Terrillon Sonia, Cheng Ling Ling, Stoev Stoytcho, Mouillac Bernard, Barberis Claude, Manning Maurice, Durroux Thierry
INSERM U 469, 141 rue de la Cardonille, 34094 Montpellier CEDEX 5, France.
J Med Chem. 2002 Jun 6;45(12):2579-88. doi: 10.1021/jm010526+.
The fluoresceinyl (Flu) group has been linked by an amide bond to the side chain amino group at position 8 of (a) two oxytocin (OT) antagonists, to give d(CH(2))(5)[Tyr(Me)(2),Thr(4),Orn(8)(5/6C-Flu),Tyr-NH(2)(9)]VT (Orn(8)(5/6C-Flu)OTA) (1) and desGly-NH(2),d(CH(2))(5)[D- Tyr(2),Thr(4),Orn(8)(5/6C-Flu)]VT (2), and (b) eight Lys(8) and Orn(8) analogues of potent OT agonists, to give d[Lys(8)(5/6C-Flu)]VT (3), d[Thr(4),Lys(8)(5/6C-Flu)]VT (4), [HO(1)][Lys(8)(5/6C-Flu)]VT (5), [HO(1)][Thr(4),Lys(8)(5/6C-Flu)]VT (6), d[Orn(8)(5/6C-Flu)]VT (7), d[Thr(4),Orn(8)(5/6C-Flu)]VT (8), [HO(1)][Orn(8)(5/6C-Flu)]VT (9), and [HO(1)][Thr(4),Orn(8)(5/6C-Flu)]VT (10). The tetramethylrhodamyl (Rhm) group was attached to the precursor peptide of 9 to give [HO(1)][Orn(8)(5/6C-Rhm)]VT (11). All 11 fluorescent peptides were evaluated in human OT and vasopressin V(1a) (vasoconstrictor), V(1b) (pituitary), and V(2) (antidiuretic) receptor binding and functional assays. With K(d) = 6.24, 217, >10000, and >10000 nM for the OT, V(1a), V(1b), and V(2) receptors, peptide 1 is a potent and selective fluorescent OT antagonist and may be useful for specifically labeling OT receptors while peptide 2 exhibits low affinities for all the receptors. The fluorescent peptides 3-10 are all very potent agonists for the human OT receptor. They exhibit the following K(d) values (nM) for the human OT, V(1a), V(1b), and V(2) receptors, respectively: (3) 0.29, 57, 124, >10000; (4) 1.8, 25.5, 150, >10000; (5) 0.34, 13.7, 66, nd (not determined); (6) 0.32, 17.3, 53, >10000; (7) 0.25, 107, 393, >10000; (8) 0.40, 30, 282, >10000; (9) 0.18, 12.2, 126, nd; (10) 0.17, 11.8, 87, >1000; (11) 0.092, 7.36, nd, nd. Peptide 7 exhibits both a high affinity and a high selectivity for human OT receptors. Peptides 7 and 11 were utilized to study the internalization of the OT receptor-ligand complex. Preliminary studies indicate that this process is similar to that observed for the vasopressin V(1a) receptor and differs from that observed for vasopressin V(2) receptors. Some or all of the fluorescent OT antagonists and agonists reported here are very promising new fluorescent ligands for labeling cells which express the human OT receptor and are also useful tools to follow endocytosis of the receptor-ligand complex.
荧光素基(Flu)已通过酰胺键与(a)两种催产素(OT)拮抗剂第8位的侧链氨基相连,得到d(CH(2))(5)[Tyr(Me)(2),Thr(4),Orn(8)(5/6C-Flu),Tyr-NH(2)(9)]VT(Orn(8)(5/6C-Flu)OTA)(1)和去甘氨酰胺、d(CH(2))(5)[D-Tyr(2),Thr(4),Orn(8)(5/6C-Flu)]VT(2);以及(b)八种强效OT激动剂的Lys(8)和Orn(8)类似物,得到d[Lys(8)(5/6C-Flu)]VT(3)、d[Thr(4),Lys(8)(5/6C-Flu)]VT(4)、[HO(1)][Lys(8)(5/6C-Flu)]VT(5)、[HO(1)][Thr(4),Lys(8)(5/6C-Flu)]VT(6)、d[Orn(8)(5/6C-Flu)]VT(7)、d[Thr(4),Orn(8)(5/6C-Flu)]VT(8)、[HO(1)][Orn(8)(5/6C-Flu)]VT(9)和[HO(1)][Thr(4),Orn(8)(5/6C-Flu)]VT(10)。四甲基罗丹明基(Rhm)连接到9的前体肽上,得到[HO(1)][Orn(8)(5/6C-Rhm)]VT(11)。对所有11种荧光肽进行了人OT和血管加压素V(1a)(血管收缩剂)、V(1b)(垂体)和V(2)(抗利尿)受体结合及功能测定。肽1对OT、V(1a)、V(1b)和V(2)受体的解离常数(K(d))分别为6.
