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1 g in a more natural and detergent-free lipid bilayer.
2 ent, hydrophobic interactions with the lipid bilayer.
3 ermine the ability of actin to adsorb to the bilayer.
4 hat the C-edge of betaarr1 engages the lipid bilayer.
5 -glycero-3-phosphocholine (DC(18:1)PC) lipid bilayer.
6 OF transporter and partition into the lipid bilayer.
7 -42) fragments that were closer to the lipid bilayer.
8 des are unaffected by dehydration within the bilayer.
9 the mechanical properties of the surrounding bilayer.
10 ecause of difficulties in modeling the lipid bilayer.
11 tate, each embedded in a phosphatidylcholine bilayer.
12 g mechanical force transmitted via the lipid bilayer.
13 eptides that interact with a supported lipid bilayer.
14 the exofacial and cytofacial aspects of the bilayer.
15 monomers, crosslinkers, and CTAs within the bilayer.
16 depends on their interactions with the lipid bilayer.
17 ee acyl coenzyme A (acyl-CoA) from the lipid bilayer.
18 an Na(V)1.7 and their affinity for the lipid bilayer.
19 mol % PS induces extensive reordering of the bilayer.
20 remarkable; it is a highly asymmetric lipid bilayer.
21 and their proximity with the supported lipid bilayer.
22 reas gamma-aminobutyric is excluded from the bilayer.
23 the bulky transport domain through the lipid bilayer.
24 he structural properties of the phospholipid bilayer.
25 the presence of cholesterol to pierce lipid bilayers.
26 s a MoN(2) layer sandwiched between two Si-N bilayers.
27 their in vivo orientation within fluid lipid bilayers.
28 in the vicinity of differently charged lipid bilayers.
29 cholesterol complexation with gp41 in lipid bilayers.
30 -angle x-ray scattering (WAXS) from oriented bilayers.
31 ns contribute to lateral clustering on lipid bilayers.
32 elated to a peptide-induced cross-linking of bilayers.
33 ane channels in cholesterol-containing lipid bilayers.
34 o potency at Na(V)1.7 and affinity for lipid bilayers.
35 cording of RyR2 activity in artificial lipid bilayers.
36 MAG are not presented as part of fluid lipid bilayers.
37 resembling the morphology of supported lipid bilayers.
38 ent conformational dynamics of MdfA in lipid bilayers.
39 of alphaS and modulates the binding to lipid bilayers.
40 ipids, especially near the midplane of lipid bilayers.
41 ted for membrane proteins in supported lipid bilayers.
42 unilamellar vesicles (SUVs) and planar lipid bilayers.
43 th or alter the physical properties of lipid bilayers.
44 ouplings between CDWs in neighbouring CuO(2) bilayers.
45 cal phenomena like phase separation in lipid bilayers.
46 from the conformation of the channel in POPC bilayers.
47 r that forms single channels in phospholipid bilayers.
48 had previously been shown to fuse with lipid bilayers.
49 tive pressures in liquids that contain lipid bilayers.
50 ctively transport anions across phospholipid bilayers.
51 complex Rabex5/Rabaptin5 on supported lipid bilayers.
52 nnel formation and pH gating in planar lipid bilayers.
53 ptical effects(8) in antiferromagnetic (AFM) bilayers.
54 ls but perturb the local properties of lipid bilayers.
55 that can otherwise pass through phospholipid bilayers.
56 s' association with zwitterionic and anionic bilayers.
57 he driving force of the reaction, large mono/bilayer (1.1 mm/200 mum) flakes or full-coverage films (
60 odifier toxins have affinity for model lipid bilayers, a tripartite relationship among gating modifie
61 nspecific neurotransmitter adsorption to the bilayer-a process not considered in the established mode
62 face profile, which displays increased lipid bilayer affinity and in vitro activity at the voltage-ga
64 ide mimics of mucins and added them to lipid bilayers, allowing chemical control of length, glycosyla
65 he ratio of negatively charged lipids in the bilayer altered membrane bending and binding properties
68 orm low order oligomers on a supported lipid bilayer and that neither membrane association nor access
69 to maximise protein integration into a lipid bilayer and the oligomerisation of the protein into func
70 namics (MD) simulations in an explicit lipid bilayer and water environment (1.6 million atoms in tota
72 ne protein W have been investigated in lipid bilayers and detergent micelles by solution NMR relaxati
73 determined that PlsX binds directly to lipid bilayers and identified its membrane anchoring moiety, c
74 the lipid-lipid interactions in model lipid bilayers and improve our understanding of the lateral or
75 onge phase contains a dense network of lipid bilayers and nanometric aqueous channels, which allows d
76 es to quantify protein-lipid interactions in bilayers and understand how membrane proteins remodel th
77 onsist of a protein belt surrounding a lipid bilayer, and are broadly used for characterization of me
78 ded hydrophilic side chains within the lipid bilayer, and it disengages concomitant with substrate fo
79 e de novo NMR structure in near-native lipid bilayers, and by accessing structural dynamics relevant
80 nel conductance measurements in planar lipid bilayers, and in vivo fluorescence imaging, we demonstra
81 rm water-filled nanoscale pores within lipid bilayers, and their properties are dependent on the comp
82 preserve the biophysical properties of lipid bilayers, and therefore, questions on binding specificit
83 teractions between actin filaments and lipid bilayers are possible and that the net charge of the bil
84 are possible and that the net charge of the bilayer as well as the presence of divalent ions in the
86 ned to evaluate the drug's affinity for DMPC bilayers, as well as to assess the drug's effects on the
87 ibit selective proton transport across lipid bilayers at a rate similar to those of natural proton ch
88 recombinant APOL1 inserts into planar lipid bilayers at acidic pH to form pH-gated nonselective cati
89 c simulations to be highly flexible in lipid bilayers at ambient temperature, with large rocking moti
93 rrelated system based on small-angle twisted bilayer-bilayer graphene (TBBG), consisting of two rotat
95 e molecular orientations in the phospholipid bilayer but cannot resolve the actual distribution of mo
96 apsed conformation at the level of the lipid bilayer, but we observed a large, hydrophilic and fully
98 e van der Waals interface of the TMDC hetero-bilayer can efficiently separate electrons and holes in
100 on membrane molecules propagate to the lipid bilayer components to generate specific nanomechanical r
101 eight, flexible, transparent, and conductive bilayer composite of polyetherimide and single-layer gra
102 ations of the protein in a complex mammalian bilayer containing more than 60 different lipid types to
105 eimer's disease that the disruption of lipid bilayers correlates linearly with the time course of the
106 ng prediction of protein orientations in the bilayer, DeltaDeltaG calculations, native structure disc
107 channels embedded in planar suspended lipid bilayers demonstrate that anionic gold nanoparticles (Au
108 -soluble fluorophores to interact with lipid bilayers, detailed fluorophore-lipid interactions and, m
109 r a wide range of conditions and exhibit the bilayered-disc morphology of ideal bicelles even at low
110 opy indicates that AuNP interaction with the bilayer does not perturb the conformation of membrane-em
111 force alters the physical state of the lipid bilayer, driving mechanosensors to assume conformations
112 rporated into encapsulated droplet interface bilayers (eDIBs), or artificial cells, and the biolumine
113 sting that physical deformation of the lipid bilayer, either by mechanical force or curvature, can in
114 spike pore follows from predictions of lipid bilayer elasticity and offers an explanation for previou
115 e molecule approaches, nanodisc-based planar bilayer electrophysiology and single-molecule FRET, to a
117 sphatase CD45 is more strongly excluded from bilayer-engaged BRCs than a transmembrane peptide, indic
118 l docking complex Pex14p/Pex17p, in a native bilayer environment, and reveal its subunit organization
121 o protrude through the enzyme into the lipid bilayer, facilitating the desaturation of very-long-chai
123 than the second-stage rate, associated with bilayer formation, indicating that the first-stage react
124 study demonstrates the role of phospholipid bilayer fragment as the key intermediate in the mechanis
126 ARS-CoV-2) virions are surrounded by a lipid bilayer from which spike (S) protein trimers protrude(1)
130 topological character in magic-angle twisted bilayer graphene (MATBG) has created a unique opportunit
131 uperconducting phases in magic-angle twisted bilayer graphene (MATBG)(1,2) crucially depend on the in
133 der Waals heterostructures of twisted double bilayer graphene (TDBG), we demonstrate a flat electron
134 t the observation of a QAH effect in twisted bilayer graphene aligned to hexagonal boron nitride.
135 cting states observed in magic-angle twisted-bilayer graphene and ABC trilayer graphene/boron nitride
136 ctroscopic properties of magic-angle twisted bilayer graphene as a function of electron filling, dete
138 inter-LL optical transitions of high-quality bilayer graphene by photocurrent spectroscopy measuremen
140 eation of weakly dispersive, 'flat' bands in bilayer graphene for certain 'magic' angles of twist bet
144 on the electronic band structure of twisted bilayer graphene using a back-gated device architecture
145 a moire superlattice potential (via aligning bilayer graphene with the top and/or bottom boron nitrid
146 and superconductivity in magic-angle twisted bilayer graphene(1,2) has enabled the experimental inves
147 ted insulating states in magic-angle twisted bilayer graphene(1-11) prompts fascinating questions abo
148 fect in the flat band of magic-angle twisted bilayer graphene(4-8) has sparked the exploration of cor
150 als, ranging from cuprate superconductors to bilayer graphene, and may arise from physics beyond the
154 t for imaging moire superlattices of twisted bilayers graphene encapsulated by hexagonal boron nitrid
157 Images of micrometer-scale domains in lipid bilayers have provided the gold standard of model-free e
159 h conventional views regarding the growth of bilayer hexagonal ices and 2D hexagonal matter in genera
160 r-type phosphatases was observed on the soft bilayers, however, even though it is yet to be demonstra
161 ell membranes and reconstituted phospholipid bilayers; however, the mechanisms by which these changes
163 iochemical properties, nucleosides are lipid bilayer impermeable and thus rely on dedicated transport
164 ntercalation of sodium dodecyl sulfate (SDS) bilayers in a PEM comprising poly(diallyldimethylammoniu
166 -transfer agents (CTA) within self-assembled bilayers in an aqueous suspension enabled the successful
168 channel electrical recording in planar lipid bilayers in conjunction with protein engineering, we exp
169 re-gel droplets were connected through lipid bilayers in predetermined architectures and photopolymer
170 to form treadmilling filaments on supported bilayers in vitro(1), as well as in live cells, in which
171 PSFL1 can transfer PIP into PA-rich membrane bilayers in vitro, suggesting that CPSFL1 potentially fa
176 s lateral movement of proteins in this lipid bilayer is possible, it is rather limited in turgid and
177 tJ (or TMBIM6) structure embedded in a lipid bilayer is uncharacterized, let alone the molecular mech
179 , emulated by the PEG molecules at the lipid bilayer, is enough to promote the polymerization of the
180 ropic behavior, available free volume of the bilayer, its excess surface area, and bending elasticity
181 rthermore, we observe MBP to insert into its bilayer leaflet side in case of the diseased lipid mixtu
183 verapamil dynamically flip flops between the bilayer leaflets, possibly rendering its net transport f
184 icial membranes, so-called sparsely tethered bilayer lipid membranes, reveal the structural aspects o
186 phosphocholine (PGPC), and each of the three bilayer lipids, 1,2-dipalmitoyl-sn-glycero-3-phosphochol
189 ted actin network interacting with the lipid bilayer membrane have been assumed to control RBC shape,
190 der reconstitution process by increasing the bilayer membrane rigidity against the dehydration tensio
192 r greigite (Fe(3)S(4)), enveloped by a lipid bilayer membrane, produced by magnetotactic bacteria.
196 Furthermore, this study expands the lipid-bilayer model by suggesting that the force-induced topol
197 explanations for mechanosensitivity, a lipid-bilayer model, suggests that a stretch of the membrane i
201 o closed (elliptical) dispersion contours in bilayers of alpha-phase molybdenum trioxide (alpha-MoO(3
202 tains exclusively the outer leaflet of lipid bilayers of liposomes, as evidenced by leaflet-specific
203 In particular, we analyze in detail twisted bilayers of Neel antiferromagnets on the honeycomb latti
204 , and here we activate B-cells via supported bilayers of phosphatidylcholine lipids, a natural ligand
205 Here, we review regulation of the lipid bilayers of the NE and suggest ways to generate lipid as
206 omparing coexisting domains with homogeneous bilayers of the same composition, we demonstrate how dom
207 by atomic manipulation on a sodium chloride bilayer on Cu(111) at 5 K, and imaged by high-resolution
208 nding atomistic structure, and the potential bilayer orientation determined by TMDET algorithm of a g
210 becomes important to be able to predict the bilayer-perturbing potency of hydrophobic/amphiphilic dr
211 nergy by drug-induced perturbations of lipid bilayer physical properties and bilayer-gramicidin inter
215 hilic [Co(L3)](2+) complex into the liposome bilayer produces a more highly shifted CEST peak at -13
218 ire lattices formed in twisted van der Waals bilayers provide a unique, tunable platform to realize c
219 avity, which opens laterally to the membrane bilayer, providing lipid access to the active site.
220 33 and 49 cm(2) V(-1) s(-1) for the mono and bilayer regions) and on/off ratio (1 ~ 5 x 10(8)) across
222 tubes capable of self-inserting into a lipid bilayer, represent a simplified model of biological memb
223 rane-embedded components within phospholipid bilayers represents a distinct class of phase transforma
224 ing a liquid-ordered phase is changed into a bilayer resembling a fluid-liquid-disordered phase surro
225 complexes induce a transformation in which a bilayer, resembling a liquid-ordered phase is changed in
227 binding via His-tag insertion into the CoPoP bilayer results in a serum-stable and conformationally i
229 patterning nucleation sites on monolayer or bilayer s-TMDs, we precisely control the nucleation and
231 ar vesicles (EVs) are membrane-derived lipid bilayers secreted by bacteria and eukaryotic cells.
233 pid membrane of liposomes was characterized (bilayer size, chain conformational order, lateral packin
234 orm ITIR-FCS measurements on supported lipid bilayers (SLBs) of various lipid compositions to charact
235 hatidylserine (PS) lipids in supported lipid bilayers (SLBs), forming a PS-Zn(2+) complex with an equ
237 ion analysis, we find that BRCs engaged with bilayers sort minimal peptide markers of liquid-ordered
241 membrane homeostasis, we identified a lipid bilayer stress (LBS) sensor in the UPR transducer protei
242 fect originates from a looser swelling lipid bilayer structure due to the adsorption and electrostati
244 led that individual nanohelices consist of a bilayer structure with the outer and inner layers derive
245 he structural properties of the phospholipid bilayer, suggesting that both ionized and neutral states
248 indicate that the presence of MGDG in lipid bilayers switches LHCII from a light-harvesting to a mor
249 SpA was attached to BioPE-DOTAP binary lipid bilayer tethered on alkane thiol molecular cushions.
250 nct alterations in the structure of the DMPC bilayer than the deprotonated/ionized form, considering
252 ram-negative bacteria is an asymmetric lipid bilayer that consists of inner leaflet phospholipids and
253 s of transient pores on a patch of the lipid bilayer that is strengthened by an elastic meshwork repr
255 ICG interaction with the cell membrane lipid bilayer, the pharmacology and toxicology in vitro and in
257 of liposome systems to DMSO in terms of the bilayer thermotropic behavior, available free volume of
258 we demonstrate that cryo-EM can distinguish bilayer thickness differences as small as 0.5 angstrom,
261 n a constitutively active state in POPC:POPG bilayers through the use of real-time fluorescence quenc
264 n is ion specific, inducible by exposing the bilayer to muM concentrations of Zn(2+) but not Mg(2+),
265 ylethanol was incorporated into the liposome bilayer to provide the nanovesicles with fluorescence wi
267 esting complex II (LHCII) in thylakoid lipid bilayers to detect LHCII conformational dynamics in its
268 We developed a method for attaching lipid bilayers to polydimethylsiloxane polymer supports, produ
270 pathways of peptide insertion into the lipid bilayer (triggered by a pH drop) and peptide exit from t
272 the dyads assemble to create an alternating bilayer type structure, with horizontal alternating alky
273 oups with linear p-alkoxyphenyl units led to bilayer-type smectic mesophases, wedge-shaped units resu
274 rane proteins embedded in their native lipid bilayer, typically by retracting the cantilever at a con
276 bedded in synthetic liquid crystalline lipid bilayers using two-dimensional J-resolved NMR spectrosco
277 tably inserted into the outer leaflet of the bilayer, verapamil dynamically flip flops between the bi
278 ionally well-defined large unilamellar lipid bilayer vesicles to study the impact of MGDG on light ha
279 PIP(2) immobilization also occurred when the bilayer was supported on a protein surface rather than g
280 ng status of reconstituted hairpins in lipid bilayers, we found that the E217G hairpin exhibits an al
282 cellular domains tethered to supported lipid bilayers, were studied using a combination of dynamic si
283 is hampered by Peierls instability, or other bilayers, where doping by applied voltage is required, r
284 r with that occurring in the edge state of a bilayer, which is terminated by ferromagnetic iron clust
285 distinct alterations in phosphatidylcholine bilayers, which are used in this work as models for the
286 model by studying angle-aligned WSe(2)/WS(2) bilayers, which form moire superlattices(6) because of t
289 ial of this technique, diffraction gratings, bilayer wire-grid polarizers, and resonant metal mesh lo
291 ring in the edge state of a pristine bismuth bilayer with that occurring in the edge state of a bilay
294 near-0 degrees -twist-angle MoSe(2)/MoSe(2) bilayers with large rhombohedral AB/BA domains(15) to di
295 e disc mediated formation of supported lipid bilayers with membrane proteins represents an attractive
296 incorporation of membrane proteins in lipid bilayers with sufficiently high concentration and contro
297 iate the formation of supported phospholipid bilayers with two different types of membrane proteins,
298 ylsiloxane polymer supports, producing "soft bilayers" with physiological levels of mechanical resist
299 st that lipids can favorably assemble into a bilayer within the larger CALHM2 pore, but not within CA
300 ily can successfully insert into a synthetic bilayer without the need for translocon insertase appara