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部分中文高特灵信息资料(仅供参考)
【商品名】:高特灵 Hytrin
【通用名】:盐酸特拉唑嗪
【制造商】 雅培
【药理作用】
本药是选择性α1肾上腺受体阻断剂,可减低外周血管总阻力,降低收缩和舒张血压,且舒张压降低更为显著。通常并不伴随反射性心动过速。本药通过阻断前列腺及膀胱出口平滑肌的肾上腺素受体,改善良性前列腺肥大病人的尿流动力和临床症状。临床对照研究中,以特拉唑嗪治疗,病人的血脂均有改进,单独服特拉唑嗪比服安慰剂患者的总胆固醇、结合的低密度及极低密度脂蛋白分数轻度降低,对比基线,这些患者的高密度脂蛋白和HDL/LDL的比率明显升高,甘油三酯明显降低。然而,安慰剂组这些改变并不明显。
【药代动力学】
口服吸收完全,不受进食的影响。首次经肝脏的代谢很少,几乎全部以原型进入循环。服药后1小时血药浓度达到峰值,半衰期约为12小时。药物与血浆蛋白高度结合,原型药物自尿中排出约占口服剂量的10%,大便排出约占20%,其余的以代谢产物形式排出。总的自尿排出量约为40%,自粪便排出约为60%。药代动力学与肾功能无关,故肾功能损害患者不需要作剂量调整。口服后15分钟内,血压逐渐降低,数小时后血药浓度达峰值,血压降低最明显,药效持续24小时。
【毒理研究】
体外体内检查评价(包括Ames试验,体外细胞遗传试验,小鼠显性致死试验,中国仓鼠染色体畸变试验和V79致突变前瞻分析),均未发现潜在致突变作用。小白鼠的致癌分析中,一系列试验未发现致突变性;未发现各形细胞致癌性 ;大鼠和小鼠两种均未发现总肿瘤数目增加。
【适应症】
高血压。良性前列腺肥大,其指征为 :无前列腺切除手术指征者 ;不能接受外科治疗者 ;择期手术者 ;不愿手术者。
【用法用量】
高血压 初始剂量1 mg/日(睡前给药),可逐渐增加剂量,最高可达20 mg/日。良性前列腺肥大 初始剂量为1mg/日,睡前服用。缓慢增加至5-10 mg/日。
【不良反应】 乏力、头痛,心悸、体位性低血压、视力模糊、头晕、瞌睡,鼻塞、恶心、肢端浮肿。
【警告】
本药能引起明显的低血压,尤其是体位性低血压,服用首剂及首几剂之后可能发生晕厥,如在服用数剂之后突然停药,亦可发生晕厥。为了减少发生晕厥及严重的体位性低血压,治疗必须从每日1mg之低剂量开始,并在睡前服用,增加剂量时应缓慢。一旦发生晕厥,应让病人平卧,并采取对症支持治疗。
【注意事项】
服首剂及增加剂量后12小时内,或停药时,应避免驾驶及操作机器。与其它抗高血压药或利尿剂合用时,应减低本药的用量。
孕妇及哺乳期妇女用药 对妊娠的安全性尚未确定,故不推荐使用。本药是否经母乳分泌尚不清楚,故哺乳者慎用。
儿童用药 儿童用药的药效和安全性尚未确定。
【药物过量】 服用过量可引起低血压,应采取对心血管的支持治疗。
【贮藏】 40°C以下保存。
Hytrin Capsules (Abbott)
DESCRIPTION
HYTRIN (terazosin hydrochloride), an alpha-1-selective adrenoceptor blocking agent, is a quinazoline derivative represented by the following chemical name and structural formula: (RS)-Piperazine, 1-(4-amino-6,7-dimethoxy-2-quinazolinyl)-4-[(tetra-hydro-2-furanyl)carbonyl]-, monohydrochloride, dihydrate.
Terazosin hydrochloride is a white, crystalline substance, freely soluble in water and isotonic saline and has a molecular weight of 459.93. HYTRIN capsules (terazosin hydrochloride capsules) for oral ingestion are supplied in four dosage strengths containing terazosin hydrochloride equivalent to 1 mg, 2 mg, 5 mg, or 10 mg of terazosin.
Inactive Ingredients:
1 mg capsules: gelatin, glycerin, iron oxide, methylparaben, mineral oil, polyethylene glycol, povidone, propylparaben, titanium dioxide, and vanillin.
2 mg capsules: D&C yellow No. 10, gelatin, glycerin, methylparaben, mineral oil, polyethylene glycol, povidone, propylparaben, titanium dioxide, and vanillin.
5 mg capsules: D&C red No. 28, FD&C red No. 40, gelatin, glycerin, methylparaben, mineral oil, polyethylene glycol, povidone, propylparaben, titanium dioxide, and vanillin.
10 mg capsules: FD&C blue No. 1, gelatin, glycerin, methylparaben, mineral oil, polyethylene glycol, povidone, propylparaben, titanium dioxide, and vanillin.
CLINICAL PHARMACOLOGY
Pharmacodynamics:
A. Benign Prostatic Hyperplasia (BPH)
The symptoms associated with BPH are related to bladder outlet obstruction, which is comprised of two underlying components: a static component and a dynamic component. The static component is a consequence of an increase in prostate size. Over time, the prostate will continue to enlarge. However, clinical studies have demonstrated that the size of the prostate does not correlate with the severity of BPH symptoms or the degree of urinary obstruction. The dynamic component is a function of an increase in smooth muscle tone in the prostate and bladder neck, leading to constriction of the bladder outlet. Smooth muscle tone is mediated by sympathetic nervous stimulation of alpha-l adrenoceptors, which are abundant in the prostate, prostatic capsule and bladder neck. The reduction in symptoms and improvement in urine flow rates following administration of terazosin is related to relaxation of smooth muscle produced by blockade of alpha-l adrenoceptors in the bladder neck and prostate. Because there are relatively few alpha-l adrenoceptors in the bladder body, terazosin is able to reduce the bladder outlet obstruction without affecting bladder contractility.
Terazosin has been studied in 1222 men with symptomatic BPH. In three placebo-controlled studies, symptom evaluation and uroflowmetric measurements were performed approximately 24 hours following dosing. Symptoms were quantified using the Boyarsky Index. The questionnaire evaluated both obstructive (hesitancy, intermittency, terminal dribbling, impairment of size and force of stream, sensation of incomplete bladder emptying) and irritative (nocturia, daytime frequency, urgency, dysuria) symptoms by rating each of the 9 symptoms from 0-3, for a total score of 27 points. Results from these studies indicated that terazosin statistically significantly improved symptoms and peak urine flow rates over placebo as follows:
|
|
N |
Symptom Score
(Range 0-27) |
|
N |
Peak Flow Rate
(mL/sec) |
|
Mean
Baseline |
Mean
Change (%) |
Mean
Baseline |
Mean
Change (%) |
|
Study 1 (10 mg) a |
|
Titration to fixed dose (12 wks) |
|
Placebo |
55 |
9.7 |
-2.3 (24) |
54 |
10.1 |
+1.0 (10) |
|
Terazosin |
54 |
10.1 |
-4.5 (45) * |
52 |
8.8 |
+3.0 (34) * |
|
Study 2 (2, 5, 10, 20 mg) b |
|
Titration to response (24 wks) |
|
Placebo |
89 |
12.5 |
-3.8 (30) |
88 |
8.8 |
+1.4 (16) |
|
Terazosin |
85 |
12.2 |
-5.3 (43) * |
84 |
8.4 |
+2.9 (35) * |
|
Study 3 (1, 2, 5, 10 mg) c |
|
Titration to response (24 wks) |
|
Placebo |
74 |
10.4 |
-1.1 (11) |
74 |
8.8 |
+1.2 (14) |
|
Terazosin |
73 |
10.9 |
-4.6 (42) * |
73 |
8.6 |
+2.6 (30) * |
|
a Highest dose 10 mg shown. |
|
b 23% of patients on 10 mg, 41% of patients on 20 mg. |
|
c 67% of patients on 10 mg. |
|
*Significantly (p </= 0.05) more improvement than placebo. | |
In all three studies, both symptom scores and peak urine flow rates showed statistically significant improvement from baseline in patients treated with terazosin from week 2 (or the first clinic visit) and throughout the study duration.
Analysis of the effect of terazosin on individual urinary symptoms demonstrated that compared to placebo, terazosin significantly improved the symptoms of hesitancy, intermittency, impairment in size and force of urinary stream, sensation of incomplete emptying, terminal dribbling, daytime frequency and nocturia.
Global assessments of overall urinary function and symptoms were also performed by investigators who were blinded to patient treatment assignment. In studies 1 and 3, patients treated with terazosin had a significantly (p </= 0.001) greater overall improvement compared to placebo treated patients.
In a short term study (Study 1), patients were randomized to either 2, 5 or 10 mg of terazosin or placebo. Patients randomized to the 10 mg group achieved a statistically significant response in both symptoms and peak flow rate compared to placebo (Figure 1).
+ for baseline values see above table
* p </= 0.05, compared to placebo group
In a long-term, open-label, non-placebo controlled clinical trial, 181 men were followed for 2 years and 58 of these men were followed for 30 months. The effect of terazosin on urinary symptom scores and peak flow rates was maintained throughout the study duration (Figures 2 and 3):
In this long-term trial, both symptom scores and peak urinary flow rates showed statistically significant improvement suggesting a relaxation of smooth muscle cells.
Although blockade of alpha-1 adrenoceptors also lowers blood pressure in hypertensive patients with increased peripheral vascular resistance, terazosin treatment of normotensive men with BPH did not result in a clinically significant blood pressure lowering effect:
Mean Changes in Blood Pressure from
Baseline to Final Visit in all Double-Blind,
Placebo-Controlled Studies
|
|
Normotensive
Patients |
Hypertensive
Patients |
| DBP </= 90 mm Hg |
DBP > 90 mm Hg |
| N |
Mean |
N |
Mean |
|
|
Group |
Change |
Change |
|
SBP |
Placebo |
293 |
-0.1 |
45 |
-5.8 |
|
(mm Hg) |
Terazosin |
519 |
-3.3 * |
65 |
-14.4 * |
|
DBP |
Placebo |
293 |
+0.4 |
45 |
-7.1 |
|
(mm Hg) |
Terazosin |
519 |
-2.2 * |
65 |
-15.1 * |
|
*p </= 0.05 vs. placebo | |
B. Hypertension
In animals, terazosin causes a decrease in blood pressure by decreasing total peripheral vascular resistance. The vasodilatory hypotensive action of terazosin appears to be produced mainly by blockade of alpha-1 adrenoceptors. Terazosin decreases blood pressure gradually within 15 minutes following oral administration.
Patients in clinical trials of terazosin were administered once daily (the great majority) and twice daily regimens with total doses usually in the range of 5-20 mg/day, and had mild (about 77%, diastolic pressure 95-105 mmHg) or moderate (23%, diastolic pressure 105-115 mmHg) hypertension. Because terazosin, like all alpha antagonists, can cause unusually large falls in blood pressure after the first dose or first few doses, the initial dose was 1 mg in virtually all trials, with subsequent titration to a specified fixed dose or titration to some specified blood pressure end point (usually a supine diastolic pressure of 90 mmHg).
Blood pressure responses were measured at the end of the dosing interval (usually 24 hours) and effects were shown to persist throughout the interval, with the usual supine responses 5-10 mmHg systolic and 3.5-8 mmHg diastolic greater than placebo. The responses in the standing position tended to be somewhat larger, by 1-3 mmHg, although this was not true in all studies. The magnitude of the blood pressure responses was similar to prazosin and less than hydrochlorothiazide (in a single study of hypertensive patients). In measurements 24 hours after dosing, heart rate was unchanged.
Limited measurements of peak response (2-3 hours after dosing) during chronic terazosin administration indicate that it is greater than about twice the trough (24 hour) response, suggesting some attenuation of response at 24 hours, presumably due to a fall in blood terazosin concentrations at the end of the dose interval. This explanation is not established with certainty, however, and is not consistent with the similarity of blood pressure response to once daily and twice daily dosing and with the absence of an observed dose-response relationship over a range of 5-20 mg, i.e., if blood concentrations had fallen to the point of providing less than full effect at 24 hours, a shorter dosing interval or larger dose should have led to increased response.
Further dose response and dose duration studies are being carried out. Blood pressure should be measured at the end of the dose interval; if response is not satisfactory, patients may be tried on a larger dose or twice daily dosing regimen. The latter should also be considered if possibly blood pressure-related side effects, such as dizziness, palpitations, or orthostatic complaints, are seen within a few hours after dosing.
The greater blood pressure effect associated with peak plasma concentrations (first few hours after dosing) appears somewhat more position-dependent (greater in the erect position) than the effect of terazosin at 24 hours and in the erect position there is also a 6-10 beat per minute increase in heart rate in the first few hours after dosing. During the first 3 hours after dosing 12.5% of patients had a systolic pressure fall of 30 mmHg or more from supine to standing, or standing systolic pressure below 90 mmHg with a fall of at least 20 mmHg, compared to 4% of a placebo group.
There was a tendency for patients to gain weight during terazosin therapy. In placebo-controlled monotherapy trials, male and female patients receiving terazosin gained a mean of 1.7 and 2.2 pounds respectively, compared to losses of 0.2 and 1.2 pounds respectively in the placebo group. Both differences were statistically significant.
During controlled clinical trials, patients receiving terazosin monotherapy had a small but statistically significant decrease (a 3% fall) compared to placebo in total cholesterol and the combined low-density and very-low-density lipoprotein fractions. No significant changes were observed in high-density lipoprotein fraction and triglycerides compared to placebo.
Analysis of clinical laboratory data following administration of terazosin suggested the possibility of hemodilution based on decreases in hematocrit, hemoglobin, white blood cells, total protein and albumin. Decreases in hematocrit and total protein have been observed with alpha-blockade and are attributed to hemodilution.
Pharmacokinetics:
Terazosin hydrochloride administered as HYTRIN capsules is essentially completely absorbed in man. Administration of capsules immediately after meals had a minimal effect on the extent of absorption. The time to reach peak plasma concentration however, was delayed by about 40 minutes. Terazosin has been shown to undergo minimal hepatic first-pass metabolism and nearly all of the circulating dose is in the form of parent drug. The plasma levels peak about one hour after dosing, and then decline with a half-life of approximately 12 hours. In a study that evaluated the effect of age on terazosin pharmacokinetics, the mean plasma half-lives were 14.0 and 11.4 hours for the age group >/=70 years and the age group of 20-39 years, respectively. After oral administration the plasma clearance was decreased by 31.7% in patients 70 years of age or older compared to that in patients 20-39 years of age.
The drug is 90-94% bound to plasma proteins and binding is constant over the clinically observed concentration range. Approximately 10% of an orally administered dose is excreted as parent drug in the urine and approximately 20% is excreted in the feces. The remainder is eliminated as metabolites. Impaired renal function had no significant effect on the elimination of terazosin, and dosage adjustment of terazosin to compensate for the drug removal during hemodialysis (approximately 10%) does not appear to be necessary. Overall, approximately 40% of the administered dose is excreted in the urine and approximately 60% in the feces. The disposition of the compound in animals is qualitatively similar to that in man.
INDICATIONS AND USAGE
HYTRIN (terazosin hydrochloride) is indicated for the treatment of symptomatic benign prostatic hyperplasia (BPH). There is a rapid response, with approximately 70% of patients experiencing an increase in urinary flow and improvement in symptoms of BPH when treated with HYTRIN. The long-term effects of HYTRIN on the incidence of surgery, acute urinary obstruction or other complications of BPH are yet to be determined.
HYTRIN is also indicated for the treatment of hypertension. It can be used alone or in combination with other antihypertensive agents such as diuretics or beta-adrenergic blocking agents.
CONTRAINDICATIONS
HYTRIN capsules are contraindicated in patients known to be hypersensitive to terazosin hydrochloride.
WARNINGS
Syncope and "First-dose" Effect:
HYTRIN capsules, like other alpha-adrenergic blocking agents, can cause marked lowering of blood pressure, especially postural hypotension, and syncope in association with the first dose or first few days of therapy. A similar effect can be anticipated if therapy is interrupted for several days and then restarted. Syncope has also been reported with other alpha-adrenergic blocking agents in association with rapid dosage increases or the introduction of another antihypertensive drug. Syncope is believed to be due to an excessive postural hypotensive effect, although occasionally the syncopal episode has been preceded by about of severe supraventricular tachycardia with heart rates of 120-160 beats per minute. Additionally, the possibility of the contribution of hemodilution to the symptoms of postural hypotension should be considered.
To decrease the likelihood of syncope or excessive hypotension, treatment should always be initiated with a 1 mg dose of terazosin, given at bedtime. The 2 mg, 5 mg and 10 mg capsules are not indicated as initial therapy. Dosage should then be increased slowly, according to recommendations in the Dosage and Administration section and additional antihypertensive agents should be added with caution. The patient should be cautioned to avoid situations, such as driving or hazardous tasks, where injury could result should syncope occur during initiation of therapy.
In early investigational studies, where increasing single doses up to 7.5 mg were given at 3 day intervals, tolerance to the first dose phenomenon did not necessarily develop and the "first-dose" effect could be observed at all doses. Syncopal episodes occurred in 3 of the 14 subjects given terazosin at doses of 2.5, 5 and 7.5 mg, which are higher than the recommended initial dose; in addition, severe orthostatic hypotension (blood pressure falling to 50/0 mmHg) was seen in two others and dizziness, tachycardia, and lightheadedness occurred in most subjects. These adverse effects all occurred within 90 minutes of dosing.
In three placebo-controlled BPH studies 1, 2, and 3 (see CLINICAL PHARMACOLOGY ), the incidence of postural hypotension in the terazosin treated patients was 5.1%, 5.2%, and 3.7% respectively.
In multiple dose clinical trials involving nearly 2000 hypertensive patients treated with terazosin, syncope was reported in about 1% of patients. Syncope was not necessarily associated only with the first dose.
If syncope occurs, the patient should be placed in a recumbent position and treated supportively as necessary. There is evidence that the orthostatic effect of terazosin is greater, even in chronic use, shortly after dosing. The risk of the events is greatest during the initial seven days of treatment, but continues at all time intervals.
Priapism:
Rarely, (probably less than once in every several thousand patients) terazosin and other (alpha) 1 -antagonists have been associated with priapism (painful penile erection, sustained for hours and unrelieved by sexual intercourse or masturbation). Two or three dozen cases have been reported. Because this condition can lead to permanent impotence if not promptly treated, patients must be advised about the seriousness of the condition (see PRECAUTIONS: Information for Patients ).
PRECAUTIONS
General:
Prostatic Cancer
Carcinoma of the prostate and BPH cause many of the same symptoms. These two diseases frequently co-exist. Therefore, patients thought to have BPH should be examined prior to starting HYTRIN therapy to rule out the presence of carcinoma of the prostate.
Orthostatic Hypotension
While syncope is the most severe orthostatic effect of terazosin (see Warnings ), other symptoms of lowered blood pressure, such as dizziness, lightheadedness and palpitations, were more common and occurred in some 28% of patients in clinical trials of hypertension. In BPH clinical trials, 21% of the patients experienced one or more of the following: dizziness, hypotension, postural hypotension, syncope, and vertigo. Patients with occupations in which such events represent potential problems should be treated with particular caution.
Information for Patients (see Patient Package Insert):
Patients should be made aware of the possibility of syncopal and orthostatic symptoms, especially at the initiation of therapy, and to avoid driving or hazardous tasks for 12 hours after the first dose, after a dosage increase and after interruption of therapy when treatment is resumed. They should be cautioned to avoid situations where injury could result should syncope occur during initiation of terazosin therapy. They should also be advised of the need to sit or lie down when symptoms of lowered blood pressure occur, although these symptoms are not always orthostatic, and to be careful when rising from a sitting or lying position. If dizziness, lightheadedness, or palpitations are bothersome they should be reported to the physician, so that dose adjustment can be considered.
Patients should also be told that drowsiness or somnolence can occur with terazosin, requiring caution in people who must drive or operate heavy machinery.
Patients should be advised about the possibility of priapism as a result of treatment with HYTRIN and other similar medications. Patients should know that this reaction to HYTRIN is extremely rare, but that if it is not brought to immediate medical attention, it can lead to permanent erectile dysfunction (impotence).
Laboratory Tests:
Small but statistically significant decreases in hematocrit, hemoglobin, white blood cells, total protein and albumin were observed in controlled clinical trials. These laboratory findings suggested the possibility of hemodilution. Treatment with terazosin for up to 24 months had no significant effect on prostate specific antigen (PSA) levels.
Drug Interactions:
In controlled trials, terazosin has been added to diuretics, and several beta-adrenergic blockers; no unexpected interactions were observed. Terazosin has also been used in patients on a variety of concomitant therapies; while these were not formal interaction studies, no interactions were observed. Terazosin has been used concomitantly in at least 50 patients on the following drugs or drug classes: 1) analgesic/anti-inflammatory (e.g., acetaminophen, aspirin, codeine, ibuprofen, indomethacin); 2) antibiotics (e.g., erythromycin, trimethoprim and sulfamethoxazole); 3) anticholinergic/sympathomimetics (e.g., phenylephrine hydrochloride, phenylpropanolamine hydrochloride, pseudoephedrine hydrochloride); 4) antigout (e.g., allopurinol); 5) antihistamines (e.g., chlorpheniramine); 6) cardiovascular agents (e.g., atenolol, hydrochlorothiazide, methyclothiazide, propranolol); 7) corticosteroids; 8) gastrointestinal agents (e.g., antacids); 9) hypoglycemics; 10) sedatives and tranquilizers (e.g., diazepam).
Use with Other Drugs:
In a study (n=24) where terazosin and verapamil were administered concomitantly, terazosin's mean AUC 0-24 increased 11% after the first verapamil dose and after 3 weeks of verapamil treatment it increased by 24% with associated increases in C max (25%) and C min (32%) means. Terazosin mean T max decreased from 1.3 hours to 0.8 hours after 3 weeks of verapamil treatment. Statistically significant differences were not found in the verapamil level with and without terazosin. In a study (n=6) where terazosin and captopril were administered concomitantly, plasma disposition of captopril was not influenced by concomitant administration of terazosin and terazosin maximum plasma concentrations increased linearly with dose at steady-state after administration of terazosin plus captopril (see Dosage and Administration ).
Carcinogenesis, Mutagenesis, Impairment of Fertility:
Terazosin was devoid of mutagenic potential when evaluated in vivo and in vitro (the Ames test, in vivo cytogenetics, the dominant lethal test in mice, in vivo Chinese hamster chromosome aberration test and V79 forward mutation assay).
Terazosin, administered in the feed to rats at doses of 8, 40, and 250 mg/kg/day (70, 350, and 2100 mg/M 2 /day), for two years, was associated with a statistically significant increase in benign adrenal medullary tumors of male rats exposed to the 250 mg/kg dose. This dose is 175 times the maximum recommended human dose of 20 mg (12 mg/M 2 ). Female rats were unaffected. Terazosin was not oncogenic in mice when administered in feed for 2 years at a maximum tolerated dose of 32 mg/kg/day (110 mg/M 2 ; 9 times the maximum recommended human dose). The absence of mutagenicity in a battery of tests, of tumorigenicity of any cell type in the mouse carcinogenicity assay, of increased total tumor incidence in either species, and of proliferative adrenal lesions in female rats, suggests a male rat species-specific event. Numerous other diverse pharmaceutical and chemical compounds have also been associated with benign adrenal medullary tumors in male rats without supporting evidence for carcinogenicity in man.
The effect of terazosin on fertility was assessed in a standard fertility/reproductive performance study in which male and female rats were administered oral doses of 8, 30 and 120 mg/kg/day. Four of 20 male rats given 30 mg/kg (240 mg/M 2 ; 20 times the maximum recommended human dose) and five of 19 male rats given 120 mg/kg (960 mg/M 2 ; 80 times the maximum recommended human dose) failed to sire a litter. Testicular weights and morphology were unaffected by treatment. Vaginal smears at 30 and 120 mg/kg/day, however, appeared to contain less sperm than smears from control matings and good correlation was reported between sperm count and subsequent pregnancy.
Oral administration of terazosin for one or two years elicited a statistically significant increase in the incidence of testicular atrophy in rats exposed to 40 and 250 mg/kg/day (29 and 175 times the maximum recommended human dose), but not in rats exposed to 8 mg/kg/day (> 6 times the maximum recommended human dose). Testicular atrophy was also observed in dogs dosed with 300 mg/kg/day (> 500 times the maximum recommended human dose) for three months but not after one year when dosed with 20 mg/kg/day (38 times the maximum recommended human dose). This lesion has also been seen with Minipress®, another (marketed) selective-alpha-1 blocking agent.
Pregnancy:
Teratogenic effects: Pregnancy Category C. Terazosin was not teratogenic in either rats or rabbits when administered at oral doses up to 280 and 60 times, respectively, the maximum recommended human dose. Fetal resorptions occurred in rats dosed with 480 mg/kg/day, approximately 280 times the maximum recommended human dose. Increased fetal resorptions, decreased fetal weight and an increased number of supernumerary ribs were observed in offspring of rabbits dosed with 60 times the maximum recommended human dose. These findings (in both species) were most likely secondary to maternal toxicity. There are no adequate and well-controlled studies in pregnant women and the safety of terazosin in pregnancy has not been established. HYTRIN is not recommended during pregnancy unless the potential benefit justifies the potential risk to the mother and fetus.
Nonteratogenic effects: In a peri- and post-natal development study in rats, significantly more pups died in the group dosed with 120 mg/kg/day (> 75 times the maximum recommended human dose) than in the control group during the three-week postpartum period.
Nursing Mothers:
It is not known whether terazosin is excreted in breast milk. Because many drugs are excreted in breast milk, caution should be exercised when terazosin is administered to a nursing woman.
Pediatric Use:
Safety and effectiveness in children have not been determined.
ADVERSE REACTIONS
Benign Prostatic Hyperplasia
The incidence of treatment-emergent adverse events has been ascertained from clinical trials conducted worldwide. All adverse events reported during these trials were recorded as adverse reactions. The incidence rates presented below are based on combined data from six placebo-controlled trials involving once-a-day administration of terazosin at doses ranging from 1 to 20 mg. Table 1 summarizes those adverse events reported for patients in these trials when the incidence rate in the terazosin group was at least 1% and was greater than that for the placebo group, or where the reaction is of clinical interest. Asthenia, postural hypotension, dizziness, somnolence, nasal congestion/rhinitis, and impotence were the only events that were significantly (p </= 0.05) more common in patients receiving terazosin than in patients receiving placebo. The incidence of urinary tract infection was significantly lower in the patients receiving terazosin than in patients receiving placebo. An analysis of the incidence rate of hypotensive adverse events (see PRECAUTIONS ) adjusted for the length of drug treatment has shown that the risk of the events is greatest during the initial seven days of treatment, but continues at all time intervals.
TABLE 1
ADVERSE REACTIONS DURING
PLACEBO-CONTROLLED TRIALS
BENIGN PROSTATIC HYPERPLASIA
|
|
Terazosin |
Placebo |
|
Body System |
(N=636) |
(N=360) |
|
BODY AS A WHOLE |
|
**/* Asthenia |
7.4% * |
3.3% |
|
Flu Syndrome |
2.4% |
1.7% |
|
Headache |
4.9% |
5.8% |
|
CARDIOVASCULAR SYSTEM |
|
Hypotension |
0.6% |
0.6% |
|
Palpitations |
0.9% |
1.1% |
|
Postural Hypotension |
3.9% * |
0.8% |
|
Syncope |
0.6% |
0.0% |
|
DIGESTIVE SYSTEM |
|
Nausea |
1.7% |
1.1% |
|
METABOLIC AND NUTRITIONAL DISORDERS |
|
Peripheral Edema |
0.9% |
0.3% |
|
Weight Gain |
0.5% |
0.0% |
|
NERVOUS SYSTEM |
|
Dizziness |
9.1% * |
4.2% |
|
Somnolence |
3.6% * |
1.9% |
|
Vertigo |
1.4% |
0.3% |
|
RESPIRATORY SYSTEM |
|
Dyspnea |
1.7% |
0.8% |
|
Nasal Congestion/Rhinitis |
1.9% * |
0.0% |
|
SPECIAL SENSES |
|
Blurred Vision/Amblyopia |
1.3% |
0.6% |
|
UROGENITAL SYSTEM |
|
Impotence |
1.6% * |
0.6% |
|
Urinary Tract Infection |
1.3% |
3.9% * |
|
**/* Includes weakness, tiredness, lassitude and fatigue. |
|
*p </= 0.05 comparison between groups. | |
Additional adverse events have been reported, but these are, in general, not distinguishable from symptoms that might have occurred in the absence of exposure to terazosin. The safety profile of patients treated in the long-term open-label study was similar to that observed in the controlled studies.
The adverse events were usually transient and mild or moderate in intensity, but sometimes were serious enough to interrupt treatment. In the placebo-controlled clinical trials, the rates of premature termination due to adverse events were not statistically different between the placebo and terazosin groups. The adverse events that were bothersome, as judged by their being reported as reasons for discontinuation of therapy by at least 0.5% of the terazosin group and being reported more often than in the placebo group, are shown in Table 2.
TABLE 2
DISCONTINUATION DURING
PLACEBO-CONTROLLED TRIALS
BENIGN PROSTATIC HYPERPLASIA
|
Body System |
Terazosin |
Placebo |
| (N=636) |
(N=360) |
|
BODY AS A WHOLE |
|
Fever |
0.5% |
0.0% |
|
Headache |
1.1% |
0.8% |
|
CARDIOVASCULAR SYSTEM |
|
Postural Hypotension |
0.5% |
0.0% |
|
Syncope |
0.5% |
0.0% |
|
DIGESTIVE SYSTEM |
|
Nausea |
0.5% |
0.3% |
|
NERVOUS SYSTEM |
|
Dizziness |
2.0% |
1.1% |
|
Vertigo |
0.5% |
0.0% |
|
RESPIRATORY SYSTEM |
|
Dyspnea |
0.5% |
0.3% |
|
SPECIAL SENSES |
|
Blurred Vision/Amblyopia |
0.6% |
0.0% |
|
UROGENITAL SYSTEM |
|
Urinary Tract Infection |
0.5% |
0.3% | |
Hypertension
The prevalence of adverse reactions has been ascertained from clinical trials conducted primarily in the United States. All adverse experiences (events) reported during these trials were recorded as adverse reactions. The prevalence rates presented below are based on combined data from fourteen placebo-controlled trials involving once-a-day administration of terazosin, as monotherapy or in combination with other antihypertensive agents, at doses ranging from 1 to 40 mg. Table 3 summarizes those adverse experiences reported for patients in these trials where the prevalence rate in the terazosin group was at least 5%, where the prevalence rate for the terazosin group was at least 2% and was greater than the prevalence rate for the placebo group, or where the reaction is of particular interest. Asthenia, blurred vision, dizziness, nasal congestion, nausea, peripheral edema, palpitations and somnolence were the only symptoms that were significantly (p < 0.05) more common in patients receiving terazosin than in patients receiving placebo. Similar adverse reaction rates were observed in placebo-controlled monotherapy trials.
TABLE 3
ADVERSE REACTIONS DURING
PLACEBO-CONTROLLED TRIALS
HYPERTENSION
|
Body System |
Terazosin |
Placebo |
| (N=859) |
(N=506) |
|
BODY AS A WHOLE |
|
**/* Asthenia |
11.3% * |
4.3% |
|
Back Pain |
2.4% |
1.2% |
|
Headache |
16.2% |
15.8% |
|
CARDIOVASCULAR SYSTEM |
|
Palpitations |
4.3% * |
1.2% |
|
Postural Hypotension |
1.3% |
0.4% |
|
Tachycardia |
1.9% |
1.2% |
|
DIGESTIVE SYSTEM |
|
Nausea |
4.4% * |
1.4% |
|
METABOLIC AND NUTRITIONAL DISORDERS |
|
Edema |
0.9% |
0.6% |
|
Peripheral Edema |
5.5% * |
2.4% |
|
Weight Gain |
0.5% |
0.2% |
|
MUSCULOSKELETAL SYSTEM |
|
Pain-Extremities |
3.5% |
3.0% |
|
NERVOUS SYSTEM |
|
Depression |
0.3% |
0.2% |
|
Dizziness |
19.3% * |
7.5% |
|
Libido Decreased |
0.6% |
0.2% |
|
Nervousness |
2.3% |
1.8% |
|
Paresthesia |
2.9% |
1.4% |
|
Somnolence |
5.4% * |
2.6% |
|
RESPIRATORY SYSTEM |
|
Dyspnea |
3.1% |
2.4% |
|
Nasal Congestion |
5.9% * |
3.4% |
|
Sinusitis |
2.6% |
1.4% |
|
SPECIAL SENSES |
|
Blurred Vision |
1.6% * |
0.0% |
|
UROGENITAL SYSTEM |
|
Impotence |
1.2% |
1.4% |
|
**/* Includes weakness, tiredness, lassitude and fatigue. |
|
*Statistically significant at p=0.05 level. | |
Additional adverse reactions have been reported, but these are, in general, not distinguishable from symptoms that might have occurred in the absence of exposure to terazosin. The following additional adverse reactions were reported by at least 1% of 1987 patients who received terazosin in controlled or open, short- or long-term clinical trials or have been reported during marketing experience: Body as a Whole: chest pain, facial edema, fever, abdominal pain, neck pain, shoulder pain; Cardiovascular System: arrhythmia, vasodilation; Digestive System: constipation, diarrhea, dry mouth, dyspepsia, flatulence, vomiting; Metabolic/Nutritional Disorders: gout; Musculoskeletal System: arthralgia, arthritis, joint disorder, myalgia; Nervous System: anxiety, insomnia; Respiratory System: bronchitis, cold symptoms, epistaxis, flu symptoms, increased cough, pharyngitis, rhinitis; Skin and Appendages: pruritus, rash, sweating; Special Senses: abnormal vision, conjunctivitis, tinnitus; Urogenital System: urinary frequency, urinary incontinence primarily reported in postmenopausal women, urinary tract infection.
The adverse reactions were usually mild or moderate in intensity but sometimes were serious enough to interrupt treatment. The adverse reactions that were most bothersome, as judged by their being reported as reasons for discontinuation of therapy by at least 0.5% of the terazosin group and being reported more often than in the placebo group, are shown in Table 4.
TABLE 4
DISCONTINUATIONS DURING
PLACEBO-CONTROLLED TRIALS
HYPERTENSION
|
|
Terazosin |
Placebo |
|
Body System |
(N=859) |
(N=506) |
|
BODY AS A WHOLE |
|
Asthenia |
1.6% |
0.0% |
|
Headache |
1.3% |
1.0% |
|
CARDIOVASCULAR SYSTEM |
|
Palpitations |
1.4% |
0.2% |
|
Postural Hypotension |
0.5% |
0.0% |
|
Syncope |
0.5% |
0.2% |
|
Tachycardia |
0.6% |
0.0% |
|
DIGESTIVE SYSTEM |
|
Nausea |
0.8% |
0.0% |
|
METABOLIC AND NUTRITIONAL DISORDERS |
|
Peripheral Edema |
0.6% |
0.0% |
|
NERVOUS SYSTEM |
|
Dizziness |
3.1% |
0.4% |
|
Paresthesia |
0.8% |
0.2% |
|
Somnolence |
0.6% |
0.2% |
|
RESPIRATORY SYSTEM |
|
Dyspnea |
0.9% |
0.6% |
|
Nasal Congestion |
0.6% |
0.0% |
|
SPECIAL SENSES |
|
Blurred Vision |
0.6% |
0.0% | |
Post-marketing Experience
Post-marketing experience indicates that in rare instances patients may develop allergic reactions, including anaphylaxis, following administration of terazosin hydrochloride. There have been reports of priapism and thrombocytopenia during post-marketing surveillance. Atrial fibrillation has been reported.
OVERDOSAGE
Should overdosage of HYTRIN lead to hypotension, support of the cardiovascular system is of first importance. Restoration of blood pressure and normalization of heart rate may be accomplished by keeping the patient in the supine position. If this measure is inadequate, shock should first be treated with volume expanders. If necessary, vasopressors should then be used and renal function should be monitored and supported as needed. Laboratory data indicate that terazosin is 90-94% protein bound; therefore, dialysis may not be of benefit.
DOSAGE AND ADMINISTRATION
If HYTRIN administration is discontinued for several days, therapy should be reinstituted using the initial dosing regimen.
Benign Prostatic Hyperplasia:
Initial Dose:
1 mg at bedtime is the starting dose for all patients, and this dose should not be exceeded as an initial dose. Patients should be closely followed during initial administration in order to minimize the risk of severe hypotensive response.
Subsequent Doses:
The dose should be increased in a stepwise fashion to 2 mg, 5 mg, or 10 mg once daily to achieve the desired improvement of symptoms and/or flow rates. Doses of 10 mg once daily are generally required for the clinical response. Therefore, treatment with 10 mg for a minimum of 4-6 weeks may be required to assess whether a beneficial response has been achieved. Some patients may not achieve a clinical response despite appropriate titration. Although some additional patients responded at a 20 mg daily dose, there was an insufficient number of patients studied to draw definitive conclusions about this dose. There are insufficient data to support the use of higher doses for those patients who show inadequate or no response to 20 mg daily. If terazosin administration is discontinued for several days or longer, therapy should be reinstituted using the initial dosing regimen.
Use with Other Drugs:
Caution should be observed when HYTRIN is administered concomitantly with other antihypertensive agents, especially the calcium channel blocker verapamil, to avoid the possibility of developing significant hypotension. When using HYTRIN and other antihypertensive agents concomitantly, dosage reduction and retitration of either agent may be necessary (see Precautions ).
Hypertension:
The dose of HYTRIN and the dose interval (12 or 24 hours) should be adjusted according to the patient's individual blood pressure response. The following is a guide to its administration:
Initial Dose:
1 mg at bedtime is the starting dose for all patients, and this dose should not be exceeded. This initial dosing regimen should be strictly observed to minimize the potential for severe hypotensive effects.
Subsequent Doses:
The dose may be slowly increased to achieve the desired blood pressure response. The usual recommended dose range is 1 mg to 5 mg administered once a day; however, some patients may benefit from doses as high as 20 mg per day. Doses over 20 mg do not appear to provide further blood pressure effect and doses over 40 mg have not been studied. Blood pressure should be monitored at the end of the dosing interval to be sure control is maintained throughout the interval. It may also be helpful to measure blood pressure 2-3 hours after dosing to see if the maximum and minimum responses are similar, and to evaluate symptoms such as dizziness or palpitations which can result from excessive hypotensive response. If response is substantially diminished at 24 hours an increased dose or use of a twice daily regimen can be considered. If terazosin administration is discontinued for several days or longer, therapy should be reinstituted using the initial dosing regimen. In clinical trials, except for the initial dose, the dose was given in the morning.
------------------------------------------------------
产地国家: 英国
原产地英文商品名:
HYTRIN-1mg/Capsule,100Capsules
原产地英文药品名:
TERAZOSIN HCL
中文参考商品译名:
高特灵-1毫克/胶囊,100胶囊
中文参考药品译名:
盐酸特拉唑嗪
生产厂家中文参考译名:
雅培公司
生产厂家英文名:
Abbott Laboratories Limited
------------------------------------------------------
产地国家: 英国
原产地英文商品名:
HYTRIN-2mg/Capsule,100Capsules
原产地英文药品名:
TERAZOSIN HCL
中文参考商品译名:
高特灵-2毫克/胶囊,100胶囊
中文参考药品译名:
盐酸特拉唑嗪
生产厂家中文参考译名:
雅培公司
生产厂家英文名:
Abbott Laboratories Limited
------------------------------------------------------
产地国家: 英国
原产地英文商品名:
HYTRIN-5mg/Capsule,100Capsules
原产地英文药品名:
TERAZOSIN HCL
中文参考商品译名:
高特灵-5毫克/胶囊,100胶囊
中文参考药品译名:
盐酸特拉唑嗪
生产厂家中文参考译名:
雅培公司
生产厂家英文名:
Abbott Laboratories Limited
------------------------------------------------------
产地国家: 英国
原产地英文商品名:
HYTRIN-10mg/Capsule,100Capsules
原产地英文药品名:
TERAZOSIN HCL
中文参考商品译名:
高特灵-10毫克/胶囊,100胶囊
中文参考药品译名:
盐酸特拉唑嗪
生产厂家中文参考译名:
雅培公司
生产厂家英文名:
Abbott Laboratories Limited |
