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微管稳定剂discodermolide竞争性抑制紫杉醇(泰素)与微管蛋白聚合物的结合,比紫杉醇更有效地增强微管蛋白的成核反应,并抑制紫杉醇耐药细胞的生长。

The microtubule-stabilizing agent discodermolide competitively inhibits the binding of paclitaxel (Taxol) to tubulin polymers, enhances tubulin nucleation reactions more potently than paclitaxel, and inhibits the growth of paclitaxel-resistant cells.

作者信息

Kowalski R J, Giannakakou P, Gunasekera S P, Longley R E, Day B W, Hamel E

机构信息

Laboratory of Drug Discovery Research and Development, Developmental Therapeutics Program, Division of Cancer Treatment, Diagnosis, and Centers, National Cancer Institute, Frederick Cancer Research and Development Center, Frederick, Maryland 21702, USA.

出版信息

Mol Pharmacol. 1997 Oct;52(4):613-22.

PMID:9380024
Abstract

The lactone-bearing polyhydroxylated alkatetraene (+)-discodermolide, which was isolated from the sponge Discodermia dissoluta, induces the polymerization of purified tubulin with and without microtubule-associated proteins or GTP, and the polymers formed are stable to cold and calcium. These effects are similar to those of paclitaxel (Taxol), but discodermolide is more potent. We confirmed that these properties represent hypernucleation phenomena; we obtained lower tubulin critical concentrations and shorter polymers with discodermolide than paclitaxel under a variety of reaction conditions. Furthermore, we demonstrated that discodermolide is a competitive inhibitor with [3H]paclitaxel in binding to tubulin polymer, with an apparent Ki value of 0.4 microM. Multidrug-resistant human colon and ovarian carcinoma cells overexpressing P-glycoprotein, which are 900- and 2800-fold resistant to paclitaxel, respectively, relative to the parental lines, retained significant sensitivity to discodermolide (25- and 89-fold more resistant relative to the parental lines). Ovarian carcinoma cells that are 20-30-fold more resistant to paclitaxel than the parental line on the basis of expression of altered beta-tubulin polypeptides retained nearly complete sensitivity to discodermolide. The effects of discodermolide on the reorganization of the microtubules of Potorous tridactylis kidney epithelial cells were examined at different times. Intracellular microtubules were reorganized into bundles in interphase cells much more rapidly after discodermolide treatment compared with paclitaxel treatment. A variety of spindle aberrations were observed after treatment with both drugs. The proportions of the different types of aberration were different for the two drugs and changed with the length of drug treatment.

摘要

从海绵溶骨盘皮海绵中分离出的含内酯多羟基化链状四烯(+)-盘状软骨素,能在有或无微管相关蛋白或鸟苷三磷酸(GTP)的情况下诱导纯化的微管蛋白聚合,形成的聚合物对冷和钙稳定。这些作用与紫杉醇(泰素)相似,但盘状软骨素的作用更强。我们证实这些特性代表了超成核现象;在各种反应条件下,与紫杉醇相比,盘状软骨素使微管蛋白临界浓度更低,聚合物更短。此外,我们证明盘状软骨素是[3H]紫杉醇与微管蛋白聚合物结合的竞争性抑制剂,其表观抑制常数(Ki)值为0.4微摩尔。过表达P-糖蛋白的多药耐药人结肠癌细胞和卵巢癌细胞,相对于亲代细胞系,对紫杉醇的耐药性分别为900倍和2800倍,但对盘状软骨素仍保持显著敏感性(相对于亲代细胞系耐药性分别低25倍和89倍)。基于β-微管蛋白多肽表达改变而对紫杉醇耐药性比亲代细胞系高20 - 30倍的卵巢癌细胞,对盘状软骨素几乎保持完全敏感性。在不同时间检测了盘状软骨素对长吻袋貂肾上皮细胞微管重组的影响。与紫杉醇处理相比,盘状软骨素处理后,间期细胞内的微管更快地重组为束状。两种药物处理后均观察到多种纺锤体畸变。两种药物不同类型畸变的比例不同,且随药物处理时间的延长而变化。

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