Development of a Platform of Antibody-Presenting Liposomes

Garnier, Boris; Tan, Sisareuth; Gounou, Céline; Brisson, Alain; Laroche‐Traineau, Jeanny; Jacobin‐Valat, Marie‐Josée; Clofent‐Sanchez, Gisèle

doi:10.1007/s13758-011-0011-9

Cited by 5 publications

(8 citation statements)

References 31 publications

(39 reference statements)

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“…EPR effect is a “gold standard” for the anticancer drug design and for targeting sites of tissue inflammation [27], [28], [29], [30]. Targeting to specific tissues is the most promising attribute of the NPs [14], [31], [32]. Therefore, to reach that capability, it is needed the covalent attachment of a defined ligand at the surface of the NP, which will specifically interact with antigens or receptors expressed at the surface of the target cells [33].…”

Section: Nanoparticles As Bioactive Agents Release Systemsmentioning

confidence: 99%

Nanoparticle-based bioactive agent release systems for bone and cartilage tissue engineering

Monteiro

Martins

Reis

et al. 2015

Regenerative Therapy

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a b s t r a c tThe inability to deliver bioactive agents locally in a transient but sustained manner is one of the challenges on the development of bio-functionalized scaffolds for tissue engineering (TE) and regenerative medicine. The mode of release is especially relevant when the bioactive agent is a growth factor (GF), because the dose and the spatiotemporal release of such agents at the site of injury are crucial to achieve a successful outcome. Strategies that combine scaffolds and drug delivery systems have the potential to provide more effective tissue regeneration relative to current therapies. Nanoparticles (NPs) can protect the bioactive agents, control its profile, decrease the occurrence and severity of side effects and deliver the bioactive agent to the target cells maximizing its effect. Scaffolds containing NPs loaded with bioactive agents can be used for their local delivery, enabling site-specific pharmacological effects such as the induction of cell proliferation and differentiation, and, consequently, neo-tissue formation. This review aims to describe the concept of combining NPs with scaffolds, and the current efforts aiming to develop highly multi-functional bioactive agent release systems, with the emphasis on their application in TE of connective tissues.

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Section: Nanoparticles As Bioactive Agents Release Systemsmentioning

confidence: 99%

Nanoparticle-based bioactive agent release systems for bone and cartilage tissue engineering

Monteiro

Martins

Reis

et al. 2015

Regenerative Therapy

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“…Second, liposomes are easily modifiable to accommodate various properties/function (Levchenko et al, 2012;Slingerland et al, 2012). For example, antibodies and polyethylene glycols can be added to improve their target specificity as well as reduced immunogenicity (Garnier et al, 2012;Wolff et al, 2010), and lipid composition has also been varied for improved solubility of specific drugs (Slingerland et al, 2012). Third, liposomes can be easily adsorbed by tissues, as evidenced by topical liposomes commonly used by the cosmetic industry (Betz et al, 2005;Posner, 2002) as well as for topical nystatin formulations (Torchilin, 2005).…”

Section: Liposomal Drug Delivery Systemmentioning

confidence: 99%

“…With the second, it is possible to produce stable modifiable liposomes smaller than 100 nm, which is small enough to cross the blood-brain barrier. With the third challenge, liposomes which directly release drugs at the target site via nanovalves and those which undergo receptormediated fusion to the target cells are currently under development (Garnier et al, 2012;Nakayama et al, 2015).…”

Section: Delivery Strategies For Liposomal Drug Delivery Systemsmentioning

confidence: 99%

“…1.4C) (Basile et al, 2012;Garnier et al, 2012;Lammers et al, 2012;Sawant & Torchilin, 2012). The specificity of these affinity tags can range from fairly low (e.g.…”

Section: Active Targetingmentioning

confidence: 99%

“…Smaller liposomes are generally favoured for drug delivery because they tend to be more permeable to physiological barriers such as blood vessels (Garnier et al, 2012). There are conflicting hypotheses, both based on molecular dynamics studies, on the influence of global curvature in small liposomes on MscL function (Bavi, Cox, et al, 2016;Meyer et al, 2006), making an experimental confirmation of whether MscL is to be engineered for gating threshold (Iscla et al, 2013;Nakayama et al, 2015).…”

Section: ) Despite Pc Not Being a Native Component Of E Coli's Imentioning

confidence: 99%

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Biophysical and Structural Studies of Escherichia coli Mechanosensitive Channel of Large Conductance in Lipid Bilayers

Chi¹

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A major challenge of drug development is maximising specificity and efficacy at the lowest possible dose to minimise toxic side effects (Basile et al., 2012). Not only are the pharmaceutical windows small for both drug candidates and approved drugs alike, but they can also vary between individuals, making a dose level safe for one individual potentially harmful for another. One strategy for overcoming this problem is to develop new drug delivery methods where the drug is preferentially concentrated at the site of disease (Basile et al., 2012). In this respect, liposomal drug delivery systems have been used with success in topical applications in skin cancer treatment, and there is significant research interest in engineering similar systems for intravenous administration (Al-Jamal & Kostarelos, 2011;Fan & Zhang, 2013). Incorporating nanovalves into liposomes with controllable gating properties would further enhance the usefulness of liposomal drug delivery systems, providing a method to further regulate the release of liposome-encapsulated drugs from liposomes at the target site (Martinac et al., 2014).The mechanosensitive channel of large conductance (MscL) has been identified as a major candidate for the development of a protein-based nanovalve (Martinac et al., 2014). More generally, MscL is a prototype for the class of ion channels primarily gated by membrane tension, which includes medically significant proteins such as Piezo channels and TRP-type sodium channels (Martinac, 2011). As a well-expressing protein from Escherichia coli, MscL has been extensively studied both structurally and biophysically (Martinac, 2011). However, the channel gating mechanism of MscL, and by extension of mechanosensitive channels in general, remains poorly understood at the molecular level.This thesis aims to investigate the relationship between E. coli MscL and phospholipids both in the context of its structure and its behaviour in a lipid bilayer environment. While much has been studied on the channel gating properties of MscL in various phospholipid environments (Anishkin et al., 2005;Iscla et al., 2004;Iscla et al., 2011;Powl et al., 2008b;Tsai et al., 2005;Yoshimura et al., 2004), there remains a limited understanding of the behaviour and distribution of MscL in the bilayer. These are not only important from academic perspective as well as in the context of nanovalve development, but also for example, to identify factors which may limit the functional studies on MscL. More specifically, this thesis has focused on the identification of phospholipids closely associating with MscL, the distribution of MscL in phospholipid bilayers, and the incorporation of MscL into liposomes with heterogeneous phospholipids.The first research chapter (Chapter 2) outlines the optimisation of MscL expression and purification system for biophysical and structural studies. The original MscL construct had problems of ii heterogeneous expression and being not well-suited to reliable quantification by routine methods.New constructs were suc...

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Functionalized liposomes: a nanovesicular system

Misra

Pathak

2022

Systems of Nanovesicular Drug Delivery

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Development of a Platform of Antibody-Presenting Liposomes

Cited by 5 publications

References 31 publications

Nanoparticle-based bioactive agent release systems for bone and cartilage tissue engineering

Nanoparticle-based bioactive agent release systems for bone and cartilage tissue engineering

Biophysical and Structural Studies of Escherichia coli Mechanosensitive Channel of Large Conductance in Lipid Bilayers

Functionalized liposomes: a nanovesicular system

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