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1 PPA at 2 mM decreased neurite outgrowth to (80.70 um +/-
2 PPA imprinted polymers bound PPA with an equilibrium con
3 PPA provides a novel perspective that uniquely addresses
4 PPA was 92.8%, 84.9%, 93.0%, 100%, and 95.6%, for norovi
7 ligand as a photosensitizer and Co(dmgH)(2) (PPA)Cl (PPA-Co, dmgH=dimethylglyoxime; PPA=4-pyridinepro
10 5% confidence interval [CI], 75.3 to 90.6%), PPA was 68.0% (95% CI, 53.3 to 80.5%), and the kappa coe
13 This paper summarizes the steps to conduct a PPA and serves as the basis for understanding country ca
16 CR reference method threshold cutoff, were a PPA of 62.1% (72 of 116 results; 95% CI, 52.6%-70.9%) an
19 amyloid burden was compared between Abeta(+) PPA and an Abeta(+) amnestic dementia groups (n = 22).
20 cluded 7-day point prevalence of abstinence (PPA) and level of readiness to quit at each follow-up.
21 mono- or dianions of phenyl phosphonic acid (PPA), phenyl sulfonic acid (PSA), and benzoic acid (BA)
24 graphene/graphite) in a polyphosphoric acid (PPA)/phosphorous pentoxide (P2 O5 ) medium are elucidate
25 e investigated the effect of Propionic acid (PPA), a short-chain fatty acid (SCFA) and a product of d
26 aging (DTI) metrics to assess changes across PPA variants and perform brain-behavioral correlations.
27 an autopsy-confirmed diagnosis of either AD (PPA-AD) or a tau variant of FTLD (PPA-FTLD) and 6 patien
29 itive and negative percentages of agreement (PPA and NPA, respectively) between CPO detect and the RM
30 nstrated a positive percentage of agreement (PPA) between 60 and 100% for four targets (blaKPC, blaND
31 d a positive and negative percent agreement (PPA and NPA, respectively) between the Aries and Xpert a
32 all positive and negative percent agreement (PPA and NPA, respectively) of the cobas Cdiff assay comp
33 ence method, the positive percent agreement (PPA) (95% confidence interval [CI]), negative percent ag
35 a combined 96.2% positive percent agreement (PPA) and 98.1% negative percent agreement (NPA) for the
37 ays, the overall positive percent agreement (PPA) and negative percent agreement (NPA) for B. pertuss
39 occus pyogenes), positive percent agreement (PPA) and negative percent agreement (NPA) ranged from 93
40 ture or EIA, the positive percent agreement (PPA) and negative percent agreement (NPA) values for the
41 rus assay showed positive percent agreement (PPA) and negative percent agreement (NPA) values of 98.3
43 aluated included positive percent agreement (PPA) and negative percent agreement (NPA) with the ARUP
44 aluated included positive percent agreement (PPA) and negative percent agreement (NPA) with the FilmA
45 udy, the overall positive percent agreement (PPA) and the overall negative percent agreement (NPA) of
46 also had highest positive percent agreement (PPA) compared to our reference standard (98.3%) followed
47 ire assays had a positive percent agreement (PPA) of 98.7%, followed by the Aptima assay at 94.7%, co
48 al cultures, the positive percent agreement (PPA) of the BC-GN assay with the reference method was as
49 rcent agreement, positive percent agreement (PPA), negative percent agreement (NPA), and Cohen's kapp
50 ve, negative, and overall percent agreement (PPA, NPA, and OPA, respectively) were the primary outcom
51 emonstrated a positive percentage agreement (PPA) of 91.1% (195 of 214 results; 95% confidence interv
52 Positive and negative percent agreements (PPA and NPA, respectively) between the assays were calcu
53 and self-rectal positive percent agreements (PPA) for NG detection were 92.8% and 97.6%; clinician-re
55 ing for renewable power purchase agreements (PPAs), displaced generation and capacity costs, and net
56 tanding cleft sentence structures, while all PPA variants and patients with bvFTD were impaired with
57 cterization of prephenate aminotransferases (PPA-ATs) that belong to class-Ib aspartate aminotransfer
59 K PEGylated-Pancreatic Polypeptide analogue (PPA) and 20K PEGylated-glucagon, we elucidated the decom
60 ional and regional patient pathway analyses (PPAs) were undertaken using existing national survey and
69 ncremental utility at low DB levels (CBS and PPA) and were associated with overlapping and distinct n
70 odalities were useful in identifying CBS and PPA, whereas DB alone was useful for identifying bvFTD.
72 n time whereas maximum inhibition of HSA and PPA by EC was reached only after 45 to 60 min of incubat
73 EGCG reached maximum inhibition of HSA and PPA with short incubation time whereas maximum inhibitio
79 tia syndrome of primary progressive aphasia (PPA) can be caused by 1 of several neuropathologic entit
84 f patients with primary progressive aphasia (PPA) variants defined by current diagnostic classificati
85 tic variants of primary progressive aphasia (PPA), progressive supranuclear palsy and corticobasal sy
89 rodegeneration (primary progressive aphasia, PPA) have overlapping symptomatology, nomenclature and a
91 al connection to parahippocampal place area (PPA) compared with adjacent regions (e.g., fusiform face
92 argued that the parahippocampal place area (PPA) represents such navigationally relevant information
93 For example, the parahippocampal place area (PPA) responds maximally to environmental scenes during f
94 we show that the parahippocampal place area (PPA), a region in human occipitotemporal cortex, exhibit
96 eriorly from the parahippocampal place area (PPA), retrosplenial complex (RSC) and occipital place ar
97 patterns in the parahippocampal place area (PPA), retrosplenial complex (RSC), and occipital place a
98 processing: the parahippocampal place area (PPA), the retrosplenial complex (RSC), and a region arou
99 responses in the parahippocampal place area (PPA), transverse occipital sulcus, and retrosplenial cor
100 stimuli, and the parahippocampal place area (PPA), which showed better texture than layout decoding.
106 This area (the parahippocampal place area [PPA]) was initially interpreted as responding selectivel
107 rtical area (the parahippocampal place area; PPA) showed distinctively higher functional magnetic res
108 Artery [SFA] and Proximal Popliteal Artery [PPA] [INPACT SFA II], NCT01566461; MDT-2113 Drug-Eluting
109 tery [SFA] and/or Proximal Popliteal Artery [PPA]) that enrolled 331 subjects with symptomatic (Ruthe
110 ere, we analyze protein-protein association (PPA) networks to identify candidate genes in the vicinit
111 ession (kappa = 0.7), parapapillary atrophy (PPA) progression (kappa = 0.7), disc hemorrhages (kappa
112 d for the presence of peripapillary atrophy (PPA), peripapillary pigment (PPP), drusen in the macula,
113 y (DOT) using preprescription authorization (PPA) vs postprescription review with feedback (PPRF) str
117 verall, these results indicate that chitosan-PPA beads show potential for lower gastrointestinal deli
119 s a photosensitizer and Co(dmgH)(2) (PPA)Cl (PPA-Co, dmgH=dimethylglyoxime; PPA=4-pyridinepropionic a
121 uasi-experimental, crossover trial comparing PPA and PPRF for adult inpatients prescribed any antibio
123 iated by boron trifluoride results in cyclic PPA in high yield, with high molecular weight, and with
124 end groups enhances the stability of cyclic PPA and makes it an attractive candidate for lithographi
125 ing to PPA's low ceiling temperature, cyclic PPA is capable of chain extension to larger molecular we
127 eo and text groups had higher rates of 7-day PPA than the control group at 6 months (video group: 24.
128 ial of this new class of prodrugs to deliver PPA to the brain following oral administration and confi
131 )(2) (PPA)Cl (PPA-Co, dmgH=dimethylglyoxime; PPA=4-pyridinepropionic acid) on the Hf(12) secondary bu
132 the single MR modality models to distinguish PPA variants (accuracy was 0.86, 0.73, and 0.68 for the
136 A subset of AspAT Ib enzymes exhibiting PPA-AT activity was further identified from both Plantae
137 central PPA levels by delivery of exogenous PPA is a recent strategy to reactivate CoA biosynthesis
138 Following discrepant resolution, the final PPA and NPA for the TBP panel were 97.7% (95% confidence
141 ly, the data supports a significant role for PPA in modulating hNSC patterning leading to gliosis, di
143 vFTD from CBS patients and 93% of bvFTD from PPA patients-30% and 13% above base rates (59%, 80%), re
144 either AD (PPA-AD) or a tau variant of FTLD (PPA-FTLD) and 6 patients who had the clinical diagnosis
147 characterization, the PLEX-ID Flu assay had PPAs and NPAs of 98.3% and 97.5% for H1N1-p, 88.6% and 1
153 the preference for cardinal orientations in PPA, thus demonstrating that the oblique effect can also
154 t the oblique effect can also be produced in PPA by simple geometrical images, with statistics simila
163 rly individuals living in nursing homes, low PPA from central to peripheral arteries strongly predict
165 rium acnes, Lactobacillus, and Micrococcus), PPA and NPA ranged from 84.5% to 100% and 99.9% to 100%,
167 eased to (0.42 ug/ul +/- 0.04 ug/ul) at 2 mM PPA compared to (0.83 ug/ul +/- 0.09 ug/ul) in control (
169 this review, I discuss linguistic aspects of PPA syndromes that may prove informative for parsing our
173 ts who had the primary clinical diagnosis of PPA and an autopsy-confirmed diagnosis of either AD (PPA
176 lity of the imaging-supported diagnostics of PPA variants in the Polish clinical setting with access
177 , the subtle learning and memory features of PPA and their neuropathologic associations have not been
180 o new series of cyclic phosphate prodrugs of PPA capable of regenerating excellent levels of CoA in t
186 t of candidates together with information on PPAs, frequency and predicted pathogenicity of the varia
196 retrospective frozen specimens, the overall PPA and NPA for both targets were 92.6% and 93.2%, respe
197 For prospective fresh specimens, the overall PPA and NPA for both targets were 97.7% and 99.3%, respe
200 and (46.63% +/- 2.5%) glia (GFAP positive), PPA treatment drastically shifted differentiation to 80%
201 phere diameter also increased at day 10 post PPA treatment to (Mean: 193.47 um +/- SEM: 6.673 um) ver
205 observed in helical poly(phenylacetylene)s (PPAs) when either the type of linkage with the pendant g
206 ion index was estimated for scene-selective (PPA) and object-selective (LOC) cortical regions while p
207 t current stimulation (tDCS) on the semantic PPA variant (sv-PPA), applying a rigorous study design t
209 ith ADT, a gene encoding prephenate-specific PPA-AT was transferred from a Chlorobi/Bacteroidetes anc
210 ere collected from 69 patients with sporadic PPA, divided into 29 semantic (svPPA), 25 nonfluent (nfv
216 predominantly left-lateralized damage in sv-PPA and accounts of interhemispheric inhibition, we appl
217 ngs demonstrate the efficiency of tDCS in sv-PPA by generating highly specific intrasemantic effects.
218 ation (tDCS) on the semantic PPA variant (sv-PPA), applying a rigorous study design to a large, homog
223 However, subsequent studies reported that PPA also responds strongly to a much wider range of imag
239 pectrum of functional groups accessible, the PPA/P2 O5 -driven Friedel-Crafts acylation offers more o
241 rovide further evidence that V1, RSC and the PPA not only contain information relevant for natural sc
242 regions of human visual cortex, such as the PPA, has been linked to the semantic and categorical pro
252 nowing the correspondences among them in the PPA but not in the other two regions, suggesting that th
253 neural response to different clusters in the PPA could be predicted by the similarity in their image
254 % and 41% of patients on days 1 and 3 in the PPA group (P < .01) and in 57% and 36% of patients on da
255 eater left lateralized amyloid uptake in the PPA group than the amnestic group (p < 0.007), consisten
256 Interestingly, the neural response in the PPA was also predicted by perceptual responses to the sc
262 d the observation that lesions involving the PPA cause topographic disorientation, there is little ca
263 Our results support the causal role of the PPA in the perception of visual scenes, demonstrate that
265 no samples positive for B. parapertussis The PPA and NPA of the Aries BA were 61.1% (95% confidence i
268 n the other two regions, suggesting that the PPA is the key region involved in learning the different
270 son study at the fourth site showed that the PPA ranged from 98.9% to 100% and that the NPA ranged fr
272 were 2686 and 2693 patients admitted to the PPA and PPRF groups, with 29% and 27% of patients prescr
277 This analysis aggregates and compares the PPAs from case studies in Kenya, Ethiopia, Indonesia, th
283 at the best markers to differentiate the two PPA variants at an individual patient level among cortic
284 a discussion of nonfluent/agrammatic variant PPA, the supporting role of short-term memory in a discu
285 al variant FTD (bvFTD), 7 non-fluent variant PPA (nfvPPA), 6 semantic variant PPA (svPPA) and 25 pati
286 pairments consistent with non-fluent variant PPA while patients with behavioural variant frontotempor
287 memory in a discussion of logopenic variant PPA, and components of language associated with discours
288 ent variant PPA (nfvPPA), 6 semantic variant PPA (svPPA) and 25 patients with subjective cognitive im
289 meaning in a discussion of semantic variant PPA, grammatical comprehension and expression in a discu
292 ges in the entire sample depth of SPA versus PPA were found for delta1/2 (T1rho, 14% +/- 12 vs 6% +/-
293 gest a tripartite division of labor, whereby PPA codes landmark identity, RSC retrieves spatial or co
296 s (4 women, 2 men) clinically diagnosed with PPA (3 with nfvPPA and 3 with lvPPA) in whom MRI and SPE
298 duces the level of selective activity within PPA, which may lead to related perceptual impairments in
300 f VCSL disruption on neural processes within PPA, HD patients showed reduced scene-selective activity