吗啡喃的恶唑和尿素类似物在阿片受体上的体外研究。
In-vitro investigation of oxazol and urea analogues of morphinan at opioid receptors.
作者信息
Peng Xuemei, Knapp Brian I, Bidlack Jean M, Neumeyer John L
机构信息
Alcohol and Drug Abuse Research Center, McLean Hospital, Harvard Medical School, Belmont, MA 02478, USA.
出版信息
Bioorg Med Chem. 2007 Jun 15;15(12):4106-12. doi: 10.1016/j.bmc.2007.03.076. Epub 2007 Mar 30.
A series of 2-amino-oxazole (7 and 8) analogs and 2-one-oxazole analogs (9 and 10) were synthesized from cyclorphan (1) or butorphan (2) and evaluated in-vitro by their binding affinity at mu, delta, and kappa opioid receptors and compared with their 2-aminothiozole analogs 5 and 6. Ligands 7-10 showed decreased affinities at kappa and mu receptors. Urea analogs (11-14) were also prepared from 2-aminocyclorphan (3) or 2-aminobutorphan (4) and evaluated in-vitro by their binding affinity at mu, delta, and kappa opioid receptors. The urea derived opioids retained their affinities at mu receptors while showing increased affinities at delta receptors and decreased affinities at kappa receptors. Functional activities of these compounds were measured in the [35S]GTPgammaS binding assay, illustrating that all of these ligands were kappa agonists. At the mu receptor, compounds 11 and 12 were mu agonist/antagonists.
由环佐辛(1)或布托啡诺(2)合成了一系列2-氨基恶唑(7和8)类似物和2-氧代恶唑类似物(9和10),并通过它们对μ、δ和κ阿片受体的结合亲和力进行体外评估,并与它们的2-氨基噻唑类似物5和6进行比较。配体7-10在κ和μ受体上的亲和力降低。脲类似物(11-14)也由2-氨基环佐辛(3)或2-氨基布托啡诺(4)制备,并通过它们对μ、δ和κ阿片受体的结合亲和力进行体外评估。脲衍生的阿片类药物在μ受体上保留了它们的亲和力,但同时在δ受体上显示出增加的亲和力,在κ受体上显示出降低的亲和力。这些化合物的功能活性在[35S]GTPγS结合试验中进行了测定,表明所有这些配体都是κ激动剂。在μ受体上,化合物11和12是μ激动剂/拮抗剂。
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