戻る
「早戻しボタン」を押すと検索画面に戻ります。 [閉じる]

コーパス検索結果 (1語後でソート)

通し番号をクリックするとPubMedの該当ページを表示します
1 pyrazole) and further characterized by X-ray crystallography.
2 ly characterized by NMR techniques and X-ray crystallography.
3 sis, UV-vis spectrum measurements, and X-ray crystallography.
4 ation of its structure and assembly by X-ray crystallography.
5 curacy of macromolecular structures in X-ray crystallography.
6 is-ethylene linkers was explored using X-ray crystallography.
7 mino-alpha-ketone group was secured by X-ray crystallography.
8 at has previously been accomplished by X-ray crystallography.
9 osteric regulation of isolated GCH1 by X-ray crystallography.
10 esolution cryo-electron tomography and X-ray crystallography.
11 ariable binding modes were observed by X-ray crystallography.
12 ferent DHHC-PATs were determined using X-ray crystallography.
13  by means of enzymatic assays, MS, and X-ray crystallography.
14 gated their binding modalities through X-ray crystallography.
15 y of NMR spectroscopic experiments and X-ray crystallography.
16 ic voltammetry, mass spectrometry, and X-ray crystallography.
17 ed to improve maps from macromolecular X-ray crystallography.
18 ansfer difference NMR spectroscopy and X-ray crystallography.
19 tructures of the inhibited protease by X-ray crystallography.
20 acilitates their precise characterization by crystallography.
21 or anticoagulant activity) as shown by X-ray crystallography.
22 of P at 1.4- angstrom resolution using X-ray crystallography.
23 followed by structure determination by X-ray crystallography.
24 r, and its structure was determined by X-ray crystallography.
25 mplex with the EGFR kinase domain with X-ray crystallography.
26 etic resonance (EPR) spectroscopy, and X-ray crystallography.
27 terized by NMR, mass spectroscopy, and X-ray crystallography.
28 ously reported homodimer identified by X-ray crystallography.
29  characterized by multinuclear NMR and X-ray crystallography.
30 lyst was prepared and characterized by X-ray crystallography.
31  are consistent with structures modeled from crystallography.
32 nd cyclic voltammetry measurements and X-ray crystallography.
33  making it unsuitable for conventional X-ray crystallography.
34 c studies, H/D isotopic labelling, and X-ray crystallography.
35 eshing a protein with a structure from x-ray crystallography.
36 damental mathematical framework of classical crystallography.
37 ere identified by NMR spectroscopy and X-ray crystallography.
38 are fully elucidated by single-crystal X-ray crystallography.
39 ed for samples that are intractable by X-ray crystallography.
40 ocused screen of proline analogs using X-ray crystallography.
41 ally used for structure elucidation by X-ray crystallography.
42 te models have been studied by NMR and X-ray crystallography.
43 acterized by (1)H NMR spectroscopy and X-ray crystallography.
44  microanalysis, mass spectrometry, and X-ray crystallography.
45 riboswitch ligand binding domain using X-ray crystallography.
46  HSPB6 that has recently been resolved using crystallography.
47  which was confirmed by single-crystal X-ray crystallography.
48 o C=C bond) has been confirmed through X-ray crystallography.
49 lying the approach was corroborated by X-ray crystallography.
50 -PH(2) (3a) have been characterized by X-ray crystallography.
51 ation of membrane proteins and time-resolved crystallography.
52 ion mass spectrometry (HRMS), NMR, and X-ray crystallography.
53 yrG promoter using soak-trigger-freeze X-ray crystallography.
54 now been structurally characterized by X-ray crystallography.
55  P11 and defined their interactions by X-ray crystallography.
56 lution by cryo-electron microscopy and X-ray crystallography.
57 nine was isolated and characterized by X-ray crystallography.
58 d, in many cases, using single-crystal X-ray crystallography.
59 electronic, and IR spectroscopy and by X-ray crystallography.
60 rotein co-structures are determined by X-ray crystallography.
61 echanisms using molecular dynamics and X-ray crystallography.
62 one structure was further confirmed by X-ray crystallography.
63 Here we use time-resolved serial femtosecond crystallography(1) using an X-ray free-electron laser(2)
64 cluding national security(1,2), medicine(3), crystallography(4) and astronomy(5).
65 igated by electron microscopy(4,5) and X-ray crystallography(6-8).
66               Here, we demonstrate via X-ray crystallography a nanobody-targeted allosteric binding s
67 rmations of MdfA have been captured by X-ray crystallography: An outward open (O(o)) conformation, st
68 try, small-angle X-ray scattering, and X-ray crystallography analyses, we have pinpointed a critical
69 stry of two products were confirmed by X-ray crystallography analysis.
70  products is discussed on the basis of X-ray crystallography analysis.
71                                We used x-ray crystallography and biochemical approaches to show that
72  is both structurally characterized by X-ray crystallography and capable of activating strong C-H bon
73             We, therefore, characterized the crystallography and carbon uptake in the shells of S. gl
74                     In the following, we use crystallography and computational modeling to show that
75 tural studies using techniques such as x-ray crystallography and cryo-electron microscopy (cryo-EM).
76                                        X-ray crystallography and cryo-electron microscopy have reveal
77             Structure determination by X-ray crystallography and cryo-electron microscopy not only co
78 form self-recognition complexes, using X-ray crystallography and cryo-electron tomography.
79 he SOSIP structures determined by both x-ray crystallography and cryo-EM.
80     The reported results complement existing crystallography and cryoelectron tomography data on the
81                                  While X-ray crystallography and electron microscopy have revealed st
82                                       Recent crystallography and electron microscopy studies have ref
83 ge mass spectrometry, room-temperature X-ray crystallography and EPR spectroscopy on four SLO variant
84    Nowadays, it is possible to combine X-ray crystallography and fragment screening in a medium throu
85   A structural study was undertaken by X-ray crystallography and in silico tools to assess the ligand
86                                           By crystallography and isothermal titration calorimetry (IT
87                      NMR spectrometry, X-ray crystallography and mass spectrometry confirm the format
88                                        X-ray crystallography and molecular docking analysis of PioOH-
89                                        X-ray crystallography and molecular dynamics simulations provi
90                                  Using X-ray crystallography and molecular dynamics simulations, we d
91                                        X-ray crystallography and mutagenesis confirmed a structure wi
92 ated structural biology approach using X-ray crystallography and NMR spectroscopy and evaluate their
93 eaction products were characterized by X-ray crystallography and NMR spectroscopy.
94 e trapped, off-pathway oligomers using X-ray crystallography and NMR, providing insight into why tetr
95  using a combination of single-crystal X-ray crystallography and paramagnetic (1)H NMR spectroscopy,
96          Here we used a combination of X-ray crystallography and protein engineering to define the de
97 ario emerged from previous findings of X-ray crystallography and rapid kinetics supporting a pre-exis
98 s (Tth) has been unambiguously determined by crystallography and reveals it to occupy the peptidyl tr
99                            Integrating x-ray crystallography and SAXS, we also describe the structure
100                                        X-ray crystallography and SDS-PAGE further show that trimer 4(
101 rming hexamers that can be observed by X-ray crystallography and SDS-PAGE.
102                            In this work, NMR crystallography and single-crystal X-ray diffraction are
103                           Here, we use X-ray crystallography and single-particle cryo-electron micros
104 ism, we determined eight structures by X-ray crystallography and single-particle cryo-electron micros
105                                        X-ray crystallography and small-angle X-ray scattering showed
106 he proposed EnT acceptors were elucidated by crystallography and spectroscopic binding studies.
107 sis, we have used ultrahigh-resolution X-ray crystallography and the recently approved beta-lactamase
108  the only system where high-resolution X-ray crystallography and toxicity data are available.
109   We solve its 3D structure by NMR and x-ray crystallography and validate leads with 3 different radi
110 pounds with binding modes confirmed by X-ray crystallography and yielded unexpectedly accurate and st
111 Combining experimental biochemistry, protein crystallography, and advanced computer simulations we sh
112 R, and EPR spectroscopies with magnetometry, crystallography, and advanced theoretical treatments sug
113 of cryo-electron microscopy (cryo-EM), x-ray crystallography, and computational predictions were used
114  using molecular dynamics simulations, X-ray crystallography, and cryoEM.
115 /mechanics molecular mechanics calculations, crystallography, and detection of intermediate (hypohalo
116  EPR spectroscopy, elemental analysis, X-ray crystallography, and DFT calculations.
117  mobility macromolecular analysis, EM, X-ray crystallography, and enzyme assays.
118 inetic analyses, fluorescence binding, X-ray crystallography, and gel filtration experiments with asp
119                   Functional analysis, x-ray crystallography, and molecular dynamics simulations reve
120  and membrane permeabilization assays, X-ray crystallography, and molecular dynamics simulations.
121 ining kinetic and biophysical methods, X-ray crystallography, and molecular modeling, as well as usin
122      Here, we employ enzymatic assays, X-ray crystallography, and molecular simulations to resolve th
123  found using cryo-electron microscopy, x-ray crystallography, and other methods.
124 ucture of the hItln-1.KO complex using X-ray crystallography, and our 1.59 angstrom resolution struct
125  pai-dimer) by UV-vis spectroscopy and X-ray crystallography, and performing computational analysis.
126 nology advancements, first in macromolecular crystallography, and recently in Cryo-electron microscop
127  selectively by stopped-flow kinetics, X-ray crystallography, and solution-state NMR.
128 lying a suite of nuclear magnetic resonance, crystallography, and stopped-flow techniques to an enzym
129 tation, we combined virtual screening, x-ray crystallography, and structure-guided design to develop
130 d into an RNA octamer were analysed by X-ray crystallography, and the structure explains the loss in
131 BC-Cullin5 has recently been solved by X-ray crystallography, and, using molecular dynamics simulatio
132                                    NMR-based crystallography approaches involving the combination of
133 at could not be captured by the conventional crystallography approaches used to obtain prior structur
134         Key differences from applications in crystallography are that the errors in Fourier coefficie
135                              Data from X-ray crystallography at 2.85 angstrom, as well as kinetic dat
136 om resolution by serial synchrotron rotation crystallography at a cryogenic temperature, and at 1.8 a
137  using a combination of time-resolved serial crystallography at an X-ray free-electron laser and ns-r
138 the C5_MG4-CirpT complex was solved by X-ray crystallography (at 2.7 angstrom).
139                  Since the advent of protein crystallography, atomic-level macromolecular structures
140                                              Crystallography-based fragment screening reveals a bindi
141                                              Crystallography-based X-ray diffraction technique is the
142                           Combined data from crystallography, biochemistry, small angle X-ray scatter
143 er coefficients are largely in the phases in crystallography but in both phases and amplitudes in cry
144 f metal centers derived from zero dose X-ray crystallography can advance our mechanistic understandin
145 broadly, these findings suggest that racemic crystallography can provide insight on native quaternary
146      Isolated and fully characterized (X-ray crystallography) Co(I)-complexes, (dppp)(3)Co(2)Cl(2) an
147                                Besides X-ray crystallography, complete spectroscopic and electrochemi
148 in assembly strength, revealed through X-ray crystallography, computational analysis, and solution-ph
149                         Here we combine NMR, crystallography, computer simulations, protein engineeri
150                                        X-ray crystallography, cryo-electron microscopy, and hydrogen-
151 termination methods including macromolecular crystallography, cryo-electron microscopy, and integrati
152                                          The crystallography data and theoretical calculations sugges
153 osals, we collected "room temperature" X-ray crystallography data for Pseudomonas putida ketosteroid
154 Intact protein mass spectrometry and protein crystallography demonstrated 8 and 9 as covalent inhibit
155 ectroscopy, reaction product analysis, X-ray crystallography, density functional theory calculations,
156                                        X-ray crystallography depicted the binding mode of phosphonic
157                                   This X-ray crystallography driven study shows that the rim of the i
158 , which previously was not detected by X-ray crystallography due to crystal packing effects.
159           Here, using a combination of X-ray crystallography, electron microscopy, and functional and
160                                  Using X-ray crystallography, electron microscopy, and mass spectrome
161 spectroscopy, global kinetic modeling, X-ray crystallography, electron paramagnetic resonance spectro
162           Experimental evidence (e.g., X-ray crystallography, electron paramagnetic resonance, electr
163 ompounds 1 and 2 were characterized by X-ray crystallography, electronic and NMR spectroscopy, and th
164                                        X-ray crystallography enabled structure-guided design, leading
165                                Through X-ray crystallography, engagement of both the catalytic Zn(2+)
166 2MeOH were confirmed by single crystal X-ray crystallography, EPR spectroscopy, and DFT calculations.
167 lization is the bottleneck in macromolecular crystallography; even when a protein crystallises, cryst
168                                        X-ray crystallography experiments allowed structural assignmen
169 aset in static and time-resolved synchrotron crystallography experiments at RT.
170 he LCP-matrix causes difficulties in protein crystallography experiments in meso, this feature of ERO
171 have been precisely identified through x-ray crystallography experiments.
172 ified sensitively and unambiguously by X-ray crystallography, exploiting the anomalous scattering of
173                           We conducted x-ray crystallography, F-actin binding and bundling assays, an
174 rus-induced gene silencing (VIGS), and X-ray crystallography for structure-guided mutagenesis, to inv
175         Detailed experimental studies (X-ray crystallography, gas sorption, and quartz-crystal microb
176                A long-standing goal of X-ray crystallography has been to combine structural informati
177                                        X-ray crystallography has facilitated the majority of protein
178                                 By combining crystallography, hydrogen-deuterium exchange coupled to
179                                  Using X-ray crystallography, identical conductive MthK structures we
180 nanomolar affinity (JH112) was determined by crystallography in complex with the OX1R and corresponde
181 JMS-053 binding site was identified by X-ray crystallography in human serum albumin at drug site 3, w
182 ption, achieved using a combination of X-ray crystallography, in vitro enzyme assays and site-directe
183 ntinues to be refined with cryo-EM and x-ray crystallography, in vivo conformational changes of the N
184                                        X-ray crystallography indicates that intermolecular pai-pai st
185                                        X-ray crystallography indicates that the amino groups of some
186                        Mix-and-inject serial crystallography is an emerging technique that utilizes X
187 g ligand-protease structures solved by X-ray crystallography led to the identification of 3 and 4.
188 NMR and X-ray absorption spectroscopy, X-ray crystallography, mass spectrometry, chromatography and h
189               In this work, the serial X-ray crystallography method was successfully adopted to probe
190 D trajectories using standard macromolecular crystallography methods.
191 e employed a combination of time-lapse X-ray crystallography, molecular dynamics simulations, and DNA
192                However, by combining kinetic crystallography, molecular dynamics simulations, and Ram
193  of several disciplines including chemistry, crystallography, molecular engineering and advanced mate
194 tpyPY2Me)](0), and characterization by X-ray crystallography, Mossbauer spectroscopy, X-ray absorptio
195  pumila (OpSTR) using a combination of X-ray crystallography, mutational, and molecular dynamics (MD)
196 re not amenable to characterization by x-ray crystallography, NMR or EM.
197 ultiple biophysical methods, including x-ray crystallography, NMR spectroscopy, and small angle x-ray
198          Here, we use a combination of X-ray crystallography, NMR spectroscopy, functional analyses,
199 ngle-particle cryoelectron microscopy, X-ray crystallography, NMR, and other biophysical methods.
200 stay structural biology techniques are X-ray crystallography, nuclear magnetic resonance (NMR) imagin
201                                        X-ray crystallography of 11s and related thieno[3,2-d]pyrimidi
202  Herein, we describe an analysis using X-ray crystallography of a diverse library of compounds prepar
203 al delivery medium in the serial femtosecond crystallography of Adenosine A(2A) receptor (A(2A)R).
204                                  Using X-ray crystallography of four apo- and cofactor-bound Mtb-MenD
205 rom nuclear magnetic resonance, modeling and crystallography of homologous receptors.
206 cture of human EMC using biochemical assays, crystallography of individual subunits, site-specific ph
207 y NMR analysis of free peptides and by X-ray crystallography of peptides in complex with antibody 6E2
208                             Subsequent X-ray crystallography of the A(2A) AR with a low and a high af
209 ly depth-resolved composition and real-space crystallography of the silicide films using a single sam
210                                        X-ray crystallography often requires non-native constructs inv
211                        High-resolution X-ray crystallography on selected derivatives in the adduct wi
212  seen experimentally, for example with x-ray crystallography or cryo-electron microscopy.
213 nal structure-determining techniques such as crystallography or nuclear magnetic resonance spectrosco
214  N terminus insertion and, as shown by X-ray crystallography, partly by Tyr-172 inserting into a cavi
215  mutagenesis, surface plasmon resonance, and crystallography, Philips et al. explore the distinct fea
216 anistic docking, machine learning, and X-ray crystallography, pointing the way for future terpene syn
217 es, such as coherent diffraction imaging and crystallography, provides a nonperturbing environment wh
218 gues using single-particle cryo-EM and x-ray crystallography, respectively.
219                                        X-ray crystallography revealed a slightly twisted geometry for
220 enesis of a Der p 2 epitope defined by x-ray crystallography revealed an IgE Ab binding site that wil
221                                        X-ray crystallography revealed that a potent, reversible, firs
222                                        X-ray crystallography revealed that Aequorea CPs contain a che
223  of the three-dimensional structure by X-ray crystallography revealed that CopG consists of a thiored
224                                        X-ray crystallography revealed the structure of Bs164, the fir
225 phenyl) structural characterization by X-ray crystallography reveals a short Al-N distance, which is
226                                        X-ray crystallography reveals distinctly different positions o
227                                        X-ray crystallography reveals face-to-face alignment of naphth
228                                        X-ray crystallography reveals that 34 occupies the classical q
229                                        X-ray crystallography reveals that peptide N+1 assembles to fo
230                                        X-ray crystallography reveals that these CNT mimics exhibit un
231                                        X-ray crystallography reveals that they bind in the enzyme RNA
232                                  While X-ray crystallography routinely provides structural characteri
233 les, which we further analyzed by ITC, X-ray crystallography, selectivity studies, the NCI60 cell-pan
234  crystals are amenable to serial femtosecond crystallography (SFX) analyses using X-ray free-electron
235                           Serial femtosecond crystallography (SFX) with X-ray free electron lasers (X
236 arly for membrane protein serial femtosecond crystallography (SFX), leveraging orders-of-magnitude fa
237               Using serial femtosecond X-ray crystallography (SFX), we have determined the pristine s
238                         Single crystal X-ray crystallography showed that in some cases, fulvenes poss
239                                        X-ray crystallography showed the inhibitors to bind to a previ
240    2 was structurally characterized by X-ray crystallography, showing a square pyramidal geometry wit
241                                        X-ray crystallography shows that peptide 3(F20Cha) forms a hex
242           While structural analysis by X-ray crystallography shows that the majority of these compoun
243                         Single crystal X-ray crystallography shows that the mononuclear [CuOH](1+) co
244                               Depth-resolved crystallography shows that the Ni films transform from a
245 cture, determined using single-crystal X-ray crystallography, shows that quantum dots (QDs) of [Na(4)
246 nced in the last decade by advances in X-ray crystallography, single-molecular imaging, and theoretic
247 lab has focused on CYP2B enzymes using X-ray crystallography, site-directed mutagenesis, deuterium-ex
248                          Herein we use X-ray crystallography, solution-state NMR, and solid-state NMR
249  the cluster in three oxidation levels using crystallography, spectroscopy, and ab initio calculation
250 -triazine), thus allowing for utilization of crystallography, spectroscopy, and theoretical simulatio
251  and maltosides are frequently used in x-ray crystallography structure determination.
252                          Additionally, x-ray crystallography studies identified key amino acid residu
253                                        X-ray crystallography studies identify subtle changes in the p
254 cells, both hexamers and octamers exist, and crystallography studies predicted the order of the hexam
255 e binding of B2 versus DDM in tubulin, X-ray crystallography studies revealed a shift in the position
256                Our thermostability and X-ray crystallography studies, together with the molecular dyn
257 (mu-NO)](2+) complex with IR, EPR, and X-ray crystallography suggests a localized mixed-valent Cu(III
258                                        X-ray crystallography supports a role for the selectivity base
259                                       Serial crystallography (SX) with X-ray free-electron lasers has
260 t be high enough to couple with conventional crystallography techniques.
261  near-infrared (NIR) spectroscopy, and X-ray crystallography techniques.
262                   We show, by means of X-ray crystallography, that the two target nitrogen atoms-the
263                         As revealed by X-ray crystallography, the highly contorted tetra-anion is sta
264                         In the case of virus crystallography this method does not require freezing of
265 finition of the RAF dimer interface (DIF) by crystallography, this review focuses on the implications
266 e of recombinant BcelPL6 was solved by X-ray crystallography to 1.3 angstrom resolution, revealing a
267 tally solved its apo-structure through X-ray crystallography to a resolution of 2.60 angstrom.
268        This study used high-resolution X-ray crystallography to demonstrate the detailed nature of th
269              Here, we use serial femtosecond crystallography to determine the Cyt1Aa protoxin structu
270  use of LMNG, a mild detergent developed for crystallography to increase membrane protein stability.
271 al time single molecule FRET experiments and crystallography to investigate the open- to closed-state
272                          Here, we used X-ray crystallography to investigate these Dsl1-SNARE interact
273 cal synthesis, biophysical mapping and X-ray crystallography to reveal the binding mode of an antagon
274          Here, we use room-temperature X-ray crystallography to study changes in the conformational e
275 equencing, biolayer interferometry and X-ray crystallography to trace mutation selection pathways whe
276  other antibodies with Pfs25 are analyzed by crystallography to understand structural requirements fo
277 ration (SILCS), and experimentally, by X-ray crystallography, to map potential interaction sites on t
278  Pv-M17 by cryoelectron microscopy and X-ray crystallography together with solution studies revealed
279 oaches, site-directed mutagenesis, and X-ray crystallography uncovered an additional nickel-binding s
280  performed sequential serial raster-scanning crystallography using a microfocused synchrotron beam th
281 nd at 1.8 angstrom by LCP-serial femtosecond crystallography, using an X-ray free-electron laser at 4
282                                        X-ray crystallography validated the dimeric mechanism of inhib
283 n analysis of the selected products by X-ray crystallography was carried out to obtain a better insig
284 lt targets for structural biology when X-ray crystallography was the mainstream approach.
285                                   With X-ray crystallography, we detected an unexpected photochemical
286 optimized (TROSY) NMR spectroscopy and X-ray crystallography, we established that the DcpS substrate
287                                  Using X-ray crystallography, we have discovered a domain-swap homodi
288                                  Using X-ray crystallography, we here show how Drosophila CAL1, an ev
289    By using time-resolved serial femtosecond crystallography, we identified a key oxygen intermediate
290                                  Using x-ray crystallography, we show how a preTCR applies the concav
291                             Here using X-ray crystallography, we show that human HC1 has a structure
292 nts, steady-state enzyme kinetics, and X-ray crystallography, we show that the P167S/D240G double mut
293      Here, using electrophysiology and X-ray crystallography, we show that UBP791 ((2S*,3R*)-1-(7-(2-
294 e investigated by NMR spectroscopy and X-ray crystallography, which revealed the occurrence of a sign
295                  The recent advent of serial crystallography, which spreads the absorbed energy over
296 n the context of recent progress using X-ray crystallography with free-electron lasers on these inter
297                           By combining X-ray crystallography with molecular dynamics simulations, in
298 ectroscopy ((1,2)H HYSCORE, ENDOR) and X-ray crystallography, with corresponding DFT studies, cement
299 istent with expectation from models based on crystallography, x-ray diffraction, and cryo-electron mi
300 fully synthesized and fully studied by X-ray crystallography, X-ray photoelectron spectroscopy, hydro

 
Page Top