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An efficient binding chemistry for glass polynucleotide microarrays.

作者信息

Lee Paul H, Sawan Samuel P, Modrusan Zora, Arnold Lyle J, Reynolds Mark A

机构信息

Incyte Genomics, Microarray Research and Development, 6519 Dumbarton Circle, Fremont, California 94555, USA.

出版信息

Bioconjug Chem. 2002 Jan-Feb;13(1):97-103. doi: 10.1021/bc015523q.

Abstract

A variety of methods have been described for making synthetic polynucleotide microarrays. These include in situ synthesis directly on the array surface, for example, by photolithography or ink-jet printing technologies, and the application of presynthesized polynucleotides that are derivatized with various nucleophiles or electrophiles. In the latter case, a variety of surface chemistries have been developed, and several are available commercially. These chemistries must be compatible with nanoliter-scale volumes of polynucleotide reagents, which contact the array over a small portion of their surface. We reasoned that a three-dimensional polymer coating could potentially offer greater surface contact and higher binding efficiency. Here we describe a polyethylenimine-based coating chemistry that provides exceptional binding and hybridization characteristics. In our preferred process, size-fractionated polyethylenimine polymers are cross-linked onto an aminopropylsilanated glass surface in the presence of cyanuric chloride. The resulting three-dimensional coating binds polynucleotides through a mixture of covalent and noncovalent interactions as evidenced by comparisons between 5'-aminoalkyl modified and unmodified polynucleotides. Binding and hybridization comparisons are presented including analogous two-dimensional electrophilic and electrostatic chemistries.

摘要

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