AMINO-TERMINAL AND CARBOXYL-TERMINAL DOMAINS SPECIFY THE IDENTITY OF THE DELTA-SUBUNIT IN ASSEMBLY OF THE MOUSE MUSCLE NICOTINIC ACETYLCHOLINE-RECEPTOR
Xm. Yu et Zw. Hall, AMINO-TERMINAL AND CARBOXYL-TERMINAL DOMAINS SPECIFY THE IDENTITY OF THE DELTA-SUBUNIT IN ASSEMBLY OF THE MOUSE MUSCLE NICOTINIC ACETYLCHOLINE-RECEPTOR, Molecular pharmacology, 46(5), 1994, pp. 964-969
We have used transient expression in COS cells of the subunits of the
nicotinic acetylcholine receptor (AChR) from mouse sketetal muscle to
investigate the role of transmembrane and cytoplasmic domains of the d
elta subunit in assembly of the AChR. When chimeric subunits whose ext
racellular amino- and carboxyl-terminal domains were from the delta su
bunit and whose transmembrane and cytoplasmic domains were from either
the beta, gamma, or epsilon subunit were expressed with alpha, beta,
and epsilon subunits, alpha-bungaro-toxin-binding activity appeared on
the surface of the transfected cells. The resulting receptor complexe
s each had sedimentation constants resembling those of the native AChR
, consistent with a pentameric structure. Further investigation of the
delta(beta) chimeric subunit showed that it formed a heterodimer with
the alpha subunit and that the resulting subunit bound d-tubocurarine
with an affinity similar to that of the alpha delta heterodimer; delt
a(beta) also formed a heterodimer with a form of the alpha subunit tha
t is truncated after the first transmembrane domain. A heterodimer for
med from the epsilon(beta) and alpha subunits also bound d-tubocurarin
e with an affinity similar to that of the alpha epsilon heterodimer. W
hen both epsilon(beta) and delta(beta) subunits were substituted for t
he epsilon and delta subunits, respectively, a receptor complex was fo
rmed whose structure appeared to be alpha(2) beta(epsilon(beta))(delta
(beta)). These results show that, as with the epsilon subunit, the ide
ntity of the delta subunit in AChR assembly arises from the extracytop
lasmic domains of the subunit.