Your search keyword '"Erik I. Hallin"' showing total 19 results

1. Ocrelizumab quantitation by liquid chromatography-tandem mass spectrometry

Author

Erik I. Hallin, Trond Trætteberg Serkland, Kjell-Morten Myhr, Øivind Torkildsen, and Silje Skrede

Subjects

Therapeutic monoclonal antibodies, Multiple sclerosis, Ocrelizumab, LC-MS/MS, Therapeutic drug monitoring, Medical technology, R855-855.5

Abstract

Introduction: Ocrelizumab is a monoclonal anti-CD20 antibody approved for the treatment of multiple sclerosis (MS). The clinical value of therapeutic drug monitoring (TDM) for this antibody in treatment of MS is unknown, and an adequately specific and precise quantitation method for ocrelizumab in patient serum could facilitate investigation. Liquid chromatography-tandem mass spectrometry (LC-MS/MS)-based quantitation methods have been shown to have higher analytic specificity and precision than enzyme-linked immunosorbent assays. Objectives: To establish and validate an LC-MS/MS-based quantitation method for ocrelizumab. Methods: We present an LC-MS/MS-based quantitation method using immunocapture purification followed by trypsinization and analysis by a triple quadrupole mass analyzer obtaining results within the same day. Results: We found that the ocrelizumab peptide GLEWVGAIYPGNGDTSYNQK (Q1/Q3 Quantifier ion: 723.683+/590.77 y112+ Qualifier ion: 723.683+/672.30 y122+) can be used for quantitation and thereby developed a method for quantifying ocrelizumab in human serum with a quantitation range of 1.56 to 200 µg/mL. The method was validated in accordance with EMA requirements in terms of selectivity, carry-over, lower limit of quantitation, calibration curve, accuracy, precision and matrix effect. Ocrelizumab serum concentrations were measured in three MS patients treated with ocrelizumab, immediately before and after ocrelizumab infusion, with additional sampling after 2, 4, 8 and 12 weeks. Measured serum concentrations of ocrelizumab showed expected values for both Cmax and drug half-life over the sampled time period. Conclusion: We have established a reliable quantitation method for serum ocrelizumab that can be applied in clinical studies, facilitating the evaluation of ocrelizumab TDM in MS.

Published

2022

2. High-affinity anti-Arc nanobodies provide tools for structural and functional studies

Author

Sigurbjörn Markússon, Erik I. Hallin, Helene J. Bustad, Arne Raasakka, Ju Xu, Gopinath Muruganandam, Remy Loris, Aurora Martinez, Clive R. Bramham, and Petri Kursula

Subjects

Medicine, Science

Abstract

Activity-regulated cytoskeleton-associated protein (Arc) is a multidomain protein of retroviral origin with a vital role in the regulation of synaptic plasticity and memory formation in mammals. However, the mechanistic and structural basis of Arc function is poorly understood. Arc has an N-terminal domain (NTD) involved in membrane binding and a C-terminal domain (CTD) that binds postsynaptic protein ligands. In addition, the NTD and CTD both function in Arc oligomerisation, including assembly of retrovirus-like capsids involved in intercellular signalling. To obtain new tools for studies on Arc structure and function, we produced and characterised six high-affinity anti-Arc nanobodies (Nb). The CTD of rat and human Arc were both crystallised in ternary complexes with two Nbs. One Nb bound deep into the stargazin-binding pocket of Arc CTD and suggested competitive binding with Arc ligand peptides. The crystallisation of the human Arc CTD in two different conformations, accompanied by SAXS data and molecular dynamics simulations, paints a dynamic picture of the mammalian Arc CTD. The collapsed conformation closely resembles Drosophila Arc in capsids, suggesting that we have trapped a capsid-like conformation of the human Arc CTD. Our data obtained with the help of anti-Arc Nbs suggest that structural dynamics of the CTD and dimerisation of the NTD may promote the formation of capsids. Taken together, the recombinant high-affinity anti-Arc Nbs are versatile tools that can be further developed for studying mammalian Arc structure and function, as well as mechanisms of Arc capsid formation, both in vitro and in vivo. For example, the Nbs could serve as a genetically encoded tools for inhibition of endogenous Arc interactions in the study of neuronal function and plasticity.

Published

2022

3. Structural properties and peptide ligand binding of the capsid homology domains of human Arc

Author

Erik I. Hallin, Clive R. Bramham, and Petri Kursula

Subjects

Crystal structure, Specificity, Peptide binding, Postsynaptic density, Protein interaction, Capsid homology, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

The activity-regulated cytoskeleton-associated protein (Arc) is important for synaptic plasticity and the normal function of the brain. Arc interacts with neuronal postsynaptic proteins, but the mechanistic details of its function have not been fully established. The C-terminal domain of Arc consists of tandem domains, termed the N- and C-lobe. The N-lobe harbours a peptide binding site, able to bind multiple targets. By measuring the affinity of human Arc towards various peptides from stargazin and guanylate kinase-associated protein (GKAP), we have refined its specificity determinants. We found two sites in the GKAP repeat region that bind to Arc and confirmed these interactions by X-ray crystallography. Phosphorylation of the stargazin peptide did not affect binding affinity but caused changes in thermodynamic parameters. Comparison of the crystal structures of three high-resolution human Arc-peptide complexes identifies three conserved C–H…π interactions at the binding cavity, explaining the sequence specificity of short linear motif binding by Arc. We further characterise central residues of the Arc lobe fold, show the effects of peptide binding on protein dynamics, and identify acyl carrier proteins as structures similar to the Arc lobes. We hypothesise that Arc may affect protein-protein interactions and phase separation at the postsynaptic density, affecting protein turnover and re-modelling of the synapse. The present data on Arc structure and ligand binding will help in further deciphering these processes.

Published

2021

4. Molecular mechanisms of Charcot-Marie-Tooth neuropathy linked to mutations in human myelin protein P2

Author

Salla Ruskamo, Tuomo Nieminen, Cecilie K. Kristiansen, Guro H. Vatne, Anne Baumann, Erik I. Hallin, Arne Raasakka, Päivi Joensuu, Ulrich Bergmann, Ilpo Vattulainen, and Petri Kursula

Subjects

Medicine, Science

Abstract

Abstract Charcot-Marie-Tooth (CMT) disease is one of the most common inherited neuropathies. Recently, three CMT1-associated point mutations (I43N, T51P, and I52T) were discovered in the abundant peripheral myelin protein P2. These mutations trigger abnormal myelin structure, leading to reduced nerve conduction velocity, muscle weakness, and distal limb atrophy. P2 is a myelin-specific protein expressed by Schwann cells that binds to fatty acids and membranes, contributing to peripheral myelin lipid homeostasis. We studied the molecular basis of the P2 patient mutations. None of the CMT1-associated mutations alter the overall folding of P2 in the crystal state. P2 disease variants show increased aggregation tendency and remarkably reduced stability, T51P being most severe. In addition, P2 disease mutations affect protein dynamics. Both fatty acid binding by P2 and the kinetics of its membrane interactions are affected by the mutations. Experiments and simulations suggest opening of the β barrel in T51P, possibly representing a general mechanism in fatty acid-binding proteins. Our findings demonstrate that altered biophysical properties and functional dynamics of P2 may cause myelin defects in CMT1 patients. At the molecular level, a few malformed hydrogen bonds lead to structural instability and misregulation of conformational changes related to ligand exchange and membrane binding.

Published

2017

5. Raptor-Mediated Proteasomal Degradation of Deamidated 4E-BP2 Regulates Postnatal Neuronal Translation and NF-κB Activity

Author

Stella Kouloulia, Erik I. Hallin, Konstanze Simbriger, Inês S. Amorim, Gilliard Lach, Theoklitos Amvrosiadis, Kleanthi Chalkiadaki, Agniete Kampaite, Vinh Tai Truong, Mehdi Hooshmandi, Seyed Mehdi Jafarnejad, Paul Skehel, Petri Kursula, Arkady Khoutorsky, and Christos G. Gkogkas

Subjects

Biology (General), QH301-705.5

Abstract

Summary: The translation initiation repressor 4E-BP2 is deamidated in the brain on asparagines N99/N102 during early postnatal brain development. This post-translational modification enhances 4E-BP2 association with Raptor, a central component of mTORC1 and alters the kinetics of excitatory synaptic transmission. We show that 4E-BP2 deamidation is neuron specific, occurs in the human brain, and changes 4E-BP2 subcellular localization, but not its disordered structure state. We demonstrate that deamidated 4E-BP2 is ubiquitinated more and degrades faster than the unmodified protein. We find that enhanced deamidated 4E-BP2 degradation is dependent on Raptor binding, concomitant with increased association with a Raptor-CUL4B E3 ubiquitin ligase complex. Deamidated 4E-BP2 stability is promoted by inhibiting mTORC1 or glutamate receptors. We further demonstrate that deamidated 4E-BP2 regulates the translation of a distinct pool of mRNAs linked to cerebral development, mitochondria, and NF-κB activity, and thus may be crucial for postnatal brain development in neurodevelopmental disorders, such as ASD. : Kouloulia et al. demonstrate that, during early postnatal brain development, deamidation of the translation initiation factor 4E-BP2 renders it susceptible to ubiquitination and proteasomal degradation via enhanced binding to the Raptor-CUL4B complex. mTORC1 or glutamate receptor inhibition stabilizes deamidated 4E-BP2. Moreover, deamidated 4E-BP2 regulates the translation of specific mRNAs and NF-κB activity. Keywords: asparagine deamidation, translational control, postnatal brain, 4E-BP2, Raptor, CUL4B, proteasome, NF-κB, mTORC1

Published

2019

6. Development and Validation of Arc Nanobodies: New Tools for Probing Arc Dynamics and Function

Author

Yuta Ishizuka, Tadiwos F. Mergiya, Rodolfo Baldinotti, Ju Xu, Erik I. Hallin, Sigurbjörn Markússon, Petri Kursula, and Clive R. Bramham

Subjects

Mammals, C-lobe, Co-immunoprecipitation, Neuronal Plasticity, Long-Term Potentiation, Nerve Tissue Proteins, Chromobody, General Medicine, Single-Domain Antibodies, Arc, Biochemistry, Intrabody, Rats, N-lobe, Cellular and Molecular Neuroscience, Cytoskeletal Proteins, Neuroblastoma, Nanobody, Animals, Humans

Abstract

Activity-regulated cytoskeleton-associated (Arc) protein plays key roles in long-term synaptic plasticity, memory, and cognitive flexibility. However, an integral understanding of Arc mechanisms is lacking. Arc is proposed to function as an interaction hub in neuronal dendrites and the nucleus, yet Arc can also form retrovirus-like capsids with proposed roles in intercellular communication. Here, we sought to develop anti-Arc nanobodies (ArcNbs) as new tools for probing Arc dynamics and function. Six ArcNbs representing different clonal lines were selected from immunized alpaca. Immunoblotting with recombinant ArcNbs fused to a small ALFA-epitope tag demonstrated binding to recombinant Arc as well as endogenous Arc from rat cortical tissue. ALFA-ArcNb also provided efficient immunoprecipitation of stimulus-induced Arc after carbachol-treatment of SH-SY5Y neuroblastoma cells and induction of long-term potentiation in the rat dentate gyrus in vivo. Epitope mapping showed that all Nbs recognize the Arc C-terminal region containing the retroviral Gag capsid homology domain, comprised of tandem N-and C-lobes. ArcNbs E5 and H11 selectively bound the N-lobe, which harbors a peptide ligand binding pocket specific to mammals. Four additional ArcNbs bound the region containing the C-lobe and terminal tail. For use as genetically encoded fluorescent intrabodies, we show that ArcNbs fused to mScarlet-I are uniformly expressed, without aggregation, in the cytoplasm and nucleus of HEK293FT cells. Finally, mScarlet-I-ArcNb H11 expressed as intrabody selectively bound the N-lobe and enabled co-immunoprecipitation of full-length intracellular Arc. ArcNbs are versatile tools for live-cell labeling and purification of Arc and analysis of capsid domain specific functions.

Published

2022

7. High-affinity nanobodies as tools for structural and functional studies on mammalian Arc

Author

Sigurbjörn Markússon, Erik I. Hallin, Helene J. Bustad, Arne Raasakka, Ju Xu, Gopinath Muruganandam, Remy Loris, Aurora Martinez, Clive R. Bramham, and Petri Kursula

Abstract

Activity-regulated cytoskeleton-associated protein (Arc) is a multidomain protein of retroviral origin with a vital role in the regulation of synaptic plasticity and memory formation in mammals. However, the mechanistic and structural basis of Arc function is little understood. Arc has an NTD involved in membrane binding and a CTD which binds postsynaptic protein ligands. In addition, the NTD and CTD both function in Arc oligomerization, including assembly of retrovirus-like capsid involved in intercellular signaling. We produced and characterised six ultra-high-affinity anti-Arc nanobodies (Nb). The CTD of both rat and human Arc could be crystallised in ternary complexes with two Nbs simultaneously bound (H11 and C11). H11 binding deep into the stargazing-binding pocket of Arc CTD suggested competitive binding with Arc ligand peptides, which was confirmed in vitro. This indicates that the H11 Nb could serve as a genetically-encoded tool for inhibition of endogenous Arc N-lobe interactions in study of neuronal function and plasticity. The crystallisation of the human Arc CTD in two different conformations, accompanied by SAXS data and molecular dynamics simulations, paints a dynamic picture of the mammalian Arc CTD. Dynamics were affected by mutations known to inhibit capsid formation, implying a role for Arc CTD dynamics in oligomerisation. Dimerisation of the NTD, together with structural dynamics of the CTD, suggest a mechanism, by which structural dynamics of the CTD may promote capsomer formation, and dimerisation of the NTD links capsomers, facilitating the formation of capsids. The described recombinant ultrahigh-affinity anti-Arc Nbs are versatile tools that can be further developed for studying mammalian Arc structure and function in vitro and in vivo.

Published

2021

8. Arc self-association and formation of virus-like capsids are mediated by an N-terminal helical coil motif

Author

Margaret M. Stratton, Erik I. Hallin, Rory O’Connell, Clive R. Bramham, Gopinath Muruganandam, Shreeram Akerkar, James J. Chambers, Yasunori Hayashi, Ian Merski, Petri Kursula, Helene J. Bustad, Remy Loris, Tambudzai Kanhema, Tomohisa Hosokawa, José M. Valpuesta, Marte I. Flydal, Christine Touma, Maria S. Eriksen, Daniela Lascu, Oleksii Nikolaienko, Sverre Grødem, Jorge Cuéllar, Aurora Martinez, Department of Bio-engineering Sciences, Structural Biology Brussels, and Faculty of Sciences and Bioengineering Sciences

Subjects

0301 basic medicine, Protein Conformation, Amino Acid Motifs, Mutant, Nerve Tissue Proteins, Crystallography, X-Ray, Endocytosis, Antiparallel (biochemistry), Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, Animals, Drosophila Proteins, Humans, Protein oligomerization, Molecular Biology, Neurons, Neuronal Plasticity, Sequence Homology, Amino Acid, Chemistry, Cryoelectron Microscopy, Virion, RNA, Cell Biology, computer.file_format, Protein Data Bank, Cytoskeletal Proteins, 030104 developmental biology, Förster resonance energy transfer, Capsid, 030220 oncology & carcinogenesis, Biophysics, Capsid Proteins, computer, Signal Transduction

Abstract

Activity-regulated cytoskeleton-associated protein (Arc) is a protein interaction hub with diverse roles in intracellular neuronal signaling, and important functions in neuronal synaptic plasticity, memory, and postnatal cortical development. Arc has homology to retroviral Gag protein and is capable of self-assembly into virus-like capsids implicated in the intercellular transfer of RNA. However, the molecular basis of Arc self-association and capsid formation is largely unknown. Here, we identified a 28-amino-acid stretch in the mammalian Arc N-terminal (NT) domain that is necessary and sufficient for self-association. Within this region, we identified a 7-residue oligomerization motif, critical for the formation of virus-like capsids. Purified wild-type Arc formed capsids as shown by transmission and cryo-electron microscopy, whereas mutant Arc with disruption of the oligomerization motif formed homogenous dimers. An atomic-resolution crystal structure of the oligomerization region peptide demonstrated an antiparallel coiled-coil interface, strongly supporting NT-NT domain interactions in Arc oligomerization. The NT coil-coil interaction was also validated in live neurons using fluorescence lifetime FRET imaging, and mutation of the oligomerization motif disrupted Arc-facilitated endocytosis. Furthermore, using single-molecule photobleaching, we show that Arc mRNA greatly enhances higher-order oligomerization in a manner dependent on the oligomerization motif. In conclusion, a helical coil in the Arc NT domain supports self-association above the dimer stage, mRNA-induced oligomerization, and formation of virus-like capsids. DATABASE: The coordinates and structure factors for crystallographic analysis of the oligomerization region were deposited at the Protein Data Bank with the entry code 6YTU.

Published

2021

9. Crystal and solution structures reveal oligomerization of individual capsid homology domains of Drosophila Arc

Author

Petri Kursula, Andrew E. Torda, Sigurbjörn Markússon, Lev Böttger, Erik I. Hallin, and Clive R. Bramham

Subjects

Models, Molecular, Protein Conformation, Dimer, Crystallography, X-Ray, Biochemistry, Homology (biology), Viral Packaging, chemistry.chemical_compound, Protein structure, 0302 clinical medicine, Animal Cells, Macromolecular Structure Analysis, Materials, Neurons, 0303 health sciences, Crystallography, Multidisciplinary, Arc (protein), biology, Physics, Monomers, Condensed Matter Physics, 3. Good health, Chemistry, Histone, Capsid, Dendritic Structure, Physical Sciences, Crystal Structure, Medicine, Drosophila, Cellular Types, Research Article, Gene isoform, Protein Structure, Science, Materials Science, Nerve Tissue Proteins, Sequence alignment, Viral Structure, Microbiology, DNA-binding protein, 03 medical and health sciences, Protein Domains, Virology, DNA-binding proteins, Solid State Physics, Animals, ddc:610, Amino Acid Sequence, Dimers, Molecular Biology, Transcription factor, 030304 developmental biology, Biology and Life Sciences, Proteins, Cell Biology, Neuronal Dendrites, Polymer Chemistry, Solution structure, Viral Replication, Cytoskeletal Proteins, chemistry, Oligomers, Cellular Neuroscience, Synaptic plasticity, biology.protein, Biophysics, Protein Multimerization, 030217 neurology & neurosurgery, Neuroscience

Abstract

Synaptic plasticity is vital for brain function and memory formation. One of the key proteins in long-term synaptic plasticity and memory is the activity-regulated cytoskeleton-associated protein (Arc). Mammalian Arc forms virus-like capsid structures in a process requiring the N-terminal domain and contains two C-terminal lobes that are structural homologues to retroviral capsids. Drosophila has two isoforms of Arc, dArc1 and dArc2, with low sequence similarity to mammalian Arc, but lacking a large N-terminal domain. Both dArc isoforms are related to the Ty3/gypsy retrotransposon capsid, consisting of N- and C-terminal lobes. Structures of dArc1, as well as capsids formed by both dArc isoforms, have been recently determined. We carried out structural characterization of the four individual dArc lobe domains. As opposed to the corresponding mammalian Arc lobe domains, which are monomeric, the dArc lobes were all oligomeric in solution, indicating a strong propensity for homophilic interactions. A truncated N-lobe from dArc2 formed a domain-swapped dimer in the crystal structure, resulting in a novel dimer interaction that could be relevant for capsid assembly or other dArc functions. This domain-swapped structure resembles the dimeric protein C of flavivirus capsids, as well as the structure of histones dimers, domain-swapped transcription factors, and membrane-interacting BAK domains. The strong oligomerization properties of the isolated dArc lobe domains explain the ability of dArc to form capsids in the absence of any large N-terminal domain, in contrast to the mammalian protein.

Published

2021

10. Structural properties and peptide ligand binding of the capsid homology domains of human Arc

Author

Petri Kursula, Erik I. Hallin, and Clive R. Bramham

Subjects

0301 basic medicine, QH301-705.5, Biophysics, Peptide, Peptide binding, QD415-436, Biochemistry, Homology (biology), 03 medical and health sciences, 0302 clinical medicine, Postsynaptic potential, Capsid homology, ddc:530, Short linear motif, Biology (General), chemistry.chemical_classification, Arc (protein), Chemistry, Crystal structure, Protein interaction, Protein dynamics, Protein turnover, Postsynaptic density, 030104 developmental biology, Capsid, 030220 oncology & carcinogenesis, Specificity, Phosphorylation, Research Article

Abstract

Biochemistry and biophysics reports 26, 100975 (2021). doi:10.1016/j.bbrep.2021.100975, The activity-regulated cytoskeleton-associated protein (Arc) is important for synaptic plasticity and the normal function of the brain. Arc interacts with neuronal postsynaptic proteins, but the mechanistic details of its function have not been fully established. The C-terminal domain of Arc consists of tandem domains, termed the N- and C-lobe. The N-lobe harbours a peptide binding site, able to bind multiple targets. By measuring the affinity of human Arc towards various peptides from stargazin and guanylate kinase-associated protein (GKAP), we have refined its specificity determinants. We found two sites in the GKAP repeat region that bind to Arc and confirmed these interactions by X-ray crystallography. Phosphorylation of the stargazin peptide did not affect binding affinity but caused changes in thermodynamic parameters. Comparison of the crystal structures of three high-resolution human Arc-peptide complexes identifies three conserved C���H����� interactions at the binding cavity, explaining the sequence specificity of short linear motif binding by Arc. We further characterise central residues of the Arc lobe fold, show the effects of peptide binding on protein dynamics, and identify acyl carrier proteins as structures similar to the Arc lobes. We hypothesise that Arc may affect protein-protein interactions and phase separation at the postsynaptic density, affecting protein turnover and re-modelling of the synapse. The present data on Arc structure and ligand binding will help in further deciphering these processes., Published by Elsevier, Amsterdam [u.a.]

Published

2020

11. Correction to: Development and Validation of Arc Nanobodies: New Tools for Probing Arc Dynamics and Function

Author

Yuta Ishizuka, Tadiwos F. Mergiya, Rodolfo Baldinotti, Ju Xu, Erik I. Hallin, Sigurbjörn Markússon, Petri Kursula, and Clive R. Bramham

Subjects

Cellular and Molecular Neuroscience, General Medicine, Biochemistry

Published

2022

12. Structure of monomeric full-length ARC sheds light on molecular flexibility, protein interactions, and functional modalities

Author

Maria S. Eriksen, Oleksii Nikolaienko, Sergei Baryshnikov, Clive R. Bramham, Yasunori Hayashi, Tomohisa Hosokawa, Erik I. Hallin, Petri Kursula, and Sverre Grødem

Subjects

Male, Models, Molecular, 0301 basic medicine, Protein Conformation, Nerve Tissue Proteins, Hippocampus, Biochemistry, Protein–protein interaction, Rats, Sprague-Dawley, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Protein structure, Protein Domains, Postsynaptic potential, Fluorescence Resonance Energy Transfer, Animals, Humans, Scattering, Radiation, Lipid bilayer, Neurons, Coiled coil, Arc (protein), Molecular Structure, Chemistry, Circular Dichroism, X-Rays, Recombinant Proteins, Rats, Cytoskeletal Proteins, 030104 developmental biology, Förster resonance energy transfer, Biophysics, CTD, Postsynaptic signal transduction, 030217 neurology & neurosurgery

Abstract

The activity-regulated cytoskeleton-associated protein (ARC) is critical for long-term synaptic plasticity and memory formation. Acting as a protein interaction hub, ARC regulates diverse signalling events in postsynaptic neurons. A protein interaction site is present in the ARC C-terminal domain (CTD), a bilobar structure homologous to the retroviral Gag capsid domain. We hypothesized that detailed knowledge of the three-dimensional molecular structure of monomeric full-length ARC is crucial to understand its function; therefore, we set out to determine the structure of ARC to understand its various functional modalities. We purified recombinant ARC and analyzed its structure using small-angle X-ray scattering and synchrotron radiation circular dichroism spectroscopy. Monomeric full-length ARC has a compact, closed structure, in which the oppositely charged N-terminal domain (NTD) and CTD are juxtaposed, and the flexible linker between them is not extended. The modeled structure of ARC is supported by intramolecular live-cell Förster resonance energy transfer imaging in rat hippocampal slices. Peptides from several postsynaptic proteins, including stargazin, bind to the N-lobe, but not to the C-lobe, of the bilobar CTD. This interaction does not induce large-scale conformational changes in the CTD or flanking unfolded regions. The ARC NTD contains long helices, predicted to form an anti-parallel coiled coil; binding of ARC to phospholipid membranes requires the NTD. Our data support a role for the ARC NTD in oligomerization as well as lipid membrane binding. The findings have important implications for the structural organization of ARC with respect to distinct functions, such as postsynaptic signal transduction and virus-like capsid formation. Open Practices Open Science: This manuscript was awarded with the Open Materials Badge. For more information see: https://cos.io/our-services/open-science-badges/.

Published

2018

13. Molecular determinants of Arc oligomerization and formation of virus-like capsids

Author

Clive R. Bramham, Gopinath Muruganandam, Remy Loris, Ian Merski, Marte I. Flydal, Jorge Cuéllar, James J. Chambers, Erik I. Hallin, Yasunori Hayashi, Margaret M. Stratton, Aurora Martinez, Tambudzai Kanhema, José M. Valpuesta, Sverre Grødem, Petri Kursula, Daniela Lascu, Helene J. Bustad, Shreeram Akerkar, Tomohisa Hosokawa, Maria S. Eriksen, Oleksii Nikolaienko, and Rory O’Connell

Subjects

education.field_of_study, Arc (protein), Capsid, Chemistry, Population, Mutant, HEK 293 cells, Biophysics, RNA, Alanine scanning, education, Green fluorescent protein

Abstract

Expression of activity-regulated cytoskeleton-associated protein (Arc) is critical for long-term synaptic plasticity, memory formation, and cognitive flexibility. The ability of Arc to self-associate and form virus-like capsid structures implies functionally distinct oligomeric states. However, the molecular mechanism of Arc oligomerization is unknown. Here, we identified a 28-amino-acid region necessary and sufficient for Arc oligomerization. This oligomerization region is located within the second coil of a predicted anti-parallel coiled-coil in the N-terminal domain (NTD). Using alanine scanning mutagenesis, we found a 7-amino-acid motif critical for oligomerization and Arc-mediated transferrin endocytosis in HEK cells. Intermolecular fluorescence lifetime imaging in hippocampal neurons confirmed self-association mediated by the motif. To quantify oligomeric size, we performed a single-molecule photobleaching analysis of purified Arc wild-type and mutant. This analysis revealed a critical role for the NTD motif in the formation of higher-order Arc oligomers (30-170 molecules). Moreover, assembly of higher-order wild-type Arc oligomers was significantly enhanced by addition of GFP RNA. Purified wild-type Arc formed virus-like capsids, as visualized by negative-stain EM, and was estimated by light scattering analysis to contain 40-55 Arc units. In contrast, mutant Arc formed a homogenous dimer population as demonstrated by single-molecule TIRF imaging, size-exclusion chromatography with multi-angle light scattering analysis, small-angle X-ray scattering analysis, and single-particle 3D EM reconstruction. Thus, the dimer appears to be the basic building block for assembly. Herein, we show that the NTD motif is essential for higher-order Arc oligomerization, assembly of virus-like capsid particles, and facilitation of oligomerization by exogenous RNA.SIGNIFICANCEArc protein is rapidly expressed in neurons in response to synaptic activity and plays critical roles in synaptic plasticity, postnatal cortical developmental, and memory. Arc has diverse molecular functions, which may be related to distinct oligomeric states of the protein. Arc has homology to retroviral Gag protein and self-assembles into retrovirus-like capsid structures that are capable of intercellular transfer of RNA. Here, we identified a motif in the N-terminal coiled-coil domain of mammalian Arc that mediates higher-order oligomerization and formation of virus-like capsids. The basic building block is the Arc dimer and exogenous RNA facilitates further assembly. The identified molecular determinants of Arc oligomerization will help to elucidate the functional modalities of Arc in the mammalian brain.

Published

2019

14. Raptor-Mediated Proteasomal Degradation of Deamidated 4E-BP2 Regulates Postnatal Neuronal Translation and NF-κB Activity

Author

Konstanze Simbriger, Inês S. Amorim, Gilliard Lach, Petri Kursula, Vinh Tai Truong, Christos G. Gkogkas, Theoklitos Amvrosiadis, Seyed Mehdi Jafarnejad, Paul A. Skehel, Erik I. Hallin, Stella Kouloulia, Kleanthi Chalkiadaki, Agniete Kampaite, Mehdi Hooshmandi, and Arkady Khoutorsky

Subjects

0301 basic medicine, Male, 4E-BP2, asparagine deamidation, mTORC1, NF-κB, Mice, 0302 clinical medicine, Ubiquitin, Eukaryotic Initiation Factors, lcsh:QH301-705.5, Cells, Cultured, Neurons, biology, Chemistry, Glutamate receptor, NF-kappa B, Brain, translational control, Translation (biology), Human brain, Cullin Proteins, postnatal brain, 3. Good health, Cell biology, Ubiquitin ligase, Raptor, medicine.anatomical_structure, NF-κBm, Female, Protein Binding, Proteasome Endopeptidase Complex, Repressor, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, medicine, Animals, Humans, Regulatory-Associated Protein of mTOR, TORC1, Mice, Inbred C57BL, 030104 developmental biology, HEK293 Cells, proteasome, lcsh:Biology (General), Proteasome, Proteolysis, biology.protein, CUL4B, 030217 neurology & neurosurgery

Abstract

Summary The translation initiation repressor 4E-BP2 is deamidated in the brain on asparagines N99/N102 during early postnatal brain development. This post-translational modification enhances 4E-BP2 association with Raptor, a central component of mTORC1 and alters the kinetics of excitatory synaptic transmission. We show that 4E-BP2 deamidation is neuron specific, occurs in the human brain, and changes 4E-BP2 subcellular localization, but not its disordered structure state. We demonstrate that deamidated 4E-BP2 is ubiquitinated more and degrades faster than the unmodified protein. We find that enhanced deamidated 4E-BP2 degradation is dependent on Raptor binding, concomitant with increased association with a Raptor-CUL4B E3 ubiquitin ligase complex. Deamidated 4E-BP2 stability is promoted by inhibiting mTORC1 or glutamate receptors. We further demonstrate that deamidated 4E-BP2 regulates the translation of a distinct pool of mRNAs linked to cerebral development, mitochondria, and NF-κB activity, and thus may be crucial for postnatal brain development in neurodevelopmental disorders, such as ASD., Graphical Abstract, Highlights • Deamidated 4E-BP2 occurs in neurons and is susceptible to ubiquitination/degradation • mTORC1 or glutamate receptor inhibition stabilizes deamidated 4E-BP2 • A Raptor-CUL4B ubiquitin ligase complex binds to deamidated 4E-BP2 • Deamidated 4E-BP2 regulates postnatal brain translation and NF-κB activity, Kouloulia et al. demonstrate that, during early postnatal brain development, deamidation of the translation initiation factor 4E-BP2 renders it susceptible to ubiquitination and proteasomal degradation via enhanced binding to the Raptor-CUL4B complex. mTORC1 or glutamate receptor inhibition stabilizes deamidated 4E-BP2. Moreover, deamidated 4E-BP2 regulates the translation of specific mRNAs and NF-κB activity.

Published

2019

15. Neuropathy-related mutations alter the membrane binding properties of the human myelin protein P0 cytoplasmic tail

Author

Arne Raasakka, Oda C. Krokengen, Hanna Wacklin-Knecht, Maximilian W. A. Skoda, Erik I. Hallin, Salla Ruskamo, Robert Barker, Cecilie Katrin Kristiansen, Søren Vrønning Hoffmann, Guro Helén Vatne, Petri Kursula, Ulrich Bergmann, and Nykola C. Jones

Subjects

0301 basic medicine, Cytoplasm, Protein Folding, Cell Membranes, Lipid Bilayers, MPZ, medicine.disease_cause, Biochemistry, Turbidity, Myelin, 0302 clinical medicine, Materials Physics, Compact myelin, INTRACELLULAR DOMAIN, P-0 GLYCOPROTEIN OVEREXPRESSION, Lipid bilayer, 0303 health sciences, Mutation, Multidisciplinary, Chemistry, Physics, Peripheral Nervous System Diseases, REFLECTOMETER, Lipids, Transmembrane protein, 3. Good health, Cell biology, Phenotype, medicine.anatomical_structure, Physical Sciences, Medicine, Cellular Structures and Organelles, Myelin P0 Protein, Research Article, Protein Binding, Science, Materials Science, Schwann cell, 03 medical and health sciences, Lipid Structure, Genetics, medicine, Point Mutation, Humans, PO PROTEIN, ddc:610, Vesicles, 030304 developmental biology, MAJOR STRUCTURAL PROTEIN, Point mutation, Saltatory conduction, Cell Membrane, Biology and Life Sciences, Membrane Proteins, Cell Biology, BASIC-PROTEIN, MODEL, 030104 developmental biology, GENE DOSAGE, Membrane protein, REFLECTIVITY, Lipid Bilayer, 030217 neurology & neurosurgery

Abstract

Schwann cells myelinate selected axons in the peripheral nervous system (PNS) and contribute to fast saltatory conduction via the formation of compact myelin, in which water is excluded from between tightly adhered lipid bilayers. Peripheral neuropathies, such as Charcot-Marie-Tooth disease (CMT) and Dejerine-Sottas syndrome (DSS), are incurable demyelinating conditions that result in pain, decrease in muscle mass, and functional impairment. Many Schwann cell proteins, which are directly involved in the stability of compact myelin or its development, are subject to mutations linked to these neuropathies. The most abundant PNS myelin protein is protein zero (P0); point mutations in this transmembrane protein cause CMT subtype 1B and DSS. P0 tethers apposing lipid bilayers together through its extracellular immunoglobulin-like domain. Additionally, P0 contains a cytoplasmic tail (P0ct), which is membrane-associated and contributes to the physical properties of the lipid membrane. Six CMT- and DSS-associated missense mutations have been reported in P0ct. We generated recombinant disease mutant variants of P0ct and characterized them using biophysical methods. Compared to wild-type P0ct, some mutants have negligible differences in function and folding, while others highlight functionally important amino acids within P0ct. For example, the D224Y variant of P0ct induced tight membrane multilayer stacking. Our results show a putative molecular basis for the hypermyelinating phenotype observed in patients with this particular mutation and provide overall information on the effects of disease-linked mutations in a flexible, membrane-binding protein segment. Using neutron reflectometry, we additionally show that P0ct embeds deep into a lipid bilayer, explaining the observed effects of P0ct on the physical properties of the membrane. publishedVersion

Published

2019

16. Structure and dynamics of a human myelin protein P2 portal region mutant indicate opening of the beta barrel in fatty acid binding proteins

Author

Arne Raasakka, Erik I. Hallin, Petri Kursula, Marc F. Lensink, Anushik Safaryan, Salla Ruskamo, Oda C. Krokengen, Guillaume Brysbaert, Saara Laulumaa, Ilpo Vattulainen, Tuomo Nieminen, Department of Physics, Tampere University, Physics, University of Eastern Finland, Univ Oulu, Bioctr Oulu, Oulu, Finland, Unité de Glycobiologie Structurale et Fonctionnelle UMR 8576 (UGSF), Université de Lille-Institut National de la Recherche Agronomique (INRA)-Centre National de la Recherche Scientifique (CNRS), Department of Physics [Helsinki], Falculty of Science [Helsinki], University of Helsinki-University of Helsinki, Institut des Hautes Etudes Scientifiques (IHES), IHES, Unité de Glycobiologie Structurale et Fonctionnelle - UMR 8576 (UGSF), Université de Lille-Centre National de la Recherche Scientifique (CNRS)-Institut National de la Recherche Agronomique (INRA), Université de Lille-Centre National de la Recherche Scientifique (CNRS), and Helsingin yliopisto = Helsingfors universitet = University of Helsinki-Helsingin yliopisto = Helsingfors universitet = University of Helsinki

Subjects

0301 basic medicine, Models, Molecular, Membrane binding, PREDICTION, [SDV]Life Sciences [q-bio], Mutant, Lipid Bilayers, POINT MUTATIONS, medicine.disease_cause, Crystallography, X-Ray, Myelin P2 Protein, Protein Structure, Secondary, 0302 clinical medicine, Structural Biology, Mutant protein, Charcot-Marie-Tooth Disease, Fatty acid binding, Protein stability, Lipid bilayer, lcsh:QH301-705.5, ComputingMilieux_MISCELLANEOUS, Mutation, Calorimetry, Differential Scanning, Chemistry, LIPID-MEMBRANES, Fatty Acids, FABPS, DIFFERENT MECHANISMS, Ligand (biochemistry), Myelin, Research Article, Phenylalanine, Molecular Dynamics Simulation, Molecular dynamics, 114 Physical sciences, Fatty acid-binding protein, PERIPHERAL NERVOUS-SYSTEM, 03 medical and health sciences, medicine, Humans, Protein Unfolding, UCSF-CHIMERA, Crystal structure, PHOSPHOLIPID-MEMBRANES, SIMULATIONS, 030104 developmental biology, lcsh:Biology (General), Structural biology, RESOLUTION, Biophysics, 1182 Biochemistry, cell and molecular biology, 030217 neurology & neurosurgery

Abstract

Background Myelin is a multilayered proteolipid sheath wrapped around selected axons in the nervous system. Its constituent proteins play major roles in forming of the highly regular membrane structure. P2 is a myelin-specific protein of the fatty acid binding protein (FABP) superfamily, which is able to stack lipid bilayers together, and it is a target for mutations in the human inherited neuropathy Charcot-Marie-Tooth disease. A conserved residue that has been proposed to participate in membrane and fatty acid binding and conformational changes in FABPs is Phe57. This residue is thought to be a gatekeeper for the opening of the portal region upon ligand entry and egress. Results We performed a structural characterization of the F57A mutant of human P2. The mutant protein was crystallized in three crystal forms, all of which showed changes in the portal region and helix α2. In addition, the behaviour of the mutant protein upon lipid bilayer binding suggested more unfolding than previously observed for wild-type P2. On the other hand, membrane binding rendered F57A heat-stable, similarly to wild-type P2. Atomistic molecular dynamics simulations showed opening of the side of the discontinuous β barrel, giving important indications on the mechanism of portal region opening and ligand entry into FABPs. The results suggest a central role for Phe57 in regulating the opening of the portal region in human P2 and other FABPs, and the F57A mutation disturbs dynamic cross-correlation networks in the portal region of P2. Conclusions Overall, the F57A variant presents similar properties to the P2 patient mutations recently linked to Charcot-Marie-Tooth disease. Our results identify Phe57 as a residue regulating conformational changes that may accompany membrane surface binding and ligand exchange in P2 and other FABPs. Electronic supplementary material The online version of this article (10.1186/s12900-018-0087-2) contains supplementary material, which is available to authorized users.

Published

2018

17. The quaternary structure of human tyrosine hydroxylase: effects of dystonia-associated missense variants on oligomeric state and enzyme activity

Author

Gopinath Muruganandam, Juha P. Kallio, Agnete Fossbakk, Erik I. Hallin, Lisbeth Birk Møller, Peter D. Szigetvari, Petri Kursula, Per M. Knappskog, Inari Kursula, Remy Loris, Jan Haavik, Department of Bio-engineering Sciences, Faculty of Sciences and Bioengineering Sciences, and Structural Biology Brussels

Subjects

0301 basic medicine, Circular dichroism, Tyrosine 3-Monooxygenase, Protein subunit, enzymatic activity, Mutation, Missense, oligomeric structure, Biochemistry, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Missense mutation, SEC-SAXS, Humans, Protein Structure, Quaternary, SEC‐SAXS, chemistry.chemical_classification, Molecular Basis of Disease, biology, Tyrosine hydroxylase, Enzyme structure, Enzyme assay, 3. Good health, tyrosine hydroxylase deficiency, 030104 developmental biology, Enzyme, chemistry, Dystonic Disorders, missense variants, biology.protein, TEM, Protein quaternary structure, Original Article, ORIGINAL ARTICLES, 030217 neurology & neurosurgery

Abstract

Tyrosine hydroxylase (TH) is a multi‐domain, homo‐oligomeric enzyme that catalyses the rate‐limiting step of catecholamine neurotransmitter biosynthesis. Missense variants of human TH are associated with a recessive neurometabolic disease with low levels of brain dopamine and noradrenaline, resulting in a variable clinical picture, from progressive brain encephalopathy to adolescent onset DOPA‐responsive dystonia (DRD). We expressed isoform 1 of human TH (hTH1) and its dystonia‐associated missense variants in E. coli, analysed their quaternary structure and thermal stability using size‐exclusion chromatography, circular dichroism, multi‐angle light scattering, transmission electron microscopy, small‐angle X‐ray scattering and assayed hydroxylase activity. Wild‐type (WT) hTH1 was a mixture of enzymatically stable tetramers (85.6%) and octamers (14.4%), with little interconversion between these species. We also observed small amounts of higher order assemblies of long chains of enzyme by transmission electron microscopy. To investigate the role of molecular assemblies in the pathogenesis of DRD, we compared the structure of WT hTH1 with the DRD‐associated variants R410P and D467G that are found in vicinity of the predicted subunit interfaces. In contrast to WT hTH1, R410P and D467G were mixtures of tetrameric and dimeric species. Inspection of the available structures revealed that Arg‐410 and Asp‐467 are important for maintaining the stability and oligomeric structure of TH. Disruption of the normal quaternary enzyme structure by missense variants is a new molecular mechanism that may explain the loss of TH enzymatic activity in DRD. Unstable missense variants could be targets for pharmacological intervention in DRD, aimed to re‐establish the normal oligomeric state of TH.

Published

2018

18. Publisher Correction: Molecular mechanisms of Charcot-Marie-Tooth neuropathy linked to mutations in human myelin protein P2

Author

Ulrich Bergmann, Erik I. Hallin, Anne Baumann, Ilpo Vattulainen, Guro Helén Vatne, Petri Kursula, Päivi Joensuu, Salla Ruskamo, Cecilie Katrin Kristiansen, Arne Raasakka, and Tuomo Nieminen

Subjects

Protein Folding, Protein Conformation, Mutation, Missense, lcsh:Medicine, Bioinformatics, Myelin P2 Protein, Biophysical Phenomena, 03 medical and health sciences, Myelin, 0302 clinical medicine, Charcot-Marie-Tooth Disease, medicine, Humans, lcsh:Science, 030304 developmental biology, 0303 health sciences, Multidisciplinary, business.industry, Protein Stability, lcsh:R, Cell Membrane, Fatty Acids, Publisher Correction, medicine.anatomical_structure, lcsh:Q, Mutant Proteins, business, 030217 neurology & neurosurgery, Protein Binding

Abstract

Charcot-Marie-Tooth (CMT) disease is one of the most common inherited neuropathies. Recently, three CMT1-associated point mutations (I43N, T51P, and I52T) were discovered in the abundant peripheral myelin protein P2. These mutations trigger abnormal myelin structure, leading to reduced nerve conduction velocity, muscle weakness, and distal limb atrophy. P2 is a myelin-specific protein expressed by Schwann cells that binds to fatty acids and membranes, contributing to peripheral myelin lipid homeostasis. We studied the molecular basis of the P2 patient mutations. None of the CMT1-associated mutations alter the overall folding of P2 in the crystal state. P2 disease variants show increased aggregation tendency and remarkably reduced stability, T51P being most severe. In addition, P2 disease mutations affect protein dynamics. Both fatty acid binding by P2 and the kinetics of its membrane interactions are affected by the mutations. Experiments and simulations suggest opening of the β barrel in T51P, possibly representing a general mechanism in fatty acid-binding proteins. Our findings demonstrate that altered biophysical properties and functional dynamics of P2 may cause myelin defects in CMT1 patients. At the molecular level, a few malformed hydrogen bonds lead to structural instability and misregulation of conformational changes related to ligand exchange and membrane binding.

Published

2018

19. Crystal and solution structures reveal oligomerization of individual capsid homology domains of Drosophila Arc.

Author

Erik I Hallin, Sigurbjörn Markússon, Lev Böttger, Andrew E Torda, Clive R Bramham, and Petri Kursula

Subjects

Medicine, Science

Abstract

Synaptic plasticity is vital for brain function and memory formation. One of the key proteins in long-term synaptic plasticity and memory is the activity-regulated cytoskeleton-associated protein (Arc). Mammalian Arc forms virus-like capsid structures in a process requiring the N-terminal domain and contains two C-terminal lobes that are structural homologues to retroviral capsids. Drosophila has two isoforms of Arc, dArc1 and dArc2, with low sequence similarity to mammalian Arc, but lacking a large N-terminal domain. Both dArc isoforms are related to the Ty3/gypsy retrotransposon capsid, consisting of N- and C-terminal lobes. Structures of dArc1, as well as capsids formed by both dArc isoforms, have been recently determined. We carried out structural characterization of the four individual dArc lobe domains. As opposed to the corresponding mammalian Arc lobe domains, which are monomeric, the dArc lobes were all oligomeric in solution, indicating a strong propensity for homophilic interactions. A truncated N-lobe from dArc2 formed a domain-swapped dimer in the crystal structure, resulting in a novel dimer interaction that could be relevant for capsid assembly or other dArc functions. This domain-swapped structure resembles the dimeric protein C of flavivirus capsids, as well as the structure of histones dimers, domain-swapped transcription factors, and membrane-interacting BAK domains. The strong oligomerization properties of the isolated dArc lobe domains explain the ability of dArc to form capsids in the absence of any large N-terminal domain, in contrast to the mammalian protein.

Published

2021