Literature DB >> 22353142

The chemistry and biology of oligonucleotide conjugates.

R L Juliano1, Xin Ming, Osamu Nakagawa.   

Abstract

Short DNA or RNA oligonucleotides have tremendous potential as therapeutic agents. Because of their ability to engage in Watson-Crick base pairing, they can interact with mRNA or pre-mRNA targets with high selectivity. As a result, they could precisely manipulate gene expression. This possibility has engendered extensive efforts to develop oligonucleotides as drugs, and many candidates are already in clinical trials. However, a major impediment to the maturation of this field of oligonucleotide-based therapeutics remains: these relatively large and often highly charged molecules don't easily cross cellular membranes, making it difficult for them to reach their sites of action in the cytosol or nucleus. In this Account, we summarize some basic features of the biology of antisense and siRNA oligonucleotides. We then discuss chemical conjugation as an approach to improving the intracellular delivery and therapeutic potential of these agents. Instead of focusing on the details of conjugation chemistry, we emphasize the pharmacological ramifications of oligonucleotide conjugates. In one important approach to improving delivery and efficacy, researchers have conjugated oligonucleotides with ligands designed to bind to particular receptors and thus provide specific interactions with cells. In another strategy, researchers have coupled antisense or siRNA with agents such as cell penetrating peptides that are designed to provoke escape of the conjugate from intracellular vesicular compartments. Although both of these strategies have had some success, further research is needed before oligonucleotide conjugates can find an important place in human therapeutics.

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Year:  2012        PMID: 22353142      PMCID: PMC3374910          DOI: 10.1021/ar2002123

Source DB:  PubMed          Journal:  Acc Chem Res        ISSN: 0001-4842            Impact factor:   22.384


  66 in total

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6.  Efficient in vivo delivery of siRNA to the liver by conjugation of alpha-tocopherol.

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  23 in total

Review 1.  Receptors, endocytosis, and trafficking: the biological basis of targeted delivery of antisense and siRNA oligonucleotides.

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2.  A Novel Family of Small Molecules that Enhance the Intracellular Delivery and Pharmacological Effectiveness of Antisense and Splice Switching Oligonucleotides.

Authors:  Ling Wang; Yamuna Ariyarathna; Xin Ming; Bing Yang; Lindsey I James; Silvia M Kreda; Melissa Porter; William Janzen; Rudolph L Juliano
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Review 3.  The delivery of therapeutic oligonucleotides.

Authors:  Rudolph L Juliano
Journal:  Nucleic Acids Res       Date:  2016-04-15       Impact factor: 16.971

Review 4.  Cellular uptake and intracellular trafficking of oligonucleotides: implications for oligonucleotide pharmacology.

Authors:  R L Juliano; Xin Ming; Kyle Carver; Brian Laing
Journal:  Nucleic Acid Ther       Date:  2014-01-02       Impact factor: 5.486

5.  miRNA inhibition by proximity-enabled Dicer inactivation.

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6.  CpG-PEG Conjugates and their Immune Modulating Effects after Systemic Administration.

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7.  Assessing histidine tags for recruiting deoxyribozymes to catalyze peptide and protein modification reactions.

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8.  Covalent conjugation of oligonucleotides with cell-targeting ligands.

Authors:  Md Rowshon Alam; Xin Ming; Osamu Nakagawa; Jian Jin; R L Juliano
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9.  Regulating miRNA-21 Biogenesis By Bifunctional Small Molecules.

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10.  A generalizable DNA-catalyzed approach to peptide-nucleic acid conjugation.

Authors:  Chih-Chi Chu; On Yi Wong; Scott K Silverman
Journal:  Chembiochem       Date:  2014-07-23       Impact factor: 3.164

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