Assembly of NADH: Ubiquinone Reductase (complex I) in Neurospora Mitochondria. Independent Pathways of Nuclear-encoded and Mitochondrially Encoded Subunits

Overview

Journal J Mol Biol

Publisher Elsevier

Specialties Microbiology
Molecular Biology

Date 1990 Jun 20

PMID 2141652

Citations 37

Authors

G Tuschen

U Sackmann

U Nehls

H Haiker

G Buse

H Weiss

Affiliations

Soon will be listed here.

Abstract

NADH:ubiquinone reductase, the respiratory chain complex I of mitochondria, consists of some 25 nuclear-encoded and seven mitochondrially encoded subunits, and contains as redox groups one FMN, probably one internal ubiquinone and at least four iron-sulphur clusters. We are studying the assembly of the enzyme in Neurospora crassa. The flux of radioactivity in cells that were pulse-labelled with [35S]methionine was followed through immunoprecipitable assembly intermediates into the holoenzyme. Labelled polypeptides were observed to accumulate transiently in a Mr 350,000 intermediate complex. This complex contains all mitochondrially encoded subunits of the enzyme as well as subunits encoded in the nucleus that have no homologous counterparts in a small, merely nuclear-encoded form of the NADH:ubiquinone reductase made by Neurospora crassa cells poisoned with chloramphenicol. With regard to their subunit compositions, the assembly intermediate and small NADH:ubiquinone reductase complement each other almost perfectly to give the subunit composition of the large complex I. These results suggest that two pathways exist in the assembly of complex I that independently lead to the preassembly of two major parts, which subsequently join to form the complex. One preassembled part is related to the small form of NADH:ubiquinone reductase and contributes most of the nuclear-encoded subunits, FMN, three iron-sulphur clusters and the site for the internal ubiquinone. The other part is the assembly intermediate and contributes all mitochondrially encoded subunits, one iron-sulphur cluster and the catalytic site for the substrate ubiquinone. We discuss the results with regard to the evolution of the electron pathway through complex I.

Citing Articles

Using cryo-EM to understand the assembly pathway of respiratory complex I.

Laube E, Schiller J, Zickermann V, Vonck J Acta Crystallogr D Struct Biol. 2024; 80(Pt 3):159-173.

PMID: 38372588 PMC: 10910544. DOI: 10.1107/S205979832400086X.

Carbon and Nitrogen Sources Have No Impact on the Organization and Composition of Respiratory Supercomplexes.

Matuz-Mares D, Flores-Herrera O, Guerra-Sanchez G, Romero-Aguilar L, Vazquez-Meza H, Matus-Ortega G J Fungi (Basel). 2021; 7(1).

PMID: 33440829 PMC: 7827470. DOI: 10.3390/jof7010042.

Insights from Drosophila on mitochondrial complex I.

Rhooms S, Murari A, Goparaju N, Vilanueva M, Owusu-Ansah E Cell Mol Life Sci. 2019; 77(4):607-618.

PMID: 31485716 PMC: 7289077. DOI: 10.1007/s00018-019-03293-0.

Regulation of Mitochondrial Complex I Biogenesis in Drosophila Flight Muscles.

Garcia C, Khajeh J, Coulanges E, Chen E, Owusu-Ansah E Cell Rep. 2017; 20(1):264-278.

PMID: 28683319 PMC: 5791762. DOI: 10.1016/j.celrep.2017.06.015.

Functional diversity of complex I subunits in Candida albicans mitochondria.

Li D, She X, Calderone R Curr Genet. 2015; 62(1):87-95.

PMID: 26373419 PMC: 4724564. DOI: 10.1007/s00294-015-0518-6.