SJ and BROWN AJH, 2012. Drug discovery opportunities and challenges at G protein coupled receptors for long chain free fatty acids Frontiers in Endocrinology: Frontiers in Molecular and Structural Endocrinology. 2,
• WATSON, S-J., BROWN, A.J.H. and HOLLIDAY, N.D., 2012. Differential signaling by splice variants of the human free fatty acid receptor, GPR120 Molecular Pharmacology. 81(5), 631-642
• KILPATRICK, L.E., BRIDDON, S.J. and HOLLIDAY, N.D., 2012. Fluorescence correlation spectroscopy, combined with bimolecular fluorescence complementation, reveal the effects of β-arrestin complexes and endocytic targeting on the membrane mobility of neuropeptide Y receptors Biochemica Biophysica Acta: Molecular Cell Research. 1823(6), 1068-1081
• HANSEN, L.V., GROENEN, M., NYGAARD, R., FRIMURER, T.M., HOLLIDAY, N.D. and SCHWARTZ, T.W., 2012. The arginine of the DRY motif in TM-III functions as a balancing microswitch in the activation of the beta2-adrenoceptor Journal of Biological Chemistry. 287, 31973-31982
• KILPATRICK LE and HOLLIDAY ND, 2012. Dissecting the pharmacology of g protein-coupled receptor signaling complexes using bimolecular fluorescence complementation. Methods in molecular biology (clifton, n.j.). 897, 109-38
• HAIDER, A.J., BRIGGS, D., SELF, T.J., CHILVERS, H.L., HOLLIDAY, N.D. and KERR, I.D., 2011. Dimerization of ABCG2 analysed by bimolecular fluorescence complementation PLoS ONE. 6(10), e25818
• EVANS, E.L., SAXTON, J., SHELTON, S.J., BEGITT, A., HOLLIDAY, N.D., HIPSKIND, R.A. and SHAW, P.E., 2011. Dimer formation and conformational flexibility ensure cytoplasmic stability and nuclear accumulation of Elk-1 Nucleic Acids Research. 39(15), 6390-6402
• SIVERTSEN, B, LANG, MJ, FRIMURER, TM, HOLLIDAY, ND, BACH, A, ELS, S, ENGELSTOFT, MS, PETERSEN, PS, MADSEN, AN, SCHWARTZ, TW, BECK-SICKINGER, AG and HOLST, B, 2011. Unique Interaction Pattern For A Functionally Biased Ghrelin Receptor Agonist Journal Of Biological Chemistry. 286(23), 20845-20860
• KILPATRICK, L.E., BRIDDON, S.J., HILL, S.J. and HOLLIDAY, N.D., 2010. Quantitative analysis of neuropeptide Y receptor association with β-arrestin2 measured by bimolecular fluorescence complementation British Journal of Pharmacology. 160(4), 892-906
• ROSE, RH, BRIDDON, SJ and HOLLIDAY, ND, 2010. Bimolecular Fluorescence Complementation:Lighting Up Seven Transmembrane Domain Receptor Signalling Networks British Journal of Pharmacology. 738-750
• JORGENSEN, R., HOLLIDAY, N.D., HANSEN, J.L., VRECL, M., HEDING, A., SCHWARTZ, T.W. and ELLING, C.E., 2008. Characterization of G-protein coupled receptor kinase interaction with the neurokinin-1 receptor using bioluminescence resonance energy transfer Molecular Pharmacology. 73(2), 349-358
• HOLLIDAY, N.D., TOUGH, I.R. and COX, H.M., 2007. A functional comparison of recombinant and native sst2 receptor variants in epithelia British Journal of Pharmacology. 152(1), 132-140
• HOLLIDAY, NICHOLAS D, HOLST, BIRGITTE, RODIONOVA, ELENA A, SCHWARTZ, THUE W and COX, HELEN M, 2007. Importance of constitutive activity and arrestin-independent mechanisms for intracellular trafficking of the ghrelin receptor. Molecular Endocrinology. 21(12), 3100-12
• TOUGH, I.R., HOLLIDAY, N.D. and COX, H.M, 2006. Y(4) receptors mediate the inhibitory responses of pancreatic polypeptide in human and mouse colon mucosa. Journal of Pharmacology and Experimental Therapeutics. 319(1), 20-30
• HOLLIDAY, N.D., LAM, C-W., TOUGH, I.R. and COX, H.M, 2005. Role of the C terminus in neuropeptide Y Y1 receptor desensitization and internalization. Molecular Pharmacology. 67(3), 655-664
• HOLST, B., HOLLIDAY, N.D., BACH, A., ELLING, C.E., COX, H.M. and SCHWARTZ, T.W, 2004. Common structural basis for constitutive activity of the ghrelin receptor family. Journal of Biological Chemistry. 279(51), 53806-53817
• HOLLIDAY,N.D, MICHEL,M.C and COX,H.M, 2004. Neuropeptide Y receptors and their signalling. In: MICHEL, MC, ed., Neuropeptide Y and related peptides Springer-Verlag. 45-73
• HOLLIDAY, N.D. and COX, H.M, 2003. Control of signalling efficacy by palmitoylation of the rat Y1 receptor. British Journal of Pharmacology. 139(3), 501-12
• COX, H.M, TOUGH, I.R, ZANDVLIET, D.W.J. and HOLLIDAY, N.D, 2001. Constitutive neuropeptide Y Y(4) receptor expression in human colonic adenocarcinoma cell lines. British Journal of Pharmacology. 132(1), 345-53
• HOLLIDAY, N D, POLLOCK, E L, TOUGH, I R and COX, H M, 2000. PYY preference is a common characteristic of neuropeptide Y receptors expressed in human, rat, and mouse gastrointestinal epithelia. Canadian Journal of Physiology and Pharmacology. 78(2), 126-33
• HOLLIDAY, N D and COX, H M, 1999. Modulation of chloride, potassium and bicarbonate transport by muscarinic receptors in a human adenocarcinoma cell line. British Journal of Pharmacology. 126(1), 269-79
• HOLLIDAY, N D, TOUGH, I R and COX, H M, 1997. Inhibition of cyclic AMP-dependent chloride secretion by PP receptors and alpha 2-adrenoceptors in a human colonic epithelial cell line. Naunyn-Schmiedeberg's Archives of Pharmacology. 355(2), 183-9
• HOLLIDAY, N D and COX, H M, 1996. The functional investigation of a human adenocarcinoma cell line, stably transfected with the neuropeptide Y Y1 receptor. British Journal of Pharmacology. 119(2), 321-9
• HOLLIDAY, N, BALBI, D, PANCE, A and ALLEN, J M, 1995. Nerve growth factor regulation of a late response gene--neuropeptide Y. Biochemical Society Transactions. 23(2), 226S
• PANCE, A, BALBI, D, HOLLIDAY, N and ALLEN, J M, 1995. Effect of cAMP elevation on the NPY gene transcription. Biochemical Society Transactions. 23(1), 47S