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Dive into the research topics where Hassan Rokni-Zadeh is active.

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Featured researches published by Hassan Rokni-Zadeh.


PLOS ONE | 2013

The Antimicrobial Compound Xantholysin Defines a New Group of Pseudomonas Cyclic Lipopeptides

Wen Li; Hassan Rokni-Zadeh; Matthias De Vleeschouwer; Maarten G. K. Ghequire; Davy Sinnaeve; Guanlin Xie; Jef Rozenski; Annemieke Madder; José Martins; René De Mot

The rhizosphere isolate Pseudomonas putida BW11M1 produces a mixture of cyclic lipopeptide congeners, designated xantholysins. Properties of the major compound xantholysin A, shared with several other Pseudomonas lipopeptides, include antifungal activity and toxicity to Gram-positive bacteria, a supportive role in biofilm formation, and facilitation of surface colonization through swarming. Atypical is the lipopeptide’s capacity to inhibit some Gram-negative bacteria, including several xanthomonads. The lipotetradecadepsipeptides are assembled by XtlA, XtlB and XtlC, three co-linearly operating non-ribosomal peptide synthetases (NRPSs) displaying similarity in modular architecture with the entolysin-producing enzymes of the entomopathogenic Pseudomonas entomophila L48. A shifted serine-incorporating unit in the eight-module enzyme XtlB elongating the central peptide moiety not only generates an amino acid sequence differing at several equivalent positions from entolysin, but also directs xantholysin’s macrocyclization into an octacyclic structure, distinct from the pentacyclic closure in entolysin. Relaxed fatty acid specificity during lipoinitiation by XtlA (acylation with 3-hydroxydodec-5-enoate instead of 3-hydroxydecanoate) and for incorporation of the ultimate amino acid by XtlC (valine instead of isoleucine) account for the production of the minor structural variants xantholysin C and B, respectively. Remarkably, the genetic backbones of the xantholysin and entolysin NRPS systems also bear pronounced phylogenetic similarity to those of the P. putida strains PCL1445 and RW10S2, albeit generating the seemingly structurally unrelated cyclic lipopeptides putisolvin (undecapeptide containing a cyclotetrapeptide) and WLIP (nonapeptide containing a cycloheptapeptide), respectively. This similarity includes the linked genes encoding the cognate LuxR-family regulator and tripartite export system components in addition to individual modules of the NRPS enzymes, and probably reflects a common evolutionary origin. Phylogenetic scrutiny of the modules used for selective amino acid activation by these synthetases indicates that bacteria such as pseudomonads recruit and reshuffle individual biosynthetic units and blocks thereof to engineer reorganized or novel NRPS assembly lines for diversified synthesis of lipopeptides.


Microbial Ecology | 2011

PCR Detection of Novel Non-ribosomal Peptide Synthetase Genes in Lipopeptide-Producing Pseudomonas

Hassan Rokni-Zadeh; Alba Mangas-Losada; René De Mot

Bacterial lipopeptides (LPs) are a diverse group of secondary metabolites synthesized through one or more non-ribosomal peptide synthetases (NRPSs). In certain genera, such as Pseudomonas and Bacillus, these enzyme systems are often involved in synthesizing biosurfactants or antimicrobial compounds. Several different types of LPs have been reported for non-pathogenic plant-associated Pseudomonas. Focusing on this group of bacteria, we devised and validated a PCR method to detect novel LP-synthesizing NRPS genes by targeting their lipoinitiation and tandem thioesterase domains, thus avoiding amplification of genes for non-LP metabolites, such as the pyoverdine siderophores present in all fluorescent Pseudomonas. This approach enabled detection of as yet unknown NRPS genes in strains producing viscosin, viscosinamide, WLIP, or lokisin. Furthermore, it proved valuable to identify novel candidate LP producers among Pseudomonas rhizosphere isolates. By phylogenetic analysis of these amplicons, several of the corresponding NRPS genes can be tentatively assigned to the viscosin, amphisin, or entolysin biosynthetic groups, while some others may represent novel NRPS systems.


ChemBioChem | 2014

Impact of a stereocentre inversion in cyclic lipodepsipeptides from the viscosin group: a comparative study of the viscosinamide and pseudodesmin conformation and self-assembly.

Niels Geudens; Matthias De Vleeschouwer; Krisztina Fehér; Hassan Rokni-Zadeh; Maarten G. K. Ghequire; Annemieke Madder; René De Mot; José Martins; Davy Sinnaeve

The viscosin group covers a series of cyclic lipodepsipeptides (CLPs) produced by Pseudomonas bacteria, with a range of biological functions and antimicrobial activities. Their oligopeptide moieties are composed of both L‐ and D‐amino acids. Remarkably, the Leu5 amino acid—centrally located in the nonapeptide sequence—is the sole residue found to possess either an L or D configuration, depending on the producing strain. The impact of this D/L switch on the solution conformation was investigated by NMR‐restrained molecular modelling of the epimers pseudodesmin A and viscosinamide A. Although the backbone fold remained unaffected, the D/L switch adjusted the segregation between hydrophobic and hydrophilic residues, and thus the amphipathicity. It also influenced the self‐assembly capacity in organic solvents. Additionally, several new minor variants of viscosinamide A from Pseudomonas fluorescens DR54 were identified, and an NMR assay is proposed to assess the presence of either an L‐ or D‐Leu5.


Genome Announcements | 2013

Draft Genome Sequence of Pseudomonas fluorescens LMG 5329, a White Line-Inducing Principle-Producing Bioindicator for the Mushroom Pathogen Pseudomonas tolaasii

Maarten G. K. Ghequire; Hassan Rokni-Zadeh; Peyman Zarrineh; René De Mot

ABSTRACT Pseudomonas tolaasii, the causative agent of Agaricus bisporus brown blotch disease, can be identified by the white line reaction, occurring upon confrontation of the tolaasin-producing mushroom pathogen with “Pseudomonas reactans,” producing the lipopeptide white line-inducing principle (WLIP). The draft genome sequence of the WLIP-producing indicator Pseudomonas fluorescens strain LMG 5329 is reported here.


Environmental Microbiology Reports | 2013

Distinct lipopeptide production systems for WLIP (white line‐inducing principle) in Pseudomonas fluorescens and Pseudomonas putida

Hassan Rokni-Zadeh; Wen Li; Eshetu Yilma; Aminael Sánchez-Rodríguez; René De Mot


Genome Announcements | 2018

Draft Genome Sequence of Pseudomonas gingeri Strain LMG 5327, the Causative Agent of Ginger Blotch in Agaricus bisporus

Tahereh Bahrami; Samira Zarvandi; René De Mot; Harald Gross; Majid Changi-Ashtiani; Tina Shahani; Hassan Rokni-Zadeh


Belgian Peptide Group, 2nd Meeting, Abstracts | 2014

Exploration on structure activity relation of natural, self-assembling cyclic lipodepsipeptides

Niels Geudens; Kristina Feher; Matthias De Vleeschouwer; Jean-Marc Crowet; Mehmet Nail Nasir; Hassan Rokni-Zadeh; René De Mot; Annemieke Madder; Laurence Lins; José Martins; David Sinnaeve


Antimicrobial Peptides, 4th International symposium, Abstracts | 2014

Membrane interactions of natural cyclic lipodepsipeptides

Niels Geudens; Krisztina Fehér; Matthias De Vleeschouwer; Jean-Marc Crowet; Mehmet Nail Nasir; Hassan Rokni-Zadeh; René De Mot; Annemieke Madder; Laurence Lins; José Martins; Davy Sinnaeve


Pseudomonas, 14th International conference, Abstracts | 2013

Xantholysin and promysalin, novel antimicrobial secondary metabolites from Pseudomonas putida rhizosphere isolates

Wen Li; Matthias De Vleeschouwer; Maarten G. K. Ghequire; Davy Sinnaeve; Hassan Rokni-Zadeh; Annemieke Madder; Jef Rozenski; José Martins; René De Mot


Genome Announcements | 2013

Draft genome sequence of Pseudomonas fluorescens LMG 5329, a WLIP-producing bioindicator for the mushroom pathogen Pseudomonas tolaasii

Maarten G. K. Ghequire; Hassan Rokni-Zadeh; Peyman Zarrineh; René De Mot

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René De Mot

Katholieke Universiteit Leuven

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Maarten G. K. Ghequire

Katholieke Universiteit Leuven

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Wen Li

Katholieke Universiteit Leuven

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