BONCAT-based Profiling of Nascent Small and Alternative Open Reading Frame-encoded Proteins

被引:3
作者
Cao, Xiongwen [1 ,2 ]
Chen, Yanran [1 ,2 ]
Khitun, Alexandra [1 ,2 ]
Slavoff, Sarah A. [2 ,3 ]
机构
[1] Yale Univ, Dept Chem, New Haven, CT 06520 USA
[2] Yale Univ, Inst Biomol Design & Discovery, West Haven, CT 06516 USA
[3] Yale Univ, Dept Mol Biophys & Biochem, New Haven, CT 06520 USA
来源
BIO-PROTOCOL | 2023年 / 13卷 / 01期
关键词
Small open reading frame (smORF); Microprotein; Alternative protein (alt-protein); Micropeptide; Chemoproteomics; Proteomics; Protein translation; Unnatural amino acid;
D O I
10.21769/BioProtoc.4585
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
RIBO-seq and proteogenomics have revealed that mammalian genomes harbor thousands of unannotated small and alternative open reading frames (smORFs, <100 amino acids, and alt-ORFs, >100 amino acids, respectively). Several dozen mammalian smORF-encoded proteins (SEPs) and alt-ORF-encoded proteins (alt-proteins) have been shown to play important biological roles, while the overwhelming majority of smORFs and alt-ORFs remain uncharacterized, particularly at the molecular level. Functional proteomics has the potential to reveal key properties of unannotated SEPs and alt-proteins in high throughput, and an approach to identify SEPs and alt-proteins undergoing regulated synthesis should be of broad utility. Here, we introduce a chemoproteomic pipeline based on bio-orthogonal non-canonical amino acid tagging (BONCAT) (Dieterich et al., 2006) to profile nascent SEPs and alt-proteins in human cells. This approach is able to identify cellular stress-induced and cell-cycle regulated SEPs and alt-proteins in cells.
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页数:11
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