Abstract
This study compares early and late effects of the injection of hyperosmolar NaCl and urea of equal osmolarity on selected aspects of brain water, electrolyte, carbohydrate, amino acid, urea, and energy metabolism in normal suckling-weanling mice. One hour after treatment, salt-treated mice were critically ill, while the behavior of urea-treated animals could not be distinguished from that of controls. This clinical difference could not be explained on the basis of differences in plasma osmolality, the brain water content, or the degree of hemorrhagic encephalopathy. The injection of NaCl induced a 14-fold increase in plasma insulin and a progressive fall in the plasma glucose concentration (a reduction of 66% at 1 hr). In contrast, plasma glucose levels in urea-injected mice were unchanged. Prior to the fall in plasma glucose levels, metabolite changes in the brains of NaCl-injected mice were compatible with facilitation of transfer of glucose from the blood to the brain, increased metabolic flux in the Embden-Meyerhof and Krebs citric acid cycle pathways, and increased energy production. With the exception of the glucose content (unchanged), similar metabolite changes were seen in brain soon after urea injection. In the brains of the hypoglycemic NaCl-treated mice, glucose levels were reduced 80%, and glycogen 41%. Other metabolite changes were compatible with decreased glycolysis and metabolic flux through the Krebs citric acid cycle. In contrast, with few exceptions, at a similar time after injection, metabolite levels had returned to normal in the urea-treated mice. Permeability of the brain to urea was also examined. Brain urea reached high levels at 2hr but returned to near baseline at 6hr. Both hyperosmolar solutions increased the brain content of aspartic and glutamic acids 1 hr after injection. The failure of hypoglycemic mice with hypernatremia and elevated plasma osmolality (range, 416–434 mOsm/kg H2O) to respond to 1M glucose (30ml/kg) may have been due to the ill effects of the additional hyperosmolar load. The possibility remains that the encephalopathy induced by hyperosmolar NaCl, but not by hyperosmolar urea, is in some way related to the sudden elevation of brain Na+ and/or Cl− ions.
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References
Atkinson, D. E. (1968). The energy charge of the adenylate pool as a regulatory parameter. Interaction with feedback modifiers.Biochemistry 7: 4030–4034.
Baethmann, A., and Van Harreveld, A. (1973). Water and electrolyte distribution in gray matter rendered edematous with a metabolic inhibitor.J. Neuropathol. Exp. Neural. 32: 408–123.
Bradbury, M. W. B., and Coxon, R. V. (1962). The penetration of urea into the central nervous system at high blood levels.J. Physiol. 163: 423–435.
Broman, T., and Lindberg-Broman, A. M. (1945). An experimental study of disorders in the permeability of the cerebral vessels (“the blood-brain-barrier”) produced by chemical and physico-chemical agents.Acta Physiol. Scand. 10: 102–125.
Cameron, J. M., and Dayan, A. D. (1966). Association of brain damage with therapeutic abortion induced by amniotic-fluid replacement: Report of two cases.Br. Med. J. 1: 1010–1013.
Chan, P. H., and Fishman, R. A. (1979). Elevation of rat brain amino acids, ammonia and idiogenic osmoles induced by hyperosmolality.Brain Res. 161: 293–301.
Clark, K., and Einspruch, B. C. (1962). Lowering of intracranial pressure with urea.Arch. Neural. 6: 414–418.
Clausen, T. (1968). The relationship between the transport of glucose and cations across cell membranes in isolated tissues. III. Effect of Na+ and hyperosmolarity on glucose metabolism and insulin responsiveness in isolated rat hemidiaphragm.Biochim. Biophys. Acta 150: 56–65.
Curtis, D. R., and Johnston, G. A. R. (1970). Amino acid transmitters. In Lajtha, A. (ed.),Handbook of Neurochemistry, Plenum Press, New York, Vol. 4, pp 115–134.
DeGenaro, F., and Nyhan, W. L. (1971). Salt-a dangerous “antidote”.J. Pediat. 78: 1048–1049.
Dodge, P. R., Sotos, J. F., and Karlsson, B. (1961). Influence of hypertonicity of the body fluids on the blood-brain barrier.Trans. Am. Neural. Assoc. 86: 12–16.
Dodge, P. R., Sotos, J. F., Gamstorp, I., DeVivo, D., Levy, M., and Rabe, T. (1962). Neurophysiologic disturbances in hypertonic dehydration.Trans. Am. Neurol. Assoc. 87: 33–36.
Duffy, T. E., Nelson, S. R., and Lowry, O. H. (1972). Cerebral carbohydrate metabolism during acute hypoxia and recovery.J. Neurochem. 19: 959–977.
Elton, N. W., Elton, W. J., and Nazareno, J. P. (1963). Pathology of acute salt poisoning in infants.Am. J. Clin. Pathol. 39: 252–264.
Fawcett, J. K., and Scott, J. E. (1960). A rapid and precise method for the determination of urea.J. Clin. Pathol. 13, 156–159.
Ferrendelli, J. A., and Chang, M.-M. (1973). Brain metabolism during hypoglycemia: Effect of insulin on regional central nervous system glucose and energy reserves in mice.Arch. Neurol. 28: 173–177.
Finberg, L., Luttrell, C., and Redd, H. (1959). Pathogenesis of lesions in the nervous system in hypernatremic states. II. Experimental studies of gross anatomic changes and alterations of chemical composition of the tissues.Pediatrics 23: 46–53.
Finberg, L., Kiley, J., and Luttrell, C. N. (1963). Mass accidental salt poisoning in infancy.JAMA 184: 187–190.
Fishman, R. A., and Chan, P. H. (1976). Changes in ammonia and amino acid metabolism induced by hyperosmolality in vivo and in vitro.Trans. Am. Neurol. Assoc. 101: 34–39.
Fishman, R. A., Reiner, M., and Chan, P. H. (1977). Metabolic changes associated with iso-osmotic regulation in brain cortex slices.J. Neurochem. 28: 1061–1067.
Goldberg, N. D., Passonneau, J. V., and Lowry, O. H. (1966). Effects of changes in brain metabolism on the levels of citric acid cycle intermediates.J. Biol. Chem. 241: 3997–003.
Goldstein, S. L., Himwich, W. A., Knapp, F. M., and Rovine, B. W. (1964). Effects of urea and other dehydrating agents upon dog brain.J. Neurosurg. 21: 672–677.
Gorell, J. M., Law, M. M., Lowry, O. H., and Ferrendelli, J. A. (1977). Levels of cerebral cortical, glycolytic and citric acid cycle metabolites during hypoglycemie stupor and its reversal.J. Neurochem. 29: 187–191.
Hirsch, H. E., and Robins, E. (1962). Distribution of γ-aminobutyric acid in the layers of the cerebral and cerebellar cortex. Implications for its physiological role.J. Neurochem. 9: 63–70.
Holliday, M. A., Kalayci, M. N., and Harrah, J. (1968). Factors that limit brain volume changes in response to acute and sustained hyper- and hyponatremia.J. Clin. Invest. 47: 1916–1928.
Howse, D. C., and Duffy, T. E. (1975). Control of the redox state of the pyridine nucleotides in the rat cerebral cortex. Effect of electroshock-induced seizures.J. Neurochem. 24: 935–940.
Javid, M., Gilboe, D., and Cesario, T. (1964). The rebound phenomenon and hypertonic solutions.J. Neurosurg. 21: 1059–1066.
Katzman, R., and Pappius, H. M. (1973)Brain Electrolytes and Fluid Metabolism, Williams and Wilkins, Baltimore.
Lambert, A. E. (1976). The regulation of insulin secretion.Rev. Physiol. Biochem. Pharmacol. 75: 95–158.
Lockwood, A. H. (1975). Acute and chronic hyperosmolality. Effects on cerebral amino acids and energy metabolism.Arch. Neurol. 32: 62–64.
Lowry, O. H., and Passonneau, J. V. (1972).A Flexible System of Enzymatic Analysis, Academic Press, New York, pp. 121–128 and 146–218.
Lowry, O. H., Passonneau, J. V., Hasselberger, F. X., and Schulz, D. W. (1964). Effect of ischemia on known substrates and cofactors of the glycolytic pathway in brain.J. Biol. Chem. 239: 18–30.
Lund-Andersen, H., Kjeldsen, C. S., Hertz, L., and Brondsted, H. E. (1976). Uptake of glucose analogues by rat brain cortex slices: Na+-independent membrane transport.J. Neurochem. 27: 369–373.
Luttrell, C. N., and Finberg, L. (1958). Clinical, pathological and biochemical features of experimental hypernatremic encephalopathy.Trans. Am. Neural. Assoc. 83: 127–132.
Luttrell, C. N., and Finberg, L. (1959). Hemorrhagic encephalopathy induced by hypernatremia, I. Clinical, laboratory and pathological observations.Arch. Neural. Psych. 81: 424–432.
Luttrell, C. N., Finberg, L., and Drawdy, L. P. (1959). Hemorrhagic encephalopathy induced by hypernatremia. II. Experimental observations on hyperosmolarity in cats.Arch. Neurol. 1: 153–160.
Malaisse, W. J. (1975). Role of cations. In Hasselblatt, A., and von Bruchausen, F. (eds.),Handbook of Experimental Pharmacology. Insulin II, Springer-Verlag, New York, Vol. 32, Part 2, pp. 145–156.
Mayman, C. I., Gatfield, P. D., and Breckenridge, B. M. (1964). The glucose content of brain in anaesthesia.J. Neurochem. 11: 483–487.
Morgan, C. R., and Lazarow, A. (1963). Immunoassay of insulin: Two antibody system. Plasma insulin levels of normal, subdiabetic and diabetic rats.Diabetes 12: 115–126.
Morris-Jones, P. H., Houston, I. B., and Evans, R. C. (1967). Prognosis of the neurologic complications of acute hypernatremia.Lancet 2: 1385–1389.
Orr, H. T., Cohen, A. L., and Lowry, O. H. (1976). The distribution of taurine in the vertebrate retina.J. Neurochem. 26: 609–611.
Pappius, H. M., Savaki, H. E., Fieschi, C., Rapoport, S. I., and Sokoloff, L. (1979). Osmotic opening of the blood-brain barrier and local cerebral glucose utilization.Ann. Neurol. 5: 211–219.
Passonneau, J. V., and Lauderdale, V. R. (1974). A comparison of three methods of glycogen measurement in tissues.Anal. Biochem. 60: 404–412.
Pickel, S., Anderson, C., and Holliday, M. A. (1970). Thirsting and hypernatremic dehydration-a form of child abuse.Pediatrics 45: 54–59.
Sotos, J. F., Dodge, P. R., Meara, P., and Talbdt, N. B. (1960). Studies in experimental hypertonicity. I. Pathogenesis of the clinical syndrome, biochemical abnormalities and cause of death.Pediatrics 26: 925–938.
Stevenson, R. E., and Bowyer, F. P. (1970). Hyperglycemia with hyperosmolal dehydration in nondiabetic infants.J. Pediat. 77: 818–823.
Thurston, J. H., Hauhart, R. E., Jones, E. M., and Ater, J. L. (1975a). Effects of salt and water loading on carbohydrate and energy metabolism and levels of selected amino acids in the brains of young mice.J. Neurochem. 24: 953–957.
Thurston, J. H., Hauhart, R. E., Jones, E. M., and Ater, J. L. (1975b). Effects of alloxan diabetes, anti-insulin serum diabetes, and non-diabetic dehydration on brain carbohydrate and energy metabolism in young mice.J. Biol. Chem. 250: 1751–1758.
Thurston, J. H., Hauhart, R. E., and Dirgo, J. A. (1976). Insulin and brain metabolism. Absence of direct action of insulin on K+ and Na+ transport in mouse brain.Diabetes 25: 758–763.
Thurston, J. H., Hauhart, R. E., and Dirgo, J. A. (1980). Taurine: A role in osmotic regulation of mammalian brain and possible clinical significance.Life Sci. 26: 1561–1568.
Thurston, J. H., Hauhart, R. E., and Dirgo, J. A. (1981). Effects of a single therapeutic dose of glycerol on cerebral metabolism in the brains of young mice. Possible increase in brain glucose transport and glucose utilization.J. Neurochem. 36: 830–838.
Thurston, J. H., Hauhart, R. E., and Schulz, D. W. (1983). Effect of chronic hypernatremic dehydration and rapid rehydration on brain carbohydrate, energy, and amino acid metabolism in weanling mice.J. Neurochem. 40: 240–245.
Tukey, J. W. (1953).The Problem of Multiple Comparisons, Ditto, Princeton University, Princeton, N.J.; Cited by Kirk, R. E. (1968).Experimental Design: Procedures for the Behavioral Sciences, Brooks/Cole, Belmont, Calif., pp. 69–98.
Wagatsuma, T. (1965). Intra-amniotic injection of saline for therapeutic abortion.Am. J. Obstet. Gynecol. 5: 743–745.
Ward, D. J. (1963). Fatal hypernatremia after a saline emetic.Br. Med. J. 2: 432.
Williamson, D. H., Mellanby, J., and Krebs, H. A. (1962). Enzymatic determination of D(-)-β-hydroxybutyric acid and acetoacetic acid in blood.Biochem. J. 82: 90–96.
Young, R. L., and Lowry, O. H. (1966). Quantitative methods for measuring the histochemical distribution of alanine, glutamate and glutamine in brain.J. Neurochem. 13: 785–793.
Young, R. S. K., and Truax, B. T. (1979). Hypernatremic hemorrhagic encephalopathy.Ann. Neurol. 5: 588–591.
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Thurston, J.H., Hauhart, R.E., Dirgo, J.A. et al. Effects of acute hyperosmolar NaCl or urea on brain H2O, Na+, K+, carbohydrate, and amino acid metabolism in weanling mice: NaCl induces insulin secretion and hypoglycemia. Metab Brain Dis 1, 129–146 (1986). https://doi.org/10.1007/BF00999383
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DOI: https://doi.org/10.1007/BF00999383