Biochemistry and Pharmacology - Research Publications

Permanent URI for this collection

http://hdl.handle.net/11343/214

Filters

2019 - 2019 2 2020 - 2023 2
Reset filters

Settings
Statistics
Citations
Author: Anderson, Alexander × Start date: 2010 × Type: Journal Article ×

Search Results

Now showing 1 - 4 of 4
  • Item
    Thumbnail Image
    Human Tim8a, Tim8b and Tim13 are auxiliary assembly factors of mature Complex IV
    Anderson, AJ ; Crameri, JJ ; Ang, C-S ; Malcolm, TR ; Kang, Y ; Baker, MJ ; Palmer, CS ; Sharpe, AJ ; Formosa, LE ; Ganio, K ; Baker, MJ ; McDevitt, CA ; Ryan, MT ; Maher, MJ ; Stojanovski, D (Wiley, 2023-06-05)
    Human Tim8a and Tim8b are paralogous intermembrane space proteins of the small TIM chaperone family. Yeast small TIMs function in the trafficking of proteins to the outer and inner mitochondrial membranes. This putative import function for hTim8a and hTim8b has been challenged in human models, but their precise molecular function(s) remains undefined. Likewise, the necessity for human cells to encode two Tim8 proteins and whether any potential redundancy exists is unclear. We demonstrate that hTim8a and hTim8b function in the assembly of cytochrome c oxidase (Complex IV). Using affinity enrichment mass spectrometry, we define the interaction network of hTim8a, hTim8b and hTim13, identifying subunits and assembly factors of the Complex IV COX2 module. hTim8‐deficient cells have a COX2 and COX3 module defect and exhibit an accumulation of the Complex IV S2 subcomplex. These data suggest that hTim8a and hTim8b function in assembly of Complex IV via interactions with intermediate‐assembly subcomplexes. We propose that hTim8–hTim13 complexes are auxiliary assembly factors involved in the formation of the Complex IV S3 subcomplex during assembly of mature Complex IV.
  • Item
    Thumbnail Image
    Mitochondrial protein import dysfunction: mitochondrial disease, neurodegenerative disease and cancer
    Palmer, CS ; Anderson, AJ ; Stojanovski, D (WILEY, 2021-04)
    The majority of proteins localised to mitochondria are encoded by the nuclear genome, with approximately 1500 proteins imported into mammalian mitochondria. Dysfunction in this fundamental cellular process is linked to a variety of pathologies including neuropathies, cardiovascular disorders, myopathies, neurodegenerative diseases and cancer, demonstrating the importance of mitochondrial protein import machinery for cellular function. Correct import of proteins into mitochondria requires the co-ordinated activity of multimeric protein translocation and sorting machineries located in both the outer and inner mitochondrial membranes, directing the imported proteins to the destined mitochondrial compartment. This dynamic process maintains cellular homeostasis, and its dysregulation significantly affects cellular signalling pathways and metabolism. This review summarises current knowledge of the mammalian mitochondrial import machinery and the pathological consequences of mutation of its components. In addition, we will discuss the role of mitochondrial import in cancer, and our current understanding of the role of mitochondrial import in neurodegenerative diseases including Alzheimer's disease, Huntington's disease and Parkinson's disease.
  • Item
    Thumbnail Image
    Mitochondria-hubs for regulating cellular biochemistry: emerging concepts and networks
    Anderson, AJ ; Jackson, TD ; Stroud, DA ; Stojanovski, D (ROYAL SOC, 2019-08)
    Mitochondria are iconic structures in biochemistry and cell biology, traditionally referred to as the powerhouse of the cell due to a central role in energy production. However, modern-day mitochondria are recognized as key players in eukaryotic cell biology and are known to regulate crucial cellular processes, including calcium signalling, cell metabolism and cell death, to name a few. In this review, we will discuss foundational knowledge in mitochondrial biology and provide snapshots of recent advances that showcase how mitochondrial function regulates other cellular responses.
  • Item
    Thumbnail Image
    Function of hTim8a in complex IV assembly in neuronal cells provides insight into pathomechanism underlying Mohr-Tranebjaerg syndrome
    Kang, Y ; Anderson, AJ ; Jackson, TD ; Palmer, CS ; De Souza, DP ; Fujihara, KM ; Stait, T ; Frazier, AE ; Clemons, NJ ; Tull, D ; Thorburn, DR ; McConville, MJ ; Ryan, MT ; Stroud, DA ; Stojanovski, D (ELIFE SCIENCES PUBLICATIONS LTD, 2019-11-04)
    Human Tim8a and Tim8b are members of an intermembrane space chaperone network, known as the small TIM family. Mutations in TIMM8A cause a neurodegenerative disease, Mohr-Tranebjærg syndrome (MTS), which is characterised by sensorineural hearing loss, dystonia and blindness. Nothing is known about the function of hTim8a in neuronal cells or how mutation of this protein leads to a neurodegenerative disease. We show that hTim8a is required for the assembly of Complex IV in neurons, which is mediated through a transient interaction with Complex IV assembly factors, in particular the copper chaperone COX17. Complex IV assembly defects resulting from loss of hTim8a leads to oxidative stress and changes to key apoptotic regulators, including cytochrome c, which primes cells for death. Alleviation of oxidative stress with Vitamin E treatment rescues cells from apoptotic vulnerability. We hypothesise that enhanced sensitivity of neuronal cells to apoptosis is the underlying mechanism of MTS.