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葡萄穗霉属真菌Stachybotrys sp.CPCC 401591中phenylspirodrimane类化合物抗肿瘤活性研究
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作者 荣小婷 何文妮 +5 位作者 郭哲 李鑫鑫 王璐 高坤 余利岩 张涛 《天然产物研究与开发》 CAS CSCD 2023年第8期1348-1356,共9页
本论文以葡萄穗霉属真菌Stachybotrys sp.CPCC 401591为研究对象,对其phenylspirodrimane(PSM)类化合物进行化学分离并评价单体化合物抗肿瘤活性。采用OSMAC(one strain many compounds)技术对菌株CPCC 401591发酵培养基优化,并结合LC-M... 本论文以葡萄穗霉属真菌Stachybotrys sp.CPCC 401591为研究对象,对其phenylspirodrimane(PSM)类化合物进行化学分离并评价单体化合物抗肿瘤活性。采用OSMAC(one strain many compounds)技术对菌株CPCC 401591发酵培养基优化,并结合LC-MS/MS质谱分子网络分析、正相硅胶柱、反相硅胶柱以及半制备高效液相色谱等分离技术,对目标菌株CPCC 401591发酵产物的乙酸乙酯提取相,进行化合物分离纯化。结合质谱、核磁波谱数据、钼试剂诱导圆二色谱(CD)以及文献检索比对,共分离获得8个PSM类单体化合物。同时,采用CCK-8比色法对化合物1~8的抗肿瘤活性进行评价。结果表明:化合物1~8均为聚酮来源杂萜分子,分别为chartarlactam H(1)、chartarlactam F(2)、stachybotrin(3)、chartarlactam K(4)、stachybotrylactam(5)、F1839-A(6)、Mer-VGF724B(7)、3α-hydroxyl-N-isopropyl carboxyl-phenylspirodrimane(8)。化合物对人肝癌细胞株HepG2、人宫颈癌细胞株HeLa和人结肠癌细胞株HCT116具有较好的抑瘤活性。本研究丰富了该菌次级代谢产物的结构多样性,也为从葡萄穗霉属类真菌中发现更多的抗肿瘤活性分子提供科学依据。 展开更多
关键词 葡萄穗霉属 天然产物分子网络分析 phenylspirodrimane 抗肿瘤活性 结构鉴定
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Phenylspirodrimanes类混源萜的合成研究进展
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作者 吴福芳 王洪涛 +1 位作者 沈晓宝 盛良全 《合成化学》 CAS CSCD 2017年第8期711-719,共9页
Phenylspirodrimanes类混源萜具有多种生物活性,其合成研究一直倍受研究人员的关注。综述了Phenylspirodrimanes类混源萜的合成研究进展,主要介绍了K-76,L-671、776,Stachybotrylactam和Corallidictyals A-D的全合成方法,并对其未来发... Phenylspirodrimanes类混源萜具有多种生物活性,其合成研究一直倍受研究人员的关注。综述了Phenylspirodrimanes类混源萜的合成研究进展,主要介绍了K-76,L-671、776,Stachybotrylactam和Corallidictyals A-D的全合成方法,并对其未来发展进行了展望。参考文献28篇。 展开更多
关键词 phenylspirodrimane 全合成 综述
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5,5,8aβ-三甲基-6β-羟基-反八氢-1-萘酮的合成及在Phenylspirodrimane类混源萜天然产物骨架构建中的应用
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作者 户志远 万秋香 +2 位作者 周航 宋传君 常俊标 《高等学校化学学报》 SCIE EI CAS CSCD 北大核心 2020年第5期955-959,共5页
以(E)-5,9-二甲基-4,8-癸二烯酸乙酯为原料,发展了一种合成5,5,8aβ-三甲基-6β-羟基-反八氢-1-萘酮(1)的新方法,并将其成功应用于phenylspirodrimane类混源萜天然产物骨架的构建.对合成过程中所涉及的关键反应如区域选择性环氧化和Cp 2... 以(E)-5,9-二甲基-4,8-癸二烯酸乙酯为原料,发展了一种合成5,5,8aβ-三甲基-6β-羟基-反八氢-1-萘酮(1)的新方法,并将其成功应用于phenylspirodrimane类混源萜天然产物骨架的构建.对合成过程中所涉及的关键反应如区域选择性环氧化和Cp 2TiCl催化的自由基串联环合反应进行了优化.所合成化合物的结构均通过核磁共振波谱(NMR)和高分辨质谱(HRMS)进行了表征和确认. 展开更多
关键词 5 5 8aβ-三甲基-6β-羟基-反八氢-1-萘酮 phenylspirodrimane类混源萜 环氧化 自由基串联环合反应
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Structural diversification of phenylspirodrimane lactams by employing a biosynthetic intermediate
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作者 Jimei Liu Zhenfei Wang +6 位作者 Jun Wu Yaotian Han Fei Ye Tiantai Zhang Haibo Yu Zhengshun Wen Jungui Dai 《Chinese Chemical Letters》 SCIE CAS CSCD 2023年第12期141-145,共5页
Phenylspirodrimanes are a kind of meroterpenoids with structural diversity and complexity,exhibiting a wide of biological properties,especially for the lactam derivatives consisting a y-lactam moiety and N-linked side... Phenylspirodrimanes are a kind of meroterpenoids with structural diversity and complexity,exhibiting a wide of biological properties,especially for the lactam derivatives consisting a y-lactam moiety and N-linked side chains.These compounds were derived from multi-step combination of enzymatic and non-enzymatic conversions of intermediates in their biosynthetic pathways.Stachbotrydial(2)with an o-phthalaldehyde unit was supposed as the high-reactivity intermediate of phenylspirodrimane lactams via nonenzymatic reaction with amines.In the present work,an effective and non-enzymatic diversification strategy was developed for the structural diversification of phenylspirodrimane lactams including monomers and dimers from 2 by feeding structurally various mono-and diamines in the fungus Stachybotrys chartarum cultures.In total,24 phenylspirodrimane lactams(1,3-25)including 18 new compounds were synthesized.Among them,stachybocin A(1),a bioactive phenylspirodrimane lactam dimer,was produced with the yield of 18.7 mg/g of cell dry weight.The structures of these compounds were elucidated by extensive spectroscopic data,single-crystal X-ray diffraction(Cu Kα),and calculated electronic circular dichroism(ECD)analyses.Bioassay revealed that compounds 1,17,and 24 displayed significant inhibitory effect on the inactivated state of hNav 1.2 channels with IC_(50) values of 0.22,2.08,and 0.53μmol/L,respectively.In addition,1 showed potent protein tyrosine phosphatase 1B(PTP1B)inhibitory N-methyl-b-aspartate(NMDA)receptor antagonistic,and anti-inflammatory activities. 展开更多
关键词 phenylspirodrimane lactams Stachbotrydial Nonenzymatic reaction hNav 1.2channels inhibitoryactivity Stachybotrys chartarum
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Bistachybotrysins D and E,one stereoisomeric pair of cytotoxic phenylspirodrimane dimers from Stachybotrys chartarum
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作者 Min Zhang Jiamin Feng +8 位作者 Xiaona Jia Jinlian Zhao Jimei Liu Ridao Chen Kebo Xie Dawei Chen Yan Li Dan Zhang Jungui Dai 《Chinese Chemical Letters》 SCIE CAS CSCD 2019年第2期435-438,共4页
Bistachybotrysins D and E (1 and 2), one stereoisomeric pair of phenylspirodrimane dimers, were isolated from Stachybotrys chartarum CGMCC 3.5365. They represent novel phenylspirodrimane dimers with a central [6,5,6]-... Bistachybotrysins D and E (1 and 2), one stereoisomeric pair of phenylspirodrimane dimers, were isolated from Stachybotrys chartarum CGMCC 3.5365. They represent novel phenylspirodrimane dimers with a central [6,5,6]-tricyclic carbon scaffold containing a cyclopentanone core. The structures of 1 and 2 were elucidated through extensive spectroscopic data analysis, and their absolute configurations were characterized by calculated electronic circular dichroism (ECD). Compounds 1 and 2 displayed potent cytotoxic activity against the four human tumor cell lines HCT116, BGC823, Daoy and HepG2 with IC_ (50)values ranging from 6.7 μmol/L to 11.6 μmol/L. Furthermore, a plausible biogenetic pathway for 1 and 2 is proposed. 展开更多
关键词 Bistachybotrysin Stereoisomeric PAIR phenylspirodrimane DIMER CYTOTOXIC ACTIVITY STACHYBOTRYS chartarum
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