Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UMLS:C0033687 (
proteinuria
)
24,015
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Mice born without CD2-associated protein (CD2AP) develop renal failure and nephrotic syndrome about 4 weeks after birth and die around 6 weeks of age. Although CD2AP is widely expressed, the severity of the renal failure precludes a clear determination of the role of CD2AP in other tissues. Here we generated transgenic mice expressing CD2AP using a podocyte-specific promoter. Podocyte-specific expression of CD2AP prevented the development of
proteinuria
, demonstrating that the renal failure is solely due to loss of CD2AP in podocytes and not in other renal or in immune cells. CD2AP-deficient mice are long-lived and appear phenotypically normal. Histological analysis demonstrated testicular abnormalities that were age-related.
CIN85
, a paralog of CD2AP, is poorly expressed in both the podocyte and the basal seminiferous tubule, suggesting that the loss of CD2AP in specific tissues may be compensated for by
CIN85
.
...
PMID:CD2-associated protein (CD2AP) expression in podocytes rescues lethality of CD2AP deficiency. 1595 37
Podocyte damage is the basis of many glomerular diseases with ultrastructural changes and decreased expression of components of the slit diaphragm such as nephrin and podocin. Under physiological conditions it is likely that the slit diaphragm underlies permanent renewal processes to indemnify its stability in response to changes in filtration pressure. This would require constant reorganization of the podocyte foot process and the renewal of slit diaphragm components. Thus far, the mechanisms underlying the turnover of slit diaphragm proteins are largely unknown. In this manuscript we examined a mechanism of nephrin endocytosis via
CIN85
/Ruk(L)-mediated ubiquitination. We can demonstrate that the loss of nephrin expression and onset of the
proteinuria
in CD2AP(-/-) mice correlates with an increased accumulation of ubiquitinated proteins and expression of
CIN85
/Ruk(L) in podocytes. In cultured murine podocytes CD2AP deficiency leads to an early ubiquitination of nephrin and podocin after stimulation with fibroblast growth factor-4. Binding assays with different
CIN85
/Ruk isoforms and mutants showed that nephrin and podocin are binding to the coiled-coil domain of
CIN85
/Ruk(L). We found that in the presence of
CIN85
/Ruk(L), which is involved in down-regulation of receptor-tyrosine kinases, nephrin is internalized after stimulation with fibroblast growth factor-4. Interestingly, coexpression of
CIN85
/Ruk(L) with CD2AP led to a decreased binding of
CIN85
/Ruk(L) to nephrin and podocin, which indicates a functional competition between CD2AP and
CIN85
/Ruk(L). Our results support a novel role for
CIN85
/Ruk(L) in slit diaphragm turnover and
proteinuria
.
...
PMID:CIN85/RukL is a novel binding partner of nephrin and podocin and mediates slit diaphragm turnover in podocytes. 2045 1
Podocytes are highly differentiated and polarized epithelial cells located on the visceral side of the glomerulus. They form an indispensable component of the glomerular filter, the slit diaphragm, formed by several transmembrane proteins and adaptor molecules. Disruption of the slit diaphragm can lead to massive
proteinuria
and nephrotic syndrome in mice and humans. CD2AP is an adaptor protein that is important for the maintenance of the slit diaphragm. Together with its paralogue,
CIN85
, CD2AP belongs to a family of adaptor proteins that are primarily described as being involved in endocytosis and downregulation of receptor tyrosine kinase activity. We have shown that full-length
CIN85
is upregulated in podocytes in the absence of CD2AP, whereas in wild-type cells, full-length
CIN85
is not detectable. In this study, we show that full-length
CIN85
is postranslationally modified by SUMOylation in wild-type podocytes. We can demonstrate that
CIN85
is SUMOylated by SUMO-1, -2, and -3 and that SUMOylation is enhanced in the presence of CD2AP. Conversion of lysine 598 to arginine completely abolishes SUMOylation and leads to increased binding of
CIN85
to nephrin. Our results indicate a novel role for CD2AP in regulating posttranslational modification of
CIN85
.
...
PMID:CD2AP regulates SUMOylation of CIN85 in podocytes. 2220 40
Diabetic nephropathy (DN) is the major cause of end-stage renal disease worldwide. Podocytes are important for glomerular filtration barrier function and maintenance of size selectivity in protein filtration in the kidney. Podocyte damage is the basis of many glomerular diseases characterized by loss of interdigitating foot processes and decreased expression of components of the slit diaphragm. Nephrin, a podocyte-specific protein, is the main component of the slit diaphragm. Loss of nephrin is observed in human and rodent models of diabetic kidney disease. The long isoform of
CIN85
(RukL) is a binding partner of nephrin that mediates nephrin endocytosis via ubiquitination in podocytes. Here we demonstrate that the loss of nephrin expression and the onset of
proteinuria
in diabetic mice correlate with an increased accumulation of ubiquitinated proteins and expression of
CIN85
/RukL in podocytes.
CIN85
/RukL deficiency preserved nephrin surface expression on the slit diaphragm and reduced
proteinuria
in diabetic mice, whereas overexpression of
CIN85
in zebrafish induced severe edema and disruption of the filtration barrier. Thus,
CIN85
/RukL is involved in endocytosis of nephrin in podocytes under diabetic conditions, causing podocyte depletion and promoting
proteinuria
.
CIN85
/RukL expression therefore shows potential to be a novel target for antiproteinuric therapy in diabetes.
...
PMID:CIN85 Deficiency Prevents Nephrin Endocytosis and Proteinuria in Diabetes. 2787 4
