AI Article Synopsis

  • - Ribosome biogenesis is a complex, energy-requiring process where GTPases play a crucial role, especially in the maturation of bacterial, cytosolic, and mitochondrial ribosomes.
  • - The study focuses on Mtg3, a GTPase involved in mitochondrial ribosome small subunit development, exploring its necessary interactions and the importance of its C-terminal domain for binding.
  • - Findings indicate that while some mutations affect GTP binding and activity, they do not hinder Mtg3's association with mitoribosomes, suggesting a model where Mtg3 facilitates ribosome maturation without needing to hydrolyze nucleotides actively.

Article Abstract

Ribosome biogenesis is a highly regulated multistep process aided by energy-consuming auxiliary factors. GTPases form the largest class of auxiliary factors used by bacterial, cytosolic, and mitochondrial ribosomes for their maturation. Mtg3, a circularly permuted YqeH family of GTPase, is implicated in the mitoribosome small subunit biogenesis. However, its precise mechanistic role has yet to be characterized. Mtg3 is likely to bind precursor mitoribosome molecules during subunit maturation in vivo. However, this interaction has yet to be observed with mitoribosomes biochemically. In this study, we delineate the specific conditions necessary for preserving the association of Mtg3 with mitoribosomes on a sucrose density gradient. We show that the C-terminal domain of Mtg3 is required for robust binding to the mitoribosome. Furthermore, point mutants likely to abrogate GTP/GDP binding and GTPase activity compromise protein function in vivo. Surprisingly, the association with the mitoribosome was not compromised in mutants likely to be deficient for nucleotide binding/hydrolysis. Thus, our finding supports a model wherein Mtg3 binds to a precursor mitoribosome through its C-terminus to facilitate a conformational change or validate a folding intermediate driven by the GTP/GDP binding and hydrolysis cycle.

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Source
http://dx.doi.org/10.1016/j.bbrc.2024.150502DOI Listing

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