AI Article Synopsis
- Super-resolution microscopy (SRM) works better when tiny, bright labels are added to proteins, but some challenges exist with using these labels.
- A new technology called genetic code expansion (GCE) helps add special amino acids to proteins, making it easier to label them.
- A new approach combines GCE with DNA-PAINT microscopy to see even tiny amounts of proteins in cells more clearly and reduces problems with unwanted background brightness.
Article Abstract
Super-resolution microscopy (SRM) greatly benefits from the ability to install small photostable fluorescent labels into proteins. Genetic code expansion (GCE) technology addresses this demand, allowing the introduction of small labeling sites, in the form of uniquely reactive noncanonical amino acids (ncAAs), at any residue in a target protein. However, low incorporation efficiency of ncAAs and high background fluorescence limit its current SRM applications. Redirecting the subcellular localization of the pyrrolysine-based GCE system for click chemistry, combined with DNA-PAINT microscopy, enables the visualization of even low-abundance proteins inside mammalian cells. This approach links a versatile, biocompatible, and potentially unbleachable labeling method with residue-specific precision. Moreover, our reengineered GCE system eliminates untargeted background fluorescence and substantially boosts the expression yield, which is of general interest for enhanced protein engineering in eukaryotes using GCE.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5215487 | PMC |
| http://dx.doi.org/10.1002/anie.201608284 | DOI Listing |
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