Novel Adjuvant Based on the Pore-Forming Protein Sticholysin II Encapsulated into Liposomes Effectively Enhances the Antigen-Specific CTL-Mediated Immune Response

Laborde, Rady J.; Sanchez-Ferras, Oraly; Luzardo, María C.; Cruz‐Leal, Yoelys; Fernández, Audry; Mesa, Circe; Oliver, Liliana; Canet, Liem; Abreu-Butin, Liane; Nogueira, Clara; Tejuca, Mayra; Pazos, Fabiola; Álvarez, Carlos; Alonso, Mercedes; Longo-Maugéri, Ieda Maria; Starnbach, Michael N.; Higgins, Darren E.; Fernández, Luis E.; Lanio, María E.

doi:10.4049/jimmunol.1600310

Cited by 23 publications

(26 citation statements)

References 87 publications

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“…Previous studies revealed that Sticholysin (St) II, an invertebrate PFP produced by the Caribbean Sea anemone Stichodactyla helianthus belonging to the actinoporin family, was encapsulated into liposome to efficiently enhance the antigen-specific CTL responses as an adjuvant and this may not depend on its pore-forming activity. 64,65 However, βγ-CAT is a vertebrate PFP from the frog B. maxima belonging to the aerolysin family. Importantly, the enhanced antigen presentation induced by βγ-CAT depends on its capacity of pore formation in BMDCs.…”

Section: Discussionmentioning

confidence: 99%

A secreted pore‐forming protein modulates cellular endolysosomes to augment antigen presentation

Deng

Liu

et al. 2020

FASEB j.

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Bacterial pore‐forming toxin aerolysin‐like proteins are widely distributed in animals and plants. Emerging evidence supports their roles in host innate immunity, but their direct actions in adaptive immunity remain elusive. In this study, we found that βγ‐CAT, an aerolysin‐like protein and trefoil factor complex identified in the frog Bombina maxima, modulated several steps of endocytic pathways during dendritic cell antigen presentation. The protein augmented the antigen uptake of dendritic cells and actively neutralized the acidification of cellular endocytic organelles to favor antigen presentation. In addition, the release of functional exosome‐like extracellular vesicles was largely enhanced in the presence of βγ‐CAT. The cellular action of βγ‐CAT increased the number of major histocompatibility complex (MHC) I‐ovalbumin and MHC II molecules on dendritic cell surfaces and the released exosome‐like extracellular vesicles. An enhanced antigen presentation capacity of dendritic cell for priming of naive T cells was detected in the presence of βγ‐CAT. Collectively, these effects led to strong cytotoxic T lymphocyte responses and antigen‐specific antibody responses. Our findings provide evidence that a vertebrate‐secreted pore‐forming protein can augment antigen presentation by directly modulating cellular endocytic and exocytic pathways, leading to robust activation of adaptive immunity.

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Section: Discussionmentioning

confidence: 99%

A secreted pore‐forming protein modulates cellular endolysosomes to augment antigen presentation

Deng

Liu

et al. 2020

FASEB j.

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“…Sticholysins I and II (StI and II) are actinoporins produced by the Caribbean Sea anemone Stichodactyla helianthus (23). These toxins are of current interest as an active component of a vaccine platform (24,25) and of immunotoxin constructs active against tumor cells (26,27). Peptides reproducing the N-terminus of StI sequence 1-31 (StI1-31) and StII sequence 1-30 (StII1-30) ( Figure 1A) can mimic the permeabilizing ability of these toxins in red blood cells and liposomes (10,12,13).…”

Section: Introductionmentioning

confidence: 99%

“…Its forms pores in human red blood cells with a similar size to those formed by the full-length toxin (9). StII1-30 has emerged as a good candidate to replace the whole toxins in some biomedical applications such as an active component of a vaccinal platform to promote the delivery of different molecules to the cytosol and enhance the immune response in anti-cancer therapies (24,25). Previously, we have analysed the conformational properties of StI1-31 and StII1-30 in solution and in membrane mimetic systems and their ability to permeabilize lipid vesicles (9,12,13,28,29).…”

Section: Introductionmentioning

confidence: 99%

Membrane remodeling by the lytic fragment of sticholysin II: implications for the toroidal pore model

Mesa-Galloso

Valiente

Epand

et al. 2019

Preprint

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Sticholysins are pore-forming toxins of biomedical interest and represent a prototype of proteins acting through the formation of protein-lipid or toroidal pores. Peptides spanning the N-terminus of sticholysins can mimic their permeabilizing activity and together with the full-length toxins have been used as a tool to understand the mechanism of pore formation in membranes. However, the lytic mechanism of these peptides and the lipid shape modulating their activity are not completely clear. In this paper, we combine molecular dynamics (MD) simulations and experimental biophysical tools to dissect different aspects of the pore-forming mechanism of StII1-30, a peptide derived from the N-terminus of sticholysin II. With this combined approach, membrane curvature induction and flip-flop movement of the lipids were identified as two important membrane remodeling steps mediated by StII1-30-pore forming activity.Pore-formation by this peptide was enhanced by the presence of the negatively-curved lipid phosphatidylethanolamine (PE) in membranes. This lipid emerged not only as a facilitator of membrane interactions but also as a structural element of the StII1-30-pore that is recruited to the pore ring upon its assembly. Collectively, these new findings support a toroidal model for the architecture of the pore formed by this peptide and provide new molecular insight into the role of PE as a membrane component that easily accommodates into the ring of toroidal pores aiding in its stabilization. This study contributes to a better understanding of the molecular mechanism underlying the permeabilizing activity of StII1-30 and peptides or proteins acting via a toroidal pore mechanism and offers an informative framework for the optimization of the biomedical application of this and similar molecules.

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“…Liposomes, such as those used to target T cells, have shown potential use for immunization and vaccine design due to their ability to transfer and release antigenic molecules in APCs and to stimulate the immune response [145][146][147]. It has been previously reported that StII and StII, toxins from the sea anemone S. helianthus encapsulated in a LP/OVA/StII formulation (mixture of SM-free lipid, ovalbumin and the toxin StII) were used to assess their stimulatory effect on a population of Ag-specific CTLs [43]. This suggests that LP/OVA/StII promotes the expansion of antigen-specific CD8+ T cells compared to that achieved using the liposome formulation that contains only the model antigen (LP/OVA).…”

Section: Actinoporins As An Adjuvant For Vaccine Designmentioning

confidence: 99%

“…Two other possible applications of actinoporins that have been sparsely explored. First, as a component of the design of adjuvant tools for vaccine development, actinoporins could act as immunomodulators to enhance the specific cytotoxic cellular response of antigens within various liposomal formulations that could ultimately be used in the development of vaccines against intracellular pathogens or in cancer [43]. Additionally, because of their preference to bind to sphingomyelin, it has been proposed that actinoporins could be a great molecular tool in the analysis of sphingolipid distribution and dynamics in biological membranes [24].…”

Section: Introductionmentioning

confidence: 99%

Actinoporins: From the Structure and Function to the Generation of Biotechnological and Therapeutic Tools

2020

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Actinoporins (APs) are a family of pore-forming toxins (PFTs) from sea anemones. These biomolecules exhibit the ability to exist as soluble monomers within an aqueous medium or as constitutively open oligomers in biological membranes. Through their conformational plasticity, actinoporins are considered good candidate molecules to be included for the rational design of molecular tools, such as immunotoxins directed against tumor cells and stochastic biosensors based on nanopores to analyze unique DNA or protein molecules. Additionally, the ability of these proteins to bind to sphingomyelin (SM) facilitates their use for the design of molecular probes to identify SM in the cells. The immunomodulatory activity of actinoporins in liposomal formulations for vaccine development has also been evaluated. In this review, we describe the potential of actinoporins for use in the development of molecular tools that could be used for possible medical and biotechnological applications.

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Novel Adjuvant Based on the Pore-Forming Protein Sticholysin II Encapsulated into Liposomes Effectively Enhances the Antigen-Specific CTL-Mediated Immune Response

Cited by 23 publications

References 87 publications

A secreted pore‐forming protein modulates cellular endolysosomes to augment antigen presentation

A secreted pore‐forming protein modulates cellular endolysosomes to augment antigen presentation

Membrane remodeling by the lytic fragment of sticholysin II: implications for the toroidal pore model

Actinoporins: From the Structure and Function to the Generation of Biotechnological and Therapeutic Tools

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