Lysosomes have a central role in the disposal of extracellular and intracellular cargo and also function as metabolic sensors and signalling platforms in the immunometabolic reprogramming of macrophages and other immune cells in atherosclerosis. Lysosomes can rapidly sense the presence of nutrients within immune cells, thereby switching from catabolism of extracellular material to the recycling of intracellular cargo. Such a fine-tuned degradative response supports the generation of metabolic building blocks through effectors such as mTORC1 or TFEB. By coupling nutrients to downstream signalling and metabolism, lysosomes serve as a crucial hub for cellular function in innate and adaptive immune cells. Lysosomal dysfunction is now recognized to be a hallmark of atherogenesis. Perturbations in nutrient-sensing and signalling have profound effects on the capacity of immune cells to handle cholesterol, perform phagocytosis and efferocytosis, and limit the activation of the inflammasome and other inflammatory pathways. Strategies to improve lysosomal function hold promise as novel modulators of the immunoinflammatory response associated with atherosclerosis. In this Review, we describe the crosstalk between lysosomal biology and immune cell function and polarization, with a particular focus on cellular immunometabolic reprogramming in the context of atherosclerosis.In this Review, the authors describe the bidirectional crosstalk between lysosome biology and immune cell function and polarization, focusing on immunometabolic reprogramming in the context of atherosclerosis and highlighting knowledge gaps and potential therapeutic strategies targeting immune cell lysosomes.Lysosomes are centralized hubs for metabolic sensing and functional reprogramming of cells.Lysosomal metabolic sensing governs immune cell homeostasis and function.Lysosome dysfunction contributes to the immunoinflammatory response and metabolic impairment in vascular atherosclerotic lesions.Lysosomes are a compelling target for the modulation of immune responses in atherosclerosis.

Lysosomes in the immunometabolic reprogramming of immune cells in atherosclerosis / F. Bonacina, X. Zhang, N. Manel, L. Yvan-Charvet, B. Razani, G.D. Norata. - In: NATURE REVIEWS. CARDIOLOGY. - ISSN 1759-5010. - (2024 Sep), pp. 1-16. [Epub ahead of print] [10.1038/s41569-024-01072-4]

Lysosomes in the immunometabolic reprogramming of immune cells in atherosclerosis

F. Bonacina
Primo
;
G.D. Norata
Ultimo
2024

Abstract

Lysosomes have a central role in the disposal of extracellular and intracellular cargo and also function as metabolic sensors and signalling platforms in the immunometabolic reprogramming of macrophages and other immune cells in atherosclerosis. Lysosomes can rapidly sense the presence of nutrients within immune cells, thereby switching from catabolism of extracellular material to the recycling of intracellular cargo. Such a fine-tuned degradative response supports the generation of metabolic building blocks through effectors such as mTORC1 or TFEB. By coupling nutrients to downstream signalling and metabolism, lysosomes serve as a crucial hub for cellular function in innate and adaptive immune cells. Lysosomal dysfunction is now recognized to be a hallmark of atherogenesis. Perturbations in nutrient-sensing and signalling have profound effects on the capacity of immune cells to handle cholesterol, perform phagocytosis and efferocytosis, and limit the activation of the inflammasome and other inflammatory pathways. Strategies to improve lysosomal function hold promise as novel modulators of the immunoinflammatory response associated with atherosclerosis. In this Review, we describe the crosstalk between lysosomal biology and immune cell function and polarization, with a particular focus on cellular immunometabolic reprogramming in the context of atherosclerosis.In this Review, the authors describe the bidirectional crosstalk between lysosome biology and immune cell function and polarization, focusing on immunometabolic reprogramming in the context of atherosclerosis and highlighting knowledge gaps and potential therapeutic strategies targeting immune cell lysosomes.Lysosomes are centralized hubs for metabolic sensing and functional reprogramming of cells.Lysosomal metabolic sensing governs immune cell homeostasis and function.Lysosome dysfunction contributes to the immunoinflammatory response and metabolic impairment in vascular atherosclerotic lesions.Lysosomes are a compelling target for the modulation of immune responses in atherosclerosis.
Settore BIOS-11/A - Farmacologia
   Investigating the neuro-immune-metabolic interfaces in human and experimental atherosclerosis
   MINISTERO DELLA SALUTE
   PNRR-MAD-2022-12375913

   Improving diagnosis and therapy for familial dyslipidaemias: a network of general practitioners and specialised lipid centers
   MINISTERO DELLA SALUTE
   RF-2019-12370896

   Immunoregulatory paths of metabolic disease: unveil molecular mechanisms of impaired immuno-vascular response to target visceral inflammation by rewiring regulatory T cell energetic circuits
   MINISTERO DELL'UNIVERSITA' E DELLA RICERCA
   2022NBKCWP_001

   Fostering a European Research Area for Health Research
   ERA4Health
   European Commission
   Horizon Europe Framework Programme
   101095426
set-2024
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/1117509
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