Your search keyword '"G P, Beardsley"' showing total 65 results

1. Accumulation of Methotrexate Polyglutamates, Ploidy and Trisomies of Both Chromosomes 4 and 10 in Lymphoblasts from Children with B-Progenitor Cell Acute Lymphoblastic Leukemia: a Pediatric Oncology Group Study

Author

Barton A. Kamen, Bruce M. Camitta, A. Emami, P. A. Koch, D. J. Pullen, M J Vuchich, Jonathan J. Shuster, Linda D. Cooley, J. J. Akabutu, A. T. Look, Yaddanapudi Ravindranath, V M Whitehead, Stephen J. Lauer, C Payment, T Bowen, Donald H. Mahoney, and G. P. Beardsley

Subjects

Male, Cancer Research, Adolescent, medicine.medical_treatment, Cell, Trisomy, Biology, Folic Acid, Bone Marrow, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Peptide Synthases, Progenitor cell, Child, Cytotoxicity, Chemotherapy, Chromosomes, Human, Pair 10, Lymphoblast, Hematology, Aneuploidy, Prognosis, Molecular biology, Methotrexate, medicine.anatomical_structure, Polyglutamic Acid, Oncology, Child, Preschool, Neoplastic Stem Cells, Female, Hyperdiploidy, Chromosomes, Human, Pair 4, Ploidy, medicine.drug

Abstract

Levels of accumulation of methotrexate polyglutamates were measured in vitro in lymphoblasts obtained at diagnosis from children with B-progenitor cell acute lymphoblastic leukemia (pro-B ALL). They were compared to numerical and structural chromosomal abnormalities present in these leukemic cells. In a series of 95 patients, the percent with high lymphoblast methotrexate polyglutamate levels increased with the increase in modal number of total chromosomes (p0.001). Thus, lymphoblast methotrexate polyglutamate accumulation appeared to be closely linked to the extent of hyperdiploidy in childhood pro-B ALL. Lymphoblasts from 35 (88%) of the 40 children with hyperdiploid (50 chromosomes) and 23 (88%) of 26 with hyperdiploid (DNA Index1.16) pro-B ALL accumulated high levels of methotrexate polyglutamate, suggesting that they were more sensitive to methotrexate cytotoxicity. While children with hyperdiploid (DNA Index1.16) pro-B ALL have a good prognosis, those with trisomies of both chromosomes 4 and 10, almost all of whom are hyperdiploid, have an even better outcome. There was no significant difference in methotrexate polyglutamate levels in lymphoblasts from 19 children with and 21 without trisomies of both chromosomes 4 and 10 (p = 0.25). The improved response to multi-agent chemotherapy conferred by the presence of trisomies of both chromosomes 4 and 10 in such patients may be due to increased sensitivity of their lymphoblasts to one or more anti-leukemic agents in addition to methotrexate.

Published

1998

2. Chiral Chemical Synthesis of DNA Containing (S)-9-(1,3-Dihydroxy-2-propoxymethyl)guanine (DHPG) and Effects on Thermal Stability, Duplex Structure, and Thermodynamics of Duplex Formation

Author

S. Marshalko, Barry Schweitzer, and G P Beardsley

Subjects

chemistry.chemical_classification, Phosphoramidite, Circular dichroism, Binding Sites, Magnetic Resonance Spectroscopy, Molecular Structure, Guanine, Guanosine, Thermodynamics, Stereoisomerism, DNA, Biochemistry, DNA Adducts, chemistry.chemical_compound, Drug Stability, Deoxyribose, chemistry, Nucleic Acid Conformation, A-DNA, Nucleotide, Ganciclovir

Abstract

The antiviral compound 9-(1,3-dihydroxy-2-propoxymethyl)guanine (DHPG, Ganciclovir) is used clinically to treat cytomegaloviral infections in immunocompromised hosts and more recently is being investigated as a chemotherapeutic agent to be used in combination with retroviral gene therapy. Structurally, DHPG, an analog of guanosine, lacks the 2'-deoxyribose carbon atom and is acyclic. It is therefore prochiral at the 4'-deoxyribose carbon, having both pro-R and pro-S isomers. This stereochemistry is critical during biochemical conversions. DHPG retains the equivalent of 3'-hydroxyl and 5'-hydroxyl moieties. These can potentially support not only initial misincorporation of DHPG into DNA but also subsequent nucleotide addition. The mechanism of DHPG antiviral action may thus not strictly be through chain terminations. To investigate the structural and biochemical consequences of incorporation of DHPG into DNA, with particular attention to the relative contributions of the deoxyribose sugar to the overall structure and stability of DNA, we have developed a methodology for the chiral chemical synthesis of DNA oligomers containing DHPG. The stereochemistry of the DHPG phosphoramidite was established by a stereoselective acetyl transfer reaction catalyzed by porcine pancreatic lipase. The DNA resisted enzymatic digestion at DHPG sites. Circular dichroism and copper phenanthroline cleavage studies indicated that the incorporation of DHPG into DNA does not significantly perturb the global B-conformation structure. Detailed thermodynamic investigations into DNA containing DHPG revealed reduced thermal stability, as evidenced by a decrease in melting temperature, with significant alteration of the enthalpy, entropy, and free energy of duplex formation. These data demonstrate that an intact deoxyribose ring significantly contributes to the stability of a DNA duplex.

Published

1995

3. Solution Structure of a DNA Dodecamer Containing the Anti-Neoplastic Agent Arabinosylcytosine: Combined Use of NMR, Restrained Molecular Dynamics, and Full Relaxation Matrix Refinement

Author

Barry Schweitzer, Thomas Mikita, G W Kellogg, Kevin H. Gardner, and G P Beardsley

Subjects

carbohydrates (lipids), Crystallography, Dodecameric protein, Chemistry, Hydrogen bond, Stacking, Proton NMR, A-DNA, Nuclear magnetic resonance spectroscopy, Dihedral angle, Biochemistry, Two-dimensional nuclear magnetic resonance spectroscopy

Abstract

The effect of araC incorporation into the dodecamer duplex [d(CGCGAATT) (araC)d(GCG)]2 was examined by comparing its nuclear magnetic resonance (NMR)-determined solution structure with that of the control duplex d[(CGCGAATTCGCG)]2. 1H and 31P resonances in both duplexes were assigned using a combination of 2-D 1H NMR and a 3-D 31P-1H heteroTOCSY-NOESY experiment. Proton-proton distances (determined from NOESY data) and sugar dihedral angles (from NOESY and COSY data) were used in restrained molecular dynamics simulations starting from canonical A- or B-form DNA models. Both the control and araC sets of simulations converged to B-type structures. These structures were subjected to full relaxation matrix refinement to produce final structures which were in excellent agreement (R1/6 < 0.05) with the observed NOE intensities. A detailed comparison of the final control and araC structures revealed a global similarity (overall RMSD approximately 1.3 A), with significant differences localized at the araC site and neighboring bases. These included changes in sugar pucker, backbone torsion angles, base stacking, and other helical parameters. These findings are in general agreement with the previously published X-ray structure of a decamer duplex containing araC. One intriguing feature of the NMR solution structure not found in the crystal structure is the presence of an intramolecular hydrogen bond between the 2' hydroxyl on the araC sugar and the 3' phosphate group.

Published

1994

4. 5,10-Dideazatetrahydrofolic acid (DDATHF) transport in CCRF-CEM and MA104 cell lines

Author

A K Smith, Arlene R. Cashmore, Giuseppe Pizzorno, B. A. Moroson, M Marling-Cason, B A Kamen, G. P. Beardsley, and A.D. Cross

Subjects

Chemistry, media_common.quotation_subject, Diastereomer, Cell Biology, Biochemistry, Molecular biology, De novo synthesis, chemistry.chemical_compound, Cell culture, Folate receptor, Antifolate, medicine, Methotrexate, Binding site, Internalization, Molecular Biology, medicine.drug, media_common

Abstract

5,10-Dideazatetrahydrolic acid (DDATHF) is representative of a new class of antifolates acting through inhibition of de novo purine synthesis. We report here the transport characteristics of the diastereomers of DDATHF, which differ in configuration at C6, and comparison studies with other folate and antifolate analogs. (6R)-DDATHF showed high affinity for the influx system of CCRF-CEM cells with a Km of 1.07 microM and an influx Vmax of 4.04 pmol/min/10(7) cells. Comparative studies with methotrexate yielded an influx Km of 4.98 microM and a Vmax of 6.64 pmol/min/10(7) cells, and with 5-formyltetrahydrofolate an influx Km of 2.18 microM and a Vmax of 6.84 pmol/min/10(7) cells. Uptake of (6R)-DDATHF was competitively inhibited by (6S)-DDATHF, methotrexate (MTX), and 5-formyltetrahydrofolate, all with Ki values similar to their influx Km. The (6S)-DDATHF diastereomer had an influx Km of 1.04 microM, similar to that of (6R)-DDATHF; however, the Vmax of 1.72 pmol/min/10(7) cells was 2.3-fold lower than for (6R)-DDATHF. The transport properties of DDATHF were also studied in a mutant cell line (CEM/MTX), resistant to MTX based on impaired drug transport. In this system (6R)-DDATHF showed an influx Km of 1.49 microM and a decreased influx Vmax of 0.60 pmol/min/10(7) cells. A similar effect was shown for MTX (Km of 7.48 microM, Vmax of 1.02 pmol/min/10(7) cells). The number of binding sites in CCRF-CEM cells was similar for (6R)-DDATHF, (6S)-DDATHF, and MTX, 0.74, 0.71, and 0.76 pmol/10(7) cells, respectively. These values were slightly higher in the CEM/MTX cell line (1.07 and 1.09 pmol/10(7) cells for (6R)-DDATHF and MTX, respectively). Treatment of CCRF-CEM cells with either the N-hydroxysuccinimide ester of MTX or the corresponding N-hydroxysuccinimide ester of (6R)-DDATHF caused substantial inhibition (> 90%) of the influx of (6R)-[3H]DDATHF and [3H]MTX, respectively. These results suggest strongly that DDATHF and MTX share a common influx mechanism through the reduced folate transport system. The internalization of DDATHF by monkey kidney epithelial MA104 cells, which express a high affinity folate receptor, was also studied. Competitive binding studies using purified folate receptor and radiolabeled 5-methyltetrahydrofolate showed that (6S)- and (6R)-DDATHF both had I50 values lower than 5-methyltetrahydrofolate (12 nM). Further studies indicate that both DDATHF isomers are actively intracellularly concentrated through this route and are also rapidly converted to high chain length polyglutamates. Transport via this system was inhibited in folate-depleted cells by 10 nM folic acid.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1993

5. ChemInform Abstract: Synthesis of Oligonucleotides Containing 5-(Hydroxymethyl)-2′- deoxyuridine at Defined Sites

Author

G. P. Beardsley and Lawrence C. Sowers

Subjects

chemistry.chemical_compound, chemistry, Oligonucleotide, Stereochemistry, Nucleic acid, Hydroxymethyl, General Medicine, Combinatorial chemistry, Deoxyuridine

Published

2010

6. Catalytic reduction in the synthesis of tritiated (6R) and (6S) 5, 10-dideaza-5,6,7,8-tetrahydrofolate

Author

Ann D. Cross, Philip G. Williams, G. P. Beardsley, and Hiromi Morimoto

Subjects

Tritium illumination, Chemistry, Organic Chemistry, Two step, Diastereomer, Selective catalytic reduction, Biochemistry, Analytical Chemistry, Catalysis, Solvent, Drug Discovery, Proton NMR, Radiology, Nuclear Medicine and imaging, Tritium, Spectroscopy, Nuclear chemistry

Abstract

[3H] 5,10-dideaza-5,6,7,8-tetrahydrofolate, DDATHF, was obtained by a two step process. First, 2n[3H2O] was produced in the reaction flask containing m[1HAc] by the reduction of n[PtO2] with 3H2, so that a 1[3H+]:18[3H+ + 1H+] ratio of solvent protic species in theory resulted. Secondly, subsequently added diethyl-2-acetyl-5,10-dideaza-9,10-didehydrofolate was reduced in this tritium labeled solvent with the pre-reduced Adams catalyst and additional carrier free tritium gas which was introduced to a pressure of 722 torr. The resulting (6R) and (6S) [3H] diastereomers were individually isolated. Each had a specific activity of 11.2 Ci/mmol, and the locations of the incorporated tritium atoms were completely determined by 1H decoupled 320 MHz 3H NMR by comparison with the 300 and 500 MHz 1H NMR spectra of [1H] (6S) DDATHF, [1H] (6R) DDATHF, and [5-2H (50% 2H), 6-2H (100% 2H), 7-2H (50% 2H), 9-2H (50% 2H), 10-2H (50% 2H)] (6RS) DDATHF.

Published

1991

7. Crystal structures of human GAR Tfase at low and high pH and with substrate beta-GAR

Author

S.E. Greasley, D L Boger, G P Beardsley, Yan Zhang, Joel Desharnais, and Ian A. Wilson

Subjects

Hydroxymethyl and Formyl Transferases, Ribonucleotide, Stereochemistry, Glycine, Crystal structure, Crystallography, X-Ray, Biochemistry, Substrate Specificity, Folic Acid, Bacterial Proteins, Multienzyme Complexes, Escherichia coli, Transferase, Humans, Carbon-Nitrogen Ligases, Beta (finance), Conformational isomerism, Phosphoribosylglycinamide Formyltransferase, chemistry.chemical_classification, Binding Sites, biology, Chemistry, Substrate (chemistry), Hydrogen-Ion Concentration, Ribonucleotides, Enzyme assay, Peptide Fragments, Enzyme Activation, Crystallography, Kinetics, Enzyme, biology.protein, Dimerization

Abstract

Glycinamide ribonucleotide transformylase (GAR Tfase) is a key folate-dependent enzyme in the de novo purine biosynthesis pathway and, as such, has been the target for antitumor drug design. Here, we describe the crystal structures of the human GAR Tfase (purN) component of the human trifunctional protein (purD-purM-purN) at various pH values and in complex with its substrate. Human GAR Tfase exhibits pH-dependent enzyme activity with its maximum around pH 7.5-8. Comparison of unliganded human GAR Tfase structures at pH 4.2 and pH 8.5 reveals conformational differences in the substrate binding loop, which at pH 4.2 occupies the binding cleft and prohibits substrate binding, while at pH 8.5 is permissive for substrate binding. The crystal structure of GAR Tfase with its natural substrate, beta-glycinamide ribonucleotide (beta-GAR), at pH 8.5 confirms this conformational isomerism. Surprisingly, several important structural differences are found between human GAR Tfase and previously reported E. coli GAR Tfase structures, which have been used as the primary template for drug design studies. While the E. coli structure gave valuable insights into the active site and formyl transfer mechanism, differences in structure and inhibition between the bacterial and mammalian enzymes suggest that the human GAR Tfase structure is now the appropriate template for the design of anti-cancer agents.

Published

2002

8. Crystal structure of a bifunctional transformylase and cyclohydrolase enzyme in purine biosynthesis

Author

S E, Greasley, P, Horton, J, Ramcharan, G P, Beardsley, S J, Benkovic, and I A, Wilson

Subjects

Birds, Hydroxymethyl and Formyl Transferases, Models, Molecular, Structure-Activity Relationship, Binding Sites, Multienzyme Complexes, Nucleotide Deaminases, Purines, Recombinant Fusion Proteins, Animals, Crystallography, X-Ray, Dimerization, Protein Structure, Tertiary

Abstract

ATIC, the product of the purH gene, is a 64 kDa bifunctional enzyme that possesses the final two activities in de novo purine biosynthesis, AICAR transformylase and IMP cyclohydrolase. The crystal structure of avian ATIC has been determined to 1.75 A resolution by the MAD method using a Se-methionine modified enzyme. ATIC forms an intertwined dimer with an extensive interface of approximately 5,000 A(2) per monomer. Each monomer is composed of two novel, separate functional domains. The N-terminal domain (up to residue 199) is responsible for the IMPCH activity, whereas the AICAR Tfase activity resides in the C-terminal domain (200-593). The active sites of the IMPCH and AICAR Tfase domains are approximately 50 A apart, with no structural evidence of a tunnel connecting the two active sites. The crystal structure of ATIC provides a framework to probe both catalytic mechanisms and to design specific inhibitors for use in cancer chemotherapy and inflammation.

Published

2001

9. Human 5-aminoimidazole-4-carboxamide ribonucleotide transformylase/inosine 5'-monophosphate cyclohydrolase. A bifunctional protein requiring dimerization for transformylase activity but not for cyclohydrolase activity

Author

J M, Vergis, K G, Bulock, K G, Fleming, and G P, Beardsley

Subjects

Hydroxymethyl and Formyl Transferases, Kinetics, Multienzyme Complexes, Nucleotide Deaminases, Humans, Dimerization

Abstract

The bifunctional enzyme aminoimidazole carboxamide ribonucleotide transformylase/inosine monophosphate cyclohydrolase (ATIC) is responsible for catalysis of the last two steps in the de novo purine pathway. Gel filtration studies performed on human enzyme suggested that this enzyme is monomeric in solution. However, cross-linking studies performed on both yeast and avian ATIC indicated that this enzyme might be dimeric. To determine the oligomeric state of this protein in solution, we carried out sedimentation equilibrium analysis of ATIC over a broad concentration range. We find that ATIC participates in a monomer/dimer equilibrium with a dissociation constant of 240 +/- 50 nM at 4 degrees C. To determine whether the presence of substrates affects the monomer/dimer equilibrium, further ultracentrifugation studies were performed. These showed that the equilibrium is only significantly shifted in the presence of both AICAR and a folate analog, resulting in a 10-fold reduction in the dissociation constant. The enzyme concentration dependence on each of the catalytic activities was studied in steady state kinetic experiments. These indicated that the transformylase activity requires dimerization whereas the cyclohydrolase activity only slightly prefers the dimeric form over the monomeric form.

Published

2000

10. Structure and functional relationships in human pur H

Author

G P, Beardsley, E A, Rayl, K, Gunn, B A, Moroson, H, Seow, K S, Anderson, J, Vergis, K, Fleming, S, Worland, B, Condon, and J, Davies

Subjects

Hydroxymethyl and Formyl Transferases, Models, Molecular, Binding Sites, Protein Conformation, Chromosome Mapping, Ribonucleotides, Aminoimidazole Carboxamide, Recombinant Proteins, Kinetics, Multienzyme Complexes, Nucleotide Deaminases, Chromosomes, Human, Pair 2, Humans, Cloning, Molecular, Purine Nucleotides

Abstract

1. The human pur H (ATIC) gene encoding a bifunctional protein, hPurH, which carries the penultimate and final enzymatic activities of the purine nucleotide synthesis pathway, AICARFTIMPCH, has been cloned and sequenced. The gene product, hPurH has been overexpressed in E. coli, purified to homogeneity and crystallized. 2. The human pur H gene lies on chromosome 2, between band q34 and q35. There is at least one intron of 278 bp near the 5' end. 3. Truncation mutant studies demonstrate two non-overlapping functional domains in the protein arranged as indicated in Figure 5. The existence of a linker or interaction region between the catalytic domains remains to be established. 4. Cleland-type kinetic inhibition experiments indicate that the AICARFT reaction is of the ordered, sequential type with the reduced folate cofactor binding first. 5. The reaction has a broad pH optimum in the alkaline range, with a maximum at about pH 8.2. 6. Preliminary transient phase kinetic studies show the presence of a "burst" indicating that a late step in the reaction sequence is rate limiting. 7. A PurH crystal structure is that of a dimer, with a putative single binding site for the reduced folate cofactor formed using elements from each of the monomer subunits. Probable binding sites for AICAR and FAICAR can be identified on each monomer. 8. Equilibrium sedimentation studies show hPurH apoprotein to be a monomer:dimer equilibrium mixture with a kD of 0.55 uM. 9. The crystal structure has permitted identification of a number of candidate amino acid residues likely to be involved in catalysis and/or substrate binding. Among these, we have thus far completed studies on two, Lysine 265 and Histidine 266. These appear to be critically involved in the AICARFT reaction, although whether their role(s) are in catalysis or binding remains to be determined.

Published

1998

11. Solution structure of a DNA decamer containing the antiviral drug ganciclovir: combined use of NMR, restrained molecular dynamics, and full relaxation matrix refinement

Author

Barry Schweitzer, Santosh Kumar, S. Marshalko, G P Beardsley, M. Foti, and E. Schurter

Subjects

Ganciclovir, Models, Molecular, Magnetic Resonance Spectroscopy, Guanine, Stereochemistry, Molecular Sequence Data, Dihedral angle, Crystallography, X-Ray, Biochemistry, Antiviral Agents, chemistry.chemical_compound, Molecular dynamics, medicine, A-DNA, Glycosides, Base Composition, Molecular Structure, Chemistry, Hydrogen Bonding, DNA, Organophosphates, Solutions, Crystallography, Duplex (building), Nucleic Acid Conformation, Thermodynamics, Two-dimensional nuclear magnetic resonance spectroscopy, medicine.drug

Abstract

The nucleoside analog 9-[(1,3-dihydroxy-2-propoxy)methyl]guanine (ganciclovir, DHPG) is an antiviral drug that is used in the treatment of a variety of herpes viruses in immunocompromised patients and in a gene therapy protocol that has shown promising activity for the treatment of cancer. To probe the structural effects of ganciclovir when incorporated into DNA, we determined and compared the solution structure of a modified ganciclovir-containing decamer duplex [d(CTG)(ganciclovir)d(ATCCAG)]2 and a control duplex d[(CTGGATCCAG)]2 using nuclear magnetic resonance techniques. 1H and 31P resonances in both duplexes were assigned using a combination of 2-D 1H and 31P NMR experiments. Proton-proton distances determined from NOESY data and dihedral angles determined from DQF-COSY data were used in restrained molecular dynamics simulations starting from canonical A- and B-form DNA models. Both the control and ganciclovir sets of simulations converged to B-type structures. These structures were subjected to full relaxation matrix refinement to produce final structures that were in excellent agreement with the observed NOE intensities. Examination of the final ganciclovir-containing structures reveals that the base of the ganciclovir residue is hydrogen bonded to its complementary dC and is stacked in the helix; in fact, the base of ganciclovir exhibits increased stacking with the 5' base relative to the control. Interestingly, some of the most significant distortions in the structures occur 3' to the lesion site, including a noticeable kink in the sugar-phosphate backbone at this position. Further examination reveals that the backbone conformation, sugar pucker, and glycosidic torsion angle of the residue 3' to the lesion site all indicate an A-type conformation at this position. A possible correlation of these structural findings with results obtained from earlier biochemical studies will be discussed.

Published

1997

12. LY231514, a pyrrolo[2,3-d]pyrimidine-based antifolate that inhibits multiple folate-requiring enzymes

Author

C, Shih, V J, Chen, L S, Gossett, S B, Gates, W C, MacKellar, L L, Habeck, K A, Shackelford, L G, Mendelsohn, D J, Soose, V F, Patel, S L, Andis, J R, Bewley, E A, Rayl, B A, Moroson, G P, Beardsley, W, Kohler, M, Ratnam, and R M, Schultz

Subjects

Hydroxymethyl and Formyl Transferases, Antimetabolites, Antineoplastic, 5,10-Methylenetetrahydrofolate Reductase (FADH2), Guanine, Pemetrexed, Thiophenes, Phosphoribosylaminoimidazolecarboxamide Formyltransferase, Formate-Tetrahydrofolate Ligase, Glutamates, Aminohydrolases, Multienzyme Complexes, Tumor Cells, Cultured, Humans, Methylenetetrahydrofolate Reductase (NADPH2), Tetrahydrofolates, Phosphoribosylglycinamide Formyltransferase, Methylenetetrahydrofolate Dehydrogenase (NADP), Molecular Structure, Thymidylate Synthase, Tetrahydrofolate Dehydrogenase, Methotrexate, Polyglutamic Acid, Quinazolines, Folic Acid Antagonists, Oxidoreductases, Acyltransferases

Abstract

N-[4-[2-(2-amino-3,4-dihydro-4-oxo-7H-pyrrolo[2,3-d]pyrimidin-5-yl)ethyl ]-benzoyl]-L-glutamic acid (LY231514) is a novel pyrrolo[2,3-d]pyrimidine-based antifolate currently undergoing extensive Phase II clinical trials. Previous studies have established that LY231514 and its synthetic gamma-polyglutamates (glu3 and glu5) exert potent inhibition against thymidylate synthase (TS). We now report that LY231514 and its polyglutamates also markedly inhibit other key folate-requiring enzymes, including dihydrofolate reductase (DHFR) and glycinamide ribonucleotide formyltransferase (GARFT). For example, the Ki values of the pentaglutamate of LY231514 are 1.3, 7.2, and 65 nM for inhibition against TS, DHFR, and GARFT, respectively. In contrast, although a similar high level of inhibitory potency was observed for the parent monoglutamate against DHFR (7.0 nM), the inhibition constants (Ki) for the parent monoglutamate are significantly weaker for TS (109 nM) and GARFT (9,300 nM). The effects of LY231514 and its polyglutamates on aminoimidazole carboxamide ribonucleotide formyltransferase, 5,10-methylenetetrahydrofolate dehydrogenase, and 10-formyltetrahydrofolate synthetase were also evaluated. The end product reversal studies conducted in human cell lines further support the concept that multiple enzyme-inhibitory mechanisms are involved in cytotoxicity. The reversal pattern of LY231514 suggests that although TS may be a major site of action for LY231514 at concentrations near the IC50, higher concentrations can lead to inhibition of DHFR and/or other enzymes along the purine de novo pathway. Studies with mutant cell lines demonstrated that LY231514 requires polyglutamation and transport via the reduced folate carrier for cytotoxic potency. Therefore, our data suggest that LY231514 is a novel classical antifolate, the antitumor activity of which may result from simultaneous and multiple inhibition of several key folate-requiring enzymes via its polyglutamated metabolites.

Published

1997

13. The human purH gene product, 5-aminoimidazole-4-carboxamide ribonucleotide formyltransferase/IMP cyclohydrolase. Cloning, sequencing, expression, purification, kinetic analysis, and domain mapping

Author

E A, Rayl, B A, Moroson, and G P, Beardsley

Subjects

Hydroxymethyl and Formyl Transferases, Binding Sites, DNA, Complementary, Base Sequence, Sequence Homology, Amino Acid, Molecular Sequence Data, Gene Expression, Phosphoribosylaminoimidazolecarboxamide Formyltransferase, Kinetics, Structure-Activity Relationship, Nucleotide Deaminases, Consensus Sequence, Mutagenesis, Site-Directed, Animals, Humans, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Sequence Alignment, Acyltransferases, DNA Primers, Formyltetrahydrofolates

Abstract

We report here the cloning and sequencing of the cDNA, purification, steady state kinetic analysis, and truncation mapping studies of the human 5-aminoimidazole- 4-carboxamide ribonucleotide formyltransferase/IMP cyclohydrolase (AICARFT/IMPCHase). These steps of de novo purine biosynthesis, respectively. In all species of both prokaryotes and eukaryotes studied, these two activities are present on a single bifunctional polypeptide encoded on the purH gene. The human purH cDNA is 1776 base pairs in length encoding for a 591-amino acid polypeptic (Mr = 64,425). The human and avian purH cDNAs are 75 and 81% similar on the nucleotide and amino acid sequence level, respectively. The Km values for AICAR and (6R,6S)10-formyltetrahydrofolate are 16.8 microM +/- 1.5 and 60.2 microM +/- 5.0, respectively, for the cloned, purified human enzyme. A 10-amino acid sequence within the COOH-terminal portion of human AICARFT/IMPCHase has some degree of homology to a previously noted "folate binding site." Site directed mutagenesis studies indicate that this sequence plays no role in enzymatic activity. We have constructed truncation mutants which demonstrate that each of the two enzyme activities can be expressed independent of the other. IMPCHase and AICARFT activities are located within the NH2-terminal 223 and COOH-terminal 406 amino acids, respectively. The truncation mutant possessing AICARFT activity displays steady state kinetic parameters identical to those of the holoenzyme.

Published

1996

14. Multifactorial resistance to 5,10-dideazatetrahydrofolic acid in cell lines derived from human lymphoblastic leukemia CCRF-CEM

Author

G, Pizzorno, B A, Moroson, A R, Cashmore, O, Russello, J R, Mayer, J, Galivan, M A, Bunni, D G, Priest, and G P, Beardsley

Subjects

Glycine Hydroxymethyltransferase, Hydroxymethyl and Formyl Transferases, Methylenetetrahydrofolate Dehydrogenase (NADP), 5,10-Methylenetetrahydrofolate Reductase (FADH2), Drug Resistance, Antineoplastic Agents, Stereoisomerism, Thymidylate Synthase, gamma-Glutamyl Hydrolase, Phosphoribosylaminoimidazolecarboxamide Formyltransferase, Clone Cells, Leukemia, Lymphoid, Formate-Tetrahydrofolate Ligase, Tetrahydrofolate Dehydrogenase, Tumor Cells, Cultured, Folic Acid Antagonists, Humans, Peptide Synthases, Oxidoreductases, Acyltransferases, Methylenetetrahydrofolate Reductase (NADPH2), Tetrahydrofolates, Phosphoribosylglycinamide Formyltransferase

Abstract

5,10-dideaza-5,6,7,8-terrahydrofolic acid (DDATHF) is a potent antiproliferative agent in cell culture systems and in vivo in a number of murine and human xenograft tumors. In contrast to classical antifolates, which are dihydrofolate reductase inhibitors, DDATHF primarily inhibits GAR transformylase, the first folate-dependent enzyme along the pathway of de novo purine biosynthesis. The (6R) diastereomer of DDATHF (Lometrexol), currently undergoing clinical investigation, was used to develop CCRF-CEM human leukemia sublines resistant to increasing concentrations of the drug. Three cell lines were selected for ability to grow in medium containing 0.1 microM, 1.0 microM, and 10 microM of (6R)DDATHF, respectively. Impaired polyglutamylation was identified as a common mechanism of resistance in all three cell lines. A progressive decrease in the level of polyglutamylation was associated with diminished folylpolyglutamate synthetase activity and paralleled increasing levels of resistance to the drug. However, the expression of folylpolyglutamate synthetase RNA was not altered in the resistant cell lines compared to the parent cells. The most resistant cell subline also displayed an increased activity of gamma-glutamyl hydrolase. The sublines were scrutinized for other possible mechanisms of resistance. No alterations in drug transport or in purine economy were found. Modest increases were found in the activity of methylene tetrahydrofolate dehydrogenase but no alterations of other folate-dependent enzymes were observed. Increases in accumulation and conversion of folic acid to reduced forms, particularly 10-formyltetrahydrofolate, was also seen. The resistant cell lines were sensitive to dihydrofolate reductase inhibitors, methotrexate and trimetrexate, for a 72-h exposure period but showed cross-resistance to methotrexate for 4 and 24 h exposures. Cross-resistance was also shown toward other deazafolate analogues for both short- and long-term exposures.

Published

1995

15. Solution structure of a DNA dodecamer containing the anti-neoplastic agent arabinosylcytosine: combined use of NMR, restrained molecular dynamics, and full relaxation matrix refinement

Author

B I, Schweitzer, T, Mikita, G W, Kellogg, K H, Gardner, and G P, Beardsley

Subjects

Models, Molecular, Base Composition, Magnetic Resonance Spectroscopy, Base Sequence, Oligodeoxyribonucleotides, Molecular Sequence Data, Cytarabine, Nucleic Acid Conformation, Computer Simulation, DNA

Abstract

The effect of araC incorporation into the dodecamer duplex [d(CGCGAATT) (araC)d(GCG)]2 was examined by comparing its nuclear magnetic resonance (NMR)-determined solution structure with that of the control duplex d[(CGCGAATTCGCG)]2. 1H and 31P resonances in both duplexes were assigned using a combination of 2-D 1H NMR and a 3-D 31P-1H heteroTOCSY-NOESY experiment. Proton-proton distances (determined from NOESY data) and sugar dihedral angles (from NOESY and COSY data) were used in restrained molecular dynamics simulations starting from canonical A- or B-form DNA models. Both the control and araC sets of simulations converged to B-type structures. These structures were subjected to full relaxation matrix refinement to produce final structures which were in excellent agreement (R1/60.05) with the observed NOE intensities. A detailed comparison of the final control and araC structures revealed a global similarity (overall RMSD approximately 1.3 A), with significant differences localized at the araC site and neighboring bases. These included changes in sugar pucker, backbone torsion angles, base stacking, and other helical parameters. These findings are in general agreement with the previously published X-ray structure of a decamer duplex containing araC. One intriguing feature of the NMR solution structure not found in the crystal structure is the presence of an intramolecular hydrogen bond between the 2' hydroxyl on the araC sugar and the 3' phosphate group.

Published

1994

16. 5,10-Dideazatetrahydrofolic acid (DDATHF) transport in CCRF-CEM and MA104 cell lines

Author

G, Pizzorno, A R, Cashmore, B A, Moroson, A D, Cross, A K, Smith, M, Marling-Cason, B A, Kamen, and G P, Beardsley

Subjects

Folate Receptors, GPI-Anchored, Drug Resistance, Biological Transport, Receptors, Cell Surface, Stereoisomerism, Tritium, Leukemia, Lymphoid, Substrate Specificity, Kinetics, Methotrexate, Tumor Cells, Cultured, Folic Acid Antagonists, Humans, Carrier Proteins, Tetrahydrofolates

Abstract

5,10-Dideazatetrahydrolic acid (DDATHF) is representative of a new class of antifolates acting through inhibition of de novo purine synthesis. We report here the transport characteristics of the diastereomers of DDATHF, which differ in configuration at C6, and comparison studies with other folate and antifolate analogs. (6R)-DDATHF showed high affinity for the influx system of CCRF-CEM cells with a Km of 1.07 microM and an influx Vmax of 4.04 pmol/min/10(7) cells. Comparative studies with methotrexate yielded an influx Km of 4.98 microM and a Vmax of 6.64 pmol/min/10(7) cells, and with 5-formyltetrahydrofolate an influx Km of 2.18 microM and a Vmax of 6.84 pmol/min/10(7) cells. Uptake of (6R)-DDATHF was competitively inhibited by (6S)-DDATHF, methotrexate (MTX), and 5-formyltetrahydrofolate, all with Ki values similar to their influx Km. The (6S)-DDATHF diastereomer had an influx Km of 1.04 microM, similar to that of (6R)-DDATHF; however, the Vmax of 1.72 pmol/min/10(7) cells was 2.3-fold lower than for (6R)-DDATHF. The transport properties of DDATHF were also studied in a mutant cell line (CEM/MTX), resistant to MTX based on impaired drug transport. In this system (6R)-DDATHF showed an influx Km of 1.49 microM and a decreased influx Vmax of 0.60 pmol/min/10(7) cells. A similar effect was shown for MTX (Km of 7.48 microM, Vmax of 1.02 pmol/min/10(7) cells). The number of binding sites in CCRF-CEM cells was similar for (6R)-DDATHF, (6S)-DDATHF, and MTX, 0.74, 0.71, and 0.76 pmol/10(7) cells, respectively. These values were slightly higher in the CEM/MTX cell line (1.07 and 1.09 pmol/10(7) cells for (6R)-DDATHF and MTX, respectively). Treatment of CCRF-CEM cells with either the N-hydroxysuccinimide ester of MTX or the corresponding N-hydroxysuccinimide ester of (6R)-DDATHF caused substantial inhibition (90%) of the influx of (6R)-[3H]DDATHF and [3H]MTX, respectively. These results suggest strongly that DDATHF and MTX share a common influx mechanism through the reduced folate transport system. The internalization of DDATHF by monkey kidney epithelial MA104 cells, which express a high affinity folate receptor, was also studied. Competitive binding studies using purified folate receptor and radiolabeled 5-methyltetrahydrofolate showed that (6S)- and (6R)-DDATHF both had I50 values lower than 5-methyltetrahydrofolate (12 nM). Further studies indicate that both DDATHF isomers are actively intracellularly concentrated through this route and are also rapidly converted to high chain length polyglutamates. Transport via this system was inhibited in folate-depleted cells by 10 nM folic acid.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1993

17. Altered transport of folic acid and antifolates through the carrier mediated reduced folate transport system in a human leukemia cell line resistant to (6R) 5,10-dideazatetrahydrofolic acid (DDATHF)

Author

M, Pavlovic, J J, Leffert, O, Russello, M A, Bunni, G P, Beardsley, D G, Priest, and G, Pizzorno

Subjects

Binding Sites, Folate Receptors, GPI-Anchored, Drug Resistance, Biological Transport, Receptors, Cell Surface, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Cell Line, Kinetics, Folic Acid, Methotrexate, Tumor Cells, Cultured, Folic Acid Antagonists, Humans, Peptide Synthases, Carrier Proteins, Tetrahydrofolates

Published

1993

18. Evidence for a relationship between intracellular GTP levels and the induction of HL-60 leukemia cell differentiation by 5,10-dideazatetrahydrofolic acid (DDATHF)

Author

J A, Sokoloski, G, Pizzorno, G P, Beardsley, and A C, Sartorelli

Subjects

Intracellular Fluid, Leukemia, Promyelocytic, Acute, Tumor Cells, Cultured, Humans, Antineoplastic Agents, Cell Differentiation, Guanosine Triphosphate, Purine Nucleotides, Cell Division, Tetrahydrofolates

Abstract

5,10-Dideazatetrahydrofolic acid (DDATHF) is an inhibitor of glycinamide ribonucleotide transformylase, the first of two tetrahydrofolate requiring enzymes in the de novo purine nucleotide biosynthetic pathway, and is a potent inducer of the maturation of HL-60 promyelocytic leukemia cells. The inhibition of cellular growth by DDATHF was effectively prevented by adenosine or deoxyadenosine, whereas guanosine or deoxyguanosine only partially prevented the growth inhibition produced by this folate antimetabolite, implying that the depletion of both ATP and GTP, which occurs with this agent, was responsible for its growth inhibitory effects. In contrast, the induction of differentiation by DDATHF was completely abolished by the presence of guanosine or deoxyguanosine, suggesting that the depletion of intracellular guanine nucleotides by DDATHF represents the event that is essential to the induction of differentiation by this folate analog. This possibility was supported by the observation that the concentration of dGTP was not decreased in cells treated with DDATHF under the conditions employed. Both guanine nucleosides selectively restored intracellular GTP pools depleted by the treatment with DDATHF to their normal level, whereas only adenine nucleosides completely restored the levels of both ATP and GTP to their normal intracellular concentrations. The relationship between guanine nucleotide pools and the induction of HL-60 differentiation by DDATHF was further supported by the finding that maturation and the depletion of intracellular GTP by DDATHF were not reversed by guanine nucleosides in HL-60 cells deficient in hypoxanthine-guanine phosphoribosyltransferase activity. The findings provide support for the hypothesis that the terminal differentiation of these leukemic cells by DDATHF is the result of the depletion of intracellular GTP pools.

Published

1993

19. (6R)-5,10-Dideaza-5,6,7,8-tetrahydrofolic acid effects on nucleotide metabolism in CCRF-CEM human T-lymphoblast leukemia cells

Author

G, Pizzorno, B A, Moroson, A R, Cashmore, and G P, Beardsley

Subjects

Hypoxanthine, Time Factors, Cytidine Triphosphate, Uridine Triphosphate, DNA, Thymidylate Synthase, Aminoimidazole Carboxamide, Adenosine Triphosphate, Hypoxanthines, Tumor Cells, Cultured, Folic Acid Antagonists, Humans, Leukemia-Lymphoma, Adult T-Cell, RNA, Guanosine Triphosphate, Tetrahydrofolates

Abstract

(6R)-5,10-Dideaza-5,6,7,8-tetrahydrofolic acid [(6R)DDATHF] is a folate antimetabolite with activity specifically directed against de novo purine synthesis, primarily through inhibition of glycinamide ribonucleotide transformylase. This inhibition resulted in major changes in the size of the nucleotide pools in CCRF-CEM cells. After a 4-h incubation with 1 microM (6R)DDATHF, dramatic reductions in the ATP and GTP pools were observed, with almost no effect on CTP, UTP, and deoxyribonucleotide pools. When the incubation was continued in drug-free medium, recovery of ATP and GTP pools was protracted. ATP did not return to normal until 24-36 h, and GTP pools were only partially repleted by 48 h. The ATP and GTP pools were not affected when the initial 4-h incubation with (6R)DDATHF was conducted in the presence of 100 microM hypoxanthine. Addition of hypoxanthine to the medium after a 4-h incubation with (6R)DDATHF caused rapid recovery of the ATP and GTP pools. Similar effects were seen when the purine precursor aminoimidazole carboxamide was used in place of hypoxanthine. The effect of (6R)DDATHF on nucleotide pools and the capability of hypoxanthine or aminoimidazole carboxamide to prevent or reverse this phenomenon correlated directly with the inhibition of cell growth. Presumably as a consequence of the decrease in purine nucleotide triphosphate levels, the conversion of exogenously added uridine, thymidine, and deoxyuridine to nucleotides was markedly decreased. These effects were protracted for almost 48 h and were also reversed by hypoxanthine. Differential repletion of ATP and GTP pools after (6R)DDATHF pre-treatment demonstrated that diminished precursor phosphorylation is primarily a consequence of GTP rather than ATP starvation.

Published

1991

20. Intracellular metabolism of 5,10-dideazatetrahydrofolic acid in human leukemia cell lines

Author

G, Pizzorno, J A, Sokoloski, A R, Cashmore, B A, Moroson, A D, Cross, and G P, Beardsley

Subjects

Polyglutamic Acid, Tumor Cells, Cultured, Humans, gamma-Glutamyl Hydrolase, Cell Division, Tetrahydrofolates, Leukemia, Lymphoid

Abstract

5,10-Dideazatetrahydrofolic acid (DDATHF) is a new potent antitumor agent that specifically inhibits purine biosynthesis, primarily through inhibition of glycinamide ribonucleotide transformylase, the first of the tetrahydrofolate-requiring enzymes in the de novo synthesis pathway. DDATHF has been shown to be an excellent substrate for mouse liver folylpolyglutamate synthetase in vitro, suggesting that intracellular conversion to polyglutamates could play an important role in the action of this antifolate. In this report, metabolic studies of the 6R-diastereomer of DDATHF in the cultured human leukemia cell lines CCRF-CEM and HL-60 are presented. At both 1 and 10 microM (6R)-DDATHF was rapidly converted to polyglutamates in both cell lines. DDATHF(Glu)5 and DDATHF(Glu)6 were the main intracellular metabolites. After incubation in drug-free medium, (6R)-DDATHF polyglutamates were better retained intracellularly with increasing glutamate chain length. (6R)-DDATHF showed reduced cytotoxicity toward a folylpolyglutamate synthetase-deficient cell line, CCRF-CEM30/6 related to a dramatically diminished accumulation of polyglutamates. The activity of (6R)-DDATHF in CCRF-CEM30/6 cells was decreased after both short and prolonged exposures. These results suggest that polyglutamylation of (6R)-DDATHF not only represents a mechanism for trapping the drug inside the cells but also produces a more potent inhibitor of the target enzyme.

Published

1991

21. Induction of HL-60 leukemia cell differentiation by tetrahydrofolate inhibitors of de novo purine nucleotide biosynthesis

Author

G P Beardsley, Alan C. Sartorelli, and John A. Sokoloski

Subjects

Purine, Phosphoribosylglycinamide formyltransferase, Hydroxymethyl and Formyl Transferases, Cancer Research, Cellular differentiation, Fluorescent Antibody Technique, Macrophage-1 Antigen, Antineoplastic Agents, Biology, Toxicology, chemistry.chemical_compound, Biosynthesis, Leukemia, Promyelocytic, Acute, Tumor Cells, Cultured, Humans, Pharmacology (medical), Nucleotide, Purine Nucleotides, Hypoxanthine, Tetrahydrofolates, Phosphoribosylglycinamide Formyltransferase, Pharmacology, chemistry.chemical_classification, Cell growth, Nitroblue Tetrazolium, Cell Differentiation, Stereoisomerism, Enzyme, Oncology, chemistry, Biochemistry, Hypoxanthines, Folic Acid Antagonists, Acyltransferases, Cell Division

Abstract

5,10-Dideazatetrahydrofolic acid (DDATHF) is a folate antimetabolite that shows activity against glycinamide ribonucleotide (GAR) transformylase, a folate-requiring enzyme in the de novo purine nucleotide biosynthetic pathway. Previous studies from our laboratory have shown that DDATHF is an effective inducer of the maturation of HL-60 promyelocytic leukemia. In solution, DDATHF is a mixture of two diastereomers due to an asymmetric configuration at carbon 6. Incubation of HL-60 cells with 1 microM of each diastereomer resulted in an inhibition of cellular proliferation after 48 h that preceded an increase in the number of differentiated myeloid cells, as determined by the ability of cells to reduce nitroblue tetrazolium (NBT) and by the binding of the myeloid-specific antibody Mo 1. Several analogs of DDATHF were also tested as inducers of the differentiation of HL-60 cells. With the exception of the 10-acetyl analog of 5-deazatetrahydrofolic acid, all compounds displayed similar activities as inducers of maturation. The finding that both stereoisomers of DDATHF, as well as the analogs tested, could selectively reduce intracellular purine nucleotide levels suggested that these compounds inhibited purine nucleotide biosynthesis de novo. This possibility was confirmed by the finding that hypoxanthine completely prevented the reduction of intracellular purine nucleotide levels, as well as the induction of differentiation and the inhibition of cellular growth, by these folate analogs. The results suggest that GAR transformylase is a target for a series of compounds whose structures resemble that of tetrahydrofolate and indicate that the inhibition of GAR transformylase by these compounds is sufficient to induce the maturation of HL-60 leukemia cells.

Published

1991

22. Biochemical pharmacology of deazatetrahydrofolates

Author

G. P. Beardsley, A.R. Cashmore, B.A. Moroson, A.D. Cross, D. Wildman, G. Pizzorno, G.B. Grindey, and O. Russello

Subjects

Chemistry, Pharmacology, Biochemical Pharmacology

Published

1990

23. Transport of 5,10-dideazatetrahydrofolic acid (DDATHF) in CCRF-CEM sensitive and methotrexate resistant cell lines

Author

A.R. Cashmore, G. Pizzorno, G. P. Beardsley, B.A. Moroson, and A.D. Cross

Subjects

Chemistry, Ccrf cem, medicine, Cancer research, Methotrexate, Resistant cell, medicine.drug

Published

1990

24. Chemical synthesis of DNA oligomers containing cytosine arabinoside

Author

Thomas Mikita, A L Nussbaum, G P Beardsley, and M M Klaus

Subjects

Chemical Phenomena, Base pair, Oligonucleotide, Stereochemistry, Cytarabine, Temperature, Biology, Nucleic Acid Denaturation, Oligomer, Chemical synthesis, carbohydrates (lipids), Chemistry, chemistry.chemical_compound, Oligodeoxyribonucleotides, Biochemistry, chemistry, Genetics, Nucleic acid, Chromatography, High Pressure Liquid, DNA, Cytosine

Abstract

The solid phase phospite triester synthesis of oligodeoxynucleotides containing cytosine arabinoside (araC) is described. A protected araC phosphoramadite was prepared for the introduction of araC residues at 5'termini and internucleotide positions in DNA oligomers. These oligomers were utilized to demonstrate the formation of correct 3'-5' linkages, to test for alkaline lability at the araC site, and to study the stability of duplexes containing araC-G base pairs. For the introduction of araC residues at 3' terminal positions, a protected derivative of araC was coupled to functionalized silica. This material was used to prepare a test oligomer which was characterized enzymatically.

Published

1988

25. Identification of dihydropteridine reductase in human platelets

Author

G P Beardsley, Herbert T. Abelson, and Carolyn Gorka

Subjects

chemistry.chemical_classification, biology, Immunology, Cell Biology, Hematology, Tetrahydrobiopterin, Dihydropteridine Reductase, medicine.disease, Biochemistry, Enzyme assay, Cofactor, Hydroxylation, chemistry.chemical_compound, Hyperphenylalaninemia, Enzyme, chemistry, medicine, biology.protein, Platelet, medicine.drug

Abstract

Normal human platelets were shown to contain the enzyme dihydropteridine reductase. The enzyme was not found in a variety of other cells of hematogenous origin. Partial purification and kinetic and physical data indicated that the platelet enzyme is similar to that previously characterized from liver. Dihydropteridine reductase is important for the regeneration of tetrahydrobiopterin, a required cofactor in hydroxylation reactions involved in biogenic amine formation. The presence of the enzyme may indicate that some synthesis de novo of serotonin and/or catecholamines occurs in platelets, as opposed to a purely storage and transport function. In addition, screening for hyperphenylalaninemia due to dihydropteridine reductase deficiency may become feasible by assaying platelets for enzyme activity.

Published

1979

26. Augmentation of Fetal-Hemoglobin Production in Anemic Monkeys by Hydroxyurea

Author

G P Beardsley, David C. Linch, K W McIntyre, Norman L. Letvin, and David G. Nathan

Subjects

medicine.medical_specialty, Transcription, Genetic, Reticulocytosis, Anemia, Azacitidine, Methylation, Internal medicine, Fetal hemoglobin, medicine, Animals, Hydroxyurea, Cytotoxic T cell, Globin, Fetal Hemoglobin, Bloodletting, business.industry, DNA, General Medicine, Phlebotomy, medicine.disease, Globins, Surgery, Macaca fascicularis, Endocrinology, DNA methylation, Erythrocyte Count, medicine.symptom, business, medicine.drug

Abstract

The increase in fetal-hemoglobin synthesis in patients with beta-thalassemia or sickle-cell anemia induced by 5-azacytidine has been attributed to hypomethylation of DNA in the region of the gamma-globin genes. To determine whether hydroxyurea, a cytotoxic/cytostatic drug that does not influence DNA methylation, might stimulate fetal-hemoglobin synthesis, we phlebotomized two juvenile cynomolgus monkeys to induce anemia and reticulocytosis and then treated them with hydroxyurea. Immediately after phlebotomy was initiated, there was a rise in the level of F cells, which stabilized at an average value of 13 per cent in one animal and 20 per cent in the other during a two-month control period. Fetal hemoglobin gradually rose from undetectable values before bleeding to 3 per cent in one animal and 5 per cent in the other. Sixty-two days after initiation of phlebotomy, hydroxyurea (50 mg per kilogram of body weight per day for five days) induced only a small and transient increase in F cells and fetal hemoglobin. Two weeks later, however, a similar course (100 mg per kilogram per day) resulted in a prompt and dramatic increase in both indexes. These results strongly suggest that S-phase-specific cytotoxic/cytostatic drugs increase fetal hemoglobin by a mechanism that does not involve inhibition of DNA methylation.

Published

1984

27. Synthesis of pyrrolo[3,2-d]pyrimidines from furazano[3,4-d]pyrimidines via enolate and ene adducts

Author

Y. Maki, L. E. Crane, and G. P. Beardsley

Subjects

Chemistry, Organic Chemistry, Medicinal chemistry, Ene reaction, Adduct

Abstract

Aus den Furazano-pyrimidinen (I) oder (IV) erhalt man mit Acetylaceton (II) die Kondensationsprodukte (III).

Published

1980

28. A thin-layer chromatographic method for separation of thymidine and deoxyuridine nucleotides

Author

G P Beardsley and Herbert T. Abelson

Subjects

chemistry.chemical_classification, Chromatography, Pyrimidine, Stereochemistry, Biophysics, Uracil, Cell Biology, In Vitro Techniques, Biochemistry, Deoxyuridine, Thymine, Mice, chemistry.chemical_compound, Methotrexate, chemistry, Thymine Nucleotides, Animals, Nucleotide, Chromatography, Thin Layer, Thymidine phosphorylase, Deoxyuracil Nucleotides, Leukemia L1210, Thymidine, Molecular Biology

Abstract

A thin-layer chromatographic method for the separation of thymidine and deoxyuridine nucleotides and nucleosides is described. This procedure involves the following sequence of steps: (i) Ion-exchange thin-layer chromatography to afford separation into fractions of increasing degree of phosphorylation, (ii) conversion of each fraction into an equivalent mixture of thymine and uracil through the combined actions of alkaline phosphatase and thymidine phosphorylase, and (iii) partition thin-layer chromatographic separation of thymine and uracil. A key feature of the method is the specificity afforded by the second step which converts only thymidine and deoxyuridine nucleotides and nucleosides to the corresponding pyrimidine bases. An application of the method to the study of [3H]deoxyuridine metabolism in L1210 cells, as well as the effect of methotrexate on this metabolism is also described.

Published

1980

29. Thymlne glycol lesions terminate chain elongation by DNA polymerase I in vitro

Author

J M Clark and G P Beardsley

Subjects

DNA clamp, Base Sequence, biology, DNA polymerase, DNA polymerase II, DNA replication, DNA, Single-Stranded, DNA-Directed DNA Polymerase, Templates, Genetic, Base excision repair, DNA Polymerase I, Coliphages, Molecular biology, Biochemistry, Escherichia coli, Genetics, biology.protein, T-Phages, Primase, DNA, Circular, DNA polymerase I, Primer (molecular biology), Thymine

Abstract

Single-strand circular DNA from bacteriophage M13mp9 was chemically modified with osmium tetroxide to introduce specifically cis-thymine glycol lesions, a major type of DNA damage produced by ionizing radiation. An oligonucleotide primer was extended on damaged and undamaged templates using either the large fragment of E. coli pol I or T4 DNA polymerase. The reaction products were analysed by electrophoresis alongside a DNA sequence ladder. Synthesis on the damaged templates terminated at positions opposite thymine bases in the template. These results indicate that cis-thymine glycol lesions in single-strand DNA constitute blocks to synthesis by DNA polymerases in vitro. Surprisingly, replication halts after the correct nucleotide, dAMP, is inserted opposite the lesion. These results imply that the primary effect of the thymine glycol lesion is suppression of DNA synthesis and that the lesion is not a potent mutagen.

Published

1986

30. A new folate antimetabolite, 5,10-dideaza-5,6,7,8-tetrahydrofolate is a potent inhibitor of de novo purine synthesis

Author

R G Moran, E C Taylor, B. A. Moroson, and G. P. Beardsley

Subjects

Purine, Phosphoribosylaminoimidazolecarboxamide formyltransferase, Cell Biology, Biology, Biochemistry, Thymidylate synthase, Dihydrofolate reductase inhibitor, chemistry.chemical_compound, chemistry, Lometrexol, Dihydrofolate reductase, biology.protein, Purine metabolism, Molecular Biology, Hypoxanthine

Abstract

5,10-Dideazatetrahydrofolate (DDATHF) is a new antimetabolite designed as an inhibitor of folate metabolism at sites other than dihydrofolate reductase. DDATHF was found to inhibit the growth of L1210 and CCRF-CEM cells in culture at concentrations in the range of 10-30 nM. The inhibitory effect of DDATHF on the growth of L1210 and CCRF-CEM cells was reversed by either hypoxanthine or aminoimidazole carboxamide. Growth inhibition by DDATHF was prevented by addition of both thymidine and hypoxanthine, but not by thymidine alone. 5-Formyltetrahydrofolate reversed the effects of DDATHF in a dose-dependent manner. DDATHF had no appreciable inhibitory activity against either dihydrofolate reductase or thymidylate synthase in vitro, but was found to be an excellent substrate for folylpolyglutamate synthetase. DDATHF had little or no effect on incorporation of either deoxyuridine or thymidine into DNA, in distinct contrast to the effects of the classical dihydrofolate reductase inhibitor, methotrexate. DDATHF was found to deplete cellular ATP and GTP over the same concentrations as those inhibitory to leukemic cell growth, suggesting that the locus of DDATHF action was in the de novo purine biosynthesis pathway. The synthesis of formylglycinamide ribonucleotide in intact L1210 cells was inhibited by DDATHF with the same concentration dependence as inhibition of growth. This suggested that DDATHF inhibited glycinamide ribonucleotide transformylase, the first folate-dependent enzyme of de novo purine synthesis. DDATHF is a potent folate analog which suppresses purine synthesis through direct or indirect inhibition of glycinamide ribonucleotide transformylase.

Published

1989

31. Identification of dihydropteridine reductase in human platelets

Author

H T, Abelson, C, Gorka, and G P, Beardsley

Subjects

Blood Platelets, Molecular Weight, Kinetics, Dihydropteridine Reductase, Immunology, Humans, NADH, NADPH Oxidoreductases, Cell Biology, Hematology, Biochemistry

Abstract

Normal human platelets were shown to contain the enzyme dihydropteridine reductase. The enzyme was not found in a variety of other cells of hematogenous origin. Partial purification and kinetic and physical data indicated that the platelet enzyme is similar to that previously characterized from liver. Dihydropteridine reductase is important for the regeneration of tetrahydrobiopterin, a required cofactor in hydroxylation reactions involved in biogenic amine formation. The presence of the enzyme may indicate that some synthesis de novo of serotonin and/or catecholamines occurs in platelets, as opposed to a purely storage and transport function. In addition, screening for hyperphenylalaninemia due to dihydropteridine reductase deficiency may become feasible by assaying platelets for enzyme activity.

Published

1979

32. Methotrexate analogs. 11. Unambiguous chemical synthesis and in vitro biological evaluation of .alpha.- and .gamma.-monoesters as potential prodrugs

Author

William D. Ensminger, Andre Rosowsky, C. S. Yu, Herbert Lazarus, and G. P. Beardsley

Subjects

Leukemia, Experimental, Esterification, Chemistry, Stereochemistry, Esterases, Alpha (ethology), In Vitro Techniques, Prodrug, Chemical synthesis, In vitro, Methotrexate, Isomerism, Species Specificity, Drug Discovery, medicine, Animals, Folic Acid Antagonists, Humans, Molecular Medicine, Biotransformation, Cell Division, Cells, Cultured, medicine.drug, Biological evaluation

Published

1978

33. Template length, sequence context, and 3'-5' exonuclease activity modulate replicative bypass of thymine glycol lesions in vitro

Author

G P Beardsley and J.M. Clark

Subjects

DNA Replication, Exonuclease, Exodeoxyribonuclease V, DNA polymerase, DNA-Directed DNA Polymerase, Biochemistry, chemistry.chemical_compound, Humans, Polymerase, Klenow fragment, Base Sequence, biology, DNA Polymerase II, Templates, Genetic, DNA Polymerase I, Molecular biology, Thymine, Exodeoxyribonucleases, Oligodeoxyribonucleotides, chemistry, biology.protein, 3'-5' Exonuclease, DNA polymerase I, DNA, DNA Damage, HeLa Cells

Abstract

cis-Thymine glycol, a product of ionizing radiation damage to DNA, has been introduced quantitatively at a single site into oligonucleotide templates. The ability of DNA polymerases to replicate templates containing thymine glycol was studied by a primer extension assay, and three factors that influence replicative bypass of this lesion in vitro have been identified. These factors include template length, sequence context, and 3{prime}-5{prime} exonuclease activity. Synthesis by the large fragment of DNA polymerase I (Klenow fragment) terminates quantitatively opposite thymine glycol when the template strand extends only two nucleotides beyond the lesion. Significant bypass is observed when the length of the template beyond the lesion is increased to six nucleotides. On the longer templates, the frequency of bypass of the Klenow fragment depends upon the identity of the base immediately 5{prime} to thymine glycol. The extent of bypass is greatest with cytosine and least with adenine at this position. Bypass of thymine glycol lesions by DNA polymerase {alpha}{sub 2} from HeLa cells shows a qualitatively similar dependence upon local sequence context. In contrast, synthesis by T4 DNA polymerase is quantitatively blocked opposite the lesion regardless of template length or DNA sequence context. Synthesis by a mutant Klenow fragment that ismore » deficient in 3{prime}-5{prime} exonuclease activity, or by AMV reverse transcriptase, results in a significant increase in the frequency of bypass. Thus, increased nucleotide turnover at, or beyond, the site of the lesion is likely to contribute significantly to the arrest of synthesis provoked by cis-thymine glycol in vitro.« less

Published

1989

34. Correlation of cytotoxicity with incorporation of ara-C into DNA

Author

G P Beardsley, P P Major, Donald Kufe, and E M Egan

Subjects

Clonogenic survival, Density gradient, Kinetics, food and beverages, RNA, Cell Biology, biochemical phenomena, metabolism, and nutrition, Biology, Biochemistry, Molecular biology, carbohydrates (lipids), chemistry.chemical_compound, chemistry, Nucleic acid, Cytotoxicity, Arabinofuranosylcytosine triphosphate, Molecular Biology, DNA

Abstract

We have employed cesium sulfate density gradient analysis to monitor the incorporation of 1-beta-D-arabinofuranosylcytosine (ara-C) into L1210 cellular nucleic acid. This methodology permits a distinct separation of RNA and DNA under nondegrading conditions. The results demonstrate specific incorporation of ara-C into DNA with less than 1% of total incorporation into nucleic acid being detectable in RNA. Moreover, we have found a highly significant relationship (p < 0.0001) between the incorporation of ara-C into DNA with the loss of clonogenic survival. This relationship had not been established due to the previous use of alkaline conditions that degrade (ara-C) DNA. Our results suggest that the incorporation of ara-C into DNA is one mechanism responsible for producing lethal cellular events.

Published

1980

35. Lethality of human myeloblasts correlates with the incorporation of arabinofuranosylcytosine into DNA

Author

E M Egan, P P Major, Mark D. Minden, Donald Kufe, and G P Beardsley

Subjects

DNA Replication, Cell Survival, Cell, Biology, Cell Line, chemistry.chemical_compound, Myeloblast, medicine, Humans, Cells, Cultured, Multidisciplinary, Cytarabine, DNA replication, medicine.disease, Virology, Molecular biology, Clone Cells, Leukemia, Myeloid, Acute, Leukemia, medicine.anatomical_structure, chemistry, Cell culture, Bone marrow, Cell Division, DNA, Research Article, medicine.drug

Abstract

We recently demonstrated a highly significant relationship between the incorporation of 1-beta-D-arabinofuranosylcytosine (ara-C) into L1210 DNA and the loss of clonogenic survival. These studies have now been extended to the human promyeloblast (HL-60) cell line and myeloblasts from a patient with acute myelogenous leukemia. Our results demonstrate: (i) the specific internucleotide incorporation of ara-C into human myeloblast DNA; (ii) the lability of [3H]ara-C-labeled DNA to alkali which necessitates the use of nondegrading assay conditions; and (iii) a highly significant relationship (P less than 0.0001) between the loss of clonogenicity of these cells and the extent of ara-C incorporation. These findings suggest that the incorporation of ara-C into DNA is one of the initial events leading to cell lethality. This method is applicable to clinical samples of bone marrow and peripheral blood as an in vitro assay for studying the sensitivity of cell populations to this drug.

Published

1981

36. A novel ring contraction of a pyridazinone to a pyrazole. A possible pyridazyne intermediate

Author

Masahiro Takaya, Yoshifumi Maki, and G. P. Beardsley

Subjects

chemistry.chemical_compound, Contraction (grammar), chemistry, Stereochemistry, Organic Chemistry, Drug Discovery, Pyrazole, Biochemistry

Published

1971

37. Pteridines. XXVII. New synthetic route to pteridines and 7-azapteridines

Author

Edward C. Taylor, Y. Maki, Stephen F. Martin, and G. P. Beardsley

Subjects

Chemistry, Organic Chemistry, Organic chemistry

Published

1973

38. High-dose methotrexate in osteogenic sarcoma

Author

N, Jaffe, M P, Link, D, Cohen, D, Traggis, E, Frei, H, Watts, G P, Beardsley, and H T, Abelson

Subjects

Kinetics, Osteosarcoma, Lung Neoplasms, Methotrexate, Doxorubicin, Vincristine, Leucovorin, Humans, Antineoplastic Agents, Bone Neoplasms, Child

Abstract

From 1972 to 1979, high-dose methotrexate (HDMTX) and 3 adjuvant regimens were used at the Sidney Farber Cancer Institute and Children's Hospital Medical Center. In the first regiment, HDMTX was used alone; the second, HDMTX and adriamycin, and the third, weekly courses of HDMTX and combination. Actuarial disease-free survival achieved with these regimens in patient with local control of the primary lesion varied from 42 to 75% at 3 years. This compared favorably with historical control patients, of whom 50% were free of disease at 6 months and only 20% at 12 months. Among 41 patients with established pulmonary metastases, 14 were alive and free of disease from more than 4 to over 60 months. The most efficacious method of administering HDMTX was a weekly schedule which produced an overall response rate of 48% in the treatment of pulmonary metastases and primary tumor in patients previously not exposed to HDMTX. Urinary alkalinization was not a standard procedure, and investigations failed to demonstrate any significant effect of alkalinization on HDMTX pharmacokinetics.

Published

1981

39. Synthesis of the antileukemic agents 5,10-dideazaaminopterin and 5,10-dideaza-5,6,7,8-tetrahydroaminopterin

Author

P. J. Harrington, Edward C. Taylor, R. G. Moran, G. P. Beardsley, and S. R. Fletcher

Subjects

Male, Chemical Phenomena, Stereochemistry, Aminopterin, Ligases, chemistry.chemical_compound, Folic Acid, In vivo, Amide Synthases, Drug Discovery, Pyridine, medicine, Animals, Leukemia L1210, Tetrahydrofolates, Leukemia, Phosphoribosylaminoimidazolecarboxamide formyltransferase, Chemistry, Biological activity, Thymidylate Synthase, medicine.disease, Combinatorial chemistry, Methotrexate, Lometrexol, Molecular Medicine, Folic Acid Antagonists, medicine.drug

Abstract

Total syntheses from pyridine precursors of 5,10-dideazaaminopterin (1) and 5,10-dideaza-5,6,7,8-tetrahydroaminopterin (2) are described. These compounds exhibit significant in vivo activity against L1210 leukemia that is comparable to that observed with methotrexate.

Published

1985

40. ChemInform Abstract: METHOTREXATE ANALOGS. 21. DIVERGENT INFLUENCE OF ALKYL CHAIN LENGTH ON THE DIHYDROFOLATE REDUCTASE AFFINITY AND CYTOTOXICITY OF METHOTREXATE MONOESTERS

Author

R. A. Forsch, G. P. Beardsley, Andre Rosowsky, C. S. Yu, and Herbert Lazarus

Subjects

Pteridine derivatives, chemistry.chemical_classification, biology, Chemistry, Stereochemistry, General Medicine, Chain length, Dihydrofolate reductase, biology.protein, medicine, Methotrexate, Cytotoxicity, Alkyl, medicine.drug

Published

1984

41. Hydroxyurea enhances fetal hemoglobin production in sickle cell anemia

Author

Orah S. Platt, Stuart H. Orkin, Barbara A. Miller, David G. Nathan, G P Beardsley, and George J. Dover

Subjects

Adult, medicine.medical_specialty, Adolescent, Anemia, medicine.medical_treatment, Anemia, Sickle Cell, Biology, Methylation, Hydroxycarbamide, Leukocyte Count, Bone Marrow, Internal medicine, Fetal hemoglobin, medicine, Humans, Hydroxyurea, Fetal Hemoglobin, Fetus, Chemotherapy, Clinical Trials as Topic, General Medicine, DNA, medicine.disease, Hematopoietic Stem Cells, Sickle cell anemia, medicine.anatomical_structure, Endocrinology, Immunology, Female, Hemoglobin, Bone marrow, medicine.drug, Granulocytes, Research Article

Abstract

Hydroxyurea, a widely used cytotoxic/cytostatic agent that does not influence methylation of DNA bases, increases fetal hemoglobin production in anemic monkeys. To determine its effect in sickle cell anemia, we treated two patients with a total of four, 5-d courses (50 mg/kg per d, divided into three oral doses). With each course, fetal reticulocytes increased within 48-72 h, peaked in 7-11 d, and fell by 18-21 d. In patient I, fetal reticulocytes increased from 16.0 +/- 2.0% to peaks of 37.7 +/- 1.2, 40.0 +/- 2.0, and 32.0 +/- 1.4% in three successive courses. In patient II the increase was from 8.7 +/- 1.2 to 50.0 +/- 2.0%. Fetal hemoglobin increased from 7.9 to 12.3% in patient I and from 5.3 to 7.4% in patient II. Hemoglobin of patient I increased from 9.0 to 10.5 g/dl and in patient II from 6.7 to 9.9 g/dl. Additional single-day courses of hydroxyurea every 7-20 d maintained the fetal hemoglobin of patient I t 10.8-14.4%, and the total hemoglobin at 8.7-10.8 g/dl for an additional 60 d. The lowest absolute granulocyte count was 1,600/mm3; the lowest platelet count was 390,000/mm3. The amount of fetal hemoglobin per erythroid burst colony-forming unit (BFU-E)-derived colony cell was unchanged, but the number of cells per BFU-E-derived colony increased. Although examination of DNA synthesis in erythroid marrow cells in vitro revealed no decreased methylcytidine incorporation, Eco RI + Hpa II digestion of DNA revealed that hypomethylation of gamma-genes had taken place in vivo after treatment. This observation suggests that hydroxyurea is a potentially useful agent for the treatment of sickle cell anemia and that demethylation of the gamma-globin genes accompanies increased gamma-globin gene activity.

Published

1984

42. ChemInform Abstract: METHOTREXATE ANALOGS. 11. UNAMBIGUOUS CHEMICAL SYNTHESIS AND IN VITRO BIOLOGICAL EVALUATION OF α- AND Γ-MONOESTERS AS POTENTIAL PRODRUGS

Author

C. S. Yu, G. P. Beardsley, Andre Rosowsky, Herbert Lazarus, and W. D. Ensminger

Subjects

Chemistry, medicine, Methotrexate, General Medicine, Prodrug, Combinatorial chemistry, Chemical synthesis, In vitro, Biological evaluation, medicine.drug

Published

1978

43. Correlation of cytotoxicity with incorporation of ara-C into DNA

Author

D W, Kufe, P P, Major, E M, Egan, and G P, Beardsley

Subjects

Kinetics, Mice, Cell Survival, Cytarabine, Animals, DNA, Neoplasm, Leukemia L1210

Abstract

We have employed cesium sulfate density gradient analysis to monitor the incorporation of 1-beta-D-arabinofuranosylcytosine (ara-C) into L1210 cellular nucleic acid. This methodology permits a distinct separation of RNA and DNA under nondegrading conditions. The results demonstrate specific incorporation of ara-C into DNA with less than 1% of total incorporation into nucleic acid being detectable in RNA. Moreover, we have found a highly significant relationship (p0.0001) between the incorporation of ara-C into DNA with the loss of clonogenic survival. This relationship had not been established due to the previous use of alkaline conditions that degrade (ara-C) DNA. Our results suggest that the incorporation of ara-C into DNA is one mechanism responsible for producing lethal cellular events.

Published

1980

44. ChemInform Abstract: SYNTHESIS OF THE ANTILEUKEMIC AGENTS 5,10-DIDEAZAAMINOPTERIN AND 5,10-DIDEAZA-5,6,7,8-TETRAHYDROAMINOPTERIN

Author

P. J. Harrington, G. P. Beardsley, R. G. Moran, S. R. Fletcher, and Edward C. Taylor

Subjects

Stereochemistry, Chemistry, General Medicine

Abstract

Uber den Ester (V) erhalt man die Verbindungen (VI), von denen die Diamine in vivo ausgezeichnet gegen L1 210-Leukamie wirksam sind.

Published

1985

45. Functional consequences of the arabinosylcytosine structural lesion in DNA

Author

Thomas Mikita and G P Beardsley

Subjects

DNA polymerase, DNA-Directed DNA Polymerase, Biochemistry, Escherichia coli, Humans, Polymerase, Klenow fragment, chemistry.chemical_classification, DNA ligase, biology, Base Sequence, Chemistry, DNA replication, Cytarabine, RNA-Directed DNA Polymerase, DNA, DNA Polymerase II, Templates, Genetic, DNA Polymerase I, Molecular biology, Reverse transcriptase, Oligodeoxyribonucleotides, biology.protein, Primer (molecular biology), DNA polymerase I, DNA Damage, HeLa Cells

Abstract

Cytosine arabinoside (araC) is a potent antileukemic agent that is misincorporated into DNA in the course of its action. We have developed a chemical synthetic method that allows site-specific introduction of araC into synthetic DNA oligomers. We describe here the utilization of these oligomers as primer/template substrates for in vitro DNA synthesis reactions and as fragments for DNA ligation. These studies were undertaken to investigate the manner in which sites of araC misincorporation constitute sites of DNA dysfunction. AraCMP at the primer terminus dramatically reduced the rate of next nucleotide addition for Escherichia coli polymerase I (Klenow fragment) (Pol I), T4 polymerase, HeLa cell polymerase alpha 2 (Pol alpha 2), and AMV reverse transcriptase. Polymerases with associated 3'-5' exonuclease activity preferentially excised araCMP from the primer terminus prior to chain elongation. AraCMP-terminated fragments were ligated more slowly than control fragments by T4 DNA ligase. AraCMP located at an internucleotide site in the template markedly slowed replicative bypass for Pol I, T4 polymerase, and Pol alpha 2, but not for reverse transcriptase. Synthesis was partially arrested after insertion of the correct nucleotide opposite the lesion site. These results suggest a complex mechanism for the inhibition of DNA replication by araC when it is misincorporated into DNA.

Published

1988

46. Induction of HL-60 leukemia cell differentiation by the novel antifolate 5,10-dideazatetrahydrofolic acid

Author

J A, Sokoloski, G P, Beardsley, and A C, Sartorelli

Subjects

Hydroxymethyl and Formyl Transferases, Cell Differentiation, Flow Cytometry, Adenosine Triphosphate, Leukemia, Promyelocytic, Acute, Tumor Cells, Cultured, Folic Acid Antagonists, Humans, Guanosine Triphosphate, Interphase, Purine Nucleotides, Acyltransferases, Cell Division, Tetrahydrofolates, Phosphoribosylglycinamide Formyltransferase

Abstract

The novel tetrahydrofolate, 5,10-dideazatetrahydrofolic acid (DDATHF), was designed as an inhibitor of folate metabolism at a site other than dihydrofolate reductase. DDATHF has been shown to inhibit glycinamide ribonucleotide transformylase, a folate-requiring enzyme that catalyzes the first of two one-carbon transfer reactions in the de novo purine nucleotide biosynthetic pathway. Incubation of HL-60 promyelocytic leukemia cells with 5 x 10(-8) to 10(-5) M DDATHF resulted in a marked inhibition of growth after 48 h, with a complete cessation of cellular replication by day 4. Cell cycle analyses of DDATHF-treated HL-60 cells demonstrated an initial block in early S phase by day 3 followed by an accumulation of cells in the G1 and G2 + M phases of the cell cycle. Inhibition of growth was accompanied by a concentration-dependent increase in the percentage of mature myeloid cells that expressed nitroblue tetrazolium positivity, and a small increase in nonspecific esterase activity. Induction of differentiation and inhibition of growth by DDATHF were completely prevented by hypoxanthine and 5(4)-amino-4(5)-imidazole carboxamide, suggesting that depletion of intracellular purine nucleotide pools has an important role in the biological effects of this inhibitor. This possibility was confirmed by the finding that DDATHF caused a pronounced reduction in intracellular GTP and ATP levels within 2 h, with maximum decreases being observed by 24 h, a time interval which preceded the inhibition of cellular proliferation by this agent. Pyrimidine nucleoside triphosphate levels were markedly increased under these conditions. The findings indicate the importance of purine nucleotides to both the inhibition of growth and the induction of differentiation of HL-60 leukemia cells by DDATHF.

Published

1989

47. Influence of cell cycle phase-specific agents on simian fetal hemoglobin synthesis

Author

David C. Linch, Barbara A. Miller, K W McIntyre, David G. Nathan, Norman L. Letvin, and G P Beardsley

Subjects

medicine.medical_specialty, Reticulocytes, Mitosis, Biology, Vinblastine, Cell cycle phase, Colony-Forming Units Assay, Internal medicine, Fetal hemoglobin, medicine, Animals, Hydroxyurea, Erythropoiesis, Reticulocytopenia, Progenitor cell, Fetal Hemoglobin, Dose-Response Relationship, Drug, Cell Cycle, General Medicine, medicine.disease, Macaca fascicularis, Endocrinology, medicine.anatomical_structure, Immunology, Hemoglobin F, Azacitidine, Bone marrow, medicine.drug, Research Article

Abstract

To determine the influence of cell cycle-specific agents on primate hematopoiesis and fetal hemoglobin production, two juvenile cynomolgus monkeys (Macaca fascicularis) were repeatedly bled to maintain their hemoglobins at approximately 6.5 g/dl and fetal hemoglobin levels at 3-5%. Six separate 5-d courses of hydroxyurea at 100 mg/kg per d were then administered over the next 200 d while phlebotomy was continued. These courses of hydroxyurea progressively raised the fetal hemoglobin levels to 17 and 18%, respectively. The drug had very little effect on the frequency of immature erythroid progenitors (BFU-E) in the bone marrow, but caused a marked reduction in the frequency of later progenitors (CFU-E) and a transient fall in the reticulocyte count. Following the courses of hydroxyurea, the number of F cells and the fetal hemoglobin level fell to base line over a period of 4 wk. Two control animals which were not phlebotomized showed no detectable increase in F cells or fetal hemoglobin when treated with the same regimen of hydroxyurea. A 5-d course of 5-azacytidine at 8 mg/kg per d was then given to each of the phlebotomized animals. This produced a more profound, albeit transient, reticulocytopenia, a fall in the CFU-E/BFU-E ratio, and a prompt increase in the fetal hemoglobin to levels even higher than were seen following a single 5-d course of hydroxyurea at 100 mg/kg/d. Subsequently, the animals were given a single dose of vinblastine at 0.4 mg/kg which reduced reticulocytes and CFU-E to the same extent as hydroxyurea; however, vinblastine at this dose had no effect on hemoglobin F (HbF) production. In contrast, when vinblastine was administered to the phlebotomized monkeys as a 5-d course at 0.2 mg/kg/d, prolonged reticulocytopenia followed by dramatic F cell and HbF responses were seen. Combinations of single dose vinblastine and a 5-d course of hydroxyurea were subsequently administered using two different schedules. When the animals received vinblastine on the first day of a 5-d course of hydroxyurea, the F cell response was double that seen following hydroxyurea treatment alone. In contrast, when vinblastine was administered on the final day of hydroxyurea treatment, the magnitude of the F cell response was the same as that which occurred following hydroxyurea treatment alone, but the onset of the rise was delayed for 4 d and HbF/F cell response was much higher. These results establish several important features of the fetal hemoglobin response to cytotoxic agents in the primate model. The response requires accelerated erythropoiesis and is preceded by transient reticulocytopenia. The response is produced by S phase- and M phase-specific agents when given in sufficient doses and at appropriate schedules. Passage of erythrocyte progenitors through M phase appears to be necessary for expression of the effect produced by S phase agents. The fetal hemoglobin response induced by cytotoxic drug administration occurs during the recovery of erythropoiesis following marrow suppression.

Published

1985

48. Synthesis and antitumor activity of 5-deaza-5,6,7,8-tetrahydrofolic acid and its N10-substituted analogues

Author

Shih Chuan, Richard G. Moran, Edward C. Taylor, James M. Hamby, G. B. Grindey, G. P. Beardsley, and S. M. Rinzel

Subjects

Chemical Phenomena, Stereochemistry, medicine.drug_class, Nitrogen, Antineoplastic Agents, Antimetabolite, chemistry.chemical_compound, Mice, In vivo, Drug Discovery, medicine, Tumor Cells, Cultured, Animals, Humans, Tetrahydrofolic acid, Purine metabolism, Leukemia L1210, Tetrahydrofolates, Biological activity, Chemistry, chemistry, Purines, Lactam, Molecular Medicine, Growth inhibition, Lead compound

Abstract

Syntheses of 5-deaza-5,6,7,8-tetrahydrofolic acid (7a) and its 10-formyl (7b), 10-acetyl (7c), and 10-methyl (7d) derivatives are described. These compounds, prepared as analogues of 5,10-dideaza-5,6,7,8-tetrahydrofolic acid (DDATHF), the lead compound of a new class of folate antimetabolites, exhibit potent growth inhibition against leukemic cells in culture as well as substantial antitumor activity against transplantable murine solid tumors in vivo.

Published

1989

49. A new folate antimetabolite, 5,10-dideaza-5,6,7,8-tetrahydrofolate is a potent inhibitor of de novo purine synthesis

Author

G P, Beardsley, B A, Moroson, E C, Taylor, and R G, Moran

Subjects

DNA Replication, Glycine, DNA, Neoplasm, gamma-Glutamyl Hydrolase, Ribonucleotides, Cell Line, Kinetics, Mice, Methotrexate, Liver, Purines, Tumor Cells, Cultured, Animals, Humans, Leukemia L1210, Cell Division, Tetrahydrofolates

Abstract

5,10-Dideazatetrahydrofolate (DDATHF) is a new antimetabolite designed as an inhibitor of folate metabolism at sites other than dihydrofolate reductase. DDATHF was found to inhibit the growth of L1210 and CCRF-CEM cells in culture at concentrations in the range of 10-30 nM. The inhibitory effect of DDATHF on the growth of L1210 and CCRF-CEM cells was reversed by either hypoxanthine or aminoimidazole carboxamide. Growth inhibition by DDATHF was prevented by addition of both thymidine and hypoxanthine, but not by thymidine alone. 5-Formyltetrahydrofolate reversed the effects of DDATHF in a dose-dependent manner. DDATHF had no appreciable inhibitory activity against either dihydrofolate reductase or thymidylate synthase in vitro, but was found to be an excellent substrate for folylpolyglutamate synthetase. DDATHF had little or no effect on incorporation of either deoxyuridine or thymidine into DNA, in distinct contrast to the effects of the classical dihydrofolate reductase inhibitor, methotrexate. DDATHF was found to deplete cellular ATP and GTP over the same concentrations as those inhibitory to leukemic cell growth, suggesting that the locus of DDATHF action was in the de novo purine biosynthesis pathway. The synthesis of formylglycinamide ribonucleotide in intact L1210 cells was inhibited by DDATHF with the same concentration dependence as inhibition of growth. This suggested that DDATHF inhibited glycinamide ribonucleotide transformylase, the first folate-dependent enzyme of de novo purine synthesis. DDATHF is a potent folate analog which suppresses purine synthesis through direct or indirect inhibition of glycinamide ribonucleotide transformylase.

Published

1989

50. Methotrexate analogues. 21. Divergent influence of alkyl chain length on the dihydrofolate reductase affinity and cytotoxicity of methotrexate monoesters

Author

R. A. Forsch, G. P. Beardsley, C. S. Yu, Herbert Lazarus, and Andre Rosowsky

Subjects

DNA Replication, Drug Evaluation, Preclinical, Cell Line, Structure-Activity Relationship, immune system diseases, Drug Discovery, Dihydrofolate reductase, medicine, Animals, Humans, heterocyclic compounds, Cytotoxicity, IC50, biology, Chemistry, Lymphoblast, Biological activity, Molecular biology, Leukemia, Lymphoid, Methotrexate, Biochemistry, Liver, Enzyme inhibitor, Cell culture, biology.protein, Molecular Medicine, Folic Acid Antagonists, lipids (amino acids, peptides, and proteins), Cattle, Indicators and Reagents, medicine.drug

Abstract

n-Octyl, n-dodecyl, and n-hexadecyl alpha- and gamma-esters of methotrexate (MTX) were compared with the previously described alpha- and gamma-n-butyl esters and with MTX as inhibitors of dihydrofolate reductase (DHFR) and human leukemic lymphoblasts (CEM cells) in culture. The overall order of activity in both test systems was MTX greater than MTX gamma-esters greater than MTX alpha-esters. In the DHFR assay the activity of the alpha-esters followed the order C4 greater than C8 congruent to C12 greater than C16, whereas for the gamma-esters this order was C4 congruent to C8 greater than C12 greater than C16. On the other hand, the order of cytotoxic activity in culture in both series was C16 greater than C12 greater than C8 greater than C4. Increasing the alkyl chain length in the ester moiety therefore decreases DHFR affinity but increases cytotoxicity. The most potent member of the compounds tested was the gamma-n-hexadecyl ester, whose IC50 against CEM cells was 0.11 microM as compared with 0.025 microM for MTX. In a comparison of the effect of treatment with the gamma-n-hexadecyl ester (10(-5) M, 1 h) on DNA synthesis in CEM and CEM/MTX cells, the latter of which are 120-fold resistant to MTX by virtue of a transport defect, the ester produced only 4-fold less inhibition in the resistant line than in the parental line. These results suggest possible use of this compound or related derivatives in the treatment of MTX-resistant tumors with impaired transport.

Published

1984