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Lectin-directed enzyme activated prodrug therapy (LEAPT): Synthesis and evaluation of rhamnose-capped prodrugs.

Abstract:
The lectin-directed enzyme activated prodrug therapy (LEAPT) bipartite drug delivery system utilizes glycosylated enzyme, localized according to its sugar pattern, and capped prodrugs released by that enzyme. In this way, the sugar coat of a synthetic enzyme determines the site of release of a given drug. Here, prodrugs of doxorubicin and 5-fluorouracil capped by the nonmammalian l-rhamnosyl sugar unit have been efficiently synthesized and evaluated for use in the LEAPT system. Both are stable in blood, released by synthetically d-galactosylated rhamnosidase enzyme, and do not inhibit the uptake of the synthetic enzyme to its liver target. These results are consistent with their proposed mode of action and efficacy in models of liver cancer, and confirm modular flexibility in the drugs that may be used in LEAPT.
Publication status:
Published

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Publisher copy:
10.3109/1061186x.2010.529909

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Journal:
Journal of drug targeting More from this journal
Volume:
18
Issue:
10
Pages:
794-802
Publication date:
2010-12-01
DOI:
EISSN:
1029-2330
ISSN:
1061-186X


Language:
English
Keywords:
Pubs id:
pubs:93189
UUID:
uuid:7d790662-cf16-4c7c-acbb-a03e5ae7fa60
Local pid:
pubs:93189
Source identifiers:
93189
Deposit date:
2012-12-19
ARK identifier:

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