Renal CD169++ resident macrophages are crucial for protection against acute systemic candidiasis.
Yi Juan TeoSee Liang NgKeng Wai MakYolanda Aphrilia SetiaganiQi ChenSajith Kumar NairJianpeng ShengChristiane RuedlPublished in: Life science alliance (2021)
Disseminated candidiasis remains as the most common hospital-acquired bloodstream fungal infection with up to 40% mortality rate despite the advancement of medical and hygienic practices. While it is well established that this infection heavily relies on the innate immune response for host survival, much less is known for the protective role elicited by the tissue-resident macrophage (TRM) subsets in the kidney, the prime organ for Candida persistence. Here, we describe a unique CD169++ TRM subset that controls Candida growth and inflammation during acute systemic candidiasis. Their absence causes severe fungal-mediated renal pathology. CD169++ TRMs, without being actively involved in direct fungal clearance, increase host resistance by promoting IFN-γ release and neutrophil ROS activity.
Keyphrases
- candida albicans
- immune response
- liver failure
- healthcare
- drug induced
- biofilm formation
- respiratory failure
- primary care
- patient safety
- quality improvement
- oxidative stress
- dendritic cells
- nk cells
- adipose tissue
- type diabetes
- dna damage
- aortic dissection
- cell death
- cell wall
- inflammatory response
- cardiovascular disease
- staphylococcus aureus
- emergency medicine
- peripheral blood
- gram negative
- acute respiratory distress syndrome
- pseudomonas aeruginosa
- klebsiella pneumoniae