Aptamer-based liposomes improve specific drug loading and release

Plourde, Kevin; Derbali, Rabeb Mouna; Desrosiers, Arnaud; Dubath, Céline; Vallée‐Bélisle, Alexis; Leblond, Jeanne

doi:10.1016/j.jconrel.2017.02.026

Cited by 51 publications

(37 citation statements)

References 52 publications

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“…However, its potential to improve drug loading and release from nano carriers has not been thoroughly analyzed. Recently Lee JB et al have proposed a general approach for loading a large amount of thrombin proteins using DNA aptamer particles [52]; other authors, have developed a new strategy of drug-loading by designing drug specific aptamers to drive drugs into liposomes [53]. Of note, Dam et al [54] showed thatloading of G-quadruplex DNA aptamer AS1411 onto AuNPs could be tuned by manipulating the charge of the ligands and the particle surface by pH.…”

Section: Aptamer Loading and Release Of Apt Onpeg-aunps And Apt In Pementioning

confidence: 99%

Aptamer Grafting onto (on) and into (in) Pegylated Gold Nanoparticles: Physicochemical Characterization and In vitro Cytotoxicity Investigation in Renal Cells

Arib¹,

Milano²,

Gerbino³

et al. 2018

J Nanomed Nanotechnol

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Gold Nanoparticles (AuNPs) have already a remarkable interest as viable biomedical materials. Additionally, the strategy of using biomolecules to modify their surface properties is a very attractive as it leads to the generation of new nanometric hybrid materials. In this respect, aptamers, functional small single-strand oligonucleotides (DNA or RNA), are ideal candidates for molecular targeting applications since the high affinity to their target molecules. Thus, the urge of new and effective methodologies to graft aptamers on AuNPs is rapidly increasing especially for applications in bioanalysis and biomedicine, including early diagnosis and drug delivery. Here we used two chemical methodologies to conjugate the aptamer (APT) onto pegylated gold nanoparticles (PEG-AuNPs): the carbodiimide chemistry (EDC/NHS) (methodology ON) and the chelation-bond (R-Au bond) (methodology IN). The aptamer's conjugations with the PEG-AuNPs were characterized by UV-Vis absorption, Raman Spectroscopy and transmission electron microscopy (TEM). In addition, the potential nanotoxicity of the two aptamer-conjugated AuNPs was evaluated on two different renal cell lines, being the kidneys one of the most important site of bioaccumulation upon systemic circulation. Interestingly, the two aptamer-conjugated AuNPs showed different cytotoxicity when exposed to human embryonic kidney (HEK293) and mouse collecting duct cells (M-1), indicating that cell viability has to be taken into account when choosing the proper strategy for NPs production. In conclusion this study provides two effective methods to graft aptamers on NPs and important insights regarding NPs conformation and the relative cell viability.The first grafting strategy consists of the conjugation of the AQP2 aptamer (APT) or on the PEG-AuNPs surface by carbodiimide Scheme 1: Schematic representation of the synthesis of a)APT ON PEG-AuNPs and b) APT IN PEG-AuNPs via carbodiimide chemistry (a) and chelation reaction (b) (Please note that drawings are not in scale and are not intended to be representative of the full samples composition).

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Section: Aptamer Loading and Release Of Apt Onpeg-aunps And Apt In Pementioning

confidence: 99%

Aptamer Grafting onto (on) and into (in) Pegylated Gold Nanoparticles: Physicochemical Characterization and In vitro Cytotoxicity Investigation in Renal Cells

Arib¹,

Milano²,

Gerbino³

et al. 2018

J Nanomed Nanotechnol

View full text Add to dashboard Cite

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“…Aptamers' targeting abilities have been widely exploited, but its potential to improve drug loading and release from nanocarriers was thoroughly unexplored. Plourde et al hence utilized drug‐binding aptamers to load DOX into cationic liposomes and optimization of the charge and drug/aptamer ratios resulted in ≥80% encapsulation efficiency, tenfold improvement than classical passively encapsulating liposomal formulations …”

Section: Biomedical Applicationsmentioning

confidence: 99%

Programmable and Multifunctional DNA‐Based Materials for Biomedical Applications

et al. 2018

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DNA encodes the genetic information; recently, it has also become a key player in material science. Given the specific Watson-Crick base-pairing interactions between only four types of nucleotides, well-designed DNA self-assembly can be programmable and predictable. Stem-loops, sticky ends, Holliday junctions, DNA tiles, and lattices are typical motifs for forming DNA-based structures. The oligonucleotides experience thermal annealing in a near-neutral buffer containing a divalent cation (usually Mg ) to produce a variety of DNA nanostructures. These structures not only show beautiful landscape, but can also be endowed with multifaceted functionalities. This Review begins with the fundamental characterization and evolutionary trajectory of DNA-based artificial structures, but concentrates on their biomedical applications. The coverage spans from controlled drug delivery to high therapeutic profile and accurate diagnosis. A variety of DNA-based materials, including aptamers, hydrogels, origamis, and tetrahedrons, are widely utilized in different biomedical fields. In addition, to achieve better performance and functionality, material hybridization is widely witnessed, and DNA nanostructure modification is also discussed. Although there are impressive advances and high expectations, the development of DNA-based structures/technologies is still hindered by several commonly recognized challenges, such as nuclease instability, lack of pharmacokinetics data, and relatively high synthesis cost.

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“…The past few years has witnessed the great advances in the synthesis and characterization of various nanomaterials, such as dots, [17,18] gold nanomaterials, [19] hydrogel [20] carbon nanotubes [21] liposome [22] and so on. The combination of aptamers with novel nanomaterials has led to a wide applications.…”

Section: Aptamer-nanoparticles Systemsmentioning

confidence: 99%

Applications of Aptamers in Drug Delivery System

Wu¹

2017

WJPR

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Aptamers, a kind of short single-stranded oligonucleic acids (DNA or RNA) or peptide molecules that can fold into secondary or tertiary structures, are well recognized as a potential tool for binding target molecules due to its high specificity and affinity. As tumor targeted ligands, aptamers have certain superiorities compared with antibodies, such as low immunogenicity, high binding specificity and so on. By the means of systematic evolution of ligands with exponential enrichment (SELEX) approach, selected aptamers showed high affinity to specific targets like proteins, peptides, and even the entire cells. In this review, we will give a brief overview of recent relevant research in the field of aptamers and their applications in cancer diagnostics and in drug delivery system.

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Aptamer-based liposomes improve specific drug loading and release

Cited by 51 publications

References 52 publications

Aptamer Grafting onto (on) and into (in) Pegylated Gold Nanoparticles: Physicochemical Characterization and In vitro Cytotoxicity Investigation in Renal Cells

Aptamer Grafting onto (on) and into (in) Pegylated Gold Nanoparticles: Physicochemical Characterization and In vitro Cytotoxicity Investigation in Renal Cells

Programmable and Multifunctional DNA‐Based Materials for Biomedical Applications

Applications of Aptamers in Drug Delivery System

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