The biochemistry of an acetylcholine receptor

Raftery, Michael A.; Vandlen, Richard; Michaelson, D. M.; Bode, Jürgen; Moody, Terry W.; Chao, Y.; Reed, K.; Deutsch, James; Duguid, John R.

doi:10.1002/jss.400020506

Cited by 46 publications

(32 citation statements)

References 4 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…to [12], yielded linear curves ( fig.lB) Hence, we conclude that the phencyclidine derivatives under investigation bind at the PM level to specific binding sites present in the Torpedo membrane preparation which are not the cwBgt binding sites of the nicotinic receptors present in this preparation [4,6,15]. These data are in good agreement with the findings [l-3] that at FM levels phencyclidines do not block binding of 12'I_(yBgt.…”

Section: Resultssupporting

confidence: 88%

“…We therefore decided to investigate the nature of this interaction by means of direct binding experiments using the 3H-labeled derivatives. The phencyclidines exhibit multiple interactions ( [l] and literature cited therein); their specific binding was studied in Torpedo electric organ since this enabled us to focus on the nicotinic cholinergic system (reviewed [4]). …”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Specific binding of [³H]phencyclidines to membrane preparation

et al. 1980

View full text Add to dashboard Cite

Section: Resultssupporting

confidence: 88%

Section: Introductionmentioning

confidence: 99%

Specific binding of [³H]phencyclidines to membrane preparation

et al. 1980

View full text Add to dashboard Cite

“…This indicates that, with respect to trypsin-sensitive residues, the 65,000-and 60,000-dalton subunits are the most exposed on the cytoplasmic face of the membrane, followed by the 50,000-dalton subunit, with the 40,000-dalton subunit exposed very little. More At the ultrastructural level, high-resolution electron micrographs of the AcChoR rosettes show from four to six similar "subunits" arranged about an electron-dense core (18,(48)(49)(50). This is consistent with recent reports that the receptor molecule consists of four homologous subunits present in the ratio 2:1:1:1 (31,32), for a total of five similar subunits, all exposed on the extracellular surface of the membrane.…”

Section: Discussionsupporting

confidence: 89%

“…Acad. Sci Examination of membrane vesicles by negative-stain electron microscopy showed no effect on the characteristic rosette structure of the AcChoR molecule (18,(48)(49)(50) either by the freeze-thawing process or by tryptic hydrolysis from either membrane face.…”

mentioning

confidence: 85%

“…Except for one account (17), both species have been found to consist of four subunits of 40,000, 50,000, 60,000, and 65,000 daltons, with binding sites for a-neurotoxins, agonists, and some antagonists located on the 40,000-dalton subunit (18)(19)(20)(21)(22)(23)(24)(25)(26)(27)(28)(29)(30). These four subunits were found to possess a high incidence of amino acid sequence homology (31) and to exist in both membrane-bound and detergent-solubilized receptor as a pentameric complex with a stoichiometry of 2:1:1:1 (31,32).…”

mentioning

confidence: 99%

See 1 more Smart Citation

Topographic studies of Torpedo acetylcholine receptor subunits as a transmembrane complex.

Strader¹,

Raftery²

1980

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

The exposure of the four subunits of the acetylcholine receptor from Torpedo californica on both the extracellular and cytoplasmic faces of the postsynaptic membranes of the electroplaque cells has been investigated. Sealed membrane vesicles containing no protein components other than the receptor were isolated and were shown to have 95% of their synaptic surfaces facing the medium. The susceptibility of the four receptor subunits in these preparations to hydrolysis by trypsin both from the external and from the internal medium was used to investigate the exposure of the subunits on the synaptic and cytoplasmic surfaces of the membrane. It was shown by sodium dodecyl sulfate gel electrophoresis of the tryptic products that all four subunits are exposed on the extracellular surface to a similar degree. All four subunits are also exposed on the internal surface of the membrane, but the apparent degree of exposure varies with the subunit size, the larger subunits being more exposed. The results are discussed in terms of a possible topographic model of the receptor as a transmembrane protein complex.Excitable membrane vesicles highly enriched in the acetylcholine receptor (AcChoR) have been purified from the electric organs of several species of electric fish. These membrane preparations possess the properties of nicotinic postsynaptic membranes: they bind a-neurotoxins (1, 2) and cholinergic ligands (3, 4) and they possess distinct binding sites for local anesthetics (4-7) and the alkaloid histrionicotoxin (8, 9). Binding of cholinergic agonists results in the flux of inorganic cations through the vesicular membrane (10-13), and the demonstration of such flux through membrane preparations containing only the AcChoR protein (14,15) suggests that the AcChoR functions as a cation-translocating protein complex.Detergent-extracted, chromatographically purified AcChoR from Torpedo californica sediments both as a 9S monomer and as a 13.7S dimer (16). Except for one account (17), both species have been found to consist of four subunits of 40,000, 50,000, 60,000, and 65,000 daltons, with binding sites for a-neurotoxins, agonists, and some antagonists located on the 40,000-dalton subunit (18-30). These four subunits were found to possess a high incidence of amino acid sequence homology (31) and to exist in both membrane-bound and detergent-solubilized receptor as a pentameric complex with a stoichiometry of 2:1:1:1 (31, 32). This stoichiometry dictates a size of 255,000 daltons for the AcChoR monomer, in agreement with the experimentally determined values of 250,000-270,000 daltons (33-35). In light of this molecular definition of the AcChoR and of its defined function alluded to above, it is of interest to determine the topography of its subunits in the membrane and eventually to assign a specific function to each polypeptide.By use of antibodies to purified AcChoR, it has been found at the electron microscopic level by both thin-sectioning (36) and examination of replicas of intact and sheared membrane vesicles (37...

show abstract

Biochemische Aspekte der cholinergen Reizung

Maelicke

1984

Angewandte Chemie

View full text Add to dashboard Cite

Lebende Organismen kbnnen sich nur entwickeln und erhalten, solange eine wirksame Kommunikation zwischen ihren Einzelkomponentenden Zellenbesteht. Diese interzellullre Kommunikation ist hauptsachlich chemischer Natur: Sie benutzt als Botenstoffe Neurotransmitter und Hormone und als Signalempfanger Rezeptoren. Die Konzentrationen aller beteiligten Komponenten sind gewbhnlich gering. Ausnahmen gibt es bei einigen synaptischen Kommunikationssystemen wie der Nerven-Muskel-Synapse oder ihrer speziellen Form, der Nerven-Elektrozyt-Synapse in den elektrischen Organen von Zitteraal (Electrophorus) und Zitterrochen (Torpedo). Diese Systeme sind der biochemischen Analyse gut zuganglich, so daD sie sich zur Aufkliirung der molekularen Grundlagen derartiger biologischer Kommunikationsprozesse eignen. Auf diese Weise ist gefunden worden, daI3 der nicotinische Acetylcholinrezeptor der Muskelzelle nicht nur das von der zugeh6rigen Nervenzelle ausgesendete Signal empfangt, sondern dieses auch selbst in eine elektrische Aktivitilt der Muskelzelle umsetzt. Fluoreszenzkinetische Untersuchungen der Wechselwirkung des Acetylcholinrezeptors nit seinen Liganden haben zu einem neuen Model1 des molekularen Mechanismus der cholinergen Reizung gefiihrt, das auch von physiologischen und immunologischen Befunden gestiitzt wird. Angew. Chem. 96 (1984) 193-219 @ Verlag Chemie GmbH. 0-6940 Weinheim. 1984 0014-8249/84/0303-0193 S 02.50/0 193 Acetylcholin J 2 prasynaptisch Verpackung in Vesikeln enzymatische Acetylierung t Wiederaufnahme von Cholin-50 ms Abb. 2. Acetylcholin-induzierte hderungen der elektrischcn Lcitfahigkeit einzelncr loncnkanalc des Acetylcholinrezeptor. a) Nach Hami// et al. [33] wurde ein McmbranstUckchen eines embryonalcn Rattenmuskels so an der McDpipettc festgcsaugt, daD ein Ubergangswiderstand von einigen Gn erreicht wurdc. Unter Bedingungen der Spannungsklemme (die Spannung Uber der Membran wird wahrcnd dcr gcsamten Mcssung konstant gehalten) werden dann die jlnderungen des Stromflusses aufgezeichnet. Diese sind den iinderungen dcr Mcmbranleitf3higkeit dirckt proportional. Eine derartige Anordnung wird als patch-clamp bezeichnct. Pipettenl6sungen: innen 150 m~ KCI, 1 mM EGTA, 4 mM HEPES, pH 7.2; auDen 150 mM NaCI. 2 mM CaCI2, 2 mM MgCh. 4 mM KCI, 4~ HEPES, pH 7.2. Das Membranpotential wurde auf -70 mV festgelcgt, was einer lcichtcn Hyperpolarisation dcr Muskelmcmbran entspricht. MeBtemperatur ca. 2 5 T .b) Die Strom-&it-Kurve wurdc nach Zugabc von Acetylcholin (2 pM) zur AuDenl6sung aufgcnommen. Wic aus den Amplituden zu erkcnnen ist, traten neben Einzelkanalereignissen auch Doppcl-und Drcifachkanalereignisse auf (gleichzeitige Aktivierung von zwei bzw. drei Rezeptorkan~len). Die Messung wurde von Dr. C. Merhfessel, Univcritit Bochum, durchgefiihrt. Angew. Chem. 96 (1984) 193-219 4 a , X = B r , 4b. X = CnH2,,+, , 4 c , X = ( C H .~-, -N H~) -N O~

show abstract

The biochemistry of an acetylcholine receptor

Cited by 46 publications

References 4 publications

Specific binding of [³H]phencyclidines to membrane preparation

Specific binding of [³H]phencyclidines to membrane preparation

Topographic studies of Torpedo acetylcholine receptor subunits as a transmembrane complex.

Biochemische Aspekte der cholinergen Reizung

Contact Info

Product

Resources

About

The biochemistry of an acetylcholine receptor

Cited by 46 publications

References 4 publications

Specific binding of [3H]phencyclidines to membrane preparation

Specific binding of [3H]phencyclidines to membrane preparation

Topographic studies of Torpedo acetylcholine receptor subunits as a transmembrane complex.

Biochemische Aspekte der cholinergen Reizung

Contact Info

Product

Resources

About

Specific binding of [³H]phencyclidines to membrane preparation

Specific binding of [³H]phencyclidines to membrane preparation