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Influence of inflammatory cells and serum on the performance of implantable glucose sensors
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2001
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| Author: |
Gerritsen, M.
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Jansen, J.A.
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Kros, A.
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Vriezema, D.M.
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Sommerdijk, N.A.J.M.
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Nolte, R.J.M.
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Lutterman, J.A.
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Hövell, S.W.F.M. van
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Gaag, A. van der
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| Keywords: |
Nutrition · Animals · Biocompatible Materials · Biosensing Techniques · Blood Glucose · Buffers · Cellulose · Coated Materials, Biocompatible · Enzymes, Immobilized · Fluorocarbon Polymers · Glucose Oxidase · Granulocytes · Inflammation · Neutrophils · Prostheses and Implants · Rabbits · Zymosan
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The objective of this investigation was to evaluate the influence of polymorphonuclear granulocytes on the performance of uncoated and cellulose acetate/Nafion® coated amperometric glucose sensors in vitro. The response of these sensors was also investigated in serum. Uncoated and coated sensors showed lower sensitivities to glucose, with a significant drift in sensor output upon exposure to serum or leukocytes. Although the use of a coating resulted in higher sensitivity, the progressive loss of output was not completely prevented. Stimulated granulocytes were shown to excrete components, probably catalase and myeloperoxidase, which consumed the hydrogen peroxide formed by the oxidation of glucose. In addition, adsorbed serum proteins formed a diffusional barrier for glucose. Furthermore, serum was found to contain low-molecular weight components that alone inhibited glucose oxidase activity. Based on preliminary electrochemical results, we postulate that rabbit serum contains oxidizing substrates that compete with molecular oxygen for the acceptance of electrons from the oxidized enzyme. Consequently, future efforts should be aimed at elucidating the mechanisms involved in the interference of unknown serum components with electron transfer. In addition, further investigations have to be performed to develop an outer membrane that minimizes protein adsorption as well as the actions of inflammatory cells. (C) 2000 John Wiley and Sons, Inc. Chemicals/CAS: Biocompatible Materials; Blood Glucose; Buffers; Cellulose, 9004-34-6; Coated Materials, Biocompatible; Enzymes, Immobilized; Fluorocarbon Polymers; Glucose Oxidase, EC 1.1.3.4; perfluorosulfonic acid, 39464-59-0; Zymosan, 9010-72-4
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[Abstract]
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| 2 |
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Further studies on mobilization of CFUs
| article |
1979
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| Author: |
Vos, O.
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Wilschut, I.J.C.
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| Keywords: |
Biology · Animal experiment · Blood and hemopoietic system · Bone marrow · Colony forming unit · Hematopoietic cell · Mouse · Animal · Clonogenic assay · Comparative study · Complement activation · Cytology · Drug effect · Hematopoietic stem cell · Male · Physiology · Salmonella typhi · Colony-Forming Units Assay · Complement 3 · Complement Activation · Concanavalin A · Dexamethasone · Hematopoietic Stem Cells · Mice · Phytohemagglutinins · Salmonella typhi · Complement component C3, 80295-41-6 · Concanavalin A, 11028-71-0 · Dexamethasone, 50-02-2 · Dyflos, 55-91-4; · Phytohemagglutinin, 9008-97-3 · Trypsin EC 3.4.21.4, 9002-07-7 · Zymosan, 58856-93-2, 68652-43-7, 9010-72-4 · Complement 3 · Concanavalin A, 11028-71-0 · Isoflurophate, 55-91-4 · Lipopolysaccharides
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Mobilization of CFUs from haemopoietic tissues into circulation was studied after injection of different bacterial lipopolysaccharides (LPS), zymosan, phytohaemagglutinin (PHA), concanavalin A (Con A), trypsin and di-isopropyl-fluorophosphate-inhibited trypsin. All bacterial LPS used gave an increase of CFUs in the peripheral blood at 1 h after i.v. injection. Some variation in activity could not be excluded. As with Salmonella typhosa LPS, zymosan gave an increase in circulating CFUs during the first few hr and a second peak a few days later. After injection of zymosan as well as S. typhosa LPS the second peak in the blood was accompanied by a large increase in CFUs numbers in the spleen. PHA gave an immediate mobilization of CFUs, but the mobilization after injection of Con A during the first few hr occurred more slowly. After injection of S. typhosa LPS, zymosan and PHA the blood C3 level was found to be depressed considerably. This might indicate that the complement system is involved in the early mobilization of CFUs. Dexamethasone, a synthetic hormone which has been reported to give sequestration of several cell types in the bone marrow, did not inhibit the early and late mobilization of CFUs which normally occurs after injection of S. typhosa LPS. Copyright © 1979, Wiley Blackwell. All rights reserved
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[Abstract]
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