hey thanks for the feed back that's what i read every where else too but i used t3 a while back and didnt know if worked or not so that is why i thought that maybe it needed the clen good to know it doesnt i think maybe because i was working with a limited ammount i under dosed i had 20mcg's and was only taking 80mcg ED amount is no longer a problem i just got 600 of the 25 mcg how long will it take to start seeing a diff or to notice it working also you mentioned Cabergoline what purpose does it serve ill look it up as well
80 mcgs of T3 and you don't see fatloss after a few days on?
This dose is 3 times the normal production in young health male.
Are you sure that your source is legit?
Cabergoline, brand name: Dostinex.
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TRADE NAME: Dostinex®
for the treatment of hyperprolactinaemia
Licensed Indication:
Cabergoline ‘is indicated for the treatment of dysfunctions associated with hyperprolactinaemia, including amenorrhoea, oligomenorrhoea, anovulation and galactorrhoea.’1
Cabergoline ‘is indicated in patients with prolactin-secreting pituitary adenomas (micro- and macroprolactinomas), idiopathic hyperprolactinaemia, or empty sella syndrome with associated hyperprolactinaemia, which represent the basic underlying pathologies contributing to the above clinical manifestations’.1
The safety and efficacy of cabergoline has not been established in individuals < 16 years of age.1
Background information
Hyperprolactinaemia is an endocrine disorder seen in men and women, which is associated with impaired gonadal function. The most common symptoms in women are secondary amenorrhoea, reduced libido, menstrual disorders, and galactorrhoea.2 In men, symptoms generally include reduced libido and/or impotence. Hypogonadism caused by hyperprolactinaemia can lead to infertility, but also to conditions such as osteoporosis due to low oestrogen levels.
Hyperprolactinaemia can be idiopathic, or caused by drugs or other disease states. Drugs noted to cause hyperprolactinaemia include those that block D2-receptors eg antipsychotics, or those that reduce dopamine levels, eg methyldopa. Conditions associated with the development of hyperprolactinaemia are described under the licensed indication (see above).
Current treatment options
In patients with drug-induced hyperprolactinaemia, the causative agent should be withdrawn.
In hyperprolactinaemia of other aetiologies, treatment options include drug therapy with dopamine agonists, surgery, or radiotherapy. Drug treatment is generally regarded as first line management.
Dopamine agonists, by stimulation of D2-receptors, inhibit prolactin secretion from the lactotroph cells of the anterior pituitary gland. Bromocriptine is regarded as the reference standard whereas quinagolide and cabergoline are newer, longer-acting compounds. The main indications for surgery are tumours resistant to dopamine agonists, poor compliance with drug treatment, or drug intolerance. Radiotherapy can be used in patients who have not responded satisfactorily to medical or surgical treatment.3
Dosage and administration
The recommended initial dosage is 0.5mg (500 micrograms) per week. This dose should be increased gradually, preferably by 0.5mg/week at monthly intervals until an optimal therapeutic response is achieved. The therapeutic dosage is usually 1mg/week (range 0.25mg to 2mg). The weekly dose may be administered as a single dose, or in 2 or more divided doses according to patient tolerability, preferably with food.1
‘Patients should be evaluated during dose escalation to determine the lowest dosage that produces the therapeutic response. Monitoring of serum prolactin levels at monthly intervals is advised.’1
Clinical Efficacy
The efficacy of cabergoline for the treatment of hyperprolactinaemia (of various aetiologies) has been evaluated in numerous open-label studies, in randomised placebo-controlled studies, and in comparative studies with bromocriptine or quinagolide. The outcomes evaluated were primarily normalisation of prolactin levels.
Placebo-controlled studies
A dose-response, double-blind, placebo-controlled, study evaluated four biweekly (twice weekly) dosages of cabergoline in 188 women with hyperprolactinaemia over a 4-week period.5 Normalisation of prolactin levels occurred in 30%, 74%, 74% and 95% of women from the 0.125mg, 0.5mg, 0.75mg and 1mg biweekly groups respectively. No women receiving placebo achieved normalisation of prolactin levels.
In an open-label follow-up study of 162 patients from the dose-response study, normal prolactin levels were achieved or maintained in 138 patients (85%) with continued cabergoline treatment for up to 1 year (dose 0.125- 4mg/week).6
Open-label studies
Two open-label studies (n>100) provide further efficacy data in patients with hyperprolactinaemia. The first enrolled 127 patients (124 women, 3 men) who were treated with cabergoline 0.2- 3.5mg/week for 3- 52 months (median 14).7 Normalisation of prolactin levels occurred in 114 (90%) patients.
The second open-label study enrolled 110 patients (70 women, 40 men) with prolactinomas, 84 of whom had previously been treated with quinagolide or bromocriptine.8 Patients were flexibly dosed with cabergoline. By study endpoint (3 years), normalisation of prolactin levels occurred in 109 patients (99%). Significant reduction in tumour size from baseline was evident in all patients after 1 year (p<0.01). In dopamine-agonist naïve patients (n=26) the nadir prolactin level was significantly lower, and tumour shrinkage significantly greater after 3 years than in the other patients (p<0.01).
Comparative studies with bromocriptine
A randomised, double-blind study with open-label follow-up compared cabergoline to bromocriptine in women with hyperprolactinaemic amenorrhoea over 24 weeks (n = 459).9 The dosages of the drugs taken by the majority of women were 1mg weekly of cabergoline (range 0.5- 2mg), and 5mg daily of bromocriptine (range 2.5- 10mg). Cabergoline or bromocriptine treatment had previously been taken by 68% of women.
Normalisation of prolactin levels occurred in 83% treated with cabergoline vs 58% with bromocriptine (25% difference, 95% CI 17%- 33%, p<0.001). Complete clinical success rates (defined as the occurrence of at least 2 consecutive menses with biochemical evidence of ovulation at least once) were 72% with cabergoline vs 52% with bromocriptine, p<0.001, (20% difference, 95% CI 11%- 28%).
Comparative studies with quinagolide
Three small, (n = 12, 20, 39) open-label, cross-over studies evaluated the effects of cabergoline and quinagolide in the treatment of hyperprolactinaemia (61 women, 10 men).10-12 The results from these studies suggest that cabergoline is at least as effective as quinagolide at normalising prolactin levels.
Pregnancies
Across these studies, 51 pregnancies were reported in women treated with cabergoline. There were 11 terminations, 38 deliveries, and 2 women lost to follow-up. All infants delivered were reported to be normal.
Adverse Events
Nausea and headache were reported with cabergoline across all studies. Other adverse effects reported in at least one study were dizziness, fatigue, asthenia, weakness, postural hypotension, vertigo, vomiting, constipation, and abdominal pain.
Compared with bromocriptine,9 it was noted that significantly fewer patients treated with cabergoline withdrew from treatment due to adverse events, (3% vs 11%, p < 0.001), or reported nausea (30% vs 49%, p < 0.001). In the cabergoline group, nausea was also less severe and shorter in duration than with bromocriptine. Vomiting also occurred less frequently with cabergoline than bromocriptine (4% vs 9%).
A reduction in blood pressure was also noted in some of the studies. In the 1 year open-label follow-up study, mean systolic and diastolic blood pressure values fell by 5mmHg and 4mmHg respectively.6 In the comparative study with bromocriptine, blood pressure fell in ~50% of women (median decrease 10mmHg), particularly diastolic pressure. This was symptomatic in 7 women (3 cabergoline, 4 bromocriptine).9 In one cross-over study with quinagolide, systolic blood pressure fell by 8 or 9 mmHg with both drugs.10
Costs
At current prices, one year’s treatment costs:
£98- £783 with cabergoline 0.25- 2mg weekly
£33- £771 with bromocriptine 1- 30mg daily
£693- £1,387 with quinagolide 0.075- 0.15mg daily.
Given the limited data available it is not possible to reach a conclusion on the overall cost-effectiveness of cabergoline compared to bromocriptine or quinagolide.
Summary
Cabergoline is a dopamine agonist for the treatment of dysfunctions associated with hyperprolactinaemia.
A dose-response was noted in a 4-week, dose-ranging placebo-controlled study with cabergoline. Normal prolactin levels were achieved or maintained in ³ 85% patients in 3 open-label studies with cabergoline (3- 52 months). In comparative studies with bromocriptine and quinagolide, cabergoline was significantly more effective than bromocriptine, and at least as effective as quinagolide at normalising prolactin levels.
Adverse events reported with cabergoline included nausea, headache, dizziness, fatigue, constipation, and a fall in blood pressure values.
Cabergoline may therefore offer a useful alternative to bromocriptine in patients with hyperprolactinaemia.
References
Pharmacia & Upjohn. Dostinex. Summary of Product Characteristics 2000.
Rains CP, Bryson HM, Fitton A. Cabergoline. Drugs 1995;49:255-79.
Conner P, Fried G. Hyperprolactinemia; etiology, diagnosis and treatment alternatives. Acta Obstet Gynecol Scand 1998;77:249-62.
Anon. New drugs for hyperprolactinaemia. DTB 1995;33:65-72.
Webster J, Piscitelli G, Polli A, D'Alberton A, Falsetti L, et al. Dose-dependent suppression of serum prolactin by cabergoline in hyperprolactinaemia: a placebo controlled, double blind, multicentre study. Clinical Endocrinology 1992;37:534-41.
Webster J, Piscitelli G, Polli A, D'Alberton A, Falsetti L, et al. The efficacy and tolerability of long-term cabergoline therapy in hyperprolactinaemic disorders: an open, uncontrolled, multicentre study. Clinical Endocrinology 1993;39:323-9.
Ferrari C, Paracchi A, Mattel AM, de Vincentiis S, D'Alberton A, et al. Cabergoline in the long-term therapy of hyperprolactinemic disorders. Acta Endocrinologica 1992;126:489-94.
Colao A, Di Sarno A, Landi ML, Scavuzzo F, Cppabianca P, et al. Macroprolactinoma shrinkage during cabergoline treatment is greater in naive patients than in patients pretreated with other dopamine agonists: A prospective study in 110 patients. J Clin Endocrinol Metab 2000;85:2247-52.
Webster J, Piscitelli G, Polli A, Ferrari CI, Ismail I, et al. A comparison of cabergoline and bromocriptine in the treatment of hyperprolactinemic amenorrhea. N Engl J Med 1994;331:904-9.
Giusti M, Porcella E, Carraro A, Cuttica M, Valenti S, et al. A cross-over study with the two novel dopaminergic drugs cabergoline and quinagolide in hyperprolactinemic patients. J Endocrinol Invest 1994;17:51-7.
De Luis D, Becerra A, Lahera M, Botella J, Valero M, et al. A randomized cross-over study comparing cabergoline and quinagolide in the treatment of hyperprolactinemic patients. Journal of Endocrinol Invest 2000;23:428-34.
De Sarno A, Landi ML, Marzullo P, Di Somma C, Pivonello R, et al. The effect of quinagolide and carbergoline, two selective dopamine receptor type 2 agonists, in the treatment of prolactinomas. Clinical Endocrinology 2000;53:53-60.
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