Summary
The blood platelet has three morphologically distinct membrane systems. In addition to the plasma membrane the platelet has an ‘open canalicular system’ (surface-connected intracytoplasmic membrane system) and a microsome-like ‘dense tubular system’. The open canalicular and dense tubular systems have been implicated in Ca2+ transport, cyclic nucleotide (cAMP) synthesis and prostaglandin and thromboxane synthesis. Precise definition of the function of the different membrane systems requires analysis of their unique chemical activities. Broken cell preparations are used to advantage for such studies. However, clean separation and definition of the origin and composition of the membrane fractions has been difficult because well-defined marker enzymes for the various membrane systems have not been conclusively estabished. Platelets were fixed for 5 min in 1% paraformaldehyde-0.2% glutaraldehyde and assayed for K+-dependentp-nitrophenyl phosphatase, Ca2+-, Mg2+-ATPase and adenylate cyclase. K+-dependentp-nitrophenyl phosphatase was localized only at the plasma membrane wnile Ca2+-, Mg2+-ATPase and adenylate cyclase were found relatively segregated to the open canalicular and dense tubular systems. The segregation of these enzymes to separate membrane compartments may have significant implications with regard to understanding platelet function.
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References
Behnke, O. (1958) Electron microscopic observations on the membrane systems of the rat platelet.Anat. Rec. 158, 121–34.
Cutler, L. S. (1975) Comments on the validity of the use of lead nitrate for the cytochemical study of adenylate cyclase.J. Histochem. Cytochem. 23, 786–7.
Cutler, L. S. &Christian, C. P. (1980) Cytochemical localization of adenylate cyclase.J. Histochem. Cytochem. 28, 62–5.
Cutler, L. S., Feinstein, M. B. &Christian, C. P. (1980) Cytochemical localization of oubain-sensitive (K+)-dependentp-nitrophenyl phosphatase (transport ATPase) in human blood platelets.J. Histochem. Cytochem. 28, 1183–8.
Cutler, L. S. &Kodan, S. B. (1976) Biochemical and cytochemical studies on adenylate cyclase in the developing rat submandibular gland: Differentiation of the acinar secretory compartment.J. Embryol. exp. Morph. 36, 291–303.
Cutler, L. S., Rodan, G. &Feinstein, M. B. (1978) Cytochemical localization of adenylate cyclase and of calcium ion, magnesium ion-activated ATPases in the dense tubular system of human blood platelets.Biochim. biophys. Acta 542, 357–71.
Cutler, L. S. &Rossomando, E. F. (1975) Localization of adenylate cyclase inDictyostelium discoideum II. Cytochemical studies on whole cells and isolated plasma membrane vesicles.Expl Cell Res. 95, 79–87.
Cutler, L. S., Mooradian, B. A. &Christian, C. P. (1977) Concurrent cytochemical localization of adenylate cyclase and peroxidase in the developing rat submandibular gland.J. Histochem. Cytochem. 25, 1207–12.
Ernst, S. A. (1972a) Transport adensosine triphosphatase cytochemistry. I. Biochemical characterization of a cytochemical medium for the ultrastructural localization of oubain sensitive, potassium-dependent phosphatase activity in the avian salt gland.J. Histochem. Cytochem. 20, 13–22.
Ernst, S. A. (1972b) Transport adenosine triphosphatase cytochemistry. II. Cytochemical localization of oubain-sensitive potassium-dependent phosphatase activity in secretory epithelium of the avian salt gland.J. Histochem. Cytochem. 20, 23–38.
Feinstein, M. B. &Fraser, C. (1975) Human platelet secretion and aggregation induced by calcium ionophores. Inhibition by PGE1 and dibutyryl cyclic AMP.J. gen. Physiol. 66, 561–75.
Feinstein, M. B., Rodan, G. A. &Cutler, L. S. (1981) Cyclic AMP and calcium, in platelet function. InPlatelets in Biology and Pathology II. (edited byGordon, J. L.). Amsterdam: North Holland.
Howell, S. L. &Whitfield, M. (1972) Cytochemical localization of adenyl cyclase activity in rat islets of Langerhans.J. Histochem. Cytochem. 20, 873–9.
Jundt, H. &Reuter, H. (1977) Is sodium-activated calcium efflux from mammalian cardiac muscle dependent on metabolic energy?J. Physiol., Lond. 266, 78–79P.
Krieger, N. S. &Tashjian, A. H., Jr, (1980) Parathyroid hormone stimulates bone resorption via a Na−Ca exchange mechanismNature Lond. 287, 843–5.
Raible, D. G., Cutler, L. S. &Rodan, G. A. (1978) Localization, of adenylate cyclase in skeletal muscle sarcoplasmic reticulum and its relation to calcium accumulation.FEBS Lett. 85, 149–52.
Reeves, J. P. &Sutko, J. L. (1979) Sodium-calcium ion exchange in cardiac membrane vesicles.Proc. natn. Acad. Sci. U.S.A. 76, 590–4.
Schulze, W., Hinterberger, U., Wollenberger, A., Krause, E. G., &Janiszewski, E. (1977) Problems of the cytochemical demonstration of adenylate cyclase.Acta Histochem. Cytochem. 10, 371–8.
Solomon, Y., Londos, C. &Rodbell, M. (1974) A highly sensitive adenylate cyclase assay.Analyt. Biochem. 58, 541–8.
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Cutler, L.S., Feinstein, M.B., Rodan, G.A. et al. Cytochemical evidence for the segregation of adenylate cyclase, Ca2+-, Mg2+-ATPase, K+-dependentp-nitrophenyl phosphatase in separate membrane compartments in human platelets. Histochem J 13, 547–554 (1981). https://doi.org/10.1007/BF01002710
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DOI: https://doi.org/10.1007/BF01002710