AI Article Synopsis

  • Mitochondrial ribosome (mitoribosome) biogenesis primarily occurs near mitochondrial DNA, involving RNA granules enriched with RNA metabolism and assembly factors.
  • Research identified GTPBP10, a small GTPase, as crucial for mitochondrial ribosome assembly; its absence in a genetically modified cell line resulted in significantly reduced mitoribosome levels and halted mitochondrial protein synthesis.
  • GTPBP10 interacts with specific rRNA components, is involved in the maturation of ribosomal subunits, and plays a key role in ensuring proper assembly and quality control during the mitoribosome formation process.

Article Abstract

Most steps on the biogenesis of the mitochondrial ribosome (mitoribosome) occur near the mitochondrial DNA nucleoid, in RNA granules, which contain dedicated RNA metabolism and mitoribosome assembly factors. Here, analysis of the RNA granule proteome identified the presence of a set of small GTPases that belong to conserved families of ribosome assembly factors. We show that GTPBP10, a member of the conserved Obg family of P-loop small G proteins, is a mitochondrial protein and have used gene-editing technologies to create a HEK293T cell line KO for GTPBP10. The absence of GTPBP10 leads to attenuated mtLSU and mtSSU levels and the virtual absence of the 55S monosome, which entirely prevents mitochondrial protein synthesis. We show that a fraction of GTPBP10 cosediments with the large mitoribosome subunit and the monosome. GTPBP10 physically interacts with the 16S rRNA, but not with the 12S rRNA, and crosslinks with several mtLSU proteins. Additionally, GTPBP10 is indirectly required for efficient processing of the 12S-16S rRNA precursor transcript, which could explain the mtSSU accumulation defect. We propose that GTPBP10 primarily ensures proper mtLSU maturation and ultimately serves to coordinate mtSSU and mtLSU accumulation then providing a quality control check-point function during mtLSU assembly that minimizes premature subunit joining.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6265488PMC
http://dx.doi.org/10.1093/nar/gky938DOI Listing

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