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CD4+ Regulatory T cells (Tregs) are crucial to maintain tolerance, balancing effector T cell responses to harmful agents and suppressing unwanted responses. However, too little control may lead to autoimmunity (e.g. juvenile idiopathic arthritis or type 1 diabetes), while too much control may contribute to the development of cancers. Co-stimulatory and co-inhibitory receptors are crucial to determine functional outcomes upon activation. We found an imbalance of co-receptor expression at the site of inflammation and mutations in co-receptor genes have been associated with autoimmunity.
We focus on the co-receptor family CD226, TIGIT and CD96; receptors highly expressed on Tregs but with little understanding of their function. We use cellular and molecular immunology techniques, including the cutting-edge gene-editing system CRISPR-Cas9, to elucidate the CD226, TIGIT and CD96 signalling, receptor-receptor and receptor-ligand interactions and study their role in primary human Treg function in health and disease.
CD4+ Regulatory T cells (Tregs) are crucial to maintain tolerance, balancing effector T cell responses to harmful agents and suppressing unwanted responses. However, too little control may lead to autoimmunity (e.g. juvenile idiopathic arthritis or type 1 diabetes), while too much control may contribute to the development of cancers. Co-stimulatory and co-inhibitory receptors are crucial to determine functional outcomes upon activation. We found an imbalance of co-receptor expression at the site of inflammation and mutations in co-receptor genes have been associated with autoimmunity.
We focus on the co-receptor family CD226, TIGIT and CD96; receptors highly expressed on Tregs but with little understanding of their function. We use cellular and molecular immunology techniques, including the cutting-edge gene-editing system CRISPR-Cas9, to elucidate the CD226, TIGIT and CD96 signalling, receptor-receptor and receptor-ligand interactions and study their role in primary human Treg function in health and disease.
Research Interests
Papers共 54 篇Author StatisticsCo-AuthorSimilar Experts
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Meryl H. Attrill, Diana Shinko, Telma Martins Viveiros,Martina Milighetti,Nina M. de Gruijter,Bethany Jebson,Melissa Kartawinata,Elizabeth C. Rosser,Lucy R. Wedderburn, CHARMS study, JIAP study,Anne M. Pesenacker
crossref(2024)
Meryl H. Attrill, Diana Shinko, Vicky Alexiou,Melissa Kartawinata,Lucy R. Wedderburn,Anne M. Pesenacker
Clinical and experimental immunologyno. 3 (2024): 221-241
AMERICAN JOURNAL OF TRANSPLANTATIONno. 6 (2023): S639-S639
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AMERICAN JOURNAL OF TRANSPLANTATIONno. 6 (2023): S481-S482
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British journal of surgeryno. Supplement_3 (2023)
Immunotherapy advancesno. 1 (2022)
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Thomas Andrew Fox,Benjamin Christopher Houghton,Lina Petersone,Erin Waters,Natalie Mona Edner, Alex McKenna,Olivier Preham,Claudia Hinze,Cayman Williams,Adriana Silva de Albuquerque,Alan Kennedy,Anne Maria Pesenacker,Pietro Genovese,Lucy Sarah Kate Walker,Siobhan Oisin Burns,David Michael Sansom,Claire Booth,Emma Catherine Morris
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Author Statistics
#Papers: 54
#Citation: 959
H-Index: 22
G-Index: 30
Sociability: 6
Diversity: 3
Activity: 22
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