ライフサイエンスコーパス: animal experiment

1 rformance of the system is illustrated by an animal experiment.

2 most up-to-date studies using these tools in animal experiments.

3 solvents and were shown to be embryotoxic in animal experiments.

4 arcinoma (HCC) are difficult to reproduce in animal experiments.

5 naling has been extensively characterized in animal experiments.

6 ielded significant functional improvement in animal experiments.

7 monstrated importance in retinal function in animal experiments.

8 s using deuterated water in cell culture and animal experiments.

9 The local animal care committee approved all animal experiments.

10 ategies for enhancing the reproducibility of animal experiments.

11 legic agents have mainly remained limited to animal experiments.

12 ntricular free wall pacing found in previous animal experiments.

13 itutional animal care committee approved all animal experiments.

14 g the angiogenic cascade by cell culture and animal experiments.

15 r mobilization of stem cells to the heart in animal experiments.

16 inhibitors of cholesterol cholelithiasis in animal experiments.

17 balloon models and in vivo and ex vivo small animal experiments.

18 molecules have produced promising results in animal experiments.

19 e defined a 'vestibulosympathetic reflex' in animal experiments.

20 ses which were similar to those found in the animal experiments.

21 human subjects are consistent with those of animal experiments.

22 -factors that are poorly modelled in current animal experiments.

23 ypokalaemia in several genetic disorders and animal experiments.

24 to metabolic disease in case studies and in animal experiments.

25 and the barriers to implementing masking in animal experiments.

26 step toward regulatory acceptance to replace animal experiments.

27 These results were also verified by animal experiments.

28 ation screening, while reducing the need for animal experiments.

29 ovascular regulation is primarily limited to animal experiments.

30 xicology models in replacement strategies of animal experiments.

31 approved by the French Ethics Committee for Animal Experiments.

32 t powerful cardioprotective interventions in animal experiments.

33 Governmental approval was obtained for animal experiments.

34 , they lack the rigor inherent in controlled animal experiments.

35 by a combined rate of 68% in two independent animal experiments.

36 e approved by the local ethics committee for animal experiments.

37 ern formation have been restricted mainly to animal experiments.

38 so displayed suitable PK profile for in vivo animal experiments.

39 periments were sequentially performed on all animals: Experiment 1--The Light and Platform test measu

40 elopment (experiment 1), as well as in adult animals (experiment 2).

41 camer duplex [d(GCGTA)-T*-d(ACGC)](2.) In an animal experiment, a 16-mer F-CeNA gapmer ASO showed sim

42 In animal experiments, administration of 16,16-dimethyl PGE

43 ft-versus-leukemia effect was predicted from animal experiments almost 40 years ago, only recently ha

44 Animal experiments also reveal that the aging process it

45 ions, cessation, dose-response relationship, animal experiments, analogy, specificity, and consistenc

46 The study included animal experiments and a retrospective analysis of ortho

47 in eliminating the translational gap between animal experiments and clinical outcomes in humans.

48 Growing evidence from animal experiments and clinical studies has demonstrated

49 transorbital, and transpalpebral ES in both animal experiments and clinical studies.

50 Animal experiments and clinical trials in adult patients

51 nucleotides (ASOs) in T(m), cell culture and animal experiments and compare them to their gap-matched

52 Animal experiments and epidemiological studies have sugg

53 Animal experiments and functional imaging studies have p

54 This cohort study supports findings from animal experiments and human observational studies in se

55 ognized phenomenon and has been described in animal experiments and human pathology.

56 Animal experiments and human studies provide compelling

57 enesis has been demonstrated in both in vivo animal experiments and in vitro cell culture experiments

58 t to produce the sharp filtering observed in animal experiments and many computational models that us

59 Animal experiments and mechanistic studies will further

60 hored in a cogent synthesis of findings from animal experiments and observational studies on diverse

61 ties in translation of cardioprotection from animal experiments and proof-of-concept trials to clinic

62 carefully considering the oral dose used in animal experiments and provides useful information in se

63 ential for ethical and scientific reasons in animal experiments and should completely cover the perio

64 he methodology can improve the efficiency of animal experiments and shows great potential for applica

65 Animal experiments and small clinical studies support a

66 f electrophysiological knowledge acquired in animal experiments and that currently being obtained in

67 d 4.6 g, making it suitable for future small animal experiments (and ultimately, potential evaluation

68 nciple of "Refining, Reducing and Replacing" animal experiments, and across the globe, different init

69 article reviews the basic science evidence, animal experiments, and human clinical data supporting t

70 of research, including organs-on-chip, small animal experiments, and neonatology.

71 either of the 2 approaches has fared well in animal experiments, and the only clinical experience wit

72 n is intriguing, accords with the results of animal experiments, and warrants further investigation.

73 on the basis of promising tissue culture and animal experiments, and yet they have failed to stop res

74 Calls to halt all animal experiments appear premature, as insufficient non

75 cannot be conducted in humans, results from animal experiments are extrapolated to humans.

76 Animal experiments are often used to determine effects o

77 and reporting from human investigations and animal experiments are urgently needed.

78 A similar effect was observed in animal experiments as cisplatin treatment increased Notc

79 s a multitude of in vitro assays and in vivo animal experiments before a compound is moved into first

80 In animal experiments, blinding (also known as masking) is

81 Animal work was approved by the Animal Experiment Board of Finland.

82 ies are cited, the latter including not only animal experiments but also clinical trials.

83 ects of alcohol on the brain is supported by animal experiments, but how in vivo CB1R levels are alte

84 ial genetics, transcriptomics, metabolomics, animal experiments, chemical inhibition, and rescue stud

85 Animal experiments clearly show that prone positioning d

86 results in strongly attenuated virulence in animal experiments, comparable in degree to classical li

87 Animal experiments confirm the above and also indicate t

88 In animal experiments, control and streptozotocin-induced d

89 We also review studies on animal experiments dealing with pathophysiological aspec

90 Animal experiments demonstrate that pre-exposure to sand

91 Animal experiments demonstrate that the abscess-inducing

92 Results from animal experiments demonstrate that the radioligand [11C

93 Animal experiments demonstrated that existing antibodies

94 We will use data from an animal experiment designed to investigate the effect of

95 -mer cEt ASO showed the best activity in the animal experiments despite significantly lower T(m) and

96 Recent animal experiments detected reactive changes in (18)F-FE

97 In animal experiments, direct infusion of visfatin in mice

98 In animal experiments, dopamine D2-like receptor stimulatio

99 imited to electrophysiological findings from animal experiments extrapolated to humans, mathematical

100 Using the exact temporal delays from the animal experiments, fast recruitment of gain co-modulati

101 In animal experiments, FHNA-modified antisense oligonucleot

102 Important laboratory and animal experiments focused on predictive models for huma

103 Animal experiments further showed that Nef facilitates v

104 In the animal experiments, gastric intramucosal PCO2 and pH wer

105 We review available evidence from animal experiments, genotoxicity studies and clinico-epi

106 Animal experiments had institutional animal care and use

107 Animal experiments have demonstrated that E6 and E7 toge

108 Animal experiments have demonstrated that energy intake

109 Animal experiments have evaluated the effects of leptin

110 However, animal experiments have found considerable variability i

111 ant human erythropoietin (rHuEPO) protein in animal experiments have not been consistently reproduced

112 53 and pRB: The observations from laboratory animal experiments have provided a rationale for examini

113 om human intervention studies and a range of animal experiments have questioned this concept.

114 Results from animal experiments have shown that human IgG2/mouse chim

115 Previous animal experiments have shown that serotonin is involved

116 Although in vitro and animal experiments have supported an inverse association

117 To this end, we replicated the same animal experiment in 3 independent laboratories, each em

118 onfocal microscopy in vitro and confirmatory animal experiment in vivo.

119 redictive model to reduce the high number of animal experiments in early stage development.

120 ensitized workers spent more time performing animal experiments in the animal facility (p = 0.0001) a

121 re expected to be promising alternatives for animal experiments in the future.

122 f patients with basal ganglia disease and in animal experiments in the skeletal motor system, the res

123 prompt treatment could be demonstrated with animal experiments in vivo, in which brain damages were

124 We conducted an independent set of animal experiments in which two different and well chara

125 In animal experiments, in utero exposure to DDE decreases a

126 Cell and animal experiments indicate tau functions as a prion, as

127 epidemiological studies, clinical trials and animal experiments indicate that NSAIDs are among the mo

128 Animal experiments indicate that the kidney may play an

129 pidemiological studies, clinical trials, and animal experiments indicates that inhibitors of prostagl

130 ccording to a license obtained by the Danish Animal Experiments Inspectorate, Ministry of Food, Agric

131 fect of zinc intake on vitamin A status from animal experiments is inconclusive, mainly because of th

132 bution of innovative models that may replace animal experiments is limited.

133 An important source of variation in animal experiments is the microbiome, but little is know

134 On the basis of the results of this initial animal experiment, it appears that dynamic 4D four-dimen

135 In animal experiments knocking in a glutamic acid (S1530E)

136 In animal experiments: lipopolysaccharides have been furthe

137 In animal experiments, local and remote ischemic pre- and p

138 ly documented in vivo, and cell cultures and animal experiments may not provide accurate models.

139 n of classical microbiology, sequencing, and animal experiments may provide further insights into how

140 In animal experiments, methylene-cLNA antisense oligonucleo

141 ), in vitro susceptibility studies (n = 14), animal experiments (n = 6, including 5 using the neutrop

142 t theories of mechanisms are mainly based on animal experiments, not on human level.

143 Human neuroimaging studies and complementary animal experiments now identify the gross elements of th

144 od pressure comes from a variety of sources: animal experiments, observational epidemiologic studies,

145 Following favorable results obtained in animal experiments, observational studies have shown ben

146 Animal experiments often use reductionist approaches and

147 The translation from numerous successful animal experiments on cardioprotection beyond that by re

148 ng effects of anesthetic agents used in most animal experiments on functional connectivity.

149 Animal experiments on Langendorff-perfused rabbit hearts

150 The new model is able to fit the animal experiments on lymphocyte recirculation.

151 In this review, we provide an overview of animal experiments on renal IRI and IPoC, demonstrating

152 las weighing 500 g were used for 2 series of animal experiments: one to obtain specimens for scanning

153 ed during the day-most findings are based on animal experiments or human studies with observational d

154 irus (RSV) infection have been obtained from animal experiments or in vitro models.

155 le branch block (LBBB) criteria are based on animal experiments or mathematical models of cardiac tis

156 Therefore, in line with previous animal experiments, our results show that low-serotonin

157 were also supported, for the first time, by animal experiments, p65 cDNA transfection and p65 small

158 interventions, randomized controlled trials, animal experiments, physiologic investigations, evolutio

159 In animal experiments, probiotics were found to improve tes

160 In animal experiments, rabbits in sham-treated groups usual

161 Animal experiments revealed that overexpression of p.104

162 In animal experiments, sepsis without any treatment (Group

163 Animal experiments should better parallel clinical studi

164 In contrast, results from animal experiments show a range of responses with the 12

165 Animal experiments show GPgV lymphotropism and promote g

166 Animal experiments show that lymphocytes activated in th

167 Dramatic results from recent animal experiments show that noise exposure can cause a

168 Finally, an animal experiment showed the effective protection of gra

169 Animal experiments showed a role of the hippocampus for

170 Early animal experiments showed that a cholesterol-rich diet c

171 Because animal experiments showed that high efficiency of intest

172 However, animal experiments showed that the reassortant Sw/Korea/

173 Our previous animal experiments showed that transplantation of isolat

174 emic penumbra was formulated on the basis of animal experiments showing functional impairment and ele

175 The clinical trials are fueled by decades of animal experiments showing that dietary restriction dela

176 This is consistent with the results of animal experiments showing that nitric oxide exerts a fa

177 During the entire animal experiment, statistically fewer ulcers occurred i

178 chanisms of HE deduced from cell culture and animal experiments, such as oxidative stress, altered Zn

179 ological studies, biomarker measurements and animal experiments suggest a role for aberrant immune pr

180 cologic analyses, case-case comparisons, and animal experiments suggest positive associations between

181 Animal experiments suggest that alterations in central p

182 In addition, findings from animal experiments suggest that CHIP is causally involve

183 Animal experiments suggest that circulating palmitoleic

184 Animal experiments suggest that hyperchloremia resulting

185 Transgenic animal experiments suggest that increased expression of

186 ally similar exotoxins, toxin A and toxin B, animal experiments suggest that only toxin A mediates di

187 Recent in vitro and animal experiments suggest that peroxisome proliferation

188 Animal experiments suggest that prolonging the duration

189 Data from in vitro and animal experiments suggest that there are biochemical in

190 Network modeling and animal experiments suggest that these genetic difference

191 Data from animal experiments suggest that treatment of non-convuls

192 Human and animal experiments suggest the involvement of MORs in hu

193 Additionally, results from an animal experiment suggested that being affected with gum

194 Decades-old animal experiments suggested that dietary long-chain mon

195 patients, and evidence from cell culture and animal experiments suggests the nucleus as a site of pat

196 Preclinical animal experiments support the use of an antisense oligo

197 ter utilize published evidence obtained from animal experiments, systematic reviews of preclinical st

198 , and BIOSIS databases were searched for all animal experiments testing tumor volume response to sora

199 These data demonstrated in a pilot large animal experiment that the BAK with RAD altered plasma c

200 It is evident from animal experiments that the percentage of energy derived

201 clinical evidence, as well as evidence from animal experiments, that Mycobacterium tuberculosis can

202 In the animal experiment, the size of the ocular melanoma and t

203 In animal experiments, the mediators evoke anti-inflammator

204 mall sample size conditions typical of large animal experiments, the MLFRA achieved an average AUROC,

205 In the animal experiments, the puncture was successful in all 1

206 Based on the results of animal experiments, the stimulation of its medial part w

207 ients are similar to those observed in these animal experiments, then the efficacy of systemic treatm

208 By analogy with animal experiments, these regions are likely to have had

209 Animal experiments to assess their chronic toxicological

210 biases on published estimates of efficacy in animal experiments to be described.

211 f cardiovascular disease, ranging from early animal experiments to current sophisticated models of he

212 nk accession number AF297868) can be used in animal experiments to define the factors that are import

213 cies differences make the extrapolation from animal experiments to human clinical settings difficult.

214 here is an ongoing debate about the value of animal experiments to inform medical practice, yet there

215 f the virus life cycle crucial for designing animal experiments to model HCV infection.

216 n addition, leucine has been demonstrated in animal experiments to modulate eating and energy homeost

217 The animal experiment trial was done with our feed supplemen

218 These results provide a basis for future animal experiments using more ecologically relevant cond

219 The animal experiment was conducted according to a license o

220 Therefore, an animal experiment was designed to simulate the transfer

221 The protocol for animal experiments was approved by the institutional ani

222 Consistent with in vitro findings, in whole-animal experiments we found that persistent elevation of

223 In whole animal experiments, we demonstrated that long-term feedi

224 In animal experiments, we have shown that metformin can be

225 In animal experiments, we observed significantly lower pH a

226 Using in vitro, cell and animal experiments, we show here that SerRS intervenes b

227 using known infection status samples, or any animal experiments were all excluded.

228 All animal experiments were approved by an Institutional Ani

229 MATERIALS AND All animal experiments were approved by an institutional ani

230 stem cell research oversight committee, and animal experiments were approved by the administrative p

231 Materials and Methods All animal experiments were approved by the animal care and

232 Animal experiments were approved by the animal care comm

233 Animal experiments were approved by the governmental rev

234 Animal experiments were approved by the institutional an

235 The animal experiments were approved by the institutional an

236 MATERIALS AND All animal experiments were approved by the institutional an

237 Materials and Methods Animal experiments were approved by the institutional an

238 All animal experiments were approved by the institutional an

239 All animal experiments were approved by the institutional an

240 Animal experiments were approved by the Johns Hopkins Un

241 Materials and Methods The animal experiments were approved by the local ethics com

242 All animal experiments were approved by the local ethics com

243 Animal experiments were approved by the Stanford Univers

244 ated YAP pathway on the pathogenesis of DCM, animal experiments were divided into 3 parts, including

245 Materials and Methods Animal experiments were performed according to a protoco

246 Animal experiments were performed according to an approv

247 Materials and Methods Animal experiments were performed according to an approv

248 All animal experiments were performed according to protocols

249 All other animal experiments were performed in animals sedated wit

250 All animal experiments were performed in compliance with ins

251 Animal experiments were performed on normal Wistar rats

252 All animal experiments were performed with adherence to the

253 Animal experiments were performed with institutional Ani

254 Animal experiments were performed with institutional ani

255 Two phases of animal experiments were performed.

256 Twenty animal experiments were performed.

257 st all of the laboratory studies and all the animal experiments were restricted to the case of statio

258 y reflect the integrated response of a whole animal, experiments were conducted in two human cell lin

259 These observations were recapitulated in the animal experiments where the 20-mer tcDNA ASO formulated

260 n cannot be taken for granted, especially in animal experiments where we cannot deliver explicit inst

261 d time was found to be unnecessary for small-animal experiments, whereas propagation delay and disper

262 chers encounter when designing and analysing animal experiments will improve the reliability of in vi

263 with an amount of training commensurate with animal experiments, without relying on parameter fine-tu