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小鼠体内分枝杆菌索状因子在毒性和致肉芽肿活性方面与分子及超分子结构相关的差异

Molecular and supra-molecular structure related differences in toxicity and granulomatogenic activity of mycobacterial cord factor in mice.

作者信息

Fujita Yukiko, Okamoto Yuko, Uenishi Yuko, Sunagawa Makoto, Uchiyama Takehiko, Yano Ikuya

机构信息

Japan BCG Central Laboratory, 3-1-5 Matsuyama, Kiyose-shi, Tokyo 204-0022, Japan.

出版信息

Microb Pathog. 2007 Jul;43(1):10-21. doi: 10.1016/j.micpath.2007.02.006. Epub 2007 Mar 12.

Abstract

To establish the structure biological activity relationship of cord factor (trehalose 6,6'-dimycolate, TDM), we compared the molecular or supra-molecular structure of TDM micelles with toxicity, thymic atrophy and granulomatogenicity in lungs and spleen of BALB/c mice. According to the difference in the mycolyl subclass composition, TDM was divided into two groups, one possessing alpha-, methoxy- and keto-mycolates in M. tuberculosis H37Rv, M. bovis BCG and M. kansasii (group A) and the other having alpha-, keto- and wax ester-mycolates in M. avium serotype 4, M. phlei and M. flavescens (group B), although mycolic acid molecular species composition differed in each group considerably. Supra-molecular structure of TDM micelle differed species to species substantially and the micelle size of TDM from M. bovis BCG Connaught was the largest. The highest toxicity was shown with TDM from M. tuberculosis H37Rv which possessed the highest amount of alpha- (47.3%) and methoxy-mycolates (40.8%), while TDM from M. phlei having the low amount of alpha-mycolate (11.6%) showed almost no toxicity with the given doses. The thymic atrophy was observed with TDM from group A, but not with TDM from group B. On the other hand, TDM from group B showed massive lung granulomatogenic activity based on the histological observations and organ indices. Taken together, group A TDM showed a wide variety of micelle sizes and specific surface areas, high to low toxicity and marked to moderate granulomatogenicity, while group B TDM showed smaller sizes of micelles and larger specific surface areas, lower toxicity but higher granulomatogenicity in lungs. Existence of higher amount of longer chain alpha-mycolates in TDM appeared to be essential for high toxicity and thymic apoptotic activity, whereas TDM possessing wax ester-mycolate with smaller sized micelles seemed to be less toxic, but more granulomatogenic in lungs in mice. Thus, the mycolic acid subclass and molecular species composition of TDM affect critically the micelle forms, toxicity and granulomatogenicity in mice, while the relative abundances and carbon chain length of alpha-mycolate affected the toxicity in mice.

摘要

为了建立索状因子(海藻糖6,6'-二霉菌酸酯,TDM)的结构与生物活性的关系,我们比较了TDM胶束的分子或超分子结构与BALB/c小鼠肺和脾中的毒性、胸腺萎缩及肉芽肿形成能力。根据霉菌酸亚类组成的差异,TDM被分为两组,一组在结核分枝杆菌H37Rv、牛分枝杆菌卡介苗和堪萨斯分枝杆菌中含有α-、甲氧基-和酮基-霉菌酸(A组),另一组在鸟分枝杆菌血清型4、草分枝杆菌和微黄分枝杆菌中含有α-、酮基-和蜡酯-霉菌酸(B组),尽管每组中霉菌酸分子种类组成差异很大。TDM胶束的超分子结构在不同菌种间有很大差异,来自牛分枝杆菌卡介苗康诺特株的TDM胶束尺寸最大。来自结核分枝杆菌H37Rv的TDM毒性最高,其α-霉菌酸含量最高(47.3%)且甲氧基-霉菌酸含量较高(40.8%),而来自草分枝杆菌的TDM中α-霉菌酸含量较低(11.6%),在给定剂量下几乎无毒性。A组的TDM可观察到胸腺萎缩,而B组的TDM则未观察到。另一方面,基于组织学观察和器官指数,B组的TDM显示出大量的肺肉芽肿形成活性。综上所述,A组TDM表现出多种胶束尺寸和比表面积,毒性从高到低,肉芽肿形成能力从明显到中等,而B组TDM表现出较小的胶束尺寸和较大的比表面积,毒性较低但在小鼠肺中的肉芽肿形成能力较高。TDM中较长链α-霉菌酸含量较高似乎是高毒性和胸腺凋亡活性所必需的,而含有蜡酯-霉菌酸且胶束尺寸较小的TDM毒性似乎较低,但在小鼠肺中更易形成肉芽肿。因此,TDM的霉菌酸亚类和分子种类组成严重影响小鼠中的胶束形式、毒性和肉芽肿形成能力,而α-霉菌酸的相对丰度和碳链长度影响小鼠中的毒性。

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