Understanding the Mechanism of Action of NAI-112, a Lanthipeptide with Potent Antinociceptive Activity

Tocchetti, Arianna; Iorio, Marianna; Hamid, Zeeshan; Armirotti, Andrea; Reggiani, Angelo; Donadio, Stefano

doi:10.3390/molecules26226764

Cited by 7 publications

(7 citation statements)

References 43 publications

(61 reference statements)

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“…S16B † ). Consistently, when tested against different S. aureus mutants selected through serial passages, phenotypically and genotypically related to vancomycin insensitive S. aureus (VISA) strains, 36 we observed an increase in the MIC of allopeptimicins A (Fig. S16c † ).…”

Section: Resultssupporting

confidence: 73%

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Allopeptimicins: unique antibacterial metabolites generated by hybrid PKS-NRPS, with original self-defense mechanism in Actinoallomurus

Iorio¹,

Gentile²,

Brunati

et al. 2022

RSC Adv.

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Section: Resultssupporting

confidence: 73%

“…Against these same mutants, a similar shi in MICs was observed for other bona de antibiotics that bind to the essential peptidoglycan precursor lipid II such as vancomycin, ramoplanin and NAI-107. 36 Self-defense mechanism in the producer strain Actinoallomurus sp. ID145808…”

Section: Bioactivitymentioning

confidence: 99%

Allopeptimicins: unique antibacterial metabolites generated by hybrid PKS-NRPS, with original self-defense mechanism in Actinoallomurus

Iorio¹,

Gentile²,

Brunati

et al. 2022

RSC Adv.

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“…(Figure ) also showed efficacy in the treatment of neuropathic pain . In mouse model studies, both compounds displayed a decrease in allodynia while NAI-112 also reduced hyperalgesia. , While neither LabyA2 nor NAI-112 have a known MOA for these activities, it has been proposed that NAI-112 may interact with the vanilloid pathway and that the molecule blocks pain sensation by decreasing the levels of lysophosphatidic acid (LPA) and increasing the levels of phosphatidic acid . LPA activates the vanilloid receptor 1 (also known as capsaicin receptor and TRPV1), triggering pain.…”

Section: Lanthipeptides and Compounds Made Via Related Pathwaysmentioning

confidence: 91%

“…LPA activates the vanilloid receptor 1 (also known as capsaicin receptor and TRPV1), triggering pain. NAI-112 also exhibits modest antibiotic activity with micromolar MIC values against various staphylococci and streptococci. , NAI-112 was initially identified as a cell wall inhibitor, with resistance mutants suggesting that the peptidoglycan intermediate lipid II (Figure ) may be a target …”

Section: Lanthipeptides and Compounds Made Via Related Pathwaysmentioning

confidence: 99%

Mechanism of Action of Ribosomally Synthesized and Post-Translationally Modified Peptides

et al. 2022

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Ribosomally synthesized and post-translationally modified peptides (RiPPs) are a natural product class that has undergone significant expansion due to the rapid growth in genome sequencing data and recognition that they are made by biosynthetic pathways that share many characteristic features. Their mode of actions cover a wide range of biological processes and include binding to membranes, receptors, enzymes, lipids, RNA, and metals as well as use as cofactors and signaling molecules. This review covers the currently known modes of action (MOA) of RiPPs. In turn, the mechanisms by which these molecules interact with their natural targets provide a rich set of molecular paradigms that can be used for the design or evolution of new or improved activities given the relative ease of engineering RiPPs. In this review, coverage is limited to RiPPs originating from bacteria.

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“…Fig. S16.A) time-kill profiles of allopeptimicin A against S. aureus ATCC6538P; B) Impact of allopeptimicins A on macromolecules synthesis by S. aureus cells: DNA (blue diamonds), RNA (orange squares), protein (grey triangles), and cell wall (yellow circles); C) growth curve of S. aureus ATCC6538P (dashed lines) and mutant R15.536 (solid lines) in the presence of allopeptimicin A.…”

mentioning

confidence: 99%

Allopeptimicins: unique antibacterial metabolites generated by hybrid PKS-NRPS, with original self-defense mechanism in Actinoallomurus

Iorio¹,

Gentile²,

Brunati³

et al. 2022

Preprint

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In the search for structurally novel metabolites with antibacterial activity, innovative approaches must be implemented to increase the probability of discovering novel chemistry from microbial sources. Here we report on the application of metabolomic tools to the genus Actinoallomurus, a poorly explored member of the Actinobacteria. From examining extracts derived from 88 isolates belonging to this genus, we identified a family of cyclodepsipeptides acylated with a C20 polyketide chain, which we named allopeptimicins. These molecules possess unusual structural features, including several double bonds in the amino-polyketide chain and four non-proteinogenic amino acids in the octapeptide. Remarkably, allopeptimicins are produced as a complex of active and inactive congeners, the latter carrying a sulfate group on the polyketide amine. This modification is also a mechanism of self-protection in the producer strain. The structural uniqueness of allopeptimicins is reflected in a biosynthetic gene cluster showing a mosaic structure, with dedicated gene cassettes devoted to formation of specialized precursors and modular assembly lines related to those from different pathways.

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Understanding the Mechanism of Action of NAI-112, a Lanthipeptide with Potent Antinociceptive Activity

Cited by 7 publications

References 43 publications

Allopeptimicins: unique antibacterial metabolites generated by hybrid PKS-NRPS, with original self-defense mechanism in Actinoallomurus

Allopeptimicins: unique antibacterial metabolites generated by hybrid PKS-NRPS, with original self-defense mechanism in Actinoallomurus

Mechanism of Action of Ribosomally Synthesized and Post-Translationally Modified Peptides

Allopeptimicins: unique antibacterial metabolites generated by hybrid PKS-NRPS, with original self-defense mechanism in Actinoallomurus

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