ライフサイエンスコーパス: crystallographic analysis

1 ative ease of expression, and amenability to crystallographic analysis.

2 51 enzyme, an observation confirmed by X-ray crystallographic analysis.

3 als of the above proteins suitable for X-ray crystallographic analysis.

4 nd 2D NMR experiments and confirmed by X-ray crystallographic analysis.

5 tion of natural proteins to facilitate X-ray crystallographic analysis.

6 pts an octahedral geometry as shown by X-ray crystallographic analysis.

7 leic acid structure, we undertook a detailed crystallographic analysis.

8 or nuclear magnetic resonance (NMR) or X-ray crystallographic analysis.

9 solute configurations were assigned by X-ray crystallographic analysis.

10 ture of one complex was established by X-ray crystallographic analysis.

11 ranging from 58 nM to 0.8 pM was chosen for crystallographic analysis.

12 e of 7k with p38alpha was confirmed by X-ray crystallographic analysis.

13 The structure of 1 was determined by X-ray crystallographic analysis.

14 to trap acyl-enzyme intermediates for X-ray crystallographic analysis.

15 N,N-dimethylamino biphenyl ligands by X-ray crystallographic analysis.

16 nctions was unambiguously confirmed by X-ray crystallographic analysis.

17 MR and IR spectroscopy, base hydrolysis, and crystallographic analysis.

18 netic and equilibrium binding parameters and crystallographic analysis.

19 istry was unequivocally established by X-ray crystallographic analysis.

20 nterface and confirmed the design with X-ray crystallographic analysis.

21 ss an (aS)-configurated biaryl axis by X-ray crystallographic analysis.

22 is mutant, evidence for which is provided by crystallographic analysis.

23 diastereomer occurred as confirmed by X-ray crystallographic analysis.

24 of miliusate was further confirmed by X-ray crystallographic analysis.

25 lidate the dimer interface proposed by prior crystallographic analysis.

26 es that was unambiguously confirmed by X-ray crystallographic analysis.

27 itions for flash-freezing crystals for X-ray crystallographic analysis.

28 multidomain proteins that are not suited to crystallographic analysis.

29 s been investigated by biochemical and X-ray crystallographic analysis.

30 e efforts, a MutS.ATP.DNA complex has eluded crystallographic analysis.

31 forms a GTP-bound complex stable enough for crystallographic analysis.

32 -azotriazapentalene, which was confirmed via crystallographic analysis.

33 tional significance that extend recent x-ray crystallographic analysis.

34 olution experiments, overcoming the need for crystallographic analysis.

35 ture of the product was elucidated via X-ray crystallographic analysis.

36 -Michael product (30) was confirmed by X-ray crystallographic analysis.

37 rocess was unambiguously determined by X-ray crystallographic analysis.

38 ic transformation and characterized by X-ray crystallographic analysis.

39 or working as NAD isostere as ascertained by crystallographic analysis.

40 tative products have been confirmed by X-ray crystallographic analysis.

41 errin A was unambiguously confirmed by X-ray crystallographic analysis.

42 Turning to crystallographic analysis, a 2.35 A resolution structure

43 X-ray crystallographic analysis allowed the quantification of

44 le quinone anion radicals suitable for X-ray crystallographic analysis allows for the first time thei

45 This same crystallographic analysis also indicates the morphologie

46 This same crystallographic analysis also reveals the identity of t

47 tive demethylation reaction was captured via crystallographic analysis and analyzed via single-crysta

48 a bowl-shaped geometry, as revealed by X-ray crystallographic analysis and density functional theory

49 se complexes could be characterized by X-ray crystallographic analysis and employed as catalysts for

50 X-Ray crystallographic analysis and first principles calculati

51 X-ray crystallographic analysis and solution NMR studies verif

52 However, an early crystallographic analysis and some of the more recent so

53 ge this gap uniquely enabling both nanoscale crystallographic analysis and the low-dose formation of

54 Early leads were discovered through X-ray crystallographic analysis, and a systematic survey of co

55 Using ligand binding assays, crystallographic analysis, and all atom MD simulations,

56 By using NMR spectroscopy, X-ray crystallographic analysis, and density functional theory

57 rized previously both structurally, by x-ray crystallographic analysis, and energetically, by scannin

58 thiones is unambiguously determined by X-ray crystallographic analysis, and this is used to correct e

59 were confirmed through single-crystal X-ray crystallographic analysis, arise from sequential inter/i

60 ient absorption spectroscopy (TA), and X-ray crystallographic analysis, assisted by unrestricted symm

61 erfering device (SQUID), FT Raman, and X-ray crystallographic analysis, assisted by unrestricted symm

62 X-ray crystallographic analysis based on Flack parameters assi

63 e sites of these enzymes are the same within crystallographic analysis, but residues in the second-sp

64 Crystallographic analysis classifies CIP-boxes into two

65 The crystallographic analysis complemented by sensitive sequ

66 We present a comprehensive crystallographic analysis comprising NetrinG1-NGL1 and N

67 EPR spectroscopy and crystallographic analysis confirm a common active-site s

68 Crystallographic analysis confirmed that the compound ta

69 Subsequent crystallographic analysis confirmed the single-crystal-t

70 Crystallographic analysis confirmed the structure of [KC

71 The crystallographic analysis confirms that the small organi

72 The X-ray crystallographic analysis confirms that while CIP and CI

73 Furthermore, crystallographic analysis demonstrated atomic accuracy t

74 Crystallographic analysis demonstrated that the Crwn-THF

75 Crystallographic analysis demonstrates that P-4G2 binds

76 X-ray crystallographic analysis details rearrangements in the

77 re comprehensively characterized by means of crystallographic analysis, determination of pK(a) values

78 As the key structural outcome, the X-ray crystallographic analysis discloses the consequences of

79 inst single-chain Fv antibodies obtained via crystallographic analysis/engineering and against commer

80 tivities, confirmed where necessary by X-ray crystallographic analysis, establish the capability of s

81 insights provide simple and accurate optical crystallographic analysis for liquid-dispersed nanomater

82 onal (2D) NMR methods and confirmed by X-ray crystallographic analysis has an unusual 3H-benzo[d]pyrr

83 In this study, X-ray crystallographic analysis has been used to authenticate

84 on the tertiary assembly of these proteins; crystallographic analysis has revealed that the two cyto

85 An X-ray crystallographic analysis has shown the compound to be a

86 More importantly, the crystallographic analysis illustrated for the first time

87 he use of kinetic isotope effects (KIEs) and crystallographic analysis, in conjunction with structure

88 Analytical ultracentrifugation and crystallographic analysis indicate that the resulting VC

89 Here, this local crystallographic analysis is applied to the in-situ-grow

90 The portion of FANCE defined by our crystallographic analysis is sufficient for interaction

91 The focus of this X-ray crystallographic analysis is the third enzyme in the pat

92 Based on the crystallographic analysis, MS data, and biochemical anal

93 lative configuration was determined by X-ray crystallographic analysis), no particular difference was

94 Crystallographic analysis of 17 different complexes of H

95 ecules within the O(2) channel, we performed crystallographic analysis of 19 Xe laden crystals freeze

96 X-ray crystallographic analysis of 1b indicates the H3CAl(C6F5

97 Crystallographic analysis of 2G12 I19R in complex with M

98 X-ray crystallographic analysis of 3 unveils its ability to se

99 Crystallographic analysis of 35 different peptide sequen

100 backbone NH of Met109 was confirmed by X-ray crystallographic analysis of 3a bound to p38alpha.

101 the intermediates were confirmed by an X-ray crystallographic analysis of 43.

102 Added corroboration was gained from a crystallographic analysis of 8.

103 X-ray crystallographic analysis of 9, 1,4-dimethoxy-2,5-bis(2-

104 X-ray crystallographic analysis of [3H]BF(4) revealed a highly

105 ation assays, surface plasmon resonance, and crystallographic analysis of a 1.5 angstrom structure de

106 ted by 2D NMR methods and confirmed by X-ray crystallographic analysis of a bromo derivative.

107 Crystallographic analysis of a complex between mammalian

108 Using high-resolution X-ray crystallographic analysis of a DNA polymerase that catal

109 Here, we present an X-ray crystallographic analysis of a four-component complex co

110 eta-fold that was not observed in an earlier crystallographic analysis of a less stable version of th

111 Crystallographic analysis of a nearly inactive W149A-sub

112 Crystallographic analysis of a pair of analogous nonpola

113 with affinity similar to that of gp120, and crystallographic analysis of a scaffold bound to b12 rev

114 X-ray crystallographic analysis of a series of halide catenane

115 DD-transpeptidase active site--discovered by crystallographic analysis of a soluble construct of PBP2

116 Based on the crystallographic analysis of a urea-checkpoint kinase 1

117 We report electron and X-ray crystallographic analysis of a variety of specimens asse

118 The recent crystallographic analysis of A2AAR agonists and antagoni

119 Crystallographic analysis of ACs with known inhibitors r

120 By using crystallographic analysis of adaptor-Fis1 complexes, we

121 X-Ray crystallographic analysis of addition product 2 and aldo

122 steric inhibitors, a finding rationalized by crystallographic analysis of allosterically inhibited L-

123 However, crystallographic analysis of an interfacially impaired p

124 d catalytic activity was elucidated by X-ray crystallographic analysis of an isolated Au(iii)-activat

125 Crystallographic analysis of an R343V complex with 1,2-D

126 this specificity with biochemical and X-ray crystallographic analysis of APPBP1-UBA3-NEDD8 complexes

127 Kinetic characterization and crystallographic analysis of BsTrpRS allowed us to probe

128 cture than had been supposed on the basis of crystallographic analysis of canonical tRNAs.

129 However, crystallographic analysis of CBM22-2 complexes shows Trp

130 Spectroscopic analysis in solution and X-ray crystallographic analysis of cocrystals of pyrene and NA

131 Crystallographic analysis of DB884 bound to an AATT site

132 X-ray crystallographic analysis of DB921 bound to -AATT- in d(

133 X-ray crystallographic analysis of DB921 bound to AATT shows t

134 Crystallographic analysis of DdPhyA enables comparisons

135 X-ray crystallographic analysis of derivatives of (+)-anti- an

136 X-ray crystallographic analysis of DHR38 reveals the absence o

137 As this segment was not resolved in previous crystallographic analysis of E1 and LTag hexameric helic

138 Previous crystallographic analysis of Escherichia coli GlpG, an i

139 Crystallographic analysis of Fab alone or in complex wit

140 Our studies represent the first crystallographic analysis of GATA zinc fingers bound to

141 Crystallographic analysis of geranylgeranyl diphosphate

142 Crystallographic analysis of GSHKT10 and GSHKT13 (harbor

143 Together with biochemical and crystallographic analysis of HD deletion mutants, we sho

144 We report crystallographic analysis of hETHE1 in complex with iron

145 Here we report the x-ray crystallographic analysis of human galactose mutarotase

146 X-ray crystallographic analysis of II revealed a rare trans-ch

147 toward this goal by setting the stage for a crystallographic analysis of inactivated Cg10062.

148 nimized insulin receptors (IRs) have enabled crystallographic analysis of insulin-bound "micro-recept

149 NMR and crystallographic analysis of IPSEDeltaNLS, a monomeric I

150 the native sodium and potassium forms, and a crystallographic analysis of it complexed with an O. nov

151 by NMR and MS methods coupled with an X-ray crystallographic analysis of its Fe-complex.

152 uorenyl group in 19b was determined by X-ray crystallographic analysis of its N-oxide derivative (23b

153 Crystallographic analysis of KIAA1718 Jumonji domain in

154 Traditionally, crystallographic analysis of macromolecules has depended

155 Crystallographic analysis of mammalian importin alpha1 i

156 Here, through electron-crystallographic analysis of membrane-embedded proteins,

157 Crystallographic analysis of nearly intact Src kinases i

158 ency to form fibrils were coupled with X-ray crystallographic analysis of nine TTR.ligand complexes.

159 X-ray crystallographic analysis of octafluoro-9,10-bis[(trimet

160 X-ray crystallographic analysis of one of the new inhibitors b

161 Crystallographic analysis of one of these analogues boun

162 X-ray crystallographic analysis of one such inhibitor in compl

163 lysozyme, and has been employed for routine crystallographic analysis of organic and inorganic mater

164 Recent crystallographic analysis of p66/p51 human immunodeficie

165 That is defined by crystallographic analysis of phenylphosphonylated reacti

166 Crystallographic analysis of PR ligand binding domain co

167 Through crystallographic analysis of protein mutants incapable o

168 utilized molecular modeling based upon X-ray crystallographic analysis of renin's active site to desi

169 rminants were established based on the X-ray crystallographic analysis of representative compounds bo

170 An X-ray crystallographic analysis of representative Ph(2)P(E)- a

171 X-ray crystallographic analysis of representative structures r

172 NMR experiments, DFT calculations and X-ray crystallographic analysis of Sc(3)N@C(78) derivative 1a.

173 Computational chemistry and X-ray crystallographic analysis of selected member compounds c

174 Crystallographic analysis of seven anthranilic acid deri

175 X-ray crystallographic analysis of several cis,cis,cis,cis-[4.

176 Crystallographic analysis of several {UO(2)[TAM(HOPO)(2)

177 pplication of LCP techniques to enable X-ray crystallographic analysis of single-pass TM interactions

178 Crystallographic analysis of SynAPSK in complex with eit

179 Through crystallographic analysis of SynCAM 2, we identified wit

180 X-ray crystallographic analysis of the 2.45 A LCAT-27C3 comple

181 critical differences are highlighted in the crystallographic analysis of the A. oryzae structure: (i

182 Crystallographic analysis of the alpha-hydroxy and alpha

183 Crystallographic analysis of the assembly unit reveals a

184 We have addressed these questions through crystallographic analysis of the Atm1/ABCB7/HMT1/ABCB6 o

185 rectly correlate binding interactions with a crystallographic analysis of the binding mechanism.

186 Crystallographic analysis of the bound form of five muta

187 pecificity is achieved, we carried out x-ray crystallographic analysis of the capsid protein domain b

188 Crystallographic analysis of the CC at 2.4 A resolution

189 X-ray crystallographic analysis of the Cdc42-RhoGDI complex su

190 Furthermore, crystallographic analysis of the complex with a modified

191 hesized and the structures assigned by X-ray crystallographic analysis of the corresponding Boc-prote

192 pared and its structure established by X-ray crystallographic analysis of the corresponding Cbz-prote

193 Single-crystal X-ray crystallographic analysis of the dimeric diaminopyridazi

194 Crystallographic analysis of the enzyme in free, acarbos

195 X-ray crystallographic analysis of the ERAP2 392K allele sugge

196 Recent progress in crystallographic analysis of the Escherichia coli rhombo

197 YA/J6 (IgG3, kappa) has been investigated by crystallographic analysis of the Fab domain and its two

198 xylappaconitine from condelphine, with X-ray crystallographic analysis of the former clarifying the N

199 Crystallographic analysis of the free ectodomain has def

200 Crystallographic analysis of the GluR2 LBD core has reve

201 In combination with a crystallographic analysis of the GluRIIB ligand binding

202 Crystallographic analysis of the hNCRD demonstrated a no

203 X-ray crystallographic analysis of the homotrimer showed that

204 Crystallographic analysis of the human neck+CRD complexe

205 We rationalized this effect by crystallographic analysis of the IgG1 Fc F241A mutant, d

206 These findings set the stage for a crystallographic analysis of the inactived enzyme to del

207 Crystallographic analysis of the interaction between bis

208 termination of NOE interactions and an X-ray crystallographic analysis of the latter product.

209 A crystallographic analysis of the LegK7-MOB1A complex rev

210 form and the structure established by X-ray crystallographic analysis of the methyl ester hydrochlor

211 A detailed crystallographic analysis of the mutant structures sugge

212 X-ray crystallographic analysis of the N(3)-thiophenylpropiony

213 Crystallographic analysis of the NHR2-N2B complex reveal

214 A high-resolution crystallographic analysis of the nitrogenase MoFe-protei

215 Crystallographic analysis of the obtained compounds reve

216 t recent advances in the field have been the crystallographic analysis of the oxidase and the use of

217 X-ray crystallographic analysis of the particles without the o

218 Crystallographic analysis of the pSP-D fragment complexe

219 Crystallographic analysis of the Saccharomyces cerevisia

220 An important advance has been the crystallographic analysis of the Sar1-Sec23/24 complex.

221 Crystallographic analysis of the shCD38:8-amino-N9-butyl

222 X-ray crystallographic analysis of the structure of SHP2 in co

223 X-ray crystallographic analysis of the supermacrocyclic struct

224 Crystallographic analysis of the T790M mutant shows how

225 Crystallographic analysis of the Taq MutS.DNA.ABF comple

226 ne of these geometries agrees with the X-ray crystallographic analysis of the thermodynamic conformat

227 ple interactions are integrated, we combined crystallographic analysis of the third and fourth PE pai

228 annot phosphorylate PtdIns(4,5)P2 Therefore, crystallographic analysis of the yeast and plant enzymes

229 Crystallographic analysis of these chromophores reveals

230 An X-ray crystallographic analysis of these complexes suggests th

231 X-ray crystallographic analysis of these compounds demonstrate

232 X-ray crystallographic analysis of these scaffold nucleoporins

233 X-ray crystallographic analysis of this hybrid-type intermedia

234 iew will highlight what we have learned from crystallographic analysis of this important protein fami

235 Crystallographic analysis of this region revealed a pair

236 X-ray crystallographic analysis of three compounds (11a, 11d,

237 heir stereochemistry was elucidated by X-ray crystallographic analysis of tosylate derivatives.

238 The crystallographic analysis of two IDT derivatives yielded

239 tein purification, and high-resolution x-ray crystallographic analysis of tyvelose epimerase from Sal

240 Crystallographic analysis of wild-type ECAO structures,

241 X-ray crystallographic analysis on six [2]rotaxanes and two [3

242 In addition, single-crystal X-ray crystallographic analysis on the most reactive derivativ

243 Because eukaryotic BATs are recalcitrant to crystallographic analysis, our understanding of the mech

244 Crystallographic analysis provided insights into the inh

245 Our crystallographic analysis provides a detailed view into

246 ght (MALDI-TOF) mass spectrometry, and X-ray crystallographic analysis reveal a bimetallic structure

247 with multi-angle laser light scattering and crystallographic analysis reveal that a DNA-binding frag

248 Our crystallographic analysis revealed a monomeric enzyme wh

249 Previously, X-ray crystallographic analysis revealed a network of contacts

250 X-ray crystallographic analysis revealed a planar backbone wit

251 Crystallographic analysis revealed structural changes th

252 tic investigation based on spectroscopic and crystallographic analysis revealed that a putative reduc

253 X-ray crystallographic analysis revealed that Abeta42 binding

254 Crystallographic analysis revealed that HIPP interacts w

255 Crystallographic analysis revealed that pyridine-palladi

256 Crystallographic analysis revealed that SB-590885 stabil

257 Crystallographic analysis revealed that the nicotinamide

258 Crystallographic analysis reveals architectural features

259 X-ray crystallographic analysis reveals interesting conformati

260 X-ray crystallographic analysis reveals that 12 adopts a simil

261 Our crystallographic analysis reveals that PLSCR1 NLS binds

262 Crystallographic analysis reveals that the only signific

263 Crystallographic analysis reveals that the overall struc

264 The crystallographic analysis reveals that the thiolate liga

265 X-ray crystallographic analysis reveals that these type II inh

266 Crystallographic analysis reveals that this specificity

267 Crystallographic analysis reveals the formation of a sta

268 d, proton, and carbon NMR spectra, and X-ray crystallographic analysis reveals the nitroso groups pos

269 X-ray crystallographic analysis reveals the Zr and Hf complexe

270 Molecular dynamics simulations and crystallographic analysis show how distinct hydrogen-bon

271 Crystallographic analysis showed a plane of symmetry tha

272 hylococcus aureus, and biochemical and X-ray crystallographic analysis showed that SpFakB1 selectivel

273 Crystallographic analysis showed that W136A mutation did

274 Crystallographic analysis shows that 3 forms a chiral cl

275 Crystallographic analysis shows that [H1](0) retains the

276 Crystallographic analysis shows that Et4N[H3(BAr(F)3)2]

277 Crystallographic analysis shows that splaying between th

278 Single-crystal X-ray crystallographic analysis shows that the cage contains a

279 Crystallographic analysis shows that the concomitant cen

280 X-ray crystallographic analysis shows that the DPX-26 has a de

281 X-ray crystallographic analysis shows that these sites adopt d

282 X-ray crystallographic analysis successfully determined the st

283 ogy-dependent polymorphism using an in-depth crystallographic analysis that correlates high-resolutio

284 Here, we demonstrate using spectroscopic and crystallographic analysis that human PARP-1 has a third

285 primary adduct and established through X-ray crystallographic analysis that the adduct is the product

286 From X-ray crystallographic analysis, the molecular analogues Lu[CH

287 As shown by crystallographic analysis, the phosphonate moiety is hig

288 the designed protein was confirmed by X-ray crystallographic analysis: The remodeled loop adopts a c

289 and purification, and high resolution x-ray crystallographic analysis to 1.44 A of wild-type DesIV c

290 used multiple solution state techniques and crystallographic analysis to investigate the importance

291 The crystallographic analysis unambiguously elucidated that

292 The crystallographic analysis unexpectedly revealed the bind

293 Our crystallographic analysis unveiled the exact position of

294 Crystallographic analysis using a labeled RNA oligonucle

295 of 1 was established by single-crystal X-ray crystallographic analysis using Cu Kalpha radiation.

296 repare single crystals suitable for accurate crystallographic analysis was missing.

297 talline photochromism phenomena of 10, X-ray crystallographic analysis was performed, revealing a sig

298 As well as full X-ray crystallographic analysis, we studied the reactivity of

299 ctural assignments for 2 and 3 through X-ray crystallographic analysis, which revealed an interesting

300 photolabeling experiments, as well as X-ray crystallographic analysis with a protein prenyltransfera