1995
DOI: 10.1093/nar/23.13.2404
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Electrophoresis for genoptyping:temporal thermal gradient gel electrophoreisis for profiling of oiligonucleotide dissociation

Abstract: Traditional use of an oligonucleotide probe to determine genotype depends on perfect base pairing to a single-stranded target which is stable to a higher temperature than when imperfect binding occurs due to a mismatch in the target sequence. Bound oligonucleotide is detected at a predetermined single temperature 'snapshot' of the melting profile, allowing the distinction of perfect from imperfect base pairing. In heterozygotes, the presence of the alternative sequence must be verified with a second oligonucle… Show more

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Cited by 11 publications
(1 citation statement)
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“…We have configured an approach compatible with MADGE, in which the independent variable is temporal rather than spatial and the dependent (denaturing) variable is thermal rather than chemical. Originally, the system was designed to determine complete sequence-specific oligonucleotide melting profiles from target sequences differing by a single base [10] and then adapted for DGGE-like examination of full duplexes, for de novo mutation scanning. This confers several advantages.…”
Section: Temporal Thermal Ramp Electrophoresis Madge (Melt-madge)mentioning
confidence: 99%
“…We have configured an approach compatible with MADGE, in which the independent variable is temporal rather than spatial and the dependent (denaturing) variable is thermal rather than chemical. Originally, the system was designed to determine complete sequence-specific oligonucleotide melting profiles from target sequences differing by a single base [10] and then adapted for DGGE-like examination of full duplexes, for de novo mutation scanning. This confers several advantages.…”
Section: Temporal Thermal Ramp Electrophoresis Madge (Melt-madge)mentioning
confidence: 99%