Systems Biology Analysis Reveals Role of MDM2 in Diabetic Nephropathy

Overview

Journal JCI Insight

Specialties Biomedical Engineering
General Medicine

Date 2016 Oct 26

PMID 27777973

Citations 23

Authors

Rintaro Saito

Anais Rocanin-Arjo

Young-Hyun You

Manjula Darshi

Benjamin Van Espen

Satoshi Miyamoto

Jessica Pham

Minya Pu

Simone Romoli

Loki Natarajan

Wenjun Ju

Matthias Kretzler

Robert Nelson

Keiichiro Ono

Dana Thomasova

Shrikant R Mulay

Trey Ideker

Vivette DAgati

Ergin Beyret

Juan Carlos Izpisua Belmonte

Hans Joachim Anders

Kumar Sharma

Affiliations

Soon will be listed here.

Abstract

To derive new insights in diabetic complications, we integrated publicly available human protein-protein interaction (PPI) networks with global metabolic networks using metabolomic data from patients with diabetic nephropathy. We focused on the participating proteins in the network that were computationally predicted to connect the urine metabolites. had the highest significant number of PPI connections. As validation, significant downregulation of gene expression was found in both glomerular and tubulointerstitial compartments of kidney biopsy tissue from 2 independent cohorts of patients with diabetic nephropathy. In diabetic mice, chemical inhibition of with Nutlin-3a led to reduction in the number of podocytes, increased blood urea nitrogen, and increased mortality. Addition of Nutlin-3a decreased cells in embryonic kidneys. Both podocyte- and tubule-specific -knockout mice exhibited severe glomerular and tubular dysfunction, respectively. Interestingly, the only 2 metabolites that were reduced in both podocyte and tubule-specific -knockout mice were 3-methylcrotonylglycine and uracil, both of which were also reduced in human diabetic kidney disease. Thus, our bioinformatics tool combined with multi-omics studies identified an important functional role for in glomeruli and tubules of the diabetic nephropathic kidney and links to a reduction in 2 key metabolite biomarkers.

Citing Articles

Ursolic Acid Alleviates Mitotic Catastrophe in Podocyte by Inhibiting Autophagic P62 Accumulation in Diabetic Nephropathy.

Mei H, Jing T, Liu H, Liu Y, Zhu X, Wang J Int J Biol Sci. 2024; 20(9):3317-3333.

PMID: 38993555 PMC: 11234211. DOI: 10.7150/ijbs.94096.

SUPPRESION OF MITOCHONDRIAL RESPIRATION IS A FEATURE OF CELLULAR GLUCOSE TOXICITY.

Sharma K, Zhang G, Saito R Trans Am Clin Climatol Assoc. 2023; 133:24-33.

PMID: 37701600 PMC: 10493723.

MDM2 Influences ACE2 Stability and SARS-CoV-2 Uptake.

Emslander Q, Krey K, Hamad S, Maidl S, Oubraham L, Hesse J Viruses. 2023; 15(8).

PMID: 37632105 PMC: 10459000. DOI: 10.3390/v15081763.

New Approaches Targeting the Renin-Angiotensin System: Inhibition of Brain Aminopeptidase A, ACE2 Ubiquitination, and Angiotensinogen.

Lazartigues E, Llorens-Cortes C, Danser A Can J Cardiol. 2023; 39(12):1900-1912.

PMID: 37348757 PMC: 10730775. DOI: 10.1016/j.cjca.2023.06.013.

p53 and Myofibroblast Apoptosis in Organ Fibrosis.

McElhinney K, Irnaten M, OBrien C Int J Mol Sci. 2023; 24(7).

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