2001
DOI: 10.1021/jm010089z
|View full text |Cite
|
Sign up to set email alerts
|

Phenoxypropoxybiguanides, Prodrugs of DHFR−Inhibiting Diaminotriazine Antimalarials

Abstract: A total of 34 analogues of the biguanide PS-15 (5s), a prodrug of the diaminotriazine WR-99210 (8s), have been prepared. Several of them, such as 5b (PS-33) and 5m (PS-26), maintain or exceed the in vivo activity of PS-15 while not requiring the use of highly regulated starting materials. The putative diaminotriazine metabolites of these new analogues (compounds 8) have also been prepared and shown to maintain the activity against resistant P. falciparum strains. The structure-activity relationships of biguani… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
2
1
1
1

Citation Types

1
66
0

Year Published

2002
2002
2020
2020

Publication Types

Select...
9
1

Relationship

0
10

Authors

Journals

citations
Cited by 89 publications
(67 citation statements)
references
References 21 publications
1
66
0
Order By: Relevance
“…Importantly, the methods employed in our study cannot distinguish between folic acid and PUR-1 competition for uptake through the PSAC channel on the outer membrane of the infected cell vs. competition for uptake across a carrier protein located on the parasite plasma membrane. However, taken together with the findings of Nzila et al (Nzila, et al, 2003) and Wang et al (Wang, et al, 1999) it seems reasonable to believe that a selective inhibitor of the NPP will block uptake of exogenous folic acid from the bloodstream and function synergistically with selective inhibitors of parasite dihydrofolate reductase, such as WR99210 (Canfield, et al, 1993,Kinyanjui, et al, 1999 and "biguanide" prodrugs of the Jacobus series (Jensen, et al, 2001). …”
Section: Inhibition Of Pur-1 Staining By Furosemidementioning
confidence: 97%
“…Importantly, the methods employed in our study cannot distinguish between folic acid and PUR-1 competition for uptake through the PSAC channel on the outer membrane of the infected cell vs. competition for uptake across a carrier protein located on the parasite plasma membrane. However, taken together with the findings of Nzila et al (Nzila, et al, 2003) and Wang et al (Wang, et al, 1999) it seems reasonable to believe that a selective inhibitor of the NPP will block uptake of exogenous folic acid from the bloodstream and function synergistically with selective inhibitors of parasite dihydrofolate reductase, such as WR99210 (Canfield, et al, 1993,Kinyanjui, et al, 1999 and "biguanide" prodrugs of the Jacobus series (Jensen, et al, 2001). …”
Section: Inhibition Of Pur-1 Staining By Furosemidementioning
confidence: 97%
“…In an effort to circumvent these problems PS-15 ( Fig. 5), the phenoxypropoxybiguanide precursor for WR99210, was synthesized [68]. However, further assessment of PS-15 was suspended because of regulatory restrictions in the use of the starting material, i.e.…”
Section: Artemisinin and Its Derivatesmentioning
confidence: 99%
“…Hastings and Sibley in particular look at many more mutants in their analysis. The drugs under comparison in Table 1 are limited to (i) pyrimethamine, a 2,4-diaminopyrimidine that is the most widely used antimalarial DHFR inhibitor and is a key component of the drug sulfadoxinepyrimethamine, (ii) chlorcycloguanil, a triazine DHFR inhibitor and the active metabolite of chlorproguanil, which is a key component of a fixed dose combination of chlorproguanil-dapsone (or Lapdap), which has undergone phase-three studies in a partnership involving GlaxoSmithKline and WHO͞TDR and is about to be submitted for regulatory approval (15), and (iii) WR99210, a phenoxypropoxydiaminotriazine, a member of a family of DHFR inhibitors that are generated as metabolites from the corresponding biguanide, some of which are being considered for development (16).…”
Section: Comparison Of Hastings and Sibley's Work (7) With Other Recementioning
confidence: 99%