Methods: The inclusion complex of berberine hydrochloride with hydroxypropyl-beta-cyclodextrin (1: 1) was prepared by freeze-drying method and compared
with the the physical mixtures of the compounds. KPT-8602 solubility dmso Inclusion complexation was studied by phase solubility diagram, differential thermal analysis, spectrophotometric characterization and dissolution rate. The solubility of the formulations was evaluated by saturation solubility studies while their bitterness was tested in human volunteers.
Results: Differential thermal analysis and spectrophotometric characterization indicate that berberine hydrochloride formed inclusion complex with hydroxypropyl-beta-cyclodextrin. The phase solubility diagram of berberine hydrochloride with hydroxypropyl-beta-cyclodextrin was of A(L)-type, with a stability constant was 694.5 L/mol at 25 degrees C. ubiquitin-Proteasome degradation The solubility of berberine hydrochloride was increased by 5.27 times for the complex at a concentration of 0.01 mol/L. The dissolution of berberine hydrochloride after 20 min from the inclusion complex, physical mixture and pure berberine hydrochloride was 89.6, 69.8 and 58.8 %, respectively. The bitterness of the inclusion complex was considerably lower than that of the drug alone or the physical mixture with hydroxypropyl-beta-cyclodextrin.
Conclusion:
The inclusion complex demonstrated improved dissolution properties and lowered the bitterness of berberine hydrochloride.”
“Gadolinium-enhancing lesions in brain magnetic resonance imaging of multiple sclerosis (MS) patients are of great interest since they are markers of disease activity. Identification of gadolinium-enhancing lesions is particularly challenging because the vast majority of enhancing voxels are associated with normal structures, particularly blood vessels. Furthermore, these lesions are typically small and in close proximity to vessels. In this paper,
we present an automatic, probabilistic framework for segmentation of gadolinium-enhancing lesions in MS using conditional random fields. GW2580 clinical trial Our approach, through the integration of different components, encodes different information such as correspondence between the intensities and tissue labels, patterns in the labels, or patterns in the intensities. The proposed algorithm is evaluated on 80 multimodal clinical datasets acquired from relapsing-remitting MS patients in the context of multicenter clinical trials. The experimental results exhibit a sensitivity of 98% with a low false positive lesion count. The performance of the proposed algorithm is also compared to a logistic regression classifier, a support vector machine and a Markov random field approach. The results demonstrate superior performance of the proposed algorithm at successfully detecting all of the gadolinium-enhancing lesions while maintaining a low false positive lesion count.