Human liver derived mesenchymal stromal cells ameliorate murine ischemia-induced inflammation through macrophage polarization

Human liver derived mesenchymal stromal cells ameliorate murine ischemia-induced inflammation through macrophage polarization

The immunomodulatory properties of mesenchymal stromal cells (MSC) have been well-characterized in and models. We have previously shown that liver MSC (L-MSC) are superior inhibitors of T-cell activation/proliferation, NK cell cytolytic function, and macrophage activation compared to adipose (A-MSC)...

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Veröffentlicht in:Frontiers in immunology 2024-07, Vol.15, p.1448092
Hauptverfasser: Liang, Yun, Ozdogan, Elif, Hansen, Michael J, Tang, Hui, Saadiq, Ishran, Jordan, Kyra L, Krier, James D, Gandhi, Deep B, Grande, Joseph P, Lerman, Lilach O, Taner, Timucin
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Disease Models, Animal
Humans
Immunology
immunomodulation
inflammation
Inflammation - immunology
Inflammation - therapy
Ischemia - immunology
Ischemia - therapy
Kidney - immunology
Kidney - pathology
Liver - immunology
Liver - pathology
liver tolerance
Macrophage Activation
Macrophages - immunology
Male
Mesenchymal Stem Cell Transplantation - methods
Mesenchymal Stem Cells
mesenchymal stromal cells
Mice
Renal Artery Obstruction - immunology
Renal Artery Obstruction - therapy
renal artery stenosis
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Zusammenfassung:The immunomodulatory properties of mesenchymal stromal cells (MSC) have been well-characterized in and models. We have previously shown that liver MSC (L-MSC) are superior inhibitors of T-cell activation/proliferation, NK cell cytolytic function, and macrophage activation compared to adipose (A-MSC) and bone marrow MSC (BM-MSC) . To test these observations , we infused these types of MSC into mice with unilateral renal artery stenosis (RAS), an established model of kidney inflammation. Unilateral RAS was induced via laparotomy in 11-week-old, male 129-S1 mice under general anesthesia. Control mice had sham operations. Human L-MSC, AMSC, and BM-MSC (5x105 cells each) or PBS vehicle were injected intra-arterially 2 weeks after surgery. Kidney morphology was studied 2 weeks after infusion using micro-MRI imaging. Renal inflammation, apoptosis, fibrosis, and MSC retention were studied utilizing western blot, immunofluorescence, and immunohistological analyses. The stenotic kidney volume was smaller in all RAS mice, confirming significant injury, and was improved by infusion of all MSC types. All MSC-infused groups had lower levels of plasma renin and proteinuria compared to untreated RAS. Serum creatinine improved in micetreated with BM- and L-MSC. All types of MSC located to and were retained within the stenotic kidneys, but L-MSC retention was significantly higher than A- and BM-MSC. While all groups of MSC-treated mice displayed reduced overall inflammation and macrophage counts, L-MSC showed superior potency at localizing to the site of inflammation and inducing M2 (reparative) macrophage polarization to reduce inflammatory changes. These findings extend our studies and suggest that L-MSC possess unique anti-inflammatory properties that may play a role in liver-induced tolerance and lend further support to their use as therapeutic agents for diseases with underlying inflammatory pathophysiology.
ISSN:1664-3224
1664-3224
DOI:10.3389/fimmu.2024.1448092