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1       Mice were challenged for one hour with inhalational 1.5% isoflurane, or intraperitoneal ketamin
2 AS pathway might be considered, for example, inhalational administration of ACEIs/ARBs (to deliver dr
3 phage administration was more effective than inhalational administration, suggesting that circulating
4  a progressive shift to using more expensive inhalational agents and total intravenous anesthesia in
5 rhaps even less effective, than titration of inhalational agents using end tidal anesthetic concentra
6                                    Among the inhalational agents, usage costs of sevoflurane and desf
7   Recording solutions were equilibrated with inhalational anaesthetic vapour delivered from a calibra
8 entobarbital, midazolam, propofol, ketamine, inhalational anaesthetics (isoflurane, desflurane), anti
9 ble individuals on exposure to commonly used inhalational anaesthetics and depolarising muscle relaxa
10                           The effects of the inhalational anaesthetics halothane and isoflurane on th
11 olved in the mechanism of action of general (inhalational) anaesthetics.
12 s encountered in vivo, as well as in vivo in inhalational and cutaneous mouse models of B. anthracis
13  which can help prioritize efforts to reduce inhalational and dermal exposures.
14 s in acute adaptive immune responses between inhalational and dermal infection with F. tularensis LVS
15 me binding site mediates recognition of both inhalational and injectable anesthetics.
16                            The comparison of inhalational and intravenous anaesthesia has been the su
17  would protect cortical neurons against both inhalational and intravenous anesthetic-induced neurotox
18 ns, we find that larval zebrafish respond to inhalational and IV anesthetics at concentrations simila
19                                        At an inhalational and oral dose of 10 mg (-)-Delta(9)-tetrahy
20 sia (TIVA) has better survival outcomes than inhalational anesthesia (INH) in several types of cancer
21           Bispectral index monitoring during inhalational anesthesia adds to the cost without providi
22 thesia offers a physiological advantage over inhalational anesthesia for thoracic surgery remain inco
23  cause temporary amnesia, yet the effects of inhalational anesthesia on human emotional memory proces
24 ed with lower incidence of laryngospasm than inhalational anesthesia.
25 esthetized with a virtually nondefluorinated inhalational anesthetic (desflurane) or with a nonfluori
26 advantages for any of the commonly available inhalational anesthetic agents and each can be used for
27                                              Inhalational anesthetic agents have also been shown to r
28                Xenon and dichloromethane are inhalational anesthetic agents whose binding to myoglobi
29 ative, analgesics, benzodiazepines, opioids, inhalational anesthetic agents, nitrous oxide, ketamine,
30 ous oxide (N2O, laughing gas), a widely used inhalational anesthetic and drug of abuse.
31                                  To identify inhalational anesthetic binding domains in a ligand-gate
32                                 To determine inhalational anesthetic binding domains on a ligand-gate
33  during surgery (derived from mean end-tidal inhalational anesthetic concentrations).
34                                              Inhalational anesthetic dose increase and reduced risk o
35                                         High inhalational anesthetic dose of 1.20 (1.13-1.30) (median
36         We sought to determine the effect of inhalational anesthetic dose on risk of severe postopera
37                           Additionally, high inhalational anesthetic dose was associated with lower 3
38                 Intraoperative use of higher inhalational anesthetic doses is strongly associated wit
39  can be utilized to probe the binding of the inhalational anesthetic halothane to an anesthetic-bindi
40 amuscular sedative was given, followed by an inhalational anesthetic induction and mechanical ventila
41 iments were performed with the commonly used inhalational anesthetic sevoflurane.
42 ectroscopic probe to study the binding of an inhalational anesthetic to a model membrane protein.
43               Clinical concentrations of the inhalational anesthetic, halothane (1 rat MAC, 1.2 vol.%
44             Isoflurane, the most widely used inhalational anesthetic, releases inorganic fluoride dur
45                           We now report that inhalational anesthetics affect gene expression of nitri
46 ersing the effects of some anesthetic drugs (inhalational anesthetics and muscle relaxants) are descr
47          This is a novel interaction between inhalational anesthetics and the NO signaling pathway an
48                                              Inhalational anesthetics are bronchodilators with immuno
49                           They also received inhalational anesthetics because of refractory bronchoco
50                        Postconditioning with inhalational anesthetics can reduce ischemia-reperfusion
51            At surgical depths of anesthesia, inhalational anesthetics cause a loss of motor response
52                     These data indicate that inhalational anesthetics cause activation of RTN neurons
53                Currently, it is thought that inhalational anesthetics cause anesthesia by binding to
54 e that clinically relevant concentrations of inhalational anesthetics dose-dependently and specifical
55          Median effective dose equivalent of inhalational anesthetics during surgery (derived from me
56                                              Inhalational anesthetics have been shown to inhibit the
57                            Increasing use of inhalational anesthetics in the ICU underscores the need
58 sting differences in the binding domains for inhalational anesthetics in the nAChR.
59 sthesia is indicated for procedures in which inhalational anesthetics may not be safely or effectivel
60 w that clinically relevant concentrations of inhalational anesthetics modulate neuronal Ih and the co
61      A better understanding of the effect of inhalational anesthetics on fetal cardiac function and s
62              The potential adverse impact of inhalational anesthetics on the developing brain was hig
63 ulate based on these data that sedation with inhalational anesthetics outside of the operating room m
64                The molecular pharmacology of inhalational anesthetics remains poorly understood.
65  in experimental traumatic brain injury with inhalational anesthetics, these results indicate that th
66 the native RTN current (i.e., suppression by inhalational anesthetics, weak rectification, inhibition
67 ures incompatible with effective delivery of inhalational anesthetics.
68 lar concentration is central to the study of inhalational anesthetics.
69 ose receptors is less certain in the case of inhalational anesthetics.
70 the PDZ domain as a new molecular target for inhalational anesthetics.
71                            Administration of inhalational anesthetics.
72                                Prevention of inhalational anthrax after Bacillus anthracis spore expo
73 ber 19 and October 26, there were 5 cases of inhalational anthrax among postal workers who were emplo
74 py appears to have slowed the progression of inhalational anthrax and has resulted to date in surviva
75 otic prophylaxis required to protect against inhalational anthrax and may impact public health manage
76 osed to prophylaxis, could effectively treat inhalational anthrax and prevent disease caused by the g
77 d cough do not reliably discriminate between inhalational anthrax and viral respiratory tract infecti
78    The cases of 2 postal workers who died of inhalational anthrax are reported here.
79  conduct credible human risk assessments for inhalational anthrax associated with exposure to a low n
80 es are decisive events in the progression of inhalational anthrax because they initiate germination a
81       Also, rabbits that were protected from inhalational anthrax by administration of ETI-204 develo
82 atocrit were more frequently recorded in the inhalational anthrax cases than in either the community-
83                                              Inhalational anthrax caused by Bacillus anthracis is ass
84 of patients who died of bioterrorism-related inhalational anthrax confirmed the route of infection.
85   This study demonstrated that the course of inhalational anthrax disease and the resulting pathology
86 ant importance to reassess the mechanisms of inhalational anthrax dissemination, since it is this for
87                               Mortality from inhalational anthrax during the 2001 U.S. attack was sub
88 g the recent bioterrorism-related outbreaks, inhalational anthrax had a 45% mortality in spite of app
89                                              Inhalational anthrax has characteristic clinical feature
90  had been mailed to a US senator, 5 cases of inhalational anthrax have occurred among postal workers
91 adenopathy led to a presumptive diagnosis of inhalational anthrax in both cases.
92 is capsule and toxins in the pathogenesis of inhalational anthrax in rabbits by comparing infection w
93  of rPA provides complete protection against inhalational anthrax in rabbits.
94  identification of patients with presumptive inhalational anthrax in the setting of a large-scale ant
95 l history, pathophysiology, and pathology of inhalational anthrax in this animal model following nose
96 ed attenuated virulence in a murine model of inhalational anthrax infection.
97 udies aiming to understand events initiating inhalational anthrax infections.
98                          The rabbit model of inhalational anthrax is an important tool in the assessm
99                                              Inhalational anthrax is caused by inhalation of Bacillus
100                                              Inhalational anthrax is caused by the sporulating bacter
101 's high index of suspicion, the diagnosis of inhalational anthrax is difficult during nonspecific pro
102                                              Inhalational anthrax is initiated by the entry of Bacill
103 ed public health responses to an outbreak of inhalational anthrax is the optimum duration of antibiot
104 advances in supportive care, fulminant-phase inhalational anthrax is usually fatal.
105 rax attack, mass screening to identify early inhalational anthrax may improve both the management of
106 istorical data sets from West Nile virus and inhalational anthrax outbreaks.
107 th authorities investigated 11 patients with inhalational anthrax related to a bioterrorism attack in
108 scribe the 11th case of bioterrorism-related inhalational anthrax reported in the United States.
109  has been proposed that the dissemination of inhalational anthrax required spores to be transported f
110                  Postexposure prophylaxis of inhalational anthrax requires prolonged antibiotic thera
111 CT) findings in two patients with documented inhalational anthrax resulting from bioterrorism exposur
112  is developed to analyze the transmission of inhalational anthrax through the postal system by cross-
113 CR and MCR model appeared to describe rabbit inhalational anthrax well.
114  competing risks (CR) computational model of inhalational anthrax where data was collected from NZW r
115 Aerosol challenge of guinea pigs resulted in inhalational anthrax with death occurring between 46 and
116 g was 100% sensitive (95% CI 84.6-100.0) for inhalational anthrax, 71.8% specific (64.8-78.1) compare
117                                              Inhalational anthrax, a disease caused by inhaling Bacil
118 osure to Bacillus anthracis spores initiates inhalational anthrax, a life-threatening infection.
119  of the central stages in the progression of inhalational anthrax, and it is commonly believed that t
120 are likely the first immune cells exposed to inhalational anthrax, and the interferon (IFN) response
121 R/MCR model with other computation models of inhalational anthrax, and using the resulting informatio
122                                       During inhalational anthrax, Bacillus anthracis survives and re
123                       The etiologic agent of inhalational anthrax, Bacillus anthracis, produces virul
124 60 days of antibiotic prophylaxis to prevent inhalational anthrax, but adherence to this regimen was
125  York City hospital employee developed fatal inhalational anthrax, but with an unknown source of anth
126   Bacillus anthracis, the causative agent of inhalational anthrax, enters a host through the pulmonar
127        In contrast to events in experimental inhalational anthrax, spore germination in these cutaneo
128 significantly attenuated in a mouse model of inhalational anthrax, suggesting that the microarray dat
129                          In the treatment of inhalational anthrax, the prolonged course of antibiotic
130      To identify clinical characteristics of inhalational anthrax, we compared 47 historical cases (i
131       Although several factors contribute to inhalational anthrax, we hypothesized that unimpeded inf
132 scription of the early infection dynamics of inhalational anthrax, while its stochastic nature allows
133 teritis; however, some recent isolates cause inhalational anthrax-like diseases and death.
134 icrobial activity, we used a murine model of inhalational anthrax.
135 ival in rabbits and monkeys with symptomatic inhalational anthrax.
136 use aerosol challenge model for the study of inhalational anthrax.
137 one and completely protected animals against inhalational anthrax.
138 urrently no approved effective treatment for inhalational anthrax.
139 tive therapy for prevention and treatment of inhalational anthrax.
140 ts toward identifying clinical predictors of inhalational anthrax.
141 s an endospore-forming bacterium that causes inhalational anthrax.
142                       The cause of death was inhalational anthrax.
143 tes, but tragically some individuals died of inhalational anthrax.
144 as been described as the classic pattern for inhalational anthrax.
145 ) in order to explain dose-response data for inhalational anthrax.
146                 Bacillus anthracis can cause inhalational anthrax.
147  vivo NK cell depletion in a murine model of inhalational anthrax.
148 ignificantly attenuated in a murine model of inhalational anthrax.
149 des unique insight into host defense against inhalational anthrax; these data also support the notion
150                                              Inhalational antibiotics reduce the bacterial burden ass
151                     Both viral infection and inhalational antigen challenge cause M(2)R dysfunction,
152          Airway eosinophils, recovered after inhalational antigen challenge in sensitized mice, expre
153 ent mice, airway eosinophils recovered after inhalational antigen challenge stimulated antigen-specif
154     We examined in vivo whether pre-existing inhalational antigen tolerance could be overcome by acti
155                                              Inhalational antigen tolerance typically protects agains
156 ice with lethal disseminated candidiasis and inhalational aspergillosis.
157 nge, the lungs of C57BL/6 mice (resistant to inhalational B. anthracis infection) had significantly h
158                                       Murine inhalational B. anthracis infections have two portals of
159 for the high mortality rates associated with inhalational Bacillus anthracis infection.
160 s applied to serum from rhesus macaques with inhalational botulism following exposure to BoNT/B, show
161 erize the rhesus macaque (RM) as a model for inhalational brucellosis in support of the U.S. Food and
162 ort the use of the RM as an animal model for inhalational brucellosis to evaluate the efficacy of nov
163 clinical presentation and pathophysiology of inhalational brucellosis, Balb/c mice were challenged wi
164 l for the evaluation of therapeutics against inhalational brucellosis.
165 induce a humoral immune response to a single inhalational challenge to HDM.
166                                    Capsaicin inhalational challenge was performed, and cough response
167  complete or nearly complete protection from inhalational challenge with 100% lethal doses of B. mall
168 and Hcp1, 100% of the mice survived a lethal inhalational challenge with B. pseudomallei Remarkably,
169  resulted in enhanced levels of IL-17A after inhalational challenge with HDM.
170                                              Inhalational challenges to histamine and methacholine (M
171 can be used to quantitate levels of skin and inhalational contact with simulant pathogen particles.
172 second only to carbon monoxide as a cause of inhalational deaths.
173  of inhaled antifungal drugs and combination inhalational devices, limitations of existing nonclinica
174 nited States in 2001 resulted in 11 cases of inhalational disease, with an attendant mortality rate o
175                Substance use, and especially inhalational drug use, increases the likelihood of both
176                                Patients with inhalational dyspnea attributed to ILO were included.
177 n contamination (via swabbing) and potential inhalational exposure (via breathing zone air sampler).
178 terium and Selenomonas, indicating that this inhalational exposure can alter the composition of the s
179 y of the human health risk assessment due to inhalational exposure to 1,3-butadiene (BD) and styrene
180 o were referred for evaluation, a history of inhalational exposure to a 2003 sulfur-mine fire in Iraq
181 indicates that adverse health effects due to inhalational exposure to BD and ST for workers in the ma
182                                    Following inhalational exposure to Francisella tularensis SCHU S4,
183 developed a model of airway inflammation and inhalational exposure to investigate regulatory pathways
184 a in female Fischer 344 rats after nose-only inhalational exposure to lethal doses of aerosolized Fra
185                                   Continuous inhalational exposure to OVA (6 or 11 weeks) resulted in
186                                Discontinuous inhalational exposure to OVA (6 weeks) produced airway i
187                                   In humans, inhalational exposure to particulate air pollutants decr
188 , while the air sampler quantified potential inhalational exposure to PSLs during doffing.
189 o products, including waterpipes, are due to inhalational exposure to toxicants either present in tob
190 hiolitis, which was possibly associated with inhalational exposure, in 38 soldiers.
191 e cause such as collagen vascular disease or inhalational exposure.
192 ysis showed significant associations between inhalational exposures (cigarette smoking, waterpipe smo
193                       However, the impact of inhalational exposures (eg, vapor, dust, gas, fumes), wh
194      These results suggest that occupational inhalational exposures are independently associated with
195  soldiers from Fort Campbell, Kentucky, with inhalational exposures during service in Iraq and Afghan
196            Toxicity classically results from inhalational exposures in individuals who work in indust
197 These findings suggest that certain military inhalational exposures may contribute to the development
198         Our findings emphasize the impact of inhalational exposures on gastrointestinal disease risk,
199 atients with lung disease from other ongoing inhalational exposures, including avian antigens in chro
200 ts should be alert to avoid excessively high inhalational flow.
201                                          The inhalational form of anthrax is the most severe and is a
202  of IL-17A and IFN-gamma in the lungs during inhalational Francisella infection and that these cytoki
203       We hypothesized that nitrous oxide, an inhalational general anesthetic and N-methyl-D-aspartate
204 We have previously shown that recognition of inhalational general anesthetics by the model protein ap
205                                              Inhalational general anesthetics have recently been show
206 + channels strongly suggest that halogenated inhalational general anesthetics interact with gates and
207 coccus neoformans H99 infection by comparing inhalational H99 infections in wild-type BALB/c and IL-4
208                         Rationale: Workplace inhalational hazards remain common worldwide, even thoug
209 phics of research studies with intranasal or inhalational ICS.
210 olam formulated in flavoured syrups, and the inhalational induction of anaesthesia may be accomplishe
211 on has become the most widely cited model of inhalational infection as well as the focus of the major
212 that bacterial dissemination patterns during inhalational infection may be more similar to the cutane
213  compared in both the murine intravenous and inhalational infection models, there were significant di
214 es an attractive strategy to protect against inhalational infection with virulent B. melitensis.
215   Using a clinically relevant mouse model of inhalational infection with virulent C. neoformans H99,
216 oning, fire-related toxic gas exposures, and inhalational injuries.
217                    In a sulfur dioxide (SO2) inhalational injury model, bromodeoxyuridine (BrdU) inco
218                                        While inhalational injury to the airway epithelium is suspecte
219  but it may not have a role in patients with inhalational injury.
220 ly an adult disease occurring after years of inhalational insults to the lungs, pinpointing abnormali
221 f-renew and critical to the health impact of inhalational insults.
222 ly used volatile anesthetic, and is used for inhalational long-term sedation in critically ill patien
223                                     The term inhalational lung disease comprises a group of entities
224                                              Inhalational lung diseases are classified as occupationa
225  results define early events occurring in an inhalational macaque monkeypox infection model, supporti
226 rranted to confirm the effectiveness of this inhalational method.
227 t than the control strains in both the mouse inhalational model and the rabbit meningitis model.
228  conducted in the African green monkey (AGM) inhalational model of pneumonic plague to test the effic
229 e and the reconstituted strain in the murine inhalational model, and it also had significantly impair
230                                      In this inhalational model, toxins have disseminated rapidly in
231 measured by cumulative survival in the mouse inhalational model.
232 measured by cumulative survival in the mouse inhalational model.
233         Here, the early pathogenic events of inhalational monkeypox infection in NHPs were characteri
234                                              Inhalational MtbDeltasigH, a stress-response-attenuated
235 ing peak nasal inspiratory flow and absolute inhalational nasal partitioning ratio) improved more in
236  acute respiratory distress syndrome (ARDS), inhalational NO has proved to be useful.
237  whatever the route of infection (cutaneous, inhalational, or digestive).
238                                              Inhalational plague in the cynomolgus macaque inoculated
239                   All control animals in the inhalational plague studies succumbed to plague and were
240 ls, are >=90% effective for the treatment of inhalational plague when administered within 2-6 hours o
241                                              Inhalational pneumonic tularemia, caused by Francisella
242 (NASBA) method was investigated by use of an inhalational rat model of IPA.
243 a civilian or military population through an inhalational route of exposure and aerosol is considered
244  administration of drugs to the lung via the inhalational route provides for high concentrations at t
245 GA) during surgery is commonly maintained by inhalational sevoflurane.
246             Asthma lightened by treatment of inhalational steroids.
247            Comparing disease manifestations, inhalational survivors reported significantly lower over
248                                Hence, adding inhalational to oral therapy can potentially accelerate
249 solution of AAD and the development of local inhalational tolerance (LIT).
250 ent resolution with the development of local inhalational tolerance (LIT).
251 appaB activation orchestrate the breaking of inhalational tolerance and allergic antigen sensitizatio
252                                              Inhalational tolerance induced by continuous OVA exposur
253 aled OVA on Day 30 in an attempt to overcome inhalational tolerance.
254  therefore, reveals novel mechanisms for the inhalational toxicity of vaping.
255 bitor, showed favorable pharmacokinetics for inhalational treatment and intranasal insufflation deliv
256       Migraine-like pain was also induced by inhalational umbellulone, a TRPA1 agonist, in animals pr
257 subthreshold (i.e. second-hit) stimulus from inhalational umbellulone, a TRPA1 agonist.
258 es developed periorbital allodynia following inhalational umbellulone.
259 ment strategies augment the response to this inhalational vasodilator.
260         MH is a severe reaction triggered by inhalational volatile anesthetics and succinylcholine in
261 s: Together, these findings demonstrate that inhalational wood smoke exposure can modify several low-
262 at a delayed HMBPP/IL-2 administration after inhalational Yersinia pestis infection induced marked ex

 
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