Tabloid
Generic Name: thioguanine
Dosage Form: Tablets
CAUTION
Tabloid brand Thioguanine is a
potent drug. It should not be used unless a diagnosis of acute nonlymphocytic
leukemia has been adequately established and the responsible physician is
knowledgeable in assessing response to chemotherapy.
Tabloid Description
Tabloid brand Thioguanine was synthesized and developed
by Hitchings, Elion, and associates at the Wellcome Research Laboratories.
It is one of a large series of purine analogues which interfere with nucleic
acid biosynthesis, and has been found active against selected human neoplastic
diseases.
Thioguanine, known chemically as 2-amino-1,7-dihydro-6H-purine-6-thione, is an analogue of the nucleic
acid constituent guanine, and is closely related structurally and functionally
to PURINETHOL® (mercaptopurine). Its structural formula is:
Tabloid
brand Thioguanine is available in tablets for oral administration. Each scored
tablet contains 40 mg thioguanine and the inactive ingredients gum acacia,
lactose, magnesium stearate, potato starch, and stearic acid.
Tabloid - Clinical Pharmacology
Clinical studies have shown that the absorption of an oral
dose of thioguanine in humans is incomplete and variable, averaging approximately
30% of the administered dose (range: 14% to 46%). Following oral administration
of 35S-6-thioguanine, total plasma radioactivity reached a maximum
at 8 hours and declined slowly thereafter. Parent drug represented only
a very small fraction of the total plasma radioactivity at any time, being
virtually undetectable throughout the period of measurements.
The
oral administration of radiolabeled thioguanine revealed only trace quantities
of parent drug in the urine. However, a methylated metabolite, 2-amino-6-methylthiopurine
(MTG), appeared very early, rose to a maximum 6 to 8 hours after drug
administration, and was still being excreted after 12 to 22 hours. Radiolabeled
sulfate appeared somewhat later than MTG but was the principal metabolite
after 8 hours. Thiouric acid and some unidentified products were found
in the urine in small amounts. Intravenous administration of 35S-6-thioguanine
disclosed a median plasma half-disappearance time of 80 minutes (range:
25 to 240 minutes) when the compound was given in single doses of 65
to 300 mg/m2. Although initial plasma levels of thioguanine
did correlate with the dose level, there was no correlation between the plasma
half-disappearance time and the dose.
Thioguanine is
incorporated into the DNA and the RNA of human bone marrow cells. Studies
with intravenous 35S-6-thioguanine have shown that the amount of
thioguanine incorporated into nucleic acids is more than 100 times higher
after 5 daily doses than after a single dose. With the 5-dose schedule,
from one-half to virtually all of the guanine in the residual DNA was replaced
by thioguanine. Tissue distribution studies of 35S-6-thioguanine
in mice showed only traces of radioactivity in brain after oral administration.
No measurements have been made of thioguanine concentrations in human cerebrospinal
fluid (CSF), but observations on tissue distribution in animals, together
with the lack of CNS penetration by the closely related compound, mercaptopurine,
suggest that thioguanine does not reach therapeutic concentrations in the
CSF.
Monitoring of plasma levels of thioguanine during
therapy is of questionable value. There is technical difficulty in determining
plasma concentrations, which are seldom greater than 1 to 2 mcg/mL after
a therapeutic oral dose. More significantly, thioguanine enters rapidly into
the anabolic and catabolic pathways for purines, and the active intracellular
metabolites have appreciably longer half-lives than the parent drug. The biochemical
effects of a single dose of thioguanine are evident long after the parent
drug has disappeared from plasma. Because of this rapid metabolism of thioguanine
to active intracellular derivatives, hemodialysis would not be expected to
appreciably reduce toxicity of the drug.
Thioguanine
competes with hypoxanthine and guanine for the enzyme hypoxanthine-guanine
phosphoribosyltransferase (HGPRTase) and is itself converted to 6-thioguanylic
acid (TGMP). This nucleotide reaches high intracellular concentrations at
therapeutic doses. TGMP interferes at several points with the synthesis of
guanine nucleotides. It inhibits de novopurine
biosynthesis by pseudo-feedback inhibition of glutamine-5-phosphoribosylpyrophosphate
amidotransferase—the first enzyme unique to the de novo pathway for
purine ribonucleotide synthesis. TGMP also inhibits the conversion of inosinic
acid (IMP) to xanthylic acid (XMP) by competition for the enzyme IMP dehydrogenase.
At one time TGMP was felt to be a significant inhibitor of ATP:GMP phosphotransferase
(guanylate kinase), but recent results have shown this not to be so.
Thioguanylic
acid is further converted to the di- and tri-phosphates, thioguanosine diphosphate
(TGDP) and thioguanosine triphosphate (TGTP) (as well as their 2′-deoxyribosyl
analogues) by the same enzymes which metabolize guanine nucleotides. Thioguanine
nucleotides are incorporated into both the RNA and the DNA by phosphodiester
linkages and it has been argued that incorporation of such fraudulent bases
contributes to the cytotoxicity of thioguanine.
Thus,
thioguanine has multiple metabolic effects and at present it is not possible
to designate one major site of action. Its tumor inhibitory properties may
be due to one or more of its effects on (a) feedback inhibition of de novo
purine synthesis; (b) inhibition of purine nucleotide interconversions; or
(c) incorporation into the DNA and the RNA. The net consequence of its actions
is a sequential blockade of the synthesis and utilization of the purine nucleotides.
The
catabolism of thioguanine and its metabolites is complex and shows significant
differences between humans and the mouse. In both humans and mice, after oral
administration of 35S-6-thioguanine, urine contains virtually no
detectable intact thioguanine. While deamination and subsequent oxidation
to thiouric acid occurs only to a small extent in humans, it is the main pathway
in mice. The product of deamination by guanase, 6-thioxanthine is inactive,
having negligible antitumor activity. This pathway of thioguanine inactivation
is not dependent on the action of xanthine oxidase, and an inhibitor of that
enzyme (such as allopurinol) will not block the detoxification of thioguanine
even though the inactive 6-thioxanthine is normally further oxidized by xanthine
oxidase to thiouric acid before it is eliminated. In humans, methylation of
thioguanine is much more extensive than in the mouse. The product of methylation,
2-amino-6-methylthiopurine, is also substantially less active and less toxic
than thioguanine and its formation is likewise unaffected by the presence
of allopurinol. Appreciable amounts of inorganic sulfate are also found in
both murine and human urine, presumably arising from further metabolism of
the methylated derivatives.
In some animal tumors,
resistance to the effect of thioguanine correlates with the loss of HGPRTase
activity and the resulting inability to convert thioguanine to thioguanylic
acid. However, other resistance mechanisms, such as increased catabolism of
TGMP by a nonspecific phosphatase, may be operative. Although not invariable,
it is usual to find cross-resistance between thioguanine and its close analogue,
PURINETHOL (mercaptopurine).
Indications and Usage for Tabloid
a) Acute Nonlymphocytic Leukemias
Tabloid brand Thioguanine is indicated for remission induction
and remission consolidation treatment of acute nonlymphocytic leukemias. However,
it is not recommended for use during maintenance therapy or similar long term
continuous treatments due to the high risk of liver toxicity (see WARNINGS
and ADVERSE REACTIONS).
The response to this agent
depends upon the age of the patient (younger patients faring better than older)
and whether thioguanine is used in previously treated or previously untreated
patients. Reliance upon thioguanine alone is seldom justified for initial
remission induction of acute nonlymphocytic leukemias because combination
chemotherapy including thioguanine results in more frequent remission induction
and longer duration of remission than thioguanine alone.
b) Other Neoplasms
Tabloid brand Thioguanine is not effective in chronic lymphocytic
leukemia, Hodgkin’s lymphoma, multiple myeloma, or solid tumors. Although
thioguanine is one of several agents with activity in the treatment of the
chronic phase of chronic myelogenous leukemia, more objective responses are
observed with MYLERAN® (busulfan), and therefore busulfan
is usually regarded as the preferred drug.
Contraindications
Thioguanine should not be used in patients whose disease
has demonstrated prior resistance to this drug. In animals and humans, there
is usually complete cross-resistance between PURINETHOL (mercaptopurine) and
Tabloid brand Thioguanine.
Warnings
SINCE DRUGS USED IN CANCER CHEMOTHERAPY ARE POTENTIALLY
HAZARDOUS, IT IS RECOMMENDED THAT ONLY PHYSICIANS EXPERIENCED WITH THE RISKS
OF THIOGUANINE AND KNOWLEDGEABLE IN THE NATURAL HISTORY OF ACUTE NONLYMPHOCYTIC
LEUKEMIAS ADMINISTER THIS DRUG.
THIOGUANINE IS NOT
RECOMMENDED FOR MAINTENANCE THERAPY OR SIMILAR LONG TERM CONTINUOUS TREATMENTS
DUE TO THE HIGH RISK OF LIVER TOXICITY ASSOCIATED WITH VASCULAR ENDOTHELIAL
DAMAGE (see DOSAGE AND ADMINISTRATION and ADVERSE REACTIONS). This liver toxicity
has been observed in a high proportion of children receiving thioguanine as
part of maintenance therapy for acute lymphoblastic leukemia and in other
conditions associated with continuous use of thioguanine. This liver toxicity
is particularly prevalent in males. Liver toxicity usually presents as the
clinical syndrome of hepatic veno-occlusive disease (hyperbilirubinemia, tender
hepatomegaly, weight gain due to fluid retention, and ascites) or with signs
of portal hypertension (splenomegaly, thrombocytopenia, and oesophageal varices).
Histopathological features associated with this toxicity include hepatoportal
sclerosis, nodular regenerative hyperplasia, peliosis hepatitis, and periportal
fibrosis.
Thioguanine therapy should be discontinued
in patients with evidence of liver toxicity as reversal of signs and symptoms
of liver toxicity have been reported upon withdrawal.
Patients
must be carefully monitored (see PRECAUTIONS, Laboratory Tests). Early indications
of liver toxicity are signs associated with portal hypertension such as thrombocytopenia
out of proportion with neutropenia and splenomegaly. Elevations of liver enzymes
have also been reported in association with liver toxicity but do not always
occur.
The most consistent, dose-related toxicity is
bone marrow suppression. This may be manifested by anemia, leukopenia, thrombocytopenia,
or any combination of these. Any one of these findings may also reflect progression
of the underlying disease. Since thioguanine may have a delayed effect, it
is important to withdraw the medication temporarily at the first sign of an
abnormally large fall in any of the formed elements of the blood.
There
are individuals with an inherited deficiency of the enzyme thiopurine methyltransferase
(TPMT) who may be unusually sensitive to the myelosuppressive effects of thioguanine
and prone to developing rapid bone marrow suppression following the initiation
of treatment. Substantial dosage reductions may be required to avoid the development
of life-threatening bone marrow suppression in these patients. Prescribers
should be aware that some laboratories offer testing for TPMT deficiency.
Since bone marrow suppression may be associated with factors other than TPMT
deficiency, TPMT testing may not identify all patients at risk for severe
toxicity. Therefore, close monitoring of clinical and hematologic parameters
is important. Bone marrow suppression could be exacerbated by coadministration
with drugs that inhibit TPMT, such as olsalazine, mesalazine, or sulphasalazine.
It
is recommended that evaluation of the hemoglobin concentration or hematocrit,
total white blood cell count and differential count, and quantitative platelet
count be obtained frequently while the patient is on thioguanine therapy.
In cases where the cause of fluctuations in the formed elements in the peripheral
blood is obscure, bone marrow examination may be useful for the evaluation
of marrow status. The decision to increase, decrease, continue, or discontinue
a given dosage of thioguanine must be based not only on the absolute hematologic
values, but also upon the rapidity with which changes are occurring. In many
instances, particularly during the induction phase of acute leukemia, complete
blood counts will need to be done more frequently in order to evaluate the
effect of the therapy. The dosage of thioguanine may need to be reduced when
this agent is combined with other drugs whose primary toxicity is myelosuppression.
Myelosuppression
is often unavoidable during the induction phase of adult acute nonlymphocytic
leukemias if remission induction is to be successful. Whether or not this
demands modification or cessation of dosage depends both upon the response
of the underlying disease and a careful consideration of supportive facilities
(granulocyte and platelet transfusions) which may be available. Life-threatening
infections and bleeding have been observed as consequences of thioguanine-induced
granulocytopenia and thrombocytopenia.
The effect of
thioguanine on the immunocompetence of patients is unknown.
Pregnancy
Pregnancy Category
D. Drugs such as thioguanine are potential mutagens and teratogens. Thioguanine
may cause fetal harm when administered to a pregnant woman. Thioguanine has
been shown to be teratogenic in rats when given in doses 5 times the
human dose. When given to the rat on the 4th and 5th days of gestation, 13%
of surviving placentas did not contain fetuses, and 19% of offspring were
malformed or stunted. The malformations noted included generalized edema,
cranial defects, and general skeletal hypoplasia, hydrocephalus, ventral hernia,
situs inversus, and incomplete development of the limbs. There are no adequate
and well-controlled studies in pregnant women. If this drug is used during
pregnancy, or if the patient becomes pregnant while taking the drug, the patient
should be apprised of the potential hazard to the fetus. Women of childbearing
potential should be advised to avoid becoming pregnant.
Precautions
General
Although the primary toxicity of thioguanine is myelosuppression,
other toxicities have occasionally been observed, particularly when thioguanine
is used in combination with other cancer chemotherapeutic agents.
A
few cases of jaundice have been reported in patients with leukemia receiving
thioguanine. Among these were 2 adult male patients and 4 pediatric
patients with acute myelogenous leukemia and an adult male with acute lymphocytic
leukemia who developed hepatic veno-occlusive disease while receiving chemotherapy
for their leukemia. Six patients had received cytarabine prior to treatment
with thioguanine, and some were receiving other chemotherapy in addition to
thioguanine when they became symptomatic. While hepatic veno-occlusive disease
has not been reported in patients treated with thioguanine alone, it is recommended
that thioguanine be withheld if there is evidence of toxic hepatitis or biliary
stasis, and that appropriate clinical and laboratory investigations be initiated
to establish the etiology of the hepatic dysfunction. Deterioration in liver
function studies during thioguanine therapy should prompt discontinuation
of treatment and a search for an explanation of the hepatotoxicity.
Administration
of live vaccines to immunocompromised patients should be avoided.
Information for Patients
Patients should be informed that the major toxicities of
thioguanine are related to myelosuppression, hepatotoxicity, and gastrointestinal
toxicity. Patients should never be allowed to take the drug without medical
supervision and should be advised to consult their physician if they experience
fever, sore throat, jaundice, nausea, vomiting, signs of local infection,
bleeding from any site, or symptoms suggestive of anemia. Women of childbearing
potential should be advised to avoid becoming pregnant.
Laboratory Tests
Prescribers should be aware that some laboratories offer
testing for TPMT deficiency (see WARNINGS).
It is
advisable to monitor liver function tests (serum transaminases, alkaline phosphatase,
bilirubin) at weekly intervals when first beginning therapy and at monthly
intervals thereafter. It may be advisable to perform liver function tests
more frequently in patients with known pre-existing liver disease or in patients
who are receiving thioguanine and other hepatotoxic drugs. Patients should
be instructed to discontinue thioguanine immediately if clinical jaundice
is detected (see WARNINGS).
Drug Interactions
There is usually complete cross-resistance between PURINETHOL
(mercaptopurine) and Tabloid brand Thioguanine.
As
there is in vitro evidence that aminosalicylate derivatives (e.g., olsalazine,
mesalazine, or sulphasalazine) inhibit the TPMT enzyme, they should be administered
with caution to patients receiving concurrent thioguanine therapy (see WARNINGS).
Carcinogenesis, Mutagenesis, Impairment of Fertility
In view of its action on cellular DNA, thioguanine is potentially
mutagenic and carcinogenic, and consideration should be given to the theoretical
risk of carcinogenesis when thioguanine is administered (see WARNINGS).
Pregnancy
Teratogenic Effects
Pregnancy Category D. See WARNINGS section.
Nursing Mothers
It is not known whether this drug is excreted in human milk.
Because of the potential for tumorigenicity shown for thioguanine, a decision
should be made whether to discontinue nursing or to discontinue the drug,
taking into account the importance of the drug to the mother.
Pediatric Use
See DOSAGE AND ADMINISTRATION section.
Geriatric Use
Clinical studies of thioguanine did not include sufficient
numbers of subjects aged 65 and over to determine whether they respond differently
from younger subjects. Other reported clinical experience has not identified
differences in responses between the elderly and younger patients. In general,dose selection for an elderly patient should be cautious, usually starting
at the low end of the dosing range, reflecting the greater frequency of decreased
hepatic, renal, or cardiac function, and of concomitant disease or other drug
therapy.
Adverse Reactions
The most frequent adverse
reaction to thioguanine is myelosuppression. The induction of complete remission
of acute myelogenous leukemia usually requires combination chemotherapy in
dosages which produce marrow hypoplasia. Since consolidation and maintenance
of remission are also effected by multiple-drug regimens whose component agents
cause myelosuppression, pancytopenia is observed in nearly all patients. Dosages
and schedules must be adjusted to prevent life-threatening cytopenias whenever
these adverse reactions are observed.
Hyperuricemia
frequently occurs in patients receiving thioguanine as a consequence of rapid
cell lysis accompanying the antineoplastic effect. Adverse effects can be
minimized by increased hydration, urine alkalinization, and the prophylactic
administration of a xanthine oxidase inhibitor such as ZYLOPRIM® (allopurinol).
Unlike PURINETHOL (mercaptopurine) and IMURAN® (azathioprine),
thioguanine may be continued in the usual dosage when allopurinol is used
conjointly to inhibit uric acid formation.
Less frequent
adverse reactions include nausea, vomiting, anorexia, and stomatitis. Intestinal
necrosis and perforation have been reported in patients who received multiple-drug
chemotherapy including thioguanine.
Hepatic Effects
Liver toxicity associated with vascular endothelial damage
has been reported when thioguanine is used in maintenance or similar long
term continuous therapy which is not recommended (see WARNINGS and DOSAGE
AND ADMINISTRATION). This usually presents as the clinical syndrome of hepatic
veno-occlusive disease (hyperbilirubinemia, tender hepatomegaly, weight gain
due to fluid retention, and ascites) or signs and symptoms of portal hypertension
(splenomegaly, thrombocytopenia, and esophageal varices). Elevation of liver
transaminases, alkaline phosphatase, and gamma glutamyl transferase and jaundice
may also occur. Histopathological features associated with this toxicity include
hepatoportal sclerosis, nodular regenerative hyperplasia, peliosis hepatitis,
and periportal fibrosis.
Liver toxicity during short
term cyclical therapy presents as veno-occlusive disease. Reversal of signs
and symptoms of this liver toxicity has been reported upon withdrawal of short
term or long term continuous therapy.
Centrilobular
hepatic necrosis has been reported in a few cases; however, the reports are
confounded by the use of high doses of thioguanine, other chemotherapeutic
agents, and oral contraceptives and chronic alcohol abuse.
Overdosage
Signs and symptoms of overdosage may be immediate, such
as nausea, vomiting, malaise, hypotension, and diaphoresis; or delayed, such
as myelosuppression and azotemia. It is not known whether thioguanine is dialyzable.
Hemodialysis is thought to be of marginal use due to the rapid intracellular
incorporation of thioguanine into active metabolites with long persistence.
The oral LD50 of thioguanine was determined to be 823 mg/kg ± 50.73 mg/kg
and 740 mg/kg ± 45.24 mg/kg for male and female rats,
respectively. Symptoms of overdosage may occur after a single dose of as little
as 2.0 to 3.0 mg/kg thioguanine. As much as 35 mg/kg has been given
in a single oral dose with reversible myelosuppression observed. There is
no known pharmacologic antagonist of thioguanine. The drug should be discontinued
immediately if unintended toxicity occurs during treatment. Severe hematologic
toxicity may require supportive therapy with platelet transfusions for bleeding,
and granulocyte transfusions and antibiotics if sepsis is documented. If a
patient is seen immediately following an accidental overdosage of the drug,
it may be useful to induce emesis.
Tabloid Dosage and Administration
Tabloid brand Thioguanine
is administered orally. The dosage which will be tolerated and effective varies
according to the stage and type of neoplastic process being treated. Because
the usual therapies for adult and pediatric acute nonlymphocytic leukemias
involve the use of thioguanine with other agents in combination, physicians
responsible for administering these therapies should be experienced in the
use of cancer chemotherapy and in the chosen protocol.
There
are individuals with an inherited deficiency of the enzyme thiopurine methyltransferase
(TPMT) who may be unusually sensitive to the myelosuppressive effects of thioguanine
and prone to developing rapid bone marrow suppression following the initiation
of treatment. Substantial dosage reductions may be required to avoid the development
of life-threatening bone marrow suppression in these patients (see WARNINGS).
Prescribers should be aware that some laboratories offer testing for TPMT
deficiency.
Ninety-six (59%) of 163 pediatric patients
with previously untreated acute nonlymphocytic leukemia obtained complete
remission with a multiple-drug protocol including thioguanine, prednisone,
cytarabine, cyclophosphamide, and vincristine. Remission was maintained with
daily thioguanine, 4-day pulses of cytarabine and cyclophosphamide, and a
single dose of vincristine every 28 days. The median duration of remission
was 11.5 months.
Fifty-three percent of previously
untreated adults with acute nonlymphocytic leukemias attained remission following
use of the combination of thioguanine and cytarabine according to a protocol
developed at The Memorial Sloan-Kettering Cancer Center. A median duration
of remission of 8.8 months was achieved with the multiple-drug maintenance
regimen which included thioguanine.
On those occasions
when single-agent chemotherapy with thioguanine may be appropriate, the usual
initial dosage for pediatric patients and adults is approximately 2 mg/kg
of body weight per day. If, after 4 weeks on this dosage, there is no
clinical improvement and no leukocyte or platelet depression, the dosage may
be cautiously increased to 3 mg/kg/day. The total daily dose may be given
at one time.
The dosage of thioguanine used does not
depend on whether or not the patient is receiving ZYLOPRIM (allopurinol); this is in contradistinction to the dosage reduction which
is mandatory when PURINETHOL (mercaptopurine) or IMURAN (azathioprine) is
given simultaneously with allopurinol.
Procedures
for proper handling and disposal of anticancer drugs should be considered.
Several guidelines on this subject have been published.1-8
There
is no general agreement that all of the procedures recommended in the guidelines
are necessary or appropriate.
How is Tabloid Supplied
Greenish-yellow, scored
tablets containing 40 mg thioguanine, imprinted with “WELLCOME”
and “U3B” on each tablet; in bottles of 25 (NDC 0173-0880-25).
Store at 15° to 25°C (59° to 77°F) in
a dry place.
REFERENCES
- ONS Clinical Practice Committee. Cancer Chemotherapy Guidelines and
Recommendations for Practice. Pittsburgh, PA: Oncology Nursing Society; 1999:32-41.
- Recommendations for the safe handling of parenteral antineoplastic drugs.
Washington, DC: Division of Safety, Clinical Center Pharmacy Department and
Cancer Nursing Services, National Institutes of Health and Human Services,
1992, US Dept of Health and Human Services, Public Health Service publication
NIH 92-2621.
- AMA Council on Scientific Affairs. Guidelines for handling parenteral
antineoplastics. JAMA. 1985;253:1590-1591.
- National Study Commission on Cytotoxic Exposure. Recommendations for
handling cytotoxic agents. 1987. Available from Louis P. Jeffrey, Chairman,
National Study Commission on Cytotoxic Exposure. Massachusetts College of
Pharmacy and Allied Health Sciences, 179 Longwood Avenue, Boston, MA 02115.
- Clinical Oncological Society of Australia. Guidelines and recommendations
for safe handling of antineoplastic agents. Med
J Australia. 1983;1:426-428.
- Jones RB, Frank R, Mass T. Safe handling of chemotherapeutic agents:
a report from the Mount Sinai Medical Center. CA-A
Cancer J for Clin. 1983;33:258-263.
- American Society of Hospital Pharmacists. ASHP technical assistance
bulletin on handling cytotoxic and hazardous drugs. Am
J Hosp Pharm. 1990;47:1033-1049.
- Controlling Occupational Exposure to Hazardous Drugs. (OSHA Work-Practice
Guidelines.) Am J Health-Syst Pharm. 1996;53:1669-1685.
Manufactured
by
DSM Pharmaceuticals, Inc.
Greenville,
NC 27834
for GlaxoSmithKline
Research
Triangle Park, NC 27709
©2004, GlaxoSmithKline.
All rights reserved.
December 2004 RL-2154
Revised: 04/2006
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