Literature DB >> 3182935

Binding and transcytosis of glycoalbumin by the microvascular endothelium of the murine myocardium: evidence that glycoalbumin behaves as a bifunctional ligand.

D Predescu1, M Simionescu, N Simionescu, G E Palade.   

Abstract

The binding and transport of glycoalbumin (gA) by the endothelium of murine myocardial microvessels were studied by perfusing in situ 125I-gA or gA-gold complexes (gA-Au) and examining the specimens by radioassays and EM, respectively. After a 3-min perfusion, the uptake of radioiodinated gA is 2.2-fold higher than that of native albumin; it is partially (approximately 55%) competed by either albumin or D-glucose, and almost completely abolished by the concomitant administration of both competitors or by gA. D-mannose and D-galactose are not effective competitors. Unlike albumin-gold complexes that bind restrictively to plasmalemmal vesicles, gA-Au labels the plasma-lemma proper, plasmalemmal vesicles open on the lumen, and most coated pits. Competing albumin prevents gA-Au binding to the membrane of plasmalemmal vesicles, while glucose significantly reduces the ligand binding to plasmalemma proper. Competition with albumin and glucose gives additive effects. Transcytosis of gA-Au, already detected at 3 min, becomes substantial by 30 min. No tracer exit via intercellular junctions was detected. gA-Au progressively accumulates in multivesicular bodies. The results of the binding and competition experiments indicate that the gA behaves as a bifunctional ligand which is recognized by two distinct binding sites: one, located on the plasma membrane, binds as a lectin the glucose residues of gA; whereas the other, confined to plasmalemmal vesicles, recognizes presumably specific domains of the albumin molecule.

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Year:  1988        PMID: 3182935      PMCID: PMC2115328          DOI: 10.1083/jcb.107.5.1729

Source DB:  PubMed          Journal:  J Cell Biol        ISSN: 0021-9525            Impact factor:   10.539


  49 in total

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Authors:  M Brownlee; A Cerami
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3.  Micropinocytic ingestion of glycosylated albumin by isolated microvessels: possible role in pathogenesis of diabetic microangiopathy.

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5.  Increased glycosylation of glomerular basement membrane collagen in diabetes.

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6.  Determinants of the penetration of proteins through the glomerular barrier in insulin-dependent diabetes mellitus.

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7.  Nonenzymatic glycosylation of erythrocyte membrane proteins. Relevance to diabetes.

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8.  Glucosylation of human collagen in aging and diabetes mellitus.

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9.  Protein and cell membrane iodinations with a sparingly soluble chloroamide, 1,3,4,6-tetrachloro-3a,6a-diphrenylglycoluril.

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10.  Nonenzymatic glycosylation, sulfhydryl oxidation, and aggregation of lens proteins in experimental sugar cataracts.

Authors:  V M Monnier; V J Stevens; A Cerami
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Authors:  D Predescu; S Predescu; T McQuistan; G E Palade
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9.  Prevention of diabetic nephropathy in db/db mice with glycated albumin antagonists. A novel treatment strategy.

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