Publications by authors named "N Garrido-Mesa"

The gut microbiota plays a role in energy homeostasis: its composition differs in lean and obese mice and may impact insulin sensitivity. The immune system has co-evolved with the gut microbiota, but direct regulation of microbial communities by the immune system and its metabolic impact is unclear. Mice lacking the immune cell specific transcription factor T-bet (Tbx21) are insulin sensitive.

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Introduction: Drug repurposing can be a successful approach to deal with the scarcity of cost-effective therapies in situations such as the COVID-19 pandemic. Tetracyclines have previously shown efficacy in preclinical acute respiratory distress syndrome (ARDS) models and initial predictions and experimental reports suggest a direct antiviral activity against SARS-CoV2. Furthermore, a few clinical reports indicate their potential in COVID-19 patients.

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Article Synopsis
  • - T-bet is a key transcription factor for CD4 T 1 cells and is also present in other CD4 T cell types, but its role in their differentiation and function is not fully understood.
  • - To investigate T-bet expression, researchers tracked its presence using a special mouse model, revealing a unique subset of CD4 T cells that show naïve cell features while being distinct from traditional naïve and memory T cells.
  • - These T-bet-experienced cells are inclined to develop into T 1 cells, produce a specific cytokine called IFN-γ upon activation, and are less likely to change into other T cell types, indicating that lineage factors can influence T cell responses even without standard activation markers.
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Innate lymphoid cells (ILCs) play an important role in regulating immune responses at mucosal surfaces. The transcription factor T-bet is crucial for the function of ILC1s and NCR ILC3s and constitutive deletion of T-bet prevents the development of these subsets. Lack of T-bet in the absence of an adaptive immune system causes microbiota-dependent colitis to occur due to aberrant ILC3 responses.

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