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1 VMA area was positively associated with younger age and
2 VMA may affect the optic disc, macular parameters, and c
3 VMA was present in 101 (25.1%) eyes with exudative AMD,
4 s were +4.7 (PVD), +3.2 (RELEASE), and -0.2 (VMA) in the quarterly regimen and +4.9 (PVD), +12.7 (REL
9 A greater proportion of patients achieved VMA resolution and total PVD at month 12 with ocriplasmi
11 ated and resulted in more patients achieving VMA resolution and PVD with less anti-VEGF use compared
12 -toprorenin ratio and vanillylmandelic acid (VMA) excretion (P < 0.025), tests of sympathetic nerve f
13 5(OH)2D3, and urinary vanillylmandelic acid (VMA) were measured by ELISA, and serum and urinary phosp
14 ue, here we turned to visuomotor adaptation (VMA)-a type of motor learning involving skill recalibrat
15 patients with focal vitreomacular adhesion (VMA) and exudative age-related macular degeneration (AMD
16 ar AMD who presented vitreomacular adhesion (VMA) detected by spectral-domain optical coherence tomog
17 ss the prevalence of vitreomacular adhesion (VMA) in consecutive naive eyes diagnosed with exudative
20 al attachment (PVA), vitreomacular adhesion (VMA), partial vitreous detachment without vitreomacular
21 sted for presence of vitreomacular adhesion (VMA), width of vitreous adhesion (focal <1500 mum versus
22 tment of symptomatic vitreomacular adhesion (VMA)/vitreomacular traction, including full-thickness ma
23 lytic asymmetric vinylogous Mukaiyama aldol (VMA) reaction applicable to linear aliphatic aldehydes a
24 KA) acute angle: varus mechanical alignment (VMA) group (HKA < - 3 ) and neutral mechanical axis (NMA
25 wer laws led to the variance-mass allometry (VMA), which states that larger species have lower spatia
28 alence of VMA was 22.6% (CI, 21.1-24.2), and VMA area ranged from 0.25 to 42.7 mm(2) (mean, 12.53 mm(
34 n binding in ventromedial hypothalamic area (VMA), medial basal hypothalamic area (MBA), arcuate nucl
37 tical meridian (vertical meridian asymmetry [VMA]).(3)(,)(4)(,)(5)(,)(6)(,)(7)(,)(8)(,)(9)(,)(10)(,)(
40 r with SD-OCT than TD-OCT to detect baseline VMA (kappa 0.6 vs. 0.52); FTMH (kappa 0.9 vs. 0.78); and
44 eveloped PVD were classified as having focal VMA, with the diameter of vitreous attachment ranging fr
45 atients with nonsurgical resolution of focal VMA at day 28, nonsurgical full-thickness macular hole (
46 ry subgroups without them: presence of focal VMA, presence of FTMH, absence of ERM, and phakic lens s
48 ent agreement was 97%, 92%, 95%, and 82% for VMA, vitreous adhesion width, FTMH, and ERM, respectivel
50 emonstrated PVD, 17 eyes showed no change in VMA status, and 2 eyes were not gradable and were exclud
52 s, Compared with NMA group, the HSS score in VMA group decreased by 0.81 units (95% CI, - 3.37 to 1.7
56 vinyl monomers including vinyl methacrylate (VMA), allyl methacrylate (AMA), 4-vinylbenzyl methacryla
57 inyl monomers, including vinyl methacrylate (VMA), allyl methacrylate (AMA), and N,N-diallyl acrylami
58 and -136 mum (RELEASE), and -93 and -87 mum (VMA) in the monthly and quarterly regimens, respectively
59 the reader-determined presence or absence of VMA (96.7%), FTMH (97.1%), and all other baseline parame
64 y and temporally, the horizontal diameter of VMA, macular thickness, visual acuity, photoreceptor lay
65 cellent agreement for the study endpoints of VMA resolution (95.4%) and FTMH closure (100%) at day 28
68 nd the theoretically predicted parameters of VMA, using detailed data on individual oak trees (Quercu
72 in more detail to estimate the prevalence of VMA and VMA area detailing size and location of VMA.
73 significant difference in the prevalence of VMA in eyes affected by AMD compared with age-matched co
75 fter treatment with ocriplasmin, the rate of VMA/VMT resolution was 45.8% (95% confidence interval [C
81 ed in a lower percentage of eyes with VMT or VMA at baseline (11.7%) than with neither condition (22.
84 with neither (n = 972), patients with VMT or VMA were younger (mean +/- standard error, 75.5 +/- 0.6
88 met its primary end point with pharmacologic VMA resolution at day 28 being significantly higher in t
92 (intein) from Saccharomyces cerevisiae (Sce VMA intein) in conjunction with a chitin-binding domain
93 sed on the observation that the modified Sce VMA intein can be induced to undergo a self-cleavage rea
94 1 intein switches, temperature-sensitive Sce VMA mutations that splice only at the permissive tempera
95 hat the N- and C-terminal regions of the Sce VMA intein may form a separate domain that is not only c
96 e have recently reported an engineered split VMA intein whose splicing activity in trans between two
97 aromyces cerevisiae vacuolar ATPase subunit (VMA) intein inserted within Gal4 and transferred these i
98 ent (intein) of the vacuolar ATPase subunit (VMA) of Saccharomyces cerevisiae catalyzes both protein
99 g the intein of the vacuolar ATPase subunit (VMA) of Saccharomyces cerevisiae that involves cysteines
101 ient-reported visual function in symptomatic VMA/vitreomacular traction (VMT) has not yet been docume
103 providing improved resolution of symptomatic VMA compared with previous phase 3 trials with no additi
104 onths and included resolution of symptomatic VMA, closure of full-thickness macular hole (FTMH), mean
108 A total of 652 patients with symptomatic VMA/VMT, including when associated with a macular hole 4
121 llow-up (n = 60), 13.8 +/- 0.7 for eyes with VMA at baseline or follow-up (n = 79), and 12.9 +/- 0.4
123 The safety of ocriplasmin in patients with VMA and wet AMD was shown to be comparable to the known