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Query: UMLS:C0019829 (
Hodgkin's disease
)
30,247
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A randomized study of patients with advanced
Hodgkin's disease
was designed to determine whether the improved therapeutic effectiveness of combination chemotherapy was due to the use of a combination of drugs or might be achieved with a single agent if given as intensively and for as long a period. A combination of nitrogen mustard, vincristine, procarbazine, and prednisone (MOPP) was compared with nitrogen mustard (
HN2
) alone. Treatment with both regimens was given to tolerance on cylic basis and was continued for six cycles of treatment. Sixty-one evaluable patients were treated with MOPP and 47 with
HN2
. The complete remission rate of 47.5% with MOPP was significantly better than the 12.8% with
HN2
(p less than .05). Complete remission lasted a median of 15 months after MOPP and 12 months after
HN2
. The survival of patients initially treated with MOPP was significantly better than that of those initially treated with
HN2
.
...
PMID:A comparison of nitrogen mustard, vincristine, procarbazine, and prednisone (MOPP) vs. nitrogen mustard in advanced Hodgkin's disease. 117 25
Complete responses lasting from 4 to 14 years were documented in 65 of 331 (20%) patients with cutaneous T cell lymphoma treated with topical mechlorethamine (
HN2
) between 1968 and 1982. Such long-lasting remissions occurred most often, but not invariably, in patients with patch or plaque phase mycosis fungoides without palpable lymphadenopathy (stage Ia or Ib). The likelihood of a continuous remission was enhanced by initiation of treatment before an unequivocal pathologic diagnosis. Despite the long-lasting responses in these patients, however, relapses have been documented in 11 (17%) of these patients, and all relapses occurred within 8 years of discontinuing maintenance topical chemotherapy. Thus, in our experience, a continuous remission lasting 8 or more years provides evidence that cutaneous T cell lymphoma can be eradicated by aggressive topical chemotherapy. This circumstance was observed in 35 patients, representing a cure rate of at least 11% overall. In addition, when compared with the general population of the United States, patients who received topical
HN2
were at an 8.6-fold and a 1.8-fold increased risk for the development of squamous cell carcinoma and enhanced for
Hodgkin's disease
and colon cancer but not for systemic cancers known to be induced by systemic administration of alkylating drugs. These results compare favorably with experiences with topical
HN2
chemotherapy at other centers but raise questions about the risks associated with long-term administration for maintenance of remissions.
...
PMID:Long-term efficacy, curative potential, and carcinogenicity of topical mechlorethamine chemotherapy in cutaneous T cell lymphoma. 253 48
Trisethylene-imino-s-triazine (triethylene melamine or TEM) produced minimal effects in inhibiting transplantable lymphoma and mammary adenocarcinoma in mice. In strain A mice, injection of the compound induced pulmonary tumors.TEM was tried on 32 patients with neoplastic disease, including nine patients with
Hodgkin's disease
and five with lymphosarcoma and lymphatic leukemia. The therapeutic and toxic effects were similar to those observed with nitrogen mustard (
HN2
). Satisfactory remissions of up to three months were observed in
Hodgkin's disease
and lymphosarcoma following parenteral administration of TEM. It is the authors' impression that the remissions obtained with TEM were not as complete and did not last as long as those obtained with
HN2
.TEM is effective by the oral route as well as parenterally, and produces much less emetic reaction than
HN2
. On the other hand, the chemotherapeutic range is narrower than that of
HN2
. Patients who do not respond to
HN2
show no response to TEM.TEM is a drug of some clinical usefulness in the same conditions and with the same general limitations and toxic effects as
HN2
. The ease of administration of TEM increases its hazards, and close clinical and hematologic observations are essential on patients receiving the agent.
...
PMID:Trisethylene-imino-s-triazine (triethylene melamine or TEM) in the treatment of neoplastic diseases. 1484 18
Alkylating agents are used in anti-tumor chemotherapy because they bind covalently to DNA and generate adducts that may lead to cell death. Bifunctional (
HN2
) and monofunctional (HN1) nitrogen are two such agents, and
HN2
was the first drug successfully employed in anti-leukemia chemotherapy. Currently,
HN2
is used either alone or combined with other drugs to treat
Hodgkin's disease
. It is well known that several crosslinking agents require metabolic activation via reactive oxygen species (ROS) to exert their lethal effects. The objective of this work was therefore to determine whether the abovementioned mustards would also require metabolic activation to exert lethal action against Escherichia coli. For this purpose, we measured survival following exposure to
HN2
in E. coli strains that were deficient in nucleotide excision repair (uvrA NER mutant), base excision repair (xthA nfo nth fpg BER mutant) or superoxide dismutase (sodAB mutant) activity. We also performed the same experiments in cells pretreated with an iron chelator (2,2'-dipyridyl, DIP). The NER and BER mutants were only sensitive to
HN2
treatment (survival rates similar to those of the wild-type were achieved with 5-fold lower
HN2
doses). However, wild-type and sodAB strains were not sensitive to treatment with
HN2
. In all tested strains, survival dropped by 2.5-fold following pretreatment with DIP compared to treatment with
HN2
alone. Furthermore, DIP treatment increased ROS generation in both wild type and sodAB-deficient strains. Based on these data and on the survival of the SOD-deficient strain, we suggest that the increased production of ROS caused by Fe(2+) chelation may potentiate the lethal effects of
HN2
but not HN1. This potentiation may arise as a consequence of enhancement in the number of or modification of the type of lesions formed. No sensitization was observed for the non-crosslinkable
HN2
analog, HN1.
...
PMID:Bipyridine (2,2'-dipyridyl) potentiates Escherichia coli lethality induced by nitrogen mustard mechlorethamine. 2463 11
