Pore-Forming Proteins from Cnidarians and Arachnids as Potential Biotechnological Tools

Rivera-de-Torre, Esperanza; Palacios-Ortega, Juan; Gavilanes, José G.; Martínez‐del‐Pozo, Álvaro; García‐Linares, Sara

doi:10.3390/toxins11060370

Cited by 18 publications

(20 citation statements)

References 146 publications

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“…[ 3‐5 ] Nonetheless, when isolated, the individual components can have significant potential as therapeutic agents. [ 6‐9 ] Notably, a number of commercially available drugs such as captopril, eptifibatide, tirofiban, ziconotide, and exenatide all have origins in venoms from a variety of organisms. [ 2 ]…”

Section: Introductionmentioning

confidence: 99%

Investigation of the structure‐activity relationship in ponericin L1 from Neoponera goeldii

2020

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Naturally derived antimicrobial peptides have been an area of great interest because of high selectivity against bacterial targets over host cells and the limited development of bacterial resistance to these molecules throughout evolution. There are also a significant number of venom-derived peptides that exhibit antimicrobial activity in addition to activity against mammals or other organisms. Many venom peptides share the same net cationic, amphiphilic nature as host-defense peptides, making them an attractive target for development as potential antibacterial agents. The peptide ponericin L1 derived from Neoponera goeldii was used as a model to investigate the role of cationic residues and net charge on peptide activity. Using a combination of spectroscopic and microbiological approaches, the role of cationic residues and net charge on antibacterial activity, lipid bilayer interactions, and bilayer and membrane permeabilization were investigated. The L1 peptide and derivatives all showed enhanced binding to lipid vesicles containing anionic lipids, but still bound to zwitterionic vesicles. None of the derivatives were especially effective at permeabilizing lipid bilayers in model vesicles, in-tact Escherichia coli, or human red blood cells. Taken together the results indicate that the lack of facial amphiphilicity regarding charge segregation may impact the ability of the L1 peptides to effectively permeabilize bilayers despite effective binding. Additionally, increasing the net charge of the peptide by replacing the lone anionic residue with either Gln or Lys dramatically improved efficacy against several bacterial strains without increasing hemolytic activity. K E Y W O R D S antimicrobial peptides, fluorescence, lipid binding, membrane permeabilization, venom peptides

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Section: Introductionmentioning

confidence: 99%

Investigation of the structure‐activity relationship in ponericin L1 from Neoponera goeldii

2020

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“…Toxins from different origins, have also been employed such as Pseudomonas exotoxin A, Diphteria toxin, actinoporins, gelonin, and the plant toxin ricin, among others [17,18,19,20,21,22,23,24,25,26]. Interestingly, ribonucleases (RNases) have acquired a significant importance due to their ideal features for being included as immunotoxin toxic domains [27,28,29,30,31,32].…”

Section: Introductionmentioning

confidence: 99%

Inclusion of a Furin Cleavage Site Enhances Antitumor Efficacy against Colorectal Cancer Cells of Ribotoxin α-Sarcin- or RNase T1-Based Immunotoxins

Ruiz-de-la-Herrán

Tomé-Amat

Lázaro-Gorines

et al. 2019

Toxins

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Immunotoxins are chimeric molecules that combine the specificity of an antibody to recognize and bind tumor antigens with the potency of the enzymatic activity of a toxin, thus, promoting the death of target cells. Among them, RNases-based immunotoxins have arisen as promising antitumor therapeutic agents. In this work, we describe the production and purification of two new immunoconjugates, based on RNase T1 and the fungal ribotoxin α-sarcin, with optimized properties for tumor treatment due to the inclusion of a furin cleavage site. Circular dichroism spectroscopy, ribonucleolytic activity studies, flow cytometry, fluorescence microscopy, and cell viability assays were carried out for structural and in vitro functional characterization. Our results confirm the enhanced antitumor efficiency showed by these furin-immunotoxin variants as a result of an improved release of their toxic domain to the cytosol, favoring the accessibility of both ribonucleases to their substrates. Overall, these results represent a step forward in the design of immunotoxins with optimized properties for potential therapeutic application in vivo.

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“…Another type of membrane-targeting toxin frequently appearing in venoms does not affect its protein constituents but directly the integrity of the whole structure, maintained mostly by phospholipids. This is the case of the aforementioned phospholipases or the widespread pore-forming proteins (PFPs) [ 12 , 23 , 24 , 25 , 26 , 27 , 28 , 29 , 30 , 31 , 32 ]. Given the critical importance of the plasma membrane for cell viability, its disruption usually has fatal consequences that, in many cases, imply cell death by osmotic shock.…”

Section: Venom Evolutionmentioning

confidence: 99%

“…PFPs are a group of toxins whose activity precisely relies on the disruption of the lipid membranes by forming pores. These kinds of toxins escape to the archetypal biochemical classification that sorts proteins into water-soluble or membrane macromolecules [ 12 , 23 , 24 , 25 , 26 , 27 , 28 , 29 , 30 , 31 , 32 , 34 , 35 , 36 , 37 ]. They are produced as soluble monomeric proteins and remain stably folded and water-soluble but, upon interaction with a membrane receptor in the target cell, undergo a molecular metamorphosis to become an oligomeric transmembrane assemble, that forms a pore within the membrane core.…”

Section: Pore-forming Proteinsmentioning

confidence: 99%

Functional and Structural Variation among Sticholysins, Pore-Forming Proteins from the Sea Anemone Stichodactyla helianthus

Rivera-de-Torre

Palacios-Ortega

Slotte

et al. 2020

IJMS

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Venoms constitute complex mixtures of many different molecules arising from evolution in processes driven by continuous prey–predator interactions. One of the most common compounds in these venomous cocktails are pore-forming proteins, a family of toxins whose activity relies on the disruption of the plasmatic membranes by forming pores. The venom of sea anemones, belonging to the oldest lineage of venomous animals, contains a large amount of a characteristic group of pore-forming proteins known as actinoporins. They bind specifically to sphingomyelin-containing membranes and suffer a conformational metamorphosis that drives them to make pores. This event usually leads cells to death by osmotic shock. Sticholysins are the actinoporins produced by Stichodactyla helianthus. Three different isotoxins are known: Sticholysins I, II, and III. They share very similar amino acid sequence and three-dimensional structure but display different behavior in terms of lytic activity and ability to interact with cholesterol, an important lipid component of vertebrate membranes. In addition, sticholysins can act in synergy when exerting their toxin action. The subtle, but important, molecular nuances that explain their different behavior are described and discussed throughout the text. Improving our knowledge about sticholysins behavior is important for eventually developing them into biotechnological tools.

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Pore-Forming Proteins from Cnidarians and Arachnids as Potential Biotechnological Tools

Cited by 18 publications

References 146 publications

Investigation of the structure‐activity relationship in ponericin L1 from Neoponera goeldii

Investigation of the structure‐activity relationship in ponericin L1 from Neoponera goeldii

Inclusion of a Furin Cleavage Site Enhances Antitumor Efficacy against Colorectal Cancer Cells of Ribotoxin α-Sarcin- or RNase T1-Based Immunotoxins

Functional and Structural Variation among Sticholysins, Pore-Forming Proteins from the Sea Anemone Stichodactyla helianthus

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