Resident macrophages reprogram toward a developmental state after acute kidney injury
Jeremie M. Lever, … , Anupam Agarwal, James F. George
Jeremie M. Lever, … , Anupam Agarwal, James F. George
Published January 24, 2019
Citation Information: JCI Insight. 2019;4(2):e125503. https://doi.org/10.1172/jci.insight.125503.
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Research Article Immunology Nephrology

Resident macrophages reprogram toward a developmental state after acute kidney injury

Abstract

Acute kidney injury (AKI) is a devastating clinical condition affecting at least two-thirds of critically ill patients, and, among these patients, it is associated with a greater than 60% risk of mortality. Kidney mononuclear phagocytes (MPs) are implicated in pathogenesis and healing in mouse models of AKI and, thus, have been the subject of investigation as potential targets for clinical intervention. We have determined that, after injury, F4/80hi-expressing kidney-resident macrophages (KRMs) are a distinct cellular subpopulation that does not differentiate from nonresident infiltrating MPs. However, if KRMs are depleted using polyinosinic/polycytidylic acid (poly I:C), they can be reconstituted from bone marrow–derived precursors. Further, KRMs lack major histocompatibility complex class II (MHCII) expression before P7 but upregulate it over the next 14 days. This MHCII– KRM phenotype reappears after injury. RNA sequencing shows that injury causes transcriptional reprogramming of KRMs such that they more closely resemble that found at P7. KRMs after injury are also enriched in Wingless-type MMTV integration site family (Wnt) signaling, indicating that a pathway vital for mouse and human kidney development is active. These data indicate that mechanisms involved in kidney development may be functioning after injury in KRMs.

Authors

Jeremie M. Lever, Travis D. Hull, Ravindra Boddu, Mark E. Pepin, Laurence M. Black, Oreoluwa O. Adedoyin, Zhengqin Yang, Amie M. Traylor, Yanlin Jiang, Zhang Li, Jacelyn E. Peabody, Han E. Eckenrode, David K. Crossman, Michael R. Crowley, Subhashini Bolisetty, Kurt A. Zimmerman, Adam R. Wende, Michal Mrug, Bradley K. Yoder, Anupam Agarwal, James F. George

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Figure 3

Kidney F4/80lo mononuclear phagocytes are derived from the peripheral circulation and turn over within 14 days.

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Kidney F4/80lo mononuclear phagocytes are derived from the peripheral ci...
(A) Schematic representation of parabiosis separation experiment of steady-state parabiotic chimeras. 10-week-old CD45 congenic mice (CD45.1 and CD45.2) were parabiotically attached for 4 weeks. The pairs were separated and blood was drawn at the time of separation and then 3, 7, and 14 days after separation. On day 14, kidneys were harvested and immune cell chimerism was studied. (B) The percentage of chimerism in peripheral blood of parabiotic chimeras at time points after separation. Mean ± SEM, n = 8 (4 pairs). Statistical comparison: day 3 Ly6Chi vs. Ly6Clo, 2-way ANOVA with Tukey’s post-test, *P < 0.05. (C) The percentage of chimerism for kidney CD45+ leukocytes, intrarenal neutrophils (PMN), and kidney MPs 14 days after separation. Mean ± SEM.