Acroamine A, a 2-Amino Adenine Alkaloid from the Marine Soft Coral Acrozoanthus australiae and Its Semisynthetic Derivatives That Inhibit cAMP-Dependent Protein Kinase A Catalytic Subunit Alpha.

IF 3.3 2区 生物学 Q2 CHEMISTRY, MEDICINAL Journal of Natural Products Pub Date : 2024-08-23 Epub Date: 2024-08-14 DOI:10.1021/acs.jnatprod.4c00477
Sarath P D Senadeera, Dongdong Wang, Brice A P Wilson, Emily A Smith, Antony Wamiru, Juliana A Martinez Fiesco, Lin Du, Ping Zhang, Barry R O'Keefe, John A Beutler
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Abstract

A high throughput screen performed to identify catalytic inhibitors of the oncogenic fusion form of cAMP-dependent protein kinase A catalytic subunit alpha (J-PKAcα) found an individual fraction from an organic extract of the marine soft coral Acrozoanthus australiae as active. Bioassay-guided isolation led to the identification of a 2-amino adenine alkaloid acroamine A (1), the first secondary metabolite discovered from this genus and previously reported as a synthetic product. As a naturally occurring protein kinase inhibitor, to unambiguously assign its chemical structure using modern spectroscopic and spectrometric techniques, five N-methylated derivatives acroamines A1-A5 (2-6) were semisynthesized. Three additional brominated congeners A6-A8 (7-9) were also semisynthesized to investigate the structure-activity relationship of the nine compounds as J-PKAcα inhibitors. Compounds 1-9 were tested for J-PKAcα and wild-type PKA inhibitory activities, which were observed exclusively in acroamine A (1) and its brominated analogs (7-9) achieving moderate potency (IC50 2-50 μM) while none of the N-methylated analogs exhibited kinase inhibition.

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Acroamine A,一种来自海洋软珊瑚 Acrozoanthus australiae 的 2-Amino Adenine Alkaloid 及其半合成衍生物,可抑制 cAMP 依赖性蛋白激酶 A 催化亚基 Alpha。
为鉴定 cAMP 依赖性蛋白激酶 A 催化亚基α(J-PKAcα)致癌融合形式的催化抑制剂而进行的高通量筛选发现,从海洋软珊瑚 Acrozoanthus australiae 的有机提取物中提取的单个馏分具有活性。生物测定指导下的分离鉴定出了一种 2-氨基腺嘌呤生物碱阿克罗胺 A (1),这是首次从该属植物中发现的次级代谢产物,之前的报道称它是一种合成产物。作为一种天然存在的蛋白激酶抑制剂,为了利用现代光谱和分光技术明确其化学结构,我们半合成了五种 N-甲基化衍生物丙胺 A1-A5 (2-6)。为了研究这九种化合物作为 J-PKAcα 抑制剂的结构-活性关系,还对另外三种溴化同系物 A6-A8 (7-9)进行了半合成。对 1-9 化合物进行了 J-PKAcα 和野生型 PKA 抑制活性测试,结果显示,只有酰丙胺 A(1)及其溴化类似物(7-9)具有中等效力(IC50 2-50 μM),而 N-甲基化类似物均未表现出激酶抑制作用。
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来源期刊
CiteScore
9.10
自引率
5.90%
发文量
294
审稿时长
2.3 months
期刊介绍: The Journal of Natural Products invites and publishes papers that make substantial and scholarly contributions to the area of natural products research. Contributions may relate to the chemistry and/or biochemistry of naturally occurring compounds or the biology of living systems from which they are obtained. Specifically, there may be articles that describe secondary metabolites of microorganisms, including antibiotics and mycotoxins; physiologically active compounds from terrestrial and marine plants and animals; biochemical studies, including biosynthesis and microbiological transformations; fermentation and plant tissue culture; the isolation, structure elucidation, and chemical synthesis of novel compounds from nature; and the pharmacology of compounds of natural origin. When new compounds are reported, manuscripts describing their biological activity are much preferred. Specifically, there may be articles that describe secondary metabolites of microorganisms, including antibiotics and mycotoxins; physiologically active compounds from terrestrial and marine plants and animals; biochemical studies, including biosynthesis and microbiological transformations; fermentation and plant tissue culture; the isolation, structure elucidation, and chemical synthesis of novel compounds from nature; and the pharmacology of compounds of natural origin.
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