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“Ping-Pong” Interactions between Mitochondrial tRNA Import Receptors within a Multiprotein Complex

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TLDR
By a combination of antibody inhibition, photochemical cross-linking, and immunoprecipitation, it was shown that binding of tRNAIle to a 21-kDa component of the complex is dependent upon tRNATyr, whilebinding of tR NATyr to a 45-KDa component is inhibited by t RNAIle, suggesting this “ping-pong” mechanism may be an effective means to maintain a balanced tRNA pool for mitochondrial translation.
Abstract
The mitochondrial genomes of a wide variety of species contain an insufficient number of functional tRNA genes, and translation of mitochondrial mRNAs is sustained by import of nucleus-encoded tRNAs. In Leishmania, transfer of tRNAs across the inner membrane can be regulated by positive and negative interactions between them. To define the factors involved in such interactions, a large multisubunit complex (molecular mass, approximately 640 kDa) from the inner mitochondrial membrane of the kinetoplastid protozoon Leishmania, consisting of approximately 130-A particles, was isolated. The complex, when incorporated into phospholipid vesicles, induced specific, ATP- and proton motive force-dependent transfer of Leishmania tRNA(Tyr) as well as of oligoribonucleotides containing the import signal YGGYAGAGC. Moreover, allosteric interactions between tRNA(Tyr) and tRNA(Ile) were observed in the RNA import complex-reconstituted system, indicating the presence of primary and secondary tRNA binding sites within the complex. By a combination of antibody inhibition, photochemical cross-linking, and immunoprecipitation, it was shown that binding of tRNA(Ile) to a 21-kDa component of the complex is dependent upon tRNA(Tyr), while binding of tRNA(Tyr) to a 45-kDa component is inhibited by tRNA(Ile). This "ping-pong" mechanism may be an effective means to maintain a balanced tRNA pool for mitochondrial translation.

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Journal ArticleDOI

tRNA-triggered ATP Hydrolysis and Generation of Membrane Potential by the Leishmania Mitochondrial tRNA Import Complex*

TL;DR: Observations imply a gating mechanism in which tRNA, on binding to its receptor, triggers the energetic activation of the complex, leading to the opening of import channels, implying an ATP requirement within the vesicles.
Journal ArticleDOI

The ins and outs of tRNA transport

TL;DR: It is now well established that a variable number of tRNA species present in the mitochondria are indeed nucleus‐encoded, and the roles of some of these transport systems have yet to be defined.
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Keep the fire burning: Current avenues in the quest of treating mitochondrial disorders.

TL;DR: An update on current developments towards treatment as well as the potential and status of transition into therapeutic use of OXPHOS disorders is provided.
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Mitochondrial gene therapy: The tortuous path from bench to bedside

TL;DR: This review summarizes the current status of various MGT protocols described in the literature and indicates that some of them will find clinical applications in the near future.
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Mitochondrially-imported RNA in drug discovery.

TL;DR: The import of nuclear transcribed RNAs into mitochondria is an emerging area that presents a tremendous opportunity to develop human metabolic therapeutics as mentioned in this paper, however, our knowledge base is quite limited.
References
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Book

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TL;DR: The goal of this series is to pinpoint areas of chemistry where recent progress has outpaced what is covered in any available textbooks, and then seek out and persuade experts in these fields to produce relatively concise but instructive introductions to their fields.
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TL;DR: The essential role of mitochondrial oxidative phosphorylation in cellular energy production, the generation of reactive oxygen species, and the initiation of apoptosis has suggested a number of novel mechanisms for mitochondrial pathology.
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Complete structure of the 11-subunit bovine mitochondrial cytochrome bc1 complex.

TL;DR: In this article, crystal structures of the 11-subunit bc1 complex from bovine heart reveal full views of this bifunctional enzyme, and the "Rieske" iron-sulfur protein subunit shows significant conformational changes in different crystal forms.
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Protein import into mitochondria.

TL;DR: Molecular chaperones in the matrix exert multiple functions in translocation, sorting, folding, and assembly of newly imported proteins.
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Protein import into mitochondria.

TL;DR: The TIM23 complex is a major translocase in the inner mitochondrial membrane that uses two energy sources, namely membrane potential and ATP, to facilitate preprotein translocation across the inner membrane and insertion into the inner membranes.
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