Your search keyword '"Clarke, David J."' showing total 41 results

1. Microbial metabolites as modulators of host physiology

Author

Joyce, Susan A., primary and Clarke, David J., additional

Published

2024

2. A mechanistic evaluation of human beta defensin 2 mediated protection of human skin barrier in vitro

Author

Shelley, Jennifer R., McHugh, Brian J., Wills, Jimi, Dorin, Julia R., Weller, Richard, Clarke, David J., and Davidson, Donald J.

Published

2023

3. Mass spectrometry-based methods for characterizing transient protein–protein interactions

Author

Veale, Clinton G.L. and Clarke, David J.

Published

2024

4. Pathological structural conversion of α-synuclein at the mitochondria induces neuronal toxicity

Author

Choi, Minee L., Chappard, Alexandre, Singh, Bhanu P., Maclachlan, Catherine, Rodrigues, Margarida, Fedotova, Evgeniya I., Berezhnov, Alexey V., De, Suman, Peddie, Christopher J., Athauda, Dilan, Virdi, Gurvir S., Zhang, Weijia, Evans, James R., Wernick, Anna I., Zanjani, Zeinab Shadman, Angelova, Plamena R., Esteras, Noemi, Vinokurov, Andrey Y., Morris, Katie, Jeacock, Kiani, Tosatto, Laura, Little, Daniel, Gissen, Paul, Clarke, David J., Kunath, Tilo, Collinson, Lucy, Klenerman, David, Abramov, Andrey Y., Horrocks, Mathew H., and Gandhi, Sonia

Published

2022

5. Can noncomplementarity of agency lead to successful problem solving? A case study on students’ interpersonal behaviors in mathematical problem-solving collaboration

Author

Haataja, Eeva S.H., Chan, Man Ching Esther, Salonen, Visajaani, and Clarke, David J.

Published

2022

6. Fidelity, pragmatism and the “grey line” in between—exploring the delivery of a pragmatic physical activity randomised controlled trial—a secondary analysis

Author

Hall, Abigail J., primary, Goodwin, Victoria A., additional, and Clarke, David J., additional

Published

2024

7. Probing TDP-43 condensation using an in silico designed aptamer

Author

Zacco, Elsa, Kantelberg, Owen, Milanetti, Edoardo, Armaos, Alexandros, Panei, Francesco Paolo, Gregory, Jenna, Jeacock, Kiani, Clarke, David J., Chandran, Siddharthan, Ruocco, Giancarlo, Gustincich, Stefano, Horrocks, Mathew H., Pastore, Annalisa, and Tartaglia, Gian Gaetano

Published

2022

8. A ribosomally synthesised and post-translationally modified peptide containing a β-enamino acid and a macrocyclic motif

Author

Wang, Shan, Lin, Sixing, Fang, Qing, Gyampoh, Roland, Lu, Zhou, Gao, Yingli, Clarke, David J., Wu, Kewen, Trembleau, Laurent, Yu, Yi, Kyeremeh, Kwaku, Milne, Bruce F., Tabudravu, Jioji, and Deng, Hai

Published

2022

9. A native mass spectrometry approach to qualitatively elucidate interfacial epitopes of transient protein–protein interactions.

Author

Veale, Clinton G. L., Chakraborty, Abir, Mhlanga, Richwell, Albericio, Fernando, de la Torre, Beatriz G., Edkins, Adrienne L., and Clarke, David J.

Subjects

MASS spectrometry, EPITOPES, HEAT shock proteins, PROTEOLYSIS, PEPTIDES

Abstract

Native mass spectrometric analysis of TPR2A and GrpE with unpurified peptides derived from limited proteolysis of their respective PPI partners (HSP90 C-terminus and DnaK) facilitated efficient, qualitative identification of interfacial epitopes involved in transient PPI formation. Application of this approach can assist in elucidating interfaces of currently uncharacterised transient PPIs. [ABSTRACT FROM AUTHOR]

Published

2024

10. Identification and expression of MarCE, a marine carboxylesterase with synthetic ester‐degrading activity.

Author

Carr, Clodagh M., Göttsch, Frederike, de Oliveira, Bruno Francesco Rodrigues, Murcia, Pedro A. Sánchez, Jackson, Stephen A., Wei, Ren, Clarke, David J., Bornscheuer, Uwe T., and Dobson, Alan D. W.

Subjects

CARBOXYLESTERASES, CARBOXYLIC acids, BIODEGRADATION, MARINE toxins, SPONGES (Invertebrates), MOLECULAR docking, BIOCHEMICAL substrates, POLYMERS

Abstract

Carboxylic ester hydrolases with the capacity to degrade polyesters are currently highly sought after for their potential use in the biological degradation of PET and other chemically synthesized polymers. Here, we describe MarCE, a carboxylesterase family protein identified via genome mining of a Maribacter sp. isolate from the marine sponge Stelligera stuposa. Based on phylogenetic analysis, MarCE and its closest relatives belong to marine‐associated genera from the Cytophaga–Flavobacterium–Bacteroides taxonomic group and appear evolutionarily distinct to any homologous carboxylesterases that have been studied to date in terms of structure or function. Molecular docking revealed putative binding of BHET, a short‐chain PET derivative, onto the predicted MarCE three‐dimensional structure. The synthetic ester‐degrading activity of MarCE was subsequently confirmed by MarCE‐mediated hydrolysis of 2 mM BHET substrate, indicated by the release of its breakdown products MHET and TPA, which were measured, respectively, as 1.28 and 0.12 mM following 2‐h incubation at 30°C. The findings of this study provide further insight into marine carboxylic ester hydrolases, which have the potential to display unique functional plasticity resulting from their adaptation to complex and fluctuating marine environmentsw. [ABSTRACT FROM AUTHOR]

Published

2024

11. Exploring liminality in the co-design of rehabilitation environments: The case of one acute stroke unit

Author

Donetto, Sara, Jones, Fiona, Clarke, David J., Cloud, Geoffrey C., Gombert-Waldron, Karolina, Harris, Ruth, Macdonald, Alastair, McKevitt, Christopher, and Robert, Glenn

Published

2021

12. Visualizing the Interface of Biotin and Fatty Acid Biosynthesis through SuFEx Probes

Author

Chen, Aochiu, primary, Re, Rebecca N., additional, Davis, Tony D., additional, Tran, Kelley, additional, Moriuchi, Yuta W., additional, Wu, Sitong, additional, La Clair, James J., additional, Louie, Gordon V., additional, Bowman, Marianne E., additional, Clarke, David J., additional, Mackay, C. Logan, additional, Campopiano, Dominic J., additional, Noel, Joseph P., additional, and Burkart, Michael D., additional

Published

2024

13. Utilising Fourier transform ion cyclotron resonance mass spectrometry (FT-ICR MS) to track the oxidation of lignin by an alkaliphilic laccase

Author

Towle, Zak, primary, Cruickshank, Faye, additional, Mackay, C. Logan, additional, Clarke, David J., additional, and Horsfall, Louise E., additional

Published

2024

14. Author Correction: Pathological structural conversion of α-synuclein at the mitochondria induces neuronal toxicity

Author

Choi, Minee L., Chappard, Alexandre, Singh, Bhanu P., Maclachlan, Catherine, Rodrigues, Margarida, Fedotova, Evgeniya I., Berezhnov, Alexey V., De, Suman, Peddie, Christopher J., Athauda, Dilan, Virdi, Gurvir S., Zhang, Weijia, Evans, James R., Wernick, Anna I., Zanjani, Zeinab Shadman, Angelova, Plamena R., Esteras, Noemi, Vinokurov, Andrey Y., Morris, Katie, Jeacock, Kiani, Tosatto, Laura, Little, Daniel, Gissen, Paul, Clarke, David J., Kunath, Tilo, Collinson, Lucy, Klenerman, David, Abramov, Andrey Y., Horrocks, Mathew H., and Gandhi, Sonia

Published

2022

15. Two-color coincidence single-molecule pulldown for the specific detection of disease-associated protein aggregates

Author

Saleeb, Rebecca S., primary, Leighton, Craig, additional, Lee, Ji-Eun, additional, O’Shaughnessy, Judi, additional, Jeacock, Kiani, additional, Chappard, Alexandre, additional, Cumberland, Robyn, additional, Zhao, Tianxiao, additional, Ball, Sarah R., additional, Sunde, Margaret, additional, Clarke, David J., additional, Piché, Kristin, additional, McPhail, Jacob A., additional, Louwrier, Ariel, additional, Angers, Rachel, additional, Gandhi, Sonia, additional, Downey, Patrick, additional, Kunath, Tilo, additional, and Horrocks, Mathew H., additional

Published

2023

16. 3′-O-β-Glucosyl-4′,5′-didehydro-5′-deoxyadenosine Is a Natural Product of the Nucleocidin Producers Streptomyces virens and Streptomyces calvus

Author

Feng, Xuan, primary, Zhang, Qingzhi, additional, Clarke, David J., additional, Deng, Hai, additional, and O’Hagan, David, additional

Published

2023

17. Intervention to reduce sedentary behaviour and improve outcomes after stroke (Get Set Go): a study protocol for the process evaluation of a pilot cluster randomised controlled trial (RECREATE)

Author

Johansson, Jessica Faye, primary, Shannon, Rosie, additional, Mossabir, Rahena, additional, Airlie, Jennifer, additional, Ozer, Seline, additional, Moreau, Lauren A, additional, Farrin, Amanda, additional, Mead, Gillian, additional, English, Coralie, additional, Fitzsimons, Claire F, additional, Clarke, David J, additional, and Forster, Anne, additional

Published

2023

18. Chapter Three - Microbial metabolites as modulators of host physiology.

Author

Joyce, Susan A. and Clarke, David J.

Abstract

The gut microbiota is increasingly recognised as a key player in influencing human health and changes in the gut microbiota have been strongly linked with many non-communicable conditions in humans such as type 2 diabetes, obesity and cardiovascular disease. However, characterising the molecular mechanisms that underpin these associations remains an important challenge for researchers. The gut microbiota is a complex microbial community that acts as a metabolic interface to transform ingested food (and other xenobiotics) into metabolites that are detected in the host faeces, urine and blood. Many of these metabolites are only produced by microbes and there is accumulating evidence to suggest that these microbe-specific metabolites do act as effectors to influence human physiology. For example, the gut microbiota can digest dietary complex polysaccharides (such as fibre) into short-chain fatty acids (SCFA) such as acetate, propionate and butyrate that have a pervasive role in host physiology from nutrition to immune function. In this review we will outline our current understanding of the role of some key microbial metabolites, such as SCFA, indole and bile acids, in human health. Whilst many studies linking microbial metabolites with human health are correlative we will try to highlight examples where genetic evidence is available to support a specific role for a microbial metabolite in host health and well-being. [ABSTRACT FROM AUTHOR]

Published

2024

19. Two-color coincidence single-molecule pull-down for the specific detection of disease-associated protein aggregates

Author

Saleeb, Rebecca S., primary, Leighton, Craig, additional, Lee, Ji-Eun, additional, O’Shaughnessy, Judi, additional, Jeacock, Kiani, additional, Chappard, Alexandre, additional, Cumberland, Robyn, additional, Ball, Sarah R., additional, Sunde, Margaret, additional, Clarke, David J., additional, Piché, Kristin, additional, McPhail, Jacob A., additional, Louwrier, Ariel, additional, Angers, Rachel, additional, Gandhi, Sonia, additional, Downey, Patrick, additional, Kunath, Tilo, additional, and Horrocks, Mathew H., additional

Published

2023

20. Purification and biochemical characterization of SM14est, a PET-hydrolyzing enzyme from the marine sponge-derived Streptomyces sp. SM14

Author

Carr, Clodagh M., primary, Keller, Malene B., additional, Paul, Bijoya, additional, Schubert, Sune W., additional, Clausen, Kristine S. R., additional, Jensen, Kenneth, additional, Clarke, David J., additional, Westh, Peter, additional, and Dobson, Alan D. W., additional

Published

2023

21. Tracking the Chemical Diversity of Enzymatically Oxidised Lignin.

Author

Towle, Zak, primary, Cruickshank, Faye, additional, Mackay, C. Logan, additional, Clarke, David J., additional, and Horsfall, Louise E., additional

Published

2023

22. Determining the Location of the α-Synuclein Dimer Interface Using Native Top-Down Fragmentation and Isotope Depletion-Mass Spectrometry

Author

Jeacock, Kiani, primary, Chappard, Alexandre, additional, Gallagher, Kelly J., additional, Mackay, C. Logan, additional, Kilgour, David P. A., additional, Horrocks, Mathew H., additional, Kunath, Tilo, additional, and Clarke, David J., additional

Published

2023

23. Membrane lipids from gut microbiome-associated bacteria as structural and signalling molecules

Author

Ryan, Eileen, primary, Joyce, Susan A., additional, and Clarke, David J., additional

Published

2023

24. Lipidomic Analysis Reveals Differences in Bacteroides Species Driven Largely by Plasmalogens, Glycerophosphoinositols and Certain Sphingolipids

Author

Ryan, Eileen, primary, Gonzalez Pastor, Belén, additional, Gethings, Lee A., additional, Clarke, David J., additional, and Joyce, Susan A., additional

Published

2023

25. Single‐Molecule Two‐Color Coincidence Detection of Unlabeled alpha‐Synuclein Aggregates

Author

Chappard, Alexandre, primary, Leighton, Craig, additional, Saleeb, Rebecca S., additional, Jeacock, Kiani, additional, Ball, Sarah R., additional, Morris, Katie, additional, Kantelberg, Owen, additional, Lee, Ji‐Eun, additional, Zacco, Elsa, additional, Pastore, Annalisa, additional, Sunde, Margaret, additional, Clarke, David J., additional, Downey, Patrick, additional, Kunath, Tilo, additional, and Horrocks, Mathew H., additional

Published

2023

26. Design and Fabrication of a Fully-Integrated, Miniaturised Fluidic System for the Analysis of Enzyme Kinetics

Author

Tsiamis, Andreas, primary, Buchoux, Anthony, additional, Mahon, Stephen T., additional, Walton, Anthony J., additional, Smith, Stewart, additional, Clarke, David J., additional, and Stokes, Adam A., additional

Published

2023

27. 3′-O-β-Glucosyl-4′,5′-didehydro-5′-deoxyadenosine Is a Natural Product of the Nucleocidin Producers Streptomyces virensand Streptomyces calvus

Author

Feng, Xuan, Zhang, Qingzhi, Clarke, David J., Deng, Hai, and O’Hagan, David

Abstract

3′-O-β-Glucosyl-4′,5′-didehydro-5′-deoxyadenosine 13is identified as a natural product of Streptomyces calvusand Streptomyces virens. It is also generated in vitroby direct β-glucosylation of 4′,5′-didehydro-5′-deoxyadenosine 12with the enzyme NucGT. The intact incorporation of oxygen-18 and deuterium isotopes from (±)[1-18O,1-2H2]-glycerol 14into C-5′ of nucleocidin 1and its related metabolites precludes 3′-O-β-glucosyl-4′,5′-didehydro-5′-deoxyadenosine 13as a biosynthetic precursor to nucleocidin 1.

Published

2023

28. Native Mass Spectrometry‐Guided Screening Identifies Hit Fragments for HOP‐HSP90 PPI Inhibition**

Author

Vaaltyn, Michaelone C., primary, Mateos‐Jimenez, Maria, additional, Müller, Ronel, additional, Mackay, C. Logan, additional, Edkins, Adrienne L., additional, Clarke, David J., additional, and Veale, Clinton G. L., additional

Published

2022

29. Lipidomic analysis reveals differences in Bacteroides species driven largely by plasmalogens, glycerophosphoinositols and certain sphingolipids

Author

Ryan, Eileen, primary, Gonzales Pastor, Belén, additional, Gethings, Lee A., additional, Clarke, David J., additional, and Joyce, Susan A., additional

Published

2022

30. Structural conversion of α-synuclein at the mitochondria induces neuronal toxicity

Author

Choi, Minee L., primary, Chappard, Alexandre, additional, Singh, Bhanu P., additional, Maclachlan, Catherine, additional, Rodrigues, Margarida, additional, Fedotova, Evgenia, additional, Berezhnov, Alexey V., additional, De, Suman, additional, Peddie, Chris, additional, Athauda, Dilan, additional, Virdi, Gurvir S., additional, Zhang, Weijia, additional, Evans, James R., additional, Wernick, Anna, additional, Zanjani, Zeinab Shadman, additional, Angelova, Plamena R., additional, Esteras, Noemi, additional, Vinikurov, Andrey, additional, Morris, Katie, additional, Jeacock, Kiani, additional, Tosatto, Laura, additional, Little, Daniel, additional, Gissen, Paul, additional, Clarke, David J., additional, Kunath, Tilo, additional, Collinson, Lucy, additional, Klenerman, David, additional, Abramov, Andrey Y., additional, Horrocks, Mathew H., additional, and Gandhi, Sonia, additional

Published

2022

31. Polyesterase activities in bacterial isolates from seaweed and sponges, with potential utility in polyethylene terephthalate plastic and nanoparticle hydrolysis

Author

Carr, Clodagh M., primary, Clarke, David J., additional, and Dobson, Alan D. W., additional

Published

2022

32. Identification of BgP, a Cutinase-Like Polyesterase From a Deep-Sea Sponge-Derived Actinobacterium

Author

Carr, Clodagh M., primary, de Oliveira, Bruno Francesco Rodrigues, additional, Jackson, Stephen A., additional, Laport, Marinella Silva, additional, Clarke, David J., additional, and Dobson, Alan D. W., additional

Published

2022

33. Editorial: New Antimicrobial Peptides From Bacteria/Invertebrate Obligate Symbiotic Associations

Author

Fodor, András, primary, Clarke, David J., additional, Dillman, Adler R., additional, Tarasco, Eustachio, additional, and Hazir, Selcuk, additional

Published

2022

34. Corrigendum to “Mass spectrometry analysis of the oxidation states of the pro oncogenic protein anterior gradient-2 reveals covalent dimerization via an intermolecular disulphide bond” [Biochimica et Biophysica Acta 1864 (2016) 551–561]

Author

Clarke, David J., Murray, Euan, Faktor, Jakub, AimanMohtar, Vojtesek, Borek, MacKay, C. Logan, Smith, Pat Langridge, and Hupp, Ted R.

Published

2022

35. Pore dynamics and asymmetric cargo loading in an encapsulin nanocompartment

Author

Ross, Jennifer, primary, McIver, Zak, additional, Lambert, Thomas, additional, Piergentili, Cecilia, additional, Bird, Jasmine Emma, additional, Gallagher, Kelly J., additional, Cruickshank, Faye L., additional, James, Patrick, additional, Zarazúa-Arvizu, Efrain, additional, Horsfall, Louise E., additional, Waldron, Kevin J., additional, Wilson, Marcus D., additional, Mackay, C. Logan, additional, Baslé, Arnaud, additional, Clarke, David J., additional, and Marles-Wright, Jon, additional

Published

2022

36. “Bind, cleave and leave”: multiple turnover catalysis of RNA cleavage by bulge–loop inducing supramolecular conjugates

Author

Amirloo, Bahareh, primary, Staroseletz, Yaroslav, additional, Yousaf, Sameen, additional, Clarke, David J, additional, Brown, Tom, additional, Aojula, Harmesh, additional, Zenkova, Marina A, additional, and Bichenkova, Elena V, additional

Published

2021

37. In Vitro and In Vivo Assessment of the Potential of Escherichia coli Phages to Treat Infections and Survive Gastric Conditions

Author

Kaczorowska, Joanna, primary, Casey, Eoghan, additional, Lugli, Gabriele A., additional, Ventura, Marco, additional, Clarke, David J., additional, van Sinderen, Douwe, additional, and Mahony, Jennifer, additional

Published

2021

38. A qualitative study of sedentary behaviours in stroke survivors: non-participant observations and interviews with stroke service staff in stroke units and community services.

Author

Morton, Sarah, Hall, Jennifer, Fitzsimons, Claire, Hall, Jessica, English, Coralie, Forster, Anne, Lawton, Rebecca, Patel, Anita, Mead, Gillian, and Clarke, David J.

Subjects

SEDENTARY lifestyles, SCIENTIFIC observation, ATTITUDES of medical personnel, RESEARCH methodology, INTERVIEWING, COMMUNITY health services, QUALITATIVE research, STROKE units, PSYCHOSOCIAL factors, STROKE patients, UNOBTRUSIVE measures, RESEARCH funding, THEMATIC analysis, DATA analysis software, PERSONNEL management

Abstract

Sedentary behaviour (SB) is associated with negative health outcomes and is prevalent post-stroke. This study explored SB after stroke from the perspective of stroke service staff. Qualitative mixed-methods study. Non-participant observations in two stroke services (England/Scotland) and semi-structured interviews with staff underpinned by the COM-B model of behaviour change. Observations were analysed thematically; interviews were analysed using the Framework approach. One hundred and thirty-two observation hours (October - December 2017), and 31 staff interviewed (January –June 2018). Four themes were identified: (1) Opportunities for staff to support stroke survivors to reduce SB; (2) Physical and psychological capability of staff to support stroke survivors to reduce SB; (3) Motivating factors influencing staff behaviour to support stroke survivors to reduce SB; (4) Staff suggestions for a future intervention to support stroke survivors to reduce SB. Staff are aware of the consequences of prolonged sitting but did not relate to SB. Explicit knowledge of SB was limited. Staff need training to support stroke survivors to reduce SB. Sedentary behaviour in the community was not reported to change markedly, highlighting the need to engage stroke survivors in movement from when capable in hospital, following through to home. Stroke survivor sedentary behaviour is influenced, directly and indirectly, by the actions and instructions of stroke service staff in the inpatient and community setting. The built and social environment, both in the inpatient and community settings, may limit opportunities for safe movement and can result in stroke survivors spending more time sedentary. Stroke service staff appreciate the benefit of encouraging stroke survivors to stand and move more, if it is safe for them to do so. Staff would be amenable to encourage stroke survivors to reduce sedentary behaviour, provided they have the knowledge and resources to equip them to support this. [ABSTRACT FROM AUTHOR]

Published

2022

39. "Bind, cleave and leave": multiple turnover catalysis of RNA cleavage by bulge–loop inducing supramolecular conjugates.

Author

Amirloo, Bahareh, Staroseletz, Yaroslav, Yousaf, Sameen, Clarke, David J, Brown, Tom, Aojula, Harmesh, Zenkova, Marina A, and Bichenkova, Elena V

Published

2022

40. A native mass spectrometry platform identifies HOP inhibitors that modulate the HSP90–HOP protein–protein interaction.

Author

Veale, Clinton G. L., Mateos-Jiménez, Maria, Vaaltyn, Michaelone C., Müller, Ronel, Makhubu, Matodzi P., Alhassan, Mahama, de la Torre, Beatriz G., Albericio, Fernando, Mackay, C. Logan, Edkins, Adrienne L., and Clarke, David J.

Subjects

PROTEIN-protein interactions, MASS spectrometry, PROOF of concept, PEPTIDES

Abstract

Herein we describe a native mass spectromery protein–peptide model as a competent surrogate for the HOP–HSP90 protein–protein interaction (PPI), application of which led to the qualititive identification of two new peptides capable of in vitro PPI disruption. This proof of concept study offers a viable alternative for PPI inhibitor screening. [ABSTRACT FROM AUTHOR]

Published

2021

41. Pathological structural conversion of α-synuclein at the mitochondria induces neuronal toxicity

Author

Minee L. Choi, Alexandre Chappard, Bhanu P. Singh, Catherine Maclachlan, Margarida Rodrigues, Evgeniya I. Fedotova, Alexey V. Berezhnov, Suman De, Christopher J. Peddie, Dilan Athauda, Gurvir S. Virdi, Weijia Zhang, James R. Evans, Anna I. Wernick, Zeinab Shadman Zanjani, Plamena R. Angelova, Noemi Esteras, Andrey Y. Vinokurov, Katie Morris, Kiani Jeacock, Laura Tosatto, Daniel Little, Paul Gissen, David J. Clarke, Tilo Kunath, Lucy Collinson, David Klenerman, Andrey Y. Abramov, Mathew H. Horrocks, Sonia Gandhi, Choi, Minee L [0000-0001-9414-8214], Chappard, Alexandre [0000-0002-9522-2575], De, Suman [0000-0003-1675-0773], Peddie, Christopher J [0000-0002-8329-5419], Evans, James R [0000-0003-2923-281X], Wernick, Anna I [0000-0001-9048-9492], Angelova, Plamena R [0000-0003-4596-9117], Esteras, Noemi [0000-0002-7938-6131], Morris, Katie [0000-0002-8944-2264], Gissen, Paul [0000-0002-9712-6122], Clarke, David J [0000-0002-3741-2952], Kunath, Tilo [0000-0002-8805-7356], Klenerman, David [0000-0001-7116-6954], Abramov, Andrey Y [0000-0002-7646-7235], Horrocks, Mathew H [0000-0001-5495-5492], Gandhi, Sonia [0000-0003-4395-2661], Apollo - University of Cambridge Repository, Choi, Minee L. [0000-0001-9414-8214], Peddie, Christopher J. [0000-0002-8329-5419], Evans, James R. [0000-0003-2923-281X], Wernick, Anna I. [0000-0001-9048-9492], Angelova, Plamena R. [0000-0003-4596-9117], Clarke, David J. [0000-0002-3741-2952], Abramov, Andrey Y. [0000-0002-7646-7235], and Horrocks, Mathew H. [0000-0001-5495-5492]

Subjects

Neurons, 631/57, Cardiolipins, General Neuroscience, FOS: Clinical medicine, Stem Cells, article, Neurons/metabolism, Neurosciences, Parkinson Disease, Cell Biology, Mitochondria, Mitochondrial Membranes/metabolism, Imaging, alpha-Synuclein/metabolism, Mitochondrial Membranes, Mitochondria/metabolism, alpha-Synuclein, 631/378/1689/1718, Humans, 631/80/642/333, Parkinson Disease/genetics, Cardiolipins/metabolism

Abstract

Aggregation of alpha-synuclein (α-Syn) drives Parkinson’s disease (PD), although the initial stages of self-assembly and structural conversion have not been directly observed inside neurons. In this study, we tracked the intracellular conformational states of α-Syn using a single-molecule Förster resonance energy transfer (smFRET) biosensor, and we show here that α-Syn converts from a monomeric state into two distinct oligomeric states in neurons in a concentration-dependent and sequence-specific manner. Three-dimensional FRET-correlative light and electron microscopy (FRET-CLEM) revealed that intracellular seeding events occur preferentially on membrane surfaces, especially at mitochondrial membranes. The mitochondrial lipid cardiolipin triggers rapid oligomerization of A53T α-Syn, and cardiolipin is sequestered within aggregating lipid–protein complexes. Mitochondrial aggregates impair complex I activity and increase mitochondrial reactive oxygen species (ROS) generation, which accelerates the oligomerization of A53T α-Syn and causes permeabilization of mitochondrial membranes and cell death. These processes were also observed in induced pluripotent stem cell (iPSC)–derived neurons harboring A53T mutations from patients with PD. Our study highlights a mechanism of de novo α-Syn oligomerization at mitochondrial membranes and subsequent neuronal toxicity.

Published

2022