TY  - JOUR
A1  - Bulitta, Jürgen B.
A1  - Jiao, Yuanyuan
A1  - Landersdorfer, Cornelia B.
A1  - Sutaria, Dhruvitkumar S.
A1  - Tao, Xun
A1  - Shin, Eunjeong
A1  - Höhl, Rainer
A1  - Holzgrabe, Ulrike
A1  - Stephan, Ulrich
A1  - Sörgel, Fritz
T1  - Comparable Bioavailability and Disposition of Pefloxacin in Patients with Cystic Fibrosis and Healthy Volunteers Assessed via Population Pharmacokinetics
JF  - Pharmaceutics
N2  - Quinolone antibiotics present an attractive oral treatment option in patients with cystic fibrosis (CF). Prior studies have reported comparable clearances and volumes of distribution in patients with CF and healthy volunteers for primarily renally cleared quinolones. We aimed to provide the first pharmacokinetic comparison for pefloxacin as a predominantly nonrenally cleared quinolone and its two metabolites between both subject groups. Eight patients with CF (fat-free mass [FFM]: 36.3 ± 6.9 kg, average ± SD) and ten healthy volunteers (FFM: 51.7 ± 9.9 kg) received 400 mg pefloxacin as a 30 min intravenous infusion and orally in a randomized, two-way crossover study. All plasma and urine data were simultaneously modelled. Bioavailability was complete in both subject groups. Pefloxacin excretion into urine was approximately 74% higher in patients with CF compared to that in healthy volunteers, whereas the urinary excretion of metabolites was only slightly higher in patients with CF. After accounting for body size and composition via allometric scaling by FFM, pharmacokinetic parameter estimates in patients with CF divided by those in healthy volunteers were 0.912 for total clearance, 0.861 for nonrenal clearance, 1.53 for renal clearance, and 0.916 for volume of distribution. Nonrenal clearance accounted for approximately 90% of total pefloxacin clearance. Overall, bioavailability and disposition were comparable between both subject groups.
KW  - cystic fibrosis patients
KW  - healthy volunteers
KW  - fluoroquinolone
KW  - pefloxacin
KW  - absolute bioavailability
KW  - population pharmacokinetics
KW  - allometric scaling
KW  - body size
KW  - body composition
KW  - S-ADAPT
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-197221
SN  - 1999-4923
VL  - 11
IS  - 7
ER  - 
TY  - JOUR
A1  - Dirimanov, Stoyan
A1  - Högger, Petra
T1  - Screening of inhibitory effects of polyphenols on Akt-phosphorylation in endothelial cells and determination of structure-activity features
JF  - Biomolecules
N2  - Polyphenols exert beneficial effects in type 2 diabetes mellitus (T2DM). However, their mechanism of action remains largely unknown. Endothelial Akt-kinase plays a key role in the pathogenesis of cardiovascular complications in T2DM and therefore the modulation of its activity is of interest. This work aimed to characterize effects of structurally different polyphenols on Akt-phosphorylation (pAkt) in endothelial cells (Ea.hy926) and to describe structure-activity features. A comprehensive screening via ELISA quantified the effects of 44 polyphenols (10 µM) on pAkt Ser473. The most pronounced inhibitors were luteolin (44 ± 18%), quercetin (36 ± 8%), urolithin A (35 ± 12%), apigenin, fisetin, and resveratrol; (p < 0.01). The results were confirmed by Western blotting and complemented with corresponding experiments in HUVEC cells. A strong positive and statistically significant correlation between the mean inhibitory effects of the tested polyphenols on both Akt-residues Ser473 and Thr308 (r = 0.9478, p = 0.0003) was determined by immunoblotting. Interestingly, the structural characteristics favoring pAkt inhibition partially differed from structural features enhancing the compounds’ antioxidant activity. The present study is the first to quantitatively compare the influence of polyphenols from nine different structural subclasses on pAkt in endothelial cells. These effects might be advantageous in certain T2DM-complications involving over-activation of the Akt-pathway. The suggested molecular mode of action of polyphenols involving Akt-inhibition contributes to understanding their effects on the cellular level.
KW  - Akt/PKB
KW  - endothelium
KW  - diabetes
KW  - polyphenols
KW  - in vitro
KW  - structure-activity relationships
KW  - screening
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-197333
SN  - 2218-273X
VL  - 9
IS  - 6
ER  - 
TY  - JOUR
A1  - Mansour, Ahmed M.
A1  - Steiger, Christoph
A1  - Nagel, Christoph
A1  - Schatzschneider, Ulrich
T1  - Wavelength‐dependent control of the CO release kinetics of manganese(I) tricarbonyl PhotoCORMs with benzimidazole coligands
JF  - European Journal of Inorganic Chemistry
N2  - A series of photoactivatable CO‐releasing molecules (PhotoCORMs) was prepared from manganese pentacarbonyl bromide and 1H‐benzimidazol‐2‐ylmethyl‐(N‐phenyl)amine ligands (L) bearing different electron‐donating and electron‐withdrawing groups R = H, 4‐CH\(_3\), 4‐OCH\(_3\), 4‐Cl, 4‐NO\(_2\), 2‐, 3‐, and 4‐COOCH\(_3\) on the phenyl substituent to give octahedral manganese(I) complexes of the general formula [MnBr(CO)\(_3\)(L)]. Aerated DMSO solutions of the compounds are stable in the dark for 16 h with no CO release. However, the compounds rapidly release CO upon illumination at 412–525 nm, depending on the substitution pattern. Its influence on the photophysical and photochemical properties was systematically explored using UV/Vis spectroscopy and CO release measurements with a commercial gas sensor system. In the nitro‐substituted compound, the electronically excited state switched from benzimidazole‐ to phenyl‐centered, leading to a markedly different photochemical behavior of this visible‐light activated PhotoCORM.
KW  - CO‐releasing molecules (CORMs)
KW  - Manganese Carbonyl ligands
KW  - Benzimidazole
KW  - TDDFT
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-218362
VL  - 2019
IS  - 42
ER  - 
TY  - JOUR
A1  - Penagos-Calvete, Diana
A1  - Duque, Valeria
A1  - Marimon, Claudia
A1  - Parra, Diana M.
A1  - Restrepo-Arango, Sandra K.
A1  - Scherf-Clavel, Oliver
A1  - Holzgrabe, Ulrike
A1  - Montoya, Guillermo
A1  - Salamanca, Constain H.
T1  - Glycerolipid composition and advanced physicochemical considerations of sacha inchi oil toward cosmetic products formulation
JF  - Cosmetics
N2  - Sacha inchi oil is a premier raw material with highly nutritional and functional features for the foodstuff, pharmaceutical, beauty, and personal care industries. One of the most important facts about this oil is the huge chemical content of unsaturated and polyunsaturated fatty acids. However, the current available information on the characterization of the triglyceride composition and the advance physicochemical parameters relevant to emulsion development is limited. Therefore, this research focused on providing a detailed description of the lipid composition using high-resolution tandem mass spectrometry and thorough physicochemical characterization to find the value of the required hydrophilic–lipophilic balance (HLB). For this, a study in the interfacial tension was evaluated, followed by the assessment of different parameters such as creaming index, droplet size, viscosity, zeta potential, pH, and electrical conductivity for a series emulsified at thermal stress condition. The results show that fatty acids are arranged into glycerolipids and the required HLB to achieve the maximum physical stability is around 8.
KW  - sacha inchi oil
KW  - unsaturated fatty acids
KW  - triacylglycerides
KW  - high-resolution tandem mass spectrometry
KW  - emulsions oil-in-water
KW  - required hydrophilic–lipophilic balance
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-193857
SN  - 2079-9284
VL  - 6
IS  - 4
ER  - 
TY  - JOUR
A1  - Pöppler, Ann-Christin
A1  - Lübtow, Michael  M.
A1  - Schlauersbach, Jonas
A1  - Wiest, Johannes
A1  - Meinel, Lorenz
A1  - Luxenhofer, Robert
T1  - Loading dependent Structural Model of Polymeric Micelles Encapsulating Curcumin by Solid-State NMR Spectroscopy
JF  - Angewandte Chemie International Edition
N2  - Detailed insight into the internal structure of drug‐loaded polymeric micelles is scarce, but important for developing optimized delivery systems. We observed that an increase in the curcumin loading of triblock copolymers based on poly(2‐oxazolines) and poly(2‐oxazines) results in poorer dissolution properties. Using solid‐state NMR spectroscopy and complementary tools we propose a loading‐dependent structural model on the molecular level that provides an explanation for these pronounced differences. Changes in the chemical shifts and cross‐peaks in 2D NMR experiments give evidence for the involvement of the hydrophobic polymer block in the curcumin coordination at low loadings, while at higher loadings an increase in the interaction with the hydrophilic polymer blocks is observed. The involvement of the hydrophilic compartment may be critical for ultrahigh‐loaded polymer micelles and can help to rationalize specific polymer modifications to improve the performance of similar drug delivery systems.
KW  - dissolution rates
KW  - micelles
KW  - polymers
KW  - short-range order
KW  - solid-state NMR spectroscopy
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-206705
VL  - 58
IS  - 51
ER  - 
TY  - JOUR
A1  - Shah, Nirav R.
A1  - Bulitta, Jürgen B.
A1  - Kinzig, Martina
A1  - Landersdorfer, Cornelia B.
A1  - Jiao, Yuanyuan
A1  - Sutaria, Dhruvitkumar S.
A1  - Tao, Xun
A1  - Höhl, Rainer
A1  - Holzgrabe, Ulrike
A1  - Kees, Frieder
A1  - Stephan, Ulrich
A1  - Sörgel, Fritz
T1  - Novel population pharmacokinetic approach to explain the differences between cystic fibrosis patients and healthy volunteers via protein binding
JF  - Pharmaceutics
N2  - The pharmacokinetics in patients with cystic fibrosis (CF) has long been thought to differ considerably from that in healthy volunteers. For highly protein bound β-lactams, profound pharmacokinetic differences were observed between comparatively morbid patients with CF and healthy volunteers. These differences could be explained by body weight and body composition for β-lactams with low protein binding. This study aimed to develop a novel population modeling approach to describe the pharmacokinetic differences between both subject groups by estimating protein binding. Eight patients with CF (lean body mass [LBM]: 39.8 ± 5.4kg) and six healthy volunteers (LBM: 53.1 ± 9.5kg) received 1027.5 mg cefotiam intravenously. Plasma concentrations and amounts in urine were simultaneously modelled. Unscaled total clearance and volume of distribution were 3% smaller in patients with CF compared to those in healthy volunteers. After allometric scaling by LBM to account for body size and composition, the remaining pharmacokinetic differences were explained by estimating the unbound fraction of cefotiam in plasma. The latter was fixed to 50% in male and estimated as 54.5% in female healthy volunteers as well as 56.3% in male and 74.4% in female patients with CF. This novel approach holds promise for characterizing the pharmacokinetics in special patient populations with altered protein binding.
KW  - cystic fibrosis patients
KW  - healthy volunteers
KW  - cefotiam
KW  - beta-lactam antibiotics
KW  - population pharmacokinetics
KW  - protein binding
KW  - allometric scaling
KW  - body size
KW  - body composition
KW  - S-ADAPT
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196934
SN  - 1999-4923
VL  - 11
IS  - 6
ER  -