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铜酞菁标记的磁性微胶囊:具有平面分子结构的诱变剂的制备及其体外和体内结合特性

Copper phthalocyanine labelled magnetic microcapsules: preparation, and binding properties in vitro and in vivo for mutagens having planar molecular structure.

作者信息

Povey A C, O'Neill I K

机构信息

Paterson Institute for Cancer Research, Department of Carcinogenesis, Withington, Manchester, UK.

出版信息

Carcinogenesis. 1990 Nov;11(11):1989-93. doi: 10.1093/carcin/11.11.1989.

Abstract

Copper phthalocyanine tetrasulphonic acid (CPTS) functions were introduced into magnetic semi-permeable polyethyleneimine (PEI) microcapsules in order to create a recoverable scavenging system for trapping and biomonitoring, within the gastrointestinal cavity, of mutagens having a planar molecular structure. Stable ionic CPTS and covalent (thionylated CPTS, TCPTS) adducts to the microcapsule PEI were produced and shown to trap benzo[a]pyrene (B[a]P) in vitro in relation to the porphyrin/B[a]P ratio employed. 3-hydroxy B[a]P and B[a]P 3,6-dione from a crude B[a]P metabolite mixture, and a set of planar mutagens from crude opium/morphine pyrolysate mixtures could also be recovered in 7-86% yields after shaking with modified microcapsules followed by methanol/ammonia (50:1) desorption. Tetraols derived from B[a]P 7,8-diol-9,10 epoxide could also be recovered. Modified microcapsules were recovered magnetically from faeces of rats treated with [14C]B[a]P, and 45-51% of trapped radioactivity could be directly desorbed for HPLC assay compared with 30% for unmodified microscapsules. The relative extent of trapping by unmodified or CPTS- or TCPTS-modified microcapsules was different for various substrates, and it appears that the copper phthalocyanine tetrasulphonic acid moiety competes with another unidentified absorption/desorption structure in the microcapsules. These results show that selective and reversible trapping of carcinogens/mutagens having planar molecular structure can be achieved within the gastrointestinal tract.

摘要

将铜酞菁四磺酸(CPTS)功能引入磁性半透性聚乙烯亚胺(PEI)微胶囊中,以创建一种可回收的清除系统,用于在胃肠道腔内捕获和生物监测具有平面分子结构的诱变剂。制备了微胶囊PEI的稳定离子型CPTS和共价型(硫酰化CPTS,TCPTS)加合物,并证明其在体外捕获苯并[a]芘(B[a]P)的能力与所采用的卟啉/B[a]P比例有关。在与改性微胶囊振荡,然后用甲醇/氨水(50:1)解吸后,粗制B[a]P代谢物混合物中的3-羟基B[a]P和B[a]P 3,6-二酮,以及粗制鸦片/吗啡热解产物混合物中的一组平面诱变剂也可以7-86%的产率回收。源自B[a]P 7,8-二醇-9,10-环氧化物的四醇也可以回收。从用[14C]B[a]P处理的大鼠粪便中磁性回收改性微胶囊,与未改性微胶囊的30%相比,45-51%的捕获放射性可以直接解吸用于HPLC分析。未改性或CPTS或TCPTS改性微胶囊对各种底物的捕获相对程度不同,并且似乎铜酞菁四磺酸部分与微胶囊中另一种未鉴定的吸收/解吸结构竞争。这些结果表明,在胃肠道内可以实现对具有平面分子结构的致癌物/诱变剂的选择性和可逆捕获。

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