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5 results on '"Boban, Drina"'

1. Cerebrospinal fluid-based kinetic biomarkers of axonal transport in monitoring neurodegeneration.

Author

Fanara, Patrizia, Wong, Po-Yin A, Husted, Kristofor H, Liu, Shanshan, Liu, Victoria M, Kohlstaedt, Lori A, Riiff, Timothy, Protasio, Joan C, Boban, Drina, Killion, Salena, Killian, Maudi, Epling, Lorrie, Sinclair, Elisabeth, Peterson, Julia, Price, Richard W, Cabin, Deborah E, Nussbaum, Robert L, Brühmann, Jörg, Brandt, Roland, Christine, Chadwick W, Aminoff, Michael J, and Hellerstein, Marc K

Subjects
Microtubules, Animals, Mice, Transgenic, Humans, Mice, Parkinson Disease, Secondary, Paclitaxel, Noscapine, 1-Methyl-4-phenyl-1, 2, 3, 6-tetrahydropyridine, Nocodazole, Superoxide Dismutase, Neuregulin-1, Amyloid beta-Protein Precursor, Microtubule-Associated Proteins, tau Proteins, Case-Control Studies, Axonal Transport, Kinetics, Mutation, Missense, Female, Male, Tubulin Modulators, alpha-Synuclein, Chromogranin B, Biomarkers, Superoxide Dismutase-1, Neurosciences, Dementia, Brain Disorders, Aging, Neurodegenerative, Acquired Cognitive Impairment, Parkinson's Disease, 2.1 Biological and endogenous factors, Aetiology, Neurological, Medical and Health Sciences, Immunology
Abstract

Progress in neurodegenerative disease research is hampered by the lack of biomarkers of neuronal dysfunction. We here identified a class of cerebrospinal fluid-based (CSF-based) kinetic biomarkers that reflect altered neuronal transport of protein cargo, a common feature of neurodegeneration. After a pulse administration of heavy water (2H2O), distinct, newly synthesized 2H-labeled neuronal proteins were transported to nerve terminals and secreted, and then appeared in CSF. In 3 mouse models of neurodegeneration, distinct 2H-cargo proteins displayed delayed appearance and disappearance kinetics in the CSF, suggestive of aberrant transport kinetics. Microtubule-modulating pharmacotherapy normalized CSF-based kinetics of affected 2H-cargo proteins and ameliorated neurodegenerative symptoms in mice. After 2H2O labeling, similar neuronal transport deficits were observed in CSF of patients with Parkinson's disease (PD) compared with non-PD control subjects, which indicates that these biomarkers are translatable and relevant to human disease. Measurement of transport kinetics may provide a sensitive method to monitor progression of neurodegeneration and treatment effects.

Published
2012

2. Measurement of reverse cholesterol transport pathways in humans: in vivo rates of free cholesterol efflux, esterification, and excretion.

Author

Turner, Scott, Voogt, Jason, Davidson, Michael, Glass, Alex, Killion, Salena, Decaris, Julie, Mohammed, Hussein, Minehira, Kaori, Boban, Drina, Murphy, Elizabeth, Luchoomun, Jayraz, Awada, Mohamad, Neese, Richard, and Hellerstein, Marc

Subjects
cholesterol efflux, esterification, isotope labeling, stable, reverse cholesterol transport, sterol excretion, isotope labeling, stable, Cardiorespiratory Medicine and Haematology
Abstract

BackgroundReverse cholesterol transport from peripheral tissues is considered the principal atheroprotective mechanism of high-density lipoprotein, but quantifying reverse cholesterol transport in humans in vivo remains a challenge. We describe here a method for measuring flux of cholesterol though 3 primary components of the reverse cholesterol transport pathway in vivo in humans: tissue free cholesterol (FC) efflux, esterification of FC in plasma, and fecal sterol excretion of plasma-derived FC.Methods and resultsA constant infusion of [2,3-(13)C(2)]-cholesterol was administered to healthy volunteers. Three-compartment SAAM II (Simulation, Analysis, and Modeling software; SAAM Institute, University of Washington, WA) fits were applied to plasma FC, red blood cell FC, and plasma cholesterol ester (13)C-enrichment profiles. Fecal sterol excretion of plasma-derived FC was quantified from fractional recovery of intravenous [2,3-(13)C(2)]-cholesterol in feces over 7 days. We examined the key assumptions of the method and evaluated the optimal clinical protocol and approach to data analysis and modeling. A total of 17 subjects from 2 study sites (n=12 from first site, age 21 to 75 years, 2 women; n=5 from second site, age 18 to 70 years, 2 women) were studied. Tissue FC efflux was 3.79±0.88 mg/kg per hour (mean ± standard deviation), or ≍8 g/d. Red blood cell-derived flux into plasma FC was 3.38±1.10 mg/kg per hour. Esterification of plasma FC was ≍28% of tissue FC efflux (1.10±0.38 mg/kg per hour). Recoveries were 7% and 12% of administered [2,3-(13)C(2)]-cholesterol in fecal bile acids and neutral sterols, respectively.ConclusionsThree components of systemic reverse cholesterol transport can be quantified, allowing dissection of this important function of high-density lipoprotein in vivo. Effects of lipoproteins, genetic mutations, lifestyle changes, and drugs on these components can be assessed in humans. (J Am Heart Assoc. 2012;1:e001826 doi: 10.1161/JAHA.112.001826.).

Published
2012

3. Inhibition of intestinal cholesterol absorption with ezetimibe increases components of reverse cholesterol transport in humans

Author

Davidson, Michael H., primary, Voogt, Jason, additional, Luchoomun, Jayraz, additional, Decaris, Julie, additional, Killion, Salena, additional, Boban, Drina, additional, Glass, Alexander, additional, Mohammad, Hussein, additional, Lu, Yun, additional, Villegas, Deona, additional, Neese, Richard, additional, Hellerstein, Marc, additional, Neff, David, additional, Musliner, Thomas, additional, Tomassini, Joanne E., additional, and Turner, Scott, additional

Published
2013
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