Delivery, Effect on Cell Viability, and Plasticity of Modified Aptamer Constructs

Gissberg, Olof; Zaghloul, Eman M.; Lundin, Karin E.; Nguyen, Chi-Hung; Landras-Guetta, Corinne; Wengel, Jesper; Zain, Rula; Smith, C. I. Edvard

doi:10.1089/nat.2015.0592

Cited by 8 publications

(3 citation statements)

References 287 publications

(303 reference statements)

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“…Further, NCL-blocked cells displayed much lower ROS production after treatment with TMPyP DNM Apt-gc34@SPION NPs with respect to blocked cells. Results of MTT assay demonstrated that cell viability was highly reduced in NCL-non-blocked cells indicating that AS1411 structure plays an important role for the cellular internalization of the designed drug delivery system resulting in a higher cell inhibition 82,121 . A significant reduction in cell growth under the visible light was observed and was due to the synergistic effect of DNM and TMPyP.…”

Section: Other Types Of As1411 Aptamer-conjugated Npsmentioning

confidence: 99%

Cell surface nucleolin as active bait for nanomedicine in cancer therapy: a promising option

Ferrara¹,

Belbekhouche²,

Habert³

et al. 2021

Nanotechnology

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HAL is a multi-disciplinary open access archive for the deposit and dissemination of scientific research documents, whether they are published or not. The documents may come from teaching and research institutions in France or abroad, or from public or private research centers. L'archive ouverte pluridisciplinaire HAL, est destinée au dépôt et à la diffusion de documents scientifiques de niveau recherche, publiés ou non, émanant des établissements d'enseignement et de recherche français ou étrangers, des laboratoires publics ou privés.

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Section: Other Types Of As1411 Aptamer-conjugated Npsmentioning

confidence: 99%

Cell surface nucleolin as active bait for nanomedicine in cancer therapy: a promising option

Ferrara¹,

Belbekhouche²,

Habert³

et al. 2021

Nanotechnology

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“…Its internalization efficiency highly depends on the chemistry of the oligonucleotides. LNA substitutions were investigated with this GQ [ 165 ]. The formation of a GQ from a G-rich 25-mer section of the vascular endothelial growth factor aptamer was highly facilitated by LNA modifications.…”

Section: Stabilization or Destabilization Of A Gq By The Same Syntmentioning

confidence: 99%

In What Ways Do Synthetic Nucleotides and Natural Base Lesions Alter the Structural Stability of G-Quadruplex Nucleic Acids?

Sági¹

2017

Journal of Nucleic Acids

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Synthetic analogs of natural nucleotides have long been utilized for structural studies of canonical and noncanonical nucleic acids, including the extensively investigated polymorphic G-quadruplexes (GQs). Dependence on the sequence and nucleotide modifications of the folding landscape of GQs has been reviewed by several recent studies. Here, an overview is compiled on the thermodynamic stability of the modified GQ folds and on how the stereochemical preferences of more than 70 synthetic and natural derivatives of nucleotides substituting for natural ones determine the stability as well as the conformation. Groups of nucleotide analogs only stabilize or only destabilize the GQ, while the majority of analogs alter the GQ stability in both ways. This depends on the preferred syn or anti N-glycosidic linkage of the modified building blocks, the position of substitution, and the folding architecture of the native GQ. Natural base lesions and epigenetic modifications of GQs explored so far also stabilize or destabilize the GQ assemblies. Learning the effect of synthetic nucleotide analogs on the stability of GQs can assist in engineering a required stable GQ topology, and exploring the in vitro action of the single and clustered natural base damage on GQ architectures may provide indications for the cellular events.

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“…Conventional optimization methods include the following: (1) Substituting a natural nucleotide for a nucleotide modified with a group to avoid degradation of the nucleic acid[44]; (2) Chemically synthesizing a mirror image sequence of the selected aptamers with high plasma and serum stability to enhance the stability of aptamers to make them have significant therapeutic potential[45]; (3) Modifying aptamers with locked nucleic acids to enhance their ribozyme resistance. Methylene-linked 2'-oxygen and 4'-carbon in carbohydrate residues have strong ability to hybridize with nucleic acid molecules and are not easily degraded by enzymes[46]; and (4) Covalently attaching PEG or cholesterol to aptamers, prolonging their residence time in the human body and reducing renal filtration rate[47,48]. The half-life of survival of aptamers in human physiological environment can be extended from a few minutes to several hours by one or more of the above methods, and aptamers with modifiable properties are superior to antibodies or polypeptides in the diagnosis and treatment of tumor diseases.…”

Section: Selex Methods For Screening Aptamersmentioning

confidence: 99%

Screening of aptamers and their potential application in targeted diagnosis and therapy of liver cancer

Zhang¹,

Zhong²,

Yang³

et al. 2019

WJG

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Aptamers are a class of single oligonucleotide molecules (DNA or RNA) that are screened from random DNA or RNA oligonucleotide chain libraries by the systemic evolution of ligands by exponential enrichment technology. The selected aptamers are capable of specifically binding to different targeting molecules, which is achieved by the three-dimensional structure of aptamers. Aptamers are similar in function to monoclonal antibodies, and therefore, they are also referred to as "chemical antibodies". Due to their high affinity and specificity and low immunogenicity, aptamers are topics of intense interest in today's biological targeting research especially in tumor research. They not only have high potential for clinical advances in tumor targeting detection but also are highly promising as targeted tumor drug carriers for use in tumor therapy. Various experimental studies have shown that aptamer-based diagnostic and therapeutic methods for liver cancer have great potential for application. This paper summarizes the structure, characteristics, and screening methods of aptamers and reviews the recent research progress on nucleic acid aptamers in the targeted diagnosis and treatment of liver cancer.

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Delivery, Effect on Cell Viability, and Plasticity of Modified Aptamer Constructs

Cited by 8 publications

References 287 publications

Cell surface nucleolin as active bait for nanomedicine in cancer therapy: a promising option

Cell surface nucleolin as active bait for nanomedicine in cancer therapy: a promising option

In What Ways Do Synthetic Nucleotides and Natural Base Lesions Alter the Structural Stability of G-Quadruplex Nucleic Acids?

Screening of aptamers and their potential application in targeted diagnosis and therapy of liver cancer

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