Your search keyword '"Allan, Victoria"' showing total 16 results

1. A human infertility-associated KASH5 variant promotes mitochondrial localization

Author

Bentebbal, Sana A., Meqbel, Bakhita R., Salter, Anna, Allan, Victoria, Burke, Brian, and Horn, Henning F.

Subjects

Science, Medicine, Reproductive medicine

Abstract

KASH5 is the most recently identified member of the KASH domain family of tail anchored, outer nuclear membrane (ONM) and endoplasmic reticulum (ER) proteins. During meiosis prophase I, KASH5 and SUN1 form a complex that spans the nuclear envelope and which links the telomeres of meiotic chromosomes to cytoplasmic dynein. This connection is essential for homologous chromosome dynamics and pairing. A recent study identified a variant in human KASH5 (L535Q) that correlated with male infertility associated with azoospermia. However, no molecular mechanism was described. Here, we report that this amino acid substitution, within the KASH5 transmembrane domain (TMD) has no predicted effects on secondary structure. However, the overall hydrophobicity of the L535Q TMD, is calculated to be lower than the wild-type KASH5, based on the GES (Goldman–Engelman–Steitz) amino acid hydrophobicity scale. This change in hydrophobicity profoundly affects the subcellular localization of KASH5. Through a series of amino acid substitution studies, we show that the L535Q substitution perturbs KASH5 localization to the ER and ONM and instead results in mistargeting to the mitochondria membrane. We suggest that this mislocalization accounts for the infertility and azoospermia phenotype in patients.Other Information Published in: Scientific Reports License: https://creativecommons.org/licenses/by/4.0See article on publisher's website: http://dx.doi.org/10.1038/s41598-021-89439-2

Published

2022

2. The flexibility and dynamics of the tubules in the endoplasmic reticulum

Author

Georgiades, Pantelis, Allan, Victoria, Wright, Graham D., Woodman, Philip, Udommai, Parinya, Chung, Manloeng, and Waigh, Thomas

Subjects

Science, persistence length, STORM, semi-flexible, Medicine, active, Super-resolution fluorescence microscopy, Endoplasmic Reticulum

Abstract

The endoplasmic reticulum (ER) is a single organelle in eukaryotic cells that extends throughout the cell and is involved in a large number of cellular functions. Using a combination of fixed and live cells (human MRC5 lung cells) in diffraction limited and super-resolved fluorescence microscopy (STORM) experiments, we determined that the average persistence length of the ER tubules was 3.03 ± 0.24 μm. Removing the branched network junctions from the analysis caused a slight increase in the average persistence length to 4.71 ± 0.14 μm, and provides the tubule’s persistence length with a moderate length scale dependence. The average radius of the tubules was 44.1 ± 3.2 nm. The bending rigidity of the ER tubule membranes was found to be 10.9 ± 1.2 kT (17.0 ± 1.3 kT without branch points). We investigated the dynamic behaviour of ER tubules in live cells, and found that the ER tubules behaved like semi-flexible fibres under tension. The majority of the ER tubules experienced equilibrium transverse fluctuations under tension, whereas a minority number of them had active super-diffusive motions driven by motor proteins. Cells thus actively modulate the dynamics of the ER in a well-defined manner, which is expected in turn to impact on its many functions.

Published

2017

3. Non-Markovian intracellular transport with sub-diffusion and run-length dependent detachment rate

Author

Korabel, Mykola, Waigh, Thomas, Fedotov, Sergei, and Allan, Victoria

Subjects

ResearchInstitutes_Networks_Beacons/photon_science_institute, Photon Science Institute

Published

2018

4. Memory effects and L��vy walk dynamics in intracellular transport of cargoes

Author

Fedotov, Sergei, Korabel, Nickolay, Waigh, Thomas A., Han, Daniel, and Allan, Victoria J.

Subjects

Statistical Mechanics (cond-mat.stat-mech), FOS: Biological sciences, FOS: Physical sciences, macromolecular substances, Subcellular Processes (q-bio.SC)

Abstract

We demonstrate the phenomenon of cumulative inertia in intracellular transport involving multiple motor proteins in human epithelial cells by measuring the empirical survival probability of cargoes on the microtubule and their detachment rates. We found the longer a cargo moves along a microtubule, the less likely it detaches from it. As a result, the movement of cargoes is non-Markovian and involves a memory. We observe memory effects on the scale of up to 2 seconds. We provide a theoretical link between the measured detachment rate and the super-diffusive Levy walk-like cargo movement., 9 pages, 6 figures

Published

2018

5. A tale of two α-tubulin tails

Author

Allan, Victoria

Published

2016

6. Tumour Suppressor Adenomatous Polyposis Coli (APC) localisation is regulated by both Kinesin-1 and Kinesin-2

Author

Ruane, Peter T, Gumy, Laura F, Bola, Becky, Anderson, Beverley, Wozniak, Marcin J, Hoogenraad, Casper C, Allan, Victoria J, Sub Cell Biology, and Celbiologie

Subjects

macromolecular substances

Abstract

Microtubules and their associated proteins (MAPs) underpin the polarity of specialised cells. Adenomatous polyposis coli (APC) is one such MAP with a multifunctional agenda that requires precise intracellular localisations. Although APC has been found to associate with kinesin-2 subfamily members, the exact mechanism for the peripheral localization of APC remains unclear. Here we show that the heavy chain of kinesin-1 directly interacts with the APC C-terminus, contributing to the peripheral localisation of APC in fibroblasts. In rat hippocampal neurons the kinesin-1 binding domain of APC is required for its axon tip enrichment. Moreover, we demonstrate that APC requires interactions with both kinesin-2 and kinesin-1 for this localisation. Underlining the importance of the kinesin-1 association, neurons expressing APC lacking kinesin-1-binding domain have shorter axons. The identification of this novel kinesin-1-APC interaction highlights the complexity and significance of APC localisation in neurons.

Published

2016

7. Reduction of coherent artefacts in super-resolution fluorescence localisation microscopy

Author

Georgiades, Pantelis, Allan, Victoria, Dickinson, Mark, and Waigh, Thomas

Abstract

Super-resolution localisation microscopy techniques depend on uniform illumination across the field of view, otherwise the resolution is degraded, resulting in imaging artefacts such as fringes. Lasers are currently the light source of choice for switching fluorophores in PALM/STORM methods due to their high power and narrow bandwidth. However, the high coherence of these sources often creates interference phenomena in the microscopes, with associated fringes/speckle artefacts in the images. We quantitatively demonstrate the use of a polymer membrane speckle scrambler to reduce the effect of the coherence phenomena. The effects of speckle in the illumination plane, at the camera and after software localisation of the fluorophores, were characterised. Speckle phenomena degrade the resolution of the microscope at large length scales in reconstructed images, effects that were suppressed by the speckle scrambler, but the small length scale resolution is unchanged at ~30 nm.

Published

2016

8. ESCRT-0 marks an APPL1-independent transit route for EGFR between the cell surface and the EEA1-positive early endosome

Author

Flores-Rodriguez, Neftali, Kenwright, David A, Chung, Pei-Hua, Harrison, Andrew W, Stefani, Flavia, Waigh, Thomas A, Allan, Victoria J, and Woodman, Philip G

Subjects

ESCRT-I, Hrs, Particle-based colocalisation, EGFR, macromolecular substances, EEA1

Abstract

ESCRT-0 sorts ubiquitinated EGFR within the early endosome, so that the receptor can be incorporated into intralumenal vesicles. An important question is whether ESCRT-0 acts solely upon EGFR that has already entered the vacuolar early endosome (characterised by the presence of EEA1) or engages EGFR within earlier compartments. Here we employ a suite of software to localise ESCRT-0 at subpixel resolution and to perform particle-based colocalisation analysis with other endocytic markers. We demonstrate that although some of the ESCRT-0 subunit Hrs colocalises with the vacuolar early endosome marker EEA1, most localises to a population of peripheral EEA1-negative endosomes that act as intermediates in transporting EGFR from the cell surface to more central early endosomes. The peripheral Hrs-labelled endosomes are distinct from APPL1-containing endosomes, but co-label with the novel endocytic adaptor SNX15. In contrast to ESCRT-0, ESCRT-I is recruited to EGF-containing endosomes at later times as they move to more a central position, whilst ESCRT-III is also recruited more gradually. RNA silencing experiments show that both ESCRT-0 and ESCRT-I are important for the transit of EGF to EEA1 endosomes.

Published

2015

9. MOESM1 of Bleeding in cardiac patients prescribed antithrombotic drugs: electronic health record phenotyping algorithms, incidence, trends and prognosis

Author

Pasea, Laura, Sheng-Chia Chung, Pujades-Rodriguez, Mar, Anoop Shah, Alvarez-Madrazo, Samantha, Allan, Victoria, Teo, James, Bean, Daniel, Reecha Sofat, Dobson, Richard, Banerjee, Amitava, Riyaz Patel, Timmis, Adam, Denaxas, Spiros, and Hemingway, Harry

Subjects

ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, ComputingMilieux_COMPUTERSANDEDUCATION, Data_FILES, ComputerApplications_COMPUTERSINOTHERSYSTEMS, 3. Good health

Abstract

Additional file 1. Supplementary methods, figures and tables.

10. MOESM1 of Bleeding in cardiac patients prescribed antithrombotic drugs: electronic health record phenotyping algorithms, incidence, trends and prognosis

Author

Pasea, Laura, Sheng-Chia Chung, Pujades-Rodriguez, Mar, Anoop Shah, Alvarez-Madrazo, Samantha, Allan, Victoria, Teo, James, Bean, Daniel, Reecha Sofat, Dobson, Richard, Banerjee, Amitava, Riyaz Patel, Timmis, Adam, Denaxas, Spiros, and Hemingway, Harry

Subjects

ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, ComputingMilieux_COMPUTERSANDEDUCATION, Data_FILES, ComputerApplications_COMPUTERSINOTHERSYSTEMS, 3. Good health

Abstract

Additional file 1. Supplementary methods, figures and tables.

11. Relating cell shape, mechanical stress and cell division in epithelial tissues

Author

Nestor-Bergmann, Alexander, ALLAN, VICTORIA VJ, JENSEN, OLIVER OE, Woolner, Sarah, Allan, Victoria, and Jensen, Oliver

Subjects

Tissue mechanics, vertex model, Cell division, Biophysics, Cell shape, spindle, mathematical biology, Cell stress

Abstract

The development and maintenance of tissues and organs depend on the careful regulation and coordinated motion of large numbers of cells. There is substantial evidence that many complex tissue functions, such as cell division, collective cell migration and gene expression, are directly regulated by mechanical forces. However, relatively little is known about how mechanical stress is distributed within a tissue and how this may guide biochemical signalling. Working in the framework of a popular vertex-based model, we derive expressions for stress tensors at the cell and tissue level to build analytic relationships between cell shape and mechanical stress. The discrete vertex model is upscaled, providing exact expressions for the bulk and shear moduli of disordered cellular networks, which bridges the gap to traditional continuum-level descriptions of tissues. Combining this theoretical work with new experimental techniques for whole-tissue stretching of Xenopus laevis tissue, we separate the roles of mechanical stress and cell shape in orienting and cueing epithelial mitosis. We find that the orientation of division is best predicted by the shape of tricellular junctions, while there appears to be a more direct role for mechanical stress as a mitotic cue.

Published

2018

12. INVESTIGATING CELLULAR FUNCTIONS OF GORAB AND ITS ROLE IN GERODERMIA OSTEODYSPLASTICA

Author

Witkos, Tomasz, ALLAN, VICTORIA VJ, Allan, Victoria, and Lowe, Martin

Subjects

gerodermia osteodysplastica, intra-Golgi trafficking, cutis laxa, GORAB

Abstract

GORAB is a protein that localises to the trans-Golgi network (TGN) and is known to interact with Rab6. The loss of GORAB leads to gerodermia osteodysplastica (GO), an autosomal recessive disorder which results in lax skin, precocious skin aging, osteoporosis, susceptibility to fractures and joint hyperelasticity. Both the function of GORAB and the mechanism of pathogenesis in GO patients are poorly defined.In this study, the cellular functions of GORAB have been investigated. Using a variety of approaches (yeast two-hybrid assays, pull-downs with recombinant proteins, proximity biotinylation assays combined with mass spectrometry and co-immunoprecipitations) it was possible to establish a network of interactions with Golgi-localised proteins, including Arf GTPases and the COPI-associated protein Scyl1, that suggests a possible role of GORAB in COPI-mediated trafficking. Consistent with this hypothesis, ultrastructural changes of the Golgi apparatus were observed as were abnormal protein glycosylation in primary skin fibroblasts derived from GO patients, detected using both lectin binding assays and mass spectrometric glycan profiling. Moreover, immuno-electron microscopy studies revealed unequal distribution of GORAB within the TGN and fluorescence recovery after photobleaching experiments show GORAB being very stably associated with Golgi membranes. These properties of GORAB seem to result from its ability to oligomerise and to interact with vimentin filaments. Based on these data, a model of GORAB acting as a scaffolding protein that organises sites of COPI budding at the TGN has been proposed. Additionally, analysis of both published and newly identified GORAB mutations found in GO patients revealed that they affect various properties of GORAB including its interaction with small GTPases and GORAB ability to oligomerise, which suggests that these features are important for GORAB cellular functions.Together, these data suggest that the underlying cause of the skin and bone defects observed in GO patients is impaired COPI trafficking at the Golgi apparatus resulting in abnormal glycosylation of extracellular matrix proteins.

Published

2016

13. Direct stochastic optical reconstruction microscopy (dSTORM) imaging of cellular structures

Author

Sanders, James Henry, DICKINSON, MARK MR, ALLAN, VICTORIA VJ, Waigh, Thomas, Dickinson, Mark, and Allan, Victoria

Subjects

Super-resolution, dSTORM, fluorescence microscopy

Abstract

The diffraction limit restricts conventional light microscopes to approximately 250 nm laterally and 500 nm axially, these limits being first proposed by Abbe in 1873. Despite this, optical microscopes have found many applications in biological research and single cells that are 10 - 100 um in size. Furthermore by coupling the non-invasive nature of a light microscope with highly sensitive fluorescent probes, fluorescence microscopy has also become a standard imaging technique. Recent advances in fluorescence microscopy now provide a number of methods to circumvent the Abbe diffraction limit, with many techniques becoming prevalent over the last 10 years including direct Stochastic Optical Reconstruction Microscopy (dSTORM). A dSTORM system has been constructed and calibrated using a commercially available inverted florescence microscope and total internal reflection florescence (TIRF) imaging. dSTORM relies on the ability to switch sparse subsets of fluorophores and temporally separate them. Provided the spatial separation is sufficient between any member of a subset, the average error with which the emission can be localized is much less than size of the emission profile itself. The underlying mechanism for this switching is detailed based on the principle of photoinduced electron transfer (PET). The switching characteristics of the common florescent dye Alexa Fluor 568 are investigated and shown to be controlled by a number of factors including the excitation intensity and concentration of the primary thiol cysteamine beta-MEA. A number of parameters are defined, including the dye switching rate, for a given set of physical parameters. U2OS cells are labelled for the microtubule protein Tubulin using immunofluorescent labelling strategies. A direct comparison is made between diffraction limited TIRF images and dSTORM reconstructed images, with an average width for microtubules determined to (58.2 ± 8.1) nm. Further measurements are made by labelling the Rab5 effector Early Endosome Antigen 1 (EEA1). From this the aspect ratio for early endosomes is determined to be 1.68 ± 0.7 with an average radius of (45.8 ± 18.8) nm. The point spatial distribution of EEA1 is investigated by using the linearised form of Ripley's K-function H(r) and the null hypothesis of complete spatial randomness tested. EEA1 is shown to cluster at radius of 58.7 nm on individual endosomes, thought to be due to the well defined binding domains present on early endosomes for EEA1. Further evidence suggests that clustering is also exhibited at another maximum of approximately 500 nm when looking at an ensemble of EEA1 and early endosomes.

Published

2015

14. THE INTERPLAY BETWEEN DYNEIN, ACCESSORY PROTEINS AND THE ENDOCYTIC PATHWAY

Author

Granger, Elizabeth, LOWE, MARTIN MP, Allan, Victoria, and Lowe, Martin

Subjects

macromolecular substances

Abstract

Elizabeth GrangerThe University of ManchesterThe interplay between dynein, accessory proteins and the endocytic pathwayDoctor of Philosophy, Organelle Function25-09-13Cytoplasmic dynein 1 (dynein) is a multi-subunit complex that transports cargo along microtubules towards their minus ends. These microtubule minus ends are normally located toward the centre of the cell. Dynein is involved in transport of endocytic and autophagic membranes and is tightly regulated by interactions between dynein subunits and by dynein-accessory proteins. Dynein accessory proteins that are involved in a wide range of dynein-driven transport events include dynactin, Lis1 and the paralogues Nde1 and Ndel1. Lis1 and Nde1/Ndel1 interact with each other and are involved in the recruitment of dynein to cargo and in regulating dynein activity. Although much is known about the specific interactions of dynein and accessory proteins, the interplay between dynein and its network of regulators in living cells is not well defined.This project used RNAi to investigate how the dynein subunits light intermediate chain (LIC) and intermediate chain (IC) as well as Lis1 and Nde1/Ndel1 influence the endocytic pathway, autophagy and cargo recruitment. Biochemical analysis of bulk membrane preparations showed that IC is important for dynein and dynactin association with intracellular membranes. In addition, dynein and dynactin recruitment to Rab interacting lysosomal protein (RILP)-positive membranes was shown to require LIC and there was redundancy between LIC1 and LIC2 in this role. Lis1 was also needed for dynactin-dynein recruitment to these membranes, in a context that was Nde1/Ndel1-independent.Loss of LIC, IC, Lis1 and Nde1 had differing effects on endocytic compartment size and distribution, but they all led to mislocalisation of early endosomes and lysosomes and caused lysosomes to become enlarged. Loss of LIC led to a specific phenotype whereby cells formed lamellipodia-like regions in which early endosomes and lysosomes accumulated. Loss of Lis1 prevented traffic from the early endosome to late endosomes and caused a striking enlargement of late endosomes and lysosomes. These enlarged lysosomes were LC3-positive, indicating that they were autophagic. In addition, loss of IC and LIC also led to an increase in LC3 puncta, but the LC3 did not colocalise specifically with lysosomes.In summary, the results from this project show that i) dynactin recruitment to intracellular membranes, including RILP-postivie membranes, requires dynein, ii) Lis1 and LIC1 or LIC2 are necessary but not sufficient, individually, to recruit dynein and dynactin to RILP-positive membranes iii) LIC, IC, Lis1 and Nde1/Ndel1 influence endocytic progression in specific ways, which may in turn affect autophagic flux.

Published

2014

15. The regulation of dynein function in membrane movement by NudEL

Author

Yang, Yen Ching, SWANTON, LISA E, Allan, Victoria, and Swanton, Lisa

Subjects

LIS1, Organelle positioning, Ndel1, Dynein, ER movement, macromolecular substances, NudEL, Motor Protein

Abstract

The accurate regulation of cytoplasmic dynein-1 (dynein) is very important since dynein performs multiple functions in cells. In interphase, dynein is responsible for the correct positioning of membrane organelles, such as the Golgi complex and lysosomes. Previous work suggests that dynein's accessory proteins NudEL/Nde1/LIS1¬ may be involved in regulating dynein-dependent organelle movement. This study focuses on how NudEL regulates dynein-driven membrane movement. By using various NudEL fragments, this work presents the first evidence that NudEL is involved in the regulation of dynein-driven ER movement in vitro. Moreover, the in vivo organelle positioning assays also indicate additional regulatory function of NudEL.NudEL fragment (1-157 aa) which contains both the dynein and LIS1 binding domains is sufficient to activate dynein-driven membrane movement, since NudEL1-157 aa activates ER motility in vitro and enhances clustering of the Golgi complex and lysosomes in the peri-nuclear region in vivo. On the other hand, NudEL 96-206 aa containing the LIS1 binding domain alone inhibits ER motility in vitro and causes scattering of the Golgi complex and lysosomes in vivo, indicating an inhibition of dynein-dependent organelle movement. The activation of dynein activity requires the recruitment of LIS1 to the dynein complex by NudEL, since NudEL 1-157 aa has strong binding affinity to both LIS1 and dynein whereas NudEL 96-206 aa binds to LIS1 but not dynein which suggests the sequestering of LIS1 from the dynein complex. Interestingly, NudEL 1-206 aa, which also contains both the dynein and LIS1 binding domains, causes the dispersal of the Golgi complex and lysosomes in vivo, but to a lesser extent than NudEL 96-206 aa. The putative NudEL regulatory domain (157 -242 aa, which contains various phosphorylation sits and is less conserved between NudEL and Nde1) in NudEL 1-206 aa may regulate the interaction of LIS1 and the dynein complex, since NudEL 1-206 aa has strong binding affinity to LIS1 and weak binding affinity to dynein. However, further work is needed to understand the exact mechanism by which this putative NudEL domain regulates dynein activity.

Published

2013

16. Function and Regulation of Kinesin-1, -2 and -3

Author

Brownhill, Kim and Allan, Victoria

Subjects

Brefeldin A, Microtubule, macromolecular substances, Kinesin, Cell cycle

Abstract

In this work the functions of the microtubule motors kinesin-1, -2 and -3 have been analysed in various settings. The reconstitution of microtubule-dependent motor activity in vitro has been primarily used to dissect the contributions of individual motors to cargo motility in two specific scenarios. Initially the regulation of kinesin-1 in a cell cycle-dependent manner has been examined by studying the ability of rat liver endoplasmic reticulum (ER) tubules to move in cytosols prepared from Xenopus laevis egg extracts arrested in interphase, meiosis or mitosis. It was found that kinesin-1-driven ER motility is significantly disrupted during metaphase in vitro. This is likely due to the recruitment or loss of binding partners which has a concomitant influence upon kinesin-1 activity. This work presents the first evidence that kinesin-1-driven ER movement, and not simply network morphology, varies during cell division. Furthermore, it is postulated that the replication of such regulation of kinesin-1 activity in vivo may contribute to the well documented changes in organelle positioning and cargo transit through membrane trafficking pathways which occur during cell division.The fungal metabolite brefeldin A (BFA) induces tubulation of several compartments located within the secretory and endocytic pathways in a microtubule-dependent fashion. The identity of the motor(s) responsible for this motility remains unconfirmed and controversial since several reports with conflicting data have been published. The contributions of kinesin-1, -2 and -3 to these processes have been investigated using in vitro motility assays in which rat liver Golgi membranes were combined with Xenopus laevis egg extract cytosol in the presence of BFA. Function blocking antibodies and dominant negative proteins were used to perturb the activities of various kinesin motors. This data indicates a particular isoform of kinesin-3, KIF1C, is solely responsible for the movement of BFA-induced tubules in vitro. This work was complemented by in vivo immunofluorescence studies using the HeLaM cultured cell line. Transient transfections of dominant negative proteins, or siRNA-mediated depletion, were used to disrupt the activities of various kinesin motors, either in isolation or in combination with each other. This approach revealed a contribution of KIF1C and kinesin-1 to the movement of early endosomal BFA-induced tubules in vivo.

Published

2010