cAMP Assay Kits

MBS433536 | Elite cAMP ELISA Assay Kit (Fluorescence)
MBS433543 | Elite cAMP 384-Well ELISA Assay Kit (Fluorescence)
MBS841511 | cAMP Direct Immunoassay Kit (Colorimetric)
MBS849587 | cAMP Phosphodiesterase Activity Assay Kit (Fluorometric)

Accession Number : KLM0000082 This work is released into the public domain; please see our release statement.
Doug Markham has contributed a molecular mechanics computation of the structure! See below for the details.

Config Rule :

% cAMP


config(cAMP,[
substituent('D-1-dehydroxy-3,O4-dehydro-ribofuranosyl'),
substituent(adenyl),
substituent(phosphodiyl),
linkage(from('D-1-dehydroxy-3,O4-dehydro-ribofuranosyl',car(1)),
to(adenyl,nit(9)),
up,single),
linkage(from(phosphodiyl,pho(1)),
to('D-1-dehydroxy-3,O4-dehydro-ribofuranosyl',attach_to([oxy,car(3)])),
nil,single),
linkage(from(phosphodiyl,pho(1)),
to('D-1-dehydroxy-3,O4-dehydro-ribofuranosyl',attach_to([oxy,car(5)])),
nil,single)]).

config('D-1-dehydroxy-3,O4-dehydro-ribofuranosyl',[
ring([
oxy,
anomeric(1,hyd),
car(2,hyd&&hydroxyl;),
car(3,hyd&& (oxy~)),
car(4,oxymethyl&&hyd;)])]).

config(adenyl,[
model(adenine,[
diff(nit(9,hyd),nit(9))])]).

config(adenine,[
model(purine,[
diff(car(6,hyd),car(6,amine(10)))])]).

config(purine,[
ring_system([
ring([
car(6,hyd)&,
car(5)&,
car(4)&,
nit(3)&,
car(2,hyd)&,
nit(1)&]),
ring([
nit(7)&,
car(8,hyd)&,
nit(9,hyd)&,
car(4)&,
car(5)&])],
conjugate(1,pseudopos([car(4),car(5)]),2,pseudopos([car(4),car(5)]))])]).

Smiles String :

[C@2H]-1([O][C@2H]-2([C@2H]([O][P@2]([O][C@2H2]-2)(=[O])[O-])[C@2H]-1[OH]))-[n+]3([cH][n][c]4([c]3[n][cH][n][c]4[NH2]))

The Terminals for all the Config Rules are in Prolog Definite Clause Grammar (DCG) form.They can be checked in the Manual here.

The compound's PDB file can be seen here.

Doug Markham of the Institute for Cancer Research, Fox Chase Cancer Center,Philadelphia, PA, has contributed the following structure for cAMP. He computed this structure in sdf format using MacroModel, a molecular mechanics program. We have used Babel to convert the .sdf format to PDB format. You'll find it interesting to compare these structures to those computed using CONCORD.

Many thanks Doug!