W. T. Colwell scite author profile

Successive alkylation of dimethyl homoterephthalate with propargyl bromide and 2,4-diamino-6-(bromomethyl)pteridine followed by ester saponification at room temperature afforded 2,4-diamino-4-deoxy-10-carboxy-10-propargyl-10-deazapteroic acid. The 10-COOH was readily decarboxylated by heating in DMSO at a temperature of only 120 degrees C to yield the diamino-10-propargyl-10-deazapteroic acid intermediate. Coupling with diethyl L-glutamate and ester hydrolysis gave the title compound. The 10-propargyl analogue was about 5 times more potent than MTX as an inhibitor of growth in L1210 cells, but was only one-third as potent as an inhibitor of DHFR from L1210. The analogue was transported inward very effectively in L1210 cells showing a 10-fold advantage over MTX. At a dose of 36 mg/kg the 10-propargyl compound caused shrinkage of the E0771 solid murine mammary tumor to only 1% of untreated controls.

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Stabilized Analogs of Thymopentin. 1. 4,5-Ketomethylene Pseudopeptides

DeGraw

Almquist

Hiebert

et al. 1997

J. Med. Chem.

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The pentapeptide, thymopentin (Arg1-Lys2-Asp3-Val4-Tyr5) is known for its activity as an immunomodulating drug, but with limited half-life in plasma. In this first paper of a series of three studies, the synthesis of analogs stabilized at the peptide bond between the C-terminal amino acids via insertion of a ketomethylene moiety is described. N-Blocked pseudopeptides containing Val(k)Phe, Ala(k)Phe, and Val(k)Val units were prepared and attached to chloromethyl Merrifield resin via the carboxy terminal. Removal of the N-BOC group by trifluoroacetic acid was followed by sequential coupling with N-BOC dipeptides of aspartic acid to yield resin-bound N-BOC pseudotetrapeptides. Removal of N-BOC and coupling with N-BOC-r-N-tosylarginine followed by total cleavage of blocking groups and resin by HF afforded the target pseudopentapeptides. The analogs were found to compete favorably with thymopentin for binding to CEM cells, but binding was reduced by about 20-30% on average. All analogs showed significant enhancement of half-life versus thymopentin in mouse serum, but most showed only modest improvement in human serum. Insertion of proline or norleucine at position 2 in the chain caused a substantial increase in half-life (3-4-fold), while N-methylnorleucine conferred complete stability in the analogs.

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¹⁵N and ¹H NMR evidence for multiple conformations of the complex of dihydrofolate reductase with its substrate, folate

Birdsall¹,

Graw²,

Feeney³

et al. 1987

FEBS Letters

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The binding of folate to Lactobacillus casei dihydrofolate reductase in the presence and absence of NADP+ has been studied by 15N NMR, using [5-15N]folate. In the presence of NADP+, three separate signals were observed for the single 15N atom, in agreement with our earlier evidence from 1H and 13C NMR for multiple conformations of this complex [(1982) Biochemistry 21, 5831-5838]. The 15N spectra of the binary enzyme-folate complex provide evidence for the first time that this complex also exists in at least two conformational states. This is confirmed by the observation of two separate resonances for the 7-proton of bound folate, located by two-dimensional exchange spectroscopy.

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W. T. Colwell

A new analogue of 10-deazaaminopterin with markedly enhanced curative effects against human tumor xenografts in mice

Synthesis and antitumor activity of 10-propargyl-10-deazaaminopterin

Stabilized Analogs of Thymopentin. 1. 4,5-Ketomethylene Pseudopeptides

¹⁵N and ¹H NMR evidence for multiple conformations of the complex of dihydrofolate reductase with its substrate, folate

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W. T. Colwell

A new analogue of 10-deazaaminopterin with markedly enhanced curative effects against human tumor xenografts in mice

Synthesis and antitumor activity of 10-propargyl-10-deazaaminopterin

Stabilized Analogs of Thymopentin. 1. 4,5-Ketomethylene Pseudopeptides

15N and 1H NMR evidence for multiple conformations of the complex of dihydrofolate reductase with its substrate, folate

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¹⁵N and ¹H NMR evidence for multiple conformations of the complex of dihydrofolate reductase with its substrate, folate