Your search keyword '"Altretamine toxicity"' showing total 25 results

1. Evaluation of the porphyrinogenic risk of antineoplastics.

Author

Cochón AC, Aldonatti C, San Martín de Viale LC, and Wainstok de Calmanovici R

Subjects

Alkylating Agents toxicity, Altretamine toxicity, Animals, Antineoplastic Agents adverse effects, Antineoplastic Agents chemistry, Azathioprine toxicity, Busulfan toxicity, Chick Embryo, Cyclophosphamide adverse effects, Cyclophosphamide chemistry, Cyclophosphamide toxicity, Dacarbazine toxicity, Female, Ferrochelatase drug effects, Ferrochelatase metabolism, Flavoproteins, Fluorouracil toxicity, Liver drug effects, Liver metabolism, Male, Mice, Mice, Inbred BALB C, Mitochondrial Proteins, Oxidoreductases drug effects, Oxidoreductases metabolism, Porphyrins metabolism, Procarbazine toxicity, Protoporphyrinogen Oxidase, Structure-Activity Relationship, Antineoplastic Agents toxicity, Dicarbethoxydihydrocollidine toxicity, Oxidoreductases Acting on CH-CH Group Donors, Porphyrias chemically induced

Abstract

The use of antineoplastics is common in cancer therapy, and some of them have been associated with the development of porphyria in patients with cancer. However, knowledge of their effects on the haeme metabolic pathway is at present scarce and unclear. So, the present study evaluates the porphyrinogenic ability of nine antineoplastics (both alkylating and non-alkylating). These were tested either alone or in conjunction with 3,5-diethoxycarbonyl-1,4-dihydrocollidine (latent porphyria model) in chick embryos and in mice. The results obtained suggest that the use of cyclophosphamide, azathioprine, 5-fluorouracil, busulphan, procarbazine and hexamethylmelamine be avoided in the treatment of porphyric patients. On the other hand, dacarbazine, chlorambucil and melphalan are non-porphyrinogenic. We also provide evidence showing that neither the presence of the mustard group in the structure of the antineoplastic nor alterations in ferrochelatase or protoporphyrinogen oxidase activities are responsible for the porphyrinogenic ability of cyclophosphamide.

Published

1997

2. Hexamethylmelamine is a potent inducer of deletions in male germ cells of Drosophila melanogaster.

Author

Aguirrezabalaga I, Nivard MJ, Comendador MA, and Vogel EW

Subjects

Animals, Base Sequence, Drosophila melanogaster, Male, Molecular Sequence Data, Mutation, Neoplasms, Second Primary etiology, Spermatozoa drug effects, Spermatozoa ultrastructure, Altretamine toxicity, Antineoplastic Agents, Alkylating toxicity, Gene Deletion, Mutagens toxicity

Abstract

Chemotherapy-related second tumors constitute a matter of concern in cancer treatment. Therefore, it is of great interest to elucidate the mechanisms by which cytostatic drugs exert their mutagenic and/or carcinogenic activity besides the anticancer effect and the possible relationship among them. A useful and informative approach to this problem is the analysis of the mutation spectra induced by these drugs in eukaryotic organisms. Sequence analysis of the mutations induced by hexamethylmelamine, a crosslinking agent extensively used in the treatment of ovarian cancer, in male germ cells of Drosophila was conducted using the v locus as reporter gene. Both intra-locus and multi-locus deletions were induced whereas based changes were almost absent. Thus, it is proposed that deletions are likely to be involved in the generation of second malignancies in hexamethylmelamine-treated patients. It has to be stressed that systems, such as v, capable of efficiently recovering mutations caused by big losses of DNA, should be used for the study of mutational spectra induced by cross-linking agents.

Published

1995

3. The hypermutability conferred by the mus308 mutation of Drosophila is not specific for cross-linking agents.

Author

Aguirrezabalaga I, Sierra LM, and Comendador MA

Subjects

Alkylating Agents toxicity, Altretamine toxicity, Animals, DNA Adducts, DNA Damage, Drosophila melanogaster genetics, Ethylnitrosourea toxicity, Female, Genes, Lethal, Hempa toxicity, Male, Methyl Methanesulfonate toxicity, Models, Genetic, Cross-Linking Reagents toxicity, DNA Repair, Drosophila melanogaster drug effects, Genes, Insect drug effects, Mutagenesis

Abstract

The hypersensitivity of the mus308 mutant of D. melanogaster to cross-linking agents has been suggested to be the consequence of a possible defect of this mutant in DNA cross-link repair. Moreover, the mus308 mutation has been proposed as an animal model for the study of Fanconi's anemia. In order to obtain more information about the function controlled by this locus, we have measured the mutability of the mus308 mutant to several mutagens with different modes of action using the sex-linked recessive lethal test. We show that this mutation confers hypermutability not only to the cross-linking agents tested, hexamethylphosphoramide and hexamethylmelamine, but to the point mutagen N-ethyl-N-nitrosourea as well, whereas the response to methyl methanesulfonate was normal. The results suggest that the mus308 locus is not defective in a repair pathway specific for cross-links but is rather involved in a step of a more general post-replication repair process responsible for the removal of non-excised adducts.

Published

1995

4. Hexamethylmelamine: activity in lymphoma and other tumors.

Author

Macdonald JS

Subjects

Altretamine administration & dosage, Altretamine toxicity, Humans, Altretamine therapeutic use, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Lymphoma drug therapy, Neoplasms drug therapy

Abstract

Hexamethylmelamine, an orally administered substituted melamine, has single agent activity in lymphoma (39% PR + CR), cervical cancer (28% PR), transitional carcinoma of the bladder (27% PR + CR), and Bilharzial bladder cancer (38% PR). Toxicity is mild and reversible and is manifested by myelosuppression, neurotoxicity and gastrointestinal toxicity. The potential role of hexamethylmelamine in combination chemotherapy in the diseases in which it has single agent activity is largely unexplored and should be investigated in clinical trials.

Published

1991

5. Hexamethylmelamine use in the treatment of metastatic breast cancer.

Author

Henderson IC and Shapiro CL

Subjects

Altretamine administration & dosage, Altretamine toxicity, Antineoplastic Agents therapeutic use, Breast Neoplasms pathology, Clinical Trials as Topic, Drug Evaluation, Female, Humans, Neoplasm Metastasis, Altretamine therapeutic use, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Breast Neoplasms drug therapy

Published

1991

6. Hexamethylmelamine: pharmacology and mechanism of action.

Author

Ames MM

Subjects

Altretamine metabolism, Altretamine therapeutic use, Altretamine toxicity, Animals, Drug Evaluation, Drug Evaluation, Preclinical, Drug Screening Assays, Antitumor, Humans, Altretamine pharmacology

Abstract

Several conclusions can be drawn from a review of HMM preclinical and clinical pharmacology data. The drug is extensively metabolized by animals and by man. The drug is well absorbed following oral administration to animals, but oral bioavailability is low due to first pass metabolism. Based on limited human data and more complete animal data, absorption of HMM following oral administration may be quite high in man. We do not yet know the oral bioavailability of HMM in patients, but again based primarily on animal studies, oral bioavailability is most likely low and variable due to extensive first pass metabolism. Systemic exposure to HMM and demethylated metabolites following oral administration varies greatly from patient to patient and is sometimes quite low. Most patients are, however, exposed to a substantial fraction of the administered dose when determined by urinary recovery of the total dose (based on parent drug and metabolites or total radioactivity) or by the total plasma AUC of parent drug and all metabolites. Systemic exposure to HMM following intravenous administration is clearly greater and less variable than following oral administration. An unresolved question is whether the highly variable and often low systemic exposure after oral administration compromise antitumor activity when compared to intravenous administration. A key issue is whether or not one accepts the hypothesis that metabolism is a prerequisite for antitumor activity. The metabolic activation studies do not rule out other mechanisms of HMM antitumor activity. Modest activity of HMM was observed after prolonged exposure to cells which did not metabolize the drug. However, most of the accumulated data are consistent with the metabolic activation hypothesis. Certainly HMM has clinical activity when administered by mouth. If metabolism is required, then exposure to the total dose (parent drug and metabolites) could be of significance even when exposure to HMM is low, since every demethylated metabolite must have come ultimately from the initial HMM demethylation. We do not know whether the initial metabolic reaction (occurring in the liver rather than in the tumor) provides sufficient exposure of tumor to reactive species. Specifically, does the variable HMM plasma AUC seen after oral administration lead to variable delivery of potentially reactive species to tumor (by rapid breakdown and/or further metabolism of MPMM before it leaves the gut and/or liver) or are quantities of MPMM delivered to tumor comparable to those delivered following intravenous administration. The issue of rate of MPMM formation compared to rate of breakdown and ultimate delivery to tumor has been noted by Judson and Rutty.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1991

7. Selecting drug combinations based on total equivalent dose (dose intensity)

Author

Simon R and Korn EL

Subjects

Altretamine administration & dosage, Altretamine toxicity, Carboplatin, Cisplatin administration & dosage, Cisplatin toxicity, Cyclophosphamide administration & dosage, Cyclophosphamide toxicity, Dose-Response Relationship, Drug, Doxorubicin administration & dosage, Doxorubicin toxicity, Drug Screening Assays, Antitumor, Drug Synergism, Female, Humans, Models, Theoretical, Organoplatinum Compounds administration & dosage, Organoplatinum Compounds toxicity, Ovarian Neoplasms drug therapy, Antineoplastic Combined Chemotherapy Protocols administration & dosage

Abstract

We describe a mathematical model for selecting cytotoxic drugs and dosages for a combination regimen based on the antitumor activities of the drugs given as single agents and their organ-specific maximum tolerated doses. The regimen defined maximizes an approximate measure of antitumor effect subject to constraints on combined toxicity. This approach does not assume that the underlying dose-response curve is steep; nor does it assume that maximally dose-intense regimens are clinically appropriate in all situations. Whether the identified regimen is superior to standard treatments should be determined by prospective, randomized clinical trials. Determining which drugs to combine and in what proportions to combine them offers combinatorially huge numbers of possibilities. The method described here offers one approach to identifying combinations worthy of evaluation in prospective trials.

Published

1990

8. Pancreatic beta cell vacuolation in rats after oral administration of hexamethylmelamine.

Author

Molello JA, Barnard SD, and Thompson DJ

Subjects

Administration, Oral, Animals, Blood Glucose, Body Weight drug effects, Female, Islets of Langerhans drug effects, Male, Rats, Rats, Inbred Strains, Vacuoles drug effects, Vacuoles ultrastructure, Altretamine toxicity, Hyperglycemia chemically induced, Islets of Langerhans ultrastructure, Triazines toxicity

Abstract

The effects of hexamethylmelamine (HMM) on morphology and function of the endocrine pancreas were investigated following the induction of a diabetic-like syndrome in a reproduction study in rats. Doses of 0, 20, 40, or 80 mg/kg/day were administered once daily, by gavage, to groups of 10 male and 10 female Sprague-Dawley rats for up to 77 days. Signs of toxicity were observed at all treatment levels and were of such severity at 80 mg/kg/day that this group was terminated after 8 days of treatment. Measurement of serum glucose levels revealed a dose- and time-related hyperglycemia in rats from the 20- and 40-mg/kg/day groups with levels exceeding 700 mg/dl in some rats after 77 days of treatment. Reversal of the hyperglycemia after discontinuing treatment with HMM occurred in some rats receiving 20 mg/kg/day, whereas the effects of higher doses were still present following a 2-month recovery period. Microscopically, there were hydropic degeneration of renal tubular epithelium and vacuolation of pancreatic beta cells. Ultrastructurally, vesiculation of the Golgi-smooth membrane reticular complex and a marked reduction in the number of insulin granules were observed. It appeared that HMM exerted a disruptive effect on the production of insulin at or prior to the level of the Golgi complex. The severity and time course of morphologic changes and hyperglycemia were dependent on dose and duration of treatment.

Published

1984

9. The curative action of hexamethylmelamine on intramuscularly or intracerebrally implanted Yoshida sarcoma.

Author

Osswald H

Subjects

Altretamine metabolism, Altretamine toxicity, Animals, Male, Rats, Rats, Inbred Strains, Altretamine therapeutic use, Sarcoma, Yoshida drug therapy, Triazines therapeutic use

Abstract

Curative effects of hexamethylmelamine (HMM, NSC 13875) against intramuscularly or intracerebrally implanted Yoshida sarcoma depend on the schedules. A twice daily oral administration over a 2-week period showed a significant chemotherapeutic advantage over a single daily administration. The observed curative effect depends on the tumour site and on its mass. The Yoshida sarcoma seems to be one of the most suitable test models for HMM or related derivatives.

Published

1984

10. Central side effects of pentamethylmelamine: biochemical and behavioural studies.

Author

Perego C, Broggini M, Garattini S, D'Incalci M, Achilli G, Lipartiti M, and Ponzio F

Subjects

Altretamine analogs & derivatives, Animals, Biogenic Amines metabolism, Body Temperature drug effects, Brain metabolism, Dopamine metabolism, Dose-Response Relationship, Drug, Female, Mice, Mice, Inbred C57BL, Motor Activity drug effects, Receptors, Dopamine metabolism, Spiperone metabolism, Altretamine toxicity, Brain drug effects, Triazines toxicity

Abstract

The central side effects of pentamethylmelamine (PMM), an antitumoral agent, were studied on brain neurotransmitters from the biochemical and behavioural points of view. PMM causes a dose-related reduction in the body temperature and motility of mice. 100 mg/kg of PMM lowers the levels of noradrenaline (NA) and raises 3-methoxy-4-hydroxyphenylethyleneglycol (MHPG) in the telencephalon. A similar dose increased striatal levels of dopamine (DA) metabolites, homovanillic acid (HVA) and dihydroxyphenylacetic acid (DOPAC), at earlier times (30 min), reducing their levels at 2 hr. These effects disappear at longer times (4 hr). No changes were observed in the levels of 3-methoxytyramine (3-MT), the extraneuronal metabolite of DA. The serotonin metabolite 5-hydroxyindolacetic acid (5HIAA) was almost not affected. PMM and its metabolites do not displace [3H]-spiroperidol from mouse striatal binding sites. These data show that some of the neurological effects induced by PMM are associated with changes in the metabolism and/or release of brain catecholamines but are not mediated by direct action on DA receptors.

Published

1984

11. Effect of particle size distribution on hexamethylmelamine toxicity in rats.

Author

Henry MC, Port CD, Rosen E, and Levine BS

Subjects

Altretamine administration & dosage, Animals, Blood Cell Count, Body Weight drug effects, Depression, Chemical, Dose-Response Relationship, Drug, Intubation, Gastrointestinal, Lethal Dose 50, Leukocyte Count, Male, Mitosis drug effects, Particle Size, Rats, Altretamine toxicity, Triazines toxicity

Abstract

Single oral dose toxicities of six hexamethylmelamine samples with different particle size distributions were evaluated in Osborne-Mendel rats. The calculated LD50 values for the 6 samples were 1706 to 2150 mg/kg )10,236 to 12,900 mg/m2). The two samples with median particle size less than 40 micron were more toxic than the other 4 samples. Among the latter samples, severity of toxic effects was not correlated with particle size. Leukocytes, lymphocytes, platelets and body weight showed dose-related decreases for all samples. Particle size appeared to have a minimal effect on these variables. The drug produced toxic effects on rapidly proliferating tissues: lymphoid, hematopoietic and germinal epithelium. At lethal doses, microscopic lesions were lymphoid tissue hypoplasia, bone marrow hypoplasia with elevated myeloid:erythroid ratios and spermatogenic arrest. The major target organs at nonlethal doses were bone marrow and germ cells, with germinal epithelium showing the most severe lesions.

Published

1979

12. Hexamethylmelamine and pentamethylmelamine: an update.

Author

Hahn DA

Subjects

Altretamine analogs & derivatives, Altretamine pharmacology, Altretamine toxicity, Antineoplastic Agents administration & dosage, Drug Therapy, Combination, Female, Humans, Leukemia drug therapy, Lung Neoplasms drug therapy, Male, Ovarian Neoplasms drug therapy, Prostatic Neoplasms drug therapy, Altretamine therapeutic use, Triazines therapeutic use

Abstract

An updated review of the anticancer agents hexamethylmelamine (HMM) and its water-soluble analog pentamethylmelamine (PMM) is presented. Severe gastrointestinal and hematologic toxicity have limited the use of HMM drug combinations in ovarian cancer. Combinations involving HMM, cyclophosphamide, cisplatin, and doxorubicin in advanced ovarian cancer have resulted in only moderate response rates, with little to no change in median survival of previously treated patients. HMM now is being studied in previously untreated patients with advanced disease, in combination with these agents. In lung cancer, HMM continues to be a part of intensive and other regimens for the treatment of small-cell and non-small-cell carcinoma, although the value of the HMM is yet to be determined. Future trials have been recommended to determine whether HMM has a role in the treatment of endometrial and prostatic carcinomas. Five phase I studies of PMM have demonstrated severe, dose-limiting gastrointestinal and central nervous system toxicities. Thus, this agent may offer little advantage over HMM. Further phase I studies, with different PMM dosage schedules, are necessary before phase II studies can be recommended.

Published

1983

13. Toxicity and antitumor activity of hexamethylmelamine and its N-demethylated metabolites in mice with transplantable tumors.

Author

Lake LM, Grunden EE, and Johnson BM

Subjects

Altretamine metabolism, Animals, Lethal Dose 50, Leukemia L1210 drug therapy, Lung Neoplasms drug therapy, Male, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Neoplasms, Experimental mortality, Sarcoma 180 drug therapy, Structure-Activity Relationship, Altretamine therapeutic use, Altretamine toxicity, Neoplasms, Experimental drug therapy, Triazines therapeutic use, Triazines toxicity

Abstract

N-Demethylated metabolites of the antineoplastic agent hexamethylmelamine were synthesized, and their toxicities and antitumor activities were determined in vivo. Determinations of the lethal dose for 10% of the male C57BL X DBA/2 F1 (hereafter called BD2F1) mice showed hexamethylmelamine toxicity to be decreased by N-demethylation; the metabolites showed a direct relationship between potency (mmoles/kg/day) and number of methyl groups present. In BD2F1 mice bearing Sarcoma 180 or Lewis lung carcinoma, the antitumor activities of the methylmelamines decreased with a reduction in number of methyl groups, but were similar at equitoxic levels. Results were similar in L1210 leukemic mice treated with lethal dose levels of the metabolites for 10% of the mice when mean survival times were measured. The therapeutic equality produced with equitoxic levels, together with the ineffectiveness of melamine, suggested that the presence of a methyl group, rather than the number, was the determining factor in the antitumor activity of the methylmelamines.

Published

1975

14. Phase II trial of combination chemotherapy for pancreatic cancer with 5-fluorouracil, mitomycin C, and hexamethylmelamine.

Author

Bruckner HW, Storch JA, Brown JC, Goldberg J, and Chamberlin K

Subjects

Altretamine toxicity, Drug Administration Schedule, Drug Evaluation, Drug Therapy, Combination, Fluorouracil toxicity, Humans, Mitomycin, Mitomycins toxicity, Altretamine therapeutic use, Antibiotics, Antineoplastic therapeutic use, Fluorouracil therapeutic use, Mitomycins therapeutic use, Pancreatic Neoplasms drug therapy, Triazines therapeutic use

Abstract

A combination consisting of hexamethylmelamine 150 mg/m2 D2-15, mitomycin C 10 mg/m2 D2 and 5-fluorouracil 30 mg/kg/day as a continuous infusion for 5 days, in 4-5 week cycles, underwent phase II trial as primary therapy for 21 patients with regional and metastatic cancer of the pancreas. Median survival from the onset of therapy was 43 weeks. There were 2 complete responses, 4 minor responses and 6 stable diseases for more than 6 months. Nonambulatory patients were among the responders. There was only 1 life-threatening toxicity (thrombocytopenia) and only 33% of patients had clinically silent severe hematological toxicity. The regimen is well tolerated, active and associated with excellent survival. This regimen is suitable for further confirmatory trials.

Published

1983

15. Weak mutagenicity to Salmonella of the formaldehyde-releasing anti-tumour agent hexamethylmelamine.

Author

Ashby J, Callander RD, and Rose FL

Subjects

Biotransformation, Mutagenicity Tests, Salmonella typhimurium drug effects, Salmonella typhimurium genetics, Altretamine toxicity, Mutation drug effects, Triazines toxicity

Abstract

Hexamethylmelamine (HEMLA) is a metabolism-dependent formaldehyde-releasing agent related in structure to hexamethylphosphoramide (HMPA). Both compounds are known to be mutagenic to Drosophila. HMPA, in common with the other formaldehyde-releasing agents studied, is non-mutagenic to Salmonella. The present paper describes the mutagenicity of HEMLA to strain TA100 of Salmonella typhimurium. Activity is dependent upon both the use of a pre-incubation assay protocol and on high concentrations of Aroclor-induced rat liver in the S9 mix. HMPA was inactive under similar conditions of test.

Published

1985

16. Effect of cimetidine and ranitidine on the metabolism and toxicity of hexamethylmelamine.

Author

Hande K, Combs G, Swingle R, Combs GL, and Anthony L

Subjects

Altretamine toxicity, Aminopyrine metabolism, Animals, Carbon Dioxide metabolism, Male, Microsomes, Liver metabolism, Rats, Rats, Inbred Strains, Altretamine metabolism, Cimetidine pharmacology, Microsomes, Liver drug effects, Ranitidine pharmacology, Triazines metabolism

Abstract

In a rat model, doses of 20-120 mg/kg of cimetidine prolonged in a dose-related manner the half-life of hexamethylmelamine by 29%-80%, while doses of 1-25 mg/kg of ranitidine did not. Administration of 120 mg/kg of cimetidine with a single 350-mg/kg dose of hexamethylmelamine increased toxicity from LD30 to LD75 (P = 0.005). When combined with 25 mg/kg of ranitidine, a statistically insignificant (P = 0.16) 15% increase in hexamethylmelamine toxicity was noted. These studies indicate that cimetidine but not ranitidine increases the toxicity of hexamethylmelamine through inhibition of microsomal metabolism.

Published

1986

17. Reproduction and teratology studies on hexamethylmelamine in the rat and rabbit.

Author

Thompson DJ, Dyke IL, and Molello JA

Subjects

Animals, Body Weight drug effects, Female, Fetal Resorption chemically induced, Male, Pregnancy, Rabbits, Rats, Rats, Inbred Strains, Abnormalities, Drug-Induced etiology, Altretamine toxicity, Fertility drug effects, Reproduction drug effects, Triazines toxicity

Abstract

The antineoplastic drug hexamethylmelamine (HMM) was evaluated for effects on reproduction and postnatal development in the rat and on embryonal and fetal development in the rat and rabbit. Daily po treatment of male rats for 62 days with doses of 0, 10, 20, or 40 mg/kg/day resulted in testicular atrophy, reduced fertility, and a possible dominant lethal mutagenic effect at the higher two dose levels. Alterations in morphology and function of the beta cells of the pancreatic islets were observed after treatment of males for more than 28 days with 20 or 40 mg/kg/day. The same dose levels administered to female rats for 14 days prior to breeding and through Day 13 or 20 of gestation had no adverse effects on fertility, but the highest dose was embryocidal and postnatal survival was decreased at both the 20- and 40-mg/kg/day dose levels. Similar effects on postnatal survival were observed when the drug was administered by gavage to rats during the last week of gestation and throughout the lactation period. Treatment of pregnant rats throughout organogenesis (Days 6 to 15) or for 4-day intervals during organogenesis (Days 6 to 9, 9 to 12, or 12 to 15) with po doses ranging from 20 to 80 mg/kg/day resulted in decreased body weight gain and food consumption, an increased resorption rate in dams receiving 80 mg/kg/day on Days 6 to 9, and decreased fetal weights at all dose levels and most treatment intervals. The incidence of minor skeletal defects was increased among litters of HMM-treated groups. Major fetal malformations were limited in number but were considered treatment related. Treatment of pregnant rabbits po on Days 6 to 18 of gestation with doses of 0, 20, 40, or 60 mg/kg/day did not result in an embryocidal or teratogenic effect. Treatment with 60 mg/kg/day did, however, result in decreased kit weights, indicating a mild embryo-fetotoxic effect.

Published

1984

18. Phase I trial of pentamethylmelamine in patients with previously treated malignancies.

Author

Van Echo DA, Chiuten DF, Whitacre M, Aisner J, Lichtenfeld JL, and Wiernik PH

Subjects

Adult, Aged, Altretamine administration & dosage, Altretamine analogs & derivatives, Altretamine toxicity, Anorexia chemically induced, Central Nervous System drug effects, Dose-Response Relationship, Drug, Drug Administration Schedule, Drug Evaluation, Female, Humans, Male, Middle Aged, Nausea chemically induced, Neoplasms pathology, Vomiting chemically induced, Altretamine therapeutic use, Neoplasms drug therapy, Triazines therapeutic use

Abstract

Pentamethylmelamine (PMM), a demethylated soluble analog of hexamethylmelamine, was given to 35 patients with solid tumors in a phase I clinical trial. Thirty patients were given single doses ranging from 80 to 2000 mg/m2 in a 2-hour infusion every 3 weeks. Once a maximum tolerated dose was defined for this schedule, an additional five new patients plus four patients who had already received PMM were treated on a multiple-dose schedule of PMM given three times a week every Monday, Wednesday, and Friday (M-W-F) for 4 weeks. Dose-limiting toxic effects for the single-dose schedule were in the central nervous system and gastrointestinal tract, manifested by nausea (60%), vomiting (49%), somnolence (37%), depression (6%), and headache (6%). Other toxic effects observed on this schedule included anorexia (34%), diarrhea (7%), and diaphoresis (21%). The toxic effects were first observed in mild form at 400 mg/m2/dose and became progressively more severe and prolonged with each dose escalation; they were considered intolerable at the 2000-mg/m2 dose level in all patients treated. The nine patients receiving the multiple-dose schedule were given PMM at a dose of 1000 mg/m2 three times a week (M-W-F). This level produced dose-limited nausea and vomiting in all patients so that no patient completed greater than 3 weeks of treatment on this schedule. One patient developed PMM-related visual hallucinations. PMM produced no hematologic, hepatic, renal, allergic, or acute side effects; no alopecia was observed. Minor tumor regressions of 1 month's duration were seen in two patients, one with pleural mesothelioma and one with a parotid gland tumor. The recommended doses for solid tumor phase II studies are 1500 mg/m2 given as a 2-hour infusion every 3 weeks and 1000 mg/m2 given three times a week (M-W-F), repeated at 3-week intervals.

Published

1980

19. Hexamethylmelamine chemotherapy for disseminated endometrial cancer.

Author

Seski JC, Edwards CL, Copeland LJ, and Gershenson DM

Subjects

Aged, Altretamine toxicity, Ataxia chemically induced, Confusion chemically induced, Female, Humans, Middle Aged, Muscle Hypotonia chemically induced, Nausea chemically induced, Reflex, Stretch drug effects, Vomiting chemically induced, Altretamine therapeutic use, Triazines therapeutic use, Uterine Neoplasms drug therapy

Abstract

To evaluate the role of hexamethylmelamine (HMM) in the treatment of endometrial cancer, 20 women with metastatic or recurrent endometrial carcinoma received HMM orally at a dose of 8 mg/kg/day. Six patients (30%) showed a partial response, with a median duration of response of 3.5 months and a range of 1 to 7 months. Two patients responded to HMM as a second-line agent following previous treatment with nonhormonal chemotherapy. There were no complete responses. The major toxicities noted with HMM therapy were nausea, vomiting, and neurotoxicity. In 6 patients (30%), therapy with HMM was discontinued because of toxicity. Although HMM is active against endometrial cancer when given at a dose of 8 mg/kg/day, it appears to have limited usefulness because toxicity precludes its prolonged administration.

Published

1981

20. [Establishment of hygienic standards for metazin in food products and in the water of reservoirs].

Author

Makarian ASh

Subjects

Altretamine analogs & derivatives, Animals, Dose-Response Relationship, Drug, Lethal Dose 50, Maximum Allowable Concentration, Mice, Pesticide Residues, Rats, Time Factors, Altretamine toxicity, Food Contamination, Herbicides toxicity, Triazines toxicity, Water Pollutants, Water Pollutants, Chemical

Published

1980

21. Mathematical and biostatistical methods for designing and analyzing complex chemical interactions.

Author

Carter WH Jr and Carchman RA

Subjects

Altretamine toxicity, Animals, Cisplatin toxicity, Fluorouracil toxicity, Mice, Mice, Inbred Strains, Models, Chemical, Razoxane, Sister Chromatid Exchange drug effects, Statistics as Topic, Drug-Related Side Effects and Adverse Reactions

Abstract

In this presentation, statistical methods for designing and analyzing experiments evaluating a mixture of drugs/chemicals are discussed. These methods are promising in that they are not limited by the number of interacting agents in the combination. Several examples are given and a discussion of the results follows.

Published

1988

22. Pentamethylmelamine: review of an aqueous analog of hexamethylmelamine.

Author

Foster BJ, Clagett-Carr K, Hoth D, and Leyland-Jones B

Subjects

Altretamine analogs & derivatives, Altretamine metabolism, Altretamine toxicity, Animals, Antineoplastic Agents metabolism, Antineoplastic Agents toxicity, Clinical Trials as Topic, Dogs, Dose-Response Relationship, Drug, Drug Evaluation, Drug Evaluation, Preclinical, Haplorhini, Humans, Kinetics, Mice, Structure-Activity Relationship, Altretamine therapeutic use, Antineoplastic Agents therapeutic use, Neoplasms drug therapy, Triazines therapeutic use

Abstract

The s-triazine derivatives have shown preclinical antitumor activity against several histologic types. The most widely used compound of this class in the clinic, hexamethylmelamine, has been largely restricted to oral use because of its low solubility and lack of stability in solutions suitable for parenteral administration. New analogs were sought which were soluble and stable and retained antitumor activity. Pentamethylmelamine (PMM), the monodemethylated derivative, showed these promising characteristics. Preclinical toxicology studies of PMM in mice, dogs, and monkeys showed toxic manifestations that involved the hematopoietic, lymphatic, renal, male reproductive, gastrointestinal, and nervous systems; these changes were both infusion-rate- and dose-dependent. Clinical phase I trials of PMM were performed using a variety of infusion durations and frequency schedules. The dose-limiting toxic effect common to all of these trials was protracted nausea and vomiting. In addition, some studies reported dose-limiting central nervous system manifestations in the form of agitation, drowsiness, somnolence, and even coma. Mild to moderate hematologic changes were noted. Because of the severity and frequency of the gastrointestinal and central nervous system toxic effects observed in the completed trials, no new clinical trials of PMM sponsored by the National Cancer Institute are planned. However, the interest in finding a clinically useful parenteral triazine continues.

Published

1986

23. Phase II trial of combination chemotherapy of colonic cancer with 5-fluorouracil, mitomycin C, and hexamethylmelamine.

Author

Bruckner HW, Storch JA, Brown JC, Goldberg J, and Chamberlin K

Subjects

Altretamine toxicity, Drug Administration Schedule, Drug Evaluation, Drug Therapy, Combination, Fluorouracil toxicity, Follow-Up Studies, Humans, Mitomycin, Mitomycins toxicity, Altretamine therapeutic use, Antibiotics, Antineoplastic therapeutic use, Colonic Neoplasms drug therapy, Fluorouracil therapeutic use, Mitomycins therapeutic use, Triazines therapeutic use

Abstract

HexMF consists of hexamethylmelamine 150 mg/m2 D2-15, mitomycin C (MMC) 10 mg/m2 D2 and 5-fluorouracil (5-FU) 30 mg/kg/day as a continuous infusion D1-5 in 4-5 week cycles. It was designed as an alternative to treating patients with standard single agents in sequence, thereby preventing the testing of new drugs as part of primary therapy. Median survival was 12+ months for patients with measurable and 18+ months for patients with nonmeasurable colorectal cancer. It was 9+ months from the onset of secondary chemotherapy. Toxicity included severe thrombocytopenia (50%), severe leukopenia (25%), and moderate stomatitis (50%). Only one instance of leukopenia was life-threatening. The MMC and 5-FU infusion skeleton provides an attractive strategy for testing new drugs as primary therapy. HexMF itself has a potentially broad antitumor spectrum and excellent acceptance by patients. It is suitable for additional phase II trials.

Published

1983

24. Phase I study of pentamethylmelamine.

Author

Goldberg RS, Griffin JP, McSherry JW, and Krakoff IH

Subjects

Adult, Altretamine analogs & derivatives, Dose-Response Relationship, Drug, Drug Evaluation, Electroencephalography, Humans, Injections, Intravenous, Leukocyte Count drug effects, Myeloproliferative Disorders chemically induced, Nausea chemically induced, Platelet Count drug effects, Psychoses, Substance-Induced etiology, Vomiting chemically induced, Altretamine toxicity, Neoplasms drug therapy, Triazines toxicity

Abstract

Pentamethylmelamine is a soluble monodemethylated derivative of hexamethylmelamine. Its activity in animal tumors is similar to that of hexamethylmelamine. When given iv at a dose of 1200 mg/m2 to patients with advanced cancer, it produced severe nausea and vomiting, severe psychotropic effects, and EEG changes. When this dose was given for 10 consecutive days, there was marked but reversible myelosuppression. The severe CNS effects which occurred at doses sufficient to produce myelosuppression cast doubt on the potential utility of pentamethylmelamine.

Published

1980

25. Hexamethylmelamine: a critical review of an active drug.

Author

Foster BJ, Harding BJ, Leyland-Jones B, and Hoth D

Subjects

Altretamine metabolism, Altretamine toxicity, Animals, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Drug Evaluation, Humans, Kinetics, Neoplasms drug therapy, Structure-Activity Relationship, Altretamine therapeutic use, Triazines therapeutic use

Abstract

Hexamethylmelamine is an s-triazine that began clinical trials during the 1960s based on its level of antitumor activity in murine tumor models. Phase I studies were performed using an oral formulation given in divided doses for varying numbers of days. The most frequently reported toxicities included nausea, vomiting, abdominal cramps, anorexia, weight loss and malaise. Less frequently reported toxicities were anemia, thrombocytopenia, leucopenia and peripheral neuropathy. Clinical antitumor activity was noted in the phase I studies in a variety of tumor types. Since then a large number of studies have been performed using hexamethylmelamine as a single agent and in a variety of combinations. Unfortunately, almost none of these studies sought to define the utility of this drug relative to other treatments for the diseases in which it showed activity, or to define the contribution of this drug to the activity of any given combination. Thus its role in the treatment of patients with malignancies remains undefined.

Published

1986