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Featured researches published by Judith A. Barry.


Biochimie | 1992

In vivo31P NMR study of early cellular responses to hyperosmotic shock in cultured glioma cells

Y.H.H. Lien; H.Z. Zhou; C. Job; Judith A. Barry; Robert J. Gillies

Cell volume regulation in the face of osmotic stress is a fundamental homeostatic activity, and is most critical in brain, which is spatially constrained. Despite the importance of this phenomenon, little is known about volume regulation in the brain, primarily because of the cellular heterogeneity in the tissue. We describe here simultaneous in vivo 31P nuclear magnetic resonance (NMR) measurements of cell volume, intracellular pH and phosphate metabolites during early responses to hyperosmotic stress in C6 glioma cells perfused in NMR-compatible bioreactors. Cell volume was measured using dimethyl methylphosphonate (DMMP) as a probe which has an intracellular NMR resonance shifted upfield from the extracellular resonance. The sensitivity of these measurements allowed 31P NMR spectra to be collected every 30 s. Following an increase in osmolarity from 320 to 480 mOsm by addition of NaCl to the perfusate, C6 glioma cells shrank to 67% of their original volume. We also observed a simultaneous increase of intracellular pH coincident with the decrease in cell volume. The signals from ATP decreased by 10%, but those from phosphocreatine (PCr) increased by 31% after hyperosmotic shock. However, correcting the ATP signals for the decrease in cell volume indicated that its intracellular concentrations increased after treatment. Signals from glycerophosphorylcholine (GPC) and glycerophosphorylethanolamine (GPE) were not changed significantly. This is the first in vivo report of early cellular responses monitored by NMR spectroscopy following hyperosmotic shock in cultured cells.


Biochemistry | 1994

Direct NMR evidence for ethanol binding to the lipid-water interface of phospholipid bilayers.

Judith A. Barry; Klaus Gawrisch


Magnetic Resonance in Medicine | 1994

In vitro and in vivo 13C and 31P NMR analyses of phosphocholine metabolism in rat glioma cells.

Robert J. Gillies; Judith A. Barry; Brian D. Ross


Biochemistry | 1992

Photoinduced destabilization of liposomes

Henry Lamparski; Ulrich Liman; Judith A. Barry; David A. Frankel; Varadarajan Ramaswami; Michael F. Brown; David F. O'Brien


Biochemistry | 1995

Effects of Ethanol on Lipid Bilayers Containing Cholesterol, Gangliosides, and Sphingomyelin

Judith A. Barry; Klaus Gawrisch


Biochemistry | 1991

Low-temperature 2H NMR spectroscopy of phospholipid bilayers containing docosahexaenoyl (22:6ω3) chains

Judith A. Barry; Theodore P. Trouard; Amir Salmon; Michael F. Brown


The Journal of Physical Chemistry | 1992

Deuterium NMR study of intermolecular interactions in lamellar phases containing palmitoyllysophosphatidylcholine

Mikael Jansson; Robin L. Thurmond; Judith A. Barry; Michael F. Brown


Biochemistry | 1993

Dimethyl methylphosphonate (DMMP) : a 31P nuclear magnetic resonance spectroscopic probe of intracellular volume in mammalian cell cultures

Judith A. Barry; Kathy Ann McGovern; Yeong Hau H. Lien; Brian Ashmore; Robert J. Gillies


Biochemistry | 1992

31P NMR and X-ray Diffraction Study of the Effect of Photopolymerization on Lipid Polymorphism+

Judith A. Barry; Henry Lamparski; Erramilli Shyamsunder; Fredrik Osterberg; John Cerne; Michael F. Brown; David F. O'Brien


Biochemistry | 1992

Correction - Low-Temperature 2H NMR Spectroscopy of Phospholipid Bilayers Containing Docosahexenoyl (22:6ι3) Chains.

Judith A. Barry; Theodore P. Trouard; Amir Salmon; Michael F. Brown

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Klaus Gawrisch

National Institutes of Health

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Robert J. Gillies

University of South Florida

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C. Job

University of Arizona

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