Abstract
The severity of poisoning following acetylcholinesterase (AChE) inhibition correlates weakly with total AChE activity. This may be partly due to the existence of functional and non-functional pools of AChE. AChE consists of several molecular forms. The aim of the present study was to investigate which of these forms will correlate best with neuromuscular transmission (NMT) remaining after partial inhibition of this enzyme. Following sublethal intoxication of rats with the irreversible AChE inhibitor soman, diaphragms were isolated after 0.5 or 3 h. It appeared that at 3 h after soman poisoning the percentage of G1 increased, while those of G4 and A12 decreased. NMT was inhibited more strongly than in preparations obtained from the 0.5 h rats with the same level of AChE inhibition, but with a normal ratio of molecular forms. NMT correlated positively with G4 as well as with A12, but inversely with G1. In vitro inhibition with the charged inhibitors DEMP and echothiophate resulted in higher levels of total AChE, relatively less G1 and more G4 and A12 than after incubation with soman, but led to less NMT. Treatment of soman-intoxicated rats with the reactivating compound HI-6 resulted in preferential reactivation of A12, persisting low levels of G1 and concurrent recovery of NMT as compared with saline-treated soman controls with equal total AChE activity. Apparently, in rat diaphragm G4 and A12 are the functional AChE forms.
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DeWilde, V., Vogelaers, D., and Colardyn, F. 1990. Prompt recovery from severe cholinesterase-inhibitor poisoning remarks on classification and therapy of organophosphate poisoning. Klin. Wochenschr., 68:615–618.
Hobbiger, F. 1976. Pharmacology of anticholinesterase drugs. Pages 503–508,in Zaimis E. (ed.), Neuromuscular Junction, Springer-Verlag, Berlin.
Van Dongen, C. J., Valkenburg, P. W., and Van Helden, H. P. M. 1988. Contribution of de novo synthesis of acetylcholinesterase to spontaneous recovery of neuromuscular transmission following soman intoxication. Eur. J. Pharmacol., 149:381–4.
Melchers, B. P. C., and Van Helden, H. P. M. 1990. On the development of behavioral tolerance to organophosphates II Neurophysiological aspects. Pharmacol. Biochem. Behav. 35:321–325.
Van Dongen, C. J., and Wolthuis, O. L. 1989. On the development of behavioral tolerance to organophosphates I: Behavioral and biochemical aspects. Pharmacol. Biochem. Behav., 34:473–481.
Clement, J. G. 1993. Pharmacological nature of soman-induced hypothermia in mice. Pharmacol. Biochem. Behav., 44:689–702.
Clement, J. G., Shiloff, J. D., and Gennings, C. 1987. Efficacy of a combination of acetylcholinesterase reactivators, HI-6 and obidoxime, against tabun and soman poisoning of mice. Arch. Toxicol., 61:70–75.
Clement, J. G. 1989. Survivors of soman poisoning: recovery of the soman LD50 to control value in the presence of extensive acetylcholinesterase inhibition. Arch. Toxicol., 63:150–154.
Jimmerson, V. R., Shih, T.-M., and Mailman, R. B. 1989. Variability in soman toxicity in the rat: correlation with biochemical and behavioral measures. Toxicology, 57:214–254.
McIsaac, R. J., and Koelle, G. B. 1959. Comparison of the effects of inhibition of external, internal and total acetylcholinesterase upon ganglionic transmission. J. Pharmacol. Exp. Ther. 126:9–20.
Mittag, T. W., Ehrenpreis, S., and Hehir, R. M. 1971. Functional acetylcholinesterase of rat diaphragm muscle. Biochem. Pharmacol., 20:2263–2273.
Massouilié, J., and Bon, S. 1982. The molecular forms of cholinesterase and acetylcholinesterase in vertebrates. Ann. Rev. Neurosci. 5:57–106.
Inestrosa, N. C., and Perelman, A. 1989. Distribution and anchoring of molecular forms of acetylcholinesterase. TIPS, 10:325–329.
Siripholvat, V., Watanabe, T., and Tomita, T. 1988. Histochemical and cytochemical localization of acetylcholinesterase in the cerebellar cortex of the chicken. Jikken Dobutsu, 37:437–446.
Fernandez, H. L., Inestrosa, N. C., and Stiles, J. R. 1984. Subcellular localization of acetylcholinesterase molecular forms in endplate regions of adult mammalian skeletal muscle. Neurochem. Res., 9:1211–1230.
Fernandez, H. L., and Hodges-Savola, C. A. 1992. Trophic regulation of acetylcholinesterase isoenzymes in adult mammalian skeletal muscle. Neurochem. Res. 17:115–124.
Fernandez, H. L., and Stiles, J. R. 1984. Intra- versus extracellular recovery of 16S acetylcholinesterase following organophosphate inactivation in the rat. Neurosci. Lett., 49:117–122.
Younkin, S. G., Rosenstein, C., Collins, P. L., and Rosenberry, T. L. 1982. Cellular localization of the molecular forms of acetylcholinesterase in rat diaphragm. J. Biol. Chem., 257:13630–13637.
Ellman, G. I., Courtney, K. D., Andres, Jr. V., and Featherstone R. M. 1961. A new and rapid colorimetric determination of acetylcholinesterase activity. Biochem. Pharmacol., 7:88–95.
Van Helden, H. P. M., De Lange, J., Busker, R. W., and Melchers, B. P. C. 1991. Therapy of organophosphate poisoning in the rat by direct effects of oximes unrelated to cholinesterase reactivation. Arch. Toxicol., 65:586–593.
Meeter, E., and Wolthuis, O. L. 1986. The spontaneous recovery of respiration and neuromuscular transmission in the rat after anticholinesterase poisoning. Eur. J. Pharmacol. 2:377–386.
Van Helden, H. P. M., Van der Wiel, H. J., De Lange, J., Busker, R. W., Melchers, B. P. C., and Wolthuis, O. L. 1992. Therapeutic efficacy of HI-6 in soman-poisoned marmoset monkeys. Toxicol. Appl. Pharmacol., 115:50–56.
Brimijoin, S., and Carter, J. 1982. Turnover of the molecular forms of acetylcholinesterase in the rat diaphragm. J. Neurochem. 38:588–59.
Tattersall, J. E. H. 1990. Effects of organophosphorus anticholinesterases on nicotinic receptor ion channels at adult mouse muscle endplates. Br. J. Pharmacol., 101:349–357.
Clement, J. G., Rosario, S., Bessette, E., and Erhardt, N. 1991. Soman and sarin inhibition of molecular forms of acetylcholinesterase in mice—time course of recovery and reactivation by the oxime HI-6. Biochem. Pharmacol., 42:329–335.
Fernandez, H. L., Duell, M. J., and Festoff, B. W. 1979. Neurotrophic control of 16S acetylcholinesterase at the vertebrate neuromuscular junction. J. Neurobiol., 10:441–454.
Fernandez, H. L., and Donoso, J. A. 1988. Exercise selectively increases G4 acetylcholinesterase activity in fast-twitch muscle. J. Appl. Physiol., 65:2245–2252.
Jasmin, B. J., Gardiner, P. F., and Gisiger, V. 1991. Muscle acetylcholinesterase adapts to compensatory overload by a general increase in its molecular forms. J. Appl. Physiol., 70:2485–2489.
Gisiger, V., Sherker, S., and Gardiner, P. F. 1991. Swimming training increases the G4 acetylcholinesterase content of both fast ankle extensors and flexors. FEBS Lett., 278:271–273.
Gregory, E. J., Hodges-Savola, C. A., and Fernandez, H. L. 1989. Selective increase of tetrameric (G4) acetylcholinesterase activity in rat hindlimb skeletal muscle following short-term denervation. J. Neurochem., 53:1411–1418.
Glantz, S. A., 1989. Primer of biostatistics. Pages 230–236, McGraw-Hill, Singapore.
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Busker, R.W., Zijlstra, J.J., van der Wiel, H.J. et al. The functional role of molecular forms of acetylcholinesterase in neuromuscular transmission. Neurochem Res 19, 713–719 (1994). https://doi.org/10.1007/BF00967711
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DOI: https://doi.org/10.1007/BF00967711