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Novel amplified fragment length polymorphism (AFLP) markers for typing medically relevant and allied fusarioid genera. | LitMetric

Novel amplified fragment length polymorphism (AFLP) markers for typing medically relevant and allied fusarioid genera.

Fungal Syst Evol

Laboratory of Emerging Fungal Pathogens, Department of Microbiology, Immunology, and Parasitology, Discipline of Cellular Biology, Federal University of São Paulo (UNIFESP), São Paulo 04023062, Brazil.

Published: June 2025


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Article Abstract

Fusariosis is an emerging mycosis caused by diverse and allied fusarioid genera that are characterized by spindle-shaped macroconidia. These fungi possess a broad ecological distribution, causing infections in a wide diversity of hosts, spanning the animal and plant kingdoms. The spectrum of human fusariosis encompasses superficial lesions like keratitis and onychomycosis to invasive fungal diseases. Notable genera within the medically relevant fusarioid group include , and . While species (formerly species complex) are primary causative agents of human fusariosis, instances involving and (formerly species complex) have been reported. There is an urgent need for DNA-based markers to explore the epidemiology of these emerging fusarioid pathogens using molecular methods. We took advantage of fusarioid genomes available in NCBI (n = 20) to optimize the development of novel amplified fragment length polymorphism (AFLP) markers by conducting in-depth analyses to refine their applicability for studies on these pathogens' genetic epidemiology. screening highlighted eight primer pair combinations (C1-C8) to be tested . The AFLP protocol was used for genotyping 40 medically relevant fusarioid fungi. Based on the overall scored AFLP markers (77-93 fragments), the values of polymorphism information content ( = 0.3474-0.3725), marker index ( = 0.0038-0.0056), effective multiplex ratio ( = 26.3750-40.4750), resolving power ( = 40.1500-54.6000), discriminating power ( = 0.7978-0.8857), expected heterozygosity ( = 0.4476-0.4949), and mean heterozygosity ( = 0.0001) demonstrated the utility of these primer combinations for discriminating ., and species. Of relevance, some AFLP panels were better than others at studying genetic trends in (#2 EcoRI-AT/MseI-TA, #3 EcoRI-AA/MseI-TT, and #5 EcoRI-AT/MseI-AG) or (mainly #2 EcoRI-AT/MseI-TA and #6 EcoRI-GA/MseI-TT) and (#1 EcoRI-GA/MseI-AG and #6 EcoRI-GA/MseI-TT), and these combinations will better resolve disease transmission routes. Our DNA fingerprint assay has proven effective by exhibiting rapidity, reproducibility, and high discriminatory capabilities, which represents a valuable asset in the ongoing efforts to combat fusariosis and enhance our scientific understanding of medically relevant and allied fusarioid genera. Monteiro RC, Yu CZ, Dolatabadi S, Hagen F, Sandoval-Denis M, Crous PW, Fisher MC, Gonçalves SS, de Camargo ZP, Hofling-Lima AL, Rodrigues AM (2025). Novel amplified fragment length polymorphism (AFLP) markers for typing medically relevant and allied fusarioid genera. : 79-96. doi: 10.3114/fuse.2025.15.03.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11959234PMC
http://dx.doi.org/10.3114/fuse.2025.15.03DOI Listing

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