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1 inst induction of pancreatic inflammation by iohexol.
2 rement (mGFR) by the plasma disappearance of iohexol.
3 Iodixanol, 8 (16%) to Iomeprol and 4 (8%) to Iohexol.
4  in GFR, measured by the plasma clearance of iohexol.
5 s were injected with 0.5, 1.0, and 2.0 mL of iohexol.
6 IV administration of a nontoxic 5-mL dose of iohexol.
7 as a GFR tracer in patients by comparison to iohexol.
8     They received a similar iodine load with iohexol 300 and were studied with a similar technique.
9 ted contrast material (50% and full-strength iohexol 300).
10 omography (CT) of the abdomen with 100 mL of iohexol (300 mg iodine per milliliter, Omnipaque; GE Hea
11                             A 150-mL dose of iohexol (300 mg of iodine per milliliter) (Omnipaque; Ny
12 dual-contrast-enhanced CT (triglyceride plus iohexol [425 mg I/kg]).
13 logram of body weight [mg I/kg]), CTAP (with iohexol [600 mg I/kg]), triglyceride-enhanced CT (126 mg
14  the baseline-adjusted GFR, as measured with iohexol, after 3 years plus a 2-month washout period.
15 tion rate (GFR) was directly measured (using iohexol) along with 12 markers of inflammation in Multic
16  GFR measured by the plasma disappearance of iohexol among 391 participants in the Chronic Kidney Dis
17 bitridol, 4 (9.5%) to Ioxaglate, 3 (7.1%) to Iohexol and 1 (2.4%) to Iopramide.
18       A total of 539 patients (258 receiving iohexol and 281 not receiving contrast material) were en
19 the plasma clearance of an IV single dose of iohexol and estimation of glomerular filtration rate wit
20 particles, prepared through cross-linking of iohexol and hexamethylene diisocyanate followed by copre
21 d with 1.5 mL per kilogram of body weight of iohexol and imaged between 2.5 and 10 minutes after inje
22 rved in 37 (14.3%) of 258 subjects receiving iohexol and in seven (2.5%) of 281 subjects in the contr
23 essary to image the specific distribution of iohexol and liposome simultaneously and independently, e
24 imated by DXA; GFR and RPF were estimated by iohexol and p-aminohippurate clearance; albuminuria was
25                                          The iohexol and subsequent ICM shortage has short-term (week
26 ng 1-compartment plasma clearance models and iohexol as the exogenous filtration marker.
27  equilibrium CT protocol was developed using iohexol at 300 mg of iodine per milliliter (bolus of 1 m
28 re at 0.625 and 1.25 mmol/L of gadolinium in iohexol at both magnet strengths.
29 ondary outcomes included the decrease in the iohexol-based GFR per year and the urinary albumin excre
30                     The mean decrease in the iohexol-based GFR was -3.0 ml per minute per 1.73 m(2) p
31 ut, the between-group difference in the mean iohexol-based GFR was 0.001 ml per minute per 1.73 m(2)
32                            The mean baseline iohexol-based GFR was 68.7 ml per minute per 1.73 m(2) i
33 ermined by measuring the plasma clearance of iohexol) between the baseline value and the last availab
34 tandem mass spectrometry and measured GFR by iohexol clearance (iGFR).
35 idney donor candidates and compare this with iohexol clearance (reference standard for measuring GFR)
36 rular filtration rate formula as compared to iohexol clearance among patients with shock.
37 m kidney donor candidates who underwent both iohexol clearance and CT urography between July 2016 and
38 vels, Kidney Injury Marker-1 expression, and iohexol clearance at 3 mo did not differ significantly b
39            ABP was measured at baseline, and iohexol clearance at baseline and twice during follow-up
40                                              Iohexol clearance calculation with a population pharmaco
41 impact of a Bayesian estimation procedure on iohexol clearance estimates, and we identified an optima
42 ong 99 included patients, we could calculate iohexol clearance for 85.
43 earance Survey, GFR was measured with plasma iohexol clearance in 1627 individuals without diabetes,
44     Participants' GFR was measured by plasma iohexol clearance in 2007-2009 (n=1627), 2013-2015 (n=13
45 ree-compartment model is optimal to estimate iohexol clearance in elderly patients with reduced GFR.
46           We demonstrated the feasibility of iohexol clearance measurement in unstable critically ill
47 eneral population through a meta-analysis of iohexol clearance measurements in three large European p
48                                    The Renal Iohexol Clearance Survey (RENIS) cohort is a representat
49                                 In the Renal Iohexol Clearance Survey (RENIS) in northern Europe, we
50                                 In the Renal Iohexol Clearance Survey, GFR was measured with plasma i
51                             All patients had iohexol clearance to measure GFR at evaluation under sta
52 rment in one patient out of two; the bias of iohexol clearance toward 24-hour urinary creatinine clea
53 R values falling within 10%, 20%, and 30% of iohexol clearance values).
54                                   The median iohexol clearance was 31 mL/min (interquartile range, 16
55                                              Iohexol clearance was an estimation of the mean glomerul
56 (mean difference between CT-measured GFR and iohexol clearance), precision (the distance between quar
57                                 According to iohexol clearance, 41 patients (48%) had severe hypofilt
58 by measured glomerular filtration rate using iohexol clearance, a relationship not detected using est
59 nsplant function, measured by creatinine and iohexol clearance, after utilizing kidneys from porcine
60  measurements of creatinine, cystatin C, and iohexol clearance, all three equations performed similar
61                    Using arterial tonometry, iohexol clearance, and magnetic resonance imaging, we re
62 nd GFR, determined by measurement of urinary iohexol clearance, measured 2 weeks after Tx.
63 tic glomerular filtration rate formulas with iohexol clearance, with or without creatinine concentrat
64 on after 3 mo, as measured by creatinine and iohexol clearance.
65 ured glomerular filtration rate (mGFR) using iohexol clearance.
66  post injection, were sufficient to estimate iohexol clearance.
67  measurements of creatinine, cystatin C, and iohexol clearance.
68 ed good agreement with GFR measured based on iohexol clearance.
69 cted Moran and Myers value was within 30% of iohexol-clearance-measured glomerular filtration rate fo
70 rance of iothalamate and plasma clearance of iohexol compared with inulin clearance.
71 velopment group comprising 546 patients with iohexol concentration data up to 300 min post injection.
72 n rate (GFR) was measured directly by plasma iohexol disappearance.
73 milar patterns of implant size expansion and iohexol distribution in the implants were observed both
74               Animals underwent nonenhanced, iohexol-enhanced (600 mg of iodine per kilogram of body
75 five helical CT examinations: unenhanced CT, iohexol-enhanced CT (600 mg iodine per kilogram of body
76 ual-contrast-enhanced CT (112.4 HU +/- 1.2), iohexol-enhanced CT (97.9 HU +/- 2.2), triglyceride-enha
77 nhanced CT was significantly greater than at iohexol-enhanced CT (P < .05), and attenuation differenc
78 trast-enhanced CT were greater than those at iohexol-enhanced CT or at CTAP (P < .05).
79 ively improved liver lesion detection versus iohexol-enhanced CT.
80 for ITG-dual-enhanced scans as compared with iohexol-enhanced scans (P: <.01).
81  demonstrated similar liver opacification to iohexol-enhanced scans obtained with 600 mg of iodine pe
82 quations in 187 former kidney donors against iohexol GFR for measuring GFR.
83  < or =1.5 mg/dl were compared with standard iohexol GFR values.
84 most precise at 0.41, and were within 30% of iohexol GFR, 89.3 and 96% of the time, respectively.
85                                       Median iohexol-GFR (iGFR) was 41.3 ml/min per 1.73 m(2) (interq
86 effectiveness of ICM substitution (ie, using iohexol in a patient with a previous iopromide reaction)
87 easured GFR (mGFR) using plasma clearance of iohexol in Stockholm, Sweden, who had 9404 concurrent me
88 nstrated identical concentrations of Na+ and iohexol in ureteral effluent (UE) compared with circulat
89 h a computed tomography (CT) contrast agent, iohexol (Ioh-Lipo), which has specific amide protons exc
90 y contrast media (ICM) iopamidol, iopromide, iohexol, iomeprol, and diatrizoate was examined in purif
91  four low-osmolar contrast media (ioxaglate, iohexol, iopamidol, and ioversol) were compared.
92 fferent CM (iobitridol, iomeprol, iodixanol, iohexol, ioversol, iopramide and ioxaglate).
93                          Plasma clearance of iohexol is a pivotal metric to quantify glomerular filtr
94 lar, iodinated intravenous products, such as iohexol, is unlikely to have a clinically important effe
95 ation, administration, and safety aspects of iohexol, laboratory analysis, blood sample collection an
96 ar cells, but not HEK293 or COS7 cells, with iohexol led to a peak and then plateau in Ca(2+) signali
97 s GFR as measured by plasma disappearance of iohexol, likely a result of a change in methods used to
98      Blood and urine chemistries, as well as iohexol-measured GFR, were assessed before and after eac
99 ntional small-molecule contrast agents, poly(iohexol) nanoparticles exhibited substantially protracte
100                           Biocompatible poly(iohexol) nanoparticles, prepared through cross-linking o
101 fter intravenous administration of 120 mL of iohexol (Omnipaque 350; GE Healthcare, Princeton, NJ) in
102 uman acinar cells to the radiocontrast agent iohexol (Omnipaque; GE Healthcare, Princeton, NJ) and me
103  of intravenous contrast material (100 mL of iohexol, Omnipaque 350; GE Healthcare, Princeton, NJ).
104 ith 150 mL of intravenous contrast material (iohexol, Omnipaque; Amersham Healthcare, Cork, Ireland)
105 ter, she underwent contrast-enhanced (100 mL iohexol, Omnipaque; GE Healthcare, Cork, Ireland) abdomi
106 re greater with lower iodine doses than with iohexol or at CTAP.
107  contrast material (59 who underwent CT with iohexol or iodixanol and 81 who underwent MR imaging wit
108 , 150 mL of 60% iodinated contrast material (iohexol or iothalamate meglumine) was injected at either
109 ured either via exogenous markers (eg, DTPA, iohexol), or estimated using equations.
110 e (GFR) using the slope-intercept method for iohexol plasma clearance (mGFR) in population cohorts fr
111                                              Iohexol plasma clearance measurement as gold standard.
112 tatin c-based formulas with a gold standard (iohexol plasma clearance) in 193 renal transplant recipi
113            Primary outcome was measured GFR (iohexol plasma clearance).
114 erular filtration rateiohexol measured using iohexol plasma clearance: 19 2 vs 16 2 mL/min/1.73 m2; p
115 ine arterial blood samples over 24 hours for iohexol plasma concentration measurements.
116                  Dilution of gadolinium into iohexol reduced the signal intensity in all samples comp
117  at rest, immediately after an 8-mL bolus of iohexol, repeated after a second 8-mL bolus, and during
118  triglyceride (especially when combined with iohexol), sensitivity values and liver-to-lesion attenua
119                                   The recent iohexol shortage has precipitated disruptions in a pharm
120            Materials and Methods Seven 50-mL iohexol solutions were used, with concentrations of 0.03
121 is diluted into a 50% or greater strength of iohexol, the signal intensity curve shifts so that the m
122 he plasma clearance of the endogenous marker iohexol, to compare performance of existing equations of
123                           GFR determination (iohexol urinary clearance) was conducted in hours 2-3 an
124 Swine cervices were injected with EC-ethanol iohexol using both injectors.
125 t of urine from neonates who did not receive iohexol was 5.6 HU +/- 3.9, and that from neonates witho
126 m 22 neonates were obtained 8-12 hours after iohexol was administered enterally.
127 ecrotizing enterocolitis who did not receive iohexol was collected.
128                                              Iohexol was selected as it is non-radio labeled, inexpen
129                         In all examinations, iohexol was used as the contrast agent.
130         Hydrodissection (0.9% saline with 2% iohexol) was injected in 17 of 22 (77.3%) procedures to
131                             Relmapirazin and iohexol were administered intravenously in consecutive b
132 ution was unveiled by the CT contrast agent, iohexol, where it shows a core-shell structure of the de
133 e urine was greater than or equal to that of iohexol with no reported severe adverse events.
134 gested nonionic iodinated contrast material (iohexol) with a concentration of 300 mg per milliliter w

 
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