Source:http://www4.wiwiss.fu-berlin.de/dailymed/resource/drugs/81
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HYDREA (Capsule)
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To minimize the risk of dermal exposure, always wear impervious
gloves when handling bottles containing HYDREA capsules. This includes all
handling activities in clinical settings, pharmacies, storerooms, and home
healthcare settings, including during unpacking and inspection, transport
within a facility, and dose preparation and administration. Procedures for proper handling and disposal of antineoplastic drugs
should be considered. Several guidelines on this subject have been published.There
is no general agreement that all of the procedures recommended in the guidelines
are necessary or appropriate. Because of the rarity of melanoma, resistant chronic myelocytic
leukemia, carcinoma of the ovary, and carcinomas of the head and neck in pediatric
patients, dosage regimens have not been established. All dosage should be based on the patient's actual or ideal weight,
whichever is less. Concurrent use of HYDREA with other myelosuppressive agents
may require adjustment of dosages.<br/>Solid Tumors:<br/>Intermittent Therapy: 80 mg/kg administered orally as a single dose every third day<br/>Continuous Therapy: 20 to 30 mg/kg administered orally as a single dose daily<br/>Concomitant Therapy with Irradiation: Carcinoma of the head and neck���80 mg/kg
administered orally as a single dose every third day Administration of hydroxyurea should begin at least seven days
before initiation of irradiation and continued during radiotherapy as well
as indefinitely afterwards provided that the patient may be kept under adequate
observation and evidences no unusual or severe reactions.<br/>Resistant Chronic Myelocytic Leukemia: Until the intermittent therapy regimen has been evaluated, CONTINUOUS
therapy (20 to 30 mg/kg administered orally as a single dose daily)
is recommended. An adequate trial period for determining the antineoplastic effectivenessof hydroxyurea is six weeks of therapy. When there is regression in tumor
size or arrest in tumor growth, therapy should be continued indefinitely.
Therapy should be interrupted if the white blood cell count drops below 2500/mm,
or the platelet count below 100,000/mm. In these
cases, the counts should be reevaluated after three days, and therapy resumed
when the counts return to acceptable levels. Since the hematopoietic rebound
is prompt, it is usually necessary to omit only a few doses. If prompt rebound
has not occurred during combined HYDREA and irradiation therapy, irradiation
may also be interrupted. However, the need for postponement of irradiation
has been rare; radiotherapy has usually been continued using the recommended
dosage and technique. Severe anemia, if it occurs, should be corrected without
interrupting hydroxyurea therapy. Because hematopoiesis may be compromised
by extensive irradiation or by other antineoplastic agents, it is recommended
that hydroxyurea be administered cautiously to patients who have recently
received extensive radiation therapy or chemotherapy with other cytotoxic
drugs. Pain or discomfort from inflammation of the mucous membranes at
the irradiated site (mucositis) is usually controlled by measures such as
topical anesthetics and orally administered analgesics. If the reaction is
severe, hydroxyurea therapy may be temporarily interrupted; if it is extremely
severe, irradiation dosage may, in addition, be temporarily postponed. However,
it has rarely been necessary to terminate these therapies. Severe gastric distress, such as nausea, vomiting, and anorexia,
resulting from combined therapy may usually be controlled by temporary interruption
of hydroxyurea administration.<br/>Renal Insufficiency: As renal excretion is a pathway of elimination, consideration should
be given to decreasing the dosage of HYDREA in patients with renal impairment.
(See PRECAUTIONS and CLINICAL
PHARMACOLOGY.) Close monitoring of hematologic parameters is
advised in these patients.<br/>Hepatic Insufficiency: There are no data that support specific guidance for dosage adjustment
in patients with hepatic impairment. Close monitoring of hematologic parameters
is advised in these patients.
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HYDREA (hydroxyurea capsules,
USP) is an antineoplastic agent available for oral use as capsules providing
500 mg hydroxyurea. Inactive ingredients: citric acid, colorants (D&C
Yellow No. 10, FD&C Blue No. 1, FD&C Red 40, and D&C Red 28),
gelatin, lactose, magnesium stearate, sodium phosphate, and titanium dioxide. Hydroxyurea occurs as an essentially tasteless, white crystalline
powder. Its structural formula is:
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Mechanism of Action: The precise mechanism by which hydroxyurea produces its antineoplastic
effects cannot, at present, be described. However, the reports of various
studies in tissue culture in rats and humans lend support to the hypothesis
that hydroxyurea causes an immediate inhibition of DNA synthesis by acting
as a ribonucleotide reductase inhibitor, without interfering with the synthesis
of ribonucleic acid or of protein. This hypothesis explains why, under certain
conditions, hydroxyurea may induce teratogenic effects. Three mechanisms of action have been postulated for the increased
effectiveness of concomitant use of hydroxyurea therapy with irradiation on
squamous cell (epidermoid) carcinomas of the head and neck. In vitro studies
utilizing Chinese hamster cells suggest that hydroxyurea (1) is lethal to
normally radioresistant S-stage cells, and (2) holds other cells of the cell
cycle in the G1 or pre-DNA synthesis stage where they are most susceptible
to the effects of irradiation. The third mechanism of action has been theorized
on the basis of in vitro studies of HeLa cells: it appears
that hydroxyurea, by inhibition of DNA synthesis, hinders the normal repair
process of cells damaged but not killed by irradiation, thereby decreasing
their survival rate; RNA and protein syntheses have shown no alteration.<br/>Pharmacokinetics:<br/>Absorption: Hydroxyurea is readily absorbed after oral administration. Peak
plasma levels are reached in 1 to 4 hours after an oral dose. With increasing
doses, disproportionately greater mean peak plasma concentrations and AUCs
are observed. There are no data on the effect of food on the absorption of hydroxyurea.<br/>Distribution: Hydroxyurea distributes rapidly and widely in the body with an
estimated volume of distribution approximating total body water. Plasma to ascites fluid ratios range from 2:1 to 7.5:1. Hydroxyurea
concentrates in leukocytes and erythrocytes.<br/>Metabolism: Up to 60% of an oral dose undergoes conversion through metabolic
pathways that are not fully characterized. One pathway is probably saturable
hepatic metabolism. Another minor pathway may be degradation by urease found
in intestinal bacteria. Acetohydroxamic acid was found in the serum of three
leukemic patients receiving hydroxyurea and may be formed from hydroxylamine
resulting from action of urease on hydroxyurea.<br/>Excretion: Excretion of hydroxyurea in humans is likely a linear first-order
renal process.<br/>Special Populations:<br/>Geriatric, Gender, Race: No information is available regarding pharmacokinetic differences
due to age, gender, or race.<br/>Pediatric: No pharmacokinetic data are available in pediatric patients treated
with hydroxyurea.<br/>Renal Insufficiency: As renal excretion is a pathway of elimination, consideration should
be given to decreasing the dosage of hydroxyurea in patients with renal impairment.
In adult patients with sickle cell disease, an open-label, non-randomized,
single-dose, multicenter study was conducted to assess the influence of renal
function on the pharmacokinetics of hydroxyurea. Patients in the study with
normal renal function (creatinine clearance [CrCl]>80 mL/min), mild (CrCl
50���80 mL/min), moderate (CrCl = 30���<50 mL/min), or severe (<30 mL/min)
renal impairment received hydroxyurea as a single oral dose of 15 mg/kg, achieved
by using combinations of the 200 mg, 300 mg, or 400 mg capsules. Patients
with end-stage renal disease (ESRD) received two doses of 15 mg/kg separated
by 7 days, the first was given following a 4-hour hemodialysis session, the
second prior to hemodialysis. In this study the mean exposure (AUC) in patients
whose creatinine clearance was<60 mL/min (or ESRD) was approximately 64%
higher than in patients with normal renal function. The results suggest that
the initial dose of hydroxyurea should be reduced when used to treat patients
with renal impairment. Close monitoring
of hematologic parameters is advised in these patients.<br/>Hepatic Insufficiency: There are no data that support specific guidance for dosage adjustment
in patients with hepatic impairment. Close monitoring of hematologic parameters
is advised in these patients.<br/>Drug Interactions: There are no data on concomitant use of hydroxyurea with other
drugs in humans.<br/>Animal Pharmacology and Toxicology: The oral LDof hydroxyurea is 7330 mg/kg
in mice and 5780 mg/kg in rats, given as a single dose. In subacute and chronic toxicity studies in the rat, the most consistent
pathological findings were an apparent dose-related mild to moderate bonemarrow hypoplasia as well as pulmonary congestion and mottling of the lungs.
At the highest dosage levels (1260 mg/kg/day for 37 days then 2520 mg/kg/day
for 40 days), testicular atrophy with absence of spermatogenesis occurred;
in several animals, hepatic cell damage with fatty metamorphosis was noted.
In the dog, mild to marked bone marrow depression was a consistent finding
except at the lower dosage levels. Additionally, at the higher dose levels
(140 to 420 mg or 140 to 1260 mg/kg/week given 3 or 7 days weekly for 12 weeks),
growth retardation, slightly increased blood glucose values, and hemosiderosis
of the liver or spleen were found; reversible spermatogenic arrest was noted.
In the monkey, bone marrow depression, lymphoid atrophy of the spleen, and
degenerative changes in the epithelium of the small and large intestines were
found. At the higher, often lethal, doses (400 to 800 mg/kg/day for 7 to 15
days), hemorrhage and congestion were found in the lungs, brain, and urinary
tract. Cardiovascular effects (changes in heart rate, blood pressure, orthostatic
hypotension, EKG changes) and hematological changes (slight hemolysis, slight
methemoglobinemia) were observed in some species of laboratory animals at
doses exceeding clinical levels.
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Hydroxyurea is contraindicated in patients with marked bone marrow
depression, i.e., leukopenia (<2500 WBC) or thrombocytopenia (<100,000),
or severe anemia. HYDREA is contraindicated in patients who have demonstrated a previous
hypersensitivity to hydroxyurea or any other component of its formulation.
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HYDREA (hydroxyurea capsules,
USP) 500 mg capsules in bottles of 100 (NDC 0003-0830-50). Capsule identification number: 830. The cap is opaque green and
the body is opaque pink. They are imprinted on both sections in black ink
with���HYDREA���and���830.���<br/>Storage: Store at 25��C (77��F); excursions permitted to 15�����30��C (59�����86��F) [see USP Controlled Room Temperature]. Keep tightly closed.
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dailymed-ingredient:D&C_Red_28,
dailymed-ingredient:D&C_Yellow_No._10,
dailymed-ingredient:FD&C_Blue_No._1,
dailymed-ingredient:FD&C_Red_40,
dailymed-ingredient:citric_acid,
dailymed-ingredient:gelatin,
dailymed-ingredient:lactose,
dailymed-ingredient:magnesium_stearate,
dailymed-ingredient:sodium_phosphate,
dailymed-ingredient:titanium_dioxide
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General: Therapy with hydroxyurea requires close supervision. The complete
status of the blood, including bone marrow examination, if indicated, as well
as kidney function and liver function should be determined prior to, and repeatedly
during, treatment. The determination of the hemoglobin level, total leukocyte
counts, and platelet counts should be performed at least once a week throughout
the course of hydroxyurea therapy. If the white blood cell count decreases
to less than 2500/mm, or the platelet count to
less than 100,000/mm, therapy should be interrupted
until the values rise significantly toward normal levels. Severe anemia, if
it occurs, should be managed without interrupting hydroxyurea therapy. Hydroxyurea should be used with caution in patients with marked
renal dysfunction. (See CLINICAL PHARMACOLOGY: Special
Populations and DOSAGE AND ADMINISTRATION.) Hydroxyurea is not indicated for the treatment of HIV infection;
however, if HIV-infected patients are treated with hydroxyurea, and in particular,
in combination with didanosine and/or stavudine, close monitoring for signs
and symptoms of pancreatitis is recommended. Patients who develop signs and
symptoms of pancreatitis should permanently discontinue therapy with hydroxyurea.
(See WARNINGS and ADVERSE
REACTIONS.) An increased risk of hepatotoxicity, which may be fatal, may occur
in patients treated with hydroxyurea, and in particular, in combination with
didanosine and stavudine. This combination should be avoided.<br/>Carcinogenesis, Mutagenesis, Impairment of Fertility: See WARNINGS for Carcinogenesis
and Mutagenesis information. Impairment of Fertility: Hydroxyurea administered to male rats
at 60 mg/kg/day (about 0.3 times the maximum recommended human daily dose
on an mg/mbasis) produced testicular atrophy,
decreased spermatogenesis, and significantly reduced their ability to impregnate
females.<br/>Pregnancy: Pregnancy Category D.<br/>Nursing Mothers: Hydroxyurea is excreted in human milk. Because of the potential for serious adverse reactions with hydroxyurea,
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.<br/>Pediatric Use: Safety and effectiveness in pediatric patients have not been established.<br/>Geriatric Use: Elderly patients may be more sensitive to the effects of hydroxyurea,
and may require a lower dose regimen. This drug is known to be excreted by the kidney, and the risk of
toxic reactions to this drug may be greater in patients with impaired renal
function. Because elderly patients are more likely to have decreased renal
function, care should be taken in dose selection, and it may be useful to
monitor renal function (see DOSAGE AND ADMINISTRATION:
Renal Insufficiency).<br/>Drug Interactions: Prospective studies on the potential for hydroxyurea to interact
with other drugs have not been performed. Concurrent use of hydroxyurea and other myelosuppressive agents
or radiation therapy may increase the likelihood of bone marrow depression
or other adverse events. Since hydroxyurea may raise the serum uric acid level, dosage adjustment
of uricosuric medication may be necessary.<br/>Information for Patients: HYDREA is a medication that must be handled with care. People who
are not taking HYDREA should not be exposed to it. To decrease the risk of
exposure, wear disposable gloves when handling HYDREA or bottles containing
HYDREA. Anyone handling HYDREA should wash their hands before and after contact
with the bottle or capsules. If the powder from the capsule is spilled, it
should be wiped up immediately with a damp disposable towel and discarded
in a closed container, such as a plastic bag. The medication should be kept
away from children and pets. Contact your doctor for instructions on how to
dispose of outdated capsules.
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Acute mucocutaneous toxicity has been reported in patients receiving
hydroxyurea at dosages several times the therapeutic dose. Soreness, violet
erythema, edema on palms and soles followed by scaling of hands and feet,
severe generalized hyperpigmentation of the skin, and stomatitis have also
been observed.
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HYDROXYUREA
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HYDREA (Capsule)
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Adverse reactions have been primarily bone marrow depression (leukopenia,
anemia, and occasionally thrombocytopenia), and less frequently gastrointestinal
symptoms (stomatitis, anorexia, nausea, vomiting, diarrhea, and constipation),
and dermatological reactions such as maculopapular rash, skin ulceration,
dermatomyositis-like skin changes, peripheral and facial erythema. Hyperpigmentation,
atrophy of skin and nails, scaling, and violet papules have been observed
in some patients after several years of long-term daily maintenance therapy
with HYDREA.Skin cancer has been reported. Cutaneous vasculitic toxicities,
including vasculitic ulcerations and gangrene, have occurred in patients with
myeloproliferative disorders during therapy with hydroxyurea. These vasculitic
toxicities were reported most often in patients with a history of, or currently
receiving, interferon therapy .
Dysuria and alopecia occur very rarely. Large doses may produce moderate drowsiness.
Neurological disturbances have occurred extremely rarely and were limited
to headache, dizziness, disorientation, hallucinations, and convulsions. HYDREA
occasionally may cause temporary impairment of renal tubular function accompanied
by elevations in serum uric acid, BUN, and creatinine levels. Abnormal BSP
retention has been reported. Fever, chills, malaise, edema, asthenia, and
elevation of hepatic enzymes have also been reported. Adverse reactions observed with combined hydroxyurea and irradiation
therapy are similar to those reported with the use of hydroxyurea or radiation
treatment alone. These effects primarily include bone marrow depression (anemia
and leukopenia), gastric irritation, and mucositis. Almost all patients receiving
an adequate course of combined hydroxyurea and irradiation therapy will demonstrate
concurrent leukopenia. Platelet depression (<100,000 cells/mm)
has occurred rarely and only in the presence of marked leukopenia. HYDREA
may potentiate some adverse reactions usually seen with irradiation alone,
such as gastric distress and mucositis. The association of hydroxyurea with the development of acute pulmonary
reactions consisting of diffuse pulmonary infiltrates, fever, and dyspnea
has been reported rarely. Pulmonary fibrosis also has been reported rarely. Fatal and nonfatal pancreatitis and hepatotoxicity, and severe
peripheral neuropathy have been reported in HIV-infected patients who received
hydroxyurea in combination with antiretroviral agents, in particular, didanosine
plus stavudine. Patients treated with hydroxyurea in combination with didanosine,
stavudine, and indinavir in Study ACTG 5025 showed a median decline in CD4
cells of approximately 100/mm.
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Significant tumor response to HYDREA (hydroxyurea capsules, USP)
has been demonstrated in melanoma, resistant chronic myelocytic leukemia,
and recurrent, metastatic, or inoperable carcinoma of the ovary. Hydroxyurea used concomitantly with irradiation therapy is intended
for use in the local control of primary squamous cell (epidermoid) carcinomas
of the head and neck, excluding the lip.
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HYDREA
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