Structural modeling of protein-RNA complexes using crosslinking of segmentally isotope-labeled RNA and MS/MS

利用分段同位素标记 RNA 交联和 MS/MS 对蛋白质-RNA 复合物进行结构建模

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作者:G Dorn #, A Leitner #, J Boudet, S Campagne, C von Schroetter, A Moursy, R Aebersold, F H-T Allain

Abstract

Ribonucleoproteins (RNPs) are key regulators of cellular function. We established an efficient approach, crosslinking of segmentally isotope-labeled RNA and tandem mass spectrometry (CLIR-MS/MS), to localize protein-RNA interactions simultaneously at amino acid and nucleotide resolution. The approach was tested on polypyrimidine tract binding protein 1 and U1 small nuclear RNP. Our method provides distance restraints to support integrative atomic-scale structural modeling and to gain mechanistic insights into RNP-regulated processes.

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