Abstract

Hyperammonemia causes glial swelling, increased intracranial pressure, impaired cerebrovascular responses to CO2, and altered brain electrical function. This proposal examines the hypothesis that glial swelling plays a prominent role in the aforementioned physiological abnormalities found in hyperammonemic states. It is further proposed that glial swelling is a consequence of the osmotic effect of the accumulation of intracellular free glutamine in glia, where glutamine synthetase activity is high. Glial swelling and glutamine accumulation may be responsible for physiological abnormalities by one or both of two potential mechanisms. By virtue of its relationship to the microcirculation, glial swelling may directly affect control of the vasculature. By virtue of its role in the regulation of the extracellular ionic environment, glial abnormalities may affect electrical activity and vascular responsivity. To test these hypotheses, a series of experiments are designed to compare the consequences of hyperammonemia in control animals with those pretreated with methionine sulfoximine (MSO), a potent glutamine synthetase inhibitor; this will permit evaluation of hyperammonemia in the presence and absence of brain glutamine accumulation. Specifically, we will determine if the increase in brain water and intracranial pressure, and the impaired cerebrovascular reactivity and brain electrical function are prevented during hyperammonemia when animals are pretreated with MSO. The gradual development of moderate hyperammonemia over a 72 hour period will be investigated by intraperitoneal infusion of urease in dogs. By evaluating the cerebrovascular responses to hypercapnia, hypocapnia, hypoxia, and increases and decreases in perfusion pressure, we will demonstrate whether hyperammonemia produces a generalized depression of vascular reactivity or if the depression is specific for a particular vasodilator or vasoconstrictor stimulus. By measuring pial arteriole diameter, we will show whether extraparenchymal vessels not surrounded by glia lose reactivity in the same fashion as the total cerebrovascular network. We will then demonstrate if alterations in extracellular fluid composition are responsible for altered reactivity. This proposal will incorporate existing biochemical evidence into an integrative physiological explanation of the cerebrovascular abnormalities which occur in experimental and clinical hyperammonemic states.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
5P01NS020020-07
Application #
3882284
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
7
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Fonken, Laura K; Gaudet, Andrew D; Gaier, Kristopher R et al. (2016) MicroRNA-155 deletion reduces anxiety- and depressive-like behaviors in mice. Psychoneuroendocrinology 63:362-9
Ni, Xinli; Yang, Zeng-Jin; Wang, Bing et al. (2012) Early antioxidant treatment and delayed hypothermia after hypoxia-ischemia have no additive neuroprotection in newborn pigs. Anesth Analg 115:627-37
Ni, Xinli; Yang, Zeng-Jin; Carter, Erin L et al. (2011) Striatal neuroprotection from neonatal hypoxia-ischemia in piglets by antioxidant treatment with EUK-134 or edaravone. Dev Neurosci 33:299-311
Woodworth, K Nina; Palmateer, Julie; Swide, Joseph et al. (2011) Short- and long-term behavioral effects of exposure to 21%, 40% and 100% oxygen after perinatal hypoxia-ischemia in the rat. Int J Dev Neurosci 29:629-38
Yang, Sufang; Abrahams, Matthew S; Hurn, Patricia D et al. (2011) Local anesthetic Schwann cell toxicity is time and concentration dependent. Reg Anesth Pain Med 36:444-51
Nakano, Takaaki; Hurn, Patricia D; Herson, Paco S et al. (2010) Testosterone exacerbates neuronal damage following cardiac arrest and cardiopulmonary resuscitation in mouse. Brain Res 1357:124-30
Yang, Zeng-Jin; Carter, Erin L; Torbey, Michel T et al. (2010) Sigma receptor ligand 4-phenyl-1-(4-phenylbutyl)-piperidine modulates neuronal nitric oxide synthase/postsynaptic density-95 coupling mechanisms and protects against neonatal ischemic degeneration of striatal neurons. Exp Neurol 221:166-74
Ohata, Hiroto; Gebremedhin, Debebe; Narayanan, Jayashree et al. (2010) Onset of pulmonary ventilation in fetal sheep produces pial arteriolar constriction dependent on cytochrome p450 omega-hydroxylase activity. J Appl Physiol 109:412-7
Zhu, W; Wang, L; Zhang, L et al. (2010) Isoflurane preconditioning neuroprotection in experimental focal stroke is androgen-dependent in male mice. Neuroscience 169:758-69
McCullough, Louise D; Koerner, Ines P; Hurn, Patricia D (2009) Effects of gender and sex steroids on ischemic injury. Handb Clin Neurol 92:149-69

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