- Preotact
Preotact is a pharmaceutical form ofparathyroid hormone (H05AA03) manufactured using a strain ofEscherichia coli modified byrecombinant DNA technology. Preotact is used in the treatment ofosteoporosis in postmenopausal women at high risk of osteoporotic fractures. A significant reduction in the incidence of vertebral fractures has been demonstrated.Preotact is marketed in Europe byNycomed . PreosTM is a registered trade mark owned by NPS Pharmaceuticals, Inc. The name PreosTM and theNew Drug Application is pendingFDA approval.Clinical indication/use
Preotact is approved by the European Medicines Agency (EMEA) for the treatment of osteoporosis in postmenopausal women at high risk of fractures. US approval is pending with the FDA.
Administration
The recommended dose is 100 micrograms of Preotact administered once-daily as a
subcutaneous injection into the abdomen, during 18 months (data support treatment up to 24 months). The injections are given using a specially designed injection device (Preotact(TM)Pen). The PreotactPen is specifically designed to allow osteoporosis patients to administer the injections, despite challenges of vision impairment and limited strength of hands and digits tributable to high age. Patients should receive supplementalcalcium andvitamin D during treatment with parathyroid hormone.Following treatment with Preotact, patients can be treated with abisphosphonate to further increase bone mineral densistyContraindications for use
Parathyroid hormone treatment should not be initiated in patients:
* with hypersensitivity to PTH or excipients
* who have receivedradiation therapy to the skeleton
* with pre-existinghypercalcemia and other disturbances in themetabolism ofphosphate orcalcium
* with metabolic bone diseases other than primary osteoporosis (includinghyperparathyroidism and Paget's disease
* with unexplained elevations of bone-specificalkaline phosphatase
* with severerenal impairment
*with severe hepatic impairmentInteractions
Parathyroid hormone is a natural
peptide that is not metabolised in the liver. PTH is not protein bound and has a lowvolume of distribution , therefore no specific drug-drug interactions are suspected. From the knowledge of themechanism of action , combined use of Preotact andcardiac glycoside s may predispose patients todigitalis toxicity if hypercalcemia develops.Undesirable effects
Hypercalcemia and/or
hypercalciuria reflect the knownpharmacodynamic actions of PTH in thegastrointestinal tract , thekidney and theskeleton , and is therefore an expected undesirable effect. Nausea is another commonly reported adverse reaction to the use of PTH.Pharmacodynamic properties
Mechanism of action
Preotact contains recombinant human parathyroid hormone which is identical to the full-length native 84-amino acid
polypeptide .Physiological actions of PTH include stimulation of bone formation by direct effects on bone forming cells (osteoblast s) indirectly increasing the intestinal absorption of calcium and increasing the tubular reabsorption of calcium and excretion of phosphate by the kidney.Pharmacodynamic effects
The skeletal effects of PTH depend upon the pattern of systemic exposure. Transient elevations in PTH levels after subcutaneous injection of Preotact stimulates new bone formation on trabecular and
cortical bone surfaces by preferential stimulation of osteoblastic activity overosteoclast ic activity.Effects on serum calcium concentrations
PTH is the principal regulator of serum calcium
hemostasis . In response to subcutaneous doses of Preotact (100 micrograms), serum total calcium levels increase gradually and reach peak concentration at approximately 6 to 8 hours after dosing. In general, serum calcium levels return to normal within 24 hours.Clinical efficacy
In an 18 month
double-blind ,placebo controlled study, the effects of Preotact on the fracture incidence in 2532 women with postmenopausal osteoporosis was studied. Approximately 19% of patients had a prevalent vertebral fracture at baseline and the mean lumbar T-score of -3.0 in both active and placebo arm.Compared to the placbo group, there was a 61% relative risk reduction of a new vertebral fracture at month 18 for the women in the Preotact group.To prevent one or more new vertebral fractures, 48 women had to be treated for a median of 18 months for the total population. For patients who were already fractured, thenumber needed to treat (NNT) was 21.Effect on bone mineral density (BMD)
In the same study mentioned above, Preotact increased BMD in the
lumbar spine after 18 months treatment by 6.5% compared with a reduction by 0.3% in the placebo group. The difference was statistically significant. The increase of BMD in the hip was also statistically significant compared to placebo, but only around 1.0% at study endpoint. Continued treatment up to 24 months lead to a continued increase in BMD.Pharmacokinetics
Absorption
Subcutaneous administration of PTH into the abdomen produces a rapid increase in plasma PTH levels which reaches peak at 1 to 2 hours after dosing. The mean half-life is approximately 1.5 hours. The absolute bioavailability of 100 micrograms of Preotact after subcutaneous administration in the abdomen is 55%.
Distribution
The volume of distribution at steady-state following intravenous administration is approximately 5.4 liters. Intersubject variability is about 40%.
Biotransformation
Parathyroid hormone is efficiently removed from the blood by a receptor-mediated process in the liver and is broken down into smaller peptide fragments. The fragments derived from the amino-terminus are further degraded within the cell while the fragments derived from the carboxy-terminus are released back into the blood and cleared by the kidney. These carboxy-terminal fragments are thought to play a role in the regulation of PTH activity. Under normal physiological conditions full-length PTH constitutes only 5-30% of the circulating forms of the molecule, while 70-95% is present as carboxy-terminal fragments. Following administration of Preotact, carboxy-terminal fragments make up about 60-90% of the circulating forms of the molecule. Intersubject variability in systemic clearance is about 15%.
Elimination
PTH is metabolised in the liver and to a lesser extent in the kidney. It is not excreted from the body in its intact form. Circulating carboxy-terminal fragments are filtered by the kidney, but are subsequently broken down into even smaller fragments during tubular reuptake. No studies have so far been performed in patients with severe hepatic impairment. The pharmacokinetics of PTH in patients with severe renal insufficiency (
creatinine clearance of less than 30 ml/min) has not been investigated either.Pharmaceutical particulars
Preotact is delivered in a two chamber, glass
ampoule . One chamber contains the active substance in the form of a white powder (withexcipient s:mannitol ,citric acid monohydrate, NaCl,NaOH , HCl). And the other contains the solvent; water for injection. The powder is mixed with the solvent when the ampoule is insterted into the injection device.torage and shelf-life
The mixed solution is stable for 28 days when stored between 2 and 8°C. During this 28 day period the mixed solution may be stored for up to 7 days at room temperature, allowing the patient the freedom to travel.Unmixed ampolues have a shelf-life of 30 months. The products should not be frozen and should be protected from light.
ee also
*
parathyroid hormone
*teriparatide
*osteoporosis External links
* [http://www.emea.europa.eu EMEA - European Medicines Agency]
* [http://www.fda.gov Food and Drug Administration]
* [http://www.preotact.net Product resource website]
* [http://www.nycomed.com Nycomed website]
* [http://www.npsp.com NPS Pharmaceuticals website]
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