Department of Chemistry, University of Hawaii at Manoa , Honolulu, Hawaii 96822, United States.
J Nat Prod. 2014 Jul 25;77(7):1644-9. doi: 10.1021/np500256w. Epub 2014 Jul 3.
New compounds 18-nor-3,17-dihydroxyspongia-3,13(16),14-trien-2-one (1), 18-nor-3,5,17-trihydroxyspongia-3,13(16),14-trien-2-one (2), and spongiapyridine (3) and the known compound 17-hydroxy-4-epi-spongialactone A (4) were isolated from an Indonesian sponge of the genus Spongia. The structures of 1-3 were deduced by analyses of physical and spectroscopic data. Diterpene 3 is unusual, as the D-ring is a pyridyl ring system rather than the standard δ-lactone. The structure elucidation of this compound was complicated by facile exchange of the axial proton at the C-11 methylene with deuterium from methanol-d4. The isolated compounds were tested for biological activity in a battery of in vitro assays (TNF-α-induced NFκB, LPS-induced iNOS, RXR stimulation, quinone reductase 1 induction, aromatase inhibition, TRPM7 ion channels, and aspartic protease BACE1 inhibition). Norditerpene 2 modestly inhibited aromatase with an IC50 of 34 μM and induced quinone reductase 1 activity with a CD (the concentration needed to double the enzymatic response) of 11.2 μM. The remaining isolates were inactive.
从印度尼西亚产的海绵属 Spongia 中分离得到了新化合物 18-降-3,17-二羟基海绵-3,13(16),14-三烯-2-酮(1)、18-降-3,5,17-三羟基海绵-3,13(16),14-三烯-2-酮(2)和海绵吡啶(3),以及已知化合物 17-羟基-4-表-海绵内酯 A(4)。通过分析物理和光谱数据推导出 1-3 的结构。二萜 3 是不寻常的,因为 D 环是吡啶环系统,而不是标准的δ-内脂。由于 C-11 亚甲基上的轴向质子易于与甲醇-d4 中的氘交换,因此该化合物的结构阐明变得复杂。对分离得到的化合物进行了一系列体外测定的生物活性测试(TNF-α 诱导的 NFκB、LPS 诱导的 iNOS、RXR 刺激、醌还原酶 1 诱导、芳香酶抑制、TRPM7 离子通道和天冬氨酸蛋白酶 BACE1 抑制)。降二萜 2 对芳香酶具有中等抑制作用,IC50 为 34 μM,并以 CD(使酶反应增加一倍所需的浓度)为 11.2 μM 诱导醌还原酶 1 活性。其余的分离物均无活性。
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