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An RNA alternative to human transferrin: a new tool for targeting human cells. | LitMetric

AI Article Synopsis

  • The transferrin receptor, CD71, is a promising target for drug development due to its high expression in various cancer cells and the blood-brain barrier.
  • Researchers modified the aptamer selection process to create RNA molecules that specifically bind to and are internalized by the human transferrin receptor, resulting in a minimized variant that outcompetes natural transferrin for binding.
  • Using this optimized aptamer, scientists created targeted liposomes carrying siRNA, which significantly enhanced cellular uptake and gene knockdown compared to standard liposomes, suggesting its potential for applications like cell imaging and targeted drug delivery.

Article Abstract

The transferrin receptor, CD71, is an attractive target for drug development because of its high expression on a number of cancer cell lines and the blood brain barrier. To generate serum-stabilized aptamers that recognize the human transferrin receptor, we have modified the traditional aptamer selection protocol by employing a functional selection step that enriches for RNA molecules which bind the target receptor and are internalized by cells. Selected aptamers were specific for the human receptor, rapidly endocytosed by cells and shared a common core structure. A minimized variant was found to compete with the natural ligand, transferrin, for receptor binding and cell uptake, but performed ~twofold better than it in competition experiments. Using this molecule, we generated aptamer-targeted siRNA-laden liposomes. Aptamer targeting enhanced both uptake and target gene knockdown in cells grown in culture when compared to nonmodified or nontargeted liposomes. The aptamer should prove useful as a surrogate for transferrin in many applications including cell imaging and targeted drug delivery.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3390244PMC
http://dx.doi.org/10.1038/mtna.2012.14DOI Listing

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