作者
Kerry O'Donnell, Deanna A Sutton, Michael G Rinaldi, Brice AJ Sarver, S Arunmozhi Balajee, Hans-Josef Schroers, Richard C Summerbell, Vincent ARG Robert, Pedro W Crous, Ning Zhang, Takayuki Aoki, Kyongyong Jung, Jongsun Park, Yong-Hwan Lee, Seogchan Kang, Bongsoo Park, David M Geiser
发表日期
2010/10
期刊
Journal of Clinical Microbiology
卷号
48
期号
10
页码范围
3708-3718
出版商
American Society for Microbiology
简介
Because less than one-third of clinically relevant fusaria can be accurately identified to species level using phenotypic data (i.e., morphological species recognition), we constructed a three-locus DNA sequence database to facilitate molecular identification of the 69 Fusarium species associated with human or animal mycoses encountered in clinical microbiology laboratories. The database comprises partial sequences from three nuclear genes: translation elongation factor 1α (EF-1α), the largest subunit of RNA polymerase (RPB1), and the second largest subunit of RNA polymerase (RPB2). These three gene fragments can be amplified by PCR and sequenced using primers that are conserved across the phylogenetic breadth of Fusarium. Phylogenetic analyses of the combined data set reveal that, with the exception of two monotypic lineages, all clinically relevant fusaria are nested in one of eight variously sized …
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