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1 OSA and <90% oxyhemoglobin saturation were not associate
2 OSA is an independent predictor for the progression to p
3 OSA is associated with a 2- to 3-fold increased risk of
4 OSA is associated with STDR in patients with type 2 diab
5 OSA is associated with structural and functional atrial
6 OSA is common and the prevalence is increasing with the
7 OSA leads to high cardiovascular morbidity and mortality
8 OSA lends itself to a personalized approach to diagnosis
9 OSA patients intolerant to CPAP have a strong positive c
10 OSA severity was classified based on conventionally acce
11 OSA treatment increased SWA, and SWA was significantly c
12 OSA was assessed using a home-based multichannel cardior
13 asured as regional grey matter volume, in 16 OSA children (8 male, 8.1 +/- 2.2 years, AHI:11.1 +/- 5.
17 he derivation cohort, screening of OSA(>=5), OSA(>=15), and OSA(>=30) revealed that GOAL questionnair
18 OAL questionnaire for screening of OSA(>=5), OSA(>=15), and OSA(>=30) was similar to No-Apnea, STOP-B
19 he validation cohort, screening of OSA(>=5), OSA(>=15), and OSA(>=30), corroborated validation steps
25 rs (hazard ratio [HR] = 1.030, P < .001) and OSA diagnosis (HR = 1.081, P < .033), and was lower in w
26 ohort, screening of OSA(>=5), OSA(>=15), and OSA(>=30) revealed that GOAL questionnaire achieved sens
27 re for screening of OSA(>=5), OSA(>=15), and OSA(>=30) was similar to No-Apnea, STOP-Bang or NoSAS.
28 ohort, screening of OSA(>=5), OSA(>=15), and OSA(>=30), corroborated validation steps with sensitivit
29 frequency bands between the SS (n = 42) and OSA (n = 129) groups during the non-rapid eye movement (
30 ive Airway Pressure in Patients with ACS and OSA) study, including 1,701 patients admitted for ACS (N
31 son, control patients with paroxysmal AF and OSA who underwent PV isolation alone without ablation on
36 : A total of 67 individuals with obesity and OSA (AHI >= 10 events/h) underwent a sleep study and upp
42 dels with interactions between age, sex, and OSA status to determine patients' risk of developing CSC
43 sputum GeneXpert (1 sample per subject) and OSA (2 samples per subject) were identical at 49/59 (83.
45 tive starch with octenyl succinic anhydride (OSA) at levels of 3% or 9%, and afterwards by its comple
46 odification with octenyl succinic anhydride (OSA) helps to control the physicochemical and thermal pr
53 high prevalence of obstructive sleep apnea (OSA) has been reported in Down syndrome (DS) owing to th
54 nce and severity of obstructive sleep apnea (OSA) have been defined by the apnea-hypopnea index (AHI)
55 mated prevalence of obstructive sleep apnea (OSA) in the United States is 10% for mild OSA and 3.8% t
57 e determine whether obstructive sleep apnea (OSA) increases serum levels of active TGF-beta1 in patie
64 e demonstrated that obstructive sleep apnea (OSA) is associated with the development and evolution of
67 ertension (ICH) and obstructive sleep apnea (OSA) on optic nerve function in children with craniosyno
69 Many adults with obstructive sleep apnea (OSA) use device treatments inadequately and remain untre
70 Moderate or severe obstructive sleep apnea (OSA) was defined as a respiratory event index >=15, and
84 liance therapy for obstructive sleep apnoea (OSA) is that therapeutic responses remain unpredictable.
86 Some patients with obstructive sleep apnoea (OSA) respond well to oral appliance therapy, whereas oth
92 ere fit to determine the association between OSA severity and uncontrolled BP or resistant hypertensi
93 , little is known about associations between OSA and glaucoma-related optic disc parameters in young
94 ted adjusting for known associations between OSA and sex, age, body mass index, and medical comorbidi
98 lar consequences.Objectives: To characterize OSA symptom subtypes and assess their association with p
99 the excessively sleepy subtype.Conclusions: OSA symptom subtypes are reproducible and associated wit
102 was insufficient to systematically decrease OSA severity as measured by the apnoea-hypopnoea index.
103 sults, 178 participants (21.0%) demonstrated OSA: 150 with mild OSA, 26 with moderate OSA, and 2 with
104 propose a control panel tool that describes OSA in four domains: disease severity, biological activi
117 ed apnea/hypopnea index thresholds: >=5.0/h (OSA(>=5)), >=15.0/h (OSA(>=15)), and >=30.0/h (OSA(>=30)
119 sis with CSC, and defined patients as having OSA if they had a diagnosis following a sleep study.
127 a trend for reduced HMW-HA concentrations in OSA (31.63/18.11-59.25/ng/mL vs. 46.83/25.41-89.95/ng/mL
132 xia, or the recurrent arousals that occur in OSA, could cause the daytime increases in blood pressure
137 , nasal mask and pneumotachograph to measure OSA severity, arousal threshold and upper airway muscle
138 a (OSA) in the United States is 10% for mild OSA and 3.8% to 6.5% for moderate to severe OSA; current
139 uped into no OSA (AHI < 5 events/hour), mild OSA (AHI >= 5 and <15 events/hour), moderate OSA (AHI >=
141 s were higher in severe OSA compared to mild OSA or non-OSA patients, whereas no differences in VEGF
143 animals, intermittent hypoxia (IH) mimicking OSA promotes tumor malignancy both directly and via host
144 OSA (AHI >= 5 and <15 events/hour), moderate OSA (AHI >= 15 and <30 events/hour), or severe OSA (AHI
146 I results, participants were grouped into no OSA (AHI < 5 events/hour), mild OSA (AHI >= 5 and <15 ev
147 er in severe OSA compared to mild OSA or non-OSA patients, whereas no differences in VEGF levels emer
148 ear localization of gammaH2AX & p16 than non-OSA individuals (20.1 +/- 10.8% vs. 10.3 +/- 2.7%, P(adj
151 nosis in patients with OSA compared with non-OSA controls (OR, 1.27; 95% confidence interval [CI], 1.
152 d an increased risk of XFS compared with non-OSA controls with HTN (OR, 2.67; 95% CI, 2.06-3.46; P <
155 line in 3 areas: diagnosis and assessment of OSA and chronic insomnia disorder, treatment and managem
156 ized on the basis of the underlying cause of OSA; patients could better understand which symptoms and
157 These tools can address the complexity of OSA and guide a physician's course of action on the basi
158 quivalent were used to define a diagnosis of OSA (ICD-9 327.23) and a diagnosis of XFS (ICD-9 365.52
160 could suggest that the deleterious effect of OSA and its contribution to CVD could depend on specific
161 ofiles.Objectives: To evaluate the effect of OSA on cardiovascular risk for patients with different A
163 the no-previous-CVD phenotype, the effect of OSA showed an adjusted hazard ratio (95% confidence inte
164 or the previous-CVD phenotype, the effect of OSA showed an adjusted hazard ratio of 0.69 (0.46-1.04;
172 SA; group 3, recurrent ICH absent history of OSA; and group 4, recurrent ICH with history of OSA.
173 ups: group 1, resolved ICH absent history of OSA; group 2, resolved ICH with history of OSA; group 3,
174 f OSA; group 2, resolved ICH with history of OSA; group 3, recurrent ICH absent history of OSA; and g
175 logists should encourage early management of OSA as well as ICH to optimize ophthalmic outcomes.
177 somnia disorder, treatment and management of OSA, and treatment and management of chronic insomnia di
179 intermittent hypoxia, a key manifestation of OSA, to shed light on the mechanisms by which OSA may gi
182 timodal imaging in this established model of OSA, a discernible neuroinflammatory response was demons
183 ment, contributing to the pathophysiology of OSA and potentially other diseases that involve hypoxia.
184 vealed glass-transition and melting peaks of OSA-starch and a cold-crystallization peak corresponding
185 clinical manifestation (i.e., phenotype) of OSA in an individual are not well described by the AHI.
189 ility of GOAL questionnaire for screening of OSA(>=5), OSA(>=15), and OSA(>=30) was similar to No-Apn
191 In this first admixture mapping study of OSA, novel associations with variants in the iron/heme m
192 (or endotypes) that help define subtypes of OSA and identify the potential use of genetics to furthe
194 gammaH2AX & p16 nuclei in adipose tissue of OSA patients receiving statin, aspirin, and/or RAS inhib
197 sion; however, randomized clinical trials of OSA treatment have not demonstrated significant benefit
199 etine) and an antimuscarinic (oxybutynin) on OSA severity (apnea-hypopnea index [AHI]; primary outcom
200 ught to determine the effects of zolpidem on OSA severity, upper airway physiology and next-day sleep
208 patients with ACS and a specific phenotype, OSA is associated with an increased risk of recurrent ca
209 Admixture mapping analysis of the primary OSA traits identified local African ancestry at the chro
210 e applied admixture mapping on three primary OSA traits [the apnea hypopnea index (AHI), overnight av
214 sed awareness of obstructive sleep apnoea's (OSA) links to Alzheimer's disease and major psychiatric
215 ortable monitor testing for detecting severe OSA syndrome (AHI >/=30 and ESS score >10) was AUC 0.80
217 indicates moderate and >30 indicates severe OSA) and the Epworth Sleepiness Scale (ESS; range, 0-24;
218 TGF-beta1 was increased in moderate-severe OSA patients vs. non-OSA or mild OSA patients with CM.
221 unders, participants with moderate or severe OSA had a 2.0 times higher odds of resistant hypertensio
222 nary study of adults with moderate or severe OSA in whom conventional therapy had failed, combined pa
223 Adults with symptomatic moderate or severe OSA in whom conventional treatments had failed were enro
226 OSA and 3.8% to 6.5% for moderate to severe OSA; current prevalence may be higher, given the increas
227 is trial, we randomized patients with severe OSA and no overt cardiovascular disease to receive 2 mon
230 octenyl succinic anhydride modified starch (OSA), water soluble soy polysaccharides (WSSP)) and gela
233 s abdominal adipose tissue which showed that OSA patients had a significantly higher percentage of ce
234 In vitro digestibility tests showed that OSA treatment reduced the fraction of fastly digestible
238 ter solubility and intrinsic viscosity, that OSA addition changed physicochemical properties of starc
240 positively correlated with beta power in the OSA group as well as in the combined group (OSA + SS).
242 ta power during NREM sleep were found in the OSA group than in the SS group, and beta power was corre
246 t has emerged from these studies is that the OSA-NAFLD association is related to the degree of noctur
251 which symptoms and outcomes will respond to OSA treatment and by how much; and researchers could sel
252 versely, undiagnosed or inadequately treated OSA adversely affects asthma control, partly via effects
257 SA, to shed light on the mechanisms by which OSA may give rise to the complex metabolic disturbances
258 To identify genetic regions associated with OSA and improve statistical power, we applied admixture
259 ts with OSA, TGF-beta1 levels correlate with OSA severity and leptin levels, whereas only associate w
260 A cohort of 81 735 patients diagnosed with OSA at ages 50 to 90 years was identified from medical r
262 Retrospective study in individuals with OSA who were intolerant to continuous positive airway pr
265 n the unadjusted analyses, participants with OSA on average showed thinner peripapillary RNFL at the
266 Study.Methods: Data from 1,207 patients with OSA (apnea-hypopnea index >= 15 events/h) were used to e
269 ents by HTN diagnosis history, patients with OSA and HTN exhibited an increased risk of XFS compared
271 s were significantly higher in patients with OSA compared to controls (0.59/0.31-0.88/ng/mL vs. 0.31/
272 ed risk of an XFS diagnosis in patients with OSA compared with non-OSA controls (OR, 1.27; 95% confid
277 STDR prevalence was higher in patients with OSA than in those without OSA (42.9% vs. 24.1%; P = 0.00
291 effective in promoting sleep in people with OSA, which may be therapeutically useful for people with
293 ongue fat is increased in obese persons with OSA, and may explain the relationship between obesity an
295 culating MDK in CM patients with and without OSA, and their relationship with tumor aggressiveness, w
298 d risk of XFS compared with patients without OSA, particularly in patients with a history of HTN.