Looking for final effectors of regulome alterations in MS: LMP1-mediated dysregulation of AID in MS pathogenesis

Anno
2021
Proponente Marco Salvetti - Professore Ordinario
Sottosettore ERC del proponente del progetto
LS5_7
Componenti gruppo di ricerca
Componente Categoria
Rachele Bigi Componenti strutturati del gruppo di ricerca
Giuliano Sette Componenti strutturati del gruppo di ricerca
Abstract

While our understanding of multiple sclerosis (MS) pathophysiology increases, the definition of the etiology of the disease remains an unmet need. As most multifactorial diseases, elusive regulome alterations are part of the problem.
Over the years we have tried to combine genetic, epidemiological and immunological information to understand how this complex picture is funneled into specific (therapeutically actionable) pathophysiological mechanism in MS. As detailed in the proposal, our data and those from other research groups, suggest that a significant part of this complex dysregulation converges on the CD40 pathway, a master regulator of B lymphocyte responses. However, key mechanistic implications of the CD40 dysregulation remain unclear. For example, the CD40 downregulation that comes along with the MS-associated CD40 risk allele appears paradoxical, distinguishes MS from many other autoimmune diseases where it goes in the opposite direction and suggests caution with respect to therapies targeting this pathway. Hence, it is urgent to expand our knowledge about these mechanisms (CD40L antagonists are progressing from phase 2 to phase 3 clinical trials).
We will investigate whether the CD40 dysregulation may be better understood taking into account possible effectors of another master regulator of the pathway (which is implicated in MS etiology), namely Epstein-Barr virus (EBV). Based on preliminary and published data we will try to understand whether and how LMP1, an EBV protein and CD40 mimic, concurs with CD40 in regulating the activity of activation-induced deaminase (AID), a major driver of acquired gene expression variability, and a master regulator of the B cell response, known to be under the control of the CD40 pathway. If confirmed, this may represent a mechanism that amplifies and sustains the regulome dysfunction in B cell response that is so relevant for MS.

ERC
LS1_10, LS6_3, LS6_5
Keywords:
NEUROSCIENZE, BIOLOGIA MOLECOLARE E INTERAZIONI, VIROLOGIA

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