1 BIIE0246, a newly synthesized non-peptide neuropeptide Y (NPY) Y-2 recept
or antagonist, was able to compete with high affinity (8 to 15 nM) for spec
ific [I-125]PYY3-36 binding sites in HEK293 cells transfected with the rat
Y-2 receptor cDNA, and in rat brain and human frontal cortex membrane homog
enates.
2 Interestingly, in rat brain homogenates while NPY, C2-NPY and PYY3-36 inh
ibited all specific [I-125]PYY3-36 labelling, BIIE0246 failed to compete fo
r all specific binding suggesting that [I-125]PYY3-36 recognized, in additi
on to the Y-2 subtype, another population of specific NPY binding sites, mo
st likely the Y-5 receptor.
3 Quantitative receptor autoradiographic data confirmed the presence of [I-
125]PYY3-36/BIIE0246-sensitive (Y-2) and-insensitive (Y-5) binding sites in
the rat brain as well as in the marmoset monkey and human hippocampal form
ation.
4 In the rat vas deferens and dog saphenous vein (two prototypical Y-2 bioa
ssays), BIIE0246 induced parallel shifts to the right of NPY concentration-
response curves with pA(2) values of 8.1 and 8.6, respectively. In the rat
colon (a Y-2/Y-4 bioassay), BIIE0246 (1 mu M) completely blocked the contra
ction induced by PYY3-36, but not that of [Leu(31),Pro(34)]NPY (a Y-1, Y-4
and Y-5 agonist) and hPP (a Y-4 and Y-5 agonist). Additionally, BIIE0246 fa
iled to alter the contractile effects of NPY in prototypical Y-1 in vitro b
ioassays.
5 Taken together, these results demonstrate that BIIE0246 is a highly poten
t, high affinity antagonist selective for the Y-2 receptor subtype. It shou
ld prove most useful to establish further the functional role of the Y-2 re
ceptor in the organism.