A new amperometric glucose microsensor: in vitro and short-term in vivo evaluation

For biosensor fabrication, it is important to optimize materials and methods in order to create predictable function in vitro and in vivo. For this reason. we designed a new glucose sensor ('revised protocol') that utilized an outer permselective membrane made of amphiphobic polyurethane which allows glucose passage through hydrophilic segments. An inner polyethersulfone membrane, stabilized with a trimethoxysilane, provided specificity. Before application of the inner membrane. it was necessary to etch the platinum electrode with a radio frequency oxygen plasma. The revised protocol sensors (n = 185) were compared with sensors fabricated with an earlier ('originals) protocol (n = 204) which used an outer polyurethane without hydrophilic segments and a complex inner membrane of cellulose acetate and Nafion. The function of revised protocol sensors was more predictable in vitro as evidenced by a much lower variation of glucose sensitivity than the original protocol sensors, Revised and original protocol sensors were nearly linear up to a glucose concentration of 20 mM, In vitro interference from 0.1 mM acetaminophen was minimal in both groups of sensors and would be expected to represent about 2% of the total sensor response at normal glucose levels for revised protocol sensors. Prolonged testing of the revised protocol sensors for I I days during immersion in buffer revealed stable sensitivities (day 1: 6.12 +/- 1.34 nA/mM; day 3: 6.33 +/- 1.40; day 8: 7.13 +/- 1.39; and day 11: 7.56 +/- 1.47; sensitivity for day I vs. each other day: not significant) and no critical loss of glucose oxidase activity. The response of the revised protocol sensors (n = 7) to intraperitoncal glucose was tested in rats approximately one day after subcutaneous implantation and the sensors tracked glucose closely with a slight lag of 3-6 min. (C) 2002 Elsevier Science B.V. All rights reserved.