AI Article Synopsis
- Small proteins that are less than 51 amino acids long are found everywhere in life, but scientists often miss them because they are tricky to study due to their small size.
- Researchers used a method called ribosome profiling, which helps find these tiny proteins by looking at where ribosomes are working on RNA, especially when drugs are used to stop the ribosomes at key points.
- By using this method, scientists discovered around 400 new tiny proteins, with 365 of them being less than 51 amino acids, and they found that many of these proteins may not be very important for how well cells work.
Article Abstract
Small proteins of <51 amino acids are abundant across all domains of life but are often overlooked because their small size makes them difficult to predict computationally, and they are refractory to standard proteomic approaches. Ribosome profiling has been used to infer the existence of small proteins by detecting the translation of the corresponding open reading frames (ORFs). Detection of translated short ORFs by ribosome profiling can be improved by treating cells with drugs that stall ribosomes at specific codons. Here, we combine the analysis of ribosome profiling data for cells treated with antibiotics that stall ribosomes at either start or stop codons. Thus, we identify ribosome-occupied start and stop codons with high sensitivity for ∼400 novel putative ORFs. The newly discovered ORFs are mostly short, with 365 encoding proteins of <51 amino acids. We validate translation of several selected short ORFs, and show that many likely encode unstable proteins. Moreover, we present evidence that most of the newly identified short ORFs are not under purifying selection, suggesting they do not impact cell fitness, although a small subset have the hallmarks of functional ORFs. Small proteins of <51 amino acids are abundant across all domains of life but are often overlooked because their small size makes them difficult to predict computationally, and they are refractory to standard proteomic approaches. Recent studies have discovered small proteins by mapping the location of translating ribosomes on RNA using a technique known as ribosome profiling. Discovery of translated sORFs using ribosome profiling can be improved by treating cells with drugs that trap initiating ribosomes. Here, we show that combining these data with equivalent data for cells treated with a drug that stalls terminating ribosomes facilitates the discovery of small proteins. We use this approach to discover 365 putative genes that encode small proteins in .
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8765432 | PMC |
| http://dx.doi.org/10.1128/JB.00352-21 | DOI Listing |
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