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  1. Attività

TITOLO: Epigenetics and microRNAs in Myocardial Function and Disease (CARDIOEPIGEN)

Progetto
Heart failure (HF) is the ultimate outcome of many cardiovascular diseases. Re-expression of fetal genes in the adult heart contributes to development of HF. Two mechanisms involved in the control of gene expression are epigenetics and microRNAs (miRs). We propose a project on epigenetic and miR-mediated mechanisms leading to HF. Epigenetics refers to heritable modification of DNA and histones that does not modify the genetic code. Depending on the type of modification and on the site affected, these chemical changes up- or down-regulate transcription of specific genes. Despite it being a major player in gene regulation, epigenetics has been only partly investigated in HF. miRs are regulatory RNAs that target mRNAs for inhibition. Dysregulation of the cardiac miR signature occurs in HF. miR expression may itself be under epigenetic control, constituting a miR-epigenetic regulatory network. To our knowledge, this possibility has not been studied yet. Our specific hypothesis is that the profile of DNA/histone methylation and the cross-talk between epigenetic enzymes and miRs have fundamental roles in defining the characteristics of cells during cardiac development and that the dysregulation of these processes determines the deleterious nature of the stressed hearts gene programme. We will test this first through a genome-wide study of DNA/histone methylation to generate maps of the main methylation modifications occurring in the genome of cardiac cells treated with a pro-hypertrophy regulator and of a HF model. We will then investigate the role of epigenetic enzymes deemed important in HF, through the generation and study of knockout mice models. Finally, we will test the possible therapeutic potential of modulating epigenetic genes. We hope to further understand the pathological mechanisms leading to HF and to generate data instrumental to the development of diagnostic and therapeutic strategies for this disease.
  • Dati Generali
  • Pubblicazioni

Dati Generali

Partecipanti

LOCATI MASSIMO   Responsabile scientifico  

Dipartimenti coinvolti

Dipartimento di Biotecnologie Mediche e Medicina Traslazionale   Principale  

Tipo

7PQ_ERC - 7 Programma Quadro_European Research Coucil

Finanziatore

EUROPEAN COMMISSION
Organizzazione Esterna Ente Finanziatore

Capofila

IRCCS - HUMANITAS MIRASOLE S.P.A. (IRIS)

Periodo di attività

Ottobre 1, 2012 - Settembre 30, 2017

Durata progetto

60 mesi

Pubblicazioni

Pubblicazioni (9)

Dietary essential amino acids for the treatment of heart failure with reduced ejection fraction 
CARDIOVASCULAR RESEARCH
OXFORD UNIVERSITY PRESS
2023
Articolo
Open Access
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Myocardial hypoxic stress mediates functional cardiac extracellular vesicle release 
EUROPEAN HEART JOURNAL
OXFORD UNIVERSITY PRESS
2021
Articolo
Reserved Access
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Epigenetic modifications and noncoding RNAs in cardiac hypertrophy and failure 
NATURE REVIEWS. CARDIOLOGY
NATURE PUBLISHING GROUP
2015
Articolo
Reserved Access
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Long noncoding RNAs and microRNAs in cardiovascular pathophysiology 
CIRCULATION RESEARCH
LIPPINCOTT WILLIAMS AND WILKINS
2015
Articolo
Reserved Access
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MicroRNAs in cardiovascular disease: an introduction for clinicians 
HEART
BMJ PUBLISHING GROUP
2015
Articolo
Reserved Access
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RNA (Epi)genetics in cardiovascular diseases 
JOURNAL OF MOLECULAR AND CELLULAR CARDIOLOGY
ELSEVIER
2015
Articolo
Reserved Access
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TGFβ triggers miR-143/145 transfer from smooth muscle cells to endothelial cells, thereby modulating vessel stabilization 
CIRCULATION RESEARCH
LIPPINCOTT WILLIAMS AND WILKINS
2015
Articolo
Reserved Access
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Therapeutic applications of noncoding RNAs 
CURRENT OPINION IN CARDIOLOGY
LIPPINCOTT WILLIAMS AND WILKINS
2015
Articolo
Reserved Access
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Post-natal cardiomyocytes can generate iPS cells with an enhanced capacity toward cardiomyogenic re-differentation 
CELL DEATH AND DIFFERENTIATION
NATURE PUBLISHING GROUP
2012
Articolo
Open Access
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Realizzato con VIVO | Progettato da Cineca | 25.11.5.0