Drabczyńska Anna, Müller Christa E, Schiedel Anke, Schumacher Britta, Karolak-Wojciechowska Janina, Fruziński Andrzej, Zobnina Weronika, Yuzlenko Olga, Kieć-Kononowicz Katarzyna
Jagiellonian University Medical College, Faculty of Pharmacy, Department of Technology and Biotechnology of Drugs, Medyczna 9, Pl 30-688 Kraków, Poland.
Bioorg Med Chem. 2007 Nov 15;15(22):6956-74. doi: 10.1016/j.bmc.2007.07.051. Epub 2007 Aug 22.
The synthesis of N-(un)substituted-phenylalkylpyrimido[2,1-f]purinediones was performed starting with 7-(3-chloropropyl)-8-bromotheophylline and 7-(3-chloropropyl)-8-bromo-1,3-dipropylxanthine. Compounds with unsubstituted or substituted ethylene spacer to an aromatic ring were synthesized. Additionally variations in the spacer-elongation of the linker containing more than two atoms, introduction of a double bond or heteroatoms were performed. Physicochemical properties of the synthesized compounds were described. The obtained compounds envisaged as sterically fixed and configurationally stable analogs of 8-styrylxanthines, were evaluated for their affinity to adenosine A(1) and A(2A) receptors, the receptor subtypes that are predominant in the brain. Selected compounds were also investigated for the affinity to the A(2B) and A(3) receptor subtypes. It was stated that phenylethyl pyrimido[2,1-f]purinediones and their analogs with variations of the ethylene spacer (substituted or extended) exhibit micromolar or submicromolar affinity for A(2A) ARs (adenosine receptors); for example compound 2Ac with p-hydroxy substituent displayed a K(i) value of 0.23 microM at the rat A(2A) receptor. In comparison to the previously obtained phenyl and benzyl pyrimido[2,1-f]purinediones compounds with a shorter spacer, phenethyl derivatives were optimal for A(2A) AR. The kind of substituent at the aromatic ring was important for the affinity. Oxygen and nitrogen atoms in the spacer resulted frequently in a slight decrease of the A(2A) AR affinity, introduction of more heteroatoms into the spacer-in carbamates-caused distinctly negative effect on the activity. In this series of compounds more frequently the adenosine A(1) activity was observed, also in submicromolar range as for dipropyl derivative 2Ba with K(i) value of 0.62 microM at the rat A(2A) AR. 3D-QSAR models were developed for the compounds presented in this paper as well as in the previous publications showing activity at adenosine A(1) and A(2A) ARs. It was concluded that for the activity at adenosine A(1) and A(2A) receptors lipophilicity, steric effects along with the molecule's electrostatic surface properties had greatest value. Chosen compounds were evaluated in vivo as anticonvulsants in MES, scMet tests and examined for neurotoxicity. Contrary to previously obtained phenyl and benzyl pyrimido[2,1-f]purinediones, all tested compounds were inactive as anticonvulsants.
N-(未)取代的苯基烷基嘧啶并[2,1-f]嘌呤二酮的合成是从7-(3-氯丙基)-8-溴茶碱和7-(3-氯丙基)-8-溴-1,3-二丙基黄嘌呤开始进行的。合成了具有未取代或取代的与芳环相连的乙烯间隔基的化合物。此外,还对含有两个以上原子的连接子的间隔基延长、引入双键或杂原子进行了变化研究。描述了合成化合物的物理化学性质。所得到的化合物被设想为8-苯乙烯基黄嘌呤的空间固定和构型稳定类似物,并对其与腺苷A(1)和A(2A)受体(大脑中占主导地位的受体亚型)的亲和力进行了评估。还对选定的化合物与A(2B)和A(3)受体亚型的亲和力进行了研究。结果表明,苯乙基嘧啶并[2,1-f]嘌呤二酮及其具有乙烯间隔基变化(取代或延长)的类似物对A(2A)腺苷受体(ARs)表现出微摩尔或亚微摩尔亲和力;例如,具有对羟基取代基的化合物2Ac在大鼠A(2A)受体处的K(i)值为0.23微摩尔。与先前得到的具有较短间隔基的苯基和苄基嘧啶并[2,1-f]嘌呤二酮化合物相比,苯乙基衍生物对A(2A) ARs是最优的。芳环上取代基的种类对亲和力很重要。间隔基中的氧和氮原子常常导致A(2A) ARs亲和力略有下降,在间隔基中引入更多杂原子(如在氨基甲酸酯中)会对活性产生明显的负面影响。在这一系列化合物中,更常观察到腺苷A(1)活性,也在亚微摩尔范围内,如二丙基衍生物2Ba在大鼠A(2A) AR处的K(i)值为0.62微摩尔。针对本文以及先前出版物中显示对腺苷A(1)和A(2A) ARs有活性的化合物建立了3D-QSAR模型。得出的结论是,对于腺苷A(1)和A(2A)受体的活性,亲脂性、空间效应以及分子的静电表面性质具有最大价值。选定的化合物在体内进行了MES、scMet试验中的抗惊厥评估,并检测了神经毒性。与先前得到的苯基和苄基嘧啶并[2,1-f]嘌呤二酮相反,所有测试化合物作为抗惊厥剂均无活性。
