Your search keyword '"Biological Transport physiology"' showing total 49 results

1. The Association of Essential Metals with APOE Genotype in Alzheimer’s Disease

Author

Patrick R. Hof, Tatjana Orct, Ena Španić, Koraljka Bačić Baronica, Spomenka Kiđemet-Piskač, Fran Borovečki, Mirjana Babić Leko, Željka Vogrinc, Vesna Lukinović Škudar, Matea Nikolac Perkovic, Goran Šimić, Nela Pivac, Ankica Sekovanić, and Jasna Jurasović

Subjects

Male, 0301 basic medicine, Apolipoprotein E, Apolipoprotein E4, Biological Transport / physiology, Metals* / blood, chemistry.chemical_compound, 0302 clinical medicine, Zinc / cerebrospinal fluid, Genotype, Cholesterol / metabolism, Correlation of Data, Metalloids, General Neuroscience, Neurodegeneration, Metals* / cerebrospinal fluid, General Medicine, Zinc, Psychiatry and Mental health, Clinical Psychology, Cholesterol, Metals, Toxicity, Metals* / classification, Metalloids* / blood, Apolipoprotein E4 / genetics, Female, medicine.medical_specialty, Alzheimer Disease* / cerebrospinal fluid, Sodium, chemistry.chemical_element, Calcium, Alzheimer’s disease, apolipoprotein E, copper, metals, mild cognitive impairment, zinc, 03 medical and health sciences, Apolipoproteins E, Alzheimer Disease, Alzheimer Disease* / blood, Internal medicine, medicine, Humans, Cognitive Dysfunction, Allele, Cognitive Dysfunction / blood, Sodium / blood, Aged, Biological Transport, medicine.disease, Cognitive Dysfunction / diagnosis, Ferritins / cerebrospinal fluid, 030104 developmental biology, Endocrinology, chemistry, Ferritins, Cognitive Dysfunction / cerebrospinal fluid, Alzheimer Disease* / genetics, Geriatrics and Gerontology, Metalloids* / cerebrospinal fluid, 030217 neurology & neurosurgery

Abstract

Background: The major confirmed genetic risk factor for late-onset, sporadic Alzheimer's disease (AD) is variant ɛ4 of apolipoprotein E gene (APOE). It is proposed that ApoE, a protein involved in transport of cholesterol to neurons can cause neurodegeneration in AD through interaction with metals. Previous studies mostly associated copper, iron, zinc, and calcium with ApoE4-mediated toxicity. ----- Objective: To test the association of essential metals with APOE genotype. ----- Methods: We compared plasma and cerebrospinal fluid (CSF) levels of copper, zinc, iron, sodium, magnesium, calcium, cobalt, molybdenum, manganese, boron, and chromium, and CSF ferritin levels among AD, mild cognitive impairment (MCI) patients, and healthy controls (HC) with different APOE genotype. ----- Results: Sodium, copper, and magnesium levels were increased in carriers of ɛ4 allele. Additionally, the increase in sodium, calcium and cobalt plasma levels was observed in carriers of ɛ4/ɛx genotype. The decrease in boron plasma levels was observed in carriers of ɛ4 allele and ɛ4/ɛ4 genotype. Additionally, CSF zinc levels as well as plasma sodium levels were increased in AD patients compared to HC. ----- Conclusion: These results indicate that the molecular underpinnings of association of essential metals and metalloids with APOE should be further tested and clarified in vivo and in vitro.

Published

2021

2. Liquid Biopsy Enables Quantification of the Abundance and Interindividual Variability of Hepatic Enzymes and Transporters

Author

Jill Barber, Peter Kilford, Amin Rostami-Hodjegan, Mian Zhang, Brahim Achour, Agnieszka Grybos‐Gajniak, David Knight, Kristi Lea, Jeoffrey Schageman, and Zubida M. Al-Majdoub

Subjects

Adult, Liver/metabolism, Male, Drug, Cytochrome P-450 Enzyme System/metabolism, Metabolic Clearance Rate, media_common.quotation_subject, In silico, Exosomes, Bioinformatics, 030226 pharmacology & pharmacy, Article, Metabolic Clearance Rate/physiology, Variable Expression, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Cytochrome P-450 Enzyme System, Inactivation, Metabolic/physiology, Membrane Transport Proteins/metabolism, Humans, Medicine, Pharmacology (medical), Liquid biopsy, Gene, Genotyping, Biological Transport/physiology, Aged, media_common, Aged, 80 and over, Pharmacology, business.industry, Research, Liquid Biopsy, Membrane Transport Proteins, Biological Transport, Articles, Liquid Biopsy/methods, Middle Aged, Exosomes/metabolism, Liver, Drug development, 030220 oncology & carcinogenesis, Inactivation, Metabolic, Female, business, Drug metabolism

Abstract

Variability in individual capacity for hepatic elimination of therapeutic drugs is well recognized and is associated with variable expression and activity of liver enzymes and transporters. Whilst genotyping offers some degree of stratification, there is often large variability within the same genotype. Direct measurement of protein expression is impractical due to limited access to tissue biopsies. Hence, determination of variability in hepatic drug metabolism and disposition using liquid biopsy (blood samples) is an attractive proposition during drug development and in clinical practice. This study employed a multi-'omic' strategy to establish a liquid biopsy technology intended to assess hepatic capacity for metabolism and disposition in individual patients. Plasma exosomal analysis (n=29) revealed expression of 533 pharmacologically relevant genes at the RNA level, with 147 genes showing evidence of expression at the protein level in matching liver tissue. Correction of exosomal RNA expression using a novel shedding factor (SF) improved correlation against liver protein expression for 97 liver-enriched genes. Strong correlation was demonstrated for 12 key drug-metabolizing enzymes and 4 drug transporters. The developed test allowed reliable patient stratification, and in silico trials demonstrated utility in adjusting drug dose to achieve similar drug exposure between patients with variable hepatic elimination. Accordingly, this approach can be applied in characterization of volunteers prior to enrolment in clinical trials and for patient stratification in clinical practice to achieve more precise individual dosing.

Published

2020

3. Transcriptional profiling of transport mechanisms and regulatory pathways in rat choroid plexus

Author

Søren N. Andreassen, Trine L. Toft-Bertelsen, Jonathan H. Wardman, Rene Villadsen, and Nanna MacAulay

Subjects

Brain, Biological Transport, Epithelial Cells, General Medicine, Epithelium, Epithelial Cells/metabolism, Rats, Epithelium/metabolism, Cellular and Molecular Neuroscience, Mice, Developmental Neuroscience, Neurology, Cerebrospinal Fluid/metabolism, Choroid Plexus, Animals, Brain/metabolism, Biological Transport/physiology, Choroid Plexus/metabolism, Cerebrospinal Fluid

Abstract

Background Dysregulation of brain fluid homeostasis associates with brain pathologies in which fluid accumulation leads to elevated intracranial pressure. Surgical intervention remains standard care, since specific and efficient pharmacological treatment options are limited for pathologies with disturbed brain fluid homeostasis. Such lack of therapeutic targets originates, in part, from the incomplete map of the molecular mechanisms underlying cerebrospinal fluid (CSF) secretion by the choroid plexus. Methods The transcriptomic profile of rat choroid plexus was generated by RNA Sequencing (RNAseq) of whole tissue and epithelial cells captured by fluorescence-activated cell sorting (FACS), and compared to proximal tubules. The bioinformatic analysis comprised mapping to reference genome followed by filtering for type, location, and association with alias and protein function. The transporters and associated regulatory modules were arranged in discovery tables according to their transcriptional abundance and tied together in association network analysis. Results The transcriptomic profile of choroid plexus displays high similarity between sex and species (human, rat, and mouse) and lesser similarity to another high-capacity fluid-transporting epithelium, the proximal tubules. The discovery tables provide lists of transport mechanisms that could participate in CSF secretion and suggest regulatory candidates. Conclusions With quantification of the transport protein transcript abundance in choroid plexus and their potentially linked regulatory modules, we envision a molecular tool to devise rational hypotheses regarding future delineation of choroidal transport proteins involved in CSF secretion and their regulation. Our vision is to obtain future pharmaceutical targets towards modulation of CSF production in pathologies involving disturbed brain water dynamics.

Published

2022

4. Interorganelle Tethering to Endocytic Organelles Determines Directional Cytokine Transport in CD4+ T Cells

Author

Yan Zhou, Heiko Rieger, Mayis Kaba, Varsha Pattu, Rahmad Akbar, Bin Qu, Volkhard Helms, Renping Zhao, Eva C. Schwarz, and Paula Nunes-Hasler

Subjects

CD4-Positive T-Lymphocytes / metabolism, Endocytosis / physiology, Endosomes / metabolism, Organelles / metabolism, CD4-Positive T-Lymphocytes, Microtubules / metabolism, Lysosomes / metabolism, Endosome, Immunology, Dynein, Endocytic cycle, Kinesins, Endosomes, ddc:616.07, Microtubules, Cell Line, Biological Transport / physiology, Motor protein, Microtubule, Organelle, Humans, Immunology and Allergy, Dyneins / metabolism, ddc:612, Organelles, Chemistry, Vesicle, Dyneins, Biological Transport, Endocytosis, Kinesins / metabolism, Cell biology, Cytokines / metabolism, HEK293 Cells, Cytokines, Kinesin, Lysosomes

Abstract

Delivery of vesicles to their desired destinations plays a central role in maintaining proper cell functionality. In certain scenarios, depending on loaded cargos, the vesicles have spatially distinct destinations. For example, in T cells, some cytokines (e.g., IL-2) are polarized to the T cell–target cell interface, whereas the other cytokines are delivered multidirectionally (e.g., TNF-α). In this study, we show that in primary human CD4+ T cells, both TNF-α+ and IL-2+ vesicles can tether with endocytic organelles (lysosomes/late endosomes) by forming membrane contact sites. Tethered cytokine-containing vesicle (CytV)–endocytic organelle pairs are released sequentially. Only endocytic organelle-tethered CytVs are preferentially transported to their desired destination. Mathematical models suggest that endocytic organelle tethering could regulate the direction of cytokine transport by selectively attaching different microtubule motor proteins (such as kinesin and dynein) to the corresponding CytVs. These findings establish the previously unknown interorganelle tethering to endocytic organelles as a universal solution for directional cytokine transport in CD4+ T cells. Modulating tethering to endocytic organelles can, therefore, coordinately control directionally distinct cytokine transport.

Published

2020

5. Mechanisms of Sodium Balance:Total Body Sodium, Surrogate Variables and Renal Sodium Excretion

Author

Peter Bie

Subjects

0301 basic medicine, medicine.medical_specialty, Physiology, Sodium, Body Fluids/physiology, chemistry.chemical_element, Renal function, Natriuresis, 030204 cardiovascular system & hematology, Sodium balance, Renin-Angiotensin System, 03 medical and health sciences, 0302 clinical medicine, Sodium excretion, Physiology (medical), Internal medicine, Extracellular fluid, medicine, Homeostasis, Humans, Animals, Hormonal control, Biological Transport/physiology, Water-Electrolyte Balance/physiology, Chemistry, Homeostasis/physiology, Total body sodium, Total body, Biological Transport, Water-Electrolyte Balance, Sodium distribution, Body Fluids, 030104 developmental biology, Endocrinology, Sodium/metabolism, Natriuresis/physiology, Renal sodium excretion, Renin-Angiotensin System/physiology

Abstract

The classical concepts of human sodium balance include 1) a total pool of Na+ of ≈4,200 mmol (total body sodium, TBS) distributed primarily in the extracellular fluid (ECV) and bone, 2) intake variations of 0.03 to ≈6 mmol·kg body mass−1·day−1, 3) asymptotic transitions between steady states with a halftime (T½) of 21 h, 4) changes in TBS driven by sodium intake measuring ≈1.3 day [ΔTBS/Δ(Na+ intake/day)], 5) adjustment of Na+ excretion to match any diet thus providing metabolic steady state, and 6) regulation of TBS via controlled excretion (90–95% renal) mediated by surrogate variables. The present focus areas include 1) uneven, nonosmotic distribution of increments in TBS primarily in “skin,” 2) long-term instability of TBS during constant Na+ intake, and 3) physiological regulation of renal Na+ excretion primarily by neurohumoral mechanisms dependent on ECV rather than arterial pressure. Under physiological conditions 1) the nonosmotic distribution of Na+ seems conceptually important, but quantitatively ill defined; 2) long-term variations in TBS represent significant deviations from steady state, but the importance is undetermined; and 3) the neurohumoral mechanisms of sodium homeostasis competing with pressure natriuresis are essential for systematic analysis of short-term and long-term regulation of TBS. Sodium homeostasis and blood pressure regulation are intimately related. Real progress is slow and will accelerate only through recognition of the present level of ignorance. Nonosmotic distribution of sodium, pressure natriuresis, and volume-mediated regulation of renal sodium excretion are essential intertwined concepts in need of clear definitions, conscious models, and future attention.

Published

2018

6. Root zone-specific localization of AMTs determines ammonium transport pathways and nitrogen allocation to shoots

Author

David E. Salt, Niko Geldner, Fengying Duan, Nicolaus von Wirén, and Ricardo Fabiano Hettwer Giehl

Subjects

0106 biological sciences, 0301 basic medicine, Leaves, Cell Membranes, Arabidopsis, Plant Science, 01 natural sciences, Transport Pathway, Biochemistry, Plant Roots, Transmembrane Transport Proteins, chemistry.chemical_compound, Cell Wall, Ammonium Compounds, Biology (General), General Neuroscience, Plant Anatomy, food and beverages, Apoplast, Chemistry, Ammonium Compounds/metabolism, Arabidopsis/physiology, Arabidopsis Proteins/physiology, Biological Transport/physiology, Cation Transport Proteins/metabolism, Cation Transport Proteins/physiology, Gene Expression Regulation, Plant/genetics, Ion Transport/physiology, Membrane Transport Proteins/physiology, Nitrogen/metabolism, Plant Proteins/metabolism, Plant Proteins/physiology, Plant Roots/metabolism, Plant Roots/physiology, Plant Physiology, Physical Sciences, Vascular Bundles, Casparian strip, Cellular Structures and Organelles, General Agricultural and Biological Sciences, Ammonium transport, Research Article, QH301-705.5, Nitrogen, Biology, General Biochemistry, Genetics and Molecular Biology, Cell wall, 03 medical and health sciences, Xylem, Apoplastic Space, Ammonium, Endodermis, Nitrates, General Immunology and Microbiology, fungi, Chemical Compounds, Biology and Life Sciences, Proteins, Biological Transport, Cell Biology, Iodides, 030104 developmental biology, Metabolism, chemistry, Biophysics, 010606 plant biology & botany

Abstract

In plants, nutrient provision of shoots depends on the uptake and transport of nutrients across the root tissue to the vascular system. Nutrient delivery to the vasculature is mediated via the apoplastic transport pathway (ATP), which uses the free space in the cell walls and is controlled by apoplastic barriers and nutrient transporters at the endodermis, or via the symplastic transport pathway (STP). However, the relative importance of these transport routes remains elusive. Here, we show that the STP, mediated by the epidermal ammonium transporter 1;3 (AMT1;3), dominates the radial movement of ammonium across the root tissue when external ammonium is low, whereas apoplastic transport controlled by AMT1;2 at the endodermis prevails at high external ammonium. Then, AMT1;2 favors nitrogen (N) allocation to the shoot, revealing a major importance of the ATP for nutrient partitioning to shoots. When an endodermal bypass was introduced by abolishing Casparian strip (CS) formation, apoplastic ammonium transport decreased. By contrast, symplastic transport was increased, indicating synergism between the STP and the endodermal bypass. We further establish that the formation of apoplastic barriers alters the cell type–specific localization of AMTs and determines STP and ATP contributions. These results show how radial transport pathways vary along the longitudinal gradient of the root axis and contribute to nutrient partitioning between roots and shoots., Author summary Radial transport of nutrients from the soil to the vascular system of plant roots occurs via the symplastic transport pathway (STP) and apoplastic transport pathway (ATP). Nutrients move along the STP when crossing the plasma membrane of outer cells and moving to xylem through the cytoplasmic continuum formed by plasmodesmata. Nutrients following the ATP, in turn, initially move passively through the extracellular space but are eventually taken up by endodermal cells, in which Casparian strips (CSs) prevent further apoplastic movement. We assessed the contribution of these transport pathways to radial transport in roots and nutrient provision to shoots by expressing cell type–specific ammonium transporters in a CS-defective mutant. Our study reveals that i) symplastic transport is more efficient at low external ammonium supply; ii) when endodermal cells become sealed by the deposition of suberin lamellae, the expression of ammonium transporters shifts to cortical cells; and iii) apoplastic transport depends on a functional apoplastic barrier at the endodermis, favoring nitrogen (N) partitioning to shoots at high external ammonium.

Published

2018

7. No increase in small-solute transport in peritoneal dialysis patients treated without hypertonic glucose for fifty-four months

Author

Eric Boulanger, Celia Lessore de Sainte Foy, Jean-Baptiste Beuscart, Alain Duhamel, Dominique Pagniez, Inserm, Université de Lille, CHU Lille, Service de Néphrologie et Transplantation rénale [CHRU-lille], Evaluation des technologies de santé et des pratiques médicales - ULR 2694 [METRICS], Lille Inflammation Research International Center - U 995 [LIRIC], Département de Néphrologie [CHRU Lille], Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille), Evaluation des technologies de santé et des pratiques médicales - ULR 2694 (METRICS), Université de Lille-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille), Lille Inflammation Research International Center - U 995 (LIRIC), Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille), This study was supported by a Clinical Evidence Council (CEC) grant from Baxter Healthcare Corporation (Deerfield, IL)., Bodescot, Myriam, Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Université de Lille, Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille-Institut Pasteur de Lille, and Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)

Subjects

Nephrology, Adult, Male, Glucose exposure, medicine.medical_specialty, Time Factors, medicine.medical_treatment, Peritoneal dialysis, 030232 urology & nephrology, Urology, Peritoneal equilibration test, 030204 cardiovascular system & hematology, lcsh:RC870-923, Glucose sparing, [SDV.MHEP.UN]Life Sciences [q-bio]/Human health and pathology/Urology and Nephrology, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Peritoneum, Glucose Solution, Hypertonic, Internal medicine, Linear regression, medicine, Humans, Peritoneal Infection, Aged, business.industry, Mesh:Kidney Failure, Mesh:Chronic/diagnosis, Mesh:Female, Mesh:Biological Transport/physiology, Mesh:Middle Aged, Mesh:Glucose Solution, Mesh:Hypertonic/administration & dosage, Mesh:Biological Transport/drug effects, Mesh:Peritoneal Dialysis/methods, Mesh:Chronic/therapy, Mesh:Cohort Studies, Mesh:Aged, Mesh:Treatment Outcome, Mesh:Time Factors, Mesh:Male, Mesh:Adult, Mesh:Follow-Up Studies, Mesh:Peritoneal Dialysis/trends, Mesh:Chronic/metabolism, Mesh:Humans, Small-solute transport, Repeated measures design, Biological Transport, Middle Aged, lcsh:Diseases of the genitourinary system. Urology, [SDV.MHEP.UN] Life Sciences [q-bio]/Human health and pathology/Urology and Nephrology, 3. Good health, Surgery, medicine.anatomical_structure, Treatment Outcome, Tonicity, Kidney Failure, Chronic, Female, business, Research Article, Follow-Up Studies

Abstract

Background Glucose is widely used as an osmotic agent in peritoneal dialysis (PD), but exerts untoward effects on the peritoneum. The potential protective effect of a reduced exposure to hypertonic glucose has never been investigated. Methods The cohort of PD patients attending our center which tackled the challenge of a restricted use of hypertonic glucose solutions has been prospectively followed since 1992. Small-solute transport was assessed using an equivalent of the glucose peritoneal equilibration test after 6 months, and then every year. Study was stopped on July 1st, 2008, before use of biocompatible solutions. Repeated measures in patients treated with PD for 54 months were analyzed by using (1) the slopes of the linear regression for D4/D0 ratios over time computed for each individual, and (2) a linear mixed model. Results In the study period, 44 patients were treated for a total of 2376 months, 2058 without hypertonic glucose. There was one episode of peritoneal infection every 18 patient-months. The mean of slopes of the linear regression for D4/D0 ratios was found to be significantly positive (Student’s test, p

Published

2017

8. KDM3A coordinates actin dynamics with intraflagellar transport to regulate cilia stability

Author

Yeyati, Patricia L., Schiller, Rachel, Mali, Girish, Kasioulis, Ioannis, Kawamura, Akane, Adams, Ian R., Playfoot, Christopher, Gilbert, Nick, van Heyningen, Veronica, Wills, Jimi, von Kriegsheim, Alex, Finch, Andrew, Sakai, Juro, Schofield, Christopher J., Jackson, Ian J., and Mill, Pleasantine

Subjects

Jumonji Domain-Containing Histone Demethylases, Gene Expression, macromolecular substances, Article, Cell Line, Mice, Cilia/metabolism, Journal Article, Morphogenesis, Animals, Humans, Cilia, Gene Expression/physiology, Research Articles, Biological Transport/physiology, Mutation/physiology, Flagella/metabolism, Histone Demethylases, fungi, Biological Transport, Actins, Phenotype, Flagella, Actins/metabolism, Mutation, Jumonji Domain-Containing Histone Demethylases/metabolism, sense organs, Histone Demethylases/metabolism, Morphogenesis/physiology

Abstract

Yeyati et al. demonstrate that the histone demethylase KDM3A acts as a negative regulator of ciliogenesis by modulating actin dynamics, both transcriptionally and by directly binding actin. KDM3A influences local actin networks to restrict intraflagellar transport during ciliogenesis; in its absence, cilia become unstable with abnormal lengths and accumulated intraflagellar transport proteins., Cilia assembly and disassembly are coupled to actin dynamics, ensuring a coherent cellular response during environmental change. How these processes are integrated remains undefined. The histone lysine demethylase KDM3A plays important roles in organismal homeostasis. Loss-of-function mouse models of Kdm3a phenocopy features associated with human ciliopathies, whereas human somatic mutations correlate with poor cancer prognosis. We demonstrate that absence of KDM3A facilitates ciliogenesis, but these resulting cilia have an abnormally wide range of axonemal lengths, delaying disassembly and accumulating intraflagellar transport (IFT) proteins. KDM3A plays a dual role by regulating actin gene expression and binding to the actin cytoskeleton, creating a responsive “actin gate” that involves ARP2/3 activity and IFT. Promoting actin filament formation rescues KDM3A mutant ciliary defects. Conversely, the simultaneous depolymerization of actin networks and IFT overexpression mimics the abnormal ciliary traits of KDM3A mutants. KDM3A is thus a negative regulator of ciliogenesis required for the controlled recruitment of IFT proteins into cilia through the modulation of actin dynamics.

Published

2017

9. Glutamate Transporters in the Blood-Brain Barrier

Author

Carsten Uhd Nielsen, Birger Brodin, Hans Christian Cederberg Helms, Helle S. Waagepetersen, Ortega, Arturo, and Schousboe, Arme

Subjects

0301 basic medicine, Central nervous system, Excitotoxicity, Biology, Neurotransmission, Blood–brain barrier, medicine.disease_cause, Glutamate metabolism, Brain glutamate efflux, 03 medical and health sciences, 0302 clinical medicine, Interstitial fluid, medicine, Animals, Humans, Biological Transport/physiology, EAAT, Amino Acid Transport System X-AG/metabolism, Glutamic acid, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Glutamic Acid/metabolism, Neurovascular unit, Efflux, Blood-Brain Barrier/metabolism, Neuroscience, 030217 neurology & neurosurgery, Homeostasis

Abstract

The amino acid L-glutamate serves a number of roles in the central nervous system, being an excitatory neurotransmitter, metabolite, and building block in protein synthesis. During pathophysiological events, where L-glutamate homeostasis cannot be maintained, the increased brain interstitial fluid concentration of L-glutamate causes excitotoxicity. A tight control of the brain interstitial fluid L-glutamate levels is therefore imperative, in order to maintain optimal neurotransmission and to avoid such excitotoxicity. The blood-brain barrier, i.e., the endothelial lining of the brain capillaries, regulates the exchange of nutrients, gases, and metabolic waste products between plasma and brain interstitial fluid. It has been suggested that brain capillary endothelial cells could play an important role in L-glutamate homeostasis by mediating brain-to-blood L-glutamate efflux. Both in vitro and in vivo studies have demonstrated blood-to-brain transport of L-glutamate, at least during pathological events. A number of studies have shown that brain endothelial cells express excitatory amino acid transporters, which may account for abluminal concentrative uptake of L-glutamate into the capillary endothelial cells. The mechanisms underlying transendothelial L-glutamate transport are however still not well understood. The present chapter summarizes the current knowledge on blood-brain barrier L-glutamate transporters and the suggested pathways for the brain-to-blood L-glutamate efflux.

Published

2017

10. Connexins and pannexins: from biology towards clinical targets

Author

Jacques-Antoine Haefliger and Paolo Meda

Subjects

0301 basic medicine, Cell signaling, Connexin, Cell Communication, Biology, Connexins, Ion Channels, 03 medical and health sciences, Insulin-Secreting Cells, Neoplasms, Renin, Extracellular, Humans, Biological Transport/physiology, Connexins/genetics, Connexins/metabolism, Endothelial Cells/metabolism, Gap Junctions/metabolism, Insulin-Secreting Cells/metabolism, Ion Channels/metabolism, Neoplasms/physiopathology, Neovascularization, Pathologic/metabolism, Renin/biosynthesis, Ion channel, Neovascularization, Pathologic, Gap junction, Endothelial Cells, Gap Junctions, Biological Transport, General Medicine, Pannexin, 3. Good health, Cell biology, 030104 developmental biology, Membrane channel, Function (biology)

Abstract

Efficient cell communication is a prerequisite for the coordinated function of tissues and organs. In vertebrates, this communication is mediated by a variety of mechanisms, including the exchange of molecules between cells, and between cells and the extracellular medium, via membrane channels made of connexin and pannexin proteins. These channels are a necessary component of all human tissues. Here, we review the biological essentials of the connexin and pannexin families, and the roles of these proteins in the function of cells which are central to major human diseases. We then discuss how connexins and pannexins participate in human pathology, and the clinical perspectives that this knowledge opens.

Published

2016

11. Microelectrodes and their use to assess ion channel function

Author

Martin J. Hug, Marc Chanson, and Aleksander Edelman

Subjects

Pulmonary and Respiratory Medicine, Ion Channel Gating/physiology, animal structures, Ion Channels, Polarized expression, Fluorescent Dyes/diagnostic use, Medicine, Animals, Epithelial Cells/physiology, Pediatrics, Perinatology, and Child Health, Gap junctions, Ion transporter, Ion channel, Biological Transport/physiology, Fluorescent Dyes, Membrane potential, Ion Transport, ddc:618, business.industry, Ion Transport/physiology, Biological Transport, Epithelial Cells, Microelectrode, Intracellular free ion concentration, Ion Channels/physiology, Pediatrics, Perinatology and Child Health, business, Ion Channel Gating, Microelectrodes, Biomedical engineering

Abstract

Impalement of living cells with microelectrodes (MEs) is a useful approach to measure a variety of biological parameters such as membrane potential (Vm), intracellular free ion concentrations and cell-to-cell communication. Despite such widespread applications, the number of trained researchers capable of using MEs is diminishing. In this article, we describe the fundamentals of the preparation and the proper use of MEs to study the physiology of transepithelial ion transport.

Published

2004

12. Urea movement across mouse colonic plasma membranes is mediated by UT-A urea transporters

Author

Frank Thévenod, Gavin Stewart, Robert A. Fenton, and Craig P. Smith

Subjects

Colon, Phloretin, Immunoblotting, RNA, Messenger/metabolism, Centrifugation, Phloretin/pharmacology, Kidney, Mice, chemistry.chemical_compound, Subcellular Fractions/metabolism, Membrane Transport Modulators, Urea, Animals, RNA, Messenger, Northern blot, Intestinal Mucosa, Transcellular, Biological Transport/physiology, Antiserum, Differential centrifugation, Microvilli, Hepatology, biology, Cell Membrane/metabolism, Immune Sera, Cell Membrane, Gastroenterology, Membrane Transport Proteins, Membrane Transport Proteins/antagonists & inhibitors, Biological Transport, Urea/metabolism, Blotting, Northern, Molecular biology, Colon/metabolism, Kidney/metabolism, Urea transport, chemistry, Biochemistry, Polyclonal antibodies, Immunologic Techniques, Microvilli/metabolism, biology.protein, Intestinal Mucosa/metabolism, Subcellular Fractions

Abstract

BACKGROUND & AIMS: Urea is a major nitrogen source for commensal bacteria that inhabit the large intestine. UT-A urea transporters mediate urea movement across plasma membranes. The aim of this study was to determine whether UT-A proteins are expressed in the mouse colon and, if so, whether they have a functional role in transcellular urea transport.METHODS: Mouse colonic UT-A transporters were investigated with Northern blot analysis, immunoblotting, immunolocalization, and refractive light flux experiments.RESULTS: Northern blot analysis showed that 4 UT-A transcripts were present in mouse colon. Two peptide-targeted polyclonal antibodies showed the presence of UT-A immunoreactive proteins in mouse colon. Antiserum ML446 targeted to the N-terminus of mouse UT-A1 detected proteins of 34 and 48 kilodaltons. Antiserum ML194 targeted to the C-terminus of mouse UT-A1 detected proteins of 48, 75, and 100 kilodaltons. Immunolocalization studies using ML446 showed the presence of UT-A proteins in cells throughout the colonic crypts. ML194 specifically stained cells located in the proliferative and stem regions of the lower portion of colonic crypts. Differential centrifugation and immunoblotting of colonic epithelia showed that UT-A proteins were present in plasma membrane-enriched fractions. Refractive light flux experiments using colonic plasma membrane vesicles showed a significant urea flux, which was completely inhibited by the UT-A inhibitor phloretin.CONCLUSIONS: Functional UT-A transporters are expressed in the plasma membranes of mouse colon, indicating that these proteins may play a key role in host/bacterial interaction.

Published

2004

13. Evaluation and Prediction of Drug Permeation

Author

Alessandra Pagliara, Bernard Testa, Pierre-Alain Carrupt, Marianne Reist, and Sandrine Geinoz

Subjects

Intestinal Absorption/physiology, Drug, Computer science, Chemistry, Pharmaceutical, media_common.quotation_subject, Pharmaceutical Science, Drug design, Nanotechnology, Models, Biological, Delivery problems, Pharmacokinetics, Pharmaceutical Preparations/chemistry/*metabolism, Animals, Humans, Pharmaceutical sciences, Biological Transport/physiology, media_common, Pharmacology, ddc:615, Drug permeation, Biological Transport, Intestinal Absorption, Pharmaceutical Preparations, Drug development, Target site, Biochemical engineering

Abstract

A major challenge confronting the pharmaceutical scientist is to optimize the selective and efficient delivery of new active entities and drug candidates. Successful drug development requires not only optimization of specific and potent pharmacodynamic activity, but also efficient delivery to the target site. Following advances in rational drug design, combinatorial chemistry and high-throughput screening techniques, the number of newly discovered and promising active compounds has increased dramatically in recent years, often making delivery problems the rate-limiting step in drug research. To overcome these problems, a good knowledge of the pharmacokinetic barriers encountered by bioactive compounds is required. This review gives an overview of the properties of relevant physiological barriers and presents some important biological models for evaluation of drug permeation and transport. Physicochemical determinants in drug permeation and the relevance of quantitative and qualitative approaches to the prediction and evaluation of passive drug absorption are also discussed.

Published

1999

14. Structure and binding of unconjugated bilirubin: relevance for physiological and pathophysiological function

Author

Pasupati Mukerjee, J. D. Ostrow, Claudio Tiribelli, Ostrow, Jd, Mukerjee, P, and Tiribelli, Claudio

Subjects

Molecular Structure, Chemistry, Cell Membrane, Bilirubin, Biological Transport, Stereoisomerism, Cell Biology, QD415-436, Biochemistry, Pathophysiology, Unconjugated bilirubin, Endocrinology, Liver metabolism, Liver, Solubility, Carrier protein, Humans, Bilirubin/chemistry* Bilirubin/metabolism Bilirubin/physiology Biological Transport/physiology Carrier Proteins Cell Membrane/metabolism Humans Liver/cytology Liver/metabolism Molecular Structure Solubility Stereoisomerism, Carrier Proteins, Function (biology)

Published

1994

15. Micro y nanocanales integrados: nuevas herramientas para control de movimiento molecular

Author

Hansford, D. (Derek)

Subjects

BIOMOLECULAR SEPARATIONS, APLICACIONES TERAPÉUTICAS, TRANSPORTE BIOLÓGICO - FISIOLOGÍA, NANOFLUIDOS, TECHNOLOGY IN HEALTH, SEPARACION BIOMOLECULAR, MICROFABRICACIÓN EN SILICIO Y POLÍMEROS, BIOLOGICAL TRANSPORT - PHYSIOLOGY, SILICON AND POLYMER MICROFABRICATION, NANOFLUIDICS, TECNOLOGÍAS PARA LA SALUD, THERAPEUTIC APPLICATIONS, RBI00057

Abstract

This paper presents a review of work on the fabrication and use of nanochannels in silicon and polymers for the control of molecular transport. The method of Sacrifi cial Layer Lithography is reviewed and demonstrated for silicon and polymers. A novel technique for the productions of conical nanopores through a polymer membrane is also reviewed. Nanochannels and nanopores have many potential applications for drug delivery, immunoprotection of cell implants, blocking of globular proteins from biosensor surfaces, and diagnostic devices. All of these applications benefi t from the more direct interactions of devices with biomolecules. El presente trabajo presenta una revisión literaria sobre los métodos de fabricación de nanocanales en silicio y diferentes materiales poliméricos; y su uso en control de transporte molecular. Se describe el método “Sacrifi cial Layer Lithography” para silicio y polímeros. Adicionalmente, una novedosa técnica para la producción de nanoporos cónicos a través de una membrana polimérica es descrita. Los nanocanales y los nanoporos poseen diversas aplicaciones potenciales en la liberación de drogas, en la inmunoprotección de implantes celulares, el bloqueo de proteínas globulares en la superfi cie de biosensores, y en dispositivos para diagnóstico. Todas estas aplicaciones se benefi cian de la interacción directa entre los dispositivos y las biomoléculas.

Published

2009

16. Requirement for aralar and its Ca2+-binding sites in Ca2+ signal transduction in mitochondria from INS-1 clonal beta-cells

Author

Beatriz Pardo, Andreas Wiederkehr, Jorgina Satrústegui, Claes B. Wollheim, Patricia Marmol, and Araceli del Arco

Subjects

Mutant, Amino Acid Motifs, Mitochondrion, Binding Sites/genetics, Biochemistry, Mitochondrial Membrane Transport Proteins, Mice, Insulin-Secreting Cells, Insulin Secretion, Glucose/metabolism, Insulin, Protein Isoforms, Cells, Cultured, Neurotransmitter Agents, Protein Isoforms/genetics/metabolism, biology, Mitochondrial Proteins/genetics/metabolism, Long-term potentiation, Mitochondria, Gene Knockdown Techniques, Insulin-Secreting Cells/cytology/metabolism, Gene isoform, Calcium/metabolism, NADP/biosynthesis, Calcium Signaling/physiology, Carbohydrate metabolism, Mitochondrial Proteins, Mitochondrial membrane transport protein, Animals, Calcium Signaling, Membrane Transport Proteins/genetics/metabolism, ddc:612, Mitochondria/genetics/metabolism, Molecular Biology, Biological Transport/physiology, Insulin/secretion, Calcium metabolism, Binding Sites, Membrane Transport Proteins, Biological Transport, Cell Biology, Molecular biology, Amino Acid Motifs/physiology, Glucose, Mutation, biology.protein, Calcium, Neurotransmitter Agents/metabolism, NAD+ kinase, NADP

Abstract

Aralar, the mitochondrial aspartate-glutamate carrier present in beta-cells, is a component of the malate-aspartate NADH shuttle (MAS). MAS is activated by Ca2+ in mitochondria from tissues with aralar as the only AGC isoform with an S0.5 of approximately 300 nm. We have studied the role of aralar and its Ca2+-binding EF-hand motifs in glucose-induced mitochondrial NAD(P)H generation by two-photon microscopy imaging in INS-1 beta-cells lacking aralar or expressing aralar mutants blocked for Ca2+ binding. Aralar knock-down in INS-1 beta-cell lines resulted in undetectable levels of aralar protein and complete loss of MAS activity in isolated mitochondria and in a 25% decrease in glucose-stimulated insulin secretion. MAS activity in mitochondria from INS-1 cells was activated 2-3-fold by extramitochondrial Ca2+, whereas aralar mutants were Ca2+ insensitive. In Ca2+-free medium, glucose-induced increases in mitochondrial NAD(P)H were small (1.3-fold) and unchanged regardless of the lack of aralar. In the presence of 1.5 mm Ca2+, glucose induced robust increases in mitochondrial NAD(P)H (approximately 2-fold) in cell lines with wild-type or mutant aralar. There was a approximately 20% reduction in NAD(P)H response in cells lacking aralar, illustrating the importance of MAS in glucose action. When small Ca2+ signals that resulted in extremely small mitochondrial Ca2+ transients were induced in the presence of glucose, the rise in mitochondrial NAD(P)H was maintained in cells with wild-type aralar but was reduced by approximately 50% in cells lacking or expressing mutant aralar. These results indicate that 1) glucose-induced activation of MAS requires Ca2+ potentiation; 2) Ca2+ activation of MAS represents a larger fraction of glucose-induced mitochondrial NAD(P)H production under conditions where suboptimal Ca2+ signals are associated with a glucose challenge (50 versus 20%, respectively); 3) inactivation of EF-hand motifs in aralar prevents activation of MAS by small Ca2+ signals. The results suggest a possible role for aralar and MAS in priming the beta-cell by Ca2+-mobilizing neurotransmitter or hormones.

Published

2008

17. Phosphorus control in peritoneal dialysis patients

Author

G.J. Vlachojannis, Taner Camsari, C.P. Stathakis, D.M. Evaggelos, Ibrahim Karayaylali, Athanasios C. Dimitriades, F. Fevzi Ersoy, A Yavuz, Dimitrios Tsakiris, Semra Bozfakioglu, Cengiz Utas, Mahmut Yavuz, Fehmi Akcicek, George Wu, Kenan Ates, Tekin Akpolat, Gultekin Suleymanlar, Dimitrios G. Oreopoulos, Rezzan Ataman, P. Tam, K.P. Katopodis, Turgay Arinsoy, Meral Gültekin, Ploumis Passadakis, N.A. Dombros, Cetin Ozener, Mehmet Emin Yilmaz, Ege Üniversitesi, Çukurova Üniversitesi, and OMÜ

Subjects

Male, medicine.medical_treatment, chemistry.chemical_compound, Hyperphosphatemia, renal osteodystrophy, Renal osteodystrophy, phosphorus, Phosphorus/*blood, biology, Calcium/blood, Hyperphosphatemia/blood/prevention & control, Middle Aged, peritoneal dialysis, Parathyroid Hormone, Nephrology, Creatinine, phosphorus control, Female, Adult, medicine.medical_specialty, Serum albumin, chemistry.chemical_element, Renal function, Peritoneal dialysis, Kidney Failure, Chronic/*blood/*therapy, Internal medicine, medicine, Humans, phosphate binders, Dialysis, Biological Transport/physiology, Peritoneal Dialysis/*methods, Aged, calcium, business.industry, Phosphorus, Biological Transport, Creatinine/blood, Alkaline Phosphatase, Phosphate, medicine.disease, Endocrinology, Cross-Sectional Studies, chemistry, Parathyroid Hormone/blood, biology.protein, Kidney Failure, Chronic, dialysis, business, Alkaline Phosphatase/blood

Abstract

WOS: 000254559100023, PubMed ID: 18379539, Hyperphosphatemia is independently associated with an increased risk of death among dialysis patients. In this study, we have assessed the status of phosphate control and its clinical and laboratory associations in a large international group of patients on chronic peritoneal dialysis (PD) treatment. This cross-sectional multicenter study was carried out in 24 centers in three different countries ( Canada, Greece, and Turkey) among 530 PD patients (235 women, 295 men) with a mean +/- s.d. age of 55716 years and mean duration of PD of 33 +/- 25 months. Serum calcium (Ca2+),ionized Ca2+, phosphate, intact parathyroid hormone (iPTH), 25-hydroxy vitamin D-3, 1,25-dihydroxy vitamin D3, total alkaline phosphatase, and bone alkaline phosphatase concentrations were investigated, along with adequacy parameters such as Kt/V, weekly creatinine clearance, and daily urine output. Mean Kt/V was 2.3 +/- 0.65, weekly creatinine clearance 78.5 +/- 76.6 l, and daily urine output 550 +/- 603 ml day(-1). Fifty-five percent of patients had a urine volume of = 9.5 mg per 100 ml in 250 patients (49%), between 8.5 and 9.5 mg per 100 ml in 214 patients (40%), and lower than 8.5 mg per 100 ml in 66 patients (12%). Ca x P product was > 55 mg(2) dl(-2) in 136 patients (26%) and lower than >55mg(2) dl(-2) in 394 patients (74%). Serum phosphorus levels were positively correlated with serum albumin (P

Published

2008

18. HIV-1 replication in dendritic cells occurs through a tetraspanin-containing compartment enriched in AP-3

Author

Eduardo Garcia, Vincent Piguet, and Damjan S. Nikolic

Subjects

CD4-Positive T-Lymphocytes, HIV Antigens, Virus Replication/physiology, Lysosome-Associated Membrane Glycoproteins/analysis, Cell Communication, Membrane Proteins/analysis/metabolism, Kangai-1 Protein, Virus Replication, Biochemistry, gag Gene Products, Human Immunodeficiency Virus, Tetraspanin, Viral Envelope Proteins, Structural Biology, RNA, Small Interfering, ddc:616, Platelet Membrane Glycoproteins/analysis, Membrane Glycoproteins, biology, Signal transducing adaptor protein, virus diseases, Compartment (chemistry), Adaptor Protein Complex delta Subunits, Cell biology, Kangai-1 Protein/analysis, Vesicular stomatitis virus, Cell Communication/physiology, Viral Envelope Proteins/physiology, HIV Antigens/analysis, Adaptor Protein Complex 3, Platelet Membrane Glycoproteins, Tetraspanin 29, Tetraspanin 28, Viral envelope, RNA Small Interfering/genetics, Antigens, CD, HIV-1/physiology, Genetics, Cytoplasmic Vesicles/chemistry/virology, HLA-DR Antigens/analysis, Humans, Gag Gene Products Human Immunodeficiency Virus/analysis, Molecular Biology, Antigens CD/analysis/metabolism, Biological Transport/physiology, Virion/chemistry/physiology, Tetraspanin 30, Cytoplasmic Vesicles, Virion, Lysosome-Associated Membrane Glycoproteins, Membrane Proteins, Biological Transport, Cell Biology, Adaptor Protein Complex 3/physiology, CD4-Positive T-Lymphocytes/virology, Dendritic Cells, HLA-DR Antigens, biology.organism_classification, Coculture Techniques, Viral replication, HIV-1, Adaptor Protein Complex delta Subunits/physiology, Dendritic Cells/metabolism/virology, CD81

Abstract

Dendritic cells (DC) are crucial components of the early events of HIV infection. Dendritic cells capture and internalize HIV at mucosal surfaces and efficiently transfer the virus to CD4+ T cells in trans through infectious synapses (trans-infection pathway). Alternatively, HIV-1 replicates in DC (R5-HIV-1) (cis-infection pathway). Here, we analyzed HIV trafficking in DC during the trans-infection pathway as well as the cis-infection pathway. Confocal immunofluorescence microscopy demonstrated that after capture by DC, R5-HIV-1 and HIV-1 pseudotyped with vesicular stomatitis virus protein G colocalized in a viral compartment enriched in tetraspanins including CD81, CD82 and CD9, although at different levels, indicating a role of the viral envelope in targeting to the tetraspanin-rich compartment. Replication of R5-HIV-1 in DC (cis-infection pathway) also led to the accumulation, in an envelope-independent manner, of mature viral particles in a tetraspanin-rich compartment. A fraction of the HIV-1-containing compartments appeared directly accessible from the cell surface. In sharp contrast with the trans-infection pathway, the delta-subunit of the adaptor protein 3 (AP-3) complex was enriched on the HIV-1-containing compartment during R5-HIV-1 replication in DC (cis-infection pathway). Downregulation of AP-3 delta-adaptin reduced significantly viral particle release from HIV-1-infected DC. Together, these studies demonstrate a role for AP-3 in HIV replication in a tetraspanin-rich compartment in DC and contribute to the elucidation of the trafficking pathways required for DC-T cell transfer of HIV-1 infection, a critical step during the early events of HIV infection.

Published

2007

19. Long-term cultures of polarized airway epithelial cells from patients with cystic fibrosis

Author

Lan Jornot, Tecla Dudez, Jean Silvain Lacroix, Thierry Rochat, Marc Chanson, Ludovic Wiszniewski, Susanne Suter, and Alessandra Pagano

Subjects

Pulmonary and Respiratory Medicine, Pathology, medicine.medical_specialty, Cystic Fibrosis, Cystic Fibrosis Transmembrane Conductance Regulator/metabolism, Clinical Biochemistry, Cell Culture Techniques, Epithelial Cells/cytology/metabolism, Cystic Fibrosis Transmembrane Conductance Regulator, Respiratory Mucosa, Biology, Cystic fibrosis, medicine, Cell Differentiation/physiology, Humans, Nasal polyps, Respiratory system, Fibroblast, Molecular Biology, Cell Shape, Biological Transport/physiology, Cells, Cultured, ddc:616, ddc:618, Cilium, Stem Cells, Interleukin-8, Mucin, Mucins, Cell Polarity, Biological Transport, Cell Differentiation, Epithelial Cells, Cell Biology, Cystic Fibrosis/physiopathology, Fibroblasts/cytology/metabolism, Fibroblasts, respiratory system, medicine.disease, Respiratory Mucosa/cytology, Epithelium, Cell biology, Electrophysiology, Mucins/metabolism, medicine.anatomical_structure, Interleukin-8/metabolism, Respiratory epithelium

Abstract

The poor ability of respiratory epithelial cells to proliferate and differentiate in vitro into a pseudostratified mucociliated epithelium limits the general use of primary airway epithelial cell (AEC) cultures generated from patients with rare diseases, such as cystic fibrosis (CF). Here, we describe a procedure to amplify AEC isolated from nasal polyps and generate long-term cultures of the respiratory epithelium. AEC were seeded onto microporous permeable supports that carried on their undersurface a preformed feeder layer of primary human airway fibroblasts. The use of fibroblast feeder layers strongly stimulated the proliferation of epithelial cells, allowing the expansion of the cell pool with successive passages. AEC at increasing passage were seeded onto supports undercoated with airway fibroblasts and exposed to air. Either freshly isolated or amplified AEC could differentiate into a pseudostratified mucociliated epithelium for at least 10 mo. Thus, CF epithelia cultures showed elevated Na+ transport, drastic hyperabsorption of surface liquid, and absence of cAMP-induced Cl- secretion as compared with non-CF cultures. They were also characterized by thick apical secretion that hampered the movement of cell surface debris by cilia. However, CF respiratory epithelia did not show increased production of mucins or IL-8. The method described here is now routinely used in our laboratory to establish long-term cultures of well differentiated respiratory epithelia from human airway biopsies.

Published

2006

20. Dynamic transport of SNARE proteins in the Golgi apparatus

Author

Allen Volchuk, James E. Rothman, Thomas H. Söllner, Oleg Varlamov, Mariella Ravazzola, Pierre Cosson, Lelio Orci, and Maurizio Di Liberto

Subjects

Blotting, Western, Golgi Apparatus, Fluorescent Antibody Technique, CHO Cells, Golgi Apparatus/metabolism/ultrastructure, Biology, symbols.namesake, Cricetulus, Cricetinae, Animals, Secretion, Transport Vesicles, ddc:612, Secretory pathway, Biological Transport/physiology, Multidisciplinary, Vesicle, Biological Transport, COPI, Biological Sciences, Golgi apparatus, Cell biology, Transport protein, Microscopy, Electron, Membrane protein, symbols, Golgi cisterna, SNARE Proteins/metabolism, Transport Vesicles/metabolism, SNARE Proteins

Abstract

Localization of a membrane protein in a subcellular compartment can be achieved by its retention in the compartment or by its continuous transport toward this compartment. Previous results have suggested that specific enzymes are localized in the Golgi apparatus at least in part by selective retention and exclusion from transport vesicles. However, the function of some Golgi SNARE (soluble N -ethylmaleimide-sensitive factor attachment protein receptor) proteins is not compatible with their exclusion from transport vesicles. To help understand the mechanism accounting for the localization of SNARE proteins in the Golgi apparatus, we analyzed their lateral distribution in the Golgi cisternae and their incorporation into transport vesicles. According to our results, all SNARE proteins are efficiently incorporated into transport vesicles, indicating that the localization of SNARE proteins in the Golgi apparatus is not based on a static retention mechanism. Detailed analysis suggested that incorporation into transport vesicles was more efficient for SNARE proteins restricted to the cis face of the Golgi as compared with SNAREs present at the trans face. Furthermore, overexpression of a cis-Golgi SNARE protein altered concomitantly its incorporation in transport vesicles and its intra-Golgi localization. These observations suggest that, contrary to resident Golgi enzymes, SNARE proteins are localized in the Golgi apparatus as the result of a dynamic transport equilibrium.

Published

2005

21. Endosome-to-cytosol transport of viral nucleocapsids

Author

Rémy Sadoul, Pierre-Philippe Luyet, Neil Emans, Jean Gruenberg, Isabelle Le Blanc, Anne Petiot, Robert G. Parton, Nicolas Demaurex, Charles Ferguson, Nathalie Mayran, Julien Fauré, Véronique Pons, Fraboulet, Sandrine, Biochemistry Department, Université de Genève = University of Geneva (UNIGE), Department of Molecular & Cell Biology [Berkeley], University of California [Berkeley] (UC Berkeley), University of California (UC)-University of California (UC), Institute for Molecular Bioscience, University of Queensland [Brisbane], Institut Pasteur Korea - Institut Pasteur de Corée, Réseau International des Instituts Pasteur (RIIP), Glycobiologie et signalisation cellulaire, Université Paris-Sud - Paris 11 (UP11)-Institut National de la Santé et de la Recherche Médicale (INSERM), Institute of Experimental Pathology, Department of Physiology, Centre médical universitaire, Neurodegenerescence et Plasticite, Université Joseph Fourier - Grenoble 1 (UJF)-Institut National de la Santé et de la Recherche Médicale (INSERM), This work was supported by the Swiss National Science Foundation (J.G.), the International Human Frontier Science Program (J.G and RGP), and the Australian National Health and Medical Research Council (RGP). ILB was supported by the award of the Bettencourt Foundation price (Prix des Jeunes Chercheurs), by the French Cancer Research Association (ARC) and by the Roche Foundation. VP was supported by the Roche Foundation and EMBO., University of Geneva [Switzerland], University of California [Berkeley], and University of California-University of California

Subjects

MESH: Signal Transduction, MESH: Vesicular Transport Proteins, Time Factors, viruses, Endocytic cycle, Vesicular Transport Proteins, MESH: Cricetinae, Epithelial Cells/virology, MESH: Microscopy, Fluorescence, Virus Replication, Membrane Fusion, Phosphoproteins/genetics/physiology, Lysophospholipids/physiology, Cytosol, Phosphatidylinositol Phosphates, MESH: Cytosol, MESH: Vesicular stomatitis Indiana virus, Cricetinae, Membrane Fusion/drug effects/physiology, MESH: Animals, Fibroblasts/virology, Sorting Nexins, Cytosol/metabolism/ultrastructure, 0303 health sciences, biology, Vesicle, 030302 biochemistry & molecular biology, MESH: Phosphatidylinositol Phosphates, 3. Good health, Cell biology, MESH: Cattle, Vesicular stomatitis virus, MESH: Epithelial Cells, MESH: RNA, Viral, ddc:540, Nucleocapsid/metabolism, RNA, Viral, Monoglycerides, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Virus Replication/genetics, MESH: Monoglycerides, Signal Transduction, Endosome, MESH: Biological Transport, MESH: Nucleocapsid, RNA, Viral/biosynthesis/metabolism, Endosomes, MESH: Microscopy, Electron, Transport Vesicles/metabolism/ultrastructure, MESH: Membrane Fusion, MESH: Phosphoproteins, Vesicular stomatitis Indiana virus, Article, MESH: Lysophospholipids, Cell Line, 03 medical and health sciences, Viral envelope, [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology, MESH: Transport Vesicles, Animals, Humans, Vesicular stomatitis Indiana virus/physiology, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, [SDV.NEU] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Nucleocapsid, Transport Vesicles, ddc:612, Biological Transport/physiology, 030304 developmental biology, Vesicular Transport Proteins/genetics/physiology, MESH: Humans, Endosomal Sorting Complexes Required for Transport, Signal Transduction/physiology, MESH: Time Factors, MESH: Virus Replication, Lipid bilayer fusion, Biological Transport, Epithelial Cells, Cell Biology, Fibroblasts, biology.organism_classification, Phosphoproteins, MESH: Cell Line, MESH: Hela Cells, Microscopy, Electron, Microscopy, Fluorescence, Cytoplasm, MESH: Endosomes, MESH: Fibroblasts, Phosphatidylinositol Phosphates/physiology, Cattle, Endosomes/metabolism/ultrastructure, Lysophospholipids, HeLa Cells

Abstract

International audience; During viral infection, fusion of the viral envelope with endosomal membranes and nucleocapsid release were thought to be concomitant events. We show here that for the vesicular stomatitis virus they occur sequentially, at two successive steps of the endocytic pathway. Fusion already occurs in transport intermediates between early and late endosomes, presumably releasing the nucleocapsid within the lumen of intra-endosomal vesicles, where it remains hidden. Transport to late endosomes is then required for the nucleocapsid to be delivered to the cytoplasm. This last step, which initiates infection, depends on the late endosomal lipid lysobisphosphatidic acid (LBPA) and its putative effector Alix/AIP1, and is regulated by phosphatidylinositol-3-phosphate (PtdIns3P) signalling via the PtdIns3P-binding protein Snx16. We conclude that the nucleocapsid is exported into the cytoplasm after the back-fusion of internal vesicles with the limiting membrane of late endosomes, and that this process is controlled by the phospholipids LBPA and PtdIns3P and their effectors.

Published

2005

22. Allogeneic red blood cell transfusions: efficacy, risks, alternatives and indications

Author

Madjdpour, C. and Spahn, D.R.

Subjects

Adaptation, Physiological/physiology, Anemia/physiopathology, Biological Transport/physiology, Communicable Diseases/etiology, Creutzfeldt-Jakob Syndrome/etiology, Erythrocyte Transfusion/adverse effects, Erythrocyte Transfusion/methods, Oxygen/physiology

Abstract

Careful assessment of risks and benefits has to precede each decision on allogeneic red blood cell (RBC) transfusion. Currently, a number of key issues in transfusion medicine are highly controversial, most importantly the influence of different transfusion thresholds on clinical outcome. The aim of this article is to review current evidence on blood transfusions, to highlight 'hot topics' with respect to efficacy, outcome and risks, and to provide the reader with transfusion guidelines. In addition, a brief synopsis of transfusion alternatives will be given. Based on up-to-date information of current evidence, together with clinical knowledge and experience, the physician will be able to make transfusion decisions that bear the lowest risk for the patient.

Published

2004

23. High-resolution dissection of phagosome maturation reveals distinct membrane trafficking phases

Author

Franz Bruckert, Thierry Soldati, Hans-Jörg Warnatz, Oliver Henschel, Daniel Gotthardt, and Michael Schleicher

Subjects

Thiazoles/metabolism, Adenosine Triphosphate/metabolism, Coronin, Vesicular Transport Proteins, Carrier Proteins/metabolism, Cathepsin D, R-SNARE Proteins, Rab GTP-Binding Proteins/metabolism, Adenosine Triphosphate, Phagosomes, Dictyostelium, Dictyostelium/cytology/metabolism, Cytoskeleton, Phagosome, Microfilament Proteins, Cell Membrane/chemistry/metabolism, Qb-SNARE Proteins, Lipids, Endocytosis, Cell biology, Biochemistry, Fluorescent Dyes/metabolism, Thiazolidines, Biological Markers, Endocytosis/physiology, SNARE Proteins, Endosome, Microfilament Proteins/metabolism, Lipids/chemistry, Biology, Karyopherins, Exocytosis, Article, Phagosome maturation, Animals, Molecular Biology, Biological Transport/physiology, Fluorescent Dyes, Phagosomes/chemistry/metabolism/ultrastructure, Proteins/chemistry/metabolism, Cell Membrane, Membrane Proteins, Proteins, rab7 GTP-Binding Proteins, Biological Transport, Cell Biology, Cathepsin D/metabolism, Bridged Bicyclo Compounds, Heterocyclic, Lipid Metabolism, Thiazoles, Bicyclo Compounds, Heterocyclic/metabolism, Membrane protein, rab GTP-Binding Proteins, Karyopherins/metabolism, biology.protein, Membrane Proteins/metabolism, Carrier Proteins, Biomarkers

Abstract

Molecular mechanisms of endocytosis in the genetically and biochemically tractable professional phagocyte Dictyostelium discoideum reveal a striking degree of similarity to higher eukaryotic cells. Pulse-chase feeding with latex beads allowed purification of phagosomes at different stages of maturation. Gentle ATP stripping of an actin meshwork entrapping contaminating organelles resulted in a 10-fold increase in yield and purity, as confirmed by electron microscopy. Temporal profiling of signaling, cytoskeletal, and trafficking proteins resulted in a complex molecular fingerprint of phagosome biogenesis and maturation. First, nascent phagosomes were associated with coronin and rapidly received a lysosomal glycoprotein, LmpB. Second, at least two phases of delivery of lysosomal hydrolases (cathepsin D [CatD] and cysteine protease [CPp34]) were accompanied by removal of plasma membrane components (PM4C4 and biotinylated surface proteins). Third, a phase of late maturation, preparing for final exocytosis of undigested material, included quantitative recycling of hydrolases and association with vacuolin. Also, lysosomal glycoproteins of the Lmp family showed distinct trafficking kinetics. The delivery and recycling of CatD was directly visualized by confocal microscopy. This heavy membrane traffic of cargos was precisely accompanied by regulatory proteins such as the Rab7 GTPases and the endosomal SNAREs Vti1 and VAMP7. This initial molecular description of phagocytosis demonstrates the feasibility of a comprehensive analysis of phagosomal lipids and proteins in genetically modified strains.

Published

2002

24. The LIM and SH3 domain-containing protein, lasp-1, may link the cAMP signaling pathway with dynamic membrane restructuring activities in ion transporting epithelia

Author

Xunsheng Chen, Christine Chaponnier, Richard S. Cameron, John A. Parente, and Catherine S. Chew

Subjects

Male, Myocardium/metabolism, src Homology Domains/ physiology, Fluorescent Antibody Technique, ddc:616.07, Actins/analysis, Chief Cells, Gastric/ metabolism/secretion, Proto-Oncogene Proteins c-myc/metabolism, Second Messenger Systems, 0302 clinical medicine, Proton transport, Cyclic AMP, Parietal Cells, Gastric/metabolism/secretion, Phosphorylation, Cytoskeleton, Parietal cell, Cyclic AMP/ metabolism, 0303 health sciences, Nuclear Proteins, Signal Transduction/ physiology, Cell biology, Gastric chief cell, medicine.anatomical_structure, Biochemistry, 030220 oncology & carcinogenesis, Rabbits, Intracellular, Signal Transduction, Blotting, Western, Biology, Proto-Oncogene Proteins c-myc, src Homology Domains, 03 medical and health sciences, Parietal Cells, Gastric, Cell cortex, Chief cell, medicine, Animals, Secretion, Muscle, Skeletal, Biological Transport/physiology, Second Messenger Systems/physiology, 030304 developmental biology, Homeodomain Proteins, Chief Cells, Gastric, Muscle, Skeletal/metabolism, Myocardium, Membrane Proteins, Proteins, Biological Transport, Cell Biology, Actins, Protein Structure, Tertiary, Cytoskeleton/metabolism, Homeodomain Proteins/ metabolism, Membrane Proteins/metabolism

Abstract

Lasp-1 is a unique LIM and src homology 3 (SH3) domain-containing protein that was initially identified as a 40 kDa cAMP-dependent phosphoprotein in the HCl-secreting gastric parietal cell. Because cAMP is a potent stimulator of parietal cell acid secretion, we have hypothesized that changes in lasp-1 phosphorylation might be involved in the regulation of ion transport-related activities, perhaps by modulating interactions among cytoskeletal and/or vesicle-associated proteins. In this study, we demonstrate that the cAMP-dependent acid secretory agonist, histamine, induces a rapid, sustained rise in parietal cell lasp-1 phosphorylation and this increase in phosphorylation is closely correlated with the acid secretory response. In addition, elevation of intracellular cAMP concentrations appear to induce a partial redistribution of lasp-1 from the cell cortex, where it predominates along with the gamma-isoform of actin in unstimulated cells, to the beta-actin enriched, apically-directed intracellular canalicular region, which is the site of active proton transport in the parietal cell. Additional studies demonstrate that although lasp-1 mRNA and protein are expressed in a wide range of tissues, the expression is specific for certain actin-rich cell types present within these tissues. For example, gastric chief cells, which contain relatively little F-actin and secrete the enzyme, pepsinogen, by regulated exocytosis, do not appear to express lasp-1. Similarly, lasp-1 was not detected in pancreatic acinar cells, which secrete enzymes by similar mechanisms and also contain relatively low levels of F-actin. Lasp-1 also was not detectable in proximal tubules in the kidney, in gastrointestinal smooth muscle, heart or skeletal muscle. In contrast, expression was prominent in the cortical regions of ion-transporting duct cells in the pancreas and in the salivary parotid gland as well as in certain F-actin-rich cells in the distal tubule/collecting duct. Interestingly, moderate levels of expression were also detected in podocytes present in renal glomeruli and in vascular endothelium. In primary cultures of gastric fibroblasts, lasp-1 was present mainly within the tips of lamellipodia and at the leading edges of membrane ruffles. Taken together these results support the hypothesis that the lasp-1 plays an important role in the regulation of dynamic actin-based, cytoskeletal activities. Agonist-dependent changes in lasp-1 phosphorylation may also serve to regulate actin-associated ion transport activities, not only in the parietal cell but also in certain other F-actin-rich secretory epithelial cell types.

Published

2000

25. Blockade of membrane transport and disassembly of the Golgi complex by expression of syntaxin 1A in neurosecretion-incompetent cells: prevention by rbSEC1

Author

Rowe, J., Corradi, N., MARIA LUISA MALOSIO, Taverna, E., Halban, P., Meldolesi, J., and Rosa, P.

Subjects

ddc:616, Neurosecretory Systems/ physiology, Cell Membrane, Vesicular Transport Proteins, Golgi Apparatus, Syntaxin 1, Biological Transport, Nerve Tissue Proteins, Cell Biology, Transfection, Neurosecretory Systems, PC12 Cells, Exocytosis, Nerve Tissue Proteins/ biosynthesis/ physiology, Cell Line, Rats, Munc18 Proteins, Cell Membrane/physiology, Antigens, Surface, Exocytosis/physiology, Animals, Antigens, Surface/ biosynthesis, Golgi Apparatus/ metabolism/ultrastructure, Biological Transport/physiology

Abstract

The t-SNAREs syntaxin1A and SNAP-25, i.e. the members of the complex involved in regulated exocytosis at synapses and neurosecretory cells, are delivered to their physiological site, the plasma membrane, when transfected into neurosecretion-competent cells, such as PC12 and AtT20. In contrast, when transfection is made into cells incompetent for neurosecretion, such as those of a defective PC12 clone and the NRK fibroblasts, which have no endogenous expression of these t-SNAREs, syntaxin1A (but neither two other syntaxin family members nor SNAP-25) remains stuck in the Golgi-TGN area with profound consequences to the cell: blockade of both membrane (SNAP-25, GAT-1) and secretory (chromogranin B) protein transport to the cell surface; progressive disassembly of the Golgi complex and TGN; ultimate disappearance of the latter structures, with intermixing of their markers (mannosidase II; TGN-38) with those of the endoplasmic reticulum (calreticulin) and with syntaxin1A itself. When, however, syntaxin 1A is transfected together with rbSec1, a protein known to participate in neurosecretory exocytosis via its dynamic interaction with the t-SNARE, neither the blockade nor the alterations of the Golgi complex take place. Our results demonstrate that syntaxin1A, in addition to its role in exocytosis at the cell surface, possesses a specific potential to interfere with intracellular membrane transport and that its interaction with rbSec1 is instrumental to its physiological function not only at the plasma membrane but also within the cell. At the latter site, the rbSec1-induced conversion of syntaxin1A into a form that can be transported and protects the cell from the development of severe structural and membrane traffic alterations.

Published

1999

26. Glutamate Transporter GLT-1 Is Transiently Localized on Growing Axons of the Mouse Spinal Cord before Establishing Astrocytic Expression

Author

Masabumi Nagashima, Masahiko Watanabe, Keiko Yamada, Yoshiro Inoue, Kohichi Tanaka, and Takashi Shibata

Subjects

Pathology, Time Factors, Amino Acid Transport System X-AG, Immunohistochemistry, Neurons/chemistry, Amino Acid Sequence, Mice, Spinal Cord/growth & development, Spinal Cord/chemistry, Astrocytes/chemistry, Biological Transport/physiology, In Situ Hybridization, Neurons, General Neuroscience, Spinal Cord/embryology, Nerve Tissue Proteins/analysis, Marginal zone, medicine.anatomical_structure, Spinal Cord, Axons/chemistry, medicine.medical_specialty, Enolase, Molecular Sequence Data, Nerve Tissue Proteins, In situ hybridization, Biology, Article, White matter, Embryonic and Fetal Development, medicine, Animals, Antibody Formation, Mantle zone, Biological Transport, Mice, Inbred C57BL, ATP-Binding Cassette Transporters/analysis, Spinal cord, Embryonic stem cell, Axolemma, Axons, Embryonic and Fetal Development/physiology, nervous system, Neurons/ultrastructure, Astrocytes, ATP-Binding Cassette Transporters

Abstract

The glutamate transporter GLT-1 is expressed in astrocytes of the mature brain and spinal cord. In the present study, we examined its expression in the developing mouse spinal cord. Byin situhybridization,35S-labeled antisense oligonucleotide probes for GLT-1 mRNA consistently labeled the mantle zone/gray matter from embryonic day 11 through the adult stage. However, immunohistochemistry with a specific antibody visualized distinct regional and cellular localizations during the time between the fetal and postnatal stages. At fetal stages, GLT-1 immunoreactivity predominated in the marginal zone/white matter, observed as tiny puncta in cross-sections and as thin fibers in longitudinal sections. The GLT-1-immunopositive structures were also labeled for neuron-specific enolase, a glycolytic enzyme specific to postmitotic neurons and endocrine cells. By electron microscopy, GLT-1 immunoreactivity was detected in axons forming frequent enlargements and was focally localized on a small portion of the axolemma, particularly that facing adjacent axons. At early postnatal stages, GLT-1 disappeared from axons in white matter tracts and, instead, appeared in astrocytic processes surrounding various neuronal elements in the gray matter. Therefore, before switching to astrocytic expression, GLT-1 is transiently expressed in neurons and localized in differentiating axons. Together with our previous finding on the localization of glutamate transporter GLAST in radial glial fibers, GLT-1 and GLAST are thus localized during development on distinct directional cellular elements along which young neurons elongate their axons or move their cell bodies, respectively.

Published

1998

27. The role of intracellular glutathione and ligand physicochemical properties in the hepatic transport of organic anions

Author

Claudio Tiribelli and Tiribelli, Claudio

Subjects

Anions, Liver/metabolism, Chemical Phenomena, Animals, Anions/metabolism, Biological Transport/physiology, Chemistry, Physical, Glutathione/physiology, Ligands, Liver/metabolism, Physicochemical Phenomena, Chemistry, Physical, Anions/metabolism, Biological Transport, Physicochemical Phenomena, Ligands, Glutathione, Chemistry, Liver, Physical, Animals, Glutathione/physiology, Biological Transport/physiology

Abstract

No abstract

28. Structural plasticity of the cardiac nuclear pore complex in response to regulators of nuclear import

Author

Carmen Perez-Terzic, Franklyn G. Prendergast, Petras P. Dzeja, Marisa Jaconi, Michel Pucéat, Ryan Bortolon, Andre Terzic, and A. Marquis Gacy

Subjects

Calcium Channel Blockers/pharmacology, Nuclear Envelope, Egtazic Acid/analogs & derivatives/pharmacology, Physiology, ddc:616.07, Biology, Myocardium/ cytology, Rats, Sprague-Dawley, Calcium/physiology, Nuclear Envelope/metabolism/ physiology, Animals, Myocyte, Thapsigargin/pharmacology, Nuclear pore, Egtazic Acid, Calcimycin, Biological Transport/physiology, Calcimycin/pharmacology, Nucleoplasm, Myocardium, Biological Transport, Anatomy, Calcium Channel Blockers, Adaptation, Physiological, Rats, Ion homeostasis, Nucleocytoplasmic Transport, Cytoplasm, Biophysics, Thapsigargin, Calcium, Nucleoporin, Nuclear transport, Cardiology and Cardiovascular Medicine

Abstract

Abstract —Communication between the cytoplasm and nucleoplasm of cardiac cells occurs by molecular transport through nuclear pores. In lower eukaryotes, nuclear transport requires the maintenance of cellular energetics and ion homeostasis. Although heart muscle is particularly sensitive to metabolic stress, the regulation of nuclear transport through nuclear pores in cardiomyocytes has not yet been characterized. With the use of laser confocal and atomic force microscopy, we observed nuclear transport in cardiomyocytes and the structure of individual nuclear pores under different cellular conditions. In response to the depletion of Ca 2+ stores or ATP/GTP pools, the cardiac nuclear pore complex adopted 2 distinct conformations that led to different patterns of nuclear import regulation. Depletion of Ca 2+ indiscriminately prevented the nuclear import of macromolecules through closure of the nuclear pore opening. Depletion of ATP/GTP only blocked facilitated transport through a simultaneous closure of the pore and relaxation of the entire complex, which allowed other molecules to pass into the nucleus through peripheral routes. The current study of the structural plasticity of the cardiac nuclear pore complex, which was observed in response to changes in cellular conditions, identifies a gating mechanism for molecular translocation across the nuclear envelope of cardiac cells. The cardiac nuclear pore complex serves as a conduit that differentially regulates nuclear transport of macromolecules and provides a mechanism for the control of nucleocytoplasmic communication in cardiac cells, in particular under stress conditions associated with disturbances in cellular bioenergetics and Ca 2+ homeostasis.

29. Golgi bypass: skirting around the heart of classical secretion

Author

Grieve, A., Rabouille, C., Grieve, A., and Rabouille, C.

Abstract

Classical secretion consists of the delivery of transmembrane and soluble proteins to the plasma membrane and the extracellular medium, respectively, and is mediated by the organelles of the secretory pathway, the Endoplasmic Reticulum (ER), the ER exit sites, and the Golgi, as described by the Nobel Prize winner George Palade (Palade 1975). At the center of this transport route, the Golgi stack has a major role in modifying, processing, sorting, and dispatching newly synthesized proteins to their final destinations. More recently, however, it has become clear that an increasing number of transmembrane proteins reach the plasma membrane unconventionally, either by exiting the ER in non-COPII vesicles or by bypassing the Golgi. Here, we discuss the evidence for Golgi bypass and the possible physiological benefits of it. Intriguingly, at least during Drosophila development, Golgi bypass seems to be mediated by a Golgi protein, dGRASP, which is found ectopically localized to the plasma membrane. [KEYWORDS: Biological Transport/physiology, Cell Membrane, Gene Expression Regulation, Golgi Apparatus/ physiology, Proteins/ metabolism], Classical secretion consists of the delivery of transmembrane and soluble proteins to the plasma membrane and the extracellular medium, respectively, and is mediated by the organelles of the secretory pathway, the Endoplasmic Reticulum (ER), the ER exit sites, and the Golgi, as described by the Nobel Prize winner George Palade (Palade 1975). At the center of this transport route, the Golgi stack has a major role in modifying, processing, sorting, and dispatching newly synthesized proteins to their final destinations. More recently, however, it has become clear that an increasing number of transmembrane proteins reach the plasma membrane unconventionally, either by exiting the ER in non-COPII vesicles or by bypassing the Golgi. Here, we discuss the evidence for Golgi bypass and the possible physiological benefits of it. Intriguingly, at least during Drosophila development, Golgi bypass seems to be mediated by a Golgi protein, dGRASP, which is found ectopically localized to the plasma membrane. [KEYWORDS: Biological Transport/physiology, Cell Membrane, Gene Expression Regulation, Golgi Apparatus/ physiology, Proteins/ metabolism]

Published

2011

30. Transcriptional profiling of transport mechanisms and regulatory pathways in rat choroid plexus

Author

Andreassen, Søren N, Toft-Bertelsen, Trine L, Wardman, Jonathan H, Villadsen, René, MacAulay, Nanna, Andreassen, Søren N, Toft-Bertelsen, Trine L, Wardman, Jonathan H, Villadsen, René, and MacAulay, Nanna

Abstract

BACKGROUND: Dysregulation of brain fluid homeostasis associates with brain pathologies in which fluid accumulation leads to elevated intracranial pressure. Surgical intervention remains standard care, since specific and efficient pharmacological treatment options are limited for pathologies with disturbed brain fluid homeostasis. Such lack of therapeutic targets originates, in part, from the incomplete map of the molecular mechanisms underlying cerebrospinal fluid (CSF) secretion by the choroid plexus.METHODS: The transcriptomic profile of rat choroid plexus was generated by RNA Sequencing (RNAseq) of whole tissue and epithelial cells captured by fluorescence-activated cell sorting (FACS), and compared to proximal tubules. The bioinformatic analysis comprised mapping to reference genome followed by filtering for type, location, and association with alias and protein function. The transporters and associated regulatory modules were arranged in discovery tables according to their transcriptional abundance and tied together in association network analysis.RESULTS: The transcriptomic profile of choroid plexus displays high similarity between sex and species (human, rat, and mouse) and lesser similarity to another high-capacity fluid-transporting epithelium, the proximal tubules. The discovery tables provide lists of transport mechanisms that could participate in CSF secretion and suggest regulatory candidates.CONCLUSIONS: With quantification of the transport protein transcript abundance in choroid plexus and their potentially linked regulatory modules, we envision a molecular tool to devise rational hypotheses regarding future delineation of choroidal transport proteins involved in CSF secretion and their regulation. Our vision is to obtain future pharmaceutical targets towards modulation of CSF production in pathologies involving disturbed brain water dynamics.

Published

2022

31. Nuclear magnetic resonance spectroscopic characterization of peptide based nanocarriers and cargo complexes

Author

Eudes, François, Hazendonk, Paul, Banwo, Inumidun Damilola, University of Lethbridge. Faculty of Arts and Science, Eudes, François, Hazendonk, Paul, Banwo, Inumidun Damilola, and University of Lethbridge. Faculty of Arts and Science

Abstract

Cell penetrating peptides (CPPs) are short peptide 8-30 amino acids polypeptides that can deliver various molecules (nanoparticles to large fragment DNA) to subcellular locations such as the plastid organelles, cytoplasm, and nucleus etc. CPPs are characterized by containing clusters of cationic side chains that allow them to interact directly with the polar membrane surface, which enables then to enter the cell. One of the function of CPPs are to deliver cargo molecules such as DNA and RNA into cells. Most application have been developed for animal cells; however, the use of CPPs in plant cells remain a small researched field because of insufficient understanding of their mode of uptake. The present research describes firstly, the use of NMR technique to elucidate the structural properties of CPP-DNA complexation. Secondly the dynamic of the complexation. Finally, to relate the observations to their translocation mechanism. For this study, short peptides such as; arginine (R), tri-arginine (R3), nano-arginine (R9), and Tat2 (RKKRRQRRRRKKRRQRRR) were complexed with single-stranded and double-stranded DNA 5’ AGTCC 3’. The interaction between the single-stranded and double-stranded DNA 5’ AGTCC 3’ with the peptides was compared to understand how different DNA strands can influence complex formation. These complexes are used at relatively high concentrations; hence, measurements were at millimolar concentration. Therefore, for the study of DNA-CPP complexes, both non-isotopically enriched DNA and CPP samples were used. The reason for using such samples is to see if complexation can be observed using NMR spectroscopy, which will reduce the use of costly materials.

Published

2018

32. Inhibition of insulin-stimulated hydrogen peroxide production prevents stimulation of sodium transport in A6 cell monolayers.

Author

Markadieu, Nicolas, Crutzen, Raphaël, Boom, Alain, Erneux, Christophe, Beauwens, Renaud, Markadieu, Nicolas, Crutzen, Raphaël, Boom, Alain, Erneux, Christophe, and Beauwens, Renaud

Abstract

Insulin-stimulated sodium transport across A6 cell (derived from amphibian distal nephron) monolayers involves the activation of a phosphatidylinositol (PI) 3-kinase. We previously demonstrated that exogenous addition of H2O2 to the incubation medium of A6 cell monolayers provokes an increase in PI 3-kinase activity and a subsequent rise in sodium transport (Markadieu N, Crutzen R, Blero D, Erneux C, Beauwens R. Am J Physiol Renal Physiol 288: F1201-F1212, 2005). We therefore questioned whether insulin would produce an intracellular burst of H2O2 leading to PI 3-kinase activation and subsequent increase in sodium transport. An acute production of reactive oxygen species (ROS) in A6 cells incubated with the oxidation-sensitive fluorescent probe 5,6-chloromethyl-2',7'-dichlorodihydrofluorescein diacetate was already detected after 2 min of insulin stimulation. This fluorescent signal and the increase in sodium transport were completely inhibited in monolayers incubated with peggylated catalase, indicating that H2O2 is the main intracellular ROS produced upon insulin stimulation. Similarly, preincubation of monolayers with different chelators of either superoxide (O2(*-); nitro blue tetrazolium, 100 microM) or H2O2 (50 microM ebselen), or blockers of NADPH oxidase (Nox) enzymes (diphenyleneiodonium, 5 microM; phenylarsine oxide, 1 microM and plumbagin, 30 microM) prevented both insulin-stimulated H2O2 production and insulin-stimulated sodium transport. Furthermore, diphenyleneiodonium pretreatment inhibited the recruitment of the p85 PI 3-kinase regulatory subunit in an anti-phosphotyrosine immunoprecipitate in insulin-stimulated cells. In contrast, PI-103, an inhibitor of class IA PI 3-kinase, inhibited insulin-stimulated sodium transport but did not significantly reduce insulin-stimulated H2O2 production. Taken together, our data suggest that insulin induces an acute burst of H2O2production which participates in an increase in phosphatidylinositol 3,4,5-trisphosphate, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2009

33. Interactions between phosphatidylethanolamine headgroup and LmrP, a multidrug transporter: a conserved mechanism for proton gradient sensing?

Author

Hakizimana, Pierre, Masureel, Matthieu, Gbaguidi, Bénédicte, Ruysschaert, Jean Marie, Govaerts, Cédric, Hakizimana, Pierre, Masureel, Matthieu, Gbaguidi, Bénédicte, Ruysschaert, Jean Marie, and Govaerts, Cédric

Abstract

In a number of cases, the function of membrane proteins appears to require the presence of specific lipid species in the bilayer. We have shown that the secondary multidrug transporter LmrP requires the presence of phosphatidylethanolamine (PE), as its replacement by phosphatidylcholine (PC) inhibits transport activity and directly affects its structure, although the underlying mechanism was unknown. Here, we show that the effect of PE on the structure and the function of LmrP is mediated by interactions between the lipid headgroup and the protein. We used methyl-PE and dimethyl-PE analogs of PE to show that only replacement of the three hydrogens by methyl moieties leads to changes in the biochemical and biophysical properties of the reconstituted protein. This suggests that LmrP does not depend on the bulk properties of the phospholipids tested but solely on the hydrogen bonding ability of the headgroup. We then show that a single point mutation in LmrP, D68C, is sufficient to recapitulate precisely every biochemical and biophysical effect observed when PE is replaced by PC, including energy transfer between the protein tryptophan residues and the lipid headgroups. We conclude that the negatively charged Asp-68 is likely to participate in the interaction with PE and that such interaction is required for proton gradient sensing, substrate binding, and transport. Because Asp-68 belongs to a highly conserved motif in the Major Facilitator Superfamily (which includes LacY and EmrD), this interaction might be a general feature of these transporters that is involved in proton gradient sensing and lipid dependence., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2008

34. Cationic liposomal lipids: from gene carriers to cell signaling

Author

Lonez, Caroline, Vandenbranden, Michel, Ruysschaert, Jean Marie, Lonez, Caroline, Vandenbranden, Michel, and Ruysschaert, Jean Marie

Abstract

Cationic lipids are positively charged amphiphilic molecules which, for most of them, form positively charged liposomes, sometimes in combination with a neutral helper lipid. Such liposomes are mainly used as efficient DNA, RNA or protein carriers for gene therapy or immunization trials. Over the past decade, significant progress has been made in the understanding of the cellular pathways and mechanisms involved in lipoplex-mediated gene transfection but the interaction of cationic lipids with cell components and the consequences of such an interaction on cell physiology remains poorly described. The data reported in the present review provide evidence that cationic lipids are not just carriers for molecular delivery into cells but do modify cellular pathways and stimulate immune or anti-inflammatory responses. Considering the wide number of cationic lipids currently available and the variety of cellular components that could be involved, it is likely that only a few cationic lipid-dependent functions have been identified so far. © 2008 Elsevier Ltd. All rights reserved., Journal Article, Research Support, Non-U.S. Gov't, Review, info:eu-repo/semantics/published

Published

2008

35. Mapping protein dynamics in catalytic intermediates of the redox-driven proton pump cytochrome c oxidase.

Author

Busenlehner, Laura S, Salomonsson, Lina, Brzezinski, Peter, Armstrong, Richard N, Busenlehner, Laura S, Salomonsson, Lina, Brzezinski, Peter, and Armstrong, Richard N

Published

2006

36. Expression, distribution and functions of organic anion transporters in the rat epididymis.

Author

Leung, Chi Ting Gideon., Chinese University of Hong Kong Graduate School. Division of Physiology., Leung, Chi Ting Gideon., and Chinese University of Hong Kong Graduate School. Division of Physiology.

Abstract

Another family of organic anion transporters, the multi-drug resistant-associated-protein (MRP) is another subject of my study. Reverse transcription PCR and immunohistochernistry showed that MRP1 is expressed by the basal cells. MRP1 was cloned from the rat epididymis and expressed in HEK cells with a view to delineate its functions. HEK cells expressed with MRP1 showed little accumulation of calcein-AM compared to cells not expressed with the protein, or cells expressed with the protein but treated with MK571, an inhibitor of MRP1. This ability of MRP1 to eliminate calcein-AM from the cells was competitively reduced by verapamil, omeprazole, lonidamine or methotrexate, all are pharmacological agents commonly used for diverse clinical conditions. These results indicate that MRP1 is a multi-specific drug transporter. Freshly isolated basal cells also excluded verapamil and this effect was blocked by MK571., In summary, my work has focused on the expression, distribution and functions of two major organic anion transporters, OAT1 and MRP1 thought to be the molecular entities involved in the transport of organic substances across the epididymal tubule. This membrane- and cell-specific placement of the two organic anion transporters that have different substrate specificity and mediate counter flows of substrates offer a mechanism whereby organic substance entry into the epididymis can be 'filtered'. Having low substrate specificity, OAT1 indiscriminately brings into the cells a diverse spectrum of organic anions, some of which might be useful organic substances that nourish spermatozoa, while others could be sperm toxicants. By virtue of the drug-specific MRP1, basal cells expel some of these toxicants from the epididymis. In this way, basal cells play a protective role. They prevent access of foreign substances to spermatozoa stored in the epididymis. This hypothesis is speculative albeit an attractive one. Further work is required to lay the experimental groundwork for this hypothesis., The functions of OAT1 in the rat epididymis were studied by measuring the secretion (basal-to-apical) of PAH by epididymal epithelia in culture. The transport exhibited non-genomic up-regulation and down-regulation by PKA and PKC, respectively. These short-term regulations are not unlike those reported for the kidney OAT1 and are thought mediated through agonists-stimulated MAPK, PLA2 or COX-1 pathway. Since COX-1 has previously been shown to be exclusively present in the basal cells, it is conceivable that organic anion transport by the principal cells is regulated by the basal cells in the manner that principal cell Cl- secretion is regulated by the basal cells., The nature of my work is to study the way by which organic substances cross the blood-epididymis barrier. My work is inspired by the anatomical and functional analogies between the epididymis and the kidney tubule. In the latter, elimination of toxic metabolites and foreign substances are known to occur through arrays of membrane proteins uniquely adapted to transport cationic and anionic organic substances across membranes. My work is to unravel the role of organic anion transporters in the epididymis using a combination of molecular biology and cellular physiology techniques carried out on cultured epithelia as well as on freshly isolated cells from the rat epididymis., Using RT-PCR and Western Blot analysis, I identified the expression of organic anion transporter genes, OAT1, OAT2 and OAT3 mRNA in the rat epididymis. Immunohistochemistry revealed that OAT1 protein is present in the basal side of the principal cells of both the corpus and cauda epididymidis. OAT3 is seen in the lamina propria and blood vessels but not on the principal or other epithelial cells. Immunohistochemistry, however, failed to detect OAT2 protein. OAT1 was cloned from the rat cauda epididymidis using standard cloning techniques and verified by gene sequencing. Functional studies of the cloned protein expressed in human embryonic kidney (HEK) cells revealed similarities between the rat epididymal OAT1 and kidney OAT1 in that both transporters take up para-aminohippurate (PAH) into cells with similar kinetics and efficacy. Rat epididymal OAT1 was able to take up the anti-fertility drug, lonidamine., Leung Chi Ting Gideon., "October 2006.", Adviser: P. Y. D. Wong., Source: Dissertation Abstracts International, Volume: 68-09, Section: B, page: 5678., Thesis (Ph.D.)--Chinese University of Hong Kong, 2006., Includes bibliographical references (p. 122-143)., Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web., Electronic reproduction. [Ann Arbor, MI] : ProQuest Information and Learning, [200-] System requirements: Adobe Acrobat Reader. Available via World Wide Web., s in English and Chinese., School code: 1307., isbn: 9780549230861, Use of this resource is governed by the terms and conditions of the Creative Commons “Attribution-NonCommercial-NoDerivatives 4.0 International” License (http://creativecommons.org/licenses/by-nc-nd/4.0/)

Published

2006

37. Asn229 in the third helix of VPAC1 receptor is essential for receptor activation but not for receptor phosphorylation and internalization: comparison with Asn216 in VPAC2 receptor.

Author

Nachtergael, Ingrid, Gaspard, Nathalie, Langlet, Christelle, Robberecht, Patrick, Langer, Ingrid, Nachtergael, Ingrid, Gaspard, Nathalie, Langlet, Christelle, Robberecht, Patrick, and Langer, Ingrid

Abstract

After stimulation with agonist, G protein coupled receptors (GPCR) undergo conformational changes that allow activation of G proteins to transduce the signal, followed by phosphorylation by kinases and arrestin binding to promote receptor internalization. Actual paradigm, based on a study of GPCR-A/rhodopsin family, suggests that a network of interactions between conserved residues located in transmembrane (TM) domains (mainly TM3, TM6 and TM7) is involved in the molecular switch leading to GPCR activation. We evaluated in CHO cells expressing the VPAC(1) receptor the role of the third transmembrane helix in agonist signalling by point mutation into Ala of the residues highly conserved in the secretin-family of receptors: Y(224), N(229), F(230), W(232), E(236), G(237), Y(239), L(240). N(229)A VPAC(1) mutant was characterized by a decrease in both potency and efficacy of VIP stimulated adenylate cyclase activity, by the absence of agonist stimulated [Ca(2+)](i) increase, by a preserved receptor recognition of agonists and antagonist and by a preserved sensitivity to GTP suggesting the importance of that residue for efficient G protein activation. N(229)D mutant was not expressed at the membrane, and the N(229)Q with a conserved mutation was less affected than the A mutant. Agonist stimulated phosphorylation and internalization of N(229)A and N(229)Q VPAC(1) were unaffected. However, the re-expression of internalized mutant receptors, but not that of the wild type receptor, was rapidly reversed after VIP washing. Receptor phosphorylation, internalization and re-expression may be thus dissociated from G protein activation and linked to another active conformation that may influence its trafficking. Mutation of that conserved amino acid in VPAC(2) could be investigated only by a conservative mutation (N(216)Q) and led to a receptor with a low VIP stimulation of adenylate cyclase, receptor phosphorylation and internalization. This indicated the importance of the conserve, Comparative Study, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2006

38. Impaired enzyme-to-enzyme channelling between hexokinase isoenzyme(s) and phosphoglucoisomerase in rat pancreatic islets incubated at a low concentration of D-glucose.

Author

Zhang, Ying, Jijakli, Hassan, Courtois, Philippe, Sener, Abdullah, Malaisse, Willy, Zhang, Ying, Jijakli, Hassan, Courtois, Philippe, Sener, Abdullah, and Malaisse, Willy

Abstract

It was recently proposed that in rat pancreatic islets exposed to 8.3 mM D-glucose, alpha-D-glucose-6-phosphate undergoes enzyme-to-enzyme channelling between hexokinase isoenzyme(s) and phosphoglucoisomerase. To explore the identity of the hexokinase isoenzyme(s) involved in such a tunnelling process, the generation of 3HOH from the alpha- and beta-anomers of either D-[2-3H]glucose or D-[5-3H]glucose was now measured over 60 min incubation at 4 degrees C in pancreatic islets exposed only to 2.8 mM D-glucose, in order to decrease the relative contribution of glucokinase to the phosphorylation of the hexose. Under these experimental conditions, the ratio for 3HOH production from D-[2-3H]glucose/D-[5-3H]glucose at anomeric equilibrium (39.7 +/- 11.6%) and the beta/alpha ratios for the generation of 3HOH from either the D-[2-3H]glucose anomers (70.9 +/- 12.6%) or the D-[5-3H]glucose anomers (59.6 +/- 12.4%) indicated that a much greater fraction of alpha-D-glucose-6-phosphate escapes from the process of enzyme-to-enzyme channelling in the islets exposed to 2.8 mM, rather than 8.3 mM D-glucose. These findings suggest, therefore, that the postulated process of enzyme-to-enzyme channelling involves mainly glucokinase., In Vitro, Journal Article, Research Support, Non-U.S. Gov't, FLWIN, info:eu-repo/semantics/published

Published

2005

39. Rafts can trigger contact-mediated secretion of bacterial effectors via a lipid-based mechanism.

Author

van der Goot, Françoise G, Tran van Nhieu, Guy, Allaoui, Abdelmounaaim, Sansonetti, Philippe, Lafont, Frank, van der Goot, Françoise G, Tran van Nhieu, Guy, Allaoui, Abdelmounaaim, Sansonetti, Philippe, and Lafont, Frank

Abstract

Infection by the Gram-negative bacterial pathogen Shigella flexneri depends on its ability to invade host cells. Bacterial engulfment requires a functional type III secretion system (TTSS) allowing the translocation into host cells of bacterial effectors that activate cell-signaling cascades. We demonstrated previously that specialized lipid membrane domains enriched in cholesterol and sphingolipids (rafts) are involved during early steps of invasion, namely in binding and host cell entry. In this study, we addressed the issue of contact-mediated secretion by the TTSS. We show that contact-mediated and TTSS-induced hemolysis depend on the presence of cholesterol on the host cell surface. We found that purified detergent resistant membranes were able to activate TTSS. Finally, we found that artificial liposomes, devoid of proteins, were able to activate the TTSS but only when their composition mimicked that of lipid rafts. Altogether, these data indicate that specific lipid packing can trigger contact-mediated secretion by S. flexneri., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2004

40. Phosphatidylinositol 3,4,5-trisphosphate: an early mediator of insulin-stimulated sodium transport in A6 cells.

Author

Markadieu, Nicolas, Blero, Daniel, Boom, Alain, Erneux, Christophe, Beauwens, Renaud, Markadieu, Nicolas, Blero, Daniel, Boom, Alain, Erneux, Christophe, and Beauwens, Renaud

Abstract

Insulin stimulates sodium transport across A6 epithelial cell monolayers. Activation of phosphatidylinositol 3-kinase (PI 3-kinase) was suggested as an early step in the insulin-stimulated sodium reabsorption (Ref. 35). To establish that the stimulation of the PI 3-kinase signaling cascade is causing stimulation of apical epithelial Na channel, we added permeant forms of phosphatidylinositol (PI) phosphate (P) derivatives complexed with a histone carrier to A6 epithelium. Only PIP(3) and PI(3,4)P(2) but not PI(4,5)P(2) stimulated sodium transport, although each of them penetrated into A6 cell monolayers as assessed using fluorescent permeant phosphoinositides derivatives. By Western blot analysis of A6 cell extracts, the inositol 3-phosphatase PTEN and the protein kinase B PKB were both detected. To further establish that the stimulation of sodium transport induced by insulin is related to PIP(3) levels, we transfected A6 cells with human PTEN cDNA and observed a 30% decrease in the natriferic effect of insulin. Similarly, the increase in sodium transport observed by addition of permeant PIP(3) was also reduced by 30% in PTEN-overexpressing cells. PKB, a main downstream effector of PI 3-kinase, was phosphorylated at both Thr 308 and Ser 473 residues upon insulin stimulation of the A6 cell monolayer. PKB phosphorylation in response to insulin stimulation was reduced in PTEN-overexpressing cells. Permeant PIP(3) also increased PKB phosphorylation. Taken together, the present results establish that the d-3-phosphorylated phosphoinositides PIP(3) and PI(3,4)P(2) mediate the effect of insulin on sodium transport across A6 cell monolayers., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2004

41. Identification of a functionally important conformation-sensitive region of the secretory Na+-K+-2Cl- cotransporter (NKCC1).

Author

Dehaye, Jean-Paul, Nagy, Akos, Premkumar, Anita, Turner, R. James, Dehaye, Jean-Paul, Nagy, Akos, Premkumar, Anita, and Turner, R. James

Abstract

The secretory Na(+)-K(+)-2Cl(-) cotransporter (NKCC1) is a member of a small gene family of electroneutral salt transporters that play essential roles in salt and water homeostasis in many mammalian tissues. We have identified a highly conserved residue (Ala-483) in the sixth membrane-spanning segment of rat NKCC1 that when mutated to cysteine renders the transporter sensitive to inhibition by the sulfhydryl reagents 2-aminoethyl methanethiosulfonate (MTSEA) and 2-(trimethylammonium)ethyl methanethiosulfonate (MTSET). The mutation of Ala-483 to cysteine (A483C) results in little or no change in the affinities of NKCC1 for substrate ions but produces a 6-fold increase in sensitivity to the inhibitor bumetanide, suggesting a specific modification of the bumetanide binding site. When residues surrounding Ala-483 were mutated to cysteine, only I484C was sensitive to inhibition by MTSEA and MTSET. Surprisingly I484C showed increased transport activity in the presence of low concentrations of mercury (1-10 microm), whereas A483C showed inhibition. The inhibition of A483C by MTSEA was unaffected by the presence or absence of sodium and potassium but required the presence of extracellular chloride. Taken together, our results indicate that Ala-483 lies at or near an important functional site of NKCC1 and that the exposure of this site to the extracellular medium is dependent on the conformation of the transporter. Specifically, our results indicate that the cysteine introduced at residue 483 is only available for interaction with MTSEA when chloride is bound to NKCC1 at the extracellular surface., Journal Article, info:eu-repo/semantics/published

Published

2003

42. Past-A, a novel proton-associated sugar transporter, regulates glucose homeostasis in the brain.

Author

Shimokawa, Noriaki, Okada, Junichi, Haglund, Kaisa, Dikic, Ivan, Koibuchi, Noriyuki, Miura, Mitsuhiko, Shimokawa, Noriaki, Okada, Junichi, Haglund, Kaisa, Dikic, Ivan, Koibuchi, Noriyuki, and Miura, Mitsuhiko

Abstract

The ventral medullary surface (VMS) of the medulla oblongata is known to be the site of the central chemosensitive neurons in mammals. These neurons sense excess H+/CO2 dissolved in the CSF and induce hyperventilation. To elucidate the mechanism of neuronal cell adaptation to changes of H+/CO2, we screened for hypercapnia-induced genes in the VMS. Here, we report cloning and characterization of a novel gene called proton-associated sugar transporter-A (Past-A), which is induced in the brain after hypercapnia and mediates glucose uptake along the pH gradient. Past-A comprises 751 amino acid residues containing 12 membrane-spanning helices, several conserved sugar transport motifs, three proline-rich regions, and leucine repeats. Past-A transcript was expressed predominantly in the brain. Moreover, the Past-A-immunoreactive neural cells were found in the VMS of the medulla oblongata, and the number of immunoreactive cells was increased by hypercapnic stimulation. Transient transfection of Past-A in COS-7 cells leads to the expression of a membrane-associated 82 kDa protein that possesses a glucose transport activity. The acidification of extracellular medium facilitated glucose uptake, whereas the addition of carbonyl cyanide m-chlorophenylhydrazone, a protonophore, inhibited glucose import. Together, our results indicate that Past-A is a brain-specific glucose transporter that may represent an adaptation mechanism regulating sugar homeostasis in neuronal cells after hypercapnia.

Published

2002

43. Structural changes in the angiofollicular units between active and hypofunctioning follicles align with differences in the epithelial expression of newly discovered proteins involved in iodine transport and organification.

Author

Gérard, A-C, Many, Marie-Christine, Daumerie, Chantal, Costagliola, Sabine, Miot, Françoise, DeVijlder, J J M, Colin, Ides M, Denef, Jean François, Gérard, A-C, Many, Marie-Christine, Daumerie, Chantal, Costagliola, Sabine, Miot, Françoise, DeVijlder, J J M, Colin, Ides M, and Denef, Jean François

Abstract

In animals, as well as in humans, the thyroid gland is made of active follicles, with cuboidal cells and hypofunctioning follicles, with flattened cells. In this study, the functional status of human follicles was dissected out, based on immunohistochemical detection of TSH receptor, Na(+)/I(-) symporter, pendrin, thyroperoxidase (TPO), thyroid oxidases (ThOXs), and T(4)-containing iodinated Tg (Tg-I). To ascertain that angiofollicular units exist in the human, we studied the microvascular bed of each follicle, in correlation with detection of vascular endothelial growth factor (VEGF), of nitric oxide synthase III, and of endothelin in normal and goitrous thyroids. In hypofunctioning follicles, pendrin, TPO, and ThOXs were not detected, and there was no Tg-I in the colloid. At the opposite, in active follicles, pendrin, TPO, and ThOXs were detected in thyrocytes, and Tg-I was present in the colloid. In normal and goitrous thyroids, the capillary networks surrounding active follicles were larger than those surrounding hypofunctioning follicles. Immunoreactivity for nitric oxide synthase III and endothelin was solely detected in active follicles. Only a few follicles in normal thyroids were immunostained for VEGF, regardless of their functional status. In multinodular goiters, VEGF was detected in contact with the extracellular matrix at the basal pole of the cells. In conclusion, the present study endorses the likelihood of angiofollicular units in the human thyroids. Vascular changes are related to the functional status of thyrocytes., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2002

44. Transport mechanism underlying the formation of microenvironment in rat efferent duct and epididymis.

Author

Leung, Pak Heng., Chinese University of Hong Kong Graduate School. Division of Physiology., Leung, Pak Heng., and Chinese University of Hong Kong Graduate School. Division of Physiology.

Abstract

Leung Pak Heng., Thesis (Ph.D.)--Chinese University of Hong Kong, 2001., Includes bibliographical references (p. 163-189)., Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web., Mode of access: World Wide Web., s in English and Chinese., http://library.cuhk.edu.hk/record=b6073356, Use of this resource is governed by the terms and conditions of the Creative Commons “Attribution-NonCommercial-NoDerivatives 4.0 International” License (http://creativecommons.org/licenses/by-nc-nd/4.0/)

Published

2001

45. The complex relationships between cystic fibrosis and congenital bilateral absence of the vas deferens: clinical, electrophysiological and genetic data

Author

Dohle, G.R. (Gert), Veeze, H.J., Overbeek, S.E. (Shelley), Ouweland, A.M.W. (Ans) van den, Halley, D.J.J. (Dicky), Weber, R.F.A. (Robert), Niermeijer, M.F. (Martinus), Dohle, G.R. (Gert), Veeze, H.J., Overbeek, S.E. (Shelley), Ouweland, A.M.W. (Ans) van den, Halley, D.J.J. (Dicky), Weber, R.F.A. (Robert), and Niermeijer, M.F. (Martinus)

Abstract

Congenital bilateral absence of the vas deferens (CBAVD) is found in 1-2% of infertile males and in most male cystic fibrosis (CF) patients. CF and some of the CBAVD cases were found to share the same genetic background. In this study, 21 males with CBAVD had extensive physical and laboratory testing for symptoms of CF. Possible defective cellular chloride transport was measured by interstitial current measurement of rectal suction biopsies. Cystic fibrosis transmembrane conductance regulator (CFTR) gene mutation analysis was performed for 10 common CFTR mutations. CF-related symptoms were found in six men. On laboratory testing slightly abnormal liver and pancreatic function was found in seven patients. The sweat test was found to be abnormal in four patients; interstitial current measurement showed defective chloride excretion in 11 patients. CFTR gene mutations were found in 66% of the patients: eight were compound heterozygotes; in six, only one common mutation could be detected. The 5T allele in one copy of intron 8 was found in four men. CBAVD appears to be a heterogeneous clinical and genetic condition. A CFTR gene mutation was found in both copies of the allele or interstitial current measurement showed defective chloride excretion in 14/21 cases. Genetic counselling is clearly indicated for couples seeking pregnancy through epididymal or testicular sperm aspiration and intracytoplasmic sperm injection.

Published

1999

46. Glutamate transporter GLT-1 is transiently localized on growing axons of the mouse spinal cord before establishing astrocytic expression.

Author

Yamada, K., Watanabe, M., Shibata, T., Nagashima, M., Tanaka, K., Inoue, Y., Yamada, K., Watanabe, M., Shibata, T., Nagashima, M., Tanaka, K., and Inoue, Y.

Abstract

The glutamate transporter GLT-1 is expressed in astrocytes of the mature brain and spinal cord. In the present study, we examined its expression in the developing mouse spinal cord. By in situ hybridization, 35S-labeled antisense oligonucleotide probes for GLT-1 mRNA consistently labeled the mantle zone/gray matter from embryonic day 11 through the adult stage. However, immunohistochemistry with a specific antibody visualized distinct regional and cellular localizations during the time between the fetal and postnatal stages. At fetal stages, GLT-1 immunoreactivity predominated in the marginal zone/white matter, observed as tiny puncta in cross-sections and as thin fibers in longitudinal sections. The GLT-1-immunopositive structures were also labeled for neuron-specific enolase, a glycolytic enzyme specific to postmitotic neurons and endocrine cells. By electron microscopy, GLT-1 immunoreactivity was detected in axons forming frequent enlargements and was focally localized on a small portion of the axolemma, particularly that facing adjacent axons. At early postnatal stages, GLT-1 disappeared from axons in white matter tracts and, instead, appeared in astrocytic processes surrounding various neuronal elements in the gray matter. Therefore, before switching to astrocytic expression, GLT-1 is transiently expressed in neurons and localized in differentiating axons. Together with our previous finding on the localization of glutamate transporter GLAST in radial glial fibers, GLT-1 and GLAST are thus localized during development on distinct directional cellular elements along which young neurons elongate their axons or move their cell bodies, respectively.

Published

1998

47. Intercellular heterogeneity of early mitogenic events: cAMP generalizes the EGF effect on c-Fos protein appearance but not on MAP kinase phosphorylation and nuclear translocation in dog thyroid epithelial cells.

Author

Baptist, Mireille, Dumont, Jacques Emile, Roger, Pierre P., Baptist, Mireille, Dumont, Jacques Emile, and Roger, Pierre P.

Abstract

When quiescent dog thyroid epithelial cells in primary culture are stimulated for 48 h with thyrotropin (TSH), forskolin acting through cAMP, or with cAMP-independent mitogens including epidermal growth factor (EGF), hepatocyte growth factor (HGF), and a tumor promoting phorbol ester (TPA), only 30-60% of cells progress through the cell cycle. A more general growth response requires the combination of EGF and TSH or forskolin. In this study we ask whether this intercellular heterogeneity in mitogen sensitivity could depend on a similar heterogeneity at early stages of the mitogenic stimulation process, i.e. at the levels of p42/p44 MAP kinase nuclear translocation and c-Fos protein appearance. We used indirect immunofluorescence microscopy with photometric quantitation and corroborated data using Western blotting. We analyzed the double staining of c-Fos and p42/p44 MAP kinases, since the nuclear translocation of these MAP kinases has been suggested as a key step for the stimulation of c-fos transcription. (i) EGF and HGF induced c-Fos accumulation and MAP kinase translocation in variable fractions of the cell population that corresponded to their relative potency as mitogens. c-Fos appearance and MAP kinase translocation poorly correlated in individual cells. Many cells accumulated c-Fos without any detectable p42/p44 MAP kinase translocation. The heterogeneity of proliferative responses to EGF could be due to the lack of c-Fos or MAP kinase responsiveness of many cells. (ii) TPA induced c-Fos accumulation and MAP kinase translocation within the whole cell population, which did not explain the heterogeneity of the growth response to this factor and showed that these events are not sufficient to elicit DNA synthesis, (iii) TSH and forskolin induced a weak c-Fos accumulation in only a minority of cells but, as previously shown, no p42/p44 MAP kinase phosphorylation and translocation. An important c-Fos expression was thus dispensable for the strong DNA synthesis stim, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1995

48. Effect of glucose and K+ depolarization on cytosolic free Ca2+ in cultured neonatal islets.

Author

Boschero, Antonio Carlos, Bordin, Silvana Auxiliadora, Plasman, Pierre-Olivier, Herchuelz, André, Boschero, Antonio Carlos, Bordin, Silvana Auxiliadora, Plasman, Pierre-Olivier, and Herchuelz, André

Abstract

In cultured neonatal islet cells, glucose (16.7 mM) and K+ (50 mM) increased cytosolic free Ca2+ ([Ca2+]i). The increments in [Ca2+]i induced by either glucose or K+ were similar to those obtained in cultured adult islet cells but only half of that recorded in freshly isolated adult islet cells. These data indicate that, in neonatal islet cells, the reduced insulin release in response to glucose is associated with a diminished increase in [Ca2+]i. This reduced insulin response may not solely be due to an impaired regulation of the ATP-sensitive K+ channels as previously suggested. It may also result from some alteration in the process of Ca2+ inflow through voltage-sensitive Ca2+ channels., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1992

49. Golgi Bypass: Skirting Around the Heart of Classical Secretion

Author

Adam G. Grieve, Catherine Rabouille, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

Endosome, Endoplasmic reticulum, Cell Membrane, Golgi Apparatus, Proteins, Biological Transport, COPI, Biology, Golgi apparatus, General Biochemistry, Genetics and Molecular Biology, Transmembrane protein, Cell biology, Cell membrane, symbols.namesake, medicine.anatomical_structure, Gene Expression Regulation, medicine, symbols, Secretion, Secretory pathway, Perspectives

Abstract

Classical secretion consists of the delivery of transmembrane and soluble proteins to the plasma membrane and the extracellular medium, respectively, and is mediated by the organelles of the secretory pathway, the Endoplasmic Reticulum (ER), the ER exit sites, and the Golgi, as described by the Nobel Prize winner George Palade (Palade 1975). At the center of this transport route, the Golgi stack has a major role in modifying, processing, sorting, and dispatching newly synthesized proteins to their final destinations. More recently, however, it has become clear that an increasing number of transmembrane proteins reach the plasma membrane unconventionally, either by exiting the ER in non-COPII vesicles or by bypassing the Golgi. Here, we discuss the evidence for Golgi bypass and the possible physiological benefits of it. Intriguingly, at least during Drosophila development, Golgi bypass seems to be mediated by a Golgi protein, dGRASP, which is found ectopically localized to the plasma membrane. [KEYWORDS: Biological Transport/physiology, Cell Membrane, Gene Expression Regulation, Golgi Apparatus/ physiology, Proteins/ metabolism]

Published

2011