Accumulation of Advanced Glycation Endproducts in the Rat Nephron: Link with Circulating AGEs During Aging

Verbeke, Philippe; Perichon, Martine; Borot–Laloi, Caroline; Schaeverbeke, J.; Bakala, Hilaire

doi:10.1177/002215549704500804

Cited by 42 publications

(36 citation statements)

References 41 publications

(36 reference statements)

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“…The following primary antibodies were used for Western blot: mouse monoclonal anti-sarcomeric ␣-actin (1:400, Sigma, recognize both cardiac and skeletal ␣-actin), mouse monoclonal anti-␣-tropomyosin, rabbit polyclonal anti-GAPDH (1:400, Santa Cruz), rabbit polyclonal anti-Histone-3 (1:400, Sigma), mouse monoclonal anti-␣B-crystallin (1:200, Abcam), and anti-phosphorylated serines 19, 45, and 59 on ␣B-crystallin (1:500, StressGen). Polyclonal anti-AGE antibody was a kind gift of Dr. Bakala and has been previously characterized (17,18). It recognizes a variety of AGE products such as carboxymethyl lysine and carboxyethyl lysine.…”

Section: Left Ventricular Tissue Preparation For Use In Proteomic Andmentioning

confidence: 99%

Muscle Creatine Kinase Deficiency Triggers Both Actin Depolymerization and Desmin Disorganization by Advanced Glycation End Products in Dilated Cardiomyopathy

Diguet

Mallat

Ladouce

et al. 2011

Journal of Biological Chemistry

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Alterations in the balance of cytoskeleton as well as energetic proteins are involved in the cardiac remodeling occurring in dilated cardiomyopathy (DCM). We used two-dimensional DIGE proteomics as a discovery approach to identify key molecular changes taking place in a temporally controlled model of DCM triggered by cardiomyocyte-specific serum response factor (SRF) knock-out in mice. We identified muscle creatine kinase (MCK) as the primary down-regulated protein followed by ␣-actin and ␣-tropomyosin down-regulation leading to a decrease of polymerized F-actin. The early response to these defects was an increase in the amount of desmin intermediate filaments and phosphorylation of the ␣B-crystallin chaperone. We found that ␣B-crystallin and desmin progressively lose their striated pattern and accumulate at the intercalated disk and the sarcolemma, respectively. We further show that desmin is a preferential target of advanced glycation end products (AGE) in mouse and human DCM. Inhibition of CK in cultured cardiomyocytes is sufficient to recapitulate both the actin depolymerization defect and the modification of desmin by AGE. Treatment with either cytochalasin D or glyoxal, a cellular AGE, indicated that both actin depolymerization and AGE contribute to desmin disorganization. Heat shock-induced phosphorylation of ␣B-crystallin provides a transient protection of desmin against glyoxal in a p38 MAPK-dependent manner. Our results show that the strong down-regulation of MCK activity contributes to F-actin instability and induces post-translational modification of ␣B-crystallin and desmin. Our results suggest that AGE may play an important role in DCM because they alter the organization of desmin filaments that normally support stress response and mitochondrial functions in cardiomyocytes.

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Section: Left Ventricular Tissue Preparation For Use In Proteomic Andmentioning

confidence: 99%

Muscle Creatine Kinase Deficiency Triggers Both Actin Depolymerization and Desmin Disorganization by Advanced Glycation End Products in Dilated Cardiomyopathy

Diguet

Mallat

Ladouce

et al. 2011

Journal of Biological Chemistry

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“…AGE are a heterogeneous group of compounds, formed by the non-enzymatic reaction between reducing sugars and free amino groups of lipids, proteins or DNA. Modification of AGEs predominantly involves long-lived molecules such as extracellular matrix proteins [8,9]. AGEs accumulate with ageing [8][9][10].…”

Section: Introductionmentioning

confidence: 99%

“…Modification of AGEs predominantly involves long-lived molecules such as extracellular matrix proteins [8,9]. AGEs accumulate with ageing [8][9][10]. However, prolonged hyperglycaemia, dyslipidaemia and oxidative stress in diabetes increases the production and accumulation of AGEs [11] in the kidney and retina and at other sites of microvascular damage [12].…”

Section: Introductionmentioning

confidence: 99%

A developmental nephron deficit in rats is associated with increased susceptibility to a secondary renal injury due to advanced glycation end-products

et al. 2006

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“…These observations are in agreement with previous determinations of AGE accumulation in the renal extracellular matrix and their correlation with circulating AGE peptides. 8 Reduced staining in kidney of the KLHimmunized diabetic rats corroborated the association between circulating AGE levels and development of nephropathy. Immunization of some murine strains 21 as well as Lewis rat 22 with CFA can exacerbate diabetes in the subdiabetogenic STZ protocol.…”

Section: Discussionmentioning

confidence: 68%

“…A number of studies indicate that low molecular weight AGE (LMW-AGE) have increased cytotoxic potential 6 and that their levels in circulation correlate with accumulation in nephrons and impaired kidney function. 7,8 Facile diffusion through microvasculature and interstitial space, resistance to proteolytic degradation, and a high ratio of glycation to peptide mass could enhance their capacity to promote vascular pathology. Accordingly, LMW-AGE are of interest as potential biomarkers in progression of complications and as targets for therapy.…”

mentioning

confidence: 99%

Reactive Immunization Suppresses Advanced Glycation and Mitigates Diabetic Nephropathy

Shcheglova

Makker

Tramontano

2009

Journal of the American Society of Nephrology

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Agents that inhibit glycation end products by reducing the carbonyl load from glycation and glycoxidation are an emerging pharmacologic approach to treat complications of diabetes. We previously demonstrated that antibodies generated to the glycoprotein keyhole limpet hemocyanin (KLH) can cross-link with reactive carbonyl residues on protein conjugates. Here, we immunized streptozotocininduced diabetic rats with KLH to assess the capacity of the elicited antibodies to intercept carbonyl residues on glycated proteins and to mitigate glycation-related pathology. Compared with diabetic rats immunized with adjuvant alone, KLH-immunized diabetic rats had decreased levels of glycated peptides in sera and demonstrated a reduction in albuminuria, proteinuria, deposition of glycation end products in the kidney, and histologic damage. In vitro, low molecular weight glycated peptides from rat serum reacted with anti-KLH antibodies at a faster rate than normal IgG and selectively modified the chains. The reaction products contained peptide sequences from type I collagen ␣ chain, albumin, and LDL receptor-related protein. These adduction reactions were inhibited by free KLH and by reduction of glycated peptides with borohydride. In summary, these results suggest that inherent reactivity of Ig light chains provides a natural mechanism for the removal of cytotoxic glycation products. This reactivity can be augmented by glycoprotein-specific reactive immunization, a potential biopharmaceutical approach to glycation-related pathology.

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Accumulation of Advanced Glycation Endproducts in the Rat Nephron: Link with Circulating AGEs During Aging

Cited by 42 publications

References 41 publications

Muscle Creatine Kinase Deficiency Triggers Both Actin Depolymerization and Desmin Disorganization by Advanced Glycation End Products in Dilated Cardiomyopathy

Muscle Creatine Kinase Deficiency Triggers Both Actin Depolymerization and Desmin Disorganization by Advanced Glycation End Products in Dilated Cardiomyopathy

A developmental nephron deficit in rats is associated with increased susceptibility to a secondary renal injury due to advanced glycation end-products

Reactive Immunization Suppresses Advanced Glycation and Mitigates Diabetic Nephropathy

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