245 research outputs found
Dataset on the activation of Mueller cells through macrophages upon hypoxia in the retina
The dataset presented in this article complements the article entitled "Myeloid cells contribute indirectly to VEGF expression upon hypoxia via activation of Mueller cells" (C. Nuernberg, N. Kociok, C. Brockmann, T. Lischke, S. Crespo-Garcia, N. Reichhart, S. Wolf, R. Baumgrass, S.A. Eming, S. Beer-Hammer, and A.M. Joussen). This complementary dataset provides further insight into the experimental validation of the VEGF(fl/fl) LysMCre (here named VEGF(mcko)) knockout model used in the main article through genomic and quantitative Real-Time PCR in various murine tissues as well as additional flow cytometry data and immunohistochemical stainings. By providing these data, we aim to enable researcher to reproduce and critically analyze our data
Placental growth factor and its potential role in diabetic retinopathy and other ocular neovascular diseases
published_or_final_versio
An exploratory investigation of brain collateral circulation plasticity after cerebral ischemia in two experimental C57BL/6 mouse models
Brain collateral circulation is an essential compensatory mechanism in response to acute brain ischemia. To study the temporal evolution of brain macro and microcollateral recruitment and their reciprocal interactions in response to different ischemic conditions, we applied a combination of complementary techniques (T2-weighted magnetic resonance imaging [MRI], time of flight [TOF] angiography [MRA], cerebral blood flow [CBF] imaging and histology) in two different mouse models. Hypoperfusion was either induced by permanent bilateral common carotid artery stenosis (BCCAS) or 60-min transient unilateral middle cerebral artery occlusion (MCAO). In both models, collateralization is a very dynamic phenomenon with a global effect affecting both hemispheres. Patency of ipsilateral posterior communicating artery (PcomA) represents the main variable survival mechanism and the main determinant of stroke lesion volume and recovery in MCAO, whereas the promptness of external carotid artery retrograde flow recruitment together with PcomA patency, critically influence survival, brain ischemic lesion volume and retinopathy in BCCAS mice. Finally, different ischemic gradients shape microcollateral density and size
WIMP-nucleon cross-section results from the second science run of ZEPLIN-III
We report experimental upper limits on WIMP-nucleon elastic scattering cross
sections from the second science run of ZEPLIN-III at the Boulby Underground
Laboratory. A raw fiducial exposure of 1,344 kg.days was accrued over 319 days
of continuous operation between June 2010 and May 2011. A total of eight events
was observed in the signal acceptance region in the nuclear recoil energy range
7-29 keV, which is compatible with background expectations. This allows the
exclusion of the scalar cross-section above 4.8E-8 pb near 50 GeV/c^2 WIMP mass
with 90% confidence. Combined with data from the first run, this result
improves to 3.9E-8 pb. The corresponding WIMP-neutron spin-dependent
cross-section limit is 8.0E-3 pb. The ZEPLIN programme reaches thus its
conclusion at Boulby, having deployed and exploited successfully three liquid
xenon experiments of increasing reach
Quenching Factor for Low Energy Nuclear Recoils in a Plastic Scintillator
Plastic scintillators are widely used in industry, medicine and scientific
research, including nuclear and particle physics. Although one of their most
common applications is in neutron detection, experimental data on their
response to low-energy nuclear recoils are scarce. Here, the relative
scintillation efficiency for neutron-induced nuclear recoils in a
polystyrene-based plastic scintillator (UPS-923A) is presented, exploring
recoil energies between 125 keV and 850 keV. Monte Carlo simulations,
incorporating light collection efficiency and energy resolution effects, are
used to generate neutron scattering spectra which are matched to observed
distributions of scintillation signals to parameterise the energy-dependent
quenching factor. At energies above 300 keV the dependence is reasonably
described using the semi-empirical formulation of Birks and a kB factor of
(0.014+/-0.002) g/MeVcm^2 has been determined. Below that energy the measured
quenching factor falls more steeply than predicted by the Birks formalism.Comment: 8 pages, 9 figure
A coumaroyl-ester-3-hydroxylase insertion mutant reveals the existence of nonredundant meta-hydroxylation pathways and essential roles for phenolic precursors in cell expansion and plant growth
Cytochromes P450 monooxygenases from the CYP98 family catalyze the meta-hydroxylation step in the phenylpropanoid biosynthetic pathway. The ref8 Arabidopsis (Arabidopsis thaliana) mutant, with a point mutation in the CYP98A3 gene, was previously described to show developmental defects, changes in lignin composition, and lack of soluble sinapoyl esters. We isolated a T-DNA insertion mutant in CYP98A3 and show that this mutation leads to a more drastic inhibition of plant development and inhibition of cell growth. Similar to the ref8 mutant, the insertion mutant has reduced lignin content, with stem lignin essentially made of p-hydroxyphenyl units and trace amounts of guaiacyl and syringyl units. However, its roots display an ectopic lignification and a substantial proportion of guaiacyl and syringyl units, suggesting the occurrence of an alternative CYP98A3-independent meta-hydroxylation mechanism active mainly in the roots. Relative to the control, mutant plantlets produce very low amounts of sinapoyl esters, but accumulate flavonol glycosides. Reduced cell growth seems correlated with alterations in the abundance of cell wall polysaccharides, in particular decrease in crystalline cellulose, and profound modifications in gene expression and homeostasis reminiscent of a stress response. CYP98A3 thus constitutes a critical bottleneck in the phenylpropanoid pathway and in the synthesis of compounds controlling plant development. CYP98A3 cosuppressed lines show a gradation of developmental defects and changes in lignin content (40% reduction) and structure (prominent frequency of p-hydroxyphenyl units), but content in foliar sinapoyl esters is similar to the control. The purple coloration of their leaves is correlated to the accumulation of sinapoylated anthocyanins
Placental growth factor and its potential role in diabetic retinopathy and other ocular neovascular diseases.
The role of vascular endothelial growth factor (VEGF), including in retinal vascular diseases, has been well studied, and pharmacological blockade of VEGF is the gold standard of treatment for neovascular age-related macular degeneration, retinal vein occlusion and diabetic macular oedema. Placental growth factor (PGF, previously known as PlGF), a homologue of VEGF, is a multifunctional peptide associated with angiogenesis-dependent pathologies in the eye and non-ocular conditions. Animal studies using genetic modification and pharmacological treatment have demonstrated a mechanistic role for PGF in pathological angiogenesis. Inhibition decreases neovascularization and microvascular abnormalities across different models, including oxygen-induced retinopathy, laser-induced choroidal neovascularization and in diabetic mice exhibiting retinopathies. High levels of PGF have been found in the vitreous of patients with diabetic retinopathy. Despite these strong animal data, the exact role of PGF in pathological angiogenesis in retinal vascular diseases remains to be defined, and the benefits of PGF-specific inhibition in humans with retinal neovascular diseases and macular oedema remain controversial. Comparative effectiveness research studies in patients with diabetic retinal disease have shown that treatment that inhibits both VEGF and PGF may provide superior outcomes in certain patients compared with treatment that inhibits only VEGF. This review summarizes current knowledge of PGF, including its relationship to VEGF and its role in pathological angiogenesis in retinal diseases, and identifies some key unanswered questions about PGF that can serve as a pathway for future basic, translational and clinical research
Effects of empagliflozin and target-organ damage in a novel rodent model of heart failure induced by combined hypertension and diabetes
Type 2 diabetes mellitus and hypertension are two major risk factors leading to heart failure and cardiovascular damage. Lowering blood sugar by the sodium-glucose co-transporter 2 inhibitor empagliflozin provides cardiac protection. We established a new rat model that develops both inducible diabetes and genetic hypertension and investigated the effect of empagliflozin treatment to test the hypothesis if empagliflozin will be protective in a heart failure model which is not based on a primary vascular event. The transgenic Tet29 rat model for inducible diabetes was crossed with the mRen27 hypertensive rat to create a novel model for heart failure with two stressors. The diabetic, hypertensive heart failure rat (mRen27/tetO-shIR) were treated with empagliflozin (10 mg/kg/d) or vehicle for 4 weeks. Cardiovascular alterations were monitored by advanced speckle tracking echocardiography, gene expression analysis and immunohistological staining. The novel model with increased blood pressure und higher blood sugar levels had a reduced survival compared to controls. The rats develop heart failure with reduced ejection fraction. Empagliflozin lowered blood sugar levels compared to vehicle treated animals (182.3 ± 10.4 mg/dl vs. 359.4 ± 35.8 mg/dl) but not blood pressure (135.7 ± 10.3 mmHg vs. 128.2 ± 3.8 mmHg). The cardiac function was improved in all three global strains (global longitudinal strain − 8.5 ± 0.5% vs. − 5.5 ± 0.6%, global radial strain 20.4 ± 2.7% vs. 8.8 ± 1.1%, global circumferential strain − 11.0 ± 0.7% vs. − 7.6 ± 0.8%) and by increased ejection fraction (42.8 ± 4.0% vs. 28.2 ± 3.0%). In addition, infiltration of macrophages was decreased by treatment (22.4 ± 1.7 vs. 32.3 ± 2.3 per field of view), despite mortality was not improved. Empagliflozin showed beneficial effects on cardiovascular dysfunction. In this novel rat model of combined hypertension and diabetes, the improvement in systolic and diastolic function was not secondary to a reduction in left ventricular mass or through modulation of the afterload, since blood pressure was not changed. The mRen27/tetO-shIR strain should provide utility in separating blood sugar from blood pressure-related treatment effects
Single electron emission in two-phase xenon with application to the detection of coherent neutrino-nucleus scattering
We present an experimental study of single electron emission in ZEPLIN-III, a
two-phase xenon experiment built to search for dark matter WIMPs, and discuss
applications enabled by the excellent signal-to-noise ratio achieved in
detecting this signature. Firstly, we demonstrate a practical method for
precise measurement of the free electron lifetime in liquid xenon during normal
operation of these detectors. Then, using a realistic detector response model
and backgrounds, we assess the feasibility of deploying such an instrument for
measuring coherent neutrino-nucleus elastic scattering using the ionisation
channel in the few-electron regime. We conclude that it should be possible to
measure this elusive neutrino signature above an ionisation threshold of
3 electrons both at a stopped pion source and at a nuclear reactor.
Detectable signal rates are larger in the reactor case, but the triggered
measurement and harder recoil energy spectrum afforded by the accelerator
source enable lower overall background and fiducialisation of the active
volume
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