共查询到20条相似文献,搜索用时 15 毫秒
1.
Andreas Gollner Dipl.‐Ing. Karl‐Heinz Altmann Prof. Dr. Jürg Gertsch Dr. Johann Mulzer Prof. Dr. 《Chemistry (Weinheim an der Bergstrasse, Germany)》2009,15(24):5979-5997
A sensitive family : The first total synthesis of the antitumor agents neolaulimalide and isolaulimalide as well as a highly efficient route to laulimalide is described. A Kulinkovich reaction followed by a cyclopropyl–allyl rearrangement is used to install the exo‐methylene group. The cytotoxicity of neolaulimalide could be confirmed for the first time since its original isolation and it could be shown that it induces tubulin polymerization as efficiently as laulimalide.
2.
3.
Gagnepain J Moulin E Nevado C Waser M Maier A Kelter G Fiebig HH Fürstner A 《Chemistry (Weinheim an der Bergstrasse, Germany)》2011,17(25):6973-6984
Systematic variation of all substructures embedded into the framework of iejimalide B (2) led to a panel of synthetic analogues of this polyunsaturated macrolide, featuring structural modifications that are not accessible by derivatization of the natural lead compound itself. The assessment of the cytotoxicity of these compounds with the aid of a monolayer proliferation assay (12 human tumor cell lines in vitro) as well as a colony formation assay (24 human tumor xenografts ex vivo) revealed the exceptional potency of 2 and several of its synthetic congeners, with IC(50) values in the picomolar range for the most sensitive cell lines. Whereas structural modifications of the macrocycle or of the side chain generally lead to a decrease in activity, changes of the peptidic terminus are not only well accommodated but engender increased tumor selectivity as well. 2 and two of the most promising analogues were selected for in vivo studies in mice, in which their activity against human tumor xenografts of breast cancer (MAXF 401) and prostate cancer (PRXF PC-3M) was tested. In contrast to a previous report in the literature however, which had claimed in vivo activity for the parent iejimalides, these tests did not show a significant therapeutic effect against the chosen solid tumors upon intraperitoneal administration. 相似文献
4.
5.
6.
7.
Håkansson AE Palmelund A Holm H Madsen R 《Chemistry (Weinheim an der Bergstrasse, Germany)》2006,12(12):3243-3253
The stereocontrolled synthesis of (+)-7-deoxypancratistatin is described. The convergent synthesis has been achieved by two different strategies, both of which commence from a pentose and piperonal. The latter is converted into allylic bromide 7, which is then coupled with a protected methyl 5-deoxy-5-iodo-D-ribofuranoside in the presence of zinc metal. The first strategy involves a total of only 13 steps from D-ribose and piperonal, but suffers from a low yield in the zinc-mediated reaction between ribofuranoside 9, benzylamine, and bromide 7. The second strategy involves a total of 18 steps from D-xylose and piperonal. The former is converted into ribofuranoside 28, which is coupled with bromide 7 in the presence of zinc, and this is followed by ring-closing olefin metathesis. Subsequent Overman rearrangement, dihydroxylation, and deprotection then affords the natural product. 相似文献
8.
9.
Dr. Andreas Rentsch Dr. Dirk Landsberg Dr. Tobias Brodmann Dr. Leila Bülow Dr. Anna‐Katharina Girbig Prof. Dr. Markus Kalesse 《Angewandte Chemie (International ed. in English)》2013,52(21):5450-5488
Shortly after the discovery of the proteasome it was proposed that inhibitors could stabilize proteins which ultimately would trigger apoptosis in tumor cells. The essential questions were whether small molecules would be able to inhibit the proteasome without generating prohibitive side effects and how one would derive these compounds. Fortunately, “Mother Nature” has generated a wide variety of natural products that provide distinct selectivities and specificities. The chemical synthesis of these natural products finally provided access to analogues and optimized drugs of which two different classes have been approved for the treatment of malignancies. Despite these achievements, additional lead structures derived from nature are under investigation and will be discussed with regard to their biological potential and chemical challenges. 相似文献
10.
11.
12.
13.
14.
Schinzer D Bourguet E Ducki S 《Chemistry (Weinheim an der Bergstrasse, Germany)》2004,10(13):3217-3224
The total synthesis of furano-epothilone D by a convergent route is reported. The key fragments are available on a large scale to provide sufficient material for biological evaluation. The approach involves a palladium-catalyzed coupling that generates a highly functionalized aldehyde which is connected in a stereoselective aldol reaction to yield the framework of furano-epothilone D. Finally, a macrolactonization provides furano-epothilone D. 相似文献
15.
16.
The Synthesis and Biological Evaluation of Desepoxyisotedanolide and a Comparison with Desepoxytedanolide 下载免费PDF全文
Arun Naini Dr. Yazh Muthukumar Dr. Aruna Raja Dr. Raimo Franke Ian Harrier Prof. Dr. Amos B. Smith III Prof. Dr. Dongjoo Lee Prof. Dr. Richard E. Taylor Dr. Florenz Sasse Prof. Dr. Markus Kalesse 《Angewandte Chemie (International ed. in English)》2015,54(23):6935-6939
The tedanolides are biologically active polyketides that exhibit a macrolactone constructed from a primary alcohol. Since polyketidal transformations only generate secondary alcohols, it has been hypothesized by Taylor that this unique lactone could arise from a postketidal transesterification. In order to probe this hypothesis and to investigate the biological profile of the putative precursor of all members of the tedanolide family, we embarked on the synthesis of desepoxyisotedanolide and its biological evaluation in comparison to desepoxytedanolide. The biological experiments unraveled a second target for desepoxytedanolide and provided evidence that the proposed transesterification indeed provides a survival advantage for the producing microorganism. 相似文献
17.
18.