2000
DOI: 10.1002/chin.200035178
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ChemInform Abstract: Design and Synthesis of Cyclopenta[g]quinazoline‐Based Antifolates as Inhibitors of Thymidylate Synthase and Potential Antitumor Agents.

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Cited by 5 publications
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“…35,36 Among other improvements, this route did not require the cobalt catalyst system used in earlier routes. 31,32 A molar yield of 13.3% with respect to the tricyclic acid starting material was achieved in very good quality. The purity results were 99.5% of area percent basis (a/a) by achiral HPLC, 99.6% enantiomeric excess (ee) 6S chiral purity, and 99.8% L,D diastereomeric purity (see Experimental Section).…”
Section: ■ Resultsmentioning
confidence: 91%
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“…35,36 Among other improvements, this route did not require the cobalt catalyst system used in earlier routes. 31,32 A molar yield of 13.3% with respect to the tricyclic acid starting material was achieved in very good quality. The purity results were 99.5% of area percent basis (a/a) by achiral HPLC, 99.6% enantiomeric excess (ee) 6S chiral purity, and 99.8% L,D diastereomeric purity (see Experimental Section).…”
Section: ■ Resultsmentioning
confidence: 91%
“…The inhibitor 1 (Figure and Scheme A) belongs to a series of cyclopenta([ g ]quinazoline-based antifolates for which synthesis and development have been described previously. , These compounds were synthesized by stepwise addition of a p -aminobenzoate moiety, an N10-substituent, and a dipeptide moiety to a cyclopenta[ g ]quinazoline ring. Importantly, an l -Glu-γ- d -Glu dipeptide moiety replaces the glutamate moiety present in other antifolates. , Further intracellular polyglutamylation of TS antifolate inhibitors by folate polyglutamate synthase increases their affinity for TS. , The l -Glu-γ- d -Glu dipeptide moiety of 1 serves the same purpose as the polyglutamate tail, increasing affinity for TS through electrostatic interactions with the positively charged polyglutamate-binding groove on the enzyme.…”
Section: Resultsmentioning
confidence: 99%
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