Litcius/Paper detail

Lung macrophages utilize unique cathepsin K–dependent phagosomal machinery to degrade intracellular collagen

Ivo Fabrik, Orsolya Bilkei‐Gorzo, Maria Öberg, Daniela Fabriková, J. Fuchs, Carina Sihlbom, Melker Göransson, Anetta Härtlová

2023Life Science Alliance16 citationsDOIOpen Access PDF

Abstract

Resident tissue macrophages are organ-specialized phagocytes responsible for the maintenance and protection of tissue homeostasis. It is well established that tissue diversity is reflected by the heterogeneity of resident tissue macrophage origin and phenotype. However, much less is known about tissue-specific phagocytic and proteolytic macrophage functions. Here, using a quantitative proteomics approach, we identify cathepsins as key determinants of phagosome maturation in primary peritoneum-, lung-, and brain-resident macrophages. The data further uncover cathepsin K (CtsK) as a molecular marker for lung phagosomes required for intracellular protein and collagen degradation. Pharmacological blockade of CtsK activity diminished phagosomal proteolysis and collagenolysis in lung-resident macrophages. Furthermore, profibrotic TGF-β negatively regulated CtsK-mediated phagosomal collagen degradation independently from classical endocytic-proteolytic pathways. In humans, phagosomal CtsK activity was reduced in COPD lung macrophages and non-COPD lung macrophages exposed to cigarette smoke extract. Taken together, this study provides a comprehensive map of how peritoneal, lung, and brain tissue environment shapes phagosomal composition, revealing CtsK as a key molecular determinant of lung phagosomes contributing to phagocytic collagen clearance in lungs.

Topics & Concepts

PhagosomeMacrophageCell biologyBiologyCathepsinLungProteolysisPhagocytosisCathepsin KPathologyBiochemistryMedicineIn vitroOsteoclastInternal medicineEnzymeS100 Proteins and AnnexinsProtease and Inhibitor MechanismsImmune cells in cancer