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Inhibition of retinoic acid signaling in proximal tubular epithelial cells protects against acute kidney injury
Min Yang, Lauren N. Lopez, Maya Brewer, Rachel Delgado, Anna Menshikh, Kelly Clouthier, Yuantee Zhu, Thitinee Vanichapol, Haichun Yang, Raymond C. Harris, Leslie Gewin, Craig R. Brooks, Alan J. Davidson, Mark de Caestecker
Min Yang, Lauren N. Lopez, Maya Brewer, Rachel Delgado, Anna Menshikh, Kelly Clouthier, Yuantee Zhu, Thitinee Vanichapol, Haichun Yang, Raymond C. Harris, Leslie Gewin, Craig R. Brooks, Alan J. Davidson, Mark de Caestecker
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Research Article Nephrology

Inhibition of retinoic acid signaling in proximal tubular epithelial cells protects against acute kidney injury

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Abstract

Retinoic acid receptor (RAR) signaling is essential for mammalian kidney development but, in the adult kidney, is restricted to occasional collecting duct epithelial cells. We now show that there is widespread reactivation of RAR signaling in proximal tubular epithelial cells (PTECs) in human sepsis-associated acute kidney injury (AKI) and in mouse models of AKI. Genetic inhibition of RAR signaling in PTECs protected against experimental AKI but was unexpectedly associated with increased expression of the PTEC injury marker Kim1. However, the protective effects of inhibiting PTEC RAR signaling were associated with increased Kim1-dependent apoptotic cell clearance, or efferocytosis, and this was associated with dedifferentiation, proliferation, and metabolic reprogramming of PTECs. These data demonstrate the functional role that reactivation of RAR signaling plays in regulating PTEC differentiation and function in human and experimental AKI.

Authors

Min Yang, Lauren N. Lopez, Maya Brewer, Rachel Delgado, Anna Menshikh, Kelly Clouthier, Yuantee Zhu, Thitinee Vanichapol, Haichun Yang, Raymond C. Harris, Leslie Gewin, Craig R. Brooks, Alan J. Davidson, Mark de Caestecker

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Figure 3

RAR signaling is extensively activated in Kim1– PTECs after Rhabdo-AKI.

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RAR signaling is extensively activated in Kim1– PTECs after Rhabdo-AKI.
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RARE-LacZ reporter mice were used to evaluate the cellular localization of RAR signaling after Rhabdo-AKI. (A and C) Percentage of LacZ+ cells in LTL+ and Kim1– PTECs (A) and in Kim1+ PTECs (C) at the different time points after injury in the cortex and OSOM: 2 mice before injury (day 0) and 4 at days 1 and 3, 3 at day 7, and 5 at day 14 after injury. (B and D) Images showing LacZ, LTL, and Kim1 staining in the cortex and OSOM. (B) Low-power images of the kidneys; regions of the kidney are demarcated by dotted lines, as indicated. Scale bars: 500 mM. (D) High-power images of the OSOM. Scale bars: 100 mM.

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