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Lymphocyte microRNAs in health and disease: Understanding lymphocyte functions through the identification of microRNA target genes and exploiting serum microRNA signatures to monitor immune responses

Progetto
Background: CD4+ T lymphocyte subsets orchestrate immune responses in health and disease. Little is known on control of T cell differentiation exerted by microRNA that affect mRNA translation. The identification of microRNA and their targets that regulate differentiation of T cell subsets may provide new therapeutic targets for immune-mediated diseases. Since microRNA are released in exosomes and circulate in blood, activities of tissue-derived lymphocytes could be assessed by microRNA signatures in the serum. We have defined microRNAs present in resting lymphocyte subsets from peripheral blood and measured lymphocyte-derived microRNAs in the serum. We have also solved important challenges for the identification of microRNA targets, the definition of signatures of activated T cells and their monitoring in the serum, which form the key topics of this application. Advancing State-of-the-Art and objectives: We will identify microRNA of CD4+ T cell subsets purified from inflamed organs and investigate microRNA target network that regulates T cell differentiation. We will exploit this knowledge to profile signatures of in vivo activated T cells and to map genes that could improve understanding of T cell commitment. We will also develop quantitative assays to monitor microRNA signatures in the serum and provide functional evidence of key genes targeted by microRNA which could be targets of immunomodulatory drugs. Significance: This application addresses important challenges at the frontiers of immunology and could lead to significant advances in immunotherapies and diagnostic tools for patients with immune mediated diseases. New ways of identifying microRNA targets and techniques to quantify microRNA signatures in the serum, could be widely applicable in biomedical research.
  • Dati Generali
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Dati Generali

Partecipanti

ABRIGNANI SERGIO   Responsabile scientifico  

Dipartimenti coinvolti

Dipartimento di Scienze Cliniche e di Comunità   Principale  

Tipo

7PQ_ERC - 7 Programma Quadro_European Research Coucil

Finanziatore

EUROPEAN COMMISSION
Organizzazione Esterna Ente Finanziatore

Capofila

UNIVERSITA' DEGLI STUDI DI MILANO

Periodo di attività

Giugno 1, 2015 - Maggio 31, 2016

Durata progetto

12 mesi

Pubblicazioni

Pubblicazioni (2)

Extracellular MicroRNA signature of human helper T cell subsets in health and autoimmunity 
THE JOURNAL OF BIOLOGICAL CHEMISTRY
AMERICAN SOCIETY FOR BIOCHEMISTRY AND MOLECULAR BIOLOGY
2017
Articolo
Reserved Access
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The long intergenic noncoding RNA landscape of human lymphocytes highlights the regulation of T cell differentiation by linc-MAF-4 
NATURE IMMUNOLOGY
NATURE
2015
Articolo
Open Access
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Realizzato con VIVO | Progettato da Cineca | 25.11.5.0