ISG20L2: an RNA nuclease regulating T cell activation

ISG20L2:一种调节T细胞活化的RNA核酸酶

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作者:Ana Rodríguez-Galán, Sara G Dosil, Anna Hrčková, Lola Fernández-Messina, Zuzana Feketová, Julie Pokorná, Irene Fernández-Delgado, Emilio Camafeita, Manuel José Gómez, Marta Ramírez-Huesca, Cristina Gutiérrez-Vázquez, Fátima Sánchez-Cabo, Jesús Vázquez, Štěpánka Vaňáčová, Francisco Sánchez-Madrid

Abstract

ISG20L2, a 3' to 5' exoribonuclease previously associated with ribosome biogenesis, is identified here in activated T cells as an enzyme with a preferential affinity for uridylated miRNA substrates. This enzyme is upregulated in T lymphocytes upon TCR and IFN type I stimulation and appears to be involved in regulating T cell function. ISG20L2 silencing leads to an increased basal expression of CD69 and induces greater IL2 secretion. However, ISG20L2 absence impairs CD25 upregulation, CD3 synaptic accumulation and MTOC translocation towards the antigen-presenting cell during immune synapsis. Remarkably, ISG20L2 controls the expression of immunoregulatory molecules, such as AHR, NKG2D, CTLA-4, CD137, TIM-3, PD-L1 or PD-1, which show increased levels in ISG20L2 knockout T cells. The dysregulation observed in these key molecules for T cell responses support a role for this exonuclease as a novel RNA-based regulator of T cell function.

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