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2 research outputs found

Defining the architecture of the human TIM22 complex by chemical crosslinking

Author: Callegari S.
Deckers M.
Ficner R.
Linden A.
Neumann P.
Rehling P.
Urlaub H.
Valpadashi A.
Publication venue: 'Wiley'
Publication date: 24/01/2021
Field of study

The majority of mitochondrial proteins are nuclear encoded and imported into mitochondria as precursor proteins via dedicated translocases. The translocase of the inner membrane 22 (TIM22) is a multisubunit molecular machine specialized for the translocation of hydrophobic, multi‐transmembrane‐spanning proteins with internal targeting signals into the inner mitochondrial membrane. Here, we undertook a crosslinking‐mass spectrometry (XL‐MS) approach to determine the molecular arrangement of subunits of the human TIM22 complex. Crosslinking of the isolated TIM22 complex using the BS3 crosslinker resulted in the broad generation of crosslinks across the majority of TIM22 components, including the small TIM chaperone complex. The crosslinking data uncovered several unexpected features, opening new avenues for a deeper investigation into the steps required for TIM22‐mediated translocation in humans

MPG.PuRe

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The SARS-CoV-2 protein ORF3c is a mitochondrial modulator of innate immunity

Author: Adewusi Yasmin
Carnell George W
Cruz-Zaragoza Luis Daniel
Davidson Andrew D
Edgar James R
Emmott Edward
Firth Andrew E
Heeney Jonathan L
High Stephen
Jungreis Irwin
Lu Yongxu
Lukhovitskaya Nina
Lulla Valeria
Matthews David A
Michel Hendrik A
Milligan Rachel
Nguyen Samantha K
O’Keefe Sarah
Rehling Peter
Smith Geoffrey L
Stewart Hazel
Valpadashi Anusha
Publication venue: iScience
Publication date: 01/09/2023
Field of study

The SARS-CoV-2 genome encodes a multitude of accessory proteins. Using comparative genomic approaches, an additional accessory protein, ORF3c, has been predicted to be encoded within the ORF3a sgmRNA. Expression of ORF3c during infection has been confirmed independently by ribosome profiling. Despite ORF3c also being present in the 2002–2003 SARS-CoV, its function has remained unexplored. Here we show that ORF3c localises to mitochondria, where it inhibits innate immunity by restricting IFN-β production, but not NF-κB activation or JAK-STAT signalling downstream of type I IFN stimulation. We find that ORF3c is inhibitory after stimulation with cytoplasmic RNA helicases RIG-I or MDA5 or adaptor protein MAVS, but not after TRIF, TBK1 or phospho-IRF3 stimulation. ORF3c co-immunoprecipitates with the antiviral proteins MAVS and PGAM5 and induces MAVS cleavage by caspase-3. Together, these data provide insight into an uncharacterised mechanism of innate immune evasion by this important human pathogen

Apollo (Cambridge)