The elastic deformability of closed multilayered membranes is the same as that of a bilayer membrane

S. Svetina; B. Žekš

doi:10.1007/bf00185119

Evaluation of 1-Naphthol as a Convenient Fluorescent Probe for Monitoring Ethanol-induced Interdigitation in Lipid Bilayer Membrane¶

Photochemistry and Photobiology ◽

10.1562/0031-8655(2001)073<0573:eonaac>2.0.co;2 ◽

2001 ◽

Vol 73 (6) ◽

pp. 573 ◽

Cited By ~ 12

Author(s):

N. Pappayee ◽

Ashok K. Mishra

Keyword(s):

Fluorescent Probe ◽

Lipid Bilayer ◽

Bilayer Membrane ◽

Lipid Bilayer Membrane

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Recent Advances in Novasome Formulation Technology

International Journal of Pharmaceutical Sciences and Nanotechnology ◽

10.37285/ijpsn.2014.7.2.1 ◽

2014 ◽

Vol 7 (2) ◽

pp. 2407-2411

Author(s):

J M Shah ◽

N.H Shah ◽

Hadiya P D

Keyword(s):

Drug Delivery ◽

Effective Means ◽

Entrapment Efficiency ◽

Bilayer Membrane ◽

Water Soluble ◽

Delivery Methods ◽

Liposomal Drug ◽

Pharmaceutical Technology ◽

Insoluble Drugs ◽

Novel Drug

Pharmaceutical technology has developed various newer modes of novel drug delivery aspects. Modifications in the previously existing drug delivery methods have led to various newly innovated technologies serving as a safe and effective means of improvement over the existing ones. Novasome technology is one of the new innovations of liposomes which have solved many of the problems related to liposomal drug delivery system. It offers a seven bilayer membrane which has the ability to incorporate both water soluble and insoluble drugs. It has an excellent entrapment efficiency which provides better medication. Formulation of novasomes is achieved in a high shear device. Due to its numerous advantages, novasomes have been used extensively in various fields like cosmetics, chemical, personal care, foods, pharmaceuticals and agrochemicals.

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Excitation of Bilayer Membrane

Seibutsu Butsuri ◽

10.2142/biophys.9.49 ◽

1969 ◽

Vol 9 (2) ◽

pp. 49-66

Author(s):

Masayuki TAKAGI

Keyword(s):

Bilayer Membrane

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Transmembrane signal transduction by cofactor transport

Chemical Science ◽

10.1039/d1sc03910e ◽

2021 ◽

Author(s):

Istvan Kocsis ◽

Yudi Ding ◽

Nicholas H. Williams ◽

Christopher A. Hunter

Keyword(s):

Signal Transduction ◽

Lipid Bilayer ◽

Metal Ion ◽

Bilayer Membrane ◽

Ester Hydrolysis ◽

Lipid Bilayer Membrane ◽

Metal Ion Cofactors

Synthetic transducers transport externally added metal ion cofactors across the lipid bilayer membrane of vesicles to trigger catalysis of ester hydrolysis in the inner compartment. Signal transduction activity is modulated by hydrazone formation.

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Evaluation of the correlation between porphyrin accumulation in cancer cells and functional positions for application as a drug carrier

Scientific Reports ◽

10.1038/s41598-021-81725-3 ◽

2021 ◽

Vol 11 (1) ◽

Author(s):

Koshi Nishida ◽

Toshifumi Tojo ◽

Takeshi Kondo ◽

Makoto Yuasa

Keyword(s):

Cancer Cells ◽

Drug Carrier ◽

Bilayer Membrane ◽

Phospholipid Bilayer ◽

Membrane Permeation ◽

Porphyrin Derivatives ◽

Phospholipid Bilayer Membrane ◽

Meso Position ◽

Tumor Accumulation ◽

Binding Position

AbstractPorphyrin derivatives accumulate selectively in cancer cells and are can be used as carriers of drugs. Until now, the substituents that bind to porphyrins (mainly at the meso-position) have been actively investigated, but the effect of the functional porphyrin positions (β-, meso-position) on tumor accumulation has not been investigated. Therefore, we investigated the correlation between the functional position of substituents and the accumulation of porphyrins in cancer cells using cancer cells. We found that the meso-derivative showed higher accumulation in cancer cells than the β-derivative, and porphyrins with less bulky substituent actively accumulate in cancer cells. When evaluating the intracellular distribution of porphyrin, we found that porphyrin was internalized by endocytosis and direct membrane permeation. As factors involved in these two permeation mechanisms, we evaluated the affinity between porphyrin-protein (endocytosis) and the permeability to the phospholipid bilayer membrane (direct membrane permeation). We found that the binding position of porphyrin affects the factors involved in the transmembrane permeation mechanisms and impacts the accumulation in cancer cells.

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Natural channel protein inserts and functions in a completely artificial, solid-supported bilayer membrane

Scientific Reports ◽

10.1038/srep02196 ◽

2013 ◽

Vol 3 (1) ◽

Cited By ~ 36

Author(s):

Xiaoyan Zhang ◽

Wangyang Fu ◽

Cornelia G. Palivan ◽

Wolfgang Meier

Keyword(s):

Bilayer Membrane ◽

Channel Protein ◽

Supported Bilayer ◽

Natural Channel

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Protein Sensing Device with Multi-Recognition Ability Composed of Self-Organized Glycopeptide Bundle

International Journal of Molecular Sciences ◽

10.3390/ijms22010366 ◽

2020 ◽

Vol 22 (1) ◽

pp. 366

Author(s):

Mao Arai ◽

Tomohiro Miura ◽

Yuriko Ito ◽

Takatoshi Kinoshita ◽

Masahiro Higuchi

Keyword(s):

Binding Site ◽

Lipid Bilayer ◽

Structural Changes ◽

Bilayer Membrane ◽

Lipid Bilayer Membrane ◽

Target Protein ◽

Self Organization ◽

Specific Response ◽

Target Proteins ◽

Recognition Ability

We designed and synthesized amphiphilic glycopeptides with glucose or galactose at the C-terminals. We observed the protein-induced structural changes of the amphiphilic glycopeptide assembly in the lipid bilayer membrane using transmission electron microscopy (TEM) and Fourier transform infrared reflection-absorption spectra (FTIR-RAS) measurements. The glycopeptides re-arranged to form a bundle that acted as an ion channel due to the interaction among the target protein and the terminal sugar groups of the glycopeptides. The bundle in the lipid bilayer membrane was fixed on a gold-deposited quartz crystal microbalance (QCM) electrode by the membrane fusion method. The protein-induced re-arrangement of the terminal sugar groups formed a binding site that acted as a receptor, and the re-binding of the target protein to the binding site induced the closing of the channel. We monitored the detection of target proteins by the changes of the electrochemical properties of the membrane. The response current of the membrane induced by the target protein recognition was expressed by an equivalent circuit consisting of resistors and capacitors when a triangular voltage was applied. We used peanut lectin (PNA) and concanavalin A (ConA) as target proteins. The sensing membrane induced by PNA shows the specific response to PNA, and the ConA-induced membrane responded selectively to ConA. Furthermore, PNA-induced sensing membranes showed relatively low recognition ability for lectin from Ricinus Agglutinin (RCA120) and mushroom lectin (ABA), which have galactose binding sites. The protein-induced self-organization formed the spatial arrangement of the sugar chains specific to the binding site of the target protein. These findings demonstrate the possibility of fabricating a sensing device with multi-recognition ability that can recognize proteins even if the structure is unknown, by the protein-induced self-organization process.

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Biocompatibility of Bacterial Magnetosomes as MRI Contrast Agent: A Long-Term In Vivo Follow-Up Study

Nanomaterials ◽

10.3390/nano11051235 ◽

2021 ◽

Vol 11 (5) ◽

pp. 1235

Author(s):

Xiaohui Nan ◽

Wenjia Lai ◽

Dan Li ◽

Jiesheng Tian ◽

Zhiyuan Hu ◽

...

Keyword(s):

Contrast Agent ◽

Magnetic Domain ◽

Bilayer Membrane ◽

The Body ◽

Mri Contrast Agent ◽

Mri Imaging ◽

Mri Contrast

Derived from magnetotactic bacteria (MTB), magnetosomes consist of magnetite crystals enclosed within a lipid bilayer membrane and are known to possess advantages over artificially synthesized nanoparticles because of the narrow size distribution, uniform morphology, high purity and crystallinity, single magnetic domain, good biocompatibility, and easy surface modification. These unique properties have increasingly attracted researchers to apply bacterial magnetosomes (BMs) in the fields of biology and medicine as MRI imaging contrast agents. Due to the concern of biosafety, a long-term follow-up of the distribution and clearance of BMs after entering the body is necessary. In this study, we tracked changes of BMs in major organs of mice up to 135 days after intravenous injection using a combination of several techniques. We not only confirmed the liver as the well-known targeted organs of BMs, but also found that BMs accumulated in the spleen. Besides, two major elimination paths, as well as the approximate length of time for BMs to be cleared from the mice, were revealed. Together, the results not only confirm that BMs have high biocompatibility, but also provide a long-term in-vivo assessment which may further help to forward the clinical applications of BMs as an MRI contrast agent.

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Quantitative Estimation of Cyclotide-Induced Bilayer Membrane Disruption by Lipid Extraction with Mesoscopic Simulation

Journal of Chemical Information and Modeling ◽

10.1021/acs.jcim.1c00332 ◽

2021 ◽

Author(s):

Karina van den Broek ◽

Matthias Epple ◽

Lisa Sophie Kersten ◽

Hubert Kuhn ◽

Achim Zielesny

Keyword(s):

Quantitative Estimation ◽

Lipid Extraction ◽

Bilayer Membrane ◽

Membrane Disruption ◽

Mesoscopic Simulation

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Molecular dynamics simulations and experimental studies reveal differential permeability of withaferin-A and withanone across the model cell membrane

Scientific Reports ◽

10.1038/s41598-021-81729-z ◽

2021 ◽

Vol 11 (1) ◽

Author(s):

Renu Wadhwa ◽

Neetu Singh Yadav ◽

Shashank P. Katiyar ◽

Tomoko Yaguchi ◽

Chohee Lee ◽

...

Keyword(s):

Molecular Dynamics ◽

Cell Membrane ◽

Molecular Dynamics Simulations ◽

Experimental Studies ◽

Bilayer Membrane ◽

Withaferin A ◽

Head Group ◽

Polar Head Group ◽

Natural Drugs ◽

Dynamics Simulations

AbstractPoor bioavailability due to the inability to cross the cell membrane is one of the major reasons for the failure of a drug in clinical trials. We have used molecular dynamics simulations to predict the membrane permeability of natural drugs—withanolides (withaferin-A and withanone) that have similar structures but remarkably differ in their cytotoxicity. We found that whereas withaferin-A, could proficiently transverse through the model membrane, withanone showed weak permeability. The free energy profiles for the interaction of withanolides with the model bilayer membrane revealed that whereas the polar head group of the membrane caused high resistance for the passage of withanone, the interior of the membrane behaves similarly for both withanolides. The solvation analysis further revealed that the high solvation of terminal O5 oxygen of withaferin-A was the major driving force for its high permeability; it interacted with the phosphate group of the membrane that led to its smooth passage across the bilayer. The computational predictions were tested by raising and recruiting unique antibodies that react to withaferin-A and withanone. The time-lapsed analyses of control and treated cells demonstrated higher permeation of withaferin-A as compared to withanone. The concurrence between the computation and experimental results thus re-emphasised the use of computational methods for predicting permeability and hence bioavailability of natural drug compounds in the drug development process.

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