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微管与淋巴细胞反应:秋水仙碱和紫杉醇对有丝分裂原诱导的人淋巴细胞活化和增殖的影响。

Microtubules and lymphocyte responses: effect of colchicine and taxol on mitogen-induced human lymphocyte activation and proliferation.

作者信息

Cuthbert J A, Shay J W

出版信息

J Cell Physiol. 1983 Aug;116(2):127-34. doi: 10.1002/jcp.1041160202.

Abstract

The role of microtubules in mitogen-induced human lymphocyte activation and proliferation was examined. The effect of colchicine, a microtubule-disrupting agent, was compared with taxol, a microtubule-stabilizing drug, and with isaxonine (N-isopropyl-amino-2-pyrimidine orthophosphate), a proposed microtubular-active drug. Lymphocyte proliferation, assessed by measuring the increase in the number of cells in mitogen-stimulated cultures, was completely suppressed by both colchicine and taxol (100 nM) whereas significant inhibition by isaxonine required much higher concentrations (5 mM). In order to characterize the inhibition, initial lymphocyte blast transformation and subsequent DNA synthesis were investigated. Neither colchicine nor taxol inhibited lymphocyte blast transformation assessed by quantitating the change in volume of the stimulated cells after a 24-hour incubation. In contrast, isaxonine (2-5 mM) suppressed blast transformation. Initial DNA synthesis, evaluated by measuring the cumulative incorporation of [3H]thymidine between 30 and 48 hours of culture, was inhibited in a concentration-dependent manner by both isaxonine and colchicine but not by taxol. Electron microscopic studies confirmed that both taxol and colchicine (10 nM) arrested the responding lymphocytes in mitosis, and that isaxonine inhibited initial activation. These results suggest that normal microtubule function is only necessary for cell division and that drug effects on blast transformation and initial DNA synthesis are unrelated to microtubules.

摘要

研究了微管在有丝分裂原诱导的人淋巴细胞活化和增殖中的作用。将微管破坏剂秋水仙碱的作用与微管稳定剂紫杉醇以及一种推测具有微管活性的药物异索诺宁(N - 异丙基 - 氨基 - 2 - 嘧啶正磷酸盐)进行了比较。通过测量有丝分裂原刺激培养物中细胞数量的增加来评估淋巴细胞增殖,秋水仙碱和紫杉醇(100 nM)均可完全抑制,而异索诺宁则需要更高的浓度(5 mM)才有显著抑制作用。为了表征这种抑制作用,研究了初始淋巴细胞的母细胞转化和随后的DNA合成。在孵育24小时后,通过定量刺激细胞体积的变化来评估,秋水仙碱和紫杉醇均未抑制淋巴细胞的母细胞转化。相比之下,异索诺宁(2 - 5 mM)可抑制母细胞转化。通过测量培养30至48小时之间[3H]胸腺嘧啶核苷的累积掺入来评估初始DNA合成,异索诺宁和秋水仙碱均以浓度依赖性方式抑制,而紫杉醇则无此作用。电子显微镜研究证实,紫杉醇和秋水仙碱(10 nM)均可使反应性淋巴细胞停滞在有丝分裂期,而异索诺宁则抑制初始活化。这些结果表明,正常的微管功能仅对细胞分裂是必需的,并且药物对母细胞转化和初始DNA合成的作用与微管无关。

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