AI Article Synopsis

  • The biogenesis of human mitochondrial complex I involves the assembly of 45 subunits from both mitochondrial and nuclear DNA, suggesting a multi-step process.
  • Using an inducible GFP tagging system in HEK293 cells, the study demonstrated that distinct intermediate subcomplexes of complex I appear during assembly, as observed through specific blotting techniques.
  • Inhibiting mitochondrial translation caused the accumulation of certain subcomplexes, confirming them as genuine assembly intermediates, and indicating that mitochondrial DNA-encoded subunits play a crucial role in this process.

Article Abstract

Biogenesis of human mitochondrial complex I (CI) requires the coordinated assembly of 45 subunits derived from both the mitochondrial and nuclear genome. The presence of CI subcomplexes in CI-deficient cells suggests that assembly occurs in distinct steps. However, discriminating between products of assembly or instability is problematic. Using an inducible NDUFS3-green fluorescent protein (GFP) expression system in HEK293 cells, we here provide direct evidence for the stepwise assembly of CI. Upon induction, six distinct NDUFS3-GFP-containing subcomplexes gradually appeared on a blue native Western blot also observed in wild type HEK293 mitochondria. Their stability was demonstrated by differential solubilization and heat incubation, which additionally allowed their distinction from specific products of CI instability and breakdown. Inhibition of mitochondrial translation under conditions of steady state labeling resulted in an accumulation of two of the NDUFS3-GFP-containing subcomplexes (100 and 150 kDa) and concomitant disappearance of the fully assembled complex. Lifting inhibition reversed this effect, demonstrating that these two subcomplexes are true assembly intermediates. Composition analysis showed that this event was accompanied by the incorporation of at least one mitochondrial DNA-encoded subunit, thereby revealing the first entry point of these subunits.

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Source
http://dx.doi.org/10.1074/jbc.M609410200DOI Listing

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