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Defective mitochondria remodelling in B cells leads to an aged immune response.

Marta Iborra-PernichiJonathan Ruiz GarcíaMaría Velasco de la EsperanzaBelén S EstradaElena R BovolentaClaudia CifuentesCristina Prieto CarroTamara González MartínezJosé García-ConsuegraMaría Fernanda Rey-StolleFrancisco Javier RupérezMilagros Guerra RodriguezRafael Jose ArgüelloSara CogliatiFernando Martín-BelmonteNuria Martínez-Martín
Published in: Nature communications (2024)
The B cell response in the germinal centre (GC) reaction requires a unique bioenergetic supply. Although mitochondria are remodelled upon antigen-mediated B cell receptor stimulation, mitochondrial function in B cells is still poorly understood. To gain a better understanding of the role of mitochondria in B cell function, here we generate mice with B cell-specific deficiency in Tfam, a transcription factor necessary for mitochondrial biogenesis. Tfam conditional knock-out (KO) mice display a blockage of the GC reaction and a bias of B cell differentiation towards memory B cells and aged-related B cells, hallmarks of an aged immune response. Unexpectedly, blocked GC reaction in Tfam KO mice is not caused by defects in the bioenergetic supply but is associated with a defect in the remodelling of the lysosomal compartment in B cells. Our results may thus describe a mitochondrial function for lysosome regulation and the downstream antigen presentation in B cells during the GC reaction, the dysruption of which is manifested as an aged immune response.
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