Affiliation:
1. Department of Chemistry and Pharmaceutical Sciences VU University Amsterdam De Boelelaan 1108 1081 HZ Amsterdam The Netherlands
2. Amsterdam Institute of Molecular and Life Sciences VU University Amsterdam De Boelelaan 1108 1081 HZ Amsterdam The Netherlands
3. Department of Medical BioSciences Radboud University Nijmegen Medical Center 6525 GA Nijmegen The Netherlands
4. Incircular B.V. De Boelelaan 1108 1081 HZ Amsterdam The Netherlands
5. Department of Medical Biochemistry College of Medicine and Medical Sciences Arabian Gulf University Manama 293 Bahrain
Abstract
AbstractDouble‐stranded RNAs (dsRNA) possess immense potential for biomedical applications. However, their therapeutic utility is limited by low stability and poor cellular uptake. Different strategies have been explored to enhance the stability of dsRNA, including the incorporation of modified nucleotides, and the use of diverse carrier systems. Nevertheless, these have not resulted in a broadly applicable approach thereby preventing the wide‐spread application of dsRNA for therapeutic purposes. Herein, we report the design of dimeric stapled peptides based on the RNA‐binding protein TAV2b. These dimers are obtained via disulfide formation and mimic the natural TAV2b assembly. They bind and stabilize dsRNA in the presence of serum, protecting it from degradation. In addition, peptide binding also promotes cellular uptake of dsRNA. Importantly, peptide dimers monomerize under reducing conditions which results in a loss of RNA binding. These findings highlight the potential of peptide‐based RNA binders for the stabilization and protection of dsRNA, representing an appealing strategy towards the environment‐triggered release of RNA. This can broaden the applicability of dsRNA, such as short interfering RNAs (siRNA), for therapeutic applications.
Funder
H2020 European Research Council
Subject
General Chemistry,Catalysis
Cited by
3 articles.
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