4.4 Article

Structural Roles of Noncoding RNAs in the Heart of Enzymatic Complexes

Journal

BIOCHEMISTRY
Volume 56, Issue 1, Pages 3-13

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.biochem.6b01106

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Funding

  1. Vanderbilt University
  2. American Heart Association [GRNT20380334]
  3. [T32-GM008320]

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Over billions of years of evolution, nature has embraced proteins as the major workhorse molecules of the cell. However, nearly every aspect of metabolism is dependent upon how structured RNAs interact with proteins, ligands, and other nucleic acids. Key processes, including telomere maintenance, RNA processing, and protein synthesis, require large RNAs that assemble into elaborate three-dimensional shapes. These RNAs can (i) act as flexible scaffolds for protein subunits, (ii) participate directly in substrate recognition, and (iii) serve as catalytic components. Here, we juxtapose the near atomic level interactions of three ribonucleoprotein complexes: ribonuclease P (involved in 5' pre-tRNA processing), the spliceosome (responsible for pre-mRNA splicing), and telomerase (an RNA-directed DNA polymerase that extends the ends of chromosomes). The focus of this perspective is profiling the structural and dynamic roles of RNAs at the core of these enzymes, highlighting how large RNAs contribute to molecular recognition and catalysis.

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