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Discovery of antimicrobial peptides clostrisin and cellulosin from Clostridium: insights into their structures, co-localized biosynthetic gene clusters, and antibiotic activity

Beilstein Journal of Organic Chemistry. 2024-07; 
Moisés Alejandro Alejo Hernandez , Katia Pamela Villavicencio Sánchez , Rosendo Sánchez Morales , Karla Georgina Hernández-Magro Gil, David Silverio Moreno-Gutiérrez , Eddie Guillermo Sanchez-Rueda , Yanet Teresa-Cruz , Brian Choi, Armando Hernández Garcia , Alba Romero-Rodríguez, Oscar Juárez , Siseth Martínez-Caballero , Mario Figueroa , Corina-Diana Ceap?
Products/Services Used Details Operation
Gene Synthesis We could not access the producing microorganisms, so the gene sequences reported in public databases (Supporting Information File 1, Table S1) were synthesized de novo, cloned, and checked by sequencing using a service (GenScript). First, the clostridial nucleotide sequences were codon adjusted for expression in E. coli using the GenScript tools, cloned in the pRSF-Duet vector in the MCS1 using the restriction enzymes BamHI and SpeI, and verified by sequencing (GenScript). Get A Quote

摘要

Antimicrobial resistance presents a substantial threat to global public health, demanding urgent attention and action. This study focuses on lanthipeptides, ribosomally encoded peptides that display significant structural diversity and hold promising potential as antibiotics. Genome mining was employed to locate biosynthetic gene clusters (BGCs) containing class II lanthipeptide synthetases encoded by lanM genes. A phylogenetic study analyzing homologous sequences of functional LanM sequences revealed a unique evolutionary clade of 17 LanM proteins associated with 12 Clostridium bacterial genomes. In silico exploration identified nine complete BGCs, including one super-cluster containing two co-localized operon... More

關鍵詞

antimicrobials; genome mining; lanthipeptides; lantibiotics; multi-drug resistant bacteria; natural products.
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