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Publication : Bovine serum albumin aggravates macrophage M1 activation and kidney injury in heterozygous Klotho-deficient mice via the gut microbiota-immune axis.

First Author  Lai L Year  2021
Journal  Int J Biol Sci Volume  17
Issue  3 Pages  742-755
PubMed ID  33767585 Mgi Jnum  J:324451
Mgi Id  MGI:6753486 Doi  10.7150/ijbs.56424
Citation  Lai L, et al. (2021) Bovine serum albumin aggravates macrophage M1 activation and kidney injury in heterozygous Klotho-deficient mice via the gut microbiota-immune axis. Int J Biol Sci 17(3):742-755
abstractText  Klotho expression abnormalities induces kidney injury and chronic kidney disease, however, the underlying mechanism remains unclear. Here, Klotho(+/-) mice and wild-type mice were treated with low-dose bovine serum albumin (BSA). Pathological examination demonstrated that the area of glomerular collagen deposition and fibrosis in BSA-Kl(-/+) mice was significantly larger than that in BSA-WT mice. The serum levels of superoxide dismutase, malondialdehyde, creatinine, and urea in BSA-Kl(-/+) mice were significantly increased. Sequencing of gut microbiota 16S rRNA v3-v4 region indicated that BSA-Kl(-/+) mice showed a significantly higher relative abundance of the genera Dubosiella, Akkermansia, Alloprevotella, and Lachnospiraceae and a significantly lower relative abundance of the genera Allobaculum and Muribaculaceae than BSA-WT mice. KEGG analysis revealed that the metabolic pathways of signal transduction, xenobiotic biodegradation and metabolism, and lipid metabolism increased significantly in BSA-Kl(-/+) mice. Flow cytometry showed that the proportion of CD68(+)/CD11b(+) cells in the peripheral blood was significantly higher in BSA-KL(-/+) mice than that in BSA-WT mice. qPCR and western blot suggested that Klotho and Nrf2 expression in MPhi1 cells of BSA-KL(-/+) mice was significantly decreased. Thus, the findings suggest during the immune activation and chronic inflammation induced by the gut microbiota imbalance in Klotho-deficient mice treated to BSA, disrupted expression of proteins in the Nrf2/NF-kappaB signaling pathway in monocyte-derived macrophage M1 cells leads to the aggravation of inflammation and kidney injury.
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