Frontiers in Immunology (May 2024)

Differential regulation of lung homeostasis and silicosis by the TAM receptors MerTk and Axl

  • Kamila Guimarães-Pinto,
  • Kamila Guimarães-Pinto,
  • Monique Leandro,
  • Antonia Corrêa,
  • Ester P. Maia,
  • Leticia Rodrigues,
  • André Luiz Amorim da Costa,
  • Jesuino Rafael Machado Ferreira,
  • Estefannia Claudio-Etienne,
  • Ulrich Siebenlist,
  • Jianping He,
  • Thaís da Silva Rigoni,
  • Tatiana Paula Teixeira Ferreira,
  • Yago Amigo Pinho Jannini-Sa,
  • Herbert Leonel Matos-Guedes,
  • Herbert Leonel Matos-Guedes,
  • Ana Caroline Costa-da-Silva,
  • Marcela Freitas Lopes,
  • Patricia Machado Rodrigues Silva,
  • Brian Lee Kelsall,
  • Alessandra Almeida Filardy

DOI
https://doi.org/10.3389/fimmu.2024.1380628
Journal volume & issue
Vol. 15

Abstract

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IntroductionTAM receptor-mediated efferocytosis plays an important function in immune regulation and may contribute to antigen tolerance in the lungs, a site with continuous cellular turnover and generation of apoptotic cells. Some studies have identified failures in efferocytosis as a common driver of inflammation and tissue destruction in lung diseases. Our study is the first to characterize the in vivo function of the TAM receptors, Axl and MerTk, in the innate immune cell compartment, cytokine and chemokine production, as well as the alveolar macrophage (AM) phenotype in different settings in the airways and lung parenchyma.MethodsWe employed MerTk and Axl defective mice to induce acute silicosis by a single exposure to crystalline silica particles (20 mg/50 μL). Although both mRNA levels of Axl and MerTk receptors were constitutively expressed by lung cells and isolated AMs, we found that MerTk was critical for maintaining lung homeostasis, whereas Axl played a role in the regulation of silica-induced inflammation. Our findings imply that MerTk and Axl differently modulated inflammatory tone via AM and neutrophil recruitment, phenotype and function by flow cytometry, and TGF-β and CXCL1 protein levels, respectively. Finally, Axl expression was upregulated in both MerTk-/- and WT AMs, confirming its importance during inflammation.ConclusionThis study provides strong evidence that MerTk and Axl are specialized to orchestrate apoptotic cell clearance across different circumstances and may have important implications for the understanding of pulmonary inflammatory disorders as well as for the development of new approaches to therapy.

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