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A profile of multiple circulating tumor necrosis factor receptors associated with early progressive kidney decline in Type 1 Diabetes is similar to profiles in autoimmune disorders.

Citation
Ihara, K., et al. “A Profile Of Multiple Circulating Tumor Necrosis Factor Receptors Associated With Early Progressive Kidney Decline In Type 1 Diabetes Is Similar To Profiles In Autoimmune Disorders.”. Kidney International, pp. 725-736.
Center Joslin Diabetes Center
Author Katsuhito Ihara, Jan Skupien, Bozena Krolewski, Zaipul I Md Dom, Kristina O'Neil, Eiichiro Satake, Hiroki Kobayashi, Narges M Rashidi, Monika A Niewczas, Andrzej S Krolewski
Keywords TNF receptors, diabetic kidney disease, End-stage kidney disease, progressive kidney decline, tumor necrosis factor (TNF) superfamily, type 1 diabetes
Abstract

This study comprehensively evaluated the association between known circulating tumor necrosis factor (TNF) superfamily ligands and receptors and the development of early progressive kidney decline (PKD) leading to end-stage kidney disease (ESKD) in Type 1 diabetes. Participants for the study were from the Macro-Albuminuria Study (198 individuals), and the Micro-Albuminuria Study (148 individuals) of the Joslin Kidney Study. All individuals initially had normal kidney function and were followed for seven-fifteen years to determine the slope of the estimate glomerular filtration rate and to ascertain onset of ESKD. Plasma concentrations of 25 TNF superfamily proteins were measured using proximity extension assay applied in the OLINK proteomics platform. In the both studies risk of early PKD, determined as estimated glomerular filtration rate loss greater than or equal to three ml/min/1.73m/year, was associated with elevated circulating levels of 13 of 19 TNF receptors examined. In the Macro-Albuminuria Study, we obtained similar findings for risk of progression to ESKD. These receptors comprised: TNF-R1A, -R1B, -R3, -R4, -R6, -R6B, -R7, -R10A, -R10B, -R11A, -R14, -R21, and -R27. Serial measurements showed that circulating levels of these TNF receptors had increased before the onset of PKD. In contrast, none of the six measured TNF ligands showed association with risk of early PKD. Of significance, the disease process that underlies PKD leading to ESKD in Type 1 diabetes has a profile also seen in autoimmune disorders. The mechanisms of this enrichment may be causally related to the development of PKD in Type 1 diabetes and must be investigated further. Thus, some of these receptors may be used as new risk predictors of ESKD.

Year of Publication
2021
Journal
Kidney international
Volume
99
Issue
3
Number of Pages
725-736
Date Published
12/2021
ISSN Number
1523-1755
DOI
10.1016/j.kint.2020.07.007
Alternate Journal
Kidney Int
PMID
32717193
PMCID
PMC7891866
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