Abstract
The objective of this study was to determine the subcellular origin of cholinergic transmitter released spontaneously from mouse forebrain minces. To accomplish this objective, minces were pretreated in ionic media and then loaded with [14C]homocholine, an analog of choline, to form the false transmitter [14C]acetylhomocholine ([14C]AHCh). The ratio of the false transmitter [14C]AHCh to the true transmitter ACh was then used as an index of cholinergic transmitter contents for both the cytoplasmic (S3) and vesicle-bound (P3) fractions. Three different pretreatment procedures were used to cause the following changes in S3 and P3 false to true transmitter ratios prior to spontaneous release: 1) a small increase in the S3 ratio of [14C]AHCh to acetylcholine (ACh) and a large increase in the P3 ratio of [14C]AHCh to ACh; 2) a decrease in the S3 ratio of [14C]AHCh to ACh and an increase in the P3 ratio of [14C]AHCh to ACh; 3) an increase in the P3 ratio of [14C]AHCh to ACh without affecting the S3 ratio of [14C]AHCh to ACh. The influence of each pretreatment on these subcellular ratios was then compared with its influence on the spontaneous release ratio of [14C]AHCh to ACh. In all 3 instances, the influence of pretreatment on the ratio of spontaneously released false and true cholinergic transmitters from minces coincided with the effect of pretreatment on the pre-release ratio of false to true transmitter in the S3 fraction. These results suggest that much of the cholinergic transmitter which is spontaneously released from mouse forebrain occurs from the cytroplasmic fraction.
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References
Ariel, M., andDow, N. W. 1982. Effects of cholinergic drugs in receptive field properties of rabbit retinal ganglion cells. J. Physiol. 324:135–160.
Bhatnagar, S. P., andMacIntosh, F. C. 1967. Effects of quaternary bases and inorganic ions on acetylcholine synthesis in nervous tissue. Can. J. Physiology Pharmacol. 45:249–268.
Boksa, P., andCollier, B. 1980. Spontaneous and evoked release of acetylcholine and a cholinergic false transmitter from brain slices: comparison to true and false transmitter in subcellular stores. Neuroscience 5:1517–1532.
Bourdois, D. S., andSzerb, J. C. 1972. The absence of ‘surplus’ acetylcholine formation in prisms prepared from rat cerebral cortex. J. Neurochem. 19:1189–1193.
Carroll, P. T., andBenishin, C. G. 1983. Depolarization of mouse forebrain minces with veratridine and high K+: failure to stimulate the Ca2+ independent, spontaneous release of acetylcholine from the cytoplasm due to hydrolysis of the acetylcholine stored there. (Brain Res., in press.)
Carroll, P. T., andAspry, J. M. 1980. Subcellular origin of cholinergic transmitter release from mouse brain. Science 210:641–642.
Carroll, P. T., andAspry, J. M. 1981. Spontaneous and potassium-induced release of acetylcholine from mouse forebrain minces. Neuroscience 6:2555–2559.
Carroll, P. T., andGoldberg, A. M. 1975. Relative importance of choline transport to spontaneous and potassium depolarized release of ACh. J. Neurochem. 25:523–527.
Carroll, P. T., andNelson, S. H. 1978. Cholinergic vesicles: ability to empty and refill independently of cytoplasmic acetylcholine. Science 199:85–86.
Carroll, P. T., Silbergeld, E. K., andGoldberg, A. M. 1977. Alteration of central cholinergic function by chronic lead acetate exposure. Biochem. Pharmacol. 26:397–402.
Collier, B., Poon, P., andSalehmoghaddam, S. 1972. The formation of choline and acetylcholine by brain in vitro. J. Neurochem. 19:51–60.
Collier, B., Lovat, S., Ilson, D., Barker, L. A., andMittag, T. W. 1977. The uptake, metabolism and release of homocholine: studies with rat brain synaptosomes and cat superior cervical ganglion. J. Neurochem. 28:331–339.
Drachman, D. B., Stanley, E. F., Pestronk, A., Griffin, J. W., andPrice, D. L. 1982. Neurotrophic regulation of two properties of skeletal muscle by impulse dependent and spontaneous acetylcholine transmission. J. Neurosci. 2:232–243.
Gibson, G. E., andPeterson, C. 1981. Aging decreases oxidative metabolism and the release and synthesis of acetylcholine. J. Neurochem. 37:978–984.
Goldberg, A. M., andMcCaman, R. E. 1973. The determination of picomole amounts of acetylcholine in mammalian brain. J. Neurochem. 20:1–8.
Gorio, A., Hurlbut, W. P., andCeccarelli, B. 1978. Acetylcholine compartments in mouse diaphragm. Comparison of the effects of black widow spider venom, electrical stimulation, and high concentrations of potassium. J. Cell. Biol. 78:716–733.
Gundersen, C. B., Jr., andHoward, B. D. 1978. The effects of botulinium toxin on acetylcholine metabolism in mouse brain slices and synaptosomes. J. Neurochem. 31:1005–1013.
Jope, R. S. 1981. Acetylcholine turnover and compartmentation in rat brain synaptosomes. J. Neurochem. 36:1712–1721.
Katz, B., andMiledi, R. 1965. The quantal release of transmitter substances. Pages 118–125,in Studies in Physiology, Berlin: Springer Verlag.
Katz, B., andMiledi, R. 1977. Transmitter leakage from motor nerve endings. Proc. R. Soc. B. 196:59–72.
Katz, B., andMiledi, R. 1981. Does the motor nerve impulse evoke ‘non-quantal’ transmitter release? Proc. R. Soc. Lond. B. 212:131–137.
Mehrotra, K. N., andDauterman, W. C. 1963. The specificity of rat brain acetylcholinesterase for N-alkyl analogues of acetyl choline. J. Neurochem. 10:119–123.
Meyer, E. M., andCooper, J. R. 1981. Correlations between Na+−K+ ATPase activity and acetylcholine release in rat cortical synaptosomes. J. Neurochem. 37:1186–1192.
Nelson, S. H., Benishin, C. G., andCarroll, P. T. 1980. Accumulation and metabolism of choline and homocholine by mouse brain subcellular fractions. Biochem. Pharmacol. 29:1949–1957.
Richter, J. A. 1976. Characteristics of acetylcholine release by superfused slices of rat brain. J. Neurochem. 26:791–797.
Richter, J. A., andWerling, L. L. 1979. K+ stimulated acetylcholine release: inhibition by several barbiturates and chloral hydrate but not by ethanol, chlordiazepoxide or 11-OH-Δa-tetrahydrocannibol. J. Neurochem. 32:935–941.
Salehmoghaddam, S. H., andCollier, B. 1976. The relationship between acetylcholine release from brain slices and the acetylcholine content of subcellular fractions prepared from brain. J. Neurochem. 27:71–76.
Sattin, A. 1966. The synthesis and storage of acetylcholine in the striatum. J. Neurochem. 13:515–524.
Spyker, J. M., Sparber, S. B., andGoldberg, A. M. 1972. Subtle consequences of methyl mercury exposure: behavioral deviation in offspring of treated mothers. Science 177:621–623.
Suskiw, J. B., andO'Leary, M. E. 1982. Differential labeling of depot and active acetylcholine pools in nondepolarized and potassium depolarized rat brain synaptosomes. J. Neurochem. 38:1668–1675.
Vizi, E. S. 1972. Stimulation by inhibition of (Na+−K+−Mg2+)-activated ATPase, of acetylcholine release in cortical slices from rat brain. J. Physiol. 226:95–117.
Vizi, E. S., andVyskocil, T. 1979. Changes in total and quantal release of acetylcholine in the mouse diaphragm during activation and inhibition of membrane ATPase. J. Physiol. Lond. 286:1–14.
Von Schwarzenfeld, I. 1979. Origin of transmitters released by electrical stimulation from a small, metabolically very active vesicular pool of cholinergic synapses in guinea pig cerebral cortex. Neuroscience 4:477–493.
Wallace, B. G., andGillon, J. W. 1982. Characterization of acetylcholinesterase in individual neurons in the leech central nervous system. J. Neurosci. 2:1108–1118.
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Carroll, P.T. Spontaneous release of acetylcholine and acetylhomocholine from mouse forebrain minces: Cytoplasmic or vesicular origin. Neurochem Res 8, 1271–1283 (1983). https://doi.org/10.1007/BF00963997
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DOI: https://doi.org/10.1007/BF00963997