Donor-acceptor [4]- and [6]rotaxanes have been prepared from bipyridinium (BIPY(2+)) oligomers and 1,5-dinaphtho[38]crown-10 (DN38C10) by a threading-followed-by-stoppering protocol employing click chemistry. An efficient, straightforward route to the BIPY(2+) oligomers has been developed that requires little to no chromatographic purification. Unlike most donor-acceptor oligorotaxanes that have been reported to date, 100% of the recognition sites on the dumbbells are occupied by rings.
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http://dx.doi.org/10.1021/ol302301r | DOI Listing |
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