Intercellular Mitochondrial Transfer as a Rescue Mechanism in Response to Protein Import Failure

Needs, Hope I; Pereira, Gonçalo C.; Glover, Emily; Witt, Alina; Hübner, Wolfgang; Dodding, Mark P.; Henley, Jeremy M.; Collinson, Ian

doi:10.1101/2022.11.30.518494

Cited by 3 publications

(21 citation statements)

References 68 publications

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“…This is consistent with previous reports that showed Tau P301L accumulation in the OMM and IMS (Cieri et al, 2018; Hu et al, 2016), and suggests that it may be associated with the translocation channel in a similar way to an artificially trapped precursor protein (Chacinska et al, 2003; Ford et al, 2022; Hope I Needs et al, 2022). Surprisingly, however, despite association of Tau P301L with the import machinery, in-cell NanoLuc import assays (Hope I. Needs et al, 2022) showed that the import kinetics of a precursor reporter were not significantly affected (Fig.…”

Section: Resultssupporting

confidence: 93%

“…This can be achieved with the small molecule inhibitor MB20 (Cheung, 2017), or with a precursor fused to DHFR which, when bound to methotrexate, becomes trapped in the channel (Chacinska et al, 2003; Ford et al, 2022). While these treatments inhibit import in isolated mitochondria (Cheung, 2017; Ford et al, 2022), we unexpectedly found that they fail to do so within whole cells (Hope I Needs et al, 2022). We wondered if the apparent lack of effect on the whole mitochondrial population of the cell could be explained by a mitochondrial replacement system.…”

Section: Resultsmentioning

confidence: 74%

“…We wondered if the apparent lack of effect on the whole mitochondrial population of the cell could be explained by a mitochondrial replacement system. We found that, at the whole cell level, defective mitochondrial function is rescued by the recruitment of healthy mitochondria from surrounding cells, and disposal of compromised mitochondria, by way of TNTs (Hope I Needs et al, 2022). Therefore, we were curious if the association of the Tau variant with the import apparatus induced a similar response.…”

Section: Resultsmentioning

confidence: 96%

“…In a parallel study, we explored the effects of artificially blocking the import machinery (Hope I Needs et al, 2022). This can be achieved with the small molecule inhibitor MB20 (Cheung, 2017), or with a precursor fused to DHFR which, when bound to methotrexate, becomes trapped in the channel (Chacinska et al, 2003; Ford et al, 2022).…”

Section: Resultsmentioning

confidence: 99%

“…TNTs induced by import impairment contain actin as well as microtubules, which are necessary for mitochondrial movement (Hope I Needs et al, 2022). Thus, drugs that target actin (cytochalasin D) and tubulin (nocodazole) polymerisation inhibit TNT formation (Bittins & Wang, 2017; Kumar et al, 2017; Luchetti et al, 2012).…”

Section: Resultsmentioning

confidence: 99%

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Perturbation of the mitochondrial import machinery by aggregation prone Tau affects organelle morphology and reduces neuronal complexity

Needs

Henley

Collinson

2022

Preprint

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Protein import into mitochondria is an intricate and highly conserved process essential for organellar biogenesis, and maintenance of its structure and function. Defects in the import apparatus impact the assembly of the respiratory chain and ATP synthase complexes required for oxidative phosphorylation, compromising the ready supply of ATP to the cell. The consequences of reduced bioenergetic function are particularly severe for cells with high energetic demands such as neurons. However, relatively little is known about how defective import contributes to neurodegeneration, or how neurotoxic proteins characteristic of neurodegenerative diseases impact mitochondrial import efficiency. Here, we used HeLa cells to investigate how expressing high levels of Tau variants affect mitochondrial import activity, morphology, and function. We found that the variant associated with neurodegeneration (TauP301L) colocalises with mitochondria. TauP301L, but not wildtype Tau, interacts with TOM40, the protein-channel component of the outer membrane protein import complex. Interestingly, TauP301L expression had no discernible effect on overall mitochondrial import function, despite associating with TOM40 and altering mitochondrial morphology, suggesting that a rescue mechanism is at play. This rescue could be explained by the appearance of microtubule and actin containing tunnelling nanotubes (TNTs), used to recruit healthy mitochondria from neighbouring cells and/or dispose of mitochondria with aggregated Tau. Furthermore, in primary neuronal cultures TauP301L induces morphological changes that resemble a neurodegeneration like phenotype, and this is mirrored in cells where the import sites are blocked artificially. These results reveal an intriguing link between the production of aggregation prone protein variants, such as Tau, and the mitochondrial protein import machinery relevant to neurodegenerative disease.

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Section: Resultssupporting

confidence: 93%

Section: Resultsmentioning

confidence: 74%

Section: Resultsmentioning

confidence: 96%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Perturbation of the mitochondrial import machinery by aggregation prone Tau affects organelle morphology and reduces neuronal complexity

Needs

Henley

Collinson

2022

Preprint

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Aggregation-prone Tau impairs mitochondrial import, which affects organelle morphology and neuronal complexity

Needs

Wilkinson

Henley

et al. 2023

Journal of Cell Science

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Mitochondrial protein import is essential for organellar biogenesis, and thereby for the sufficient supply of cytosolic ATP–particularly important for cells with high energy demands like neurons. This study explores the prospect of import machinery perturbation as a cause of neurodegeneration instigated by the accumulation of aggregating proteins linked to disease. The aggregation-prone Tau variant (TauP301L) reduces the levels of components of the import machinery of the outer (TOM20) and inner membrane (TIM23) while associating with TOM40. Intriguingly, this interaction affects mitochondrial morphology, but not protein import or respiratory function; raising the prospect of an intrinsic rescue mechanism. Indeed, TauP301L induced the formation of tunnelling nanotubes (TNTs), potentially for the recruitment of healthy mitochondria from neighbouring cells and/or the disposal of mitochondria incapacitated by aggregated Tau. Consistent with this, inhibition of TNT formation (and rescue) reveals Tau-induced import impairment. In primary neuronal cultures, TauP301L induced morphological changes characteristic of neurodegeneration. Interestingly, these effects were mirrored in cells where the import sites were blocked artificially. Our results reveal a link between aggregation-prone Tau and defective mitochondrial import machinery relevant to disease.

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Analysis of Sigma-1 Receptor Antagonist BD1047 Effect on Upregulating Proteins in HIV-1-Infected Macrophages Exposed to Cocaine Using Quantitative Proteomics

Vélez-López,

Carrasquillo-Carrión,

Cantres-Rosario

et al. 2024

Biomedicines

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HIV-1 infects monocyte-derived macrophages (MDM) that migrate into the brain and secrete virus and neurotoxic molecules, including cathepsin B (CATB), causing cognitive dysfunction. Cocaine potentiates CATB secretion and neurotoxicity in HIV-infected MDM. Pretreatment with BD1047, a sigma-1 receptor antagonist, before cocaine exposure reduces HIV-1, CATB secretion, and neuronal apoptosis. We aimed to elucidate the intracellular pathways modulated by BD1047 in HIV-infected MDM exposed to cocaine. We hypothesized that the Sig1R antagonist BD1047, prior to cocaine, significantly deregulates proteins and pathways involved in HIV-1 replication and CATB secretion that lead to neurotoxicity. MDM culture lysates from HIV-1-infected women treated with BD1047 before cocaine were compared with untreated controls using TMT quantitative proteomics, bioinformatics, Lima statistics, and pathway analyses. Results demonstrate that pretreatment with BD1047 before cocaine dysregulated eighty (80) proteins when compared with the infected cocaine group. We found fifteen (15) proteins related to HIV-1 infection, CATB, and mitochondrial function. Upregulated proteins were related to oxidative phosphorylation (SLC25A-31), mitochondria (ATP5PD), ion transport (VDAC2–3), endoplasmic reticulum transport (PHB, TMED10, CANX), and cytoskeleton remodeling (TUB1A-C, ANXA1). BD1047 treatment protects HIV-1-infected MDM exposed to cocaine by upregulating proteins that reduce mitochondrial damage, ER transport, and exocytosis associated with CATB-induced neurotoxicity.

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Intercellular Mitochondrial Transfer as a Rescue Mechanism in Response to Protein Import Failure

Cited by 3 publications

References 68 publications

Perturbation of the mitochondrial import machinery by aggregation prone Tau affects organelle morphology and reduces neuronal complexity

Perturbation of the mitochondrial import machinery by aggregation prone Tau affects organelle morphology and reduces neuronal complexity

Aggregation-prone Tau impairs mitochondrial import, which affects organelle morphology and neuronal complexity

Analysis of Sigma-1 Receptor Antagonist BD1047 Effect on Upregulating Proteins in HIV-1-Infected Macrophages Exposed to Cocaine Using Quantitative Proteomics

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