Mycotoxigenic potential of Penicillium species isolated from fresh chestnuts and derived products.
Contributo in Atti di convegno
Data di Pubblicazione:
2023
Abstract:
Species of genus Penicillium produce a great variety of secondary
metabolites, including mycotoxins. This characteristic
is associated with the presence of biosynthetic enzymes
organized in biosynthetic gene clusters (BGCs). In the present
work, the genomes of ten Penicillium species isolated
from fresh chestnuts and derived products were sequenced
and annotated. Predicted protein sequences were pooled
with those of previously annotated Penicillium spp. and
outgroup species in the Eurotiales order to generate phylomes.
Phylome data was parsed using the protein sequence
of enzymes experimentally associated with the production
of target mycotoxins (patulin, andrastin A, mycophenolic
acid, penitrem A, meleagrin and verrucosidin) to identify putative homologues in the new strains’ proteome. Production
of associated mycotoxins was verified by both HPLCDAD
and HPLC-MS/MS on whole mycelium extracts.
Results of bioinformatic analyses showed the presence of a
complete andrastin A cluster in Penicillium bialowiezense,
Penicillium crustosum, Penicillium glandicola and Penicillium
taurinense; a complete mycophenolic acid cluster
in P. bialowiezense; a complete penitrem A cluster in P.
crustosum and P. glandicola; a shortened, biosynthetically
active roquefortine C cluster in P. crustosum and P. taurinense,
as well as a complete meleagrin cluster in P. glandicola.
In addition, putative partial andrastin A clusters from
Penicillium palitans and Penicillium discolor were subsequently
identified as an atlantinone A cluster. For all of
them, chemical analyses confirmed production of the associated
metabolite. These results elucidate the genetic bases
of mycotoxin production and permit the evaluation of the
evolution of BGCs in different species of Penicillium spp.
Tipologia CRIS:
04B-Conference paper in rivista
Elenco autori:
M. Garello, E. Piombo, S. Valente, G. R. Meloni, S. Prencipe, F. Buonsenso, M. Marcet‑Houben, T. Gabaldon,
D. Spadaro
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