Your search keyword '"Karen, Leavens"' showing total 8 results

1. Depletion of LAG‐3 + T Cells Translated to Pharmacology and Improvement in Psoriasis Disease Activity: A Phase I Randomized Study of mAb GSK2831781

Author

Christopher J. Delves, Caroline O. S. Savage, Tim S. Schmidt, Lea Fortunato, Emilie Charles, Thomas Matthew Webb, Lia Liefaard, Nicolas Wisniacki, John Stone, Rainard Fuhr, Sara Brett, Stephen A. Hughes, Ruth M. Tarzi, Muna Albayaty, Christine Barrett, Ken Edwards, Karen Leavens, Katherine Nevin, Rabia Anselm, Joanne Ellis, Shuo Tang, Martin Coenen, T.G. Hopkins, N Srinivasan, Yi Cui, Daniel J.B. Marks, Anna Richards, and Maria Feeney

Subjects

Pharmacology, Antibody-dependent cell-mediated cytotoxicity, business.industry, GSK2831781, T cell, medicine.disease, 030226 pharmacology & pharmacy, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Tolerability, 030220 oncology & carcinogenesis, Psoriasis, medicine, Pharmacology (medical), business, Receptor, CD8

Abstract

Activated T cells drive a range of immune-mediated inflammatory diseases. LAG-3 is transiently expressed on recently activated CD4+ and CD8+ T cells. We describe the engineering and first-in-human clinical study (NCT02195349) of GSK2831781 (an afucosylated humanized IgG1 monoclonal antibody enhanced with high affinity for Fc receptors and LAG-3 and antibody-dependent cellular cytotoxicity capabilities), which depletes LAG-3 expressing cells. GSK2831781 was tested in a phase I/Ib, double-blind, placebo-controlled clinical study, which randomized 40 healthy participants (part A) and 27 patients with psoriasis (part B) to single doses of GSK2831781 (up to 0.15 and 5 mg/kg, respectively) or placebo. Adverse events were generally balanced across groups, with no safety or tolerability concern identified. LAG-3+ cell depletion in peripheral blood was observed at doses ≥ 0.15 mg/kg and was dose-dependent. In biopsies of psoriasis plaques, a reduction in mean group LAG-3+ and CD3+ T-cell counts was observed following treatment. Downregulation of proinflammatory genes (IL-17A, IL-17F, IFNγ, and S100A12) and upregulation of the epithelial barrier integrity gene, CDHR1, was observed with the 5 mg/kg dose of GSK2831781. Psoriasis disease activity improved up to day 43 at all GSK2831781 doses (0.5, 1.5, and 5 mg/kg) compared with placebo. Depletion of LAG-3-expressing activated T cells is a novel approach, and this first clinical study shows that GSK2831781 is pharmacologically active and provides encouraging early evidence of clinical effects in psoriasis, which warrants further investigation in T-cell-mediated inflammatory diseases.

Published

2020

2. Lymphocyte Activation Gene (LAG)-3 Is Associated With Mucosal Inflammation and Disease Activity in Ulcerative Colitis

Author

Karen Leavens, Lucy C. Garner, Stephen A. Hughes, Kevin R. Page, D Krull, Stephanie Slevin, Kate D. Lynch, Ruth M. Tarzi, Carolina V. Arancibia-Cárcamo, Malcolm Tan, Conor Lahiff, B Greenaway, Katherine Nevin, Simon Travis, Helen Ferry, Alessandra Geremia, Lai Mun Wang, Satish Keshav, Marks Djb., Paul Klenerman, and N Srinivasan

Subjects

0301 basic medicine, LAG3, medicine.medical_treatment, T cell, Inflammation, Lymphocyte Activation, Severity of Illness Index, 03 medical and health sciences, 0302 clinical medicine, Immune system, Drug Development, Antigens, CD, T-Lymphocyte Subsets, LAG-3, Medicine, Humans, Intestinal Mucosa, immune checkpoint, AcademicSubjects/MED00260, ulcerative colitis, business.industry, Gastroenterology, Patient Acuity, FOXP3, Endoscopy, General Medicine, Original Articles, Mixed lymphocyte reaction, Immune Checkpoint Proteins, Eccojc/1020, Lymphocyte Activation Gene 3 Protein, Immune checkpoint, Eccojc/1000, 030104 developmental biology, Cytokine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, Colitis, Ulcerative, medicine.symptom, business

Abstract

Background and Aims Lymphocyte activation gene [LAG]-3 is an immune checkpoint and its expression identifies recently activated lymphocytes that may contribute to inflammation. We investigated the role of LAG-3 by analysing its expression and function in immune cells from blood and tissue of patients with ulcerative colitis [UC]. Methods The phenotypic properties of LAG-3+ T cells were determined by flow cytometry, qRT-PCR and single-cell RNA-sequencing. LAG-3+ cells were quantified and correlated with disease activity. The functional effects of LAG-3+ cells were tested using a depleting anti-LAG-3 monoclonal antibody [mAb] in a mixed lymphocyte reaction [MLR]. Results LAG-3+ cells in the blood were negligible. LAG-3+ lymphocytes were markedly increased in inflamed mucosal tissue and both frequencies of LAG-3+ T cells and transcript levels of LAG3 correlated with endoscopic severity. LAG-3 expression was predominantly on effector memory T cells, and single-cell RNA-sequencing revealed LAG3 expression in activated and cytokine-producing T cell subsets. Foxp3+CD25hi Tregs also expressed LAG-3, although most mucosal Tregs were LAG-3−. Mucosal LAG-3+ cells produced mainly interferon γ [IFNγ] and interleukin-17A. LAG-3+ cell numbers decreased in patients who responded to biologics, and remained elevated in non-responders. Treatment with a depleting anti-LAG-3 mAb led to a reduction in proliferation and IFNγ production in an MLR. Conclusions LAG-3+ cells are increased in the inflamed mucosa, predominantly on effector memory T cells with an activated phenotype and their cell numbers positively correlate with disease activity. Depleting LAG-3 eliminates activated proliferating T cells, and hence LAG-3 could be a therapeutic target in UC.

Published

2020

3. Depletion of LAG-3

Author

Joanne, Ellis, Daniel, J B Marks, Naren, Srinivasan, Christine, Barrett, Thomas G, Hopkins, Anna, Richards, Rainard, Fuhr, Muna, Albayaty, Martin, Coenen, Lia, Liefaard, Karen, Leavens, Katherine L, Nevin, Shuo, Tang, Stephen A, Hughes, Léa, Fortunato, Ken, Edwards, Yi, Cui, Rabia, Anselm, Christopher J, Delves, Emilie, Charles, Maria, Feeney, Thomas M, Webb, Sara J, Brett, Tim S, Schmidt, John, Stone, Caroline O S, Savage, Nicolas, Wisniacki, and Ruth M, Tarzi

Subjects

Adult, Male, CD3 Complex, T-Lymphocytes, Research, Dose-Response Relationship, Immunologic, Antibodies, Monoclonal, Articles, Middle Aged, Lymphocyte Activation Gene 3 Protein, Article, Treatment Outcome, Gene Expression Regulation, Antigens, CD, Humans, Psoriasis, Female

Abstract

Activated T cells drive a range of immune‐mediated inflammatory diseases. LAG‐3 is transiently expressed on recently activated CD4+ and CD8+ T cells. We describe the engineering and first‐in‐human clinical study (NCT02195349) of GSK2831781 (an afucosylated humanized IgG1 monoclonal antibody enhanced with high affinity for Fc receptors and LAG‐3 and antibody‐dependent cellular cytotoxicity capabilities), which depletes LAG‐3 expressing cells. GSK2831781 was tested in a phase I/Ib, double‐blind, placebo‐controlled clinical study, which randomized 40 healthy participants (part A) and 27 patients with psoriasis (part B) to single doses of GSK2831781 (up to 0.15 and 5 mg/kg, respectively) or placebo. Adverse events were generally balanced across groups, with no safety or tolerability concern identified. LAG‐3+ cell depletion in peripheral blood was observed at doses ≥ 0.15 mg/kg and was dose‐dependent. In biopsies of psoriasis plaques, a reduction in mean group LAG‐3+ and CD3+ T‐cell counts was observed following treatment. Downregulation of proinflammatory genes (IL‐17A, IL‐17F, IFNγ, and S100A12) and upregulation of the epithelial barrier integrity gene, CDHR1, was observed with the 5 mg/kg dose of GSK2831781. Psoriasis disease activity improved up to day 43 at all GSK2831781 doses (0.5, 1.5, and 5 mg/kg) compared with placebo. Depletion of LAG‐3‐expressing activated T cells is a novel approach, and this first clinical study shows that GSK2831781 is pharmacologically active and provides encouraging early evidence of clinical effects in psoriasis, which warrants further investigation in T‐cell‐mediated inflammatory diseases.

Published

2020

4. Discovery of GW870086: a potent anti-inflammatory steroid with a unique pharmacological profile

Author

Deborah Needham, Jason A. Holt, Stuart N. Farrow, Robert J. H. Austin, Keith Biggadike, Karen Leavens, Iain Uings, Davina C. Angell, Michael V. Haase, and Joyce Lesley Matthews

Subjects

Pharmacology, Regulation of gene expression, Gene expression profiling, Reporter gene, Transactivation, Cell culture, medicine, Biology, Glucocorticoid, Allergic inflammation, Transrepression, medicine.drug

Abstract

Background and Purpose Glucocorticoids are highly effective therapies for a range of inflammatory diseases. Advances in the understanding of the diverse molecular mechanisms underpinning glucocorticoid action suggest that anti-inflammatory molecules with reduced side effect liabilities can be discovered. Here we set out to explore whether modification of the 17α position of the steroid nucleus could generate molecules with a unique pharmacological profile and to determine whether such molecules would retain anti-inflammatory activity. Experimental Approach The pharmacological properties of GW870086 were compared with fluticasone propionate (FP) using a range of cellular and in vivo model systems, including extensive gene expression profiling. Key Results GW870086 repressed inflammatory cytokine release from lung epithelial cells in a similar manner to FP but antagonized the effect of dexamethasone on MMTV-driven reporter gene transactivation. GW870086 had a strong effect on the expression of some glucocorticoid-regulated genes (such as PTGS2), while having minimal impact on the expression of other known target genes (such as SGK). GW870086 retained the ability to strengthen tight junctions in epithelial cell culture but, unlike FP, was unable to protect the culture from elastase-mediated damage. In murine models of irritant-induced contact dermatitis and ovalbumin-induced allergic inflammation, GW870086 showed comparable anti-inflammatory efficacy to FP. Conclusion and Implications GW870086 is a potent anti-inflammatory compound with a unique ability to regulate only a subset of those genes that are normally affected by classical glucocorticoids. It has the potential to become a new topical steroid with a different safety profile to existing therapies.

Published

2013

5. The utility of pharmacokinetic–pharmacodynamic modeling in the discovery and optimization of selective S1P1agonists

Author

Nigel Deeks, Karen Leavens, Aarti Patel, Colin A. Campbell, Helen Garden, Jenni Cryan, Emmanuel Hubert Demont, Simon Taylor, Jason Witherington, Pam Gaskin, Andrea C. Haynes, Simon J. Dowell, Robert Willis, James Gray, and Mary A. Morse

Subjects

Male, Agonist, medicine.drug_class, Health, Toxicology and Mutagenesis, Pharmacology, Biology, Toxicology, Biochemistry, Multiple Sclerosis, Relapsing-Remitting, Pharmacokinetics, GTP-Binding Proteins, Sphingosine, In vivo, medicine, Animals, Potency, Lymphocytes, PK/PD models, Arrestin, Fingolimod Hydrochloride, Drug discovery, Rats, Inbred Strains, General Medicine, Fingolimod, Rats, Propylene Glycols, Pharmacodynamics, Lysophospholipids, Signal Transduction, medicine.drug

Abstract

Sphingosine-1-phosphate (S1P(1)) receptor agonists such as Fingolimod (FTY-720) are a novel class of immunomodulators that have clinical utility in the treatment of remitting relapsing multiples sclerosis. This class of compound act by inducing peripheral lymphopenia. Using an integrated pharmacokinetic/pharmacodynamic (PK-PD) approach based on an in vivo rat model, novel S1P(1) agonists were identified with a predicted more rapid rate of reversibility of lymphocyte reduction in human compared to Fingolimod. The in vivo potency of 15 compounds based on PK-PD modelling of the rat lymphocyte reduction model was correlated with in vitro measures of potency at the S1P(1) receptor using β arrestin recruitment and G-protein signalling. A structurally novel S1P(1) agonist was identified and predictions of human pharmacokinetics and clinical dose are presented.

Published

2012

6. Discovery of GSK143, a highly potent, selective and orally efficacious spleen tyrosine kinase inhibitor

Author

Philip Alan Skone, Donald O. Somers, Marion C. Dickson, Nick Smithers, Ann Louise Walker, Thomas George Christopher Hayhow, Stuart G. Leach, Karen Leavens, Clement Douault, Emma J. Jones, Dorothy Elwes, Robert J. Watson, Margarete Neu, Robert P. Davis, Matthew Gray, Neil Stuart Garton, Clare I. Hobbs, Alex Preston, Michael David Barker, Vipulkumar Kantibhai Patel, Cesar Ramirez-Molina, Paul S. Carter, Scott McCleary, Gordon G. Weingarten, Huw D. Lewis, Francis Louis Atkinson, John Liddle, Tracy Jane Shipley, and Neil R. Curtis

Subjects

Models, Molecular, medicine.drug_class, Clinical Biochemistry, hERG, Anti-Inflammatory Agents, Administration, Oral, Pharmaceutical Science, Syk, Carboxamide, Pharmacology, Crystallography, X-Ray, Biochemistry, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Arthus Reaction, medicine, Animals, Humans, Syk Kinase, Tyrosine, Protein Kinase Inhibitors, Molecular Biology, Aniline Compounds, biology, Arthus reaction, Drug discovery, Kinase, Organic Chemistry, Intracellular Signaling Peptides and Proteins, Protein-Tyrosine Kinases, medicine.disease, Rats, Pyrimidines, Diaminopyrimidine, chemistry, biology.protein, Molecular Medicine

Abstract

The lead optimisation of the diaminopyrimidine carboxamide series of spleen tyrosine kinase inhibitors is described. The medicinal chemistry strategy was focused on optimising the human whole blood activity whilst achieving a sufficient margin over liability kinases and hERG activity. GSK143 is a potent and highly selective SYK inhibitor showing good efficacy in the rat Arthus model.

Published

2011

7. DOP11 Lymphocyte activation gene (LAG)-3 on T cells is a potential therapeutic target in ulcerative colitis

Author

Ruth M. Tarzi, B Greenaway, Marks Djb., Stephen A. Hughes, Katherine Nevin, S Slevin, Kate D. Lynch, M Tan, N Srinivasan, Simon Travis, Conor Lahiff, Satish Keshav, Karen Leavens, Alessandra Geremia, Lai Mun Wang, and C Arancibia

Subjects

business.industry, Immunology, Gastroenterology, medicine, Lymphocyte activation, General Medicine, medicine.disease, business, Gene, Ulcerative colitis

Published

2019

8. P449 Selective depletion of LAG3+ cells in T-cell-driven inflammation: a randomised, double-blind, placebo-controlled, FTIH phase I/Ib clinical trial

Author

Katherine Nevin, Karen Leavens, D Marks, Martin Coenen, J Stone, R Anselm, Anna Richards, Lia Liefaard, Stephen A. Hughes, N Srinivasan, Ruth M. Tarzi, Tim S. Schmidt, Rainard Fuhr, Nicolas Wisniacki, Muna Albayaty, Christine Barrett, Ken Edwards, T.G. Hopkins, S Tang, Joanne Ellis, and Caroline O. S. Savage

Subjects

medicine.medical_specialty, LAG3, business.industry, T cell, Gastroenterology, Inflammation, General Medicine, Placebo, Double blind, Clinical trial, medicine.anatomical_structure, Internal medicine, Phase (matter), Medicine, medicine.symptom, business

Published

2019