Enhanced podophyllotoxin production of endophyte Fusarium proliferatum TQN5T by host extract and phenylalanine

Giang Thu Nguyen; Ha Thi Hong Nguyen; Hoa Thi Tran; Huyen Thi Tran; Anh Ngoc Ho; Quang Ho Tran; Ngoc Bich Pham

doi:10.1007/s00253-023-12659-1

Enhanced podophyllotoxin production of endophyte Fusarium proliferatum TQN5T by host extract and phenylalanine

Appl Microbiol Biotechnol. 2023 Sep;107(17):5367-5378. doi: 10.1007/s00253-023-12659-1. Epub 2023 Jul 12.

Authors

Giang Thu Nguyen¹, Ha Thi Hong Nguyen¹, Hoa Thi Tran^{1

2}, Huyen Thi Tran¹, Anh Ngoc Ho¹, Quang Ho Tran^{1

2}, Ngoc Bich Pham^{3

4}

Affiliations

¹ Institute of Biotechnology, Vietnam Academy of Science and Technology, Hanoi, Vietnam.
² Graduate University of Science and Technology, Vietnam Academy of Science and Technology, Hanoi, Vietnam.
³ Institute of Biotechnology, Vietnam Academy of Science and Technology, Hanoi, Vietnam. pbngoc@ibt.ac.vn.
⁴ Graduate University of Science and Technology, Vietnam Academy of Science and Technology, Hanoi, Vietnam. pbngoc@ibt.ac.vn.

PMID: 37436482
DOI: 10.1007/s00253-023-12659-1

Abstract

Fermentation technology using endophytes is considered a potential alternative approach for producing pharmaceutical compounds like podophyllotoxin (PTOX). In this study, fungus TQN5T (VCCM 44284) was selected from endophytic fungi isolated from Dysosma versipellis in Vietnam for PTOX production through TLC. The presence of PTOX in TQN5T was further confirmed by HPLC. Molecular identification indicated TQN5T as Fusarium proliferatum with 99.43% identity. This result was asserted by morphological characteristics such as white cottony, filamentous colony, layer and branched mycelium, and clear hyphae septa. Cytotoxic assay indicated both biomass extract and culture filtrate of TQN5T presented strong cytotoxicity on LU-1 and HepG2 with IC50 of 0.11, 0.20, 0.041, and 0071, respectively, implying anti-cancer compounds were accumulated in the mycelium and secreted into the medium. Further, the production of PTOX in TQN5T was investigated in the fermentation condition supplemented with 10 µg/ml of host plant extract or phenylalanine as elicitors. The results revealed a significantly higher amount of PTOX in the PDB + PE and PDB + PA at all studied time points in comparison with PDB (control). Especially, after 168 h of culture, PTOX content in the PDB with plant extract reached the peak with 314 µg/g DW which is 10% higher than the best yield of PTOX in previous studies, denoting F. proliferatum TQN5T as a promising PTOX producer. This is the first study on enhancing the PTOX production in endophytic fungi by supplementing phenylalanine-a precursor for PTOX biosynthesis in plants into fermented media, suggesting a common PTOX biosynthetic pathway between host plant and endophytes. KEY POINTS: • Fusarium proliferatum TQN5T was proven for PTOX production. • Both mycelia extract and spent broth extract of Fusarium proliferatum TQN5T presented strong cytotoxicity on cancer cell lines LU-1 and HepG2. • The supplementation of 10 µg/ml host plant extract and phenylalanine into fermentation media of F. proliferatum TQN5T improved the yield of PTOX.

Keywords: Anti-cancer compounds; Cytotoxic assay; Elicitor; Endophytes; Fermentation.

MeSH terms

Endophytes / metabolism
Fusarium* / metabolism
Plant Extracts / metabolism
Plants / metabolism
Podophyllotoxin* / metabolism

Substances

Podophyllotoxin
Plant Extracts

Supplementary concepts

Fusarium proliferatum

Grants and funding

TDCN.01/ 20-22/Vietnam Academy of Science and Technology