AI Article Synopsis

  • Radiation treatment for head and neck cancer can hurt salivary glands, causing dry mouth and affecting health and quality of life.
  • Macrophages are important immune cells in these glands and might help with repair, but we don't fully understand how they work yet.
  • The study found different types of macrophages in salivary glands that change with age, and those linked to the gland's tissue are crucial for fixing damage and keeping saliva production normal after radiation treatment.

Article Abstract

The salivary glands often become damaged in individuals receiving radiotherapy for head and neck cancer, resulting in chronic dry mouth. This leads to detrimental effects on their health and quality of life, for which there is no regenerative therapy. Macrophages are the predominant immune cell in the salivary glands and are attractive therapeutic targets due to their unrivaled capacity to drive tissue repair. Yet, the nature and role of macrophages in salivary gland homeostasis and how they may contribute to tissue repair after injury are not well understood. Here, we show that at least two phenotypically and transcriptionally distinct CX3CR1 macrophage populations are present in the adult salivary gland, which occupy anatomically distinct niches. CD11cCD206CD163 macrophages typically associate with gland epithelium, whereas CD11cCD206CD163 macrophages associate with blood vessels and nerves. Using a suite of complementary fate mapping systems, we show that there are highly dynamic changes in the ontogeny and composition of salivary gland macrophages with age. Using an in vivo model of radiation-induced salivary gland injury combined with genetic or antibody-mediated depletion of macrophages, we demonstrate an essential role for macrophages in clearance of cells with DNA damage. Furthermore, we show that epithelial-associated macrophages are indispensable for effective tissue repair and gland function after radiation-induced injury, with their depletion resulting in reduced saliva production. Our data, therefore, provide a strong case for exploring the therapeutic potential of manipulating macrophages to promote tissue repair and thus minimize salivary gland dysfunction after radiotherapy.

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Source
http://dx.doi.org/10.1126/sciimmunol.add4374DOI Listing

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