NGAL release from peripheral blood mononuclear cells protects against acute kidney injury and prevents AKI induced fibrosis

NGAL release from peripheral blood mononuclear cells protects against acute kidney injury and prevents AKI induced fibrosis

We propose the use of a peripheral blood mononuclear cell therapy based on cell NGAL release to be used in the clinical setting for acute kidney injury (AKI) and the derived fibrosis. First, we designed a procedure whereby PBMC overexpress NGAL and anti-inflammatory agents when subjected to repetiti...

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Veröffentlicht in:Biomedicine & pharmacotherapy 2022-09, Vol.153, p.113415-113415, Article 113415
Hauptverfasser: Játiva, Soraya, Torrico, Selene, Calle, Priscila, Muñoz, Ángeles, García, Miriam, Larque, Ana Belén, Poch, Esteban, Hotter, Georgina
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Acute kidney failure
Inflammation
Macrophage
Monocyte
NGAL
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container_end_page 113415
container_issue
container_start_page 113415
container_title Biomedicine & pharmacotherapy
container_volume 153
creator Játiva, Soraya
Torrico, Selene
Calle, Priscila
Muñoz, Ángeles
García, Miriam
Larque, Ana Belén
Poch, Esteban
Hotter, Georgina
description We propose the use of a peripheral blood mononuclear cell therapy based on cell NGAL release to be used in the clinical setting for acute kidney injury (AKI) and the derived fibrosis. First, we designed a procedure whereby PBMC overexpress NGAL and anti-inflammatory agents when subjected to repetitive anoxia/reoxygenation (PBMC (A/R)). Using an in vivo AKI model, we observed that PBMC(A/R) reduces BUN and creatinine levels in blood and inflammation, enhances anti-inflammation, induces proliferation of tubular epithelial cells and reduces AKI-induced fibrosis. Flow cytometry analysis evidenced that monocytes are the only cells accumulated in the injured kidney and phenotype analysis of freshly isolated kidney macrophages, revealed that the healing phenotype is maintained the time needed for recovery. NGAL release from PBMC(A/R) determines the beneficial effect of the therapy since administration of a NGAL antibody previous to the therapy or injection of PBMC(A/R) obtained from NGAL KO animals abolished the beneficial effects. CD11b–NGAL positive cells were enhanced in tissue after PBMC (A/R) therapy and were produced by the injected monocytes. In an in vitro model with tubular epithelial cells (NRK52e) we proved that NGAL release by PBMC(A/R) induced epithelial proliferation and activation of PI3K/Akt pathway. [Display omitted] •PBMC polarized by repetitive anoxia/ reoxygenation overexpress NGAL.•NGAL release from polarized PBMC induces antiinflammation and proliferation.•Therapy with PBMC polarized induces kidney repair and antiinflammation.•Therapy with PBMC polarized prevents kidney fibrosis associated to acute kidney injury.
doi_str_mv 10.1016/j.biopha.2022.113415
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subjects Acute kidney failure
Inflammation
Macrophage
Monocyte
NGAL
title NGAL release from peripheral blood mononuclear cells protects against acute kidney injury and prevents AKI induced fibrosis
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