Your search keyword '"Methotrexate toxicity"' showing total 12 results

1. Carboxypeptidase G2 rescue in patients with methotrexate intoxication and renal failure.

Author

Buchen, S., Ngampolo, D., Melton, R. G., Hasan, C., Zoubek, A., Henze, G., Bode, U., and Fleischhack, G.

Subjects

*METHOTREXATE, *HETEROCYCLIC compounds, *IMMUNOSUPPRESSIVE agents, *BENZOIC acid, *ENZYMES, *BLOOD plasma, *RESEARCH, *CLINICAL trials, *RESEARCH methodology, *PROTEOLYTIC enzymes, *ANTINEOPLASTIC agents, *MEDICAL cooperation, *EVALUATION research, *ANTIMETABOLITES, *SEPSIS, *COMPARATIVE studies, *BLOOD diseases, *ACUTE kidney failure

Abstract

The methotrexate (MTX) rescue agent carboxypeptidase G2 (CPDG2) rapidly hydrolyses MTX to the inactive metabolite DAMPA (4-[[2,4-diamino-6-(pteridinyl)methyl]-methylamino]-benzoic acid) and glutamate in patients with MTX-induced renal failure and delayed MTX excretion. DAMPA is thought to be an inactive metabolite of MTX because it is not an effective inhibitor of the MTX target enzyme dihydrofolate reductase. DAMPA is eliminated more rapidly than MTX in these patients, which suggests a nonrenal route of elimination. In a phase II study (May 1997-March 2002), CPDG2 was administered intravenously to 82 patients at a median dose of 50 U kg(-1) (range 33-60 U kg(-1)). Eligible patients for this study had serum MTX concentrations of >10 microM at 36 h or >5 microM at 42 h after start of MTX infusion and documented renal failure (serum creatinine > or =1.5 times the upper limit of normal). Immediately before CPDG2 administration, a median MTX serum level of 11.93 microM (range 0.52-901 microM) was documented. Carboxypeptidase G2 was given at a median of 52 h (range 25-178 h) following the start of an MTX infusion of 1-12 g m(-2) 4-36 h(-1) and resulted in a rapid 97% (range 73-99%) reduction of the MTX serum level. Toxicity related to CPDG2 was not observed. Toxicity related to MTX was documented in about half the patients; four patients died despite CPDG2 administration due to severe myelosuppression and septic complications. In conclusion, administration of CPDG2 is a well-tolerated, safe and a very effective way of MTX elimination in delayed excretion due to renal failure. [ABSTRACT FROM AUTHOR]

Published

2005

2. Carboxypeptidase G2 rescue in patients with methotrexate intoxication and renal failure

Author

Gudrun Fleischhack, Udo Bode, Roger G. Melton, Carola Hasan, Günter Henze, D Ngampolo, S. Buchen, and Andreas Zoubek

Subjects

musculoskeletal diseases, Adult, Male, Cancer Research, medicine.medical_specialty, Antimetabolites, Antineoplastic, Adolescent, medicine.drug_class, Pharmacology, Antimetabolite, acute renal failure, chemistry.chemical_compound, Glutamate carboxypeptidase, Internal medicine, Sepsis, Carboxypeptidase-G2, Clinical Studies, medicine, methotrexate toxicity, Humans, heterocyclic compounds, skin and connective tissue diseases, high-dose methotrexate, Child, carboxypeptidase G2, Aged, Creatinine, business.industry, Glucarpidase, Infant, gamma-Glutamyl Hydrolase, Acute Kidney Injury, Middle Aged, Hematologic Diseases, Endocrinology, Methotrexate, Oncology, chemistry, Child, Preschool, Toxicity, Antifolate, Female, business, medicine.drug

Abstract

The methotrexate (MTX) rescue agent carboxypeptidase G2 (CPDG2) rapidly hydrolyses MTX to the inactive metabolite DAMPA (4-[[2,4-diamino-6-(pteridinyl)methyl]-methylamino]-benzoic acid) and glutamate in patients with MTX-induced renal failure and delayed MTX excretion. DAMPA is thought to be an inactive metabolite of MTX because it is not an effective inhibitor of the MTX target enzyme dihydrofolate reductase. DAMPA is eliminated more rapidly than MTX in these patients, which suggests a nonrenal route of elimination. In a phase II study (May 1997-March 2002), CPDG2 was administered intravenously to 82 patients at a median dose of 50 U kg(-1) (range 33-60 U kg(-1)). Eligible patients for this study had serum MTX concentrations of10 microM at 36 h or5 microM at 42 h after start of MTX infusion and documented renal failure (serum creatinineor =1.5 times the upper limit of normal). Immediately before CPDG2 administration, a median MTX serum level of 11.93 microM (range 0.52-901 microM) was documented. Carboxypeptidase G2 was given at a median of 52 h (range 25-178 h) following the start of an MTX infusion of 1-12 g m(-2) 4-36 h(-1) and resulted in a rapid 97% (range 73-99%) reduction of the MTX serum level. Toxicity related to CPDG2 was not observed. Toxicity related to MTX was documented in about half the patients; four patients died despite CPDG2 administration due to severe myelosuppression and septic complications. In conclusion, administration of CPDG2 is a well-tolerated, safe and a very effective way of MTX elimination in delayed excretion due to renal failure.

Published

2005

3. Effect of modulation of the transferrin receptor on gallium-67 uptake and cytotoxicity in lymphoma cell lines.

Author

van Leeuwen-Stok AE, Schuurhuis GJ, Dräger AM, Visser-Platier AW, Teule GJ, and Huijgens PC

Subjects

Biological Transport, Cell Cycle drug effects, Cell Division drug effects, Cell Line, Cell Survival drug effects, Cytarabine toxicity, Flow Cytometry, Gallium Radioisotopes toxicity, Gene Expression drug effects, Humans, Hydroxyurea toxicity, Lymphoma, Methotrexate toxicity, Tumor Cells, Cultured, Tumor Stem Cell Assay, Antineoplastic Agents toxicity, Cell Survival radiation effects, Gallium Radioisotopes pharmacokinetics, Receptors, Transferrin biosynthesis

Abstract

Gallium-67 is a radionuclide that accumulates in haematological malignancies and is used for diagnostic purposes. Uptake of 67Ga into the cell occurs via the transferrin receptor, which is differentially expressed during the various cell cycle phases. With the aim of selectively increasing 67Ga uptake, we studied whether the transferrin receptor (TfR) expression could be modulated in the U937 and U715 lymphoma cell lines by cytostatic drugs inducing cell cycle phase accumulation. We tested clinically relevant drugs such as 1-beta-D-arabinofuranosylcytosine (Ara-C), hydroxyurea and methotrexate. Cytotoxicity was determined by testing the clonogenic capacity of the lymphoma cell lines. All three drugs induced an increase in S-phase content, TfR expression and 67Ga uptake in U937 and U715 single cells. The combinations of drugs and 67Ga resulted in an additive effect on the clonogenic capacity. In U937 spheroids, cultured by the fibrin clot technique, we found an accumulation in the S-phase too as well as an increase of the transferrin receptor expression after Ara-C preincubation. As in single cells 67Ga uptake was increased without synergistic effects on the clonogenic capacity. In conclusion, priming with drugs induces increased transferrin receptor expression and 67Ga uptake. Inhibition of clonogenic capacity was additive rather than synergistic.

Published

1996

4. Monoclonal antibody targeting of methotrexate (MTX) against MTX-resistant tumour cell lines.

Author

Affleck K and Embleton MJ

Subjects

Antibodies, Monoclonal immunology, Antibodies, Neoplasm immunology, Antigens, Neoplasm immunology, Binding, Competitive, Biological Transport, Drug Resistance, Humans, Immunotoxins administration & dosage, In Vitro Techniques, Methotrexate toxicity, Osteosarcoma immunology, Tetrahydrofolate Dehydrogenase metabolism, Tumor Cells, Cultured, Methotrexate administration & dosage, Osteosarcoma drug therapy

Abstract

Several Methotrexate (MTX)-resistant sublines of the osteogenic sarcoma cell line 791T were derived by continuous selection in the presence of MTX and 12-O-tetradecanoylphorbol-13-acetate (TPA). Studies including assays of the uptake and binding of [3H]MTX and fluoresceinated-MTX, determined that these sublines showed diminished MTX transport, and that none of them appeared to overproduce the MTX-target enzyme dihydrofolate reductase. Conjugates of the anti-791T monoclonal antibody 791T/36 linked to MTX via human serum albumin (HSA) were prepared by Dr M.C. Garnett. These were cytotoxic selectively for cells bearing the 791T/36-defined antigen (gp72), and were found to be as cytotoxic to most of the MTX-resistant 791T sublines as they were to parental 791T cells. Furthermore, an anti-MTX/anti-gp72 bispecific antibody 516 augmented the cytotoxicity of HSA-MTX conjugate to the MTX-resistant 791T variant R120 apparently as efficiently as for parental 791T cells. It is suggested that acquired drug resistance caused by deficient transport mechanisms may be partially or wholly overcome by targeting the drug to a readily-internalised cell surface antigen.

Published

1992

5. DNA fragmentation, dATP pool elevation and potentiation of antifolate cytotoxicity in L1210 cells by hypoxanthine.

Author

Kwok JB and Tattersall MH

Subjects

Animals, Drug Synergism, Folic Acid toxicity, Hypoxanthine, In Vitro Techniques, Leukemia L1210, Mice, Tumor Cells, Cultured, DNA Damage, Deoxyadenine Nucleotides metabolism, Folic Acid analogs & derivatives, Hypoxanthines administration & dosage, Methotrexate toxicity

Abstract

Exogenous purines (greater than or equal to 10(-5)M) can modulate the cytotoxicity of methotrexate (MTX) in cultured cells, protecting cells at low MTX concentrations (less than or equal to 8 x 10(-8) M) and markedly potentiating its effect at higher concentrations. The ability of hypoxanthine (HX) to modulate the effects of two antifolates-ICI 198583 (an inhibitor of thymidylate synthetase) and piritrexim (PTX, a lipophilic inhibitor of DHFR)-was investigated using cultured mouse leukaemic cells, L1210. HX (10(-4) M) was found to potentiate only the cytotoxicity of DHFR inhibitors (MTS and PTX), increasing cell kill by 20-70 fold to the level achieved by an equivalent concentration (10(-5) M) of ICI 198583 alone. Agarose gel electrophoresis of DNA extracted from cells exposed to antifolates for 24 h demonstrated that the chromatin was cleaved into multimers of 200 base pairs. This pattern of DNA cleavage indicates cell death via apoptosis. The degree of DNA fragmentation was found to be closely linked to cytotoxicity. DNA fragmentation increased from 50% in cells treated with 10(-5) M MTX or PTX to 70% when HX was added with the drugs, a level achieved by 10(-5)M ICI 198583 alone. HX potentiation of cytotoxicity was correlated with a substantial increase in dATP in conjunction with low dTTP pools. The specific potentiation of DHFR inhibitors by HX may be due to their inhibition of purine synthesis with a concurrent rise in PRPP levels. Addition of HX with MTX substantially raised intracellular purine levels via the salvage pathway as indicated by ribonucleotide pool measurements. ICI 198583, on the other hand, stimulated de novo purine synthesis with or without added HX. Treatment with MTX plus HX or ICI 198583 (with or without HX) caused a reduction of dTTP pools to 8% of untreated control and excess dATP accumulation. The subsequent elevation (to 300% of control) of the dATP pool may provide a signal for endonucleolytic fragmentation of DNA and subsequent cell death.

Published

1992

6. The effect of methotrexate on spontaneous mammary adenocarcinomata in female C3H mice.

Author

Shewell J

Subjects

Adenocarcinoma pathology, Animals, Dose-Response Relationship, Drug, Female, Lethal Dose 50, Leucovorin pharmacology, Mammary Neoplasms, Experimental pathology, Methotrexate administration & dosage, Methotrexate toxicity, Mice, Mice, Inbred C3H, Time Factors, Adenocarcinoma drug therapy, Mammary Neoplasms, Experimental drug therapy, Methotrexate therapeutic use

Abstract

The effect of methotrexate on solid rodent tumours has been investigated using the spontaneous mammary adenocarcinoma of the female C3H/Bts mouse. As these tumours exhibit a wide range of volume doubling times, calculations of tumour response to methotrexate must be related to doubling time. When methotrexate is injected into the tumour a dose-dependent tumour response is obtained. Systemic citrovorum "rescue" prevents methotrexate lethalities but reduces tumour response by a factor of 2. Methotrexate-treated tumours have an increased volume doubling time post treatment.

Published

1976

7. Methotrexate enterotoxicity: influence of drug dose and timing in the rat.

Author

Pinkerton CR and Milla PJ

Subjects

Animals, Drug Administration Schedule, Glucose metabolism, Male, Methotrexate administration & dosage, Rats, Rats, Inbred Strains, Sodium metabolism, Water metabolism, Intestinal Absorption drug effects, Jejunum drug effects, Methotrexate toxicity

Published

1984

8. Effects of varying the interval between courses of methotrexate on its myelotoxic and anti-leukaemic activities.

Author

Harding B, Culvenor J, and MacLennan IC

Subjects

Animals, Body Weight drug effects, Bone Marrow Cells, Cell Count, Dose-Response Relationship, Drug, Leukocyte Count, Methotrexate therapeutic use, Methotrexate toxicity, Neoplasm Transplantation, Neutropenia chemically induced, Neutrophils, Rats, Time Factors, Transplantation, Isogeneic, Leukemia, Experimental drug therapy, Methotrexate administration & dosage

Abstract

The toxicity produced by two courses of methotrexate separated by different intervals has been studied in matched groups of rats. The maximum degree of neutropenia reached when courses were separated by 8 days or more was no greater than that seen after a single course of methotrexate. However, when courses of neutropenia following the second course of methotrexate was directly related to the level of depression of bone marrow cell numbers at the time of the second course. Conversely the anti-leukaemic effects of 2 courses of methotrexate, in terms of time of onset of leukaemia and time of death in rats transplanted with a syngeneic T-cell leukaemia, are shown to be similar when courses of methotrexate are separated by between 2 and 12 days. Thus in this system, chemotherapeutic schedules using methotrexate may be designed on the basis of minimal host toxicity without prejudicing anti-leukaemic effects. These results are discussed in relation to toxicity and anti-leukaemic effects observed during UKALL trials of treatment in acute lymphoblastic leukaemia.

Published

1977

9. Antagonism between inhibitors of DNA synthesis.

Author

Bagshawe KD and Woods RJ

Subjects

Animals, Body Weight drug effects, Drug Combinations, Leukemia drug therapy, Male, Meninges, Methotrexate toxicity, Mice, Mice, Inbred CBA, Rats, Rats, Inbred Strains, Cytarabine toxicity, Methotrexate antagonists & inhibitors

Published

1972

10. The sensitivity to chemotherapeutic agents of a rat tumour grown in immunosuppressed mice.

Author

Sheard CE, Double JA, and Berenbaum MC

Subjects

Animals, Antilymphocyte Serum, Azirines therapeutic use, Azirines toxicity, Benzoates therapeutic use, Benzoates toxicity, Lethal Dose 50, Melphalan therapeutic use, Melphalan toxicity, Methotrexate therapeutic use, Methotrexate toxicity, Mice, Neoplasm Transplantation, Nitro Compounds toxicity, Nitrogen Mustard Compounds therapeutic use, Nitrogen Mustard Compounds toxicity, Rats, Thymectomy, Transplantation, Heterologous, Antineoplastic Agents therapeutic use, Carcinoma 256, Walker drug therapy, Immunosuppression Therapy

Abstract

The rat Walker 256 tumour was grown in mice that had previously been thymectomized and treated with anti-lymphocyte serum. These rat tumour-bearing mice were used to determine the therapeutic indices of 4 anti-tumour drugs.The agent with the highest index of the four examined was 5-aziridino 2,4-dinitrobenzamide (CB1954), followed by melphalan, aniline mustard and methotrexate, in that order. This rank order is the same as that found when therapeutic indices are determined on the Walker tumour growing in the rat. In this system, therefore, drugs have been ranked correctly in effectiveness against a rat tumour by measuring their effects on the tumour when growing in an immunosuppressed xenogeneic species. The implications for testing the drug sensitivity of individual human tumours before treating the patient are discussed.

Published

1971

11. Reversal of methotrexate toxicity in mice by 5-methyltetrahydrofolic acid.

Author

Blair JA and Searle CE

Subjects

Animals, Folic Acid administration & dosage, Leucovorin pharmacology, Male, Methotrexate toxicity, Mice, Folic Acid pharmacology, Methotrexate antagonists & inhibitors

Abstract

1. Mice have been compeletly protected against the lethal effects of repeated injections of methotrexate by 5-methyltetrahydrofolic acid. Methotrexate-resistant cells probably owe their resistance to their high content of this substance.2. Daily small doses were much more effective than fewer but larger doses.3. The reduced efficiency found in counteracting high dosages of methotrexate may be due to interference with folate transport across cell walls.4. 5-Methyltetrahydrofolic acid and citrovorum factor did not differ greatly in their ability to inhibit methotre toxicity. It is suggested that the pharmaceutical effects of citrovorum factor are due to its conversion to 5-methyltetrahydrofolic acid.

Published

1970

12. The variability of individual tolerance to methotrexate in cancer patients.

Author

Hansen HH, Selawry OS, Holland JF, and McCall CB

Subjects

Adult, Age Factors, Aged, Alopecia chemically induced, Blood Urea Nitrogen, Body Weight, Chemical and Drug Induced Liver Injury, Conjunctivitis chemically induced, Creatinine blood, Diarrhea chemically induced, Drug Eruptions etiology, Folic Acid blood, Humans, Injections, Intravenous, Leukopenia chemically induced, Methotrexate administration & dosage, Middle Aged, Nausea chemically induced, Neoplasms radiotherapy, Serum Albumin analysis, Stomatitis chemically induced, Thrombocytopenia chemically induced, Time Factors, Vomiting chemically induced, Methotrexate toxicity, Neoplasms drug therapy

Abstract

Individual tolerance to single or widely spaced doses of methotrexate was explored in 49 patients with advanced cancer with normal serum creatinine and/or blood urea nitrogen. Methotrexate was given as an intravenous infusion over 1 hour at initial doses of 80-120 mg./m(2) body surface area. The doses were increased by 50% increments every 2 weeks until moderate toxicity occurred, arbitrarily defined as leukopenia <5000/mm.(3), and/or thrombocytopenia <100,000/mm.(3), and/or the appearance of oral mucous or intestinal toxicity.The individual dose required to produce initial evidence of toxicity varied by a factor of 18 between 50 and 900 mg./m(2). Starting doses above 80 mg./m(2) were potentially hazardous. Dose limiting toxicity consisted of leukopenia with or without stomatitis in 81% of the patients, and stomatitis without leukopenia, in 19%. Thrombocytopenia was seen in 19% of the patients, but was never a dose limiting factor alone. Leukopenia always preceded thrombocytopenia. The nadir for haematologic toxicity varied considerably between day 5-15 and 9-14 for leukocytes and platelets, respectively, while oral ulcerations, when they occurred, consistently began between days 3-6 after drug administration. Other toxic manifestations included dermatologic changes in 8 patients, hepatic dysfunction in 7, conjunctivitis in 7, nausea and vomiting in 6, alopecia in 4, and diarrhea in 3 patients.The only factor which predicted toxicity was the patient's age. Drug tolerance was independent of previous chemotherapy or radiotherapy, weight loss, serum albumin or pretreatment serum folic acid levels.

Published

1971