Your search keyword '"Sabine Kupzig"' showing total 28 results

1. Blood group type A secretors are associated with a higher risk of COVID‐19 cardiovascular disease complications

Author

Tosti J. Mankelow, Belinda K. Singleton, Pedro L. Moura, Christian J. Stevens‐Hernandez, Nicola M. Cogan, Gyongyver Gyorffy, Sabine Kupzig, Luned Nichols, Claire Asby, Jennifer Pooley, Gabriella Ruffino, Faroakh Hosseini, Fiona Moghaddas, Marie Attwood, Alan Noel, Alex Cooper, David T. Arnold, Fergus Hamilton, Catherine Hyams, Adam Finn, Ashley M. Toye, and David J. Anstee

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Abstract The SARS‐CoV‐2 virus causes COVID‐19, an infection capable of causing severe disease and death but which can also be asymptomatic or oligosymptomatic. We investigated whether ABO blood group or secretor status was associated with COVID‐19 severity. We investigated secretor status because expression of ABO glycans on secreted proteins and non‐erythroid cells are controlled by a fucosyltransferase (FUT2), and inactivating FUT2 mutations result in a non‐secretor phenotype which protects against some viral infections. Data combined from healthcare records and our own laboratory tests (n = 275) of hospitalized SARS‐CoV‐2 polymerase chain reaction positive patients confirmed higher than expected numbers of blood group A individuals compared to O (RR = 1.24, CI 95% [1.05, 1.47], p = 0.0111). There was also a significant association between group A and COVID‐19‐related cardiovascular complications (RR = 2.56, CI 95% [1.43, 4.55], p = 0.0011) which is independent of gender. Molecular analysis revealed that group A non‐secretors are significantly less likely to be hospitalized than secretors. Testing of convalescent plasma donors, among whom the majority displayed COVID‐19 symptoms and only a small minority required hospitalization, group A non‐secretors were slightly over‐represented. Our findings showed that group A non‐secretors are not resistant to infection by SARS‐CoV‐2, but are more likely to experience a less severe form of associated disease.

Published

2021

2. Reticulocyte Maturation and Variant Red Blood Cells

Author

Christian J. Stevens-Hernandez, Joanna F. Flatt, Sabine Kupzig, and Lesley J. Bruce

Subjects

reticulocyte maturation, stomatocytosis, OHSt, hereditary spherocytosis, Southeast Asian ovalocytosis, cryohydrocytosis, Physiology, QP1-981

Abstract

The bone marrow produces billions of reticulocytes daily. These reticulocytes mature into red blood cells by reducing their plasma membrane by 20% and ejecting or degrading residual internal organelles, membranes and proteins not required by the mature cell. This process occurs by autophagy, protein degradation and vesiculation but is not well understood. We previously reported that Southeast Asian Ovalocytic RBCs demonstrate incomplete reticulocyte maturation and we have now extended this study to a number of other variant RBCs. By comparing the profile of a pure reticulocyte preparation of cultured red cells with these variant cells, we show that the largest of these cells, the overhydrated hereditary stomatocytosis cells, are the least mature, they barely reduced their plasma membrane and contain large amounts of proteins that should have been reduced or removed. Intermediate sized variant RBCs appear to be more mature but retain some endoplasmic reticulum and residual membrane proteins. We propose that the size and composition of these variant cell types correlate with the different stages of reticulocyte maturation and provide insight into the reticulocyte maturation process.

Published

2022

3. An immortalized adult human erythroid line facilitates sustainable and scalable generation of functional red cells

Author

Kongtana Trakarnsanga, Rebecca E. Griffiths, Marieangela C. Wilson, Allison Blair, Timothy J. Satchwell, Marjolein Meinders, Nicola Cogan, Sabine Kupzig, Ryo Kurita, Yukio Nakamura, Ashley M. Toye, David J. Anstee, and Jan Frayne

Subjects

Science

Abstract

The generation of a sustainable supply of erythroid progenitors is essential for the reliable production of anin vitroderived red blood cell clinical product. Here the authors immortalize early human erythroblasts to generate the first cell line capable of differentiation into functional adult reticulocytes.

Published

2017

4. Superior survival of ex vivo cultured human reticulocytes following transfusion into mice

Author

Sabine Kupzig, Stephen F. Parsons, Elinor Curnow, David J. Anstee, and Allison Blair

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

The generation of cultured red blood cells from stem cell sources may fill an unmet clinical need for transfusion-dependent patients, particularly in countries that lack a sufficient and safe blood supply. Cultured red blood cells were generated from human CD34+ cells from adult peripheral blood or cord blood by ex vivo expansion, and a comprehensive in vivo survival comparison with standard red cell concentrates was undertaken. Significant amplification (>105-fold) was achieved using CD34+ cells from both cord blood and peripheral blood, generating high yields of enucleated cultured red blood cells. Following transfusion, higher levels of cultured red cells could be detected in the murine circulation compared to standard adult red cells. The proportions of cultured blood cells from cord or peripheral blood sources remained high 24 hours post-transfusion (82±5% and 78±9%, respectively), while standard adult blood cells declined rapidly to only 49±9% by this time. In addition, the survival time of cultured blood cells in mice was longer than that of standard adult red cells. A paired comparison of cultured blood cells and standard adult red blood cells from the same donor confirmed the enhanced in vivo survival capacity of the cultured cells. The study herein represents the first demonstration that ex vivo generated cultured red blood cells survive longer than donor red cells using an in vivo model that more closely mimics clinical transfusion. Cultured red blood cells may offer advantages for transfusion-dependent patients by reducing the number of transfusions required.

Published

2017

5. Protein distribution during human erythroblast enucleation in vitro.

Author

Amanda J Bell, Timothy J Satchwell, Kate J Heesom, Bethan R Hawley, Sabine Kupzig, Matthew Hazell, Rosey Mushens, Andrew Herman, and Ashley M Toye

Subjects

Medicine, Science

Abstract

Enucleation is the step in erythroid terminal differentiation when the nucleus is expelled from developing erythroblasts creating reticulocytes and free nuclei surrounded by plasma membrane. We have studied protein sorting during human erythroblast enucleation using fluorescence activated cell sorting (FACS) to obtain pure populations of reticulocytes and nuclei produced by in vitro culture. Nano LC mass spectrometry was first used to determine the protein distribution profile obtained from the purified reticulocyte and extruded nuclei populations. In general cytoskeletal proteins and erythroid membrane proteins were preferentially restricted to the reticulocyte alongside key endocytic machinery and cytosolic proteins. The bulk of nuclear and ER proteins were lost with the nucleus. In contrast to the localization reported in mice, several key erythroid membrane proteins were detected in the membrane surrounding extruded nuclei, including band 3 and GPC. This distribution of key erythroid membrane and cytoskeletal proteins was confirmed using western blotting. Protein partitioning during enucleation was investigated by confocal microscopy with partitioning of cytoskeletal and membrane proteins to the reticulocyte observed to occur at a late stage of this process when the nucleus is under greatest constriction and almost completely extruded. Importantly, band 3 and CD44 were shown not to restrict specifically to the reticulocyte plasma membrane. This highlights enucleation as a stage at which excess erythroid membrane proteins are discarded in human erythroblast differentiation. Given the striking restriction of cytoskeleton proteins and the fact that membrane proteins located in macromolecular membrane complexes (e.g. GPA, Rh and RhAG) are segregated to the reticulocyte, we propose that the membrane proteins lost with the nucleus represent an excess mobile population of either individual proteins or protein complexes.

Published

2013

6. Blood group type A secretors are associated with a higher risk of COVID‐19 cardiovascular disease complications

Author

Marie Attwood, Jennifer Pooley, Catherine Hyams, Fiona Moghaddas, David J. Anstee, Adam Finn, Gabriella Ruffino, Nicola Cogan, Faroakh Hosseini, Alex Cooper, David T Arnold, Luned Nichols, Belinda K. Singleton, Gyongyver Gyorffy, Ashley M. Toye, Claire Asby, Pedro Luis Moura, Christian J Stevens-Hernandez, Alan R. Noel, Sabine Kupzig, Fergus Hamilton, and Tosti J. Mankelow

Subjects

medicine.medical_specialty, Fucosyltransferase, Coronavirus disease 2019 (COVID-19), biology, business.industry, Covid19, Disease, Group A, Asymptomatic, Gastroenterology, Virus, law.invention, fluids and secretions, law, Internal medicine, ABO blood group system, biology.protein, Medicine, medicine.symptom, Sickle Cell, Thrombosis, and Haematology, business, Research Articles, Polymerase chain reaction, Research Article

Abstract

The SARS‐CoV‐2 virus causes COVID‐19, an infection capable of causing severe disease and death but which can also be asymptomatic or oligosymptomatic. We investigated whether ABO blood group or secretor status was associated with COVID‐19 severity. We investigated secretor status because expression of ABO glycans on secreted proteins and non‐erythroid cells are controlled by a fucosyltransferase (FUT2), and inactivating FUT2 mutations result in a non‐secretor phenotype which protects against some viral infections. Data combined from healthcare records and our own laboratory tests (n = 275) of hospitalized SARS‐CoV‐2 polymerase chain reaction positive patients confirmed higher than expected numbers of blood group A individuals compared to O (RR = 1.24, CI 95% [1.05, 1.47], p = 0.0111). There was also a significant association between group A and COVID‐19‐related cardiovascular complications (RR = 2.56, CI 95% [1.43, 4.55], p = 0.0011) which is independent of gender. Molecular analysis revealed that group A non‐secretors are significantly less likely to be hospitalized than secretors. Testing of convalescent plasma donors, among whom the majority displayed COVID‐19 symptoms and only a small minority required hospitalization, group A non‐secretors were slightly over‐represented. Our findings showed that group A non‐secretors are not resistant to infection by SARS‐CoV‐2, but are more likely to experience a less severe form of associated disease.

Published

2021

7. Blood group A Secretors are associated with a higher risk of COVID-19 cardiovascular disease complications

Author

Christian J Stevens-Hernandez, Marie Attwood, Jennifer Pooley, Sabine Kupzig, David T Arnold, Fergus Hamilton, A Cooper, Nicola Cogan, David J. Anstee, Adam Finn, Ashley M. Toye, Claire Asby, Belinda K. Singleton, F Hosseini, Pedro Luis Moura, Gabriella Ruffino, Tosti J. Mankelow, L Nichols, G Gyorffy, F Moghaddas, Catherine Hyams, and Alan R. Noel

Subjects

medicine.medical_specialty, Fucosyltransferase, biology, business.industry, Disease, Group A, Phenotype, Asymptomatic, Virus, ABO blood group system, Internal medicine, Cohort, biology.protein, Medicine, medicine.symptom, business

Abstract

The SARS-CoV-2 virus causes COVID-19, an infection capable of causing severe disease and death but which may also be asymptomatic or oligosymptomatic in many individuals. While several risk factors, including age, have been described, the mechanisms of this variation are poorly understood. Several studies have described associations between blood group and COVID-19 severity, while others do not. Expression of ABO glycans on secreted proteins and non-erythroid cells is controlled by a fucosyltransferase (FUT2). Inactivating mutations result in a non-secretor phenotype which is known to protect against some viral infections. We investigated whether ABO or secretor status was associated with COVID-19 severity. Data combined from healthcare records and laboratory tests (n=275) of SARS-CoV-2 PCR positive patients hospitalised with COVID-19, confirmed higher than expected numbers of blood group A individuals compared to O (RR=1.24, CI 95% [1.05,1.47], P=0.0111). There was also a significant association between group A and COVID-19-related cardiovascular complications (RR=2.56, CI 95% [1.43,4.55], P=0.0011) which is independent of gender. Molecular analysis of phenotype revealed that group A patients who are non-secretors are significantly less likely to be hospitalised than secretors. In a larger cohort of 1000 convalescent plasma donors, among whom the majority displayed COVID-19 symptoms and only a small minority required hospitalisation, group A non-secretors were slightly over-represented. Our findings indicate that group A non-secretors are not resistant to infection by SARS-CoV-2, but they are likely to experience a less severe form of its associated disease.Key PointsBlood group type A is associated with an increased risk of cardiovascular complications in COVID-19 patients.FUT2 “non-secretor” status reduces the risk of severe COVID-19 outcomes in patients with blood group A.

Published

2020

8. Superior survival of ex vivo cultured human reticulocytes following transfusion into mice

Author

David J. Anstee, Sabine Kupzig, Allison Blair, Stephen F. Parsons, and Elinor Curnow

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Red Cell, business.industry, Cellular differentiation, CD34, Hematology, Andrology, 03 medical and health sciences, 030104 developmental biology, Immunophenotyping, Blood Component Transfusion, Cord blood, Medicine, Stem cell, business, Ex vivo

Abstract

The generation of cultured red blood cells from stem cell sources may fill an unmet clinical need for transfusion-dependent patients, particularly in countries that lack a sufficient and safe blood supply. Cultured red blood cells were generated from human CD34+ cells from adult peripheral blood or cord blood by ex vivo expansion, and a comprehensive in vivo survival comparison with standard red cell concentrates was undertaken. Significant amplification (>105-fold) was achieved using CD34+ cells from both cord blood and peripheral blood, generating high yields of enucleated cultured red blood cells. Following transfusion, higher levels of cultured red cells could be detected in the murine circulation compared to standard adult red cells. The proportions of cultured blood cells from cord or peripheral blood sources remained high 24 hours post-transfusion (82±5% and 78±9%, respectively), while standard adult blood cells declined rapidly to only 49±9% by this time. In addition, the survival time of cultured blood cells in mice was longer than that of standard adult red cells. A paired comparison of cultured blood cells and standard adult red blood cells from the same donor confirmed the enhanced in vivo survival capacity of the cultured cells. The study herein represents the first demonstration that ex vivo generated cultured red blood cells survive longer than donor red cells using an in vivo model that more closely mimics clinical transfusion. Cultured red blood cells may offer advantages for transfusion-dependent patients by reducing the number of transfusions required.

Published

2016

9. Ex vivo Engineering of Red Blood Cells

Author

Jan Frayne, Deborah E Daniels, Timothy J Satchwell, Joseph Hawksworth, Belinda K Singleton, Tatyana N Andrienko, Marieangela C Wilson, Sabine Kupzig, Marjolein Meinders, Ryo Kurita, Yukio Nakamura, Ivan Ferrer Vicens, Rebecca Griffiths, Nicola Cogan, Kongtana Trakarnsanga, David J. Anstee, and Ashley Mark Toye

Subjects

Immunology, KLF1, Cell Biology, Hematology, Biology, Biochemistry, Cell biology, Erythropoietin receptor, medicine.anatomical_structure, Reticulocyte, Cell culture, ABO blood group system, medicine, Erythropoiesis, Bone marrow, Stem cell

Abstract

Culture systems for human in vitro erythropoiesis are now well established. Using our 3-stage feeder-free erythroid culture system we can efficiently differentiate erythroid cells from adult and cord blood (CB) CD34+ cells with >105 fold expansion, enucleation rates of up to 95% and producing packed reticulocyte yields of >12ml post leukofiltration1. The final preparations for a first in man clinical trial of adult cultured reticulocytes produced under good manufacturing practice (RESTORE) are underway. Although we have shown that it is possible to modify the CD34+ derived cells using lentivirus for reengineering or additions to the medium, the finite proliferative capacity of CD34+ cells in culture currently limits yield. We therefore took the alternative approach of immortalising early erythroid cells differentiated from adult bone marrow (BM) CD34+ cells, creating the BEL-A (Bristol Erythroid Line Adult) line2, a sustainable erythroid cell source that recapitulates normal adult erythropoiesis, terminally differentiating to generate enucleated reticulocytes that express normal levels of adult globin. We have created a further 13 lines from BM, adult peripheral blood, CB and iPSC CD34+ cells, demonstrating reproducibility of the approach and its application to create lines from more accessible stem cell sources. Analysis of surface marker and globin profiles demonstrate the lines follow a similar differentiation profile to their respective primary cell source, with comparative proteomics confirming cell source representation of the lines. Lines always established at the pro-erythroblast/early basophilic stage, even when later stage erythroid cells were present in populations. As well as proof of principal as an alternative transfusion product and improved tools for studying erythropoiesis, such lines have far reaching additional applications, a number of which we are now exploring: Diagnostic and 'Universal' transfusion products: Presently serological testing by blood group reference laboratories relies on donated blood, which represent a finite resource and for some blood group phenotypes can be difficult to source. We used CRISPR-Cas9 gene editing to remove blood group antigens in order to generate a sustainable bank of cell lines with useful blood group phenotypes for diagnostic purposes3. Building on this, with the aim of developing a more compatible "universal" transfusion product to meet the needs of chronically transfused patients and those with rare blood group phenotypes, we used combinatorial gene targeting to create sublines deficient in multiple antigens responsible for the most common transfusion incompatibilities (ABO [Bombay], Rh [Rhnull], Kell [K0], Duffy [Fynull], GPB [S-s-U-]). Individual and multiple blood group knockout lines retained the ability to undergo terminal differentiation and enucleation, also illustrating the capacity for coexistence of multiple rare blood group phenotypes within viable reticulocytes3. Cytokine independent lines Cytokines represent a substantial cost contribution to erythroid culture systems. We therefore exploited activating mutations found in patient c-Kit and EPOR that cause hypersensitivity to ligand, to create cytokine independent lines thus increasing economic viability of cultured red cells. Bi-allelic EPOR or c-kit edits were introduced into BEL-A with confirmation and exploration of mechanism on differentiation in the absence, or with substantially reduced levels of cytokines. Model disease systems In addition to potential therapeutic applications we are also creating lines as model cellular disease systems for studying molecular mechanisms and as drug screening platforms, via CRISPR-Cas9 gene editing of BEL-A and by directly immortalising patient stem cells. To date we have made b-thalassemia major, HbE thalassemia and lines with KLF1 mutations. Furthermore, we have shown BEL-A reticulocytes support invasion and growth of Plasmodium falciparum and are utilising the line to study mechanisms of malaria parasite invasion4. Kupzig S, Parsons SF, Curnow E, Anstee DJ, Blair A. Superior survival of ex vivo cultured human reticulocytes following transfusion into mice. 2016;102:476-483Trakarnsanga K, Griffiths RE, Wilson MC, et al. An immortalized adult human erythroid line facilitates sustainable and scalable generation of functional red cells. Nat. Commun. 2017;8:14750Hawksworth J, Satchwell TJ, Meinders M, et al. Enhancement of red blood cell transfusion compatibility using CRISPR-mediated erythroblast gene editing. EMBO Mol. Med. 2018; 10:e8454Satchwell TJ, Wright K, Haydn-Smith K, et al. Genetic manipulation of cell line derived reticulocytes enables dissection of host malaria invasion requirements. Nat. Comm. 2019;10:3806 Disclosures No relevant conflicts of interest to declare.

Published

2019

10. Superior survival of

Author

Sabine, Kupzig, Stephen F, Parsons, Elinor, Curnow, David J, Anstee, and Allison, Blair

Subjects

Erythrocytes, Reticulocytes, Cell Survival, Macrophages, Transplantation, Heterologous, Antigens, CD34, Blood Component Transfusion, Cell Differentiation, Articles, Hematopoietic Stem Cells, Immunophenotyping, Mice, Phenotype, Cytophagocytosis, Animals, Humans, Blood Transfusion, Cells, Cultured

Abstract

The generation of cultured red blood cells from stem cell sources may fill an unmet clinical need for transfusion-dependent patients, particularly in countries that lack a sufficient and safe blood supply. Cultured red blood cells were generated from human CD34+ cells from adult peripheral blood or cord blood by ex vivo expansion, and a comprehensive in vivo survival comparison with standard red cell concentrates was undertaken. Significant amplification (>105-fold) was achieved using CD34+ cells from both cord blood and peripheral blood, generating high yields of enucleated cultured red blood cells. Following transfusion, higher levels of cultured red cells could be detected in the murine circulation compared to standard adult red cells. The proportions of cultured blood cells from cord or peripheral blood sources remained high 24 hours post-transfusion (82±5% and 78±9%, respectively), while standard adult blood cells declined rapidly to only 49±9% by this time. In addition, the survival time of cultured blood cells in mice was longer than that of standard adult red cells. A paired comparison of cultured blood cells and standard adult red blood cells from the same donor confirmed the enhanced in vivo survival capacity of the cultured cells. The study herein represents the first demonstration that ex vivo generated cultured red blood cells survive longer than donor red cells using an in vivo model that more closely mimics clinical transfusion. Cultured red blood cells may offer advantages for transfusion-dependent patients by reducing the number of transfusions required.

Published

2016

11. The Ability of GAP1IP4BP To Function as a Rap1 GTPase-Activating Protein (GAP) Requires Its Ras GAP-Related Domain and an Arginine Finger Rather than an Asparagine Thumb

Author

Peter J. Cullen, Richard B. Sessions, Dalila Bouyoucef-Cherchalli, Sabine Kupzig, and Sam Yarwood

Subjects

Models, Molecular, endocrine system, GTPase-activating protein, Arginine, Recombinant Fusion Proteins, Molecular Sequence Data, Receptors, Cytoplasmic and Nuclear, GTPase, In Vitro Techniques, Humans, Bruton's tyrosine kinase, Amino Acid Sequence, Asparagine, Binding site, Molecular Biology, Peptide sequence, DNA Primers, Binding Sites, Base Sequence, Sequence Homology, Amino Acid, biology, GTPase-Activating Proteins, Articles, Cell Biology, Protein Structure, Tertiary, Amino Acid Substitution, Biochemistry, Mutagenesis, Site-Directed, biology.protein, Biophysics, Rap1

Abstract

GAP1(IP4BP) is a member of the GAP1 family of Ras GTPase-activating proteins (GAPs) that includes GAP1(m), CAPRI, and RASAL. Composed of a central Ras GAP-related domain (RasGRD), surrounded by amino-terminal C2 domains and a carboxy-terminal PH/Btk domain, these proteins, with the notable exception of GAP1(m), possess an unexpected arginine finger-dependent GAP activity on the Ras-related protein Rap1 (S. Kupzig, D. Deaconescu, D. Bouyoucef, S. A. Walker, Q. Liu, C. L. Polte, O. Daumke, T. Ishizaki, P. J. Lockyer, A. Wittinghofer, and P. J. Cullen, J. Biol. Chem. 281:9891-9900, 2006). Here, we have examined the mechanism through which GAP1(IP4BP) can function as a Rap1 GAP. We show that deletion of domains on either side of the RasGRD, while not affecting Ras GAP activity, do dramatically perturb Rap1 GAP activity. By utilizing GAP1(IP4BP)/GAP1(m) chimeras, we establish that although the C2 and PH/Btk domains are required to stabilize the RasGRD, it is this domain which contains the catalytic machinery required for Rap1 GAP activity. Finally, a key residue in Rap1-specific GAPs is a catalytic asparagine, the so-called asparagine thumb. By generating a molecular model describing the predicted Rap1-binding site in the RasGRD of GAP1(IP4BP), we show that mutagenesis of individual asparagine or glutamine residues that lie in close proximity to the predicted binding site has no detectable effect on the in vivo Rap1 GAP activity of GAP1(IP4BP). In contrast, we present evidence consistent with a model in which the RasGRD of GAP1(IP4BP) functions to stabilize the switch II region of Rap1, allowing stabilization of the transition state during GTP hydrolysis initiated by the arginine finger.

Published

2009

12. The GAP1 family of GTPase-activating proteins: spatial and temporal regulators of small GTPase signalling

Author

Sabine Kupzig, Dalila Bouyoucef-Cherchalli, Peter J. Cullen, and Sam Yarwood

Subjects

GTPase-activating protein, Biology, Biochemistry, GTP Phosphohydrolases, Cell biology, GTP-binding protein regulators, Cdc42 GTP-Binding Protein, ras GTPase-Activating Proteins, Anti-apoptotic Ras signalling cascade, Humans, RNA Interference, Small GTPase, HRAS, RNA, Small Interfering, Signal transduction, cdc42 GTP-Binding Protein, Signal Transduction, Calcium signaling

Abstract

Ras proteins are binary switches that, by cycling between inactive GDP-bound and active GTP-bound conformations, regulate multiple cellular signalling pathways including those that control cell growth, differentiation and survival. Approximately 30% of all human tumours express Ras-containing oncogenic mutations that lock the protein into a constitutively active conformation. The activation status of Ras is regulated by two groups of proteins: GEFs (guanine nucleotide-exchange factors) bind to Ras and enhance the exchange of GDP for GTP, thereby activating it, whereas GAPs (GTPase-activating proteins) inactivate Ras by binding to the GTP-bound form and enhancing the hydrolysis of the bound nucleotide back to GDP. In this review, we focus on a group of key regulators of Ras inactivation, the GAP1 family of Ras-GAPs. The members of this family are GAP1m, GAP1IP4BP, CAPRI (Ca2+-promoted Ras inactivator) and RASAL (Ras-GTPase-activating-like protein) and, as we will discuss, they are emerging as important modulators of Ras and small GTPase signalling that are subject to regulation by a diverse array of events and second messenger signals.

Published

2006

13. The frequencies of calcium oscillations are optimized for efficient calcium-mediated activation of Ras and the ERK/MAPK cascade

Author

Sabine Kupzig, Simon Walker, and Peter J. Cullen

Subjects

MAPK/ERK pathway, Benzylamines, Cell signaling, Blotting, Western, chemistry.chemical_element, Calcium-Calmodulin-Dependent Protein Kinase Kinase, Protein Serine-Threonine Kinases, Calcium, Biology, Anti-apoptotic Ras signalling cascade, Nitriles, Butadienes, Extracellular, Humans, Calcium Signaling, Extracellular Signal-Regulated MAP Kinases, Protein kinase A, Receptor, Glutathione Transferase, Sulfonamides, Multidisciplinary, Kinase, Biological Sciences, Isoquinolines, Cell biology, Enzyme Activation, Naphthalimides, chemistry, Calcium-Calmodulin-Dependent Protein Kinases, ras Proteins, Benzimidazoles, Electrophoresis, Polyacrylamide Gel, ras Guanine Nucleotide Exchange Factors, Calcium-Calmodulin-Dependent Protein Kinase Type 2, HeLa Cells, Signal Transduction

Abstract

Ras proteins are binary switches that, by cycling through inactive GDP- and active GTP-bound conformations, regulate multiple cellular signaling pathways, including those that control growth and differentiation. For some time, it has been known that receptor-mediated increases in the concentration of intracellular free calcium ([Ca 2+ ] i ) can modulate Ras activation. Increases in [Ca 2+ ] i often occur as repetitive Ca 2+ spikes or oscillations. Induced by electrical or receptor stimuli, these repetitive Ca 2+ oscillations increase in frequency with the amplitude of receptor stimuli, a phenomenon critical for the induction of selective cellular functions. Here, we show that Ca 2+ oscillations are optimized for Ca 2+ -mediated activation of Ras and signaling through the extracellular signal-regulated kinase (ERK)/mitogen-activated protein kinase (MAPK) cascade. We present additional evidence that Ca 2+ oscillations reduce the effective Ca 2+ threshold for the activation of Ras and that the oscillatory frequency is optimized for activation of Ras and the ERK/MAPK pathway. Our results describe a hitherto unrecognized link between complex Ca 2+ signals and the modulation of the Ras/ERK/MAPK signaling cascade.

Published

2005

14. Identification of a Ras GTPase-activating protein regulated by receptor-mediated Ca2+ oscillations

Author

Sabine Kupzig, Takashi Tsuboi, Trever G. Bivona, Peter J. Lockyer, Louise C Davies, Maxine J. Allen, Gyles E. Cozier, Guy A. Rutter, Peter J. Cullen, Simon Walker, Alan Buckler, Dalila Bouyoucef, and Mark R. Philips

Subjects

GTPase-activating protein, Molecular Sequence Data, Phosphatidylserines, Plasma protein binding, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Cell Line, Cell membrane, Enzyme activator, Chlorocebus aethiops, medicine, Animals, Humans, Amino Acid Sequence, Calcium Signaling, RNA, Small Interfering, Receptor, Molecular Biology, Calcium signaling, General Immunology and Microbiology, General Neuroscience, Cell Membrane, Receptor-mediated endocytosis, Protein Structure, Tertiary, Transport protein, Cell biology, Electrophysiology, Enzyme Activation, Protein Transport, medicine.anatomical_structure, Biochemistry, ras GTPase-Activating Proteins, Liposomes, Phosphatidylcholines, ras Proteins, Calcium, Sequence Alignment, Protein Binding

Abstract

Receptor-mediated increases in the concentration of intracellular free calcium ([Ca2+]i) are responsible for controlling a plethora of physiological processes including gene expression, secretion, contraction, proliferation, neural signalling, and learning. Increases in [Ca2+]i often occur as repetitive Ca2+ spikes or oscillations. Induced by electrical or receptor stimuli, these repetitive Ca2+ spikes increase their frequency with the amplitude of the receptor stimuli, a phenomenon that appears critical for the induction of selective cellular functions. Here we report the characterisation of RASAL, a Ras GTPase-activating protein that senses the frequency of repetitive Ca2+ spikes by undergoing synchronous oscillatory associations with the plasma membrane. Importantly, we show that only during periods of plasma membrane association does RASAL inactivate Ras signalling. Thus, RASAL senses the frequency of complex Ca2+ signals, decoding them through a regulation of the activation state of Ras. Our data provide a hitherto unrecognised link between complex Ca2+ signals and the regulation of Ras.

Published

2004

15. Bst-2/HM1.24 Is a Raft-Associated Apical Membrane Protein with an Unusual Topology

Author

Sabine Kupzig, Anna Sugden, Andrew Wilde, Ruth Rollason, George Banting, and Viktor I. Korolchuk

Subjects

Vesicle-associated membrane protein 8, biology, Peripheral membrane protein, Cell Biology, Apical membrane, Topology, Biochemistry, Cell biology, Transmembrane domain, Membrane glycoproteins, Membrane protein, Structural Biology, Genetics, biology.protein, Molecular Biology, Integral membrane protein, Lipid raft

Abstract

An expression screen of a rat cDNA library for sequences encoding Golgi-localized integral membrane proteins identified a protein with an apparent novel topology, i.e. with both an N-terminal transmembrane domain and a C-terminal glycosyl-phosphatidylinositol (GPI) anchor. Our data are consistent with this. Thus, the protein would have a topology that, in mammalian cells, is shared only by a minor, but pathologically important, topological isoform of the prion protein (PrP). The human orthologue of this protein has been described previously (BST-2 or HM1.24 antigen) as a cell surface molecule that appears to be involved in early pre-B-cell development and which is present at elevated levels at the surface of myeloma cells. We show that rat BST-2/HM1.24 has both a cell surface and an intracellular (juxtanuclear) location and is efficiently internalized from the cell surface. We also show that the cell surface pool of BST-2/HM1.24 is predominantly present in the apical plasma membrane of polarized cells. The fact that rat BST-2/HM1.24 apparently possesses a GPI anchor led us to speculate that it might exist in cholesterol-rich lipid microdomains (lipid rafts) at the plasma membrane. Data from several experiments are consistent with this localization. We present a model in which BST-2/HM1.24 serves to link adjacent lipid rafts within the plasma membrane.

Published

2003

16. Identification of the Ras GTPase-activating protein GAP1m as a phosphatidylinositol-3,4,5-trisphosphate-binding protein in vivo

Author

Peter J. Lockyer, Stefan Wennström, Kanamarlapudi Venkateswarlu, Julian Downward, Sabine Kupzig, and Peter J. Cullen

Subjects

GTPase-activating protein, Recombinant Fusion Proteins, Biology, PC12 Cells, General Biochemistry, Genetics and Molecular Biology, Phosphatidylinositol 3-Kinases, chemistry.chemical_compound, Phosphatidylinositol Phosphates, Epidermal growth factor, Animals, Inositol, Phosphatidylinositol, Phosphoinositide-3 Kinase Inhibitors, Agricultural and Biological Sciences(all), Biochemistry, Genetics and Molecular Biology(all), Phosphatidylinositol (3,4,5)-trisphosphate, Binding protein, Proteins, Molecular biology, Rats, Cell biology, Pleckstrin homology domain, chemistry, ras GTPase-Activating Proteins, COS Cells, Second messenger system, ras Proteins, General Agricultural and Biological Sciences

Abstract

GAP1(m) is a member of the GAP1 family of Ras GTPase-activating proteins (GAPs) [1]. In vitro, it has been shown to bind inositol 1, 3,4,5-tetrakisphosphate (IP4), the water-soluble inositol head group of the lipid second messenger phosphatidylinositol 3,4, 5-trisphosphate (PIP3) [2] [3]. This has led to the suggestion that GAP1(m) might function as a PIP3 receptor in vivo [4]. Here, using rat pheochromocytoma PC12 cells transiently transfected with a plasmid expressing a chimera of green fluorescent protein fused to GAP1(m) (GFP-GAP1(m)), we show that epidermal growth factor (EGF) induces a rapid (less than 60 seconds) recruitment of GFP-GAP1(m) from the cytosol to the plasma membrane. This recruitment required a functional GAP1(m) pleckstrin homology (PH) domain, because a specific point mutation (R629C) in the PH domain that inhibits IP4 binding in vitro [5] totally blocked EGF-induced GAP1(m) translocation. Furthermore, the membrane translocation was dependent on PI 3-kinase, and the time course of translocation paralleled the rate by which EGF stimulates the generation of plasma membrane PIP3 [6]. Significantly, the PIP3-induced recruitment of GAP1(m) did not appear to result in any detectable enhancement in its basal Ras GAP activity. From these results, we conclude that GAP1(m) binds PIP3 in vivo, and it is recruited to the plasma membrane, but does not appear to be activated, following agonist stimulation of PI 3-kinase.

Published

1999

17. Maturing reticulocytes internalize plasma membrane in glycophorin A-containing vesicles that fuse with autophagosomes before exocytosis

Author

Jon D. Lane, Kongtana Trakarnsanga, Rebecca E. Griffiths, David J. Anstee, Nicola Cogan, Tosti J. Mankelow, Stephen F. Parsons, Sabine Kupzig, Virginie M S Betin, and Edwin Massey

Subjects

Adult, Erythrocytes, Reticulocytes, Immunology, Biochemistry, Membrane Fusion, Exocytosis, Cell membrane, Reticulocyte, Phagosomes, medicine, Glycophorin, Humans, Glycophorins, Transport Vesicles, Phagosome, Microscopy, Confocal, biology, Vesicle, Cell Membrane, Lipid bilayer fusion, Cell Differentiation, Cell Biology, Hematology, Autophagic Punctum, Cell biology, Oxygen, medicine.anatomical_structure, Membrane protein, biology.protein

Abstract

The maturation of reticulocytes into functional erythrocytes is a complex process requiring extensive cytoplasmic and plasma membrane remodeling, cytoskeletal rearrangements and changes to cellular architecture. Autophagy is implicated in the sequential removal of erythroid organelles during erythropoiesis, although how this is regulated during late stages of erythroid differentiation, and the potential contribution of autophagy during reticulocyte maturation, remain unclear. Using an optimized ex vivo differentiation system for human erythropoiesis, we have observed that maturing reticulocytes are characterized by the presence of one or few large vacuolar compartments. These label strongly for glycophorin A (GYPA/GPA) which is internalized from the plasma membrane; however, they also contain organellar remnants (ER, Golgi, mitochondria) and stain strongly for LC3, suggesting that they are endocytic/autophagic hybrid structures. Interestingly, we observed the release of these vacuoles by exocytosis in maturing reticulocytes, and speculate that autophagy is needed to concentrate the final remnants of the reticulocyte endomembrane system in autophagosome/endosome hybrid compartments that are primed to undergo exocytosis.

Published

2012

18. Critical band 3 multiprotein complex interactions establish early during human erythropoiesis

Author

Ashley M. Toye, Emile van den Akker, Stephanie Pellegrin, Sabine Kupzig, Kay Ridgwell, David J. Anstee, Geoff Daniels, Amanda J. Bell, and Timothy J. Satchwell

Subjects

Erythrocytes, Multiprotein complex, Reticulocytes, Erythroblasts, Immunology, Golgi Apparatus, Endoplasmic Reticulum, Biochemistry, Article, Reticulocyte, Erythroblast, Anion Exchange Protein 1, Erythrocyte, medicine, Humans, Erythropoiesis, RNA, Small Interfering, Band 3, Membrane Glycoproteins, biology, Erythrocyte Membrane, Membrane Proteins, Anemia, Cell Differentiation, Cell Biology, Hematology, Blood Proteins, Transport protein, Cell biology, Cytoskeletal Proteins, medicine.anatomical_structure, Multiprotein Complexes, RHAG, biology.protein, Basophilic Erythroblast, Peptide Hydrolases, Protein Binding

Abstract

Band 3, the major anion transport protein of human erythrocytes, forms the core of a multiprotein complex in the erythrocyte membrane. Here we studied the spatiotemporal mechanisms of band 3 multiprotein complex assembly during erythropoiesis. Significant pools of intracellular band 3 and Rh-associated glycoprotein (RhAG) were found in the basophilic erythroblast. These intracellular pools decreased in the polychromatic erythroblast, whereas surface expression increased and were lowest in the orthochromatic erythroblast and reticulocytes. Protease treatment of intact cells to remove extracellular epitopes recognized by antibodies to band 3 and RhAG was used to study surface delivery kinetics and intracellular complex composition from the proerythroblast stage to the enucleated reticulocyte. Newly synthesized band 3 and protein 4.2 interact initially in the early stages of the secretory pathway and are found associated at the plasma membrane from the basophilic stage of erythropoiesis. Although we could successfully coimmunoprecipitate Rh with RhAG from plasma membrane pools at a similar stage, no intracellular interaction between these proteins was detectable. Knockdown of RhAG during early erythropoiesis was accompanied by a concomitant drop in membrane expression of Rh polypeptides. These data are consistent with assembly of major components of the band 3 macrocomplex at an early stage during erythropoiesis.

Published

2011

19. Epigenetic silencing of a Ca(2+)-regulated Ras GTPase-activating protein RASAL defines a new mechanism of Ras activation in human cancers

Author

Jianming Ying, Xian Wang, Qian Zhang, Hongchuan Jin, Zhong Ying Shen, Jie Jin, Qian Tao, Ada H.Y. Wong, Yan Cui, Gopesh Srivastava, Anthony T.C. Chan, En Min Li, Peter J. Cullen, and Sabine Kupzig

Subjects

GTPase-activating protein, Tumor suppressor gene, Ras Proteins - Metabolism, Down-Regulation, GTPase, Biology, medicine.disease_cause, Methylation, Anti-apoptotic Ras signalling cascade, Cell Line, Tumor, Neoplasms, Chromosomes, Human, Pair 12 - Genetics, medicine, Gene silencing, Humans, Gene Silencing, Multidisciplinary, Chromosomes, Human, Pair 12, Oncogene, Ras Gtpase-Activating Proteins - Genetics - Metabolism, Biological Sciences, Cell biology, Enzyme Activation, Gene Expression Regulation, Neoplastic, Neoplasms - Genetics - Metabolism - Pathology, Phenotype, ras GTPase-Activating Proteins, DNA methylation, ras Proteins, Calcium, CpG Islands, Calcium - Metabolism, Carcinogenesis

Abstract

Ras has achieved notoriety as an oncogene aberrantly activated in multiple human tumors. Approximately 30% of all human tumors express an oncogenic form of this GTPase that is locked in an active conformation as a result of being insensitive to Ras GTPase-activating proteins (GAPs), proteins that normally regulate the inactivation of Ras by enhancing its intrinsic GTPase activity. Besides oncogenic mutations in Ras, signaling by wild-type Ras is also frequently deregulated in tumors through aberrant coupling to activated cell surface receptors. This indicates that alternative mechanisms of aberrant wild-type Ras activation may be involved in tumorigenesis. Here, we describe another mechanism through which aberrant Ras activation is achieved in human cancers. We have established that Ras GTPase-activating-like protein (RASAL), a Ca 2+-regulated Ras GAP that decodes the frequency of Ca 2+ oscillations, is silenced through CpG methylation in multiple tumors. With the finding that ectopic expression of catalytically active RASAL leads to growth inhibition of these tumor cells by Ras inactivation, we have provided evidence that epigenetically silencing of this Ras GAP represents a mechanism of aberrant Ras activation in certain cancers. Our demonstration that RASAL constitutes a tumor suppressor gene has therefore further emphasized the importance of Ca 2+ in the regulation of Ras signaling and has established that deregulation of this pathway is an important step in Ras-mediated tumorigenesis. © 2007 by The National Academy of Sciences of the USA., link_to_OA_fulltext

Published

2007

20. Studying the spatial and temporal regulation of Ras GTPase-activating proteins

Author

Sabine, Kupzig, Dalila, Bouyoucef, Gyles E, Cozier, and Peter J, Cullen

Subjects

Gene Expression Regulation, ras GTPase-Activating Proteins, Recombinant Fusion Proteins, Liposomes, Guanine Nucleotide Exchange Factors, Humans, raf Kinases, Glutathione Transferase, HeLa Cells

Abstract

Two classes of proteins govern Ras activation. Guanine-nucleotide exchange factors (Ras GEFs) catalyze the activation of Ras by inducing the dissociation of GDP to allow association of the more abundant GTP, whereas GTPase-activating proteins (Ras GAPs), bind to the GTP-bound form and, by enhancing the intrinsic GTPase activity, catalyze Ras inactivation. A wide range of Ras GEFs and Ras GAPs have been identified from the various genome projects, and in a few instances, the mechanisms by which signals originating from activated receptors converge on specific GEFs and GAPs have been mapped. However, for most Ras GEFs and GAPs we have a poor understanding of their regulation. Here we focus on describing methods used to study the regulation of the GAP1 family of Ras GAPs. In particular, we emphasize how by combining biochemical, molecular, and imaging techniques, one can determine some of the complex array of mechanisms that have evolved to modulate the spatial and temporal dynamics of Ras regulation through these various Ras GAPs. By combining biochemical, molecular, and imaging techniques, we describe the visualization of the diverse and dynamic mechanisms through which stimulation of cell surface receptors leads to the regulation of these proteins. Thus, although each member of the GAP1 family performs the same basic biological function, that is, they function as Ras GAPs, each is designed to respond and decode signals from distinct second messenger pathways.

Published

2006

21. Studying the Spatial and Temporal Regulation of Ras GTPase‐Activating Proteins

Author

Gyles E. Cozier, Dalila Bouyoucef, Sabine Kupzig, and Peter J. Cullen

Subjects

GTP', Cell surface receptor, Ras GTPase-Activating Proteins, Second messenger system, GTPase, Biology, Receptor, Function (biology), Cell biology

Abstract

Two classes of proteins govern Ras activation. Guanine‐nucleotide exchange factors (Ras GEFs) catalyze the activation of Ras by inducing the dissociation of GDP to allow association of the more abundant GTP, whereas GTPase‐activating proteins (Ras GAPs), bind to the GTP‐bound form and, by enhancing the intrinsic GTPase activity, catalyze Ras inactivation. A wide range of Ras GEFs and Ras GAPs have been identified from the various genome projects, and in a few instances, the mechanisms by which signals originating from activated receptors converge on specific GEFs and GAPs have been mapped. However, for most Ras GEFs and GAPs we have a poor understanding of their regulation. Here we focus on describing methods used to study the regulation of the GAP1 family of Ras GAPs. In particular, we emphasize how by combining biochemical, molecular, and imaging techniques, one can determine some of the complex array of mechanisms that have evolved to modulate the spatial and temporal dynamics of Ras regulation through these various Ras GAPs. By combining biochemical, molecular, and imaging techniques, we describe the visualization of the diverse and dynamic mechanisms through which stimulation of cell surface receptors leads to the regulation of these proteins. Thus, although each member of the GAP1 family performs the same basic biological function, that is, they function as Ras GAPs, each is designed to respond and decode signals from distinct second messenger pathways.

Published

2006

22. Analyzing the role of the putative inositol 1,3,4,5-tetrakisphosphate receptor GAP1IP4BP in intracellular Ca2+ homeostasis

Author

Peter J. Lockyer, Dorit Zharhary, Sabine Kupzig, Simon Walker, Sara Bilu, and Peter J. Cullen

Subjects

Small interfering RNA, Oligonucleotides, Receptors, Cytoplasmic and Nuclear, Stimulation, Endogeny, Phospholipase, Biology, Biochemistry, chemistry.chemical_compound, Homeostasis, Humans, Inositol, Calcium Signaling, Receptor, Molecular Biology, Base Sequence, Cell Biology, Recombinant Proteins, Cell biology, chemistry, ras GTPase-Activating Proteins, Calcium, Intracellular, Histamine, HeLa Cells

Abstract

Inositol 1,3,4,5-tetrakisphosphate (IP(4)) has been linked to a potential role in the regulation of intracellular free Ca(2+) concentration ([Ca(2+)](i)) following cellular stimulation with agonists that activate phosphoinositide-specific phospholipase C. However, despite many studies, the function of IP(4) remains unclear and indeed there is still some debate over whether it has a function at all. Here we have used various molecular approaches to address whether manipulation of the potential IP(4) receptor, GAP1(IP4BP), affects [Ca(2+)](i) following cellular stimulation. Using single cell imaging, we show that the overexpression of a constitutively active and a potential dominant negative form of GAP1(IP4BP) appear to have no effect on Ca(2+) mobilization or Ca(2+) entry following stimulation of HeLa cells with histamine. In addition, through the use of small interfering RNA duplexes, we have examined the effect of suppressing endogenous GAP1(IP4BP) production on [Ca(2+)](i). In HeLa cells in which the endogenous level of GAP1(IP4BP) has been suppressed by approximately 95%, we failed to observe any effect on Ca(2+) mobilization or Ca(2+) entry following histamine stimulation. Thus, using various approaches to manipulate the function of endogenous GAP1(IP4BP) in intact HeLa cells, we have been unable to observe any detectable effect of GAP1(IP4BP) on [Ca(2+)](i).

Published

2002

23. A Robust Ex Vivo culture System for Production of Mature Human Reticulocytes From a Single Donor

Author

David J. Anstee, Steve F. Parsons, Nicola Cogan, and Sabine Kupzig

Subjects

medicine.medical_specialty, Pathology, Hematology, Red Cell, Immunology, Cell, CD34, Cell Biology, Biology, Biochemistry, Molecular biology, medicine.anatomical_structure, Internal medicine, medicine, Erythropoiesis, Transfusion therapy, Progenitor cell, Ex vivo

Abstract

Abstract 2096 We have formulated a robust culture system simulating human erythropoiesis, producing mature reticulocytes from adult peripheral blood CD34+ progenitor cells in 20 days. Expansion of cell numbers over the course of the culture exceeded 104-fold and enucleation efficiency was up to 90% without the use of feeder layers. Mature reticulocytes and erythrocytes were isolated from culture by passage through a standard leucocyte filter. Scanning and transmission electron microscopy of the reticulocytes revealed morphological features indistinguishable from those of mature reticulocytes isolated from the peripheral blood of normal donors. Post-filtration cells expressed adult haemoglobin and had a capacity to bind and release oxygen comparable to that of adult peripheral blood erythrocytes. Examination of blood group active- and other cell surface antigens revealed a normal glycosylation profile and normal cell surface protein expression. Most notably, the cells did not express cryptantigens T and Tn. LORCA analysis indicated that cultured cells had slightly reduced membrane stability and deformability compared to peripheral blood erythrocytes. Haematology parameters demonstrated a typical mean cell volume of 131fL and mean cell haemoglobin of 37.7pg. This, scalable approach has allowed us to culture cells from a single apheresis cone to produce 1010 reticulocytes, which represents a packed cell volume of 1ml. These results clearly demonstrate the feasibility of producing cultured red cell products suitable for transfusion therapy ex vivo from adult peripheral blood stem cells. Disclosures: No relevant conflicts of interest to declare.

Published

2011

24. Plasma Membrane Loss in Maturing Human Reticulocytes Occurs Through Endocytosis of Large Glycophorin A- Containing Vacuoles Which Fuse with Autophagosomes Before Exocytosis

Author

Jon D. Lane, Virginie M S Betin, Rebecca E. Griffiths, Steve F. Parsons, David J. Anstee, Nicola Cogan, Sabine Kupzig, and Tosti J. Mankelow

Subjects

CD98, biology, Chemistry, Immunology, Cell Biology, Hematology, Vacuole, Endocytosis, Biochemistry, Exocytosis, Cell biology, medicine.anatomical_structure, Reticulocyte, Membrane protein, Organelle, medicine, biology.protein, Glycophorin

Abstract

Abstract 177 The erythrocyte is one of the best characterized human cells. However, studies of the process whereby human reticulocytes mature to erythrocytes have been hampered by the difficulty of obtaining sufficient numbers of cells for analysis. We have developed an in vitro culture system permitting the production of millilitre quantities of functional mature human adult reticulocytes from peripheral blood CD34+ cells. Analysis of reticulocytes obtained from culture using confocal microscopy on permeabilized cells reveals that the final stage of reticulocyte maturation occurs by a previously undescribed mechanism in which large Glycophorin A-containing vacuoles forming at the cytosolic face of the plasma membrane are internalised and fuse with autophagosomes (defined by reactivity with anti-LC3) before expulsion from the cell. Our results constitute the first demonstration of linkage between plasma membrane remodelling and autophagy, and suggest reticulocyte plasma membrane remodelling occurs in two stages. Early maturation is characterized by the selective elimination of unwanted plasma membrane proteins (CD71, CD98, β1 integrin) through the endosome-exosome pathway. In contrast, final maturation is characterized by the generation and expulsion of large Glycophorin A-decorated vacuoles of autophagic origin, thereby simultaneously permitting optimisation of membrane:skeleton interactions to yield the more stable and deformable membrane of mature erythrocytes and eliminating unwanted residual organelles. Disclosures: No relevant conflicts of interest to declare.

Published

2011

25. PI 3-kinase effector molecules

Author

Peter J. Cullen, Kanamarlapudi Venkateswarlu, Sabine Kupzig, Gyles E. Cozier, Louise Wheeler, Jon S. Reynolds, and Peter J. Lockyer

Subjects

Effector, Chemistry, Molecule, Biochemistry, Pi 3 kinase, Cell biology

Published

1999

26. Identification of the Ras GTPase-activating protein GAP1m as an in vivo phosphatidylinositol 3,4,5-trisphosphate-binding protein

Author

Julian Downward, Stefan Wennström, Kanamarlapudi Venkateswarlu, Peter J. Lockyer, Sabine Kupzig, and Peter J. Cullen

Subjects

Pleckstrin homology domain, chemistry.chemical_compound, chemistry, GTPase-activating protein, Phosphatidylinositol (3,4,5)-trisphosphate, Binding protein, NCK1, Autophagy-related protein 13, Biochemistry, SH3 domain, Cell biology, Phosphoinositide-dependent kinase-1

Published

1999

27. CAPRI regulates Ca2+-dependent inactivation of the Ras-MAPK pathway

Author

Peter J. Lockyer, Sabine Kupzig, and Peter J. Cullen

Subjects

MAP Kinase Signaling System, Recombinant Fusion Proteins, Immunoblotting, Molecular Sequence Data, Biology, General Biochemistry, Genetics and Molecular Biology, Culture Media, Serum-Free, Cell Line, chemistry.chemical_compound, Adenosine Triphosphate, Genes, Reporter, Animals, Humans, Amino Acid Sequence, Receptor, Agricultural and Biological Sciences(all), Ionophores, Biochemistry, Genetics and Molecular Biology(all), Kinase, Cell growth, Ionomycin, Cell biology, Protein Structure, Tertiary, chemistry, ras GTPase-Activating Proteins, Second messenger system, ras Proteins, Calcium, GTP Phosphohydrolase Activators, Guanine nucleotide exchange factor, General Agricultural and Biological Sciences, Tyrosine kinase, Adenosine triphosphate, Sequence Alignment, Histamine

Abstract

Ca2+ is a universal second messenger that is critical for cell growth and is intimately associated with many Ras-dependent cellular processes such as proliferation and differentiation [1]. Ras is a small GTP binding protein that operates as a molecular switch regulating the control of gene expression, cell growth, and differentiation through a pathway from receptors to mitogen-activated protein kinases (MAPKs) [2]. A role for intracellular Ca2+ in the activation of Ras has been previously demonstrated, e.g., via the nonreceptor tyrosine kinase PYK2 [3] and by Ca2+/calmodulin-dependent guanine nucleotide exchange factors (GEFs) such as Ras-GRF [4]; however, there is no Ca2+-dependent mechanism for direct inactivation. An important advance toward greater understanding of the complex coordination within the Ras-signaling network is the spatio-temporal analysis of signaling events in vivo. Here, we describe the identification of CAPRI (Ca2+-promoted Ras inactivator), a Ca2+-dependent Ras GTPase-activating protein (GAP) that switches off the Ras-MAPK pathway following a stimulus that elevates intracellular Ca2+. Analysis of the spatio-temporal dynamics of CAPRI indicates that Ca2+ regulates the GAP by a fast C2 domain-dependent translocation mechanism.

28. GAP1IP4BP contains a novel group I pleckstrin homology domain that directs constitutive plasma membrane association

Author

Sabine Kupzig, Peter J. Cullen, Thomas H. Millard, Joanna R. Bottomley, Peter J. Lockyer, George Banting, Gyles E. Cozier, and Jon S. Reynolds

Subjects

Sucrose, Inositol Phosphates, Recombinant Fusion Proteins, Receptors, Cytoplasmic and Nuclear, Transfection, Biochemistry, chemistry.chemical_compound, Phosphatidylinositol Phosphates, Animals, Humans, Inositol, Phosphatidylinositol, Binding site, Receptor, Molecular Biology, Cell Nucleus, Binding Sites, COS cells, Cell Membrane, Cell Biology, Pleckstrin homology domain, Cytosol, Amino Acid Substitution, chemistry, COS Cells, Liposomes, Mutagenesis, Site-Directed, HeLa Cells, Subcellular Fractions

Abstract

The group I family of pleckstrin homology (PH) domains are characterized by their inherent ability to specifically bind phosphatidylinositol 3,4,5-trisphosphate (PtdIns(3,4,5)P(3)) and its corresponding inositol head-group inositol 1,3,4,5-tetrakisphosphate (Ins(1,3,4,5)P(4)). In vivo this interaction results in the regulated plasma membrane recruitment of cytosolic group I PH domain-containing proteins following agonist-stimulated PtdIns(3,4,5)P(3) production. Among group I PH domain-containing proteins, the Ras GTPase-activating protein GAP1(IP4BP) is unique in being constitutively associated with the plasma membrane. Here we show that, although the GAP1(IP4BP) PH domain interacts with PtdIns(3,4, 5)P(3), it also binds, with a comparable affinity, phosphatidylinositol 4,5-bisphosphate (PtdIns(4,5)P(2)) (K(d) values of 0.5 +/- 0.2 and 0.8 +/- 0.5 microm, respectively). Intriguingly, whereas this binding site overlaps with that for Ins(1,3,4,5)P(4), consistent with the constitutive plasma membrane association of GAP1(IP4BP) resulting from its PH domain-binding PtdIns(4,5)P(2), we show that in vivo depletion of PtdIns(4,5)P(2), but not PtdIns(3,4,5)P(3), results in dissociation of GAP1(IP4BP) from this membrane. Thus, the Ins(1,3,4,5)P(4)-binding PH domain from GAP1(IP4BP) defines a novel class of group I PH domains that constitutively targets the protein to the plasma membrane and may allow GAP1(IP4BP) to be regulated in vivo by Ins(1,3,4,5)P(4) rather than PtdIns(3,4,5)P(3).