Your search keyword '"Nick J. Reynolds"' showing total 159 results

151. Human Clinical Research and Therapeutics

Author

M Donaldson, P Mcgil, Paul A. Wilson, Ha Long, Nick J. Reynolds, P Marshall, M Elias, and Carla F. Newman

Subjects

Gene knockdown, business.industry, Cell Biology, Dermatology, Biochemistry, Hedgehog signaling pathway, Cell biology, Stress (mechanics), Skin equivalent, Medicine, business, Molecular Biology, Barrier function, Filaggrin

152. Wound Healing, Angiogenesis and Vascular Biology

Author

Darren L Johnson, Colin A.B. Jahoda, and Nick J. Reynolds

Subjects

Beta-catenin, biology, business.industry, Human skin, chemical and pharmacologic phenomena, Cell Biology, Dermatology, Biochemistry, Signalling, GSK-3, biology.protein, Cancer research, Medicine, Beta (finance), Wound healing, business, Molecular Biology

153. Differential Drug Survival of Biologic Therapies for the Treatment of Psoriasis: A Prospective Observational Cohort Study from the British Association of Dermatologists Biologic Interventions Register (BADBIR)

Author

Zenas Z N Yiu, Christopher E.M. Griffiths, Kathleen McElhone, C. M. Owen, Anthony Ormerod, A. David Burden, Jonathan Barker, Mark Lunt, Richard B. Warren, Darren M. Ashcroft, Catherine H. Smith, and Nick J. Reynolds

Subjects

Adult, Male, medicine.medical_specialty, Maximum Tolerated Dose, Kaplan-Meier Estimate, Dermatology, Biochemistry, Drug Administration Schedule, Etanercept, Cohort Studies, Psoriatic arthritis, Internal medicine, Ustekinumab, medicine, Adalimumab, Humans, Psoriasis, Prospective Studies, Registries, Molecular Biology, Societies, Medical, Proportional Hazards Models, Biological Products, Dose-Response Relationship, Drug, business.industry, Hazard ratio, Cell Biology, Dermatology Life Quality Index, Middle Aged, medicine.disease, Infliximab, Surgery, Discontinuation, Biological Therapy, Tolerability, Female, business, medicine.drug

Abstract

Drug survival reflects a drug's effectiveness, safety, and tolerability. We assessed the drug survival of biologics used to treat psoriasis in a prospective national pharmacovigilance cohort (British Association of Dermatologists Biologic Interventions Register (BADBIR)). The survival rates of the first course of biologics for 3,523 biologic-naive patients with chronic plaque psoriasis were compared using survival analysis techniques and predictors of discontinuation analyzed using a multivariate Cox proportional hazards model. Data for patients on adalimumab (n=1,879), etanercept (n=1,098), infliximab (n=96), and ustekinumab (n=450) were available. The overall survival rate in the first year was 77%, falling to 53% in the third year. Multivariate analysis showed that female gender (hazard ratio (HR) 1.22; 95% confidence interval (CI): 1.09-1.37), being a current smoker (HR 1.19; 95% CI: 1.03-1.38), and a higher baseline dermatology life quality index (HR 1.01; 95% CI: 1.00-1.02) were predictors of discontinuation. Presence of psoriatic arthritis (HR 0.82; 95% CI: 0.71-0.96) was a predictor for drug survival. As compared with adalimumab, patients on etanercept (HR 1.63; 95% CI: 1.45-1.84) or infliximab (HR 1.56; 95% CI: 1.16-2.09) were more likely to discontinue therapy, whereas patients on ustekinumab were more likely to persist (HR 0.48; 95% CI: 0.37-0.62). After accounting for relevant covariates, ustekinumab had the highest first-course drug survival. The results of this study will aid clinical decision making when choosing biologic therapy for psoriasis patients.

154. Up-Regulation of p21WAF1/CIP1 in Psoriasis and After the Application of Irritants and Tape Stripping

Author

Jonathan L. Rees, Elaine Doherty, Christine Campbell, Martin D. Smith, Eugene Healy, Nick J. Reynolds, and David K. Harrison

Subjects

Cyclin-Dependent Kinase Inhibitor p21, p53, proliferation, In situ hybridization, Dermatology, Biology, Biochemistry, Downregulation and upregulation, Epidermal growth factor, Cyclins, Physical Stimulation, Psoriasis, Dithranol, medicine, Humans, RNA, Messenger, Molecular Biology, neoplasms, Epidermis (botany), Kinase, Sodium Dodecyl Sulfate, Cell Biology, differentiation, Anthralin, medicine.disease, Cell biology, Immunology, Irritants, Epidermis, Tumor Suppressor Protein p53, Signal transduction, medicine.drug

Abstract

p21WAF1/CIP1 is a nucleoprotein that was initially characterized by its ability to be regulated transcriptionally by p53 and by its ability to mediate growth arrest by binding to cyclin-dependent kinases. Although p21WAF1/CIP1 is thought to mediate the effects of p53 in causing growth arrest, p21WAF1/CIP1 is also regulated in a p53-independent manner, e.g., during terminal differentiation of some cell lines. Growth factors including epidermal growth factor also induce p21WAF1/CIP1 through p53-independent pathways. Because the epidermal growth factor signaling pathway is abnormal in psoriatic epidermis, we studied p21WAF1/CIP1 expression, using in situ hybridization and immunohistochemistry, in psoriasis. Both p21WAF1/CIP1 mRNA and protein were significantly elevated in untreated psoriatic plaques compared with uninvolved psoriatic skin (p < 0.0001), with the up-regulation of p21WAF1/CIP1 being predominantly suprabasal. This increase was accompanied by a small increase in p53 protein expression of uncertain significance. Furthermore, p21WAF1/CIP1 expression was induced in skin after sellotape stripping and by the application of agents, such as dithranol, that are capable of inducing hyperproliferation. The pattern of p21WAF1/CIP1 expression observed is consistent with a role in induction and maintenance of differentiation. Our experiments, however, cannot determine whether the abnormalities of p21WAF1/CIP1 epidermal expression in psoriasis and after insult are independent of changes in p53 expression.

155. Epidermal Structure and Function

Author

H Long, BM Taal, M Donaldson, M Elias, and Nick J. Reynolds

Subjects

Epidermal barrier, Cell Biology, Dermatology, Biology, Biochemistry, Cell biology, medicine.anatomical_structure, Apoptosis, Immunology, medicine, Tonicity, Keratinocyte, Molecular Biology, Filaggrin

156. Lysophosphatidic Acid Promotes Cell Migration through STIM1- and Orai1-Mediated Ca2+i Mobilization and NFAT2 Activation

Author

Laura Mottram, Kehinde Ross, Nick J. Reynolds, AM Brown, Ralph Jans, Stephen Sikkink, and Darren L Johnson

Subjects

Keratinocytes, Male, ORAI1 Protein, Motility, Dermatology, Biology, Biochemistry, chemistry.chemical_compound, Cell Movement, Cyclosporin a, Lysophosphatidic acid, Humans, Calcium Signaling, Stromal Interaction Molecule 1, Molecular Biology, Cells, Cultured, Calcium signaling, Wound Healing, NFATC Transcription Factors, Calcineurin, Membrane Proteins, Cell migration, NFAT, Cell Biology, Neoplasm Proteins, Cell biology, chemistry, Calcium, Female, RNA Interference, Original Article, lipids (amino acids, peptides, and proteins), Calcium Channels, Lysophospholipids, Signal transduction, Signal Transduction

Abstract

Lysophosphatidic acid (LPA) enhances cell migration and promotes wound healing in vivo, but the intracellular signaling pathways regulating these processes remain incompletely understood. Here we investigated the involvement of agonist-induced Ca(2+) entry and STIM1 and Orai1 proteins in regulating nuclear factor of activated T cell (NFAT) signaling and LPA-induced keratinocyte cell motility. As monitored by Fluo-4 imaging, stimulation with 10 μM LPA in 60 μM Ca(2+)(o) evoked Ca(2+)(i) transients owing to store release, whereas addition of LPA in physiological 1.2 mM Ca(2+)(o) triggered store release coupled to extracellular Ca(2+) entry. Store-operated Ca(2+) entry (SOCE) was blocked by the SOCE inhibitor diethylstilbestrol (DES), STIM1 silencing using RNA interference (RNAi), and expression of dominant/negative Orai1(R91W). LPA induced significant NFAT activation as monitored by nuclear translocation of green fluorescent protein-tagged NFAT2 and a luciferase reporter assay, which was impaired by DES, expression of Orai1(R91W), and inhibition of calcineurin using cyclosporin A (CsA). By using chemotactic migration assays, LPA-induced cell motility was significantly impaired by STIM1, CsA, and NFAT2 knockdown using RNAi. These data indicate that in conditions relevant to epidermal wound healing, LPA induces SOCE and NFAT activation through Orai1 channels and promotes cell migration through a calcineurin/NFAT2-dependent pathway.

157. Elevated expression and genetic association links the SOCS3 gene to atopic dermatitis

Author

E Ekelund, J Link, SJ Meggitt, Ingrid Kockum, C.-F Wahlgren, Juha Kere, Erik Melén, Maria Bradley, Göran Pershagen, Magnus Nordenskjöld, Magnus Wickman, Jonathan Barker, A Sääf, Nick J. Reynolds, and M Tengvall-Linder

Subjects

Adult, Male, Allergy, Deception, Genetic Linkage, Gene Expression, Suppressor of Cytokine Signaling Proteins, Biology, Polymorphism, Single Nucleotide, Dermatitis, Atopic, Atopy, Report, Gene expression, medicine, Genetics, Humans, Genetics(clinical), RNA, Messenger, Gene, Genetics (clinical), Genetic association, Skin, Haplotype, digestive, oral, and skin physiology, Atopic dermatitis, medicine.disease, Physical Chromosome Mapping, Up-Regulation, body regions, Haplotypes, Suppressor of Cytokine Signaling 3 Protein, Immunology, Chromosomal region, Female, Chromosomes, Human, Pair 17

Abstract

In a systematic analysis of global gene-expression patterns, we found that SOCS3 messenger RNA was significantly more highly expressed in skin from patients with atopic dermatitis than in skin from healthy controls, and immunohistochemical analysis confirmed a similar elevation of SOCS3 protein. Furthermore, we found a genetic association between atopic dermatitis and a haplotype in the SOCS3 gene in two independent groups of patients (P

158. Differences in Clinical Features and Comorbid Burden between HLA-C∗06:02 Carrier Groups in >9,000 People with Psoriasis

Author

Konstantinos Douroudis, Ravi Ramessur, Ines A. Barbosa, David Baudry, Michael Duckworth, Caroline Angit, Francesca Capon, Raymond Chung, Charles J. Curtis, Paola Di Meglio, Jonathan M.R. Goulding, Christopher E.M. Griffiths, Sang Hyuck Lee, Satveer K. Mahil, Richard Parslew, Nick J. Reynolds, Alexa R. Shipman, Richard B. Warren, Zenas Z.N. Yiu, Michael A. Simpson, Jonathan N. Barker, Nick Dand, Catherine H. Smith, Ian Evans, Ruth Murphy, Tess McPherson, Elise Kleyn, Philip Laws, Gabrielle Becher, Anthony Bewley, Amir Rashid, Oras Alabas, Simon Morrison, Shehnaz Ahmed, Eleanor Pearson, Josh Richards, Teena Mackenzie, Brian Kirby, David Burden, Linda Lawson, Kathleen McElhone, Anthony Ormerod, Caroline Owen, Nadia Aldoori, Mahmud Ali, Alex Anstey, Fiona Antony, Charles Archer, Suzanna August, Periasamy Balasubramaniam, Kay Baxter, Alexandra Bonsall, Victoria Brown, Katya Burova, Aamir Butt, Mel Caswell, Sandeep Cliff, Mihaela Costache, Sharmela Darne, Emily Davies, Claudia DeGiovanni, Trupti Desai, Bernadette DeSilva, Victoria Diba, Eva Domanne, Harvey Dymond, Caoimhe Fahy, Leila Ferguson, Maria-Angeliki Gkini, Alison Godwin, Fiona Hammonds, Sarah Johnson, Teresa Joseph, Manju Kalavala, Mohsen Khorshid, Liberta Labinoti, Nicole Lawson, Alison Layton, Tara Lees, Nick Levell, Helen Lewis, Calum Lyon, Sandy McBride, Sally McCormack, Kevin McKenna, Serap Mellor, Paul Norris, Urvi Popli, Gay Perera, Nabil Ponnambath, Helen Ramsay, Aruni Ranasinghe, Saskia Reeken, Rebecca Rose, Rada Rotarescu, Ingrid Salvary, Kathy Sands, Tapati Sinha, Simina Stefanescu, Kavitha Sundararaj, Kathy Taghipour, Michelle Taylor, Michelle Thomson, Joanne Topliffe, Roberto Verdolini, Rachel Wachsmuth, Martin Wade, Shyamal Wahie, Sarah Walsh, Shernaz Walton, Louise Wilcox, and Andrew Wright

Subjects

medicine.medical_specialty, Endotype, HLA-C Antigens, Dermatology, Disease, Biochemistry, Psoriatic arthritis, Internal medicine, Psoriasis, medicine, Humans, Genetic Predisposition to Disease, Clinical significance, Expressivity (genetics), Molecular Biology, Alleles, business.industry, Cell Biology, Odds ratio, medicine.disease, Biobank, Cross-Sectional Studies, Female, business, Biomarkers

Abstract

The identification of robust endotypes—disease subgroups of clinical relevance—is fundamental to stratified medicine. We hypothesized that HLA-C∗06:02 status, the major genetic determinant of psoriasis, defines a psoriasis endotype of clinical relevance. Using two United Kingdom–based cross-sectional datasets—an observational severe-psoriasis study (Biomarkers of Systemic Treatment Outcomes in Psoriasis; n = 3,767) and a large population-based bioresource (UK Biobank, including n = 5,519 individuals with psoriasis)—we compared demographic, environmental, and clinical variables of interest in HLA-C∗06:02–positive (one or two copies of the HLA-C∗06:02 allele) with those in HLA-C∗06:02‒negative (no copies) individuals of European ancestry. We used multivariable regression analyses to account for mediation effects established a priori. We confirm previous observations that HLA-C∗06:02–positive status is associated with earlier age of psoriasis onset and extend findings to reveal an association with disease expressivity in females (Biomarkers of Systemic Treatment Outcomes in Psoriasis: P = 2.7 × 10 –14, UK Biobank: P = 1.0 × 10 –8). We also show HLA-C∗06:02–negative status to be associated with characteristic clinical features (large plaque disease, OR for HLA-C∗06:02 = 0.73, P = 7.4 × 10 –4; nail involvement, OR = 0.70, P = 2.4 × 10 –6); higher central adiposity (Biomarkers of Systemic Treatment Outcomes in Psoriasis: waist circumference difference of 2.0 cm, P = 8.4 × 10 –4; UK Biobank: waist circumference difference of 1.4 cm, P = 1.5 × 10 –4), especially in women; and a higher prevalence of other cardiometabolic comorbidities. These findings extend the clinical phenotype delineated by HLA-C∗06:02 and highlight its potential as an important biomarker to consider in future multimarker stratified medicine approaches.

159. Ethnic differences in early onset multimorbidity and associations with health service use, long-term prescribing, years of life lost, and mortality: A cross-sectional study using clustering in the UK Clinical Practice Research Datalink.

Author

Fabiola Eto, Miriam Samuel, Rafael Henkin, Meera Mahesh, Tahania Ahmad, Alisha Angdembe, R Hamish McAllister-Williams, Paolo Missier, Nick J Reynolds, Michael R Barnes, Sally Hull, Sarah Finer, and Rohini Mathur

Subjects

Medicine

Abstract

BackgroundThe population prevalence of multimorbidity (the existence of at least 2 or more long-term conditions [LTCs] in an individual) is increasing among young adults, particularly in minority ethnic groups and individuals living in socioeconomically deprived areas. In this study, we applied a data-driven approach to identify clusters of individuals who had an early onset multimorbidity in an ethnically and socioeconomically diverse population. We identified associations between clusters and a range of health outcomes.Methods and findingsUsing linked primary and secondary care data from the Clinical Practice Research Datalink GOLD (CPRD GOLD), we conducted a cross-sectional study of 837,869 individuals with early onset multimorbidity (aged between 16 and 39 years old when the second LTC was recorded) registered with an English general practice between 2010 and 2020. The study population included 777,906 people of White ethnicity (93%), 33,915 people of South Asian ethnicity (4%), and 26,048 people of Black African/Caribbean ethnicity (3%). A total of 204 LTCs were considered. Latent class analysis stratified by ethnicity identified 4 clusters of multimorbidity in White groups and 3 clusters in South Asian and Black groups. We found that early onset multimorbidity was more common among South Asian (59%, 33,915) and Black (56% 26,048) groups compared to the White population (42%, 777,906). Latent class analysis revealed physical and mental health conditions that were common across all ethnic groups (i.e., hypertension, depression, and painful conditions). However, each ethnic group also presented exclusive LTCs and different sociodemographic profiles: In White groups, the cluster with the highest rates/odds of the outcomes was predominantly male (54%, 44,150) and more socioeconomically deprived than the cluster with the lowest rates/odds of the outcomes. On the other hand, South Asian and Black groups were more socioeconomically deprived than White groups, with a consistent deprivation gradient across all multimorbidity clusters. At the end of the study, 4% (34,922) of the White early onset multimorbidity population had died compared to 2% of the South Asian and Black early onset multimorbidity populations (535 and 570, respectively); however, the latter groups died younger and lost more years of life. The 3 ethnic groups each displayed a cluster of individuals with increased rates of primary care consultations, hospitalisations, long-term prescribing, and odds of mortality. Study limitations include the exclusion of individuals with missing ethnicity information, the age of diagnosis not reflecting the actual age of onset, and the exclusion of people from Mixed, Chinese, and other ethnic groups due to insufficient power to investigate associations between multimorbidity and health-related outcomes in these groups.ConclusionsThese findings emphasise the need to identify, prevent, and manage multimorbidity early in the life course. Our work provides additional insights into the excess burden of early onset multimorbidity in those from socioeconomically deprived and diverse groups who are disproportionately and more severely affected by multimorbidity and highlights the need to ensure healthcare improvements are equitable.

Published

2023