异喹啉衍生物选择性抑制环amp依赖性蛋白激酶。

Z X Lu, N H Quazi, L W Deady, G M Polya
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引用次数: 40

摘要

合成了大量的异喹啉衍生物,包括异喹啉衍生物、异喹啉[3,4-c]呋喃唑、1,2-二氢-1-氧异喹啉、6-氧嘧啶[1,2-d]异喹啉、苯并[c][1,8]-萘啶、吡嗪[2,3-c]异喹啉和苯并咪唑[2,1- A]异喹啉,以及结构上相关的异喹啉衍生物和吡啶-2,3-呋喃唑。所有这些类异喹啉的代表是大鼠肝脏环amp依赖性蛋白激酶(PKA)催化亚基(cAK)的有效和选择性抑制剂。最有效的cAK抑制剂是一系列1,3-二取代和1,3,4-三取代异喹啉(IC50值为30-50 nM)(化合物A1, A2, A3, A4和A5)和2-乙基羧基-3-氨基-5,6-二氢-6-氧苯并[c][1,8]萘啶(E1) (IC50值为0.08微米)。化合物A1-A5抑制cAK的方式与作为底物的ATP竞争。异喹啉抑制剂A1-A5是小麦胚Ca(2+)依赖性蛋白激酶(CDPK)、大鼠脑Ca(2+)依赖性蛋白激酶C (PKC)、鸡肫肌球蛋白轻链激酶(MLCK)和马铃薯薯类环核苷酸结合磷酸酶(Pase)的无效或极差抑制剂。E1是一种中等有效的CDPK和PKC抑制剂(IC50值分别为30和61微米)。双异喹啉-1(2H)- 1化合物B7抑制cAK、CDPK、PKC和MLCK (IC50值分别为8、95、24和7微米),J1[2-(对溴苯基)pyrrolo-[2,3-c]异喹啉-5(4H)- 1] (IC50值分别为2、50、44和7微米)也具有抑制作用。这里发现的非常有效的异喹啉衍生的cAK抑制剂涉及取代含n的异喹啉环系统,这些抑制剂对cAK具有高特异性。
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Selective inhibition of cyclic AMP-dependent protein kinase by isoquinoline derivatives.

A large series of isoquinoline derivatives was synthesised including derivatives of isoquinoline, isoquinolino[3,4-c]furazan, 1,2-dihydro-1-oxoisoquinoline, 6-oxopyrimido[1,2-d]isoquinoline, benzo[c][1,8]-naphthyridine, pyrazino[2,3-c]isoquinoline and benzimidazo[2,1-a]isoquinoline as well as further structurally related isoquinoline derivatives and pyrido-2,3-furazans. Representatives of all of these classes of isoquinolines are potent and selective inhibitors of the cyclic AMP-dependent protein kinase (PKA) catalytic subunit (cAK) from rat liver. The most effective cAK inhibitors are a series of 1,3-di-substituted and 1,3,4-tri-substituted isoquinolines (IC50 values 30-50 nM) (compounds A1, A2, A3, A4 and A5) and 2-ethylcarboxy-3-amino-5,6-dihydro-6-oxobenzo[c] [1,8]naphthyridine (E1) (IC50 0.08 microM). Compounds A1-A5 inhibit cAK in a fashion that is competitive with respect to ATP as substrate. The isoquinoline inhibitors A1-A5 are ineffective or very poor inhibitors of wheat embryo Ca(2+)-dependent protein kinase (CDPK) and rat brain Ca(2+)-dependent protein kinase C (PKC), chicken gizzard myosin light chain kinase (MLCK) and potato tuber cyclic nucleotide-binding phosphatase (Pase). E1 is a moderately effective inhibitor of CDPK and PKC (IC50 values 30 and 61 microM, respectively). The bisisoquinoline-1(2H)-one compound B7 inhibits cAK, CDPK, PKC and MLCK (IC50 values 8, 95, 24 and 7 microM, respectively) as does J1 [2-(p-bromophenyl)pyrrolo-[2,3-c]isoquinoline-5(4H)-one] (IC50 values 2, 50, 44 and 7 microM, respectively). The very potent isoquinoline-derived cAK inhibitors found here involve substitution of the N-containing isoquinoline ring system and these inhibitors show high specificity for cAK.

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Sialic acids structure-analysis-metabolism-occurrence-recognition. Glycyl-tRNA synthetase. Rapid purification and characterization of two distinct N-deoxyribosyltransferases of Lactobacillus leichmannii. Purification of the CIC-0 chloride channel from Torpedo california electroplax identification of a phosphorylation site for cAMP-dependent protein kinase. Selective inhibition of cyclic AMP-dependent protein kinase by isoquinoline derivatives.
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