Abstract

Alterations in cerebral function and levels of consciousness occur in certain metabolic diseases where changes in circulating substrates and hormones influence the synthesis and turnover of brain neurotransmitters. The pathophysiologic mechanisms responsible for cerebral dysfunction in these metabolic encephalopathies remain to be clarified. There have been several important technical advances in recent years which will permit further progress in the study of these diseases. Current hypotheses of the etiology of metabolic encephalopathy have tended to focus only on isolated facets of the disease. But the multifactorial nature of metabolic encephalopathy suggests that the most productive approach to elucidating its etiology will be to integrate the various abnormalities which have been described. Correlation of alterations in neurotransmitter metabolism and distribution, receptor density and distribution, protein synthesis, and cerebral function, at different stages of the disease may reveal crucial steps in the development of encephalopathy that might remain obscure in studies of single variables at isolated time points. Accordingly, the goals of this proposal will emphasize the following aspects: the identification of those biochemical, physiologic and structural changes which are important in causing alterations in consciousness in metabolic disease, followed by the determination of any etiologic factors common to various metabolic encephalopathies (e.g., hepatic, uremic and diabetic). Encephalopathy caused by portal-systemic shunting will be studied first. Regional localization of neurotransmitters and their metabolism will be related to the functional stages of metabolic encephalopathy. Regional glucose use will be measured by quantitative autoradiography and used as an index of cerebral function. Regional brain content of major neurotransmitters and their metabolites will be determined by high performance liquid chromatography. Distribution of their receptors will be evaluated by quantitative autoradiography. A method for measuring the regional rate of ammonia metabolism will be developed and validated. Amino acid profiles in blood and brain, which may effect neurotransmitter metabolism, will be measured concurrently. Subsequently studies will be extended to models of uremic and diabetic encephalopathy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS016389-11
Application #
3396859
Study Section
Neurology A Study Section (NEUA)
Project Start
1988-07-01
Project End
1992-06-30
Budget Start
1991-07-01
Budget End
1992-06-30
Support Year
11
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Rosalind Franklin University
Department
Type
Schools of Medicine
DUNS #
069501252
City
North Chicago
State
IL
Country
United States
Zip Code
60064

  Publications

Lee, W J; Hawkins, R A; Vina, J R et al. (1998) Glutamine transport by the blood-brain barrier: a possible mechanism for nitrogen removal. Am J Physiol 274:C1101-7
Hawkins, P A; DeJoseph, M R; Hawkins, R A (1998) Diurnal rhythm returns to normal after elimination of portacaval shunting. Am J Physiol 274:E426-31
Hawkins, P A; DeJoseph, M R; Vina, J R et al. (1996) Comparison of the metabolic disturbances caused by end-to-side and side-to-side portacaval shunts. J Appl Physiol 80:885-91
Hawkins, P A; DeJoseph, M R; Hawkins, R A (1996) Reversal of portacaval shunting normalizes brain energy consumption in most brain structures. Am J Physiol 271:E1015-20
Hawkins, P A; DeJoseph, M R; Hawkins, R A (1996) Eliminating metabolic abnormalities of portacaval shunting by restoring normal liver blood flow. Am J Physiol 270:E1037-42
Sanchez del Pino, M M; Hawkins, R A; Peterson, D R (1995) Biochemical discrimination between luminal and abluminal enzyme and transport activities of the blood-brain barrier. J Biol Chem 270:14907-12
Sanchez del Pino, M M; Peterson, D R; Hawkins, R A (1995) Neutral amino acid transport characterization of isolated luminal and abluminal membranes of the blood-brain barrier. J Biol Chem 270:14913-8
Hawkins, R A; Mans, A M (1994) Brain metabolism in encephalopathy caused by hyperammonemia. Adv Exp Med Biol 368:11-21
Hawkins, R A; Jessy, J; Mans, A M et al. (1994) Neomycin reduces the intestinal production of ammonia from glutamine. Adv Exp Med Biol 368:125-34
Hawkins, R A; Hawkins, P A; Mans, A M et al. (1994) Optimizing the measurement of regional cerebral glucose consumption with [6-14C]glucose. J Neurosci Methods 54:49-62

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