Analysis of tyrosinase gene mutations using direct automated infrared fluorescence DNA sequencing of amplified exons

Artigo Revisado por pares

Analysis of tyrosinase gene mutations using direct automated infrared fluorescence DNA sequencing of amplified exons

1994; Wiley; Volume: 15; Issue: 1 Linguagem: Inglês

10.1002/elps.1150150127

ISSN

1522-2683

Autores

William S. Oetting, James P. Fryer, Yasuhisa Oofuji, Lyle R. Middendorf, John Brumbaugh, C. Gail Summers, Richard A. King,

Tópico(s)

Identification and Quantification in Food

Resumo

Abstract The ability to correctly diagnose the molecular cause of genetic diseases is becoming increasingly important in medicine. This requires an efficient method for the analysis of the DNA sequence of specific genes and the detection of mutations in affected individuals. We report a method to determine the mutations responsible for tyrosinase related albinism (OCA1) using a combination of polymerase chain reaction‐single stranded conformational polymorphism (PCR‐SSCP) analysis and direct DNA cycle sequencing using fluorescently labeled oligonucleotides and an automated DNA sequencer based on infrared fluorescence technology. This method allows DNA from several individuals to be sequenced quickly and simultaneously so that the specific location of each mutation and the carrier status of family members can be determined.

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Analysis of tyrosinase gene mutations using direct automated infrared fluorescence DNA sequencing of amplified exons