Cell-type-specific and site-specific N-glycosylation of type I and type II human tissue plasminogen activator

Parekh, Raj B.; Dwek, Raymond A.; Thomas, Jerry R.; Opdenakker, Ghislain; Rademacher, Thomas W.; Wittwer, Arthur J.; Howard, Susan C.; Nelson, Rickey; Siegel, Ned R.; Jennings, Michael P.; Harakas, Nikos K.; Feder, Joseph

doi:10.1021/bi00445a021

Cited by 163 publications

(114 citation statements)

References 39 publications

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“…5a and b). The differences in these profiles, which compare the overall glycosylation of CD59 expressed in two different cell types, confirm previous findings that glycosylation is cell type-specific (41). There are more than 40 peaks in each of these profiles indicating that platelet and erythrocyte CD59 are both expressed as a population of many different glycoforms.…”

Section: Comparison Of the Glycosylation Profiles Of Humansupporting

confidence: 71%

The Glycosylation of the Complement Regulatory Protein, Human Erythrocyte CD59

Rudd

Morgan

Wormald

et al. 1997

Journal of Biological Chemistry

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164

103

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Section: Comparison Of the Glycosylation Profiles Of Humansupporting

confidence: 71%

The Glycosylation of the Complement Regulatory Protein, Human Erythrocyte CD59

Rudd

Morgan

Wormald

et al. 1997

Journal of Biological Chemistry

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164

103

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“…The N-linked carbohydrate chains of K,tu-PA were completely a(l-6)-fucosylated at the innermost GlcNAc residue. The i-ecombinant t-PA [45] and variant recombinant t-PA [53], expressed in CHO cells, are also almost fully fucosylated, whereas human colon fibroblast t-PA is fucosylated for 58% [8]. Other structural differences occur in the ratio of tri-and tri'-antennary structures, being about 1 : 3 for K,tu-PA, 1 : 8 for human colon fibroblast t-PA, 1 : 1.3 for recombinant t-PA [45], and 1 : 4.4 for variant recombinant t-PA [53].…”

Section: Discussionmentioning

confidence: 99%

“…In t-PA from human colon fibroblast and Bowes melanoma cells, the oligosaccharides bound to Asnll7 are predominantly of the oligomannose type [8]. The oligosaccharides at Asn184 and Asn448 comprise predominantly Nacetyllactosamine type of structures in the case of human colon fibroblast cells [8], and contain predominantly GalNAcPl4GlcNAc elements in the case of Bowes melanoma cells [9]. The presence and the nature of the N-linked carbohydrate chains in t-PA have been reported to play a role in various biological phenomena [lo-121.…”

mentioning

confidence: 99%

Primary structure of N‐linked carbohydrate chains of a human chimeric plasminogen activator K₂tu‐PA expressed in Chinese hamster ovary cells

Bergwerff

Oostrum

Asselbergs

et al. 1993

European Journal of Biochemistry

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A recombinant human plasminogen activator hybrid variant KJu-PA, expressed in Chinese hamster ovary cells, is partially glycosylated at Asnl2 (A chain, kringle-2 domain) and completely glycosylated at Asn247 (B chain, protease domain). After release of the N-linked carbohydrate chains by peptide-N4-(N-acetyl-/3-glucosaminyl)asparagine amidase F, the oligosaccharides were separated from the protein by gel permeation chromatography, then fractionated by FPLC on Mono Q, followed by HPLC on Lichrosorb-NH,, and analysed by 500-MHz 'H-NMR spectroscopy. The following types of carbohydrates occur : monosialylated diantennary (8 %), disialylated diantennary (45 %), disialylated tri-and tri'-antennary (1 %), trisialylated tri-and tri'-antennary (28 %), and tetrasialylated tetra-antennary (18 %) structures, all having fucose in a(l-g)-linkage at the Asn-bound Nacetylglucosamine. Sialic acid occurred exclusively in a(2-3)-linkage to galactose, and consisted of N-acetylneuraminic acid (94 %), N-glycolylneuraminic acid (3 %), and N-acetyl-9-O-acetylneuraminic acid (3%). In addition, glycopeptide fragments corresponding with the A or B chain of K,tu-PA were analysed. The oligosaccharides attached to Asnl2 are less processed than those attached to Asn247. Comparison of the glycosylation pattern of K,tu-PA with that of tissue-type plasminogen activator from different biological sources showed significant differences.Profiling studies on different K,tu-PA production batches demonstrated that the structures of Nlinked oligosaccharides were identical, but that relative amounts vary with the applied isolation procedure of the chimeric glycoprotein.Plasminogen activators (PA) are serine proteases, that convert the inactive proenzyme plasminogen into the active enzyme plasmin, thereby functioning as important initiators of fibrinolysis. Two types of plasminogen activators can be distinguished, namely, the urinary-type (urokinase, u-PA) and the tissue-type (t-PA) [l]. Urokinase and recombinant t-PA are of clinical interest for the treatment of acute vascular diseases like myocardial infarction [2-41. To obtain artery reperfusion, high blood levels of PA are required, because of its rapid clearance by the liver. Such pharmaceutical use is associated with a variable degree of systemic fibrinolytic acCorrespondence to J. P. Kamerling, Bijvoet Center, Department of Bio-Organic Chemistry, Utrecht University, P. 0. Box 80.075, NL-3508 TB Utrecht, The Netherlands Abbreviations. PNGase-F, peptide-P-(N-acetyl-/%glucosaminyl)-asparagine amidase F; PA, plasminogen activator; u-PA, urinarytype plasminogen activator; t-PA, tissue-type plasminogen activator; CHO, Chinese hamster ovary ; NeuSAc, N-acetylneuraminic acid; NeuSGc, N-glycolylneuraminic acid ; Neu5,9Ac2, N-acetyl-9-O-acetylneuraminic acid; lD, one-dimensional ; 2D, two-dimensional; HOHAHA, homonuclear Hartmann-Hahn ; MLEV, composite pulse devised by Malcom Levitt; COSY, scalar shift correlated spectroscopy ; ROESY, rotating-frame nuclear Overhauser enhancement spectroscopy.Enzymes. Peptid...

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“…(Greenwich, CT). Monoclonal antibody 79 -7 against HCF-t-PA was obtained as described previously (25). Purified HCF t-PA and HCF t-PA⅐PAI-1 complexes were kindly provided by Dr. A. Wittwer (Monsanto Co., St. Louis, MO).…”

Section: Methodsmentioning

confidence: 99%

Low Density Lipoprotein Receptor-related Protein Modulates the Expression of Tissue-type Plasminogen Activator in Human Colon Fibroblasts

Hardy

Feder

Wolfe

et al. 1997

Journal of Biological Chemistry

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Human colon fibroblasts (HCF) produce tissue-type plasminogen activator (t-PA) in culture, but after 24 -48 h, t-PA ceases to accumulate in the medium. Here, we report negative feedback regulation of t-PA expression, exerted by t-PA or complexes of t-PA with its physiological inhibitor, plasminogen activator inhibitor type 1 (PAI-1). Inhibition of t-PA expression could be induced by addition of exogenous t-PA or t-PA⅐PAI-1 complexes and reversed by monoclonal antibody directed against the active site of t-PA. Analysis of metabolically radiolabeled protein and cellular mRNA showed that both t-PA protein and mRNA levels declined considerably after 24 h. When 125 I-labeled t-PA or t-PA⅐PAI-1 complexes were incubated with HCF, monensin-inhibitable endocytosis and catabolism were observed. The low density lipoprotein receptor-related protein (LRP) was found to be expressed by HCF and to mediate these events. Addition of the 39-kDa receptor-associated protein (RAP), an antagonist for ligand interactions with LRP, removed the block to t-PA expression and restored its accumulation in the medium. Moreover, RAP completely prevented the degradation of exogenous 125 I-labeled t-PA by HCF, suggesting that LRP is the endocytic receptor for t-PA in these cells. These results demonstrate that cellular modulation of t-PA expression in HCF involves LRP receptor-mediated clearance of t-PA. This LRP receptor-mediated event results in down-regulation of t-PA expression at the mRNA level.Fibrinolysis is a complex process that requires precise regulation in vivo to ensure that it is neither deficient nor excessive. The plasminogen activator system is critical for thrombolysis, as well as other physiological processes including cell migration and tissue remodeling (1, 2). Human tissue-type plasminogen activator (t-PA) 1 (M r 68,000), a key serine protease in this system, is of particular pharmacological interest because of its value in the treatment of thromboembolic disorders. Regulation of the plasminogen activator system involves modulation by cofactors and inhibitors as well as controlled synthesis of the key components. It is well documented that t-PA expression is influenced by a variety of exogenous factors such as hormones, growth factors, and cytokines (3-6). Regulation by these factors appears to be receptor-mediated and is imposed at the transcriptional level (7-10). However, information on the role of t-PA in the local regulation of its own biosynthesis, release, and clearance is limited. Kadouri and Bohak (11) suggested a negative feedback-type control for t-PA expression in human lung fibroblasts but did not identify the mechanism by which expression was regulated. Although t-PA has been reported to undergo receptor-mediated binding to a variety of cultured cells (12-15), the biological significance of this phenomenon remains uncertain. Reports on the internalization and lysosomal degradation of t-PA have been largely confined to studies on hepatocytes, which have a known clearance function (for reviews, see Refs. 16,17)....

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Cell-type-specific and site-specific N-glycosylation of type I and type II human tissue plasminogen activator

Cited by 163 publications

References 39 publications

The Glycosylation of the Complement Regulatory Protein, Human Erythrocyte CD59

The Glycosylation of the Complement Regulatory Protein, Human Erythrocyte CD59

Primary structure of N‐linked carbohydrate chains of a human chimeric plasminogen activator K₂tu‐PA expressed in Chinese hamster ovary cells

Low Density Lipoprotein Receptor-related Protein Modulates the Expression of Tissue-type Plasminogen Activator in Human Colon Fibroblasts

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Cell-type-specific and site-specific N-glycosylation of type I and type II human tissue plasminogen activator

Cited by 163 publications

References 39 publications

The Glycosylation of the Complement Regulatory Protein, Human Erythrocyte CD59

The Glycosylation of the Complement Regulatory Protein, Human Erythrocyte CD59

Primary structure of N‐linked carbohydrate chains of a human chimeric plasminogen activator K2tu‐PA expressed in Chinese hamster ovary cells

Low Density Lipoprotein Receptor-related Protein Modulates the Expression of Tissue-type Plasminogen Activator in Human Colon Fibroblasts

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Primary structure of N‐linked carbohydrate chains of a human chimeric plasminogen activator K₂tu‐PA expressed in Chinese hamster ovary cells