Your search keyword '"Fabien Kieken"' showing total 22 results

1. Chemical shift assignments of the partially deuterated Fyn SH2–SH3 domain

Author

Peter Tompa, Karine Loth, Fabien Kieken, Nico A. J. van Nuland, Tom Lenaerts, Informatics and Applied Informatics, Structural Biology Brussels, Department of Bio-engineering Sciences, Structural Biology Brussels (SBB), Vrije Universiteit Brussel (VUB), VIB-VUB Center for Structural Biology [Bruxelles], VIB [Belgium], Centre de biophysique moléculaire (CBM), Université d'Orléans (UO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Chimie du CNRS (INC), AI-lab, Vakgroep Computerwetenschappen, Université Libre de Bruxelles, Département d'informatique (MLG), Interuniversity Institute of Bioinformatics in Brussels (IB2), Université libre de Bruxelles (ULB)-Vrije Universiteit Brussel (VUB), Vrije Universiteit [Brussels] (VUB), Université d'Orléans (UO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), and Université Libre de Bruxelles - Institut de Bioinformatique de Bruxelles

Subjects

0301 basic medicine, animal structures, Chemistry, Stereochemistry, Kinase, [SDV]Life Sciences [q-bio], Phosphatase, SH3–SH2, Biochemistry, NMR, SH3 domain, Homology (biology), Src family, 03 medical and health sciences, Fyn kinase, Tandem domains, 030104 developmental biology, FYN, Deuterium, Structural Biology, Tyrosine kinase, Proto-oncogene tyrosine-protein kinase Src

Abstract

Src Homology 2 and 3 (SH2 and SH3) are two key protein interaction modules involved in regulating the activity of many proteins such as tyrosine kinases and phosphatases by respective recognition of phosphotyrosine and proline-rich regions. In the Src family kinases, the inactive state of the protein is the direct result of the interaction of the SH2 and the SH3 domain with intra-molecular regions, leading to a closed structure incompetent with substrate modification. Here, we report the 1H, 15N and 13C backbone- and side-chain chemical shift assignments of the partially deuterated Fyn SH3-SH2 domain and structural differences between tandem and single domains. The BMRB accession number is 27165.

Published

2017

2. Calmodulin Directly Interacts with the Cx43 Carboxyl-Terminus and Cytoplasmic Loop Containing Three ODDD-Linked Mutants (M147T, R148Q, and T154A) that Retain α-Helical Structure, but Exhibit Loss-of-Function and Cellular Trafficking Defects

Author

Sylvie Chenavas, Fabien Kieken, Sarah Brownell, Paul L. Sorgen, Asokan Anbanandam, Andrew J. Trease, Li Zheng, and Gaelle Spagnol

Subjects

Protein Conformation, alpha-Helical, 0301 basic medicine, Cytoplasm, calmodulin, Circular dichroism, Foot Deformities, Congenital, Calmodulin, Mutant, lcsh:QR1-502, Oculodentodigital dysplasia, Biochemistry, lcsh:Microbiology, Article, Craniofacial Abnormalities, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Loss of Function Mutation, medicine, Humans, Eye Abnormalities, Molecular Biology, gap junctions, biology, Tooth Abnormalities, Chemistry, ODDD, medicine.disease, NMR, connexin43, circular dichroism, Cell biology, Protein Transport, Focal Adhesion Kinase 2, 030104 developmental biology, Connexin 43, biology.protein, Phosphorylation, Syndactyly, 030217 neurology & neurosurgery, Intracellular, HeLa Cells, Protein Binding, cytoplasmic loop domain, Proto-oncogene tyrosine-protein kinase Src

Abstract

The autosomal-dominant pleiotropic disorder called oculodentodigital dysplasia (ODDD) is caused by mutations in the gap junction protein Cx43. Of the 73 mutations identified to date, over one-third are localized in the cytoplasmic loop (Cx43CL) domain. Here, we determined the mechanism by which three ODDD mutations (M147T, R148Q, and T154A), all of which localize within the predicted 1-5-10 calmodulin-binding motif of the Cx43CL, manifest the disease. Nuclear magnetic resonance (NMR) and circular dichroism revealed that the three ODDD mutations had little-to-no effect on the ability of the Cx43CL to form &alpha, helical structure as well as bind calmodulin. Combination of microscopy and a dye-transfer assay uncovered these mutations increased the intracellular level of Cx43 and those that trafficked to the plasma membrane did not form functional channels. NMR also identify that CaM can directly interact with the Cx43CT domain. The Cx43CT residues involved in the CaM interaction overlap with tyrosines phosphorylated by Pyk2 and Src. In vitro and in cyto data provide evidence that the importance of the CaM interaction with the Cx43CT may lie in restricting Pyk2 and Src phosphorylation, and their subsequent downstream effects.

Published

2020

3. Structural Characterization of Monomeric/Dimeric State of p59(fyn) SH2 Domain

Author

Radu Huculeci, Fabien Kieken, Tom Lenaerts, Abel Garcia-Pino, Nico A. J. van Nuland, Lieven Buts, Structural Biology Brussels, Informatics and Applied Informatics, and Department of Bio-engineering Sciences

Subjects

0301 basic medicine, Circular dichroism, 030102 biochemistry & molecular biology, Gel filtration chromatography, Chemistry, Monomer/dimer, Size-exclusion chromatography, SH2 domain, Circular dichroism (CD), Homology (biology), 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, FYN, Monomer, Biophysics, genetics, Signal transduction, Nuclear magnetic resonance (NMR), Molecular Biology, Proto-oncogene tyrosine-protein kinase Src

Abstract

Src homology 2 (SH2) domains are key modulators in various signaling pathways allowing the recognition of phosphotyrosine sites of different proteins. Despite the fact that SH2 domains acquire their biological functions in a monomeric state, a multitude of reports have shown their tendency to dimerize. Here, we provide a technical description on how to isolate and characterize by gel filtration, circular dichroism (CD), and nuclear magnetic resonance (NMR) each conformational state of p59(fyn) SH2 domain.

Published

2017

4. 1H, 13C, and 15N backbone resonance assignments of the connexin43 carboxyl terminal domain attached to the 4th transmembrane domain in detergent micelles

Author

Fabien Kieken, Rosslyn Grosely, and Paul L. Sorgen

Subjects

Chemistry, Gap junction, Biochemistry, Domain (software engineering), Transmembrane domain, Terminal (electronics), Structural Biology, cardiovascular system, Biophysics, Membrane channel, Peptide sequence, Protein secondary structure, Function (biology)

Abstract

Gap junctions are specialized membrane channels that enable coordination of cellular functions and whole-organ responses by facilitating both molecular and electrical communication between neighboring cells. Connexin43 (Cx43) is the most widely expressed and well-studied gap junction protein. In the heart, Cx43 is essential for normal cardiac development and function. Studies using a soluble version of the Cx43 carboxyl-terminal domain (Cx43CT; S255-I382) have established the central role it plays in channel regulation. However, in purifying and characterizing a more ‘native-like’ construct (Cx43CT attached to the fourth transmembrane domain (TM4-Cx43CT; D196-I382)), we have identified that the TM4-Cx43CT is a better model than the soluble Cx43CT to further investigate the mechanisms governing Cx43 channel regulation. Here, we report the backbone 1H, 15N, and 13C assignments and predicted secondary structure of the TM4-Cx43CT. Assignment of the TM4-Cx43CT is a key step towards a better understanding of the structural basis of Cx43 regulation, which will lead to improved strategies for modulation of junctional communication that has been altered due to disease or ischemic injury.

Published

2012

5. Mechanism for modulation of gating of connexin26-containing channels by taurine

Author

Fabien Kieken, Andrew L. Harris, Liang Tao, Paul L. Sorgen, and Darren Locke

Subjects

HEPES, 0303 health sciences, Taurine, Physiology, Chemistry, 030302 biochemistry & molecular biology, Gap junction, Connexin, Gating, Cell junction, 03 medical and health sciences, chemistry.chemical_compound, Biochemistry, Cytoplasm, otorhinolaryngologic diseases, Biophysics, Homomeric, 030304 developmental biology

Abstract

The mechanisms of action of endogenous modulatory ligands of connexin channels are largely unknown. Previous work showed that protonated aminosulfonates (AS), notably taurine, directly and reversibly inhibit homomeric and heteromeric channels that contain Cx26, a widely distributed connexin, but not homomeric Cx32 channels. The present study investigated the molecular mechanisms of connexin channel modulation by taurine, using hemichannels and junctional channels composed of Cx26 (homomeric) and Cx26/Cx32 (heteromeric). The addition of a 28–amino acid “tag” to the carboxyl-terminal domain (CT) of Cx26 (Cx26T) eliminated taurine sensitivity of homomeric and heteromeric hemichannels in cells and liposomes. Cleavage of all but four residues of the tag (Cx26Tc) resulted in taurine-induced pore narrowing in homomeric hemichannels, and restored taurine inhibition of heteromeric hemichannels (Cx26Tc/Cx32). Taurine actions on junctional channels were fully consistent with those on hemichannels. Taurine-induced inhibition of Cx26/Cx32T and nontagged Cx26 junctional channels was blocked by extracellular HEPES, a blocker of the taurine transporter, confirming that the taurine-sensitive site of Cx26 is cytoplasmic. Nuclear magnetic resonance of peptides corresponding to Cx26 cytoplasmic domains showed that taurine binds to the cytoplasmic loop (CL) and not the CT, and that the CT and CL directly interact. ELISA showed that taurine disrupts a pH-dependent interaction between the CT and the CT-proximal half of the CL. These studies reveal that AS disrupt a pH-driven cytoplasmic interdomain interaction in Cx26-containing channels, causing closure, and that the Cx26CT has a modulatory role in Cx26 function.

Published

2011

6. Stabilization of a G-Quadruplex from Unfolding by Replication Protein A Using Potassium and the Porphyrin TMPyP4

Author

Fabien Kieken, Gloria E. O. Borgstahl, Luis A. Marky, and Aishwarya Prakash

Subjects

Article Subject, lcsh:QH426-470, Potassium, chemistry.chemical_element, Sequence (biology), Biology, 010402 general chemistry, G-quadruplex, Bioinformatics, 01 natural sciences, Biochemistry, lcsh:Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, lcsh:QD415-436, SsDNA binding, Molecular Biology, Replication protein A, 030304 developmental biology, 0303 health sciences, DNA replication, Porphyrin, 0104 chemical sciences, lcsh:Genetics, chemistry, Biophysics, DNA, Research Article

Abstract

Replication protein A (RPA) plays an essential role in DNA replication by binding and unfolding non-canonical single-stranded DNA (ssDNA) structures. Of the six RPA ssDNA binding domains (labeled A-F), RPA-CDE selectively binds a G-quadruplex forming sequence (5′-TAGGGGAAGGGTTGGAGTGGGTT-3′called Gq23). In K+, Gq23 forms a mixed parallel/antiparallel conformation, and in Na+Gq23 has a less stable (TMlowered by ∼20∘C), antiparallel conformation. Gq23 is intramolecular and 1D NMR confirms a stable G-quadruplex structure in K+. Full-length RPA and RPA-CDE-core can bind and unfold the Na+form of Gq23 very efficiently, but complete unfolding is not observed with the K+form. Studies with G-quadruplex ligands, indicate that TMPyP4 has a thermal stabilization effect on Gq23 in K+, and inhibits complete unfolding by RPA and RPA-CDE-core. Overall these data indicate that G-quadruplexes present a unique problem for RPA to unfold and ligands, such as TMPyP4, could possibly hinder DNA replication by blocking unfolding by RPA.

Published

2011

7. NMR structure note: UBA domain of CIP75

Author

Fabien Kieken, Paul L. Sorgen, Vivian Su, Gaelle Spagnol, and Alan F. Lau

Subjects

Magnetic Resonance Spectroscopy, Sequence Homology, Amino Acid, biology, Protein family, Chemistry, Protein subunit, Molecular Sequence Data, Proteins, Plasma protein binding, Biochemistry, Protein Structure, Secondary, Article, Protein Structure, Tertiary, Mice, PEST sequence, Ubiquitins, Proteasome, Ubiquitin, biology.protein, Animals, Amino Acid Sequence, Peptide sequence, Spectroscopy

Abstract

Ubiquitination is a post-translational process in eukaryotes that covalently modifies substrate proteins with ubiquitin. Ubiquitin can act as a tag that signals the protein-transport machinery to shuttle the protein to the proteasome for degradation. Within the ubiquitin receptor family of proteins is a group that can directly connect ubiquitinated proteins to the proteasome for degradation. Of these receptors, the best-studied are the ubiquitin-like (UBL)ubiquitin-associated (UBA) proteins, Rad23A, PLIC2, and Ddi1. These proteins contain an UBL domain that interacts with the proteasome and the UBA domain that recognizes mono and polyubiquitinated proteins [see review (Su and Lau 2009)]. Recently, a potentially new member of this UBL-UBA domain-containing protein family, named connexin43interacting protein of approximately 75 kDa (CIP75), was identified in a yeast-two hybrid screen (mouse embryonic c-DNA library) to interact with the gap junction protein connexin43 (Cx43) (Li et al. 2008). CIP75 contains an UBL domain at its N-terminus and an UBA domain at its C-terminus; as well as a heat shock chaperonin-binding domain and a PEST sequence. PEST sequences have been shown to direct the ubiquitination and subsequent degradation of proteins undergoing rapid turnover (Roth et al. 1998). CIP75 has 596 amino acids and exhibits high sequence homology (75%) with the human A1Up protein (Davidson et al. 2000). The general domain organization of CIP75 also shows high similarity with the UBL-UBA domain-containing protein family members Ubiquilin-1, PLIC2, Rad23A, Rad23B, and the yeast protein Dsk2 (Li et al. 2008). CIP75 functions in a similar manner as these family members in that the UBL domain of CIP75 is essential for the interaction with the S2/RPN1 and S5a/ RPN10 subunits of the 19S subunit from the 26S proteasome complex. However, the UBA domain may associate with non-ubiquitinated Cx43, and this interaction appears to still regulate the turnover of Cx43 through the proteasomal pathway (Li et al. 2008). UBA domains typically consist of approximately 45 amino acids and are characterized by relatively poor sequence conservation (Hofmann and Bucher 1996). UBA domains adopt a common, compact fold comprising a bundle of three helices and the hydrophobic surface formed by the C-terminus of a-helix 1, loop 1, and a-helix 3, is the principal interface with ubiquitin [see review (Hurley et al. 2006)]. Studies using the two UBA domains from HHR23A established that there are functional differences (i.e. differential protein partners) between UBA domains (Withers-Ward et al. 2000), suggesting the hydrophobic surface may be a more general protein–protein interaction module. Support for this is provided from a survey of the ubiquitin interaction properties of 30 UBA domains, which Fabien Kieken and Gaelle Spagnol contributed equally to this work.

Published

2010

8. Structural insight into the interaction of proteins containing NPF, DPF, and GPF motifs with the C-terminal EH-domain of EHD1

Author

Marco Tonelli, Naava Naslavsky, Steve Caplan, Paul L. Sorgen, Marko Jovic, and Fabien Kieken

Subjects

Membrane, Biochemistry, Chemistry, Stereochemistry, Ligand, Hydrogen bond, Endocytic cycle, Complex formation, Vesicular Transport Proteins, Tripeptide, Plasma protein binding, Molecular Biology

Abstract

Eps15 homology (EH)-domain containing proteins are regulators of endocytic membrane trafficking. EH-domain binding to proteins containing the tripeptide NPF has been well characterized, but recent studies have shown that EH-domains are also able to interact with ligands containing DPF or GPF motifs. We demonstrate that the three motifs interact in a similar way with the EH-domain of EHD1, with the NPF motif having the highest affinity due to the presence of an intermolecular hydrogen bond. The weaker affinity for the DPF and GPF motifs suggests that if complex formation occurs in vivo, they may require high ligand concentrations, the presence of successive motifs and/or specific flanking residues.

Published

2009

9. Eps15 Homology Domain 1-associated Tubules Contain Phosphatidylinositol-4-Phosphate and Phosphatidylinositol-(4,5)-Bisphosphate and Are Required for Efficient Recycling

Author

Steve Caplan, Paul L. Sorgen, Fabien Kieken, Naava Naslavsky, and Marko Jovic

Subjects

Phosphatidylinositol 4,5-Diphosphate, Magnetic Resonance Spectroscopy, Phosphatidylinositol 4-phosphate, Green Fluorescent Proteins, Phosphatidylinositol Phosphates, Vesicular Transport Proteins, Fluorescent Antibody Technique, Plasma protein binding, Biology, Phosphatidylinositols, Transfection, Endocytosis, Cell membrane, chemistry.chemical_compound, medicine, Humans, Binding site, Molecular Biology, Binding Sites, Microscopy, Confocal, Cell Membrane, Articles, Cell Biology, Cell biology, medicine.anatomical_structure, chemistry, Phosphatidylinositol 4,5-bisphosphate, Biochemistry, Mutation, RNA Interference, HeLa Cells, Protein Binding

Abstract

The C-terminal Eps15 homology domain (EHD) 1/receptor-mediated endocytosis-1 protein regulates recycling of proteins and lipids from the recycling compartment to the plasma membrane. Recent studies have provided insight into the mode by which EHD1-associated tubular membranes are generated and the mechanisms by which EHD1 functions. Despite these advances, the physiological function of these striking EHD1-associated tubular membranes remains unknown. Nuclear magnetic resonance spectroscopy demonstrated that the Eps15 homology (EH) domain of EHD1 binds to phosphoinositides, including phosphatidylinositol-4-phosphate. Herein, we identify phosphatidylinositol-4-phosphate as an essential component of EHD1-associated tubules in vivo. Indeed, an EHD1 EH domain mutant (K483E) that associates exclusively with punctate membranes displayed decreased binding to phosphatidylinositol-4-phosphate and other phosphoinositides. Moreover, we provide evidence that although the tubular membranes to which EHD1 associates may be stabilized and/or enhanced by EHD1 expression, these membranes are, at least in part, pre-existing structures. Finally, to underscore the function of EHD1-containing tubules in vivo, we used a small interfering RNA (siRNA)/rescue assay. On transfection, wild-type, tubule-associated, siRNA-resistant EHD1 rescued transferrin and β1 integrin recycling defects observed in EHD1-depleted cells, whereas expression of the EHD1 K483E mutant did not. We propose that phosphatidylinositol-4-phosphate is an essential component of EHD1-associated tubules that also contain phosphatidylinositol-(4,5)-bisphosphate and that these structures are required for efficient recycling to the plasma membrane.

Published

2009

10. Characterization of the pH-dependent Interaction between the Gap Junction Protein Connexin43 Carboxyl Terminus and Cytoplasmic Loop Domains

Author

Bethany J. Hirst-Jensen, Paul L. Sorgen, Fabien Kieken, Mario Delmar, and Prangya Sahoo

Subjects

Models, Molecular, Stereochemistry, Mutant, Peptide, Gating, Biochemistry, Protein Structure, Secondary, Structure-Activity Relationship, Protein structure, Animals, Humans, Structure–activity relationship, Receptor, Molecular Biology, chemistry.chemical_classification, Chemistry, Gap junction, Cell Biology, Hydrogen-Ion Concentration, Protein Structure, Tertiary, Amino Acid Substitution, Cytoplasm, Connexin 43, Biophysics, Dimerization, Protein Binding

Abstract

A prevailing view regarding the regulation of connexin43 (Cx43) gap junction channels is that, upon intracellular acidification, the carboxyl-terminal domain (Cx43CT) moves toward the channel opening to interact with specific residues acting as a receptor site. Previous studies have demonstrated a direct, pH-dependent interaction between the Cx43CT and a Cx43 cytoplasmic loop (Cx43CL) peptide. This interaction was dependent on alpha-helical formation for the peptide in response to acidification; more recent studies have shown that acidification also induces Cx43CT dimerization. Whether Cx43CT dimerization is an important structural component in Cx43 regulation remains to be determined. Here we used an assortment of complimentary biophysical techniques to characterize the binding of Cx43CT or its mutants to itself and/or to a more native-like Cx43CL construct (Cx43CL(100-155), residues 100-155). Our studies expand the observation that specific Cx43CT domains are important for dimerization. We further show that properties of the Cx43CL(100-155) are different from those of the Cx43CL peptide; solvent acidification leads to Cx43CL(100-155) oligomerization and a change in the stoichiometry and binding affinity for the Cx43CT. Homo-Cx43CT and Cx43CL(100-155) oligomerization as well as the Cx43CT/Cx43CL(100-155) interaction can occur under in vivo conditions; moreover, we show that Cx43CL(100-155) strongly affects resonance peaks corresponding to Cx43CT residues Arg-376-Asp-379 and Asn-343-Lys-346. Overall, our data indicate that many of the sites involved in Cx43CT dimerization are also involved in the Cx43CT/Cx43CL interaction; we further propose that chemically induced Cx43CT and Cx43CL oligomerization is important for the interaction between these cytoplasmic domains, which leads to chemically induced gating of Cx43 channels.

Published

2007

11. Structural Studies of the Nedd4 WW Domains and Their Selectivity for the Connexin43 (Cx43) Carboxyl Terminus

Author

Sydney Zach, Fabien Kieken, Rosslyn Grosely, Paul L. Sorgen, Jennifer L. Kopanic, Hanjun Li, Kelly L. Stauch, and Gaelle Spagnol

Subjects

0301 basic medicine, Stereochemistry, Nedd4 Ubiquitin Protein Ligases, Ubiquitin-Protein Ligases, NEDD4, Plasma protein binding, Biochemistry, Serine, 03 medical and health sciences, Ubiquitin, Animals, Phosphorylation, Molecular Biology, Nuclear Magnetic Resonance, Biomolecular, chemistry.chemical_classification, DNA ligase, 030102 biochemistry & molecular biology, biology, Endosomal Sorting Complexes Required for Transport, Cell Biology, Ubiquitin ligase, Protein Structure, Tertiary, Rats, 030104 developmental biology, chemistry, Connexin 43, Protein Structure and Folding, biology.protein, Protein Binding

Abstract

Neuronal precursor cell-expressed developmentally down-regulated 4 (Nedd4) was the first ubiquitin protein ligase identified to interact with connexin43 (Cx43), and its suppressed expression results in accumulation of gap junction plaques at the plasma membrane. Nedd4-mediated ubiquitination of Cx43 is required to recruit Eps15 and target Cx43 to the endocytic pathway. Although the Cx43 residues that undergo ubiquitination are still unknown, in this study we address other unresolved questions pertaining to the molecular mechanisms mediating the direct interaction between Nedd4 (WW1-3 domains) and Cx43 (carboxyl terminus (CT)). All three WW domains display a similar three antiparallel β-strand structure and interact with the same Cx43CT(283)PPXY(286)sequence. Although Tyr(286)is essential for the interaction, MAPK phosphorylation of the preceding serine residues (Ser(P)(279)and Ser(P)(282)) increases the binding affinity by 2-fold for the WW domains (WW2 > WW3 ≫ WW1). The structure of the WW2·Cx43CT(276-289)(Ser(P)(279), Ser(P)(282)) complex reveals that coordination of Ser(P)(282)with the end of β-strand 3 enables Ser(P)(279)to interact with the back face of β-strand 3 (Tyr(286)is on the front face) and loop 2, forming a horseshoe-shaped arrangement. The close sequence identity of WW2 with WW1 and WW3 residues that interact with the Cx43CT PPXY motif and Ser(P)(279)/Ser(P)(282)strongly suggests that the significantly lower binding affinity of WW1 is the result of a more rigid structure. This study presents the first structure illustrating how phosphorylation of the Cx43CT domain helps mediate the interaction with a molecular partner involved in gap junction regulation.

Published

2015

12. A model for the role of EHD1-containing membrane tubules in endocytic recycling

Author

Fabien Kieken, Paul L. Sorgen, Marko Jovic, Naava Naslavsky, Mahak Sharma, and Steve Caplan

Subjects

Receptor recycling, Phosphatidylinositol 4-phosphate, Mutant, Regulator, Endocytic recycling, Biology, Homology (biology), Article Addendum, Cell biology, chemistry.chemical_compound, Membrane, Phosphatidylinositol 4,5-bisphosphate, chemistry, General Agricultural and Biological Sciences

Abstract

The C-terminal Eps15 homology domain-containing protein, EHD1, is an important regulator of receptor recycling back to the plasma membrane. In addition to its vesicular localization, EHD1 also localizes to a unique array of tubular membrane structures that emanate from the endocytic recycling compartment. While these structures have been described over seven years ago, addressing their lipid composition and physiological function has been challenging. Moreover, it was not known whether EHD1 itself induces tubule formation, or whether it localizes to pre-existing tubular membrane structures. We have demonstrated that in vivo, EHD1 localizes to pre-existing tubular membranes that contain both phosphatidylinositol-4-phosphate and phosphatidylinositol-(4,5)-bisphosphate. Moreover, we have determined that ‘non-tubular’ EHD1 mutants with a single residue substitution do not efficiently facilitate receptor recycling. Our data suggest that EHD1-associated tubules are required for efficient recycling and we propose models that describe the potential mechanisms by which EHD1 functions.

Published

2009

13. Optimizing the Solution Conditions to Solve the Structure of the Connexin43 Carboxyl Terminus Attached to the 4th Transmembrane Domain in Detergent Micelles

Author

Fabien Kieken, Paul L. Sorgen, and Rosslyn Grosely

Subjects

Circular dichroism, Magnetic Resonance Spectroscopy, Clinical Biochemistry, Detergents, Model system, Gating, Micelle, Article, Domain (software engineering), Animals, Micelles, Channel gating, Chemistry, Circular Dichroism, Cell Biology, General Medicine, Nuclear magnetic resonance spectroscopy, Trifluoroethanol, Hydrogen-Ion Concentration, Recombinant Proteins, Protein Structure, Tertiary, Rats, Transmembrane domain, Biochemistry, Connexin 43, Biophysics

Abstract

pH-mediated gating of Cx43 channels following an ischemic event is believed to contribute to the development of lethal cardiac arrhythmias. Studies using a soluble version of the Cx43 carboxyl-terminal domain (Cx43CT; S255–I382) have established the central role it plays in channel regulation; however, research in the authors’ laboratory suggests that this construct may not be the ideal model system. Therefore, we have developed a more ‘native-like’ construct (Cx43CT attached to the 4th transmembrane domain [TM4-Cx43CT; G178–I382]) than the soluble Cx43CT to further investigate the mechanism(s) governing this regulation. Here, we utilize circular dichroism and nuclear magnetic resonance (NMR) were used to validate the TM4-Cx43CT for studying channel gating and optimize solution conditions for structural studies. The data indicate that, unlike the soluble Cx43-CT, the TM4-Cx43CT is structurally responsive to changes in pH, suggesting the presence of the TM4 facilitates pH-induced structural alterations. Additionally, the optimal solution conditions for solving the NMR solution structure include 10% 2,2,2 trifluoroethanol and removal of the 2nd extracellular loop (G178-V196).

Published

2010

14. EH domain of EHD1

Author

Naava Naslavsky, Marko Jovic, Steve Caplan, Paul L. Sorgen, and Fabien Kieken

Subjects

Protein family, Extramural, Chemistry, Molecular Sequence Data, Vesicular Transport Proteins, Endocytic recycling, Subcellular localization, Biochemistry, Solution structure, Homology (biology), Cell biology, Protein Structure, Tertiary, Protein structure, Humans, Amino Acid Sequence, Peptide sequence, Nuclear Magnetic Resonance, Biomolecular, Spectroscopy

Abstract

EHD1 is a member of the mammalian C-terminal Eps15 homology domain (EH) containing protein family, and regulates the recycling of various receptors from the endocytic recycling compartment to the plasma membrane. The EH domain of EHD1 binds to proteins containing either an Asn-Pro-Phe or Asp-Pro-Phe motif, and plays an important role in the subcellular localization and function of EHD1. Thus far, the structures of five N-terminal EH domains from other proteins have been solved, but to date, the structure of the EH domains from the four C-terminal EHD family paralogs remains unknown. In this study, we have assigned the 133 C-terminal residues of EHD1, which includes the EH domain, and solved its solution structure. While the overall structure resembles that of the second of the three N-terminal Eps15 EH domains, potentially significant differences in surface charge and the structure of the tripeptide-binding pocket are discussed.

Published

2007

15. (1)H, (13)C, and (15)N backbone resonance assignments of the carboxyl terminal domain of Connexin40

Author

Denis Bouvier, Fabien Kieken, and Paul L. Sorgen

Subjects

Carbon Isotopes, Magnetic Resonance Spectroscopy, Gap junction protein, Nitrogen Isotopes, Stereochemistry, Chemistry, Nuclear magnetic resonance spectroscopy, Resonance (chemistry), Biochemistry, Connexins, Domain (software engineering), Protein Structure, Tertiary, Terminal (electronics), Structural Biology, Intramolecular force, Amino Acid Sequence, Protons, Peptide sequence

Abstract

Connexin40 is a gap junction protein involved in cell communication in the heart and other tissues. The assignments of an important Connexin40 regulatory domain, the carboxyl terminus, will aid in identifying the types of inter- and intramolecular interactions that affect channel activity.

Published

2007

16. Effect of Charge Substitutions at Residue His-142 on Voltage Gating of Connexin43 Channels

Author

Paul L. Sorgen, Junko Shibayama, Steven M. Taffet, Cristina Gutiérrez, Akiko Seki, Jesús Requena Carrión, Fabien Kieken, Luis C. Barrio, Daniel González, and Mario Delmar

Subjects

Magnetic Resonance Spectroscopy, Patch-Clamp Techniques, Mutant, Molecular Sequence Data, Biophysics, Gating, Biology, Protein Structure, Secondary, 03 medical and health sciences, Xenopus laevis, 0302 clinical medicine, Animals, Histidine, Patch clamp, Channels, Receptors, and Electrical Signaling, Amino Acid Sequence, Protein secondary structure, Peptide sequence, 030304 developmental biology, Alanine, chemistry.chemical_classification, 0303 health sciences, Nuclear magnetic resonance spectroscopy, Recombinant Proteins, Amino acid, Protein Structure, Tertiary, Rats, chemistry, Biochemistry, Connexin 43, Mutation, Mutagenesis, Site-Directed, 030217 neurology & neurosurgery

Abstract

Previous studies indicate that the carboxyl terminal of connexin43 (Cx43CT) is involved in fast transjunctional voltage gating. Separate studies support the notion of an intramolecular association between Cx43CT and a region of the cytoplasmic loop (amino acids 119–144; referred to as “L2”). Structural analysis of L2 shows two α-helical domains, each with a histidine residue in its sequence (H126 and H142). Here, we determined the effect of H142 replacement by lysine, alanine, and glutamate on the voltage gating of Cx43 channels. Mutation H142E led to a significant reduction in the frequency of occurrence of the residual state and a prolongation of dwell open time. Macroscopically, there was a large reduction in the fast component of voltage gating. These results resembled those observed for a mutant lacking the carboxyl terminal (CT) domain. NMR experiments showed that mutation H142E significantly decreased the Cx43CT-L2 interaction and disrupted the secondary structure of L2. Overall, our data support the hypothesis that fast voltage gating involves an intramolecular particle-receptor interaction between CT and L2. Some of the structural constrains of fast voltage gating may be shared with those involved in the chemical gating of Cx43.

Published

2006

17. Identification of a novel peptide that interferes with the chemical regulation of connexin43

Author

Junko Shibayama, Paul L. Sorgen, Sejal Shah, Rebecca Lewandowski, Fabien Kieken, Steven M. Taffet, Wanda Coombs, and Mario Delmar

Subjects

Octanols, Phage display, Magnetic Resonance Spectroscopy, Patch-Clamp Techniques, Arginine, Physiology, Molecular Sequence Data, Peptide, Cell Communication, Biology, Binding, Competitive, Ion Channels, Protein structure, Peptide Library, Cell Line, Tumor, Animals, Amino Acid Sequence, Peptide library, Peptide sequence, chemistry.chemical_classification, Uncoupling Agents, Gap Junctions, Nuclear magnetic resonance spectroscopy, Surface Plasmon Resonance, Peptide Fragments, Amino acid, Protein Structure, Tertiary, chemistry, Biochemistry, Connexin 43, Cardiology and Cardiovascular Medicine, Carrier Proteins, Peptides, Acids

Abstract

The carboxyl-terminal domain of connexin43 (Cx43CT) is involved in various intra- and intermolecular interactions that regulate gap junctions. Here, we used phage display to identify novel peptidic sequences that bind Cx43CT and modify Cx43 regulation. We found that Cx43CT binds preferentially to peptides containing a sequence RXP, where X represents any amino acid and R and P correspond to the amino acids arginine and proline, respectively. A biased “RXP library” led to the identification of a peptide (dubbed “RXP-E”) that bound Cx43CT with high affinity. Nuclear magnetic resonance data showed RXP-E–induced shifts in the resonance peaks of residues 343 to 346 and 376 to 379 of Cx43CT. Patch-clamp studies revealed that RXP-E partially prevented octanol-induced and acidification-induced uncoupling in Cx43-expressing cells. Moreover, RXP-E increased mean open time of Cx43 channels. The full effect of RXP-E was dependent on the integrity of the CT domain. These data suggest that RXP-based peptides could serve as tools to help determine the role of Cx43 as a regulator of function in conditions such as ischemia-induced arrhythmias.

Published

2006

18. A new NMR solution structure of the SL1 HIV-1Lai loop-loop dimer

Author

Françoise Paquet, Gérard Lancelot, Fabien Kieken, Jacques Paoletti, Fabienne Brulé, Centre de biophysique moléculaire (CBM), and Université d'Orléans (UO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Chimie du CNRS (INC)

Subjects

Models, Molecular, 0303 health sciences, Base Sequence, Base pair, Dimer, 030302 biochemistry & molecular biology, Intermolecular force, RNA, Sequence (biology), Nuclear magnetic resonance spectroscopy of nucleic acids, Nuclear magnetic resonance spectroscopy, Biology, Article, 03 medical and health sciences, chemistry.chemical_compound, Crystallography, Heteronuclear molecule, chemistry, Genetics, HIV-1, Nucleic Acid Conformation, RNA, Viral, Dimerization, Nuclear Magnetic Resonance, Biomolecular, 030304 developmental biology

Abstract

Dimerization of genomic RNA is directly related with the event of encapsidation and maturation of the virion. The initiating sequence of the dimerization is a short autocomplementary region in the hairpin loop SL1. We describe here a new solution structure of the RNA dimerization initiation site (DIS) of HIV-1(Lai). NMR pulsed field-gradient spin-echo techniques and multidimensional heteronuclear NMR spectroscopy indicate that this structure is formed by two hairpins linked by six Watson-Crick GC base pairs. Hinges between the stems and the loops are stabilized by intra and intermolecular interactions involving the A8, A9 and A16 adenines. The coaxial alignment of the three A-type helices present in the structure is supported by previous crystallography analysis but the A8 and A9 adenines are found in a bulged in position. These data suggest the existence of an equilibrium between bulged in and bulged out conformations in solution.

Published

2006

19. HIV-1Lai genomic RNA: combined used of NMR and molecular dynamics simulation for studying the structure and internal dynamics of a mutated SL1 hairpin

Author

Eric Arnoult, Gérard Lancelot, Jacques Paoletti, Fabien Kieken, Florent Barbault, Daniel Genest, Tam Huynh-Dinh, Françoise Paquet, Centre de biophysique moléculaire (CBM), and Université d'Orléans (UO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Chimie du CNRS (INC)

Subjects

Models, Molecular, RNA, Spliced Leader, Macromolecular Substances, Base pair, Dimer, [SDV]Life Sciences [q-bio], Molecular Sequence Data, 030303 biophysics, Biophysics, Genome, Viral, Molecular dynamics, Motion, 03 medical and health sciences, chemistry.chemical_compound, [CHIM]Chemical Sciences, Computer Simulation, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Loop modeling, Nuclear Magnetic Resonance, Biomolecular, 030304 developmental biology, 0303 health sciences, Base Sequence, Molecular Structure, [SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], Nucleotides, RNA, HIV, Hydrogen Bonding, General Medicine, SL1, Stem-loop, NMR, [SDV.BBM.BP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biophysics, Crystallography, chemistry, Duplex (building), HIV-1, Mutagenesis, Site-Directed, Nucleic Acid Conformation, RNA, Viral, Protons, Two-dimensional nuclear magnetic resonance spectroscopy

Abstract

International audience; The genome of all retroviruses consists of two identical copies of an RNA sequence associated in a non-covalent dimer. A region upstream from the splice donor (SL1) comprising a self-complementary sequence is responsible for the initiation of the dimerization. This region is able to dimerize in two conformations: a loop-loop complex or an extended duplex. Here, we solve by 2D NMR techniques the solution structure of a 23-nucleotide sequence corresponding to HIV-1 SL1(Lai) in which the mutation G12-->A12 is included to prevent dimerization. It is shown that this monomer adopts a stem-loop conformation with a seven base pairs stem and a nine nucleotide loop containing the G10 C11 A12 C13 G14 C15 sequence. The stem is well structured in an A-form duplex, while the loop is more flexible even though elements of structure are evident. We show that the structure adopted by the stem can be appreciably different from its relaxed structure when the adenines A8, A9 and A16 in the loop are mechanically constrained. This point could be important for the efficiency of the dimerization. This experimental study is complemented with a 10 ns molecular dynamics simulation in the presence of counterions and explicit water molecules. This simulation brings about information on the flexibility of the loop, such as a hinge motion between the stem and the loop and a labile lattice of hydrogen bonds in the loop. The bases of the nucleotides G10 to C15 were found outside of the loop during a part of the trajectory, which is certainly necessary to initiate the dimerization process of the genuine SL1(Lai) sequence.

Published

2002

20. Chemical Gating Mechanism Of Connexin26-containing Channels By Aminosulfonate

Author

Liang Tao, Fabien Kieken, Darren Locke, Jade Liu, Paul L. Sorgen, and Andrew L. Harris

Subjects

chemistry.chemical_classification, Taurine, Taurine binding, Chemistry, Biophysics, Peptide, Gating, chemistry.chemical_compound, Biochemistry, Cytoplasm, otorhinolaryngologic diseases, Extracellular, Homomeric, Intracellular

Abstract

Protonated taurine directly and reversibly inhibits homomeric and heteromeric Cx26-containing hemichannels but not homomeric Cx32 hemichannels. It is unknown if taurine interacts with Cx26 and/or Cx32 in heteromeric channels, which domains are involved, or if junctional channels are taurine-sensitive. These issues were addressed with channels composed of Cx26 and/or Cx32 with/without cleavable 3KDa carboxyl-terminal (CT) tags (T). Hemichannel activity was assessed in liposomes, and by extracellular dye-uptake in cells. In contrast to untagged hemichannels, Cx26T/Cx32 and Cx26T hemichannels were not taurine-sensitive, but Cx26/Cx32T hemichannels were. Tag cleavage (Tc, leaving 4aa at the carboxyl-terminus) restored taurine-sensitivity of Cx26Tc/Cx32 hemichannels, but taurine surprisingly narrowed rather than closed Cx26Tc hemichannels. Thus, the 3KDa CT tag blocks taurine-sensitivity, unless hemichannels also contain Cx32, and the short 4aa CT extension affects Cx26Tc channel open state. Taurine effects on junctional channels were assessed by intercellular dye-coupling. Taurine substantially reduced dye-coupling by Cx26 and Cx26/Cx32T channels, but not by Cx26T, Cx26T/Cx32 or Cx32T channels. Junctional channels therefore have identical taurine-sensitivity as their component hemichannels. An intracellular site for taurine action was shown by a membrane-impermeable blocker of taurine uptake. Thus, all data indicate taurine-induced pore closure utilizes the Cx26 CT. Taurine binding to Cx26-CT was assessed by natural-abundance 13C-HMQC-NMR. Overlapping resonances of Cx26-CT peptide in the presence and absence of taurine indicate no direct taurine binding to Cx26-CT. Peptide ‘elisa’ showed a pH dependent interaction occurs between Cx26-CT and the carboxyl-terminal 20aa of the Cx26 cytoplasmic loop (Cx26-CL). Acidification increases the binding affinity of Cx26-CL and Cx26-CT peptides, and only the protonated form of taurine negatively affects this interaction, suggesting that its disruption leads to channel closure. Structural analysis of Cx26-CT and Cx26-CL peptides in the presence and absence of taurine are ongoing. Supported by GM36044, DC7470.

Published

2009

21. Purification And Reconstitution Of The Connexin43 Carboxyl Terminus Attached To The 4Th Transmembrane Domain In Detergent Micelles

Author

Paul L. Sorgen, Fabien Kieken, Rosslyn Grosely, Admir Kellezi, and Gloria E. O. Borgstahl

Subjects

Circular dichroism, Protein Folding, Protein Conformation, Detergents, Biophysics, 010402 general chemistry, 01 natural sciences, SH3 domain, Article, Cell membrane, 03 medical and health sciences, Protein structure, 0302 clinical medicine, medicine, Animals, Micelles, 030304 developmental biology, 0303 health sciences, Chemistry, Peripheral membrane protein, Cell Membrane, 0104 chemical sciences, Protein Structure, Tertiary, Rats, Transmembrane domain, medicine.anatomical_structure, Biochemistry, Membrane protein, Connexin 43, Protein folding, 030217 neurology & neurosurgery, Biotechnology

Abstract

In recent years, reports have identified that many eukaryotic proteins contain disordered regions spanning greater than 30 consecutive residues in length. In particular, a number of these intrinsically disordered regions occur in the cytoplasmic segments of plasma membrane proteins. These intrinsically disordered regions play important roles in cell signaling events, as they are sites for protein-protein interactions and phosphorylation. Unfortunately, in many crystallographic studies of membrane proteins, these domains are removed because they hinder the crystallization process. Therefore, a purification procedure was developed to enable the biophysical and structural characterization of these intrinsically disordered regions while still associated with the lipid environment. The carboxyl terminal domain from the gap junction protein connexin43 attached to the 4th transmembrane domain (TM4-Cx43CT) was used as a model system (residues G178-I382). The purification was optimized for structural analysis by nuclear magnetic resonance (NMR) because this method is well suited for small membrane proteins and proteins that lack a well-structured three-dimensional fold. The TM4-Cx43CT was purified to homogeneity with a yield of approximately 6 mg/L from C41(DE3) bacterial cells, reconstituted in the anionic detergent 1-palmitoyl-2-hydroxy-sn-glycero-3-[phospho-RAC-(1-glycerol)], and analyzed by circular dichroism and NMR to demonstrate that the TM4-Cx43CT was properly folded into a functional conformation by its ability to form alpha-helical structure and associate with a known binding partner, the c-Src SH3 domain, respectively.

22. Structural Determination of the Carboxyl Terminal Domain from the Gap Junction Protein Connexin45

Author

Jennifer L. Kopanic, Paul L. Sorgen, and Fabien Kieken

Subjects

Gap Junction Proteins, Circular dichroism, Biochemistry, Gap junction protein, Chemistry, Second messenger system, Biophysics, Gap junction, Homomeric, Nuclear magnetic resonance spectroscopy, Small molecule

Abstract

Gap junctions are intercellular channels that enable ions, small molecules, and second messenger metabolites to travel between adjacent cells. Gap junctions provide a pathway for molecules involved in growth, regulation, and development. In the cardiac conduction system, they are critical for impulse propagation. Alterations in the gap junction proteins or connexins (Cx) are associated with life threatening arrhythmias. The major connexins in the heart are Cx40, Cx43, and Cx45. Previous studies have shown that these connexins are able to interact causing the formation of heteromeric gap junction channels, which have different biophysical properties than homomeric channels. The mechanisms involved in the regulation of these heteromeric channels are still largely unknown, but recent evidence supports involvement of their carboxyl terminal (CT) domains. Our laboratory has focused biophysical studies on the Cx43CT and Cx40CT domains, and here we have extended our studies to the Cx45CT. Using different biophysical methods, including NMR spectroscopy and Circular Dichroism, we have found that the Cx45CT is predominately unstructured, like the Cx43CT and Cx40CT domains. Ongoing studies are focused on identifying if hetero-CT domain interactions are involved in the regulation of heteromeric channels.