Your search keyword '"endoH, endoglycosidase H"' showing total 16 results

1. The IgGFc-binding protein FCGBP is secreted with all GDPH sequences cleaved but maintained by interfragment disulfide bonds

Author

Erik Ehrencrona, Christian V. Recktenwald, Sergio Trillo-Muyo, Malin Bäckström, Pablo Gallego, Malin Johansson, Maria-Jose Garcia-Bonete, Ana M. Rodríguez-Piñeiro, Sjoerd van der Post, and Gunnar C. Hansson

Subjects

0301 basic medicine, MUC5AC, mucin-5AC, MUC2, mucin-2 (Muc2, mouse), vWF, von Willebrand factor, Biochemistry, von Willebrand domain, chemistry.chemical_compound, PVDF, polyvinylidene difluoride, Mice, Cricetinae, Disulfides, Intestinal Mucosa, Peptide sequence, EndoH, endoglycosidase H, biology, Chemistry, respiratory system, GDPH, Gly-Asp-Pro-His, Chaotropic agent, WB, Western blot, Iodoacetamide, GuHCl, guanidinium chloride, Research Article, IgG, immunoglobulin G, vWD, von Willebrand D domain, CHO Cells, CHO, Chinese hamster ovary, 03 medical and health sciences, Endoglycosidase H, Cricetulus, Protein Domains, mucus, von Willebrand Factor, Animals, Humans, intestinal epithelium, Molecular Biology, intestine, FCGBP, IgGFc-binding protein (Fcgbp, mouse), GAPH, Gly-Ala-Pro-His, Mucin-2, 030102 biochemistry & molecular biology, colon, Binding protein, Endoplasmic reticulum, Mucin, ITH3, inter-alpha-trypsin inhibitor heavy chain 3, Cell Biology, Mucus, Mice, Inbred C57BL, 030104 developmental biology, MUC2, Proteolysis, biology.protein, Immunoglobulin G (IgG), IAA, iodoacetamide, Cell Adhesion Molecules, disulfide

Abstract

Mucus forms an important protective barrier that minimizes bacterial contact with the colonic epithelium. Intestinal mucus is organized in a complex network with several specific proteins, including the mucin-2 (MUC2) and the abundant IgGFc-binding protein, FCGBP. FCGBP is expressed in all intestinal goblet cells and is secreted into the mucus. It is comprised of repeated von Willebrand D (vWD) domain assemblies, most of which have a GDPH amino acid sequence that can be autocatalytically cleaved, as previously observed in the mucins MUC2 and mucin-5AC. However, the functions of FCGBP in the mucus are not understood. We show that all vWD domains of FCGBP with a GDPH sequence are cleaved and that these cleavages occur early during biosynthesis in the endoplasmic reticulum. All cleaved fragments, however, remain connected via a disulfide bond within each vWD domain. This cleavage generates a C-terminal-reactive Asp-anhydride that could react with other molecules, such as MUC2, but this was not observed. Quantitative analyses by MS showed that FCGBP was mainly soluble in chaotropic solutions, whereas MUC2 was insoluble, and most of the secreted FCGBP was not covalently bound to MUC2. Although FCGBP has been suggested to bind immunoglobulin G, we were unable to reproduce this binding in vitro using purified proteins. In conclusion, while the function of FCGBP is still unknown, our results suggest that it does not contribute to covalent crosslinking in the mucus, nor incorporate immunoglobulin G into mucus, instead the single disulfide bond linking each fragment could mediate controlled dissociation.

Published

2021

2. PCSK9 is not secreted from mature differentiated intestinal cells

Author

Melissa Touvron, Cédric Le May, Thibaud Sotin, Xavier Prieur, L. Arnaud, Annik Prat, Anna Roubtsova, Claire Blanchard, Nabil G. Seidah, Wieneke Dijk, Audrey Ayer, Moreau François, Bertrand Cariou, Laurianne Van Landeghem, Gilliane Chadeuf, Damien Garçon, Aurélie Thedrez, Mikaël Croyal, Unité de recherche de l'institut du thorax (ITX-lab), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), Université de Nantes (UN)-Université de Nantes (UN), Université de Montréal (UdeM), Centre hospitalier universitaire de Nantes (CHU Nantes), North Carolina State University [Raleigh] (NC State), University of North Carolina System (UNC), Dijk, Wieneke, unité de recherche de l'institut du thorax UMR1087 UMR6291 (ITX), Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), Université de Nantes (UN)-Université de Nantes (UN)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Institut de Recherches Cliniques de Montréal (IRCM), and Le May, Cedric

Subjects

[SDV.MHEP.PHY] Life Sciences [q-bio]/Human health and pathology/Tissues and Organs [q-bio.TO], [SDV]Life Sciences [q-bio], 3′DGE, 3′ digital gene expression, Regulator, 030204 cardiovascular system & hematology, Biochemistry, Caco-2 cell, PCSK9, Mice, 0302 clinical medicine, Endocrinology, Intestine, Small, liver-specific knockout, Cells, Cultured, ComputingMilieux_MISCELLANEOUS, portal blood, Mice, Knockout, [SDV.MHEP.EM] Life Sciences [q-bio]/Human health and pathology/Endocrinology and metabolism, lipoprotein metabolism, 0303 health sciences, [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, medicine.diagnostic_test, Chemistry, Cell Differentiation, [SDV.MHEP.EM]Life Sciences [q-bio]/Human health and pathology/Endocrinology and metabolism, [SDV.MHEP.CSC] Life Sciences [q-bio]/Human health and pathology/Cardiology and cardiovascular system, Cell biology, [SDV] Life Sciences [q-bio], medicine.anatomical_structure, WB, Western blot, Kexin, Proprotein Convertase 9, Corrigendum, Research Article, DEGs, differentially expressed genes, Mice, Transgenic, QD415-436, Ussing chambers, endoH, endoglycosidase H, TICE, trans-intestinal cholesterol excretion, 03 medical and health sciences, Western blot, [SDV.MHEP.CSC]Life Sciences [q-bio]/Human health and pathology/Cardiology and cardiovascular system, medicine, [SDV.MHEP.PHY]Life Sciences [q-bio]/Human health and pathology/Tissues and Organs [q-bio.TO], [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology, Animals, Humans, Secretion, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, PCSK9 LivKO, mouse model lacking PCSK9 specifically in hepatocytes, intestine, 030304 developmental biology, PPL, postprandial lipemia, systemic blood, [SDV.MHEP.HEG]Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology, Cell Biology, Proprotein convertase, [SDV.MHEP.HEG] Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology, Small intestine, Mice, Inbred C57BL, LDL receptor, cholesterol metabolism, Caco-2 Cells, PCSK9, proprotein convertase subtilisin/kexin type 9, PNGase F, N-glycosidase F, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology

Abstract

International audience; Proprotein convertase subtilisin/kexin type 9 (PCSK9) promotes lysosomal degradation of the LDL receptor and is a key regulator of cholesterol metabolism. After the liver, the small intestine is the second organ that highly expresses PCSK9. However, the small intestine's ability to secrete PCSK9 remains a matter of debate. While liver-specific PCSK9-deficient mice present no PCSK9 in systemic blood, human intestinal Caco-2 cells can actively secrete PCSK9. This raises the possibility for active intestinal secretion via the portal blood. Here, we aimed to determine whether enterocytes can secrete PCSK9 using in vitro, ex vivo, and in vivo approaches. We first observed that PCSK9 secretion from Caco-2 cells was biphasic and dependent on Caco-2 maturation status. Transcriptional analysis suggested that this transient reduction in PCSK9 secretion might be due to loss of SREBP2-mediated transcription of PCSK9. Consistently, PCSK9 secretion was not detected ex vivo in human or mouse intestinal biopsies mounted in Ussing chambers. Finally, direct comparison of systemic versus portal blood PCSK9 concentrations in WT or liver-specific PCSK9-deficient mice confirmed the inability of the small intestine to secrete PCSK9 into the portal compartment. Altogether, our data demonstrate that mature enterocytes do not secrete PCSK9 and reinforce the central role of the liver in the regulation of the concentration of circulating PCSK9 and consequently of cellular LDL receptors.

Published

2021

3. Scalar nanostructure of the

Author

Megan D, Lenardon, Prashant, Sood, Helge C, Dorfmueller, Alistair J P, Brown, and Neil A R, Gow

Subjects

GPI, glycosylphosphatidylinositol, WGA, wheat germ agglutinin, rpm, revolutions per minute, 3D, three dimensions, Chitin, β-glucan, Article, PBS, phosphate buffered saline, PRRs, pattern recognition receptors, Cell wall proteins, CWPs, cell wall proteins, ChBD, chitin binding domain, SEM, scanning electron microscopy, Fungal cell wall ultrastructure, NMR, nuclear magnetic resonance, TEM, transmission electron microscopy, EndoH, endoglycosidase H, 2°, secondary, HPF/FS, high pressure freezing/freeze substitution, OD600, optical density at 600 nm, carbohydrates (lipids), AFM, atomic force microscopy, 3°, tertiary, Fc-dectin-1, soluble chimeric form of dectin-1, HuCκ, human kappa light chain, N-mannan, BSA, bovine serum albumin, 6xHis, hexahistidine tag, PAMPs, pathogen associated molecular patterns, scAb, single chain antibody, 2D, two dimensions

Abstract

Highlights • In wild type C. albicans yeast cells grown in standard lab conditions: • Chitin microfibrils are interspersed throughout the inner layer of the cell wall. • Cell wall proteins are embedded throughout the inner layer of the cell wall. • The outer fibrillar layer represents N-mannan outer chains. • The length of fibrils correlates with the length of the α(1,6)-N-mannan backbone. • Side chains extend from the α(1,6)-backbone at fixed angles every 10 mannose residues., Despite the importance of fungal cell walls as the principle determinant of fungal morphology and the defining element determining fungal interactions with other cells, few scalar models have been developed that reconcile chemical and microscopic attributes of its structure. The cell wall of the fungal pathogen Candida albicans is comprised of an amorphous inner skeletal layer of β(1,3)- and β(1,6)-glucan and chitin and an outer fibrillar layer thought to be dominated by highly mannosylated cell wall proteins. The architecture of these two layers can be resolved at the electron microscopy level, but the visualised structure of the wall has not yet been defined precisely in chemical terms. We have therefore examined the precise structure, location and molecular sizes of the cell wall components using transmission electron microscopy and tomography and tested predictions of the cell wall models using mutants and agents that perturb the normal cell wall structure. We demonstrate that the fibrils are comprised of a frond of N-linked outer chain mannans linked to a basal layer of GPI-proteins concentrated in the mid-wall region and that the non-elastic chitin microfibrils are cantilevered with sufficient lengths of non-fibrillar chitin and/or β-glucan to enable the chitin-glucan cage to flex, e.g. during morphogenesis and osmotic swelling. We present the first three-dimensional nano-scalar model of the C. albicans cell wall which can be used to test hypotheses relating to the structure–function relationships that underpin the pathobiology of this fungal pathogen.

Published

2020

4. Intestinal gel-forming mucins polymerize by disulfide-mediated dimerization of D3 domains

Author

Gabriel Javitt, Deborah Fass, Lis Albert, María Luisa Gómez Calvo, Tal Ilani, Nava Reznik, and Ron Diskin

Subjects

Models, Molecular, Dimer, D1D2D3CysD1, mucin 2 recombinant protein spanning residues 21 to 1397, quaternary structure, disulfide bonds, Mucin 2, Polymerization, chemistry.chemical_compound, 0302 clinical medicine, Structural Biology, Golgi, Disulfides, Conserved Sequence, chemistry.chemical_classification, 0303 health sciences, biology, Chemistry, 3. Good health, Amino acid, Intestines, SEC-MALS, size exclusion chromatography with multi-angle light scattering, Crystallization, Dimerization, VWF, von Willebrand factor, Protein family, MUC2D3, mucin 2 recombinant protein spanning residues 858 to 1259, Models, Biological, endoH, endoglycosidase H, Article, 03 medical and health sciences, Protein Domains, mucin, Von Willebrand factor, von Willebrand Factor, Humans, Amino Acid Sequence, Molecular Biology, 030304 developmental biology, colon, Mucin, Mucins, MUC2, mucin 2, DTT, dithiothreitol, SDS-PAGE, sodium dodecyl sulfate polyacrylamide gel electrophoresis, Biophysics, biology.protein, Protein quaternary structure, Protein Multimerization, Glycoprotein, Gels, 030217 neurology & neurosurgery, D1D2D3, mucin 2 recombinant protein spanning residues 21 to 1259

Abstract

The mucin 2 glycoprotein assembles into a complex hydrogel that protects intestinal epithelia and houses the gut microbiome. A major step in mucin 2 assembly is further multimerization of preformed mucin dimers, thought to produce a honeycomb-like arrangement upon hydrogel expansion. Important open questions are how multiple mucin 2 dimers become covalently linked to one another and how mucin 2 multimerization compares with analogous processes in related polymers such as respiratory tract mucins and the hemostasis protein von Willebrand factor. Here we report the x-ray crystal structure of the mucin 2 multimerization module, found to form a dimer linked by two intersubunit disulfide bonds. The dimer structure calls into question the current model for intestinal mucin assembly, which proposes disulfide-mediated trimerization of the same module. Key residues making interactions across the dimer interface are highly conserved in intestinal mucin orthologs, supporting the physiological relevance of the observed quaternary structure. With knowledge of the interface residues, it can be demonstrated that many of these amino acids are also present in other mucins and in von Willebrand factor, further indicating that the stable dimer arrangement reported herein is likely to be shared across this functionally broad protein family. The mucin 2 module structure thus reveals the manner by which both mucins and von Willebrand factor polymerize, drawing deep structural parallels between macromolecular assemblies critical to mucosal epithelia and the vasculature., Graphical abstract Unlabelled Image, Highlights • Network formation by gel-forming mucins protects epithelia but is poorly understood • Intestinal mucin N-terminal module dimerizes rather than trimerizes • The mucin dimer forms through atypical protein-protein interaction sites • Gut mucins and a blood hemostasis factor share polymerization mechanisms

Published

2019

5. Scalar nanostructure of the Candida albicans cell wall; a molecular, cellular and ultrastructural analysis and interpretation

Author

Lenardon, MD ; https://orcid.org/0000-0002-9471-7402, Sood, P, Dorfmueller, HC, Brown, AJP, Gow, NAR, Lenardon, MD ; https://orcid.org/0000-0002-9471-7402, Sood, P, Dorfmueller, HC, Brown, AJP, and Gow, NAR

Published

2020

6. HSP90 inhibitors reduce cholesterol storage in Niemann-Pick type C1 mutant fibroblasts

Author

Syed Z. Saad, Paul Helquist, Aisha al-Motawa, Nina H. Pipalia, Olaf Wiest, Daniel S. Ory, Kunal Garg, Brian S. J. Blagg, Len Neckers, Kanagaraj Subramanian, Abigail Cross, and Frederick R. Maxfield

Subjects

Mutant, EndoHS, EndoH-sensitive, DMSO, dimethyl sulfoxide, Arimoclomol, fluorescence microscopy, Biochemistry, chemistry.chemical_compound, Endocrinology, hemic and lymphatic diseases, chaperone, arimoclomol, HSP70, HDACi, histone deacetylase inhibitor, Cells, Cultured, EndoH, endoglycosidase H, biology, GRP94, glucose regulated protein 94, Chemistry, Histone deacetylase inhibitor, EndoHR, EndoH-resistant, Hsp90, drug therapy, lysosomal storage, NPC1, Niemann-Pick type C1, lipids (amino acids, peptides, and proteins), Niemann–Pick disease, Cholesterol storage, Niemann-Pick disease, Research Article, Lipid storage disorder, medicine.drug_class, QD415-436, ER, endoplasmic reticulum, Niemann-Pick C1 Protein, medicine, HSP90, Humans, endocytosis, HSP70 Heat-Shock Proteins, HSP90 Heat-Shock Proteins, LE/Ly, late endosomes and lysosomes, Endoplasmic reticulum, cholesterol, nutritional and metabolic diseases, Cell Biology, Fibroblasts, medicine.disease, PFI, perinuclear filipin intensity, Molecular biology, HSF1, heat shock transcription factor 1, Mutation, biology.protein, Histone deacetylase, PFA, paraformaldehyde, NPC1, HPCD, 2-hydroxypropyl beta-cyclodextrin

Abstract

Niemann Pick type C1 (NPC1) disease is a lysosomal lipid storage disorder caused by mutations of the NPC1 gene. More than 300 disease-associated mutations are reported in patients, resulting in abnormal accumulation of unesterified cholesterol, glycosphingolipids and other lipids in late endosomes and lysosomes (LE/Ly) of many cell types. Previously, we showed that treatment of many different NPC1 mutant fibroblasts with histone deacetylase inhibitors resulted in reduction of cholesterol storage, and we found that this was associated with enhanced exit of the NPC1 protein from the endoplasmic reticulum and delivery to LE/Ly. This suggested that histone deacetylase inhibitors may work through changes in protein chaperones to enhance the folding of NPC1 mutants, allowing them to be delivered to LE/Ly. In this study we evaluated the effect of several HSP90 inhibitors on NPC1I1061T skin fibroblasts. We found that HSP90 inhibition resulted in clearance of cholesterol from LE/Ly, and this was associated with enhanced delivery of the mutant NPC1I1061T protein to LE/Ly. We also observed that inhibition of HSP90 increased the expression of HSP70, and overexpression of HSP70 also reduced cholesterol storage in NPC1I1061T fibroblasts. However, we did not see correction of cholesterol storage by arimoclomol, a drug that is reported to increase HSP70 expression, at doses up to 0.5 mM. These results indicate that manipulation of molecular chaperones may lead to effective treatments for NPC1 disease, but further investigation of mechanisms will be required.

Published

2021

7. Thyroglobulin Interactome Profiling Defines Altered Proteostasis Topology Associated With Thyroid Dyshormonogenesis

Author

Madison T. Wright, Logan Kouba, and Lars Plate

Subjects

Proteomics, DSP, dithiobis(succinimidyl propionate), GRP94, 94 kDa glucose regulated protein, affinity purification - mass spectrometry, STT3B, oligosaccharyl transferase complex catalytic subunit B, medicine.medical_treatment, Hsp90, heat shock protein 90, protein-protein interactions, Gene mutation, T3, Triiodothyronine, Biochemistry, Interactome, ERAD, ER-associated degradation, Analytical Chemistry, N-glycosylation, asparagine-linked protein glycosylation, OST, oligosaccharyl transferase complex, UPR, unfolded protein response, GANAB, glucosidase II alpha subunit, Tandem Mass Spectrometry, ChEL, cholinesterase-like domain, protein folding, UGGT1, UDP-glucose glycoprotein glucosyltansferase 1, TMT, tandem mass tags, Protein Interaction Maps, PDIA6, protein disulfide isomerase family A member 6, EndoH, endoglycosidase H, OS-9, OS9 endoplasmic reticulum lectin, 0303 health sciences, biology, Chemistry, 030302 biochemistry & molecular biology, congenital hypothyroidism, BiP, binding immunoglobulin protein, cell secretion, Cell biology, tandem mass tags, DNAJB11, DnaJ heat shock protein family member B11, SEL1L, SEL1L adaptor subunit of ERAD E3 ubiquitin ligase, Oligosaccharyltransferase complex, CANX, calnexin, DNAJC10, DnaJ heat shock protein family member C10, MAN1B1, mannosidase alpha class 1B member 1, EDEM, ER degradation enhancing alpha-mannosidase, PDIA4, protein disulfide isomerase family A member 4, Endoplasmic-reticulum-associated protein degradation, Thyroglobulin, FOXRED2, RAD-dependent oxidoreductase domain containing 2, Cell Line, ER, endoplasmic reticulum, 03 medical and health sciences, CHX, cycloheximide, Calnexin, T4, thyroxine, medicine, Humans, protein quality control, PQC, protein quality control, PDIA3, protein disulfide isomerase family A member 3, Molecular Biology, CH, congenital hypothyroidism, GO, gene ontology, 030304 developmental biology, Research, CALR, calreticulin, Hsp70/40, heat shock protein 70 kDa and 40 kDa chaperone/co-chaperone system, PN, proteostasis network, Tg, thyroglobulin, Proteostasis, STT3A, oligosaccharyl transferase complex catalytic subunit A, Chaperone (protein), Mutation, biology.protein

Abstract

Thyroglobulin (Tg) is a secreted iodoglycoprotein serving as the precursor for triiodothyronine and thyroxine hormones. Many characterized Tg gene mutations produce secretion-defective variants resulting in congenital hypothyroidism. Tg processing and secretion is controlled by extensive interactions with chaperone, trafficking, and degradation factors comprising the secretory proteostasis network. While dependencies on individual proteostasis network components are known, the integration of proteostasis pathways mediating Tg protein quality control and the molecular basis of mutant Tg misprocessing remain poorly understood. We employ a multiplexed quantitative affinity purification–mass spectrometry approach to define the Tg proteostasis interactome and changes between WT and several congenital hypothyroidism variants. Mutant Tg processing is associated with common imbalances in proteostasis engagement including increased chaperoning, oxidative folding, and engagement by targeting factors for endoplasmic reticulum–associated degradation. Furthermore, we reveal mutation-specific changes in engagement with N-glycosylation components, suggesting distinct requirements for 1 Tg variant on dual engagement of both oligosaccharyltransferase complex isoforms for degradation. Modulating dysregulated proteostasis components and pathways may serve as a therapeutic strategy to restore Tg secretion and thyroid hormone biosynthesis., Graphical Abstract, Highlights • Quantitative multiplexed affinity purification—mass spectrometry was used to map the comprehensive thyroglobulin interactome. • Tg interactome consist of a diverse set of protein quality control components. • Mutants share imbalances with folding, disulfide processing, and degradation elements. • N-glycosylation plays a key role in the degradation of mutant thyroglobulin., In Brief Congenital hypothyroidism can result from mutations in the thyroglobulin (Tg) gene impairing protein secretion of the defective Tg variants. The molecular basis of mutant Tg misprocessing has remained poorly understood. Here we map the Tg interactome and quantify mutation specific changes in protein–protein interactions between Tg and protein quality control components. By integrating interactions across protein quality control pathways, we highlight shared imbalances in protein folding, disulfide processing, and degradation, and reveal mutant-specific roles for N-glycosylation in Tg processing.

Published

2021

8. Functional impact of intramolecular cleavage and dissociation of adhesion G protein–coupled receptor GPR133 (ADGRD1) on canonical signaling

Author

Dimitris G. Placantonakis, Jordan Wilcox, Joshua D. Frenster, Devin Bready, Torsten Schöneberg, Caroline Wilde, Niklas Ravn-Boess, Ines Liebscher, Giselle R. Wiggin, Bjoern Kieslich, Gabriele Stephan, and Norbert Sträter

Subjects

0301 basic medicine, BFA, brefeldin A, PAR1, protease-activated receptor 1, Biochemistry, Receptors, G-Protein-Coupled, intramolecular cleavage, DDM, n-dodecyl β-D-maltoside, Cyclic AMP, Tumor Cells, Cultured, Receptor, EndoH, endoglycosidase H, Chemistry, adhesion GPCR, subcellular fractionation, Cell biology, PM, plasma membrane, GPCRs, G protein–coupled receptors, medicine.symptom, signaling, Research Article, CTF, C-terminal fragment, Signal Transduction, glycosylation, intracellular trafficking, Immunoprecipitation, GPS, GPCR proteolysis site, Cleavage (embryo), Nuc, nucleus, ER, endoplasmic reticulum, 03 medical and health sciences, medicine, Humans, HTRF, homogenous time-resolved fluorescence, NTF–CTF dissociation, Molecular Biology, G protein-coupled receptor, 030102 biochemistry & molecular biology, Golgi, Golgi apparatus, hPAR1, human protease-activated receptor 1, HEK 293 cells, glioblastoma, Cell Biology, Cytosol, NTF, N-terminal fragment, 030104 developmental biology, Protease-Activated Receptor 1, Mechanism of action, receptor structure–function, Proteolysis, GBM, glioblastoma, BSA, bovine serum albumin, MWs, molecular weights

Abstract

GPR133 (ADGRD1), an adhesion G protein–coupled receptor (GPCR) whose canonical signaling activates GαS-mediated generation of cytosolic cAMP, has been shown to be necessary for the growth of glioblastoma (GBM), a brain malignancy. The extracellular N terminus of GPR133 is thought to be autoproteolytically cleaved into N-terminal and C- terminal fragments (NTF and CTF, respectively). However, the role of this cleavage in receptor activation remains unclear. Here, we used subcellular fractionation and immunoprecipitation approaches to show that the WT GPR133 receptor is cleaved shortly after protein synthesis and generates significantly more canonical signaling than an uncleavable point mutant GPR133 (H543R) in patient-derived GBM cultures and HEK293T cells. After cleavage, the resulting NTF and CTF remain noncovalently bound to each other until the receptor is trafficked to the plasma membrane, where we demonstrated NTF–CTF dissociation occurs. Using a fusion of the CTF of GPR133 and the N terminus of thrombin-activated human protease-activated receptor 1 as a controllable proxy system to test the effect of intramolecular cleavage and dissociation, we also showed that thrombin-induced cleavage and shedding of the human protease-activated receptor 1 NTF increased intracellular cAMP levels. These results support a model wherein dissociation of the NTF from the CTF at the plasma membrane promotes GPR133 activation and downstream signaling. These findings add depth to our understanding of the molecular life cycle and mechanism of action of GPR133 and provide critical insights that will inform therapeutic targeting of GPR133 in GBM.

Published

2021

9. Proteolytic processing of QSOX1A ensures efficient secretion of a potent disulfide catalyst

Author

Jana Rudolf, Neil J. Bulleid, and Marie A. Pringle

Subjects

Golgi Apparatus, QSOX, quiescin sulfhydryl oxidase, Biochemistry, DMEM, Dulbecco’s modified Eagle’s medium, Epitopes, Cricetinae, Oxidoreductases Acting on Sulfur Group Donors, Protein disulfide-isomerase, Peptide sequence, EndoH, endoglycosidase H, disulfide formation, 0303 health sciences, 030302 biochemistry & molecular biology, Transport protein, Isoenzymes, Protein Transport, Transmembrane domain, GAPDH, glyceraldehyde-3-phosphate dehydrogenase, symbols, proprotein convertase, Dimerization, Research Article, SEC, size-exclusion chromatography, Recombinant Fusion Proteins, Green Fluorescent Proteins, quiescin sulfhydryl oxidase 1 (QSOX1), CHO Cells, TBST, TBS containing 0.1% Tween 20, Biology, sulfhydryl oxidase, TCA, trichloroacetic acid, Cleavage (embryo), Cell Line, ER, endoplasmic reticulum, 03 medical and health sciences, symbols.namesake, Cricetulus, GM130, cis-Golgi matrix protein of 130 kDa, Animals, Humans, PDI, protein disulfide-isomerase, Secretion, Amino Acid Sequence, Ero1, endoplasmic reticulum oxidase 1, BMH, 1,6-bismaleimidohexane, Molecular Biology, Secretory pathway, 030304 developmental biology, PPC, proprotein convertase, Cell Biology, Golgi apparatus, Peptide Fragments, Protein Structure, Tertiary, PNGase, peptide N-glycosidase, Solubility, proteolytic processing, Proteolysis, Biocatalysis, CHO, Chinese-hamster ovary, NEM, N-ethylmaleimide, Protein Processing, Post-Translational, DDM, dodecylmaltoside, TM, transmembrane

Abstract

QSOX1 (quiescin sulfhydryl oxidase 1) efficiently catalyses the insertion of disulfide bonds into a wide range of proteins. The enzyme is mechanistically well characterized, but its subcellular location and the identity of its protein substrates remain ill-defined. The function of QSOX1 is likely to involve disulfide formation in proteins entering the secretory pathway or outside the cell. In the present study, we show that this enzyme is efficiently secreted from mammalian cells despite the presence of a transmembrane domain. We identify internal cleavage sites and demonstrate that the protein is processed within the Golgi apparatus to yield soluble enzyme. As a consequence of this efficient processing, QSOX1 is probably functional outside the cell. Also, QSOX1 forms a dimer upon cleavage of the C-terminal domain. The processing of QSOX1 suggests a novel level of regulation of secretion of this potent disulfide catalyst and producer of hydrogen peroxide.

Published

2013

10. Inhibition of protein translocation at the endoplasmic reticulum promotes activation of the unfolded protein response

Author

Stig Linder, Michela Piacenti, Sabine L. Flitsch, Alina Mares, Anna C. Callan, Peristera Roboti, Stephen High, Roger C. Whitehead, Karolina Lesiak-Mieczkowska, Hanna Harant, Marjo Puumalainen, Eileithyia Swanton, Craig McKibbin, and Helen L. Williams

Subjects

Protein Folding, XBP1, X-box-binding protein 1, non-translocated protein, EDEM-1, ER degradation-enhancing α-mannosidase-like 1, Endoplasmic Reticulum, Biochemistry, ERAD, ER-associated degradation, UPR, unfolded protein response, Cytosol, Ubiquitin, ES, eeyarestatin, Hydroxyurea, TCRα, T-cell receptor α subunit, EndoH, endoglycosidase H, 0303 health sciences, DMEM, Dulbecco's modified Eagle's medium, RT, reverse transcription, biology, 030302 biochemistry & molecular biology, IP, immunoprecipitation, unfolded protein response, PS2, proteasome inhibitor 2, eeyarestatin, Transport protein, Cell biology, DNA-Binding Proteins, Protein Transport, Protein folding, PERK, PKR (double-stranded-RNA-dependent protein kinase)-like ER kinase, Research Article, UPS, ubiquitin–proteasome system, Sec61, eIF2α, eukaryotic initiation factor 2α, IRE1, inositol-requiring enzyme 1, Endoplasmic-reticulum-associated protein degradation, Transfection, ER, endoplasmic reticulum, HEK, human embryonic kidney, 03 medical and health sciences, CHX, cycloheximide, Humans, cpd A, translocation inhibitor compound A, PDI, protein disulfide-isomerase, Molecular Biology, 030304 developmental biology, Endoplasmic reticulum, Hydrazones, Cell Biology, DTT, dithiothreitol, Unfolded protein response, biology.protein, Peptides, HeLa Cells

Abstract

Selective small-molecule inhibitors represent powerful tools for the dissection of complex biological processes. ESI (eeyarestatin I) is a novel modulator of ER (endoplasmic reticulum) function. In the present study, we show that in addition to acutely inhibiting ERAD (ER-associated degradation), ESI causes production of mislocalized polypeptides that are ubiquitinated and degraded. Unexpectedly, our results suggest that these non-translocated polypeptides promote activation of the UPR (unfolded protein response), and indeed we can recapitulate UPR activation with an alternative and quite distinct inhibitor of ER translocation. These results suggest that the accumulation of non-translocated proteins in the cytosol may represent a novel mechanism that contributes to UPR activation.

Published

2012

11. A biochemical analysis of the constraints of tail-anchored protein biogenesis

Author

Pawel Leznicki, Stephen High, and Jim Warwicker

Subjects

Cytb5, cytochrome b5, TRC40, transmembrane domain recognition complex of 40 kDa, tail-anchored protein (TA protein), Endoplasmic Reticulum, Biochemistry, Hsp, heat-shock protein, Polyethylene Glycols, 0302 clinical medicine, Cytosol, mPEG, methoxypoly(ethylene glycol), PEG, poly(ethylene glycol), Drosophila Proteins, Lipid bilayer, OPG, opsin glycosylation tag, EndoH, endoglycosidase H, 0303 health sciences, PEGylation, BODIPY®, boron dipyrromethene (4,4-difluoro-4-bora-3a,4a-diaza-s-indacene), Recombinant Proteins, Transmembrane domain, Tetratricopeptide, Protein Transport, Membrane, BMH, bis(maleimido)hexane, Research Article, Protein Binding, TA, tail-anchored, Biology, SRP, signal recognition particle, TMS, transmembrane segment, SGTA, small glutamine-rich tetratricopeptide repeat-containing protein α, ER, endoplasmic reticulum, 03 medical and health sciences, IASD, 4-acetamido-4′-[(iodoacetyl)amino]stilbene-2,2′-disulfonate, Animals, Humans, PDI, protein disulfide-isomerase, Molecular Biology, 030304 developmental biology, Endoplasmic reticulum, HisTrx, histidine–thioredoxin, transmembrane domain recognition complex of 40 kDa (TRC40), Membrane Proteins, Cell Biology, Cytochromes b5, small glutamine-rich tetratricopeptide repeat-containing protein α (SGTA), Biophysics, Sec61β, cytochrome b5 (Cytb5), Get, guided entry of tail-anchored proteins, Carrier Proteins, 030217 neurology & neurosurgery, Biogenesis, SEC Translocation Channels, Molecular Chaperones

Abstract

TA (tail-anchored) proteins utilize distinct biosynthetic pathways, including TRC40 (transmembrane domain recognition complex of 40 kDa)-mediated, chaperone-dependent and/or unassisted routes to the ER (endoplasmic reticulum) membrane. We have addressed the flexibility of cytosolic components participating in these pathways, and explored the thermodynamic constraints of their membrane insertion, by exploiting recombinant forms of Sec61β and Cytb5 (cytochrome b5) bearing covalent modifications within their TA region. In both cases, efficient membrane insertion relied on cytosolic factors capable of accommodating a surprising range of covalent modifications to the TA region. For Sec61β, we found that both SGTA (small glutamine-rich tetratricopeptide repeat-containing protein α) and TRC40 can bind this substrate with a singly PEGylated TA region. However, by introducing two PEG [poly(ethylene glycol)] moieties, TRC40 binding can be prevented, resulting in a block of subsequent membrane integration. Although TRC40 can bind Sec61β polypeptides singly PEGylated at different locations, membrane insertion is more sensitive to the precise location of PEG attachment. Modelling and experimentation indicate that this post-TRC40 effect results from an increased energetic cost of inserting different PEGylated TA regions into the lipid bilayer. We therefore propose that the membrane integration of TA proteins delivered via TRC40 is strongly dependent upon underlying thermodynamics, and speculate that their insertion is via a phospholipid-mediated process.

Published

2011

12. Scalar nanostructure of the Candida albicans cell wall; a molecular, cellular and ultrastructural analysis and interpretation.

Author

Lenardon MD, Sood P, Dorfmueller HC, Brown AJP, and Gow NAR

Abstract

Despite the importance of fungal cell walls as the principle determinant of fungal morphology and the defining element determining fungal interactions with other cells, few scalar models have been developed that reconcile chemical and microscopic attributes of its structure. The cell wall of the fungal pathogen Candida albicans is comprised of an amorphous inner skeletal layer of β(1,3)- and β(1,6)-glucan and chitin and an outer fibrillar layer thought to be dominated by highly mannosylated cell wall proteins. The architecture of these two layers can be resolved at the electron microscopy level, but the visualised structure of the wall has not yet been defined precisely in chemical terms. We have therefore examined the precise structure, location and molecular sizes of the cell wall components using transmission electron microscopy and tomography and tested predictions of the cell wall models using mutants and agents that perturb the normal cell wall structure. We demonstrate that the fibrils are comprised of a frond of N -linked outer chain mannans linked to a basal layer of GPI-proteins concentrated in the mid-wall region and that the non-elastic chitin microfibrils are cantilevered with sufficient lengths of non-fibrillar chitin and/or β-glucan to enable the chitin-glucan cage to flex, e.g. during morphogenesis and osmotic swelling. We present the first three-dimensional nano-scalar model of the C. albicans cell wall which can be used to test hypotheses relating to the structure-function relationships that underpin the pathobiology of this fungal pathogen., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2020 The Authors.)

Published

2020

13. Biochemical Characterization of Protein Quality Control Mechanisms during Disease Progression in the C22 Mouse Model of CMT1A

Author

Irina Madorsky, Lee Sooyeon, Jordan T. Schmidt, Jessica Nicks, Lucia Notterpek, Vinita G. Chittoor, Sunitha Rangaraju, and Diana C. Narvaez

Subjects

Wt, wild-type, Chaperonins, LAMP1, lysosomal membrane-associated protein 1, pUb, polyubiquitinated, CathD, Cathepsin D, Hsp, heat-shock protein, Mice, Myelin, 0302 clinical medicine, Egr2, early growth response 2, Charcot-Marie-Tooth Disease, Peripheral myelin protein 22, chaperone, TFEB, transcription factor EB, PNGaseF, N-glycosidase F, 0303 health sciences, CD11b Antigen, biology, General Neuroscience, Age Factors, HRP, horseradish peroxidase, CMT1A, Charcot–Marie–Tooth disease type 1A, Sciatic Nerve, 3. Good health, Cell biology, myelin, medicine.anatomical_structure, Neutrophil Infiltration, Disease Progression, Myelin Proteins, Research Article, Proteasome Endopeptidase Complex, autophagy, UPS, ubiquitin–proteasome system, Transgene, MCP-1, monocyte chemoattractant protein 1, Schwann cell, Mice, Transgenic, S3, endoH, endoglycosidase H, protein aggregation, MS, multiple sclerosis, lcsh:RC321-571, ER, endoplasmic reticulum, 03 medical and health sciences, Oct6, octamer-binding transcription factor 6, Lysosome, ubiquitin, medicine, Animals, Humans, HSP70 Heat-Shock Proteins, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, 030304 developmental biology, AMC, amino-methyl coumarin, Macrophages, Autophagy, PMP22, peripheral myelin protein 22, Proteins, HSF1, heat-shock factor 1, di-8-ANEPPS, 4-[2-(6-dibutylamino)-2-naphthalenyl)ethenyl]-1-(3-sulfopropyl) hydroxide, LC3, light chain 3, Mice, Inbred C57BL, Disease Models, Animal, Gene Expression Regulation, Proteasome, Chaperone (protein), Immunology, biology.protein, Schwann Cells, Neurology (clinical), IgG, immunoglobulin, 030217 neurology & neurosurgery

Abstract

Charcot–Marie–Tooth disease type 1A (CMT1A) is a hereditary demyelinating neuropathy linked with duplication of the peripheral myelin protein 22 (PMP22) gene. Transgenic C22 mice, a model of CMT1A, display many features of the human disease, including slowed nerve conduction velocity and demyelination of peripheral nerves. How overproduction of PMP22 leads to compromised myelin and axonal pathology is not fully understood, but likely involves subcellular alterations in protein homoeostatic mechanisms within affected Schwann cells. The subcellular response to abnormally localized PMP22 includes the recruitment of the ubiquitin–proteasome system (UPS), autophagosomes and heat-shock proteins (HSPs). Here we assessed biochemical markers of these protein homoeostatic pathways in nerves from PMP22-overexpressing neuropathic mice between the ages of 2 and 12 months to ascertain their potential contribution to disease progression. In nerves of 3-week-old mice, using endoglycosidases and Western blotting, we found altered processing of the exogenous human PMP22, an abnormality that becomes more prevalent with age. Along with the ongoing accrual of misfolded PMP22, the activity of the proteasome becomes compromised and proteins required for autophagy induction and lysosome biogenesis are up-regulated. Moreover, cytosolic chaperones are consistently elevated in nerves from neuropathic mice, with the most prominent change in HSP70. The gradual alterations in protein homoeostatic response are accompanied by Schwann cell de-differentiation and macrophage infiltration. Together, these results show that while subcellular protein quality control mechanisms respond appropriately to the presence of the overproduced PMP22, with aging they are unable to prevent the accrual of misfolded proteins., In peripheral nerves of neuropathic C22 mice the frequency of cytosolic PMP22 aggregates increases with age, which elicits a response from protein quality control mechanisms. The combined effects of aging and neuropathic genotype exacerbate disease progression leading to nerve defects.

Published

2013

14. Reorientation of the first signal-anchor sequence during potassium channel biogenesis at the Sec61 complex

Author

Helen R, Watson, Lydia, Wunderley, Tereza, Andreou, Jim, Warwicker, and Stephen, High

Subjects

OPG, opsin N-glycosylation tag, TASK-1, TWIK (tandem-pore weak inwardly rectifying potassium channel)-related acid-sensitive potassium channel 1, Membrane Proteins, BMH, bismaleimidohexane, Nerve Tissue Proteins, Intracellular Membranes, Protein Sorting Signals, TWIK (tandem-pore weak inwardly rectifying potassium channel)-related acid-sensitive potassium channel 1 (TASK-1), membrane protein folding, TRAM, translocating chain-associated membrane protein, Endoplasmic Reticulum, Peptide Fragments, Protein Structure, Secondary, ER, endoplasmic reticulum, Potassium Channels, Tandem Pore Domain, TM, transmembrane region, site-specific cross-linking, Cys-null, cysteine-null, Humans, potassium channel protein of chlorella virus (Kcv channel), Kcv, potassium channel protein of chlorella virus, SEC Translocation Channels, HeLa Cells, Research Article, EndoH, endoglycosidase H

Abstract

The majority of the polytopic proteins that are synthesized at the ER (endoplasmic reticulum) are integrated co-translationally via the Sec61 translocon, which provides lateral access for their hydrophobic TMs (transmembrane regions) to the phospholipid bilayer. A prolonged association between TMs of the potassium channel subunit, TASK-1 [TWIK (tandem-pore weak inwardly rectifying potassium channel)-related acid-sensitive potassium channel 1], and the Sec61 complex suggests that the ER translocon co-ordinates the folding/assembly of the TMs present in the nascent chain. The N-terminus of both TASK-1 and Kcv (potassium channel protein of chlorella virus), another potassium channel subunit of viral origin, has access to the N-glycosylation machinery located in the ER lumen, indicating that the Sec61 complex can accommodate multiple arrangements/orientations of TMs within the nascent chain, both in vitro and in vivo. Hence the ER translocon can provide the ribosome-bound nascent chain with a dynamic environment in which it can explore a range of different conformations en route to its correct transmembrane topology and final native structure., The Sec61 translocon provides an unexpectedly flexible and dynamic environment within which transmembrane regions of nascent polypeptides can be completely reoriented during the biosynthesis of multiple-spanning membrane proteins.

Published

2013

15. Cell surface delivery and structural re-organization by pharmacological chaperones of an oligomerization-defective α1b-adrenoceptor mutant demonstrates membrane targeting of GPCR oligomers

Author

Graeme Milligan, Juan F. López-Giménez, Meritxell Canals, Biochemistry and Molecular Biology, and University of Glasgow

Subjects

Glycosylation, Mutant, Endoplasmic Reticulum, BFA, brefeldin A, endoplasmic reticulum retention, Biochemistry, Receptors, G-Protein-Coupled, Cell membrane, chemistry.chemical_compound, HEK cell, human embryonic kidney cell, 0302 clinical medicine, TM, transmembrane domain, eYFP, enhanced yellow fluorescent protein, Receptor, NGaseF, N-glycosidase F, EndoH, endoglycosidase H, 0303 health sciences, DMEM, Dulbecco's modified Eagle's medium, Life Sciences, α1b-adrenoceptor TMI-TMIV, a form of the hamster α1b-adrenoceptor containing point mutations (L1.52A, V1.53A) in transmembrane domain I and (L4.46A, L4.47A) in transmembrane domain IV, STIM1, Brefeldin A, Immunohistochemistry, G-protein-coupled receptor (GPCR), Cell biology, Transmembrane domain, medicine.anatomical_structure, Dimerization, Protein Binding, Research Article, Enzyme-Linked Immunosorbent Assay, Biology, FRET, fluorescence resonance energy transfer, Cell Line, ER, endoplasmic reticulum, 03 medical and health sciences, medicine, Humans, Biotinylation, Molecular Biology, Adrenergic alpha-Antagonists, GPCR, G-protein-coupled receptor, 030304 developmental biology, G protein-coupled receptor, Endoplasmic reticulum, Cell Membrane, Biological Transport, Prazosin, Cell Biology, Receptors, Adrenergic, alpha, pharmacological chaperone, chemistry, Mutation, eCFP, enhanced cyan fluorescent protein, GABA, γ-aminobutyric acid, [35S]GTP[S], [35S]guanosine 5′-[γ-thio]triphosphate, 030217 neurology & neurosurgery, Molecular Chaperones

Abstract

Many G-protein-coupled receptors, including the alpha(1b)-adrenoceptor, form homo-dimers or oligomers. Mutation of hydrophobic residues in transmembrane domains I and IV alters the organization of the alpha(1b)-adrenoceptor oligomer, with transmembrane domain IV playing a critical role. These mutations also result in endoplasmic reticulum trapping of the receptor. Following stable expression of this alpha(1b)-adrenoceptor mutant, cell surface delivery, receptor function and structural organization were recovered by treatment with a range of alpha(1b)-adrenoceptor antagonists that acted at the level of the endoplasmic reticulum. This was accompanied by maturation of the mutant receptor to a terminally N-glycosylated form, and only this mature form was trafficked to the cell surface. Co-expression of the mutant receptor with an otherwise wild-type form of the alpha(1b)-adrenoceptor that is unable to bind ligands resulted in this wild-type variant also being retained in the endoplasmic reticulum. Ligand-induced cell surface delivery of the mutant alpha(1b)-adrenoceptor now allowed co-recovery to the plasma membrane of the ligand-binding-deficient mutant. These results demonstrate that interactions between alpha(1b)-adrenoceptor monomers occur at an early stage in protein synthesis, that ligands of the alpha(1b)-adrenoceptor can act as pharmacological chaperones to allow a structurally compromised form of the receptor to pass cellular quality control, that the mutated receptor is not inherently deficient in function and that an oligomeric assembly of ligand-binding-competent and -incompetent forms of the alpha(1b)-adrenoceptor can be trafficked to the cell surface by binding of a ligand to only one component of the receptor oligomer.

Published

2008

16. Role of the domain encompassing Arg304–Ile328 in rat P2X2 receptor conformation revealed by alterations in complex glycosylation at Asn298

Author

Helen Broomhead, Lishuang Cao, Yi-Hong Zhang, Lin-Hua Jiang, and Mark T. Young

Subjects

Glycosylation, topology, Protein Conformation, Biology, Kidney, Q1, Biochemistry, HEK, human embryonic kidney, 03 medical and health sciences, chemistry.chemical_compound, Protein structure, TM, transmembrane domain, Animals, Humans, scanning cysteine mutagenesis, Amino Acid Sequence, Receptor, Molecular Biology, Peptide sequence, Ion channel, EndoH, endoglycosidase H, 030304 developmental biology, pre-transmembrane segment 2 (TM2), chemistry.chemical_classification, 0303 health sciences, Receptors, Purinergic P2, 030302 biochemistry & molecular biology, Cell Biology, Protein Structure, Tertiary, Rats, Amino acid, Transmembrane domain, chemistry, Ectodomain, ion channel, Biophysics, Asparagine, Receptors, Purinergic P2X2, Research Article

Abstract

The final 25 amino acids of the ectodomain of the P2X receptors, immediately prior to the second TM (transmembrane domain) (pre-TM2: Arg(304)-Ile(328) in rat P2X(2)), are highly conserved. Whole-cell patch clamp recordings showed that single cysteine substitutions in the N-terminal half of pre-TM2 (Arg(304)-Ile(314)) led to loss of function at Arg(304), Leu(306), Lys(308) and Ile(312). Cysteine substitutions within this region also resulted in a significant reduction in the apparent molecular mass of receptors, due to loss of complex glycosylation at the nearby acceptor site Asn(298), which was not seen for the C-terminal portion of pre-TM2 (Asp(315)-Ile(328)). The reduction in complex glycosylation was not due to reduced cell-surface presentation, demonstrating that glycosylation at Asn(298) was acting as a sensor of subtle changes in receptor conformation within the pre-TM2 region. When this N-glycan site was repositioned closer to the plasma membrane by mutagenesis (N298S together with G299N, T300N, T301N or T303N), glycosylation was restored at G299N and T300N, but was impaired for T301N and completely absent for T303N. These results suggest that the region in the vicinity of Asp(315) is at the plasma membrane interface and that the N-terminal portion of pre-TM2 (Arg(304)-Ile(314)) is important for the correct conformation of the receptor at the extracellular face of the membrane.

Published

2008