Lee J, Sharma R, Wang S, Milne G W, Lewin N E, Szallasi Z, Blumberg P M, George C, Marquez V E
Laboratory of Medicinal Chemistry, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA.
J Med Chem. 1996 Jan 5;39(1):36-45. doi: 10.1021/jm950278f.
Conformationally constrained analogues of diacylglycerol (DAG) built on a 5(-)[(acyloxy)methyl]-5-(hydroxymethyl)tetrahydro-2-furanone template (1, Chart 1) were shown previously to bind tightly to protein kinase C alpha (PK-C alpha) in a stereospecific manner. These compounds, however, racemized readily through rapid acyl migration and lost biological potency. In order to circumvent this problem, the "reversed ester" analogues were designed as a new set of PK-C ligands. This reversal of the ester function produced some new DAG mimetics that are embedded in a C-4 doubly-branched heptono-1,4-lactone template. The reversed ester analogues were impervious to racemization, and their chemically distinct branches facilitated the enantiospecific syntheses of all targets. Compound 2, the simplest reversed ester analogue of 1 (Chart 1), exhibited a 3.5-fold reduction in binding affinity toward PK-C alpha which we attributed to the loss of a stabilizing gauche interaction that caused the ester branch in 2 to be more disordered than in the normal ester 1. However, conversion of the propanoyl branch of 2 into a propenoyl branch restored binding affinity (3 versus 5). As expected, the compounds bound to the enzyme with strict enantioselectivity (3 and 5 versus 4 and 6). Functionalization of the propenoyl-branched compounds as alpha-alkylidene lactones, in a manner which proved successful with the 5(-)[(acyloxy)methyl]-5-(hydroxymethyl)tetrahydro-2-furanone template (9 and 10), produced stable compounds with equivalent ultrapotent binding affinities for PK-C alpha (7 and 8). The additional incorporation of the propenoyl-branched carbonyl into a gamma-lactone ring was performed (11-14) not only to derive a possible additional entropic advantage but also to confirm the spatial disposition of this carbonyl function in the ligand-enzyme complex. Although no additional entropic advantage was derived, the high binding affinities displayed by compounds 11 and 12 helped to establish the correct orientation of the equivalent carbonyl group in PK-C-bound DAG. As expected, these DAG analogues activated PK-C alpha. The most potent agonist, compound 8, stimulated phosphorylation of the alpha-pseudosubstrate peptide, and in primary mouse keratinocytes it caused inhibition of binding of epidermal growth factor with an ED50 of approximately 1 microM. In contrast to the phorbol esters, compound 8 did not induce acute edema or hyperplasia in skin of CD-1 mice, and its pattern of downregulation with several PK-C isozymes was different from that of phorbol 12-myristate 13-acetate (PMA).
先前已表明,基于5-[(酰氧基)甲基]-5-(羟甲基)四氢-2-呋喃酮模板(图1中的1)构建的二酰基甘油(DAG)的构象受限类似物以立体特异性方式与蛋白激酶Cα(PK-Cα)紧密结合。然而,这些化合物通过快速的酰基迁移容易发生外消旋化并失去生物活性。为了解决这个问题,设计了“反向酯”类似物作为一组新的PK-C配体。酯功能的这种反转产生了一些新的DAG模拟物,它们嵌入在C-4双分支庚糖-1,4-内酯模板中。反向酯类似物不易发生外消旋化,并且它们化学性质不同的分支促进了所有目标物的对映体特异性合成。化合物2是1(图1)最简单的反向酯类似物,其对PK-Cα的结合亲和力降低了3.5倍,我们将其归因于稳定的邻位交叉相互作用的丧失,这导致化合物2中的酯分支比正常酯1中的酯分支更无序。然而,将化合物2的丙酰基分支转化为丙烯酰基分支恢复了结合亲和力(3对5)。正如预期的那样,这些化合物以严格的对映选择性与酶结合(3和5对4和6)。以在5-[(酰氧基)甲基]-5-(羟甲基)四氢-2-呋喃酮模板(9和10)中证明成功的方式,将丙烯酰基分支的化合物官能化为α-亚烷基内酯,产生了对PK-Cα具有等效超强力结合亲和力的稳定化合物(7和8)。将丙烯酰基分支的羰基进一步并入γ-内酯环中(11 - 14),不仅是为了获得可能的额外熵优势,也是为了确认该羰基官能团在配体 - 酶复合物中的空间排列。虽然没有获得额外的熵优势,但化合物11和12显示出的高结合亲和力有助于确定PK-C结合的DAG中等效羰基的正确取向。正如预期一样,这些DAG类似物激活了PK-Cα。最有效的激动剂化合物8刺激了α-假底物肽的磷酸化,并且在原代小鼠角质形成细胞中,它导致表皮生长因子结合的抑制,ED50约为1 microM。与佛波酯不同,化合物8在CD-1小鼠的皮肤中不诱导急性水肿或增生,并且其对几种PK-C同工酶的下调模式与佛波醇12-肉豆蔻酸酯13-乙酸酯(PMA)不同。
