de Costa B R, Bowen W D, Hellewell S B, Walker J M, Thurkauf A, Jacobson A E, Rice K C
Laboratory of Medicinal Chemistry, National Institute of Digestive, Diabetes, and Kidney Diseases, Bethesda, MD 20892.
FEBS Lett. 1989 Jul 17;251(1-2):53-8. doi: 10.1016/0014-5793(89)81427-9.
Tritium-labeled (+)-pentazocine ([3H]-1b) of specific activity 26.6 Ci/mmol was synthesized in 3 steps starting with (+)-normetazocine (2) of defined optical purity. [3H]-1b has been characterized as a highly selective ligand for labeling of sigma receptors. Competition data revealed that [3H]-1b could be displaced from guinea pig brain membrane preparations with a number of commonly used sigma receptor ligands. [3H]-1b exhibited saturable, enantioselective binding with a Kd of 5.13 +/- 0.97 nM and a Bmax of 1146 +/- 122 fmol/mg protein. Phencyclidine (PCP) displaced [3H]-1b with low affinity while MK-801 was inactive, thus indicating insignificant activity at the PCP-binding site; apomorphine failed to displace [3H]-1b indicating lack of dopamine receptor cross-reactivity. Since the affinity of [3H]-1b is about 6 times that of the two commonly employed sigma ligands ((+)-3-[3H]PPP and [3H]DTG) and since it is more selective for sigma receptors than the benzomorphan [3H]SKF-10,047, it represents the first example of a highly selective benzomorphan based sigma receptor ligand. [3H]-1b should prove useful for further study of the structure and function of sigma receptors.
以具有特定光学纯度的(+)-去甲美沙酮(2)为起始原料,通过三步合成了比活度为26.6 Ci/mmol的氚标记(+)-喷他佐辛([3H]-1b)。[3H]-1b已被表征为用于标记σ受体的高选择性配体。竞争数据表明,[3H]-1b可被多种常用的σ受体配体从豚鼠脑膜制剂中置换出来。[3H]-1b表现出可饱和的、对映体选择性结合,Kd为5.13±0.97 nM,Bmax为1146±122 fmol/mg蛋白质。苯环己哌啶(PCP)以低亲和力置换[3H]-1b,而MK-801无活性,因此表明在PCP结合位点活性不显著;阿扑吗啡未能置换[3H]-1b,表明不存在多巴胺受体交叉反应性。由于[3H]-1b的亲和力约为两种常用σ配体((+)-3-[3H]PPP和[3H]DTG)的6倍,且其对σ受体的选择性高于苯并吗啡烷[3H]SKF-10,047,它代表了基于苯并吗啡烷的高选择性σ受体配体的首个实例。[3H]-1b应被证明对进一步研究σ受体的结构和功能有用。
