GeneSet Information

Tier II GS223814 • Kidney mass QTL 43 (Kidm43 Published QTL Chr 4)

DESCRIPTION:

QTL Associated with Kidney mass. On Chromosome 4 with a LOD score= 18, p-value =. From a(n) intercross of

LABEL:

QTL-Kidm43-Rat-Chr 4

SCORE TYPE:

Binary

DATE ADDED:

2015-06-10

DATE UPDATED:

2024-04-25

SPECIES:

AUTHORS:

Yagil Y, Roif D, Sapojnikov M, Ben-Dor D, Tobar A, Rosenmann E, Yagil C

TITLE:

Unmasking of proteinuria in the course of genetic dissection of nonproteinuric diabetic nephropathy.

JOURNAL:

Physiological genomics None None, Vol 46, pp. 29-38

ABSTRACT:

1. Physiol Genomics. 2014 Jan 1;46(1):29-38. doi: 10.1152/physiolgenomics.00133.2013. Epub 2013 Nov 5. Unmasking of proteinuria in the course of genetic dissection of nonproteinuric diabetic nephropathy. Yagil Y(1), Roif D, Sapojnikov M, Ben-Dor D, Tobar A, Rosenmann E, Yagil C. Author information: (1)Laboratory for Molecular Medicine and Israeli Rat Genome Center, Ben-Gurion University Barzilai Medical Center Campus, Ashkelon, Israel; We previously described the development of nonproteinuric diabetic nephropathy (NPDN) in the Cohen diabetic rat (CDs), a model that simulates Type 2 diabetes in humans. Using linkage analysis in an F2 cross, we currently set out to investigate the mechanisms underlying NPDN. We crossbred between CDs and SBN/y, a nondiabetic rat strain, generated F1 and F2 progenies, fed them diabetogenic diet that elicits diabetes and NPDN in CDs but not in SBN/y, and determined metabolic and renal phenotypes. Over 5 mo, ∼75% of F2 developed a diabetic phenotype. In parallel, a nephropathy developed in F2, with glomerular filtration rate (GFR) declining in ∼25% and, unexpectedly, significant proteinuria appearing in ∼75%. We scanned the F2 genome with microsatellite markers and used linkage analysis to identify quantitative trait loci (QTLs). We detected diabetes-related QTLs on RNO4 and 13. We also detected two QTLs for the decline in GFR on RNO4 and 13 and another QTL for proteinuria on RNO13. The metabolic and renal-related QTLs overlapped. These results suggest that the mechanisms underlying the nephropathy in F2 are related to genes that map to RNO4 and 13, as well as a common genetic background for the development of diabetes and the renal disease. Our findings further indicate that proteinuria is inhibited in parental diabetic CDs, thus accounting for the nonproteinuric phenotype, but "unmasked" in diabetic F2 whose genome has been modified. Identifying the nature of the factor inhibiting proteinuria in diabetic CDs but not in F2 may provide a clue to treatment and prevention of proteinuria in diabetes. PMID: 24192394 [PubMed - indexed for MEDLINE] PUBMED: 24192394
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