Macrophage Heterogeneity in Liver Ischemia-Reperfusion Injury
Yuan Zhai, Yue Wang, Cheng Zhong, Jackson Chin, Nan Xia, Yi-Chu Kao, Tori Huey, Hesham El-Shewy, Dirk Van der Windt, Kris Helke, Thomas Morinelli, Aaron Meyer

TL;DR
This study explores how different types of liver macrophages affect injury during liver ischemia and reperfusion.
Contribution
The study identifies Gr-1+Trem-2+ infiltrating macrophages as protective and reveals an IL-1a/b-dependent pro-inflammatory role of Kupffer cells.
Findings
Gr-1+CD11b+ infiltrating macrophages protect the liver from IRI through Trem-2 expression.
Kupffer cell replacement with iMФs reduces IL-1a and IL-1b levels, decreasing inflammation.
Blocking IL-1a or IL-1b reduces liver injury in a Kupffer cell-dependent manner.
Abstract
Kupffer cells (KCs) are implicated in liver ischemia reperfusion injury (IRI). However, their precise roles vs. bone marrow–derived infiltrating macrophages (iMФs) remain controversial. In this study, we used Clec4F-tdTomato (DTR) mice to track KC-specific changes and assessed their function by DT-mediated depletion in the acute phase of liver IRI. We found that liver IR leads to substantial loss of embryonically derived Clec4F+TIM-4+ KCs, coinciding with pronounced infiltration of monocytes and neutrophils. A single dose of DT resulted in a complete replacement of Clec4F+ KCs with iMФs, leading to a temporally dynamic modulation of liver susceptibility to IRI: reduced at 24 hours but aggravated at 14 days following DT administration. The early liver protection was mediated by Gr-1+CD11b+ iMФs with high expression of Trem2. Anti-Gr-1 Abs or Trem-2 blockade abolished the cytoprotective…
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Taxonomy
TopicsOrgan Transplantation Techniques and Outcomes · Immune cells in cancer · Inflammation biomarkers and pathways
