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Cytotoxic veraguamides, alkynyl bromide-containing cyclic depsipeptides from the marine cyanobacterium cf. Oscillatoria margaritifera.细胞毒性的韦拉古胺类化合物,来自海洋蓝藻 cf. 珍珠硷旋藻的含炔基溴的环状缩肽。
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Pitiprolamide, a proline-rich dolastatin 16 analogue from the marine cyanobacterium Lyngbya majuscula from Guam.来自关岛海洋蓝细菌 Lyngbya majuscula 的脯氨酸丰富的 dolastatin 16 类似物 Pitiprolamide。
J Nat Prod. 2011 Jan 28;74(1):109-12. doi: 10.1021/np1006839. Epub 2010 Dec 7.
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Biologically active secondary metabolites from marine cyanobacteria.海洋蓝细菌中的生物活性次生代谢产物。
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Anticolon cancer activity of largazole, a marine-derived tunable histone deacetylase inhibitor.拉帕醇作为一种海洋来源的组蛋白去乙酰化酶抑制剂,具有抗肿瘤活性。
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Natural antifoulants from the marine cyanobacterium Lyngbya majuscula.海洋蓝藻 Lyngbya majuscula 的天然防污剂。
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Hantupeptins B and C, cytotoxic cyclodepsipeptides from the marine cyanobacterium Lyngbya majuscula.海兔肽 B 和 C,来源于海洋蓝藻 Lyngbya majuscula 的细胞毒环二肽。
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Hantupeptin A, a cytotoxic cyclic depsipeptide from a Singapore collection of Lyngbya majuscula.汉图肽素A,一种从新加坡采集的巨大鞘丝藻中提取的具有细胞毒性的环缩肽。
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Structure and activity of largazole, a potent antiproliferative agent from the Floridian marine cyanobacterium Symploca sp.来自佛罗里达海洋蓝藻Symploca sp.的强效抗增殖剂拉戈唑的结构与活性
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瓦拉瓜米德 A-G,来自关岛产海兔素 16 的蓝细菌 Symploca cf. hydnoides 的环状六肽。

Veraguamides A-G, cyclic hexadepsipeptides from a dolastatin 16-producing cyanobacterium Symploca cf. hydnoides from Guam.

机构信息

Department of Medicinal Chemistry, University of Florida, 1600 SW Archer Road, Gainesville, Florida 32610, United States.

出版信息

J Nat Prod. 2011 May 27;74(5):917-27. doi: 10.1021/np200076t. Epub 2011 Mar 29.

DOI:10.1021/np200076t
PMID:21446699
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3103655/
Abstract

Cytotoxicity-directed purification of a Symploca cf. hydnoides sample from Cetti Bay, Guam, afforded seven new cyclic depsipeptides, veraguamides A-G (1-7), together with the known compound dolastatin 16. The planar structures of 1-7 were elucidated using NMR and MS experiments, while enantioselective HPLC and Mosher's analysis of acid and base hydrolysates, respectively, were utilized to assign the absolute configurations of the stereocenters. Veraguamides A-G (1-7) are characterized by the presence of an invariant proline residue, multiple N-methylated amino acids, an α-hydroxy acid, and a C8-polyketide-derived β-hydroxy acid moiety with a characteristic terminus as either an alkynyl bromide, alkyne, or vinyl group. These compounds and a semisynthetic analogue (8) showed moderate to weak cytotoxic activity against HT29 colorectal adenocarcinoma and HeLa cervical carcinoma cell lines. Preliminary structure-activity relationship analysis identified several sensitive positions in the veraguamide scaffold that affect the cytotoxic activity of this compound class. Dolastatin 16 showed only weak cytotoxic activity on both cell lines tested. The complete stereostructure of dolastatin 16 was proposed for the first time through degradation followed by a combination of advanced Marfey's analysis and modified Mosher's analysis using phenylglycine methyl ester as a chiral anisotropic reagent.

摘要

从关岛切蒂湾的 Symploca cf. hydnoides 样品中进行细胞毒性导向的纯化,得到了 7 个新的环状 depsipeptides,即 veraguamides A-G(1-7),以及已知的化合物 dolastatin 16。使用 NMR 和 MS 实验阐明了 1-7 的平面结构,而分别通过对酸和碱水解产物进行对映选择性 HPLC 和 Mosher 分析,用于确定手性中心的绝对构型。Veraguamides A-G(1-7)的特征在于存在不变的脯氨酸残基、多个 N-甲基化的氨基酸、α-羟基酸和 C8-聚酮衍生的β-羟基酸部分,其特征末端为炔基溴、炔烃或乙烯基。这些化合物和半合成类似物(8)对 HT29 结肠直肠腺癌细胞系和 HeLa 宫颈癌细胞系表现出中等至弱的细胞毒性。初步的结构-活性关系分析确定了 veraguamide 支架中几个影响该化合物类别的细胞毒性的敏感位置。Dolastatin 16 在两种测试的细胞系上仅显示出弱的细胞毒性活性。通过降解,然后使用苯甘氨酸甲酯作为手性各向异性试剂,结合先进的 Marfey 分析和改良的 Mosher 分析,首次提出了 dolastatin 16 的完整立体结构。