Your search keyword '"Ohnishi S"' showing total 22 results

1. In vitro effects of aged garlic extract and other nutritional supplements on sickle erythrocytes.

Author

Ohnishi ST and Ohnishi T

Subjects

Anemia, Sickle Cell blood, Antioxidants pharmacology, Antioxidants therapeutic use, Cell Count, Cells, Cultured, Cysteine therapeutic use, Erythrocyte Membrane metabolism, Garlic chemistry, Humans, Plant Extracts pharmacology, Plant Extracts therapeutic use, Reactive Oxygen Species metabolism, Anemia, Sickle Cell drug therapy, Cysteine analogs & derivatives, Cysteine pharmacology, Dietary Supplements, Erythrocyte Membrane drug effects, Garlic therapeutic use, Phytotherapy, Plants, Medicinal

Abstract

In the circulation of sickle cell anemia patients, a certain population of erythrocytes has an elevated density. These abnormally dense cells are believed to be at the root of the painful crisis and anemia of the patients. We have developed an in vitro method for the preparation of these heavier erythrocytes by a repeated deoxy-oxy cycling of erythrocytes from sickle cell anemia patients. By using this method, we studied whether certain nutritional supplements would inhibit the formation of dense cells in vitro. It was found that aged garlic extract (AGE) as well as its components with antioxidant activity, i.e., S-allylcysteine and N alpha-(1-deoxy-D-fructos-1-yl)-L-arginine (fructosyl arginine), inhibited the formation of dense cells in vitro. Vitamin C, vitamin E and the spin-trapping agents, 5-diethoxyphophoryl-5-methyl-1-pyrroline-N-oxide and alpha-(4-pyridyl-1-oxide)-N-t-butylnitrone were all found to inhibit the formation of dense cells in vitro. These results suggest that, when extremely stretched sickle-shaped cells are formed by the repeated deoxy-oxy cycling, the erythrocyte membrane becomes susceptible to oxidative injury by reactive oxygen species. The protection of the erythrocyte membrane from such an oxidative injury would prevent the membranes from becoming leaky to the calcium ion, thus inhibiting the activation of the calcium-activated potassium efflux channel and the formation of dense cells. We also developed a new ex vivo method of studying the possible efficacy of antioxidants taken orally on the dense cell formation in sickle cell patients. It involved the use of blood plasma taken from a healthy donor (with normal hemoglobin) of AB blood type who had consumed different types of antioxidants orally. By suspending sickle erythrocytes in such plasma and exposing them to the deoxy-oxy cycling, the degree of dense cell formation was determined. The degree of inhibition in vitro by antioxidants taken orally may be related to their efficacy in inhibiting dense cell formation in the patients. On the basis of these in vivo and ex vivo studies, we propose that a cocktail of antioxidants would have beneficial effects in lessening the incidence and severity of crisis and reducing anemia in sickle cell disease.

Published

2001

2. Electron spin resonance methods for studying virus-cell membrane fusion.

Author

Ohnishi S and Kuroda K

Subjects

Animals, Cyclic N-Oxides, Electron Spin Resonance Spectroscopy methods, Hemolysis, Humans, Kinetics, Mathematics, Models, Biological, Phosphatidylcholines, Spin Labels, Cell Membrane physiology, Erythrocyte Membrane physiology, Erythrocytes physiology, Gene Products, env metabolism, Membrane Fusion, Parainfluenza Virus 1, Human physiology

Published

1993

3. Development of a streak-camera-based time-resolved microscope fluorimeter and its application to studies of membrane fusion in single cells.

Author

Kusumi A, Tsuji A, Murata M, Sako Y, Yoshizawa AC, Kagiwada S, Hayakawa T, and Ohnishi S

Subjects

Animals, Cell Line, Erythrocyte Membrane ultrastructure, Fluorescent Dyes, Humans, Liposomes, Mice, Microscopy, Fluorescence methods, Naphthalenesulfonates, Organelles ultrastructure, Serum Albumin, Bovine chemistry, Anion Exchange Protein 1, Erythrocyte analysis, Erythrocyte Membrane physiology, Membrane Fusion, Microscopy, Fluorescence instrumentation, Organelles physiology

Abstract

A time-resolved microscope fluorimeter based on a synchroscan streak camera and a fast pulsed laser system has been developed to measure the fluorescence lifetime decay under the fluorescence microscope. This system allows one to measure the nanosecond fluorescence lifetimes of fluorophores in a small spot (0.8-6.3 microns diameter) in single cultured cells under a fluorescence microscope, while the cells are being viewed under a high-power objective lens. A signal acquisition time between a second and a minute was usually sufficient to obtain fluorescence decay curves with good quality for 10(3)-10(5) fluorophores localized in 1 microns 2 domain. A signal-to-noise ratio better than 30 was obtained for approximately 30,000 fluorescein-labeled band 3 molecules in a 2 microns 2 region in a single human erythrocyte ghost after signal accumulation for 30 s. The measured lifetimes for a variety of fluorescent probes attached to proteins in solution and lipids in liposomes showed a good agreement with those measured in a cuvette under standard conditions by time-correlated single photon counting. With the development of this instrument, microscope fluorimetry has become a practical, straightforward, quantitative technique for investigation of molecular processes in single cells in culture. Time-resolved microscope fluorimetry has been applied to observe fusion of liposomes in vitro and that of endosomes in single cells by monitoring resonance energy transfer. Inspection of individual liposomes and endosomes revealed the extent of fusion for each vesicle. Since the use of time-resolved microscope fluorimetry eliminates the need for subcellular fractionation or the complex correction procedures in steady-state microfluorimetry, it greatly simplifies the assay for endosome fusion in vivo. The results showed that extensive fusion of sequentially formed endosomes takes place all over the cell matrix in cultured cells. This suggests that extensive fusion with incoming endosomes takes place in many endosomal compartments, possibly sorting organelles, or that the early endosomes fuse with the preexisting network of tubular cisternae of the endosomal compartment at many points in the network. It is concluded that time-resolved microscope fluorimetry is a powerful noninvasive technique for studies of in situ biochemistry and biophysics using cells and tissues.

Published

1991

4. Interaction of influenza virus hemagglutinin with target membrane lipids is a key step in virus-induced hemolysis and fusion at pH 5.2.

Author

Maeda T, Kawasaki K, and Ohnishi S

Subjects

Humans, Hydrogen-Ion Concentration, Liposomes, Membrane Fusion, Membrane Lipids metabolism, Phospholipids metabolism, Spin Labels, Structure-Activity Relationship, Cell Fusion drug effects, Erythrocyte Membrane physiology, Erythrocytes physiology, Hemagglutinins, Viral pharmacology, Hemolysis drug effects, Influenza A virus

Abstract

The molecular mechanism of hemolysis and fusion by influenza virus in acidic media was studied. First, the effect of trypsin treatment on the activity of fibroblast-grown influenza virus was studied. The results showed that the split form of viral hemagglutinin, HA1 and HA2, but not the precursor, is responsible for the activity. Second, the interaction of egg-grown influenza virus, which contains the split hemagglutinin, with lipid liposomes was studied by spin labeling and electron microscopy. Phospholipid transfer from the viral envelope to the lipid bilayer membrane occurred within 30 s at pH 4.5-5.4. The transfer is largely independent of the lipid composition and the crystalline vs. liquid/crystalline state of the membrane. Virus-induced lysis of liposomes also took place rapidly in the same pH range. Envelope fusion with liposomes occurred at pH 5.2 but not at pH 7.0. These characteristic interactions were similar to those between influenza virus and erythrocytes reported previously. On the other hand, hemagglutinating virus of Japan did not interact with liposomes at neutral pH. These results suggest that protonation of the NH2-terminal segment of the HA2 form causes interaction of the segment with the lipid core of the target cell membrane, leading to hemolysis and fusion.

Published

1981

5. Antisickling effects of membrane-interacting compounds.

Author

Ohnishi ST

Subjects

Anemia, Sickle Cell blood, Calmodulin metabolism, Chlorpromazine pharmacology, Humans, Sulfonamides pharmacology, Vasodilator Agents pharmacology, Antipsychotic Agents pharmacology, Antisickling Agents pharmacology, Erythrocyte Membrane drug effects, Erythrocytes drug effects, Erythrocytes, Abnormal drug effects

Abstract

Several anti-psychotic drugs were found to have an in vitro antisickling effect. A linear relationship was found between the antisickling activity and the inhibition of calmodulin stimulated phosphodiesterase activity. These membrane-interacting compounds produce a "cup-shaped" red blood cell at the concentration where they demonstrate an antisickling effect. The volume of a "cup-shaped" red cell (with chlorpromazine) does not change significantly from that of an untreated control red cell. The anti-sickling mechanism of these membrane-interacting compounds is not known at this point.

Published

1982

6. Rotational mobility of an erythrocyte membrane integral protein band 3 in dimyristoylphosphatidylcholine reconstituted vesicles and effect of binding of cytoskeletal peripheral proteins.

Author

Sakaki T, Tsuji A, Chang CH, and Ohnishi S

Subjects

Anion Exchange Protein 1, Erythrocyte, Dimyristoylphosphatidylcholine, Electron Spin Resonance Spectroscopy, Humans, In Vitro Techniques, Liposomes, Phosphatidylcholines, Spin Labels, Blood Proteins metabolism, Cytoskeletal Proteins, Erythrocyte Membrane metabolism, Erythrocytes metabolism, Membrane Proteins, Neuropeptides

Abstract

Band 3 protein was isolated from human erythrocyte membranes, purified, and reconstituted into a well-defined phospholipid bilayer matrix (dimyristoylphosphatidylcholine). The preparation yielded uniform single-bilayered vesicles of the diameter 40--80 nm. The rotational motion of band 3 was studied by saturation transfer electron spin resonance (ESR) spectroscopy of covalently attached maleimide spin-labels. The rotational mobility changed in response to the host lipid phase transition. The rotational correlation time was in a range from 73 (37 degrees C) to 94 microseconds (26 degrees C) in the fluid phase and from 240 (15 degrees C) to 420 microseconds (5 degrees C) in the solid phase. The motion was analyzed based on the anisotropic rotation of band 3 in the reconstituted vesicles. To obtain information on the rotational diffusion constant around the axis parallel to the membrane normal, we made an attempt to measure the angle between the spin-label magnetic axis and the membrane normal. The result gave 3.9 x 10(4) s-1 at 37 degrees C as a rough estimate for the diffusion constant. This is compatible to anisotropic rotation of a cylinder of radius 3.3 nm in a two-dimensional matrix with inner viscosity 2 P and inner thickness 4 nm. The cytoskeletal peripheral proteins caused a definite increase in the rotational correlation time (from 73 to 180 microseconds at 37 degrees C, for example). The restriction of the rotational mobility was shown to be due to the ankyrin-linked interaction between band 3 and spectrin-actin-band 4.1 proteins in the reconstituted membranes.

Published

1982

7. Enhancement of phospholipid transfer from Sendai virus to erythrocytes is mediated by target cell membrane.

Author

Kuroda K, Maeda T, and Ohnishi S

Subjects

Humans, Parainfluenza Virus 1, Human ultrastructure, Spin Labels, Temperature, Time Factors, Erythrocyte Membrane physiology, Erythrocytes physiology, Membrane Lipids metabolism, Parainfluenza Virus 1, Human physiology, Phospholipids metabolism

Abstract

Transfer of phospholipid from the envelope of Sendai virus to erythrocyte membrane was measured by using spin-labeled phosphatidylcholine. The transfer was enhanced autocatalytically above a threshold dose (about five adsorbed viruses per cell). There was an inflection point in the time course of transfer, after which the transfer was greatly accelerated. The time to reach the inflection point became shorter with increased viral dose. The transfer reaction was markedly enhanced above 19 degrees C and the inflection point was observed above this temperature. There was negligible transfer from trypsin-treated virus to erythrocyte membrane, but the transfer was greatly enhanced by intact virus. The enhancement was larger with increased amount of intact virus, and the inflection point was observed in the transfer curves. All the kinetic data can be satisfactorily analyzed by a model which assumes that the virus modifies the cell membrane at the attachment site, the modification is propagated in the membrane, and transfer of phospholipid to the modified sites is greatly enhanced. The propagation rate is estimated as approximately equal to 10(-11) cm2s-1 and the activation energy as 13 kcal mol-1 (54 kJ mol-1). The viral F glycoproteins are suggested as a possible entity for the modification and its propagation: they are introduced into the target cell membrane by envelope fusion, diffuse laterally, and enhance both phospholipid exchange and envelope fusion with viruses attached to the membrane sites.

Published

1980

8. Halothane induced disorder of red cell membranes of subjects susceptible to malignant hyperthermia.

Author

Ohnishi ST and Ohnishi T

Subjects

Animals, Electron Spin Resonance Spectroscopy, Humans, Malignant Hyperthermia genetics, Membrane Fluidity drug effects, Spin Labels, Swine, Erythrocyte Membrane drug effects, Halothane toxicity, Malignant Hyperthermia blood

Abstract

Membrane fluidity of red blood cells drawn from malignant hyperthermic pigs and humans was studied using spin-probes and electron paramagnetic resonance technique. The order parameter and rotational correlation time were determined with 12-doxylstearate and 16-doxylstearate, respectively. It was found that halothane decreased both parameters, but that the decrease of these parameters in subjects susceptible to malignant hyperthermia was much greater than that in normal subjects. The differences were most pronounced at 3 mM halothane. A possibility of using blood for a non-invasive screening for malignant hyperthermia is discussed.

Published

1988

9. Activation of influenza virus by acidic media causes hemolysis and fusion of erythrocytes.

Author

Maeda T and Ohnishi S

Subjects

Hemagglutinins, Viral pharmacology, Hydrogen-Ion Concentration, Phospholipids, Sonication, Viral Proteins pharmacology, Cell Fusion, Erythrocyte Membrane drug effects, Erythrocytes drug effects, Hemolysis, Influenza A virus

Published

1980

10. Regulation of band 3 mobilities in erythrocyte ghost membranes by protein association and cytoskeletal meshwork.

Author

Tsuji A, Kawasaki K, Ohnishi S, Merkle H, and Kusumi A

Subjects

Affinity Labels, Diffusion, Electrophoresis, Polyacrylamide Gel, Eosine Yellowish-(YS) analogs & derivatives, Humans, Macromolecular Substances, Mathematics, Photometry, Putrescine pharmacology, Sodium Chloride pharmacology, Spermidine pharmacology, Spermine pharmacology, Anion Exchange Protein 1, Erythrocyte metabolism, Cytoskeleton metabolism, Erythrocyte Membrane metabolism, Membrane Proteins blood

Abstract

Rotational diffusion of erythrocyte anion channel protein band 3 was measured in ghost membranes by observing time-resolved phosphorescence anisotropy decays of eosinyl-5-maleimide covalently attached to the protein. Experiments were carried out under conditions similar to those employed by Tsuji and Ohnishi (1986) for translational diffusion measurement of band 3 [(1986) Biochemistry 25, 6133-6139] to allow direct comparison of rotational and translational diffusion of band 3. Detailed analysis of diffusive properties of band 3 in ghost membranes was made on the basis of these rotational and translational diffusion data. Rotational diffusion measurements indicated that there are at least three populations of band 3 molecules with high, low, and no rotational mobilities in the time scale of 10(-4)-10(-2) s. These populations are in equilibrium, and the fractional ratios are strongly temperature dependent. At 26 degrees C, 44% of band 3 molecules are mobile (16% have an average rotational correlation time of 0.19 ms, and 28% have an average correlation time of 2.4 ms), and 56% are immobile. These results correlate well with translational diffusion data which indicated 40% mobile and 60% immobile fractions of band 3. The rotational diffusion data together with the translational diffusion data by Tsuji and Ohnishi (1986) and Golan and Veatch [(1980) Proc. Natl. Acad. Sci. U.S.A. 77, 2537-2541] suggest that immobilization of band 3 is largely caused by binding of band 3 oligomers to ankyrin, which abolishes both rotational and translational diffusion of band 3.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1988

11. Lateral mobility of erythrocyte membrane proteins studied by the fluorescence photobleaching recovery technique.

Author

Chang CH, Takeuchi H, Ito T, Machida K, and Ohnishi S

Subjects

Anion Exchange Protein 1, Erythrocyte, Ankyrins, Blood Proteins, Diffusion, Dimyristoylphosphatidylcholine, Fluorescence, Humans, Lipid Bilayers metabolism, Phosphatidylcholines, Phospholipids blood, Spectrin blood, Viscosity, Cytoskeletal Proteins, Erythrocyte Membrane metabolism, Erythrocytes metabolism, Membrane Proteins blood, Neuropeptides

Abstract

Erythrocyte membrane peripheral and integral proteins have been isolated and purified, and the lateral diffusion of these proteins in a well-defined phospholipid bilayer matrix (dimyristoylphosphatidylcholine) has been studied by fluorescence photobleaching recovery measurements. Our own instrument for the recovery measurements is described and some data for lipid diffusions are compared with those previously reported by other investigators. The peripheral proteins (spectrin and band 4.1) diffuse rapidly on the lipid membrane in its fluid phase. The diffusion constant of approximately 5 x 10(-8) cm2 . s-1 (30 degrees C) was only a little smaller than that for lipid diffusion. The diffusion was greatly slowed down when the host lipid matrix became solid. The integral protein band 3 also diffuses rapidly in the fluid membrane. The diffusion constant of 1.6 x 10(-8) cm2 . s-1 (30 degrees C) was smaller than those for lipids and for the peripheral proteins. The lateral motion is compatible with diffusion of a cylinder with radius 3 nm in a two dimensional matrix with an inner viscosity of 2 poises and an inner thickness of 4 nm. The band 3 lateral motion was restricted by binding of the cytoskeletal component proteins (ankyrin, spectrin, actin, and band 4.1) to the reconstituted membranes. The diffusion constant decreased to half. The results provide a basis for the elucidation of transmembrane control mechanisms in more complex cellular systems.

Published

1981

12. Interaction of hemagglutinating virus of Japan with erythrocytes as studied by release of a spin probe from virus.

Author

Maeda T, Kuroda K, Toyama S, and Ohnishi S

Subjects

Choline metabolism, Electron Spin Resonance Spectroscopy, Hot Temperature, Humans, In Vitro Techniques, Choline analogs & derivatives, Cyclic N-Oxides, Erythrocyte Membrane microbiology, Erythrocytes microbiology, Parainfluenza Virus 1, Human metabolism, Piperidines metabolism, Spin Labels

Published

1981

13. Mobilization and aggregation of integral membrane proteins in erythrocytes induced by interaction with influenza virus at acidic pH.

Author

Yoshimura A, Yamashina S, and Ohnishi S

Subjects

Cell Fusion, Erythrocyte Membrane analysis, Erythrocytes microbiology, Hemagglutinin Glycoproteins, Influenza Virus, Hemagglutinins, Viral analysis, Hemolysis, Humans, Hydrogen-Ion Concentration, Microscopy, Electron, Spectrin analysis, Temperature, Blood Proteins metabolism, Erythrocyte Membrane microbiology, Hemagglutinins, Viral physiology, Influenza A virus physiology, Membrane Proteins metabolism, Parainfluenza Virus 1, Human physiology

Abstract

Effect of influenza virus on erythrocyte membranes was investigated by electron microscopy and fluorescence photobleaching recovery measurements. The virus induced mobilization of integral proteins in erythrocyte membrane at acidic pH, where it fused with the cell membrane to cause hemolysis and also cell fusions but not at neutral pH. At lower temperatures (e.g., 4 degrees C), the proteins aggregated in the membrane and, consequently, large protein-free lipid bilayer area was produced. At higher temperatures (e.g., 37 degrees C) the protein distribution became randomized. Spectrin meshwork underneath the erythrocyte membrane was also markedly modified by the virus at acidic pH. Diffuse fibril structure was converted into dense spots and the membrane area lacking the fibril structure was produced. Isolated hemagglutinin rosettes also caused mobilization and aggregation of the integral proteins at acidic pH but to smaller extent than that induced by virus. The membrane perturbation detected as the protein mobilization by the action of hemagglutinin was assigned to be the cause for envelope fusion.

Published

1985

14. Kinetic analysis of fusion of hemagglutinating virus of Japan with erythrocyte membrane using spin-labeled phosphatidylcholine.

Author

Kuroda K, Kawasaki K, and Ohnishi S

Subjects

Electron Spin Resonance Spectroscopy, Humans, Kinetics, Mathematics, Phosphatidylcholines, Spin Labels, Erythrocyte Membrane microbiology, Receptors, Virus metabolism, Respirovirus metabolism

Abstract

HVJ* (hemagglutinating virus of Japan containing spin-labeled phosphatidylcholine in its envelope around 10 mol %) was adsorbed onto erythrocytes or erythrocyte ghosts at various doses, and the ESR spectrum of the virus-cell system was measured at 37 degrees C. The peak-height increase for the HVJ*-ghost system was satisfactorily analyzed on the basis of envelope fusion by a first-order kinetic equation with two different rate constants. The rate constant was obtained as k1 = 0.84 min-1 and k2 = 0.011 min-1, independent of the virus dose. The fraction of virus fused at the rate constant k1 decreased with the dose. However, the average number of fast-fusing viruses per cell was nearly independent of the dose, and the value was one to two. The peak-height increase in the HVJ*-erythrocyte system was caused by both envelope fusion and phospholipid exchange catalyzed by the virus-induced hemolyzate. At lower doses, where the virus-induced hemolysis was small and, therefore, the rate of phospholipid exchange was small, the peak-height increase could be analyzed by the same kinetic equation with nearly the same rate constant value for k1 as that for HVJ*-ghosts. However, the k2 was larger than that for HVJ*-ghost, owing to the additional transfer by phospholipid exchange.

Published

1985

15. Interaction of a peripheral protein of the erythrocyte membrane, band 4.1, with phosphatidylserine-containing liposomes and erythrocyte inside-out vesicles.

Author

Sato SB and Ohnishi S

Subjects

Carboxy-Lyases metabolism, Cyclic N-Oxides metabolism, Electron Spin Resonance Spectroscopy, Humans, Phospholipids metabolism, Spectrometry, Fluorescence, Spin Labels, Blood Proteins metabolism, Cytoskeletal Proteins, Erythrocyte Membrane metabolism, Erythrocytes metabolism, Liposomes metabolism, Membrane Proteins, Neuropeptides, Phosphatidylserines metabolism

Abstract

Interactions of band 4.1 with mixed phospholipid membranes [phosphatidylserine (PtdSer), phosphatidylethanolamine, phosphatidylcholine, etc.] and erythrocyte inside-out vesicles were studied. Band 4.1 showed a higher affinity to PtdSer-containing membranes. The amount of binding to PtdSer-containing liposomes was larger than that to PtdSer-lacking liposomes. The amount of binding to inside-out vesicles did not change significantly on a protease treatment of the vesicles. The amount of band 4.1 bound on inside-out vesicles decreased on PtdSer-decarboxylase treatment of the vesicles. Ca2+ acted inhibitory to the binding of band 4.1. Band 4.1 together with PtdSer-containing vesicles but not with PtdSer-lacking vesicles induced gelation of spectrin-actin copolymer solution. Ca2+ inhibited the gelation. Fluorescence energy transfer from PtdSer-containing vesicles to band 4.1 was larger than that from PtdSer-lacking vesicles. Band 4.1 caused a marked release of tempocholine from preloaded PtdSer-containing liposomes but not from PtdSer-lacking liposomes. The release was larger from liposomes containing more PtdSer. Ca2+ was inhibitory to the tempocholine release. We suggest from these results that band 4.1 provides another anchoring site for the cytoskeletal spectrin-actin network to PtdSer domains in the inner layer of erythrocyte membrane. This anchoring may be involved in functional regulation since the interaction causes the membrane permeability change that is dependent on Ca2+.

Published

1983

16. Erythrocyte membrane fluidity change induced by intracellular delivery of Ca2+.

Author

Yamada S and Ohnishi S

Subjects

Animals, Phospholipids pharmacology, Ranula, Sheep, Viscosity, Calcium metabolism, Erythrocyte Membrane physiology, Membrane Fluidity drug effects

Published

1983

17. Transmembrane phospholipid motions induced by F glycoprotein in hemagglutinating virus of Japan.

Author

Maeda T, Asano A, Okada Y, and Ohnishi SI

Subjects

Animals, Cell Fusion, Chickens, Erythrocyte Membrane drug effects, Hemolysis, Humans, Parainfluenza Virus 1, Human drug effects, Trypsin pharmacology, Erythrocyte Membrane metabolism, Erythrocytes metabolism, Glycoproteins pharmacology, Parainfluenza Virus 1, Human metabolism, Phosphatidylcholines metabolism, Viral Proteins pharmacology

Abstract

Transfer of phospholipid from the envelope of hemagglutinating virus of Japan (HVJ) to erythrocyte (RBC) membrane and the virus-induced transfer of phospholipid between RBC membranes were studied using spin-labeled phosphatidylcholine (PC). The transfer of PC from membranes labeled densely with PC to unlabeled membranes was followed by the peak height increase in the electron spin resonance spectrum. The two kinds of transfer reactions took place very rapidly as reported previously. To obtain further details, the transfer reactions were studied with HVJ, HVJ inactivated by trypsin, HVJ harvested early, HVJ grown in fibroblast cells, the fibroblast HVJ activated by trypsin, influenza virus, and glutaraldehyde-treated RBCs. The results demonstrated that the viral F glycoprotein played a crucial role in the transmembrane phospholipid movements as well as in the fusion and hemolysis of RBCs. The transfer from HVJ to RBC's occurred partially through an exchange mechanism not accompanying the envelope fusion. This was shown by a decrease in the exchange broadening of the electron spin resonance spectrum of released spin-labeled HVJ (HVJ) and also by an increase in the ratio of PC to viral proteins incorporated into RBC membranes. HVJ modified RBC membrane so as to be able to exchange its phospholipids with those of inactive membranes such as fibroblast HVJ, influenza virus, glutaraldehyde-treated RBC'S, and phosphatidylcholine vesicles. HVJ affected the fluidity of RBC membranes markedly, the environments around PC being much fluidized. The virus-induced fusion was discussed based on close apposition of the membranes by HANA proteins and on the destabilization and fluidization of RBC membranes by F glycoproteins.

Published

1977

18. Spin-label studies of the oligomeric structure of band 3 protein in erythrocyte membranes and in reconstituted systems.

Author

Bittman R, Sakaki T, Tsuji A, Devaux PF, and Ohnishi S

Subjects

Actins, Electron Spin Resonance Spectroscopy, Humans, Membrane Fluidity, Membrane Lipids, Protein Binding, Spectrin, Temperature, Anion Exchange Protein 1, Erythrocyte, Erythrocyte Membrane ultrastructure

Abstract

A spin-labeled fatty acid (16-doxylstearic acid), linked by an ester bond to a maleimide or a nitrene residue, was covalently attached to band 3 of erythrocyte membranes. The electron spin resonance spectrum of the spin-labeled protein was examined at different temperatures in: (a) whole erythrocyte ghosts; (b) ghosts depleted of spectrin and actin; (c) alkaline-treated ghosts; (d) vesicles made with purified band 3 reassociated with dimyristoylphosphatidylcholine. Most spectra are composite with a major component corresponding to a large overall splitting. The determination of the percentage of the immobilized component was carried out by pairwise subtraction. At low temperatures (1-7 degrees C), the highest fraction of immobilized component was found in dimyristoylphosphatidylcholine vesicles (approx. 100%); alkaline-treated membranes had approx. 75% of the immobilized component at the same temperature; whole erythrocyte, spectrin/actin-depleted and spectrin/actin/ankyrin-depleted ghosts gave identical results (approx. 60% of immobilized component). The immobilized fraction decreased in all samples with increasing temperature or addition of a nonsolubilizing concentration of dodecyl octaethylene glycol monoether. In dimyristoylphosphatidylcholine vesicles, however, the modification in the ration of the two components was obtained only above the lipid transition temperature (23 degrees C). The strong immobilization of the spin-labeled lipid chain at all temperatures suggested trapping of the lipid chain between proteins. At low temperature, in dimyristoylphosphatidylcholine vesicles or in alkaline-treated ghosts, lipid-protein segregation is likely to take place. In whole erythrocyte ghosts, on the other hand, the large contribution of the motionally restricted component at physiological temperature indicates the oligomeric nature of band 3. Partial dissociation of the oligomers occurs as the temperature is increased, but the presence or absence of cytoskeletal proteins has no influence on the state of oligomerization of band 3.

Published

1984

19. Virus-induced fusion of human erythrocyte ghosts. I. Effects of macromolecules on the final stages of the fusion reaction.

Author

Sekiguchi K, Kuroda K, Ohnishi SI, and Asano A

Subjects

Albumins pharmacology, Cell Fusion drug effects, Glycoproteins pharmacology, Humans, In Vitro Techniques, Models, Biological, Parainfluenza Virus 1, Human, Erythrocyte Membrane drug effects, Erythrocytes drug effects, Macromolecular Substances

Abstract

Human erythrocyte ghosts prepared by hypotonic hemolysis can be fused by Sendai virus, provided that certain macromolecules (bovine serum albumin, dextran and others) are sequestered in the ghosts. Since fusion of the ghosts is dependent on intactness of the F(fusion)-glycoprotein of the virion, and since the other requirements for this reaction are also similar to those for the Sendai virus-induced fusion of intact erythrocytes, this system can be used as a model for the Sendai virus-induced cell fusion reaction. Sequestered macromolecules seem to be required for rounding of locally fused ghosts. Under low osmotic swelling conditions, such as use of ghosts sealed without macromolecules or using bovine serum albumin-loaded ghosts sealed in the presence of external macromolecules, no apparently complete cell fusion (large spherical polyghost formation) could be observed. Even under these conditions, however, occurrence of local cell fusion could be demonstrated either by transfer of fluorescent-labeled albumin from one ghost to an other, or by observation of polyghost formation after osmotic swelling in the cold. Thus, final stages of the fusion reaction can be divided into local cell-cell fusion which could not be observed by phase-contrast microscopy, and rounding (i.e. formation of spherical polyghosts). For the observation of fusion of ghosts, the last step seems to be important.

Published

1981

20. Effect of cetiedil on erythrocyte sickling: new type of antisickling agent that may affect erythrocyte membranes.

Author

Asakura T, Ohnishi ST, Adachi K, Ozguc M, Hashimoto K, Singer M, Russell MO, and Schwartz E

Subjects

Gels, Hemoglobin A, Hemoglobin, Sickle metabolism, Humans, Oxygen blood, Protein Denaturation drug effects, Rheology, Solubility, Antisickling Agents pharmacology, Azepines pharmacology, Erythrocyte Membrane drug effects, Erythrocytes drug effects, Erythrocytes, Abnormal drug effects, Thiophenes pharmacology

Abstract

The antisickling effect of cetiedil, alpha-cyclohexyl-3-thiopheneacetic acid 2-(hexahydro-1H-azepin-1-yl)-ethyl ester, has been investigated. The concentration of cetiedil required for 50% inhibition of erythrocyte sickling was about 140 micro M. An antisickling effect was achieved regardless of whether cetiedil was added before or after deoxygenation. The minimal gelling concentration of deoxy Hb S was increased by less than 10% in the presence of 218 micro M cetiedil. The oxygen equilibrium curves of Hb S were not significantly affected by cetiedil. Erythrocytes treated with high concentrations of cetiedil were swollen and became spheroidal. The antisickling effects of cetiedil might be due to an effect on erythrocyte membranes.

Published

1980

21. Membrane fluidity change in erythrocytes induced by complement system.

Author

Nakamura M, Ohnishi S, Kitamura H, and Inai S

Subjects

Animals, Complement C9 pharmacology, Electron Spin Resonance Spectroscopy, Erythrocytes immunology, Humans, Liposomes, Magnesium pharmacology, Osmotic Fragility drug effects, Phosphatidylcholines blood, Phosphatidylethanolamines blood, Rabbits immunology, Sheep, Spin Labels, Erythrocyte Membrane ultrastructure, Erythrocytes ultrastructure

Abstract

The structural change in erythrocyte membranes induced by antibody and complement was studied using phospholipid spin-labels. Sheep erythrocytes were labeled with phosphatidylcholine spin-label and various intermediate cells (erythrocyte-antibody complex (EA), EA bound with complement components from C1 to C7 (EAC1-7), EAC1-8, and EAC1-9) were prepared. Electron spin resonance spectra of EA, EAC1-7, and EAC1-8 were very similar to that of the erythrocytes, while that of EAC1-9 was markedly different. The overall splitting value for the lysed EAC1-9 (53 G) was much smaller than that for the erythrocytes (57 G), indicating a marked fluidization around the phosphatidylcholine label. The unlysed EAC1-9 membranes contained a limited fraction of the fluidized area. When EA was reacted with complement in the presence of 36% bovine serum albumin, the membranes were fluidized similarly to the lysed EAC1-9, although the hemolysis was largely blocked. The membranes of unlysed EAC1-9 prepared in isotonic (ethylenedinitrilo)tetraacetic acid were also fluidized, but to somewhat smaller extent. The role of C9 in the modification of erythrocyte membranes was also demonstrated using Mg2+ ghosts, which were prepared by hypotonic hemolysis in the presence of Mg2+. The membranes of Mg2+ ghost of EAC1-7 were markedly fluidized when bound with C8 and C9, but not affected by binding of C8 only. The component C8 was found to give a latent effect on the membranes that caused irreversible fluidization upon osmotic shock. The terminal component thus creates a fluidized area in the erythrocyte membranes through which small ions and molecules may diffuse more easily and the resulting osmotic unbalance may finally cause hemolysis.

Published

1976

22. Restriction of the lateral motion of band 3 in the erythrocyte membrane by the cytoskeletal network: dependence on spectrin association state.

Author

Tsuji A and Ohnishi S

Subjects

Cytoskeleton ultrastructure, Erythrocyte Membrane ultrastructure, Erythrocytes metabolism, Erythrocytes ultrastructure, Humans, Kinetics, Osmolar Concentration, Sodium Chloride pharmacology, Anion Exchange Protein 1, Erythrocyte metabolism, Cytoskeleton metabolism, Erythrocyte Membrane metabolism, Spectrin metabolism

Abstract

The effects of incubation of erythrocyte ghosts under various conditions (ionic strength or addition of ankyrin, diamines, or ATP) on the lateral motion of band 3 in the membranes were studied by using the fluorescence photobleaching recovery technique. Incubation of ghosts with exogenous ankyrin increased the immobile fraction of band 3, from 0.6 in intact ghosts to 0.8-0.9 when an average of 0.2 mol of extra ankyrin was bound per mole of band 3. Ankyrin-free band 3 proteins were mobile, but their mobility was governed by the spectrin association state in the cytoskeletal network. The diffusion constant was 5.3 X 10(-11) cm2 s-1 at a spectrin tetramer mole fraction of 0.3-0.4 in 10 mM NaCl/5 mM sodium phosphate, pH 7.8, and decreased 1 order of magnitude when the tetramer fraction increased to 0.5 in higher NaCl concentration (150 mM NaCl). A similar decrease was observed when the spectrin tetramer fraction was increased by 0.2 mM spermine in 10 mM NaCl/10 mM tris(hydroxymethyl)aminomethane hydrochloride, pH 7.6. On the other hand, the rotational motion of band 3 in the membranes was not affected by the spectrin association state. Trypsin treatment of ghosts cleaved off the cytoplasmic domain of band 3 and caused a marked (8-fold) increase in the lateral mobility, D = 4.0 X 10(-10) cm2 s-1. These results indicate that the lateral mobility of ankyrin-free band 3 protein is restricted by interactions of their cytoplasmic domain with the cytoskeletal network. A model is presented that band 3 can pass the network when spectrins are in dissociated dimers and cannot pass when they are tetramers. The lateral diffusion constant is thus determined by the spectrin dimer population in the network.

Published

1986