Your search keyword '"NE, nuclear envelope"' showing total 26 results

1. Characterization of a Unique Form of Arrhythmic Cardiomyopathy Caused by Recessive Mutation in LEMD2

Author

Paul M. K. Gordon, Ruping Chen, Patrick Frosk, Stephanie Clarke, Davinder S. Jassal, Nelly Abdelfatah, Colette M. Seifer, Cathleen Huculak, Brenda Gerull, Henry J. Duff, Robin Clegg, Carole Ober, and Ilan Buffo

Subjects

0301 basic medicine, Premature aging, Pathology, medicine.medical_specialty, EMD, emerin, LEMD2, ACM, arrhythmogenic cardiomyopathy, Population, PBS, phosphate-buffered saline, Cardiomyopathy, sudden death, SAHF, senescence-associated heterochromatin foci, 030204 cardiovascular system & hematology, Sudden death, inner nuclear membrane, LMNA, lamin A/C, chromatin remodeling, Sudden cardiac death, PRECLINICAL RESEARCH, 03 medical and health sciences, DNA, deoxyribonucleic acid, 0302 clinical medicine, CMR, cardiac magnetic resonance, Fibrosis, medicine, education, DCM, dilated cardiomyopathy, LV, left ventricular, education.field_of_study, LGE, late gadolinium enhancement, BANF, barrier to autointegration factor, SNV, single nucleotide variant, business.industry, Dilated cardiomyopathy, medicine.disease, ICD, implantable cardioverter-defibrillator, DAPI, 4′,6′-diamidino-2-phenylindole, dilated cardiomyopathy, P, passage, 030104 developmental biology, medicine.anatomical_structure, eGFP, enhanced green fluorescent protein, Ventricle, NE, nuclear envelope, Cardiology and Cardiovascular Medicine, business, LEMD2, LEM domain containing protein 2

Abstract

Visual Abstract, Highlights • The homozygous c.38T>G mutation in the LEMD2 gene causes arrhythmic cardiomyopathy with bilateral juvenile cataract in the Hutterite population. • The cardiac phenotype is characterized by localized inferior and inferolateral fibrosis of the left ventricle and mild impairment of left ventricular systolic function but severe ventricular arrhythmias leading to sudden cardiac death. • Affected heart tissue and fibroblasts exhibit abnormally shaped nuclei with condensed peripheral heterochromatin. • Functional assays on affected fibroblasts show decreased proliferation capacity, cellular senescence, and a prolonged G1 phase, suggesting premature aging and cellular senescence in proliferating cells., Summary Nuclear envelope proteins have been shown to play an important role in the pathogenesis of inherited dilated cardiomyopathy. Here, we present a remarkable cardiac phenotype caused by a homozygous LEMD2 mutation in patients of the Hutterite population with juvenile cataract. Mutation carriers develop arrhythmic cardiomyopathy with mild impairment of left ventricular systolic function but severe ventricular arrhythmias leading to sudden cardiac death. Affected cardiac tissue from a deceased patient and fibroblasts exhibit elongated nuclei with abnormal condensed heterochromatin at the periphery. The patient fibroblasts demonstrate cellular senescence and reduced proliferation capacity, which may suggest an involvement of LEM domain containing protein 2 in chromatin remodeling processes and premature aging.

Published

2019

2. Quantified effects of chromosome-nuclear envelope attachments on 3D organization of chromosomes.

Author

Kinney, Nicholas Allen, Onufriev, Alexey V, and Sharakhov, Igor V

Subjects

*CHROMOSOMES, *NUCLEAR membranes, *CENTRAL processing units, *DROSOPHILA melanogaster, *POLYMERS

Abstract

We use a combined experimental and computational approach to study the effects of chromosome-nuclear envelope (Chr-NE) attachments on the 3D genome organization ofDrosophila melanogaster(fruit fly) salivary gland nuclei. We consider 3 distinct models: a Null model – without specific Chr-NE attachments, a 15-attachment model – with 15 previously known Chr-NE attachments, and a 48-attachment model – with 15 original and 33 recently identified Chr-NE attachments. The radial densities of chromosomes in the models are compared to the densities observed in 100 experimental images of optically sectioned salivary gland nuclei forming “z-stacks.” Most of the experimental z-stacks support the Chr-NE 48-attachment model suggesting that as many as 48 chromosome loci with appreciable affinity for the NE are necessary to reproduce the experimentally observed distribution of chromosome density in fruit fly nuclei. Next, we investigate if and how the presence and the number of Chr-NE attachments affect several key characteristics of 3D genome organization: chromosome territories and gene-gene contacts. This analysis leads to novel insight about the possible role of Chr-NE attachments in regulating the genome architecture. Specifically, we find that model nuclei with more numerous Chr-NE attachments form more distinct chromosome territories and their chromosomes intertwine less frequently. Intra-chromosome and intra-arm contacts are more common in model nuclei with Chr-NE attachments compared to the Null model (no specific attachments), while inter-chromosome and inter-arm contacts are less common in nuclei with Chr-NE attachments. We demonstrate that Chr-NE attachments increase the specificity of long-range inter-chromosome and inter-arm contacts. The predicted effects of Chr-NE attachments are rationalized by intuitive volumevs.surface accessibility arguments. [ABSTRACT FROM PUBLISHER]

Published

2015

3. ESCRTs breach the nuclear border.

Author

Webster, Brant M and Lusk, C Patrick

Subjects

*NUCLEAR membranes, *NUCLEAR pore complex, *QUALITY control, *ENDOSOMES, *MEMBRANE proteins

Abstract

The endosomal sorting complexes required for transport (ESCRT) are best known for their role in sorting ubiquitylated membrane proteins into endosomes. The most ancient component of the ESCRT machinery is ESCRT-III, which is capable of oligomerizing into a helical filament that drives the invagination and scission of membranes aided by the AAA ATPase, Vps4, in several additional subcellular contexts. Our recent study broadens the work of ESCRT-III by identifying its role in a quality control pathway at the nuclear envelope (NE) that ensures the normal biogenesis of nuclear pore complexes (NPCs). Here, we will elaborate on how we envision this mechanism to progress and incorporate ESCRT-III into an emerging model of nuclear pore formation. Moreover, we speculate there are additional roles for the ESCRT-III machinery at the NE that broadly function to ensure its integrity and the maintenance of the nuclear compartment. [ABSTRACT FROM PUBLISHER]

Published

2015

4. Plant nuclear shape is independently determined by the SUN-WIP-WIT2-myosin XI-i complex and CRWN1.

Author

Zhou, Xiao, Groves, Norman Reid, and Meier, Iris

Subjects

*CELL nuclei, *PLANT development, *ARABIDOPSIS, *MYOSIN, *NUCLEAR membranes, *CYTOSKELETON

Abstract

Nuclei undergo dynamic shape changes during plant development, but the mechanism is unclear. In Arabidopsis, Sad1/UNC-84 (SUN) proteins, WPP domain-interacting proteins (WIPs), WPP domain-interacting tail-anchored proteins (WITs), myosin XI-i, and CROWDED NUCLEI 1 (CRWN1) have been shown to be essential for nuclear elongation in various epidermal cell types. It has been proposed that WITs serve as adaptors linking myosin XI-i to the SUN-WIP complex at the nuclear envelope (NE). Recently, an interaction between Arabidopsis SUN1 and SUN2 proteins and CRWN1, a plant analog of lamins, has been reported. Therefore, the CRWN1-SUN-WIP-WIT-myosin XI-i interaction may form a linker of the nucleoskeleton to the cytoskeleton complex. In this study, we investigate this proposed mechanism in detail for nuclei of Arabidopsis root hairs and trichomes. We show that WIT2, but not WIT1, plays an essential role in nuclear shape determination by recruiting myosin XI-i to the SUN-WIP NE bridges. Compared with SUN2, SUN1 plays a predominant role in nuclear shape. The NE localization of SUN1, SUN2, WIP1, and a truncated WIT2 does not depend on CRWN1. While crwn1 mutant nuclei are smooth, the nuclei of sun or wit mutants are invaginated, similar to the reported myosin XI-i mutant phenotype. Together, this indicates that the roles of the respective WIT and SUN paralogs have diverged in trichomes and root hairs, and that the SUN-WIP-WIT2-myosin XI-i complex and CRWN1 independently determine elongated nuclear shape. This supports a model of nuclei being shaped both by cytoplasmic forces transferred to the NE and by nucleoplasmic filaments formed under the NE. [ABSTRACT FROM AUTHOR]

Published

2015

5. Purification of nuclear localization signal-containing proteins and its application to investigation of the mechanisms of the cell division cycle.

Author

Christodoulou, Andri and Yokoyama, Hideki

Subjects

*NUCLEAR proteins, *SEPARATION technology equipment, *CELL lines, *GUANOSINE triphosphatase, *CELLULAR signal transduction, *MITOSIS regulation, *CELL division

Abstract

The GTP bound form of the Ran GTPase (RanGTP) in the nucleus promotes nuclear import of the proteins bearing nuclear localization signals (NLS). When nuclear envelopes break down during mitosis, RanGTP is locally produced around chromosomes and drives the assembly of the spindle early in mitosis and the nuclear envelope (NE) later. RanGTP binds to the heterodimeric nuclear transport receptor importin α/β and releases NLS proteins from the receptor. Liberated NLS proteins around chromosomes have been shown to play distinct, essential roles in spindle and NE assembly. Here we provide a highly specific protocol to purify NLS proteins from crude cell lysates. The pure NLS fraction is an excellent resource to investigate the NLS protein function and identify new mitotic regulators, uncovering fundamental mechanisms of the cell division cycle. It takes 2–3 days to obtain the NLS fraction. [ABSTRACT FROM PUBLISHER]

Published

2015

6. Structural characterization of altered nucleoporin Nup153 expression in human cells by thin-section electron microscopy.

Author

Duheron, Vincent, Chatel, Guillaume, Sauder, Ursula, Oliveri, Vesna, and Fahrenkrog, Birthe

Subjects

*NUCLEOPORINS, *NUCLEAR pore complex, *HUMAN cell nuclei, *ELECTRON microscopy, *NUCLEAR membranes, *NUCLEOCYTOPLASMIC interactions, *MACROMOLECULES

Abstract

Nuclear pore complexes (NPCs) span the 2 membranes of the nuclear envelope (NE) and facilitate nucleocytoplasmic exchange of macromolecules. NPCs have a roughly tripartite structural organization with the so-called nuclear basket emanating from the NPC scaffold into the nucleoplasm. The nuclear basket is composed of the 3 nucleoporins Nup153, Nup50, and Tpr, but their specific role for the structural organization of this NPC substructure is, however, not well established. In this study, we have used thin-section transmission electron microscopy to determine the structural consequences of altering the expression of Nup153 in human cells. We show that the assembly and integrity of the nuclear basket is not affected by Nup153 depletion, whereas its integrity is perturbed in cells expressing high concentrations of the zinc-finger domain of Nup153. Moreover, even mild over-expression of Nup153 is coinciding with massive changes in nuclear organization and it is the excess of the zinc-finger domain of Nup153 that is sufficient to induce these rearrangements. Our data indicate a central function of Nup153 in the organization of the nucleus, not only at the periphery, but throughout the entire nuclear interior. [ABSTRACT FROM AUTHOR]

Published

2014

7. Cellular stress induces Bax-regulated nuclear bubble budding and rupture followed by nuclear protein release.

Author

Lindenboim, Liora, Sasson, Tiki, Worman, Howard J, Borner, Christoph, and Stein, Reuven

Subjects

*NUCLEAR proteins, *BAX protein, *APOPTOTIC bodies, *CYTOPLASM, *NUCLEAR membranes, *PHYSIOLOGICAL stress, *LAMINS, *APOPTOSIS

Abstract

Cellular stress triggers many pathways including nuclear protein redistribution. We previously discovered that this process is regulated by Bax but the underlying mechanism has not yet been studied. Here we define this mechanism by showing that apoptotic stimuli cause Bax-regulated disturbances in lamin A/C and nuclear envelope (NE)-associated proteins which results in the generation and subsequent rupture of nuclear protein-containing bubbles. The bubbles do not contain DNA and are encapsulated by impaired nuclear pore-depleted NE. Stress-induced generation and rupture of nuclear bubbles ultimately leads to the discharge of nuclear proteins into the cytoplasm. This process precedes morphological changes of apoptosis and occurs independently of caspases. Rescue experiments revealed that this Bax effect is non-canonical, i.e. it requires the BH3 domain and α-helices 5 and 6 but it is not inhibited by Bcl-xL. Targeting Bax to the NE by the Klarsicht/ANC-1/Syne-1 homology (KASH) domain effectively triggers the generation and rupture of nuclear bubbles. Overall, our findings provide evidence for a novel stress-response, which is regulated by a non-canonical action of Bax on the NE. [ABSTRACT FROM AUTHOR]

Published

2014

8. Ongoing replication forks delay the nuclear envelope breakdown upon mitotic entry

Author

Hirofumi Tanaka and Yoshitami Hashimoto

Subjects

0301 basic medicine, Aphidicolin, DNA Replication, Nuclear Envelope, CDK, nuclear envelope breakdown (NEB), Mitosis, Biology, Wee1/Myt1, Biochemistry, Xenopus egg extract, 03 medical and health sciences, chemistry.chemical_compound, Xenopus laevis, p97i, p97 inhibitor, Animals, Molecular Biology, S phase, NEB, nuclear envelope breakdown, 030102 biochemistry & molecular biology, Cell-Free System, replisome, Ara-CTP, Ara-cytidine-5′-triphosphate, CDKs, cyclin-dependent kinases, DNA replication, M-CDK, M-phase CDK, replication forks, Cell Biology, Cell cycle, Chromatin, Cell biology, Wee1, ex-dCTP, excessive amounts of dCTP, 030104 developmental biology, chemistry, S-extract, S-phase extract, biology.protein, M-extract, M-phase extract, NE, nuclear envelope, Replisome, PD, PD166285, Pre-RCs, prereplicative complex, MiDAS, mitotic DNA synthesis, Research Article

Abstract

DNA replication is a major contributor to genomic instability, and protection against DNA replication perturbation is essential for normal cell division. Certain types of replication stress agents, such as aphidicolin and hydroxyurea, have been shown to cause reversible replication fork stalling, wherein replisome complexes are stably maintained with competence to restart in the S phase of the cell cycle. If these stalled forks persist into the M phase without a replication restart, replisomes are disassembled in a p97-dependent pathway and under-replicated DNA is subjected to mitotic DNA repair synthesis. Here, using Xenopus egg extracts, we investigated the consequences that arise when stalled forks are released simultaneously with the induction of mitosis. Ara-cytidine-5'-triphosphate-induced stalled forks were able to restart with the addition of excess dCTP during early mitosis before the nuclear envelope breakdown (NEB). However, stalled forks could no longer restart efficiently after the NEB. Although replisome complexes were finally disassembled in a p97-dependent manner during mitotic progression whether or not fork stalling was relieved, the timing of the NEB was delayed with the ongoing forks, rather than the stalled forks, and the delay was dependent on Wee1/Myt1 kinase activities. Thus, ongoing DNA replication was found to be directly linked to the regulation of Wee1/Myt1 kinases to modulate cyclin-dependent kinase activities because of which DNA replication and mitosis occur in a mutually exclusive and sequential manner.

Published

2020

9. p63 Transcription Factor Regulates Nuclear Shape and Expression of Nuclear Envelope-Associated Genes in Epidermal Keratinocytes

Author

Krzysztof Poterlowicz, Andrei N. Mardaryev, I. Malashchuk, Vladimir A. Botchkarev, Michael Y. Fessing, Iakowos Karakesisoglou, Inemo E. Asamaowei, Andrey A. Sharov, and Valentina Rapisarda

Subjects

Keratinocytes, 0301 basic medicine, H3K27me3, trimethylation on lysine 27 of histone H3, NM, nuclear membrane, Transcription, Genetic, Nuclear Envelope, Dermatology, Biology, Biochemistry, Mice, 03 medical and health sciences, Histone H3, Gene expression, Keratinocytes/Epidermis, Animals, Humans, Molecular Biology, Transcription factor, Nuclear receptor co-repressor 1, Nuclear receptor co-repressor 2, Cell Nucleus, IF, intermediate filament, integumentary system, CC, chromocenter, Gene Expression Regulation, Developmental, Cell Differentiation, Promoter, Cell Biology, H3K9me3, trimethylation on lysine 9 of histone H3, Phosphoproteins, WT, wild-type, Molecular biology, PMK, primary mouse keratinocyte, Chromatin, 030104 developmental biology, Models, Animal, NE, nuclear envelope, Trans-Activators, RNA, Original Article, KtyII, keratin type II, Epidermis, ChIP-qPCR, chromatin immunoprecipitation-quantitative PCR, KtyI, keratin type I, Lamin, Transcription Factors

Abstract

The maintenance of a proper nuclear architecture and three-dimensional organization of the genes, enhancer elements, and transcription machinery plays an essential role in tissue development and regeneration. Here we show that in the developing skin, epidermal progenitor cells of mice lacking p63 transcription factor display alterations in the nuclear shape accompanied by a marked decrease in expression of several nuclear envelope-associated components (Lamin B1, Lamin A/C, Sun1, Nesprin-3, Plectin) compared with controls. Furthermore, chromatin immunoprecipitation-quantitative PCR assay showed enrichment of p63 on Sun1, Syne3, and Plec promoters, suggesting them as p63 targets. Alterations in the nuclei shape and expression of nuclear envelope-associated proteins were accompanied by altered distribution patterns of the repressive histone marks trimethylation on lysine 27 of histone H3, trimethylation on lysine 9 of histone H3, and heterochromatin protein 1-alpha in p63-null keratinocytes. These changes were also accompanied by downregulation of the transcriptional activity and relocation of the keratinocyte-specific gene loci away from the sites of active transcription toward the heterochromatin-enriched repressive nuclear compartments in p63-null cells. These data demonstrate functional links between the nuclear envelope organization, chromatin architecture, and gene expression in keratinocytes and suggest nuclear envelope-associated genes as important targets mediating p63-regulated gene expression program in the epidermis.

Published

2017

10. Presence of the inositol 1,4,5-triphosphate receptor isoforms in the nucleoplasm

Author

Huh, Yang Hoon and Yoo, Seung Hyun

Subjects

*INOSITOL, *CALCIUM, *ENDOPLASMIC reticulum, *CHROMATIN

Abstract

Although the inositol 1,4,5-triphosphate (IP3)-induced nuclear Ca2+ release has been shown to play key roles in nuclear functions, the presence of IP3 receptor (IP3R)/Ca2+ channels in the nucleoplasm has not been found. Recently, the IP3R/Ca2+ channels were reported to exist in the nucleoplasmic reticulum structure, an extension of the nuclear envelope. Here we investigated the potential existence of the IP3Rs in the nucleoplasm and found the presence of all three IP3R isoforms in neuroendocrine and non-neuroendocrine cells. The IP3Rs were widely scattered in the nucleoplasm, localizing in both the heterochromatin and euchromatin regions. [Copyright &y& Elsevier]

Published

2003

11. Cryo-electron Tomography Provides Novel Insights into Nuclear Pore Architecture: Implications for Nucleocytoplasmic Transport

Author

Stoffler, Daniel, Feja, Bernhard, Fahrenkrog, Birthe, Walz, Jochen, Typke, Dieter, and Aebi, Ueli

Subjects

*ELECTRON microscopy, *TOMOGRAPHY

Abstract

To go beyond the current structural consensus model of the nuclear pore complex (NPC), we performed cryo-electron tomography of fully native NPCs from Xenopus oocyte nuclear envelopes (NEs). The cytoplasmic face of the NPC revealed distinct anchoring sites for the cytoplasmic filaments, whereas the nuclear face was topped with a massive distal ring positioned above the central pore with indications of the anchoring sites for the nuclear basket filaments and putative intranuclear filaments. The rather “spongy” central framework of the NPC was perforated by an elaborate channel and void system, and at the membrane pore interface it exhibited distinct “handles” protruding into the lumen of the NE. The most variable structural moiety of the NPC was a rather tenuous central plug partially obstructing the central pore. Its mobile character was documented by time-lapse atomic force microscopy. Taken together, the new insights we gained into NPC structure support the notion that the NPC acts as a constrained diffusion pore for molecules and particles without retention signal and as an affinity gate for signal-bearing cargoes. [Copyright &y& Elsevier]

Published

2003

12. Identification of the evolutionarily conserved nuclear envelope proteins Lem2 and MicLem2 in Tetrahymena thermophila

Author

Tokuko Haraguchi, Yasuhiro Fukuda, Chie Mori, Hiroko Osakada, Yasushi Hiraoka, and Masaaki Iwamoto

Subjects

0301 basic medicine, BAF, barrier-to-autointegration factor, LEM, LAP2-Emerin-MAN1, Man1-Src1p-C-terminal domain, MAC, macronucleus, PB, phosphate buffer, medicine.disease_cause, Nuclear envelope, 0302 clinical medicine, Nuclear dimorphism, Nuclear pore, MSC domain, Macronucleus, biology, Protist, Tetrahymena, General Medicine, LAP2, lamina associated polypeptide 2, Transmembrane protein, Cell biology, HeH domain, 030220 oncology & carcinogenesis, Man1, GA, glutaraldehyde, MSC, Man1-Src1p-C-terminal, lcsh:QH426-470, Immunoelectron microscopy, DAPI, 4′,6‑diamidino‑2‑phenylindole, NPC, nuclear pore complex, LEM domain, Article, ER, endoplasmic reticulum, 03 medical and health sciences, PBS, phosphate buffered saline, ONM and INM, outer and inner nuclear membranes, Genetics, medicine, Ciliate, HeH, helix-extension-helix, EDTA, ethylenediaminetetraacetic acid, biology.organism_classification, RRM, RNA recognition motif, lcsh:Genetics, 030104 developmental biology, NLS, nuclear localization signal, DDW, double distilled water, NE, nuclear envelope, MIC, micronucleus, TM, transmembrane

Abstract

Lem2 family proteins, i.e. the LAP2-Emerin-MAN1 (LEM) domain-containing nuclear envelope proteins, are well-conserved from yeasts to humans, both of which belong to the Opisthokonta supergroup. However, whether their homologs are present in other eukaryotic phylogenies remains unclear. In this study, we identified two Lem2 homolog proteins, which we named as Lem2 and MicLem2, in a ciliate Tetrahymena thermophila belonging to the SAR supergroup. Lem2 was localized to the nuclear envelope of the macronucleus (MAC) and micronucleus (MIC), while MicLem2 was exclusively localized to the nuclear envelope of the MIC. Immunoelectron microscopy revealed that Lem2 in T. thermophila was localized to both the inner and outer nuclear envelopes of the MAC and MIC, while MicLem2 was mostly localized to the nuclear pores of the MIC. Molecular domain analysis using GFP-fused protein showed that the N-terminal and luminal domains, including the transmembrane segments, are responsible for nuclear envelope localization. During sexual reproduction, enrichment of Lem2 occurred in the nuclear envelopes of the MAC and MIC to be degraded, while MicLem2 was enriched in the nuclear envelope of the MIC that escaped degradation. These findings suggest the unique characteristics of Tetrahymena Lem2 proteins. Our findings provide insight into the evolutionary divergence of nuclear envelope proteins., Graphical abstract Unlabelled Image, Highlights • Conserved nuclear envelope proteins Lem2 and MicLem2 are identified in Tetrahymena. • Lem2 is localized to the nuclear envelope of the macronucleus and the micronucleus. • MicLem2 is localized to the nuclear pore complex of the micronucleus. • In sexual reproduction, Lem2 is enriched to the nuclei assigned to degradation. • MicLem2 is enriched to the micronuclei that are escaped from degradation.

Published

2019

13. ATR-mediated regulation of nuclear and cellular plasticity

Author

Gururaj Rao Kidiyoor, Amit Kumar, and Marco Foiani

Subjects

0301 basic medicine, DNA Repair, Nuclear Envelope, Nucleolus, DNA repair, DNA damage, Cell Plasticity, Ataxia Telangiectasia Mutated Proteins, Biology, Biochemistry, Article, DDR, DNA damage response, PIKK, Phosphatidylinositol 3-Kinase-related Kinases, 03 medical and health sciences, PIKK, PTM, Post Translation Modification, medicine, Humans, ATR, Ataxia Telangiectasia and Rad3-related, NE, Nuclear Envelope, Molecular Biology, Centrosome, ATRIP, ATR interacting protein, Kinase, RPA, Replication Protein A, FAT, domainFRAP-ATM-TRRAP domain, DNA, Cell Biology, Cellular plasticity, medicine.disease, Cell biology, Eukaryotic Cells, ssDNA, single stranded DNA, ATR, 030104 developmental biology, Ataxia-telangiectasia, HEAT, Huntingtin, Elongation factor 3 Alpha-regulatory subunit of protein phosphatase 2A and TOR1, Cell Nucleolus, DNA Damage

Abstract

ATR (Ataxia Telangiectasia and Rad3-related) is a member of the Phosphatidylinositol 3-kinase-related kinases (PIKKs) family, amongst six other vertebrate proteins known so far. ATR is indispensable for cell survival and its essential role is in sensing DNA damage and initiating appropriate repair responses. In this review we highlight emerging and recent observations connecting ATR to alternative roles in controlling the nuclear envelope, nucleolus, centrosome and other organelles in response to both internal and external stress conditions. We propose that ATR functions control cell plasticity by sensing structural deformations of different cellular components, including DNA and initiating appropriate repair responses, most of which are yet to be understood completely.

Published

2016

14. Lamina-associated polypeptide (LAP)2α and nucleoplasmic lamins in adult stem cell regulation and disease

Author

Gesson, Kevin, Vidak, Sandra, and Foisner, Roland

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, BAF, barrier-to-autointegration factor, MDPSC, muscle-derived stem/progenitor cells, animal structures, ESC, embryonic stem cell, LEM, LAP2-Emerin-Man1, MSC, mesenchymal stem cell, Review, Nuclear envelopathies, FPLD, familial partial lipodystrophy, Retinoblastoma Protein, Muscular Dystrophies, Nuclear envelope, LAD, lamina-associated domain, Mice, Progeria, LAP, lamina-associated polypeptide, Animals, Humans, Nucleoplasmins, Dam, DNA adenine methyltransferase, DCM, dilated cardiomyopathy, Cell Proliferation, Adult stem cells, pRb, retinoblastoma protein, integumentary system, Laminopathies, INM, inner nuclear membrane, Membrane Proteins, Aging, Premature, Cell Differentiation, Cell Biology, Lamin Type A, Chromatin, Lamins, HGPS, Hutchinson–Gilford Progeria Syndrome, DNA-Binding Proteins, stomatognathic diseases, EDMD, Emery Dreifuss muscular dystrophy, Gene Expression Regulation, iPS, induced pluripotent stem cell, embryonic structures, ASC, (somatic) adult stem cell, NE, nuclear envelope, Self-renewal, LRD, lamin rich domain, Developmental Biology

Abstract

Highlights • A-type lamins localize to the lamina at the nuclear periphery and throughout the nucleoplasm. • A-type lamins in the nuclear interior bind to and depend on lamina-associated polypeptide 2α (LAP2α). • Lamin A/C–LAP2α complexes regulate tissue progenitor cell proliferation through retinoblastoma protein-linked pathways. • A-type lamins regulate chromatin organization and gene expression at the nuclear periphery and throughout the nucleoplasm. • Deregulation of nucleoplasmic A-type lamins and LAP2α contributes to abnormal phenotypes in laminopathies., A-type lamins are components of the lamina network at the nuclear envelope, which mediates nuclear stiffness and anchors chromatin to the nuclear periphery. However, A-type lamins are also found in the nuclear interior. Here we review the roles of the chromatin-associated, nucleoplasmic LEM protein, lamina-associated polypeptide 2α (LAP2α) in the regulation of A-type lamins in the nuclear interior. The lamin A/C–LAP2α complex may be involved in the regulation of the retinoblastoma protein-mediated pathway and other signaling pathways balancing proliferation and differentiation, and in the stabilization of higher-order chromatin organization throughout the nucleus. Loss of LAP2α in mice leads to selective depletion of the nucleoplasmic A-type lamin pool, promotes the proliferative stem cell phenotype of tissue progenitor cells, and delays stem cell differentiation. These findings support the hypothesis that LAP2α and nucleoplasmic lamins are regulators of adult stem cell function and tissue homeostasis. Finally, we discuss potential implications of this concept for defining the molecular disease mechanisms of lamin-linked diseases such as muscular dystrophy and premature aging syndromes.

Published

2014

15. Regulation of nucleocytoplasmic trafficking of viral proteins: An integral role in pathogenesis?☆

Author

Alex J. Fulcher and David A. Jans

Subjects

Simian virus 40 T-ag, Nuclear import, viruses, PML, promyelocytic leukaemia protein, Human papillomavirus E1, BRAP2, BRCA1-associated protein 2, RbBS, retinoblastoma binding site, medicine.disease_cause, Nup, nucleoporin, HTLV, human T-cell leukaemia virus, Nuclear protein, Nuclear pore, RPP, Rabies virus phospho-protein, Phosphorylation, Rb, retinoblastoma, biology, CK2, protein kinase CK2, NES, nuclear export sequence, CTD, C-terminal domain, Cell biology, STAT, signal transducer and activator of transcription, medicine.anatomical_structure, Virus Diseases, T-ag, large tumour antigen, dsDNA-PK, double stranded DNA-dependent protein kinase, EBV, Epstein–Barr virus, BPV, bovine papillomavirus, CK1, protein kinase CK1, IMP, importin, Viral protein, CBP, CREB binding protein, Active Transport, Cell Nucleus, KSHV, Kaposi's sarcoma-associated herpes virus, NPC, nuclear pore complex, Importin, DLC-AS, DLC-association sequence, NLS, nuclear localisation sequence, Article, VZV, varicella zoster virus, Viral Proteins, MT-AS, MT-association sequence, Cyclin-dependent kinase, PKC, protein kinase C, medicine, GSK3, glycogen synthase kinase 3, Animals, Humans, DLC, dynein light chain, EXP, exportin, IFN, interferon, SARS, severe acute respiratory syndrome, Molecular Biology, PKA, protein kinase A PKC, protein kinase C, SV40, simian virus 40, FG, phenylalanine–glycine, HCMV, human cytomegalovirus, Cell Biology, Crm1, chromosome region maintenance protein 1, Virology, HPV, human papilloma virus, Rabies virus P, CAV, chicken anaemia virus, Human cytomegalovirus ppUL44, Cell nucleus, RV, Rabies virus, Viral replication, biology.protein, NE, nuclear envelope, Cdk, cyclin dependent kinase, LANA2, latency associated nuclear antigen 2, Nuclear transport, MT, microtubule

Abstract

Signal-dependent targeting of proteins into and out of the nucleus is mediated by members of the importin (IMP) family of transport receptors, which recognise targeting signals within a cargo protein and mediate passage through the nuclear envelope-embedded nuclear pore complexes. Regulation of this process is paramount to processes such as cell division and differentiation, but is also critically important for viral replication and pathogenesis; phosphorylation appears to play a major role in regulating viral protein nucleocytoplasmic trafficking, along with other posttranslational modifications. This review focuses on viral proteins that utilise the host cell IMP machinery in order to traffic into/out of the nucleus, and in particular those where trafficking is critical to viral replication and/or pathogenesis, such as simian virus SV40 large tumour antigen (T-ag), human papilloma virus E1 protein, human cytomegalovirus processivity factor ppUL44, and various gene products from RNA viruses such as Rabies. Understanding of the mechanisms regulating viral protein nucleocytoplasmic trafficking is paramount to the future development of urgently needed specific and effective anti-viral therapeutics. This article was originally intended for the special issue “Regulation of Signaling and Cellular Fate through Modulation of Nuclear Protein Import”. The Publisher apologizes for any inconvenience caused., Research highlights ► Nucleocytoplasmic trafficking of viral proteins is central to viral infection. ► Posttranslational modification is a key means to regulate viral protein trafficking. ► Nuclear trafficking of viral proteins can be a target for development of anti-virals.

Published

2011

16. N-terminal nesprin-2 variants regulate β-catenin signalling

Author

Qiuping, Zhang, Rose-Marie, Minaisah, Elisa, Ferraro, Chen, Li, Lauren J, Porter, Can, Zhou, Fang, Gao, Junyi, Zhang, Dipen, Rajgor, Flavia, Autore, Catherine M, Shanahan, and Derek T, Warren

Subjects

HDF, human dermal fibroblast cell, Transcription, Genetic, CHD, calponin homology domain, ESC, embryonic stem cells, Nerve Tissue Proteins, Cell Line, Mice, VSMC, human vascular smooth muscle cell, HUVEC, human umbilical vein endothelial cells, Animals, Humans, Protein Isoforms, beta Catenin, Scaffold protein, Cell Nucleus, ONM, outer nuclear membrane, Microfilament Proteins, INM, inner nuclear membrane, Membrane Proteins, Nuclear Proteins, Reproducibility of Results, IP, immunoprecipitation, Cell-cell junctions, EDMD, Emery–Dreifuss muscular dystrophy, IF, immunofluorescence microscopy, Protein Transport, F-actin, filamentous actin, Intercellular Junctions, WB, Western blot, NE, nuclear envelope, Nesprin-2, Β-catenin, SR, spectrin repeat, LINC, Linker of nucleoskeleton and cytoskeleton, Protein Binding, Signal Transduction, Research Article

Abstract

The spatial compartmentalisation of biochemical signalling pathways is essential for cell function. Nesprins are a multi-isomeric family of proteins that have emerged as signalling scaffolds, herein, we investigate the localisation and function of novel nesprin-2 N-terminal variants. We show that these nesprin-2 variants display cell specific distribution and reside in both the cytoplasm and nucleus. Immunofluorescence microscopy revealed that nesprin-2 N-terminal variants colocalised with β-catenin at cell-cell junctions in U2OS cells. Calcium switch assays demonstrated that nesprin-2 and β-catenin are lost from cell-cell junctions in low calcium conditions whereas emerin localisation at the NE remained unaltered, furthermore, an N-terminal fragment of nesprin-2 was sufficient for cell-cell junction localisation and interacted with β-catenin. Disruption of these N-terminal nesprin-2 variants, using siRNA depletion resulted in loss of β-catenin from cell-cell junctions, nuclear accumulation of active β-catenin and augmented β-catenin transcriptional activity. Importantly, we show that U2OS cells lack nesprin-2 giant, suggesting that the N-terminal nesprin-2 variants regulate β-catenin signalling independently of the NE. Together, these data identify N-terminal nesprin-2 variants as novel regulators of β-catenin signalling that tether β-catenin to cell-cell contacts to inhibit β-catenin transcriptional activity., Highlights • N-terminal nesprin-2 variants display cell specific expression patterns. • N-terminal spectrin repeats of nesprin-2 interact with β-catenin. • N-terminal nesprin-2 variants scaffold β-catenin at cell-cell junctions.. • Nesprin-2 variants play multiple roles in β-catenin signalling.

Published

2015

17. Characterization of a Unique Form of Arrhythmic Cardiomyopathy Caused by Recessive Mutation in LEMD2.

Author

Abdelfatah N, Chen R, Duff HJ, Seifer CM, Buffo I, Huculak C, Clarke S, Clegg R, Jassal DS, Gordon PMK, Ober C, Frosk P, and Gerull B

Abstract

Nuclear envelope proteins have been shown to play an important role in the pathogenesis of inherited dilated cardiomyopathy. Here, we present a remarkable cardiac phenotype caused by a homozygous LEMD2 mutation in patients of the Hutterite population with juvenile cataract. Mutation carriers develop arrhythmic cardiomyopathy with mild impairment of left ventricular systolic function but severe ventricular arrhythmias leading to sudden cardiac death. Affected cardiac tissue from a deceased patient and fibroblasts exhibit elongated nuclei with abnormal condensed heterochromatin at the periphery. The patient fibroblasts demonstrate cellular senescence and reduced proliferation capacity, which may suggest an involvement of LEM domain containing protein 2 in chromatin remodeling processes and premature aging.

Published

2019

18. Identification of the evolutionarily conserved nuclear envelope proteins Lem2 and MicLem2 in Tetrahymena thermophila .

Author

Iwamoto M, Fukuda Y, Osakada H, Mori C, Hiraoka Y, and Haraguchi T

Abstract

Lem2 family proteins, i.e. the LAP2-Emerin-MAN1 (LEM) domain-containing nuclear envelope proteins, are well-conserved from yeasts to humans, both of which belong to the Opisthokonta supergroup. However, whether their homologs are present in other eukaryotic phylogenies remains unclear. In this study, we identified two Lem2 homolog proteins, which we named as Lem2 and MicLem2, in a ciliate Tetrahymena thermophila belonging to the SAR supergroup. Lem2 was localized to the nuclear envelope of the macronucleus (MAC) and micronucleus (MIC), while MicLem2 was exclusively localized to the nuclear envelope of the MIC. Immunoelectron microscopy revealed that Lem2 in T. thermophila was localized to both the inner and outer nuclear envelopes of the MAC and MIC, while MicLem2 was mostly localized to the nuclear pores of the MIC. Molecular domain analysis using GFP-fused protein showed that the N-terminal and luminal domains, including the transmembrane segments, are responsible for nuclear envelope localization. During sexual reproduction, enrichment of Lem2 occurred in the nuclear envelopes of the MAC and MIC to be degraded, while MicLem2 was enriched in the nuclear envelope of the MIC that escaped degradation. These findings suggest the unique characteristics of Tetrahymena Lem2 proteins. Our findings provide insight into the evolutionary divergence of nuclear envelope proteins., (© 2019 The Author(s).)

Published

2019

19. Depletion of nucleophosmin leads to distortion of nucleolar and nuclear structures in HeLa cells

Author

Sachihiro Matsunaga, Mohammed Abdullahel Amin, Susumu Uchiyama, and Kiichi Fukui

Subjects

RNA interference (RNAi), Nucleolus, nucleophosmin (NPM), Ribosome biogenesis, Accelerated Publication, Biology, Biochemistry, FBS, fetal bovine serum, medicine, Humans, Centrosome duplication, Nuclear protein, DIC, differential interference contrast, NPMr, RNAi-refractory GFP-NPM, nucleolar structure, Molecular Biology, Mitosis, Microtubule nucleation, GFP, green fluorescent protein, Cell Nucleus, Nucleophosmin, integumentary system, NPM, nucleophosmin, PNB, pre-nucleolar body, Nuclear Proteins, Cell Biology, Cell biology, Cell nucleus, medicine.anatomical_structure, RNAi, RNA interference, Microscopy, Fluorescence, siRNA, small interfering RNA, nuclear structure, NE, nuclear envelope, RNA Interference, HeLa cell, Cell Nucleolus, HeLa Cells

Abstract

Mohammed Abdullahel Amin, Sachihiro Matsunaga, Susumu Uchiyama, Kiichi Fukui; Depletion of nucleophosmin leads to distortion of nucleolar and nuclear structures in HeLa cells. Biochem J 1 November 2008; 415 (3): 345–351. doi: https://doi.org/10.1042/BJ20081411., NPM (nucleophosmin; also known as B23) is an abundantly and ubiquitously expressed multifunctional nucleolar phosphoprotein, which is involved in numerous cellular processes, including ribosome biogenesis, protein chaperoning and centrosome duplication; however, the role of NPM in the cell cycle still remains unknown. In the present study, we show dynamic localization of NPM throughout the cell cycle of HeLa cells. Using a combination of RNAi (RNA interference) and three-dimensional microscopy we show that NPM is localized at the chromosome periphery during mitosis. We also demonstrate that depletion of NPM causes distortion of nucleolar structure as expected and leads to unexpected dramatic changes in nuclear morphology with multiple micronuclei formation. The defect in nuclear shape of NPM-depleted cells, which is clearly observed by live-cell imaging, is due to the distortion of cytoskeletal (α-tubulin and β-actin) structure, resulting from the defects in centrosomal microtubule nucleation. These results indicate that NPM is an essential protein not only for the formation of normal nucleolar structure, but also for the maintenance of regular nuclear shape in HeLa cells.

Published

2008

20. Uncleavable Nup98-Nup96 is functional in the fission yeast Schizosaccharomyces pombe.

Author

Asakawa H, Mori C, Ohtsuki C, Iwamoto M, Hiraoka Y, and Haraguchi T

Abstract

Essential nucleoporins Nup98 and Nup96 are coded by a single open reading frame, and produced by autopeptidase cleavage. The autocleavage site of Nup98-Nup96 is highly conserved in a wide range of organisms. To understand the importance of autocleavage, we examined a mutant that produces the Nup98-Nup96 joint molecule as a sole protein product of the nup189 (+) gene in the fission yeast Schizosaccharomyces pombe. Cells expressing only the joint molecule were found to be viable. This result indicates that autocleavage of Nup98-Nup96 is dispensable for cell growth, at least under normal culture conditions in S. pombe.

Published

2015

21. Cytosolic and nuclear calcium signaling in atrial myocytes: IP3-mediated calcium release and the role of mitochondria.

Author

Hohendanner F, Maxwell JT, and Blatter LA

Subjects

Animals, Calcium metabolism, Cytosol metabolism, Inositol 1,4,5-Trisphosphate Receptors, Mitochondria metabolism, Myocytes, Cardiac physiology, Rabbits, Calcium Signaling, Myocytes, Cardiac metabolism

Abstract

In rabbit atrial myocytes Ca signaling has unique features due to the lack of transverse (t) tubules, the spatial arrangement of mitochondria and the contribution of inositol-1,4,5-trisphosphate (IP3) receptor-induced Ca release (IICR). During excitation-contraction coupling action potential-induced elevation of cytosolic [Ca] originates in the cell periphery from Ca released from the junctional sarcoplasmic reticulum (j-SR) and then propagates by Ca-induced Ca release from non-junctional (nj-) SR toward the cell center. The subsarcolemmal region between j-SR and the first array of nj-SR Ca release sites is devoid of mitochondria which results in a rapid propagation of activation through this domain, whereas the subsequent propagation through the nj-SR network occurs at a velocity typical for a propagating Ca wave. Inhibition of mitochondrial Ca uptake with the Ca uniporter blocker Ru360 accelerates propagation and increases the amplitude of Ca transients (CaTs) originating from nj-SR. Elevation of cytosolic IP3 levels by rapid photolysis of caged IP3 has profound effects on the magnitude of subcellular CaTs with increased Ca release from nj-SR and enhanced CaTs in the nuclear compartment. IP3 uncaging restricted to the nucleus elicites 'mini'-Ca waves that remain confined to this compartment. Elementary IICR events (Ca puffs) preferentially originate in the nucleus in close physical association with membrane structures of the nuclear envelope and the nucleoplasmic reticulum. The data suggest that in atrial myocytes the nucleus is an autonomous Ca signaling domain where Ca dynamics are primarily governed by IICR.

Published

2015

22. The cytoplasmic tail of heparin-binding EGF-like growth factor regulates bidirectional intracellular trafficking between the plasma membrane and ER.

Author

Hieda M, Koizumi M, Higashi C, Tachibana T, Taguchi T, and Higashiyama S

Abstract

Heparin-binding epidermal growth factor (EGF)- like growth factor (HB-EGF) is synthesized in the ER, transported along the exocytic pathway, and expressed on the plasma membrane as a type I transmembrane protein. Upon extracellular stimulation, HB-EGF, either proHB-EGF or the shed form HB-EGF-CTF, undergoes endocytosis and is then transported retrogradely to the ER. In this study, we showed the essential contribution of the short cytoplasmic tail of HB-EGF (HB-EGF-cyto) to the bidirectional intracellular trafficking between the ER and plasma membrane and revealed several critical amino acids residues that are responsible for internalization from the plasma membrane and ER targeting. We suggest that these anterograde and retrograde sorting signals within HB-EGF-cyto are strictly regulated by protein modification and conformation.

Published

2012

23. Uncleavable Nup98–Nup96 is functional in the fission yeast Schizosaccharomyces pombe

Author

Chizuru Ohtsuki, Tokuko Haraguchi, Yasushi Hiraoka, Haruhiko Asakawa, Masaaki Iwamoto, and Chie Mori

Subjects

QH301-705.5, Mutant, NPC, nuclear pore complex, Biology, Cleavage (embryo), General Biochemistry, Genetics and Molecular Biology, Research article, Nup107-160 complex, Nuclear pore, Biology (General), Gene, ComputingMethodologies_COMPUTERGRAPHICS, Genetics, Nucleoporins, GLFG repeat, Gly-Leu-Phe-Gly repeat, biology.organism_classification, Fission yeast, Yeast, Cell biology, Nuclear pore complex, FG nup, Open reading frame, Schizosaccharomyces pombe, NE, nuclear envelope, Nucleoporin, Alternative splicing

Abstract

Graphical abstract, Highlights • Nup98 and Nup96 are produced via alternative splicing and autocleavage in S. pombe. • Splicing and autocleavage are both dispensable for S. pombe cell viability. • Nup98 and Nup96 expressed from different loci are functional for cell viability. • A Nup98–Nup96 joint molecule as a sole protein product of nup189 gene is functional. • Autocleavage is essential for Nup98 to remove a part of Nup96 generated by splicing., Essential nucleoporins Nup98 and Nup96 are coded by a single open reading frame, and produced by autopeptidase cleavage. The autocleavage site of Nup98–Nup96 is highly conserved in a wide range of organisms. To understand the importance of autocleavage, we examined a mutant that produces the Nup98–Nup96 joint molecule as a sole protein product of the nup189+ gene in the fission yeast Schizosaccharomyces pombe. Cells expressing only the joint molecule were found to be viable. This result indicates that autocleavage of Nup98–Nup96 is dispensable for cell growth, at least under normal culture conditions in S. pombe.

24. The cytoplasmic tail of heparin-binding EGF-like growth factor regulates bidirectional intracellular trafficking between the plasma membrane and ER

Author

Shigeki Higashiyama, Chiduru Higashi, Miki Hieda, Taro Tachibana, Tomohiko Taguchi, and Michiko Koizumi

Subjects

maHB-EGF-cyto, membrane anchored HB-EGF-cyto, Heparin-binding EGF-like growth factor, medicine.medical_treatment, media_common.quotation_subject, Ectodomain shedding, Biology, Endocytosis, TCA, trichloroacetic acid, ER retrieval, CTF, carboxy-terminal fragment, General Biochemistry, Genetics and Molecular Biology, Article, Epidermal growth factor, medicine, Internalization, media_common, EGF, epidermal growth factor, Growth factor, Transmembrane protein, Cell biology, HB-EGF, Biochemistry, Cytoplasm, HB-EGF-cyto, cytoplasmic tail of HB-EGF, HB-EGF, heparin-binding EGF-like growth factor, EGFR, EGF receptor, NE, nuclear envelope, TPA, phorbol ester 12-O-tetradecanoylphorbol-13-acetate, Intracellular, hormones, hormone substitutes, and hormone antagonists, Intracellular trafficking

Abstract

Heparin-binding epidermal growth factor (EGF)- like growth factor (HB-EGF) is synthesized in the ER, transported along the exocytic pathway, and expressed on the plasma membrane as a type I transmembrane protein. Upon extracellular stimulation, HB-EGF, either proHB-EGF or the shed form HB-EGF-CTF, undergoes endocytosis and is then transported retrogradely to the ER. In this study, we showed the essential contribution of the short cytoplasmic tail of HB-EGF (HB-EGF-cyto) to the bidirectional intracellular trafficking between the ER and plasma membrane and revealed several critical amino acids residues that are responsible for internalization from the plasma membrane and ER targeting. We suggest that these anterograde and retrograde sorting signals within HB-EGF-cyto are strictly regulated by protein modification and conformation., Highlights ▸ The cytoplasmic tail of HB-EGF contributes to bidirectional intracellular trafficking. ▸ The carboxyl-terminal five amino acids are indispensable for internalization. ▸ Amino acids S207 and K201 play essential roles in retrograde transport to the ER. ▸ Sorting signals in HB-EGF are regulated by protein modification and conformation. ▸ The extracellular domain of proHB-EGF is not required for intracellular trafficking.

25. Transport of estradiol-17β-glucuronide, estrone-3-sulfate and taurocholate across the endoplasmic reticulum membrane: evidence for different transport systems

Author

Wlcek Katrin, Hofstetter Lia, Stieger Bruno, University of Zurich, and Stieger, Bruno

Subjects

Taurocholic Acid, UDPGA, Uridine diphosphate glucuronic acid, 1303 Biochemistry, Ntcp, Na-taurocholate co-transporting polypeptide, Estradiol-17β-glucuronide, Transport, 610 Medicine & health, In Vitro Techniques, Biochemistry, Permeability, Article, Membrane Potentials, Rats, Sprague-Dawley, ER, endoplasmic reticulum, Glucuronides, U6 Integrative Human Physiology, G6P, glucose-6-phosphate, Animals, DHEAS, dehydroepiandrosteronesulfate, ABC, ATP binding cassette, Rats, Wistar, SER, smooth endoplasmic reticulum, CYPs, cytochrome P450s, Biotransformation, ComputingMethodologies_COMPUTERGRAPHICS, Pharmacology, Estradiol, Estrone-3-sulfate, Biological Transport, UGTs, Uridine diphosphate glucuronosyltransferases, Intracellular Membranes, Endoplasmic Reticulum, Smooth, Rats, Kinetics, RER, rough endoplasmic reticulum, 3004 Pharmacology, Liver, 10199 Clinic for Clinical Pharmacology and Toxicology, TC, taurocholate, E17βG, estradiol-17β-glucuronide, NE, nuclear envelope, Endoplasmic Reticulum, Rough, MRP2, multidrug resistance associated protein 2, Oatp, organic anion transporting polypeptide, STS, steroidsulfatase, E3S, estrone-3-sulfate, HPTLC, high performance thin layer chromatography, Endoplasmic reticulum

Abstract

Graphical abstract, Important reactions of drug metabolism, including UGT mediated glucuronidation and steroidsulfatase mediated hydrolysis of sulfates, take place in the endoplasmic reticulum (ER) of hepatocytes. Consequently, UGT generated glucuronides, like estradiol-17β-glucuronide, have to be translocated back into the cytoplasm to reach their site of excretion. Also steroidsulfatase substrates, including estrone-3-sulfate, have to cross the ER membrane to reach their site of hydrolysis. Based on their physicochemical properties such compounds are not favored for passive diffusion and therefore likely necessitate transport system(s) to cross the ER membrane in either direction. The current study aims to investigate the transport of taurocholate, estradiol-17β-glucuronide, and estrone-3-sulfate in smooth (SER) and rough (RER) endoplasmic reticulum membrane vesicles isolated from Wistar and TR− rat liver. Time-dependent and bidirectional transport was demonstrated for taurocholate, showing higher uptake rates in SER than RER vesicles. For estradiol-17β-glucuronide a fast time-dependent efflux with similar efficiencies from SER and RER but no clear protein-mediated uptake was shown, indicating an asymmetric transport system for this substrate. Estrone-3-sulfate uptake was time-dependent and higher in SER than in RER vesicles. Inhibition of steroidsulfatase mediated estrone-3-sulfate hydrolysis decreased estrone-3-sulfate uptake but had no effect on taurocholate or estradiol-17β-glucuronide transport. Based on inhibition studies and transport characteristics, three different transport mechanisms are suggested to be involved in the transport of taurocholate, estrone-3-sulfate and estradiol-17β-glucuronide across the ER membrane.

26. Structure Determination of the Nuclear Pore Complex with Three-Dimensional Cryo electron Microscopy

Author

Alexander von Appen and Martin Beck

Subjects

0301 basic medicine, Materials science, Cryo-electron microscopy, cryoET, cryoelectron tomography, X.l., Xenopus laevis, cryoelectron microscopy, NPC, nuclear pore complex, Nanotechnology, Article, D.d., Dictyostelium discoideum, 03 medical and health sciences, Structural Biology, nuclear pore complex, otorhinolaryngologic diseases, Animals, Humans, Nuclear pore, Molecular Biology, EM, electron microscopy, Membranes, S.c., Saccharomyces cerevisiae, 3D, three-dimensional, RCT, random conical tilt, 030104 developmental biology, Membrane, cryoEM, cryoelectron microscopy, Vertebrates, NE, nuclear envelope, Nuclear Pore

Abstract

Determining the structure of the nuclear pore complex (NPC) imposes an enormous challenge due to its size, intricate composition and membrane-embedded nature. In vertebrates, about 1000 protein building blocks assemble into a 110-MDa complex that fuses the inner and outer membranes of a cell's nucleus. Here, we review the recent progress in understanding the in situ architecture of the NPC with a specific focus on approaches using three-dimensional cryo electron microscopy. We discuss technological benefits and limitations and give an outlook toward obtaining a high-resolution structure of the NPC., Graphical Abstract, Highlights • Overview over three-dimensional electron microscopic analysis of the nuclear pore complex. • Review of recent integrative structural biology studies of the nuclear pore complex scaffold architecture.