The assembly and function of the mitochondrial respiratory chain (RC) involve the organization of RC enzyme complexes in supercomplexes or respirasomes through an unknown biosynthetic process. This leads to structural interdependences between RC complexes, which are highly relevant from biological and biomedical perspectives, because RC defects lead to severe human disorders. We show that in human cells, respirasome biogenesis involves a complex I assembly intermediate acting as a scaffold for the combined incorporation of complexes III and IV subunits, rather than originating from the association of preassembled individual holoenzymes. The process ends with the incorporation of complex I NADH dehydrogenase catalytic module, which leads to the respirasome activation. While complexes III and IV assemble either as free holoenzymes or by incorporation of free subunits into supercomplexes, the respirasomes constitute the structural units where complex I is assembled and activated, thus explaining the functional significance of the respirasomes for RC function

Arenas, Joaquín

Barrientos, Antoni

Fontanesi, Flavia

García Consuegra, Inés

Martín, Miguel A.

Moreno Lastres, David

Ugalde, Cristina

PubMed

Ugalde, C.

Moreno-Lastres, D.

Fontanesi, F.

García-Consuegra, I.

Martín, M.A.

Barrientos, A.

Arenas, J.

Elsevier - Publisher Connector 

Mitochondrial complex I plays an essential role in human respirasome assembly 

The biogenesis and function of the mitochondrial respiratory chain (RC) involve the organization of RC enzyme complexes in supercomplexes or respirasomes through an unknown biosynthetic process. This leads to structural interdependences between RC complexes, which are highly relevant from biological and biomedical perspectives, because RC defects often lead to severe neuromuscular disorders. We show that in human cells, respirasome biogenesis involves a complex I assembly intermediate acting as a scaffold for the combined incorporation of complexes III and IV subunits, rather than originating from the association of preassembled individual holoenzymes. The process ends with the incorporation of complex I NADH dehydrogenase catalytic module, which leads to the respirasome activation. While complexes III and IV assemble either as free holoenzymes or by incorporation of free subunits into supercomplexes, the respirasomes constitute the structural units where complex I is assembled and activated, thus explaining the significance of the respirasomes for RC function.
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► Mitochondrial respirasome biogenesis is a multistep biosynthetic process ► It does not require the associations of independent preassembled RC complexes ► A CI intermediate acts as a scaffold for the incorporation of free CIII+CIV subunits ► Respirasomes are the structural units in which CI is fully assembled and activate

Moreno-Lastres, David

Fontanesi, Flavia

García-Consuegra, Inés

Martín, Miguel A

Arenas, Joaquín

Barrientos, Antoni

Ugalde, Cristina

University of Miami: Scholarship Miami

Cell Metabolism

Mitochondrial Complex I Plays an Essential Role in Human Respirasome Assembly

C. Ugalde

D. Moreno-Lastres

F. Fontanesi

I. García-Consuegra

M.A. Martín

A. Barrientos

J. Arenas

Crossref

Biochimica et Biophysica Acta (BBA) - Bioenergetics

Mitochondrial complex I plays an essential role in human respirasome assembly

Biblos-e Archivo

Ugalde, C

Moreno-Lastres, D

Fontanesi, F

García-Consuegra, I

Martín, M.A

Barrientos, A

Arenas, J

David Moreno-Lastres

Flavia Fontanesi

Inés García-Consuegra

Miguel A. Martín

Joaquín Arenas

Antoni Barrientos

Cristina Ugalde

systemic disorders of variable severity. Due to the complex III dual
genetic origin, these enzyme defects can be attributed to mutations
located either in mitochondrial or in nuclear genes. An increasing
number of speciﬁc regulatory proteins involved in the biosynthesis
of this respiratory chain complex that may also lead to complex III
deﬁciency has been described. One of these proteins is BCS1L, an
assembly factor that facilitates the insertion of the catalytic Rieske
Iron–Sulfur subunit into respiratory chain complex III. Mutations in
the BCS1L gene constitue the main cause of complex III deﬁciency. In
the search for potential biomarkers for complex III deﬁciency we
performed two-dimensional difference gel electrophoresis (2D DIGE)
followed by spot picking and subsequent protein digestion for mass
spectrometry (MS) identiﬁcation in ﬁbroblasts from four complex III-
deﬁcient patients harboring mutations in the BCS1L gene and four
independent controls. Here we report 41 proteins that are differen-
tially expressed in patients harbouring BCS1L mutations compared to
controls. These proteins are mainly related to energy metabolism,
cytoskeleton maintenance processes, regulation of DNA transcription
and replication and protein synthesis, cell cycle regulation and oxidative
stress response. Further studies are required for the validation and
functional characterization of possible biomarkers that may be of im-
portance for future diagnostic, therapeutic, and prognostic approaches in
mitochondrial disorders.
doi:10.1016/j.bbabio.2012.06.367
18P5
Structural interactions of mitochondrial ATP
synthasome components
H. Nůsková, T. Mikulová, M. Vrbacký, T. Mráček, J. Houštěk
Department of Bioenergetics, Institute of Physiology Academy of Sciences
of the Czech Republic v.v.i., Vídeňská 1083, 14220 Prague, Czech Republic
E-mail: hana.nuskova@gmail.com
The mitochondrial phosphorylation apparatus consists of three
protein components — ADP/ATP carrier (AAC), inorganic phosphate
carrier (PiC), and F1Fo-ATP synthase. According to some experimen-
tal evidence, these proteins of the inner mitochondrial membrane
could interact not only functionally, but also structurally [1]. Their
supercomplex called ATP synthasome would show better catalytic
efﬁciency of ATP synthesis.
To characterize interactions of AAC, PiC, and ATP synthase in
mammalian cells, we used two models of isolated ATP synthase
deﬁciency — rat brown adipose tissue with physiological deﬁciency of
ATP synthase due to low expression of Fo-c subunit and ﬁbroblast
cultures of patients with ATP synthase deﬁciency caused by a mutation
in the assembly factor TMEM70. SDS-PAGE/WB analysis of isolated
mitochondria revealed that among rat tissues, AAC and PiC are most
abundant in the tissues with high energetic demands, i.e. in heart and
skeletalmuscle. However, their amountwas also high in brown adipose
tissue despite the low content of ATP synthase. In the ATP synthase
deﬁcient patients' ﬁbroblasts, we also found a high content of AAC and
PiC that was even increased in comparison to control cells. The lack of
correlation in the contents of ATP synthase and mitochondrial carriers
AAC and PiC does not support a direct relationship in the regulation of
their biogenesis.
Simultaneously, we studied structural interactions of AAC, PiC,
and ATP synthase using various approaches. Detergent-solubilized
mitochondria were used for immunoprecipitation and native
and two-dimensional gel electrophoreses combined with either
immunodetection with speciﬁc antibodies or MS analysis. Our results
indicate that both carriers interact with monomeric and oligomeric
forms of ATP synthase. The majority of these carriers, however, are
present out of ATP synthasome, probably as dimers.
This work was supported by the Grant Agency of the Czech
Republic (grant P303/10/0P227).
Reference
[1] Y.H. Ko, M. Delannoy, J. Hullihen, W. Chiu, P.L. Pedersen, J. Biol.
Chem. 278 (2003) 12305–12309.
doi:10.1016/j.bbabio.2012.06.368
18P6
Mitochondrial complex I plays an essential role in human
respirasome assembly
C. Ugalde, D. Moreno-Lastres, F. Fontanesi, I. García-Consuegra,
M.A. Martín, A. Barrientos, J. Arenas
Instituto de Investigación and Centro de Investigación Biomédica en Red
de Enfermedades Raras (CIBERER- U723), Hospital Universitario 12 de
Octubre, Avenida de Córdoba sn, Madrid 28041, Spain
Department of Neurology, University of Miami Miller School of Medicine,
1600 NW 10th Avenue, Miami, FL 33136, USA
Department of Biochemistry, University ofMiamiMiller School ofMedicine,
1600 NW 10th Avenue, Miami, FL 33136, USA
E-mail: cugalde@h12o.es
The biogenesis and function of themitochondrial respiratory chain
(RC) involves the association of individual RC enzyme complexes into
supercomplexes or respirasomes, through a biosynthetic process
that remains largely unknown. Here we show that in human cells,
I+III2+IVn supercomplexes do not originate from the association
of fully-assembled individual holoenzymes. Rather, we demonstrate
that respirasome biogenesis involves a complex I assembly interme-
diate acting as a scaffold for the combined incorporation of free
subunits and subcomplexes from complexes III and IV. The process
ends with the association of the complex I NADH dehydrogenase
catalytic module, which leads to complex I and respirasome activa-
tion. Our studies reveal that while complexes III and IV can assemble
either as free holoenzymes or by incorporation of free subunits into
supercomplexes, the respirasomes constitute the structural units
where complex I is assembled and activated, thus explaining the
signiﬁcance of the respirasomes for RC function.
Reference
[1] D. Moreno-Lastres, F. Fontanesi, I. García-Consuegra, M.A.
Martín, J. Arenas, A. Barrientos, C. Ugalde, Cell Metab. 15 (2012)
324–335.
doi:10.1016/j.bbabio.2012.06.369
18P7
FRET reveals lactacystin-induced increase of Tom20/TOM assembly
Bettina Rieger, Wladislaw Kohl, Karin Busch
Department of Biology/Chemistry, Mitochondrial Dynamics,
University of Osnabrück, D-49076 Osnabrück, Germany
E-mail: Bettina.Rieger@Biologie.Uni-Osnabrueck.de
The Translocase of the Outer mitochondrial Membrane (TOM) is a
protein complex that translocates nuclear encoded proteins into
mitochondria. The isolated TOM holo complex consists of the pore-
forming channel protein Tom40, Tom22 and the small Tom proteins
AbstractsS140


SummaryThe biogenesis and function of the mitochondrial respiratory chain (RC) involve the organization of RC enzyme complexes in supercomplexes or respirasomes through an unknown biosynthetic process. This leads to structural interdependences between RC complexes, which are highly relevant from biological and biomedical perspectives, because RC defects often lead to severe neuromuscular disorders. We show that in human cells, respirasome biogenesis involves a complex I assembly intermediate acting as a scaffold for the combined incorporation of complexes III and IV subunits, rather than originating from the association of preassembled individual holoenzymes. The process ends with the incorporation of complex I NADH dehydrogenase catalytic module, which leads to the respirasome activation. While complexes III and IV assemble either as free holoenzymes or by incorporation of free subunits into supercomplexes, the respirasomes constitute the structural units where complex I is assembled and activated, thus explaining the significance of the respirasomes for RC function

Moreno-Lastres, David

García-Consuegra, Inés

Martín, Miguel A.

Mitochondrial Complex I Plays an Essential Role in Human Respirasome Assembly 

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Mitochondrial complex I plays an essential role in human respirasome assembly

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