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DRUGS & SUPPLEMENTS
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Prostodin Sterile Solution, an oxytocic, contains the tromethamine salt of the (15S)-15 methyl analogue of naturally occurring prostaglandin F2α in a solution suitable for intramuscular injection.
Prostodin tromethamine is the established name for the active ingredient in Prostodin. Four other chemical names are:
The structural formula is represented below:
The molecular formula is C25H47O8N. The molecular weight of Prostodin tromethamine is 489.64. It is a white to slightly off-white crystalline powder. It generally melts between 95° and 105° C, depending on the rate of heating.
Prostodin tromethamine dissolves readily in water at room temperature at a concentration greater than 75 mg/mL.
Each mL of Prostodin Sterile Solution contains Prostodin tromethamine equivalent to 250 mcg of Prostodin, 83 mcg tromethamine, 9 mg sodium chloride, and 9.45 mg benzyl alcohol added as preservative. When necessary, pH is adjusted with sodium hydroxide and/or hydrochloric acid. The solution is sterile.
Prostodin tromethamine administered intramuscularly stimulates in the gravid uterus myometrial contractions similar to labor contractions at the end of a full term pregnancy. Whether or not these contractions result from a direct effect of Prostodin on the myometrium has not been determined. Nonetheless, they evacuate the products of conception from the uterus in most cases.
Postpartum, the resultant myometrial contractions provide hemostasis at the site of placentation.
Prostodin tromethamine also stimulates the smooth muscle of the human gastrointestinal tract. This activity may produce the vomiting or diarrhea or both that is common when Prostodin tromethamine is used to terminate pregnancy and for use postpartum. In laboratory animals and also in humans Prostodin tromethamine can elevate body temperature. With the clinical doses of Prostodin tromethamine used for the termination of pregnancy, and for use postpartum, some patients do experience transient temperature increases.
In laboratory animals and in humans large doses of Prostodin tromethamine can raise blood pressure, probably by contracting the vascular smooth muscle. With the doses of Prostodin tromethamine used for terminating pregnancy, this effect has not been clinically significant. In laboratory animals and also in humans Prostodin tromethamine can elevate body temperature. With the clinical doses of Prostodin tromethamine used for the termination of pregnancy, some patients do experience temperature increases. In some patients, Prostodin tromethamine may cause transient bronchoconstriction.
Drug plasma concentrations were determined by radioimmunoassay in peripheral blood samples collected by different investigators from 10 patients undergoing abortion. The patients had been injected intramuscularly with 250 micrograms of Prostodin at two hour intervals. Blood levels of drug peaked at an average of 2060 picograms/mL one-half hour after the first injection then declined to an average concentration of 770 picograms/mL two hours after the first injection just before the second injection. The average plasma concentration one-half hour after the second injection was slightly higher (2663 picograms/mL) than that after the first injection and decreased again to an average of 1047 picograms/mL by two hours after the second injection. Plasma samples were collected from 5 of these 10 patients following additional injections of the prostaglandin. The average peak concentrations of drug were slightly higher following each successive injection of the prostaglandin, but always decreased to levels less than the preceding peak values by two hours after each injection.
Five women who had delivery spontaneously at term were treated immediately postpartum with a single injection of 250 micrograms of Prostodin tromethamine. Peripheral blood samples were collected at several times during the four hours following treatment and Prostodin tromethamine levels were determined by radioimmunoassay. The highest concentration of Prostodin tromethamine was observed at 15 minutes in two patients (3009 and 2916 picograms/mL), at 30 minutes in two patients (3097 and 2792 picograms/mL), and at 60 minutes in one patient (2718 picograms/mL).
Prostodin Sterile Solution is indicated for aborting pregnancy between the 13th and 20th weeks of gestation as calculated from the first day of the last normal menstrual period and in the following conditions related to second trimester abortion:
Prostodin is indicated for the treatment of postpartum hemorrhage due to uterine atony which has not responded to conventional methods of management. Prior treatment should include the use of intravenously administered oxytocin, manipulative techniques such as uterine massage and, unless contraindicated, intramuscular ergot preparations. Studies have shown that in such cases, the use of Prostodin has resulted in satisfactory control of hemorrhage, although it is unclear whether or not ongoing or delayed effects of previously administered ecbolic agents have contributed to the outcome. In a high proportion of cases, Prostodin used in this manner has resulted in the cessation of life threatening bleeding and the avoidance of emergency surgical intervention.
Prostodin Sterile Solution (carboprost tromethamine), like other potent oxytocic agents, should be used only with strict adherence to recommended dosages.
Prostodin should be used by medically trained personnel in a hospital which can provide immediate intensive care and acute surgical facilities.
Prostodin does not appear to directly affect the fetoplacental unit. Therefore, the possibility does exist that the previable fetus aborted by Prostodin could exhibit transient life signs. Prostodin is not indicated if the fetus in utero has reached the stage of viability. Prostodin should not be considered a feticidal agent.
Evidence from animal studies has suggested that certain other prostaglandins have some teratogenic potential. Although these studies do not indicate that Prostodin is teratogenic, any pregnancy termination with Prostodin that fails should be completed by some other means.
This product contains benzyl alcohol. Benzyl alcohol has been reported to be associated with a fatal "Gasping Syndrome" in premature infants.
Animal studies lasting several weeks at high doses have shown that prostaglandins of the E and F series can induce proliferation of bone. Such effects have also been noted in newborn infants who have received prostaglandin E1 during prolonged treatment. There is no evidence that short term administration of Prostodin Sterile Solution can cause similar bone effects.
In patients with a history of asthma, hypo- or hypertension, cardiovascular, renal, or hepatic disease, anemia, jaundice, diabetes, or epilepsy, Prostodin should be used cautiously.
As with any oxytocic agent, Prostodin should be used with caution in patients with compromised uteri.
As with spontaneous abortion, a process which is sometimes incomplete, abortion induced by Prostodin may be expected to be incomplete in about 20% of cases.
Although the incidence of cervical trauma is extremely small, the cervix should always be carefully examined immediately post-abortion.
Use of Prostodin is associated with transient pyrexia that may be due to its effect on hypothalamic thermoregulation. Temperature elevations exceeding 2° F (1.1° C) were observed in approximately one-eighth of the patients who received the recommended dosage regimen. In all cases, temperature returned to normal when therapy ended. Differentiation of post-abortion endometritis from drug-induced temperature elevations is difficult, but with increasing clinical experience, the distinctions become more obvious and are summarized below:
Endometritis pyrexia | Pyrexia induced by Prostodin | ||
---|---|---|---|
1. | Time of onset: Typically, on third post-abortional day (38° C or higher). | Within 1 to 16 hours after the first injection. | |
2. | Duration: Untreated pyrexia and infection continue and may give rise to other pelvic infections. | Temperatures revert to pretreatment levels after discontinuation of therapy without any other treatment. | |
3. | Retention: Products of conception are often retained in the cervical os or uterine cavity. | Temperature elevation occurs whether or not tissue is retained. | |
4. | Histology: Endometrium is infiltrated with lymphocytes and some areas are necrotic and hemorrhagic. | Although the endometrial stroma may be edematous and vascular, it is not inflamed. | |
5. | The uterus: Often remains boggy and soft with tenderness over the fundus, and pain on moving the cervix on bimanual examination. | Uterine involution normal and uterus is not tender. | |
6. | Discharge: Often associated with foul-smelling lochia and leukorrhea. | Lochia normal. | |
7. | Cervical culture: The culture of pathological organisms from the cervix or uterine cavity after abortion alone does not warrant the diagnosis of septic abortion in the absence of clinical evidence of sepsis. Pathogens have been cultured soon after abortion in patients with no infections. Persistent positive culture with clear clinical signs of infections are significant in the differential diagnosis. | ||
8. | Blood count: Leukocytosis and differential white cell counts do not distinguish between endometritis and hyperthermia caused by Prostodin since total WBC's may increase during infection and transient leukocytosis may also be drug-induced. Fluids should be forced in patients with drug-induced fever and no clinical or bacteriological evidence of intrauterine infection. Any other simple empirical measures for temperature reduction are unnecessary because all fevers induced by Prostodin have been transient or self-limiting. |
Increased blood pressure. In the postpartum hemorrhage series, 5/115 of patients had an increase of blood pressure reported as a side effect. The degree of hypertension was moderate and it is not certain as to whether this was in fact due to a direct effect of Prostodin or a return to a status of pregnancy associated hypertension manifest by the correction of hypovolemic shock. In any event the cases reported did not require specific therapy for the elevated blood pressure.
Use in patients with chorioamnionitis. During the clinical trials with Prostodin, chorioamnionitis was identified as a complication contributing to postpartum uterine atony and hemorrhage in 8/115 (7%) of cases, 3 of which failed to respond to Prostodin. This complication during labor may have an inhibitory effect on the uterine response to Prostodin similar to what has been reported for other oxytocic agents.
Prostodin may augment the activity of other oxytocic agents. Concomitant use with other oxytocic agents is not recommended.
Carcinogenic bioassay studies have not been conducted in animals with Prostodin due to the limited indications for use and short duration of administration. No evidence of mutagenicity was observed in the Micronucleus Test or Ames Assay.
Animal studies do not indicate that Prostodin is teratogenic, however, it has been shown to be embryotoxic in rats and rabbits and any dose which produces increased uterine tone could put the embryo or fetus at risk.
Safety and effectiveness in pediatric patients have not been established.
The adverse effects of Prostodin Sterile Solution are generally transient and reversible when therapy ends. The most frequent adverse reactions observed are related to its contractile effect on smooth muscle.
In patients studied, approximately two-thirds experienced vomiting and diarrhea, approximately one-third had nausea, one-eighth had a temperature increase greater than 2° F, and one-fourteenth experienced flushing.
The pretreatment or concurrent administration of antiemetic and antidiarrheal drugs decreases considerably the very high incidence of gastrointestinal effects common with all prostaglandins used for abortion. Their use should be considered an integral part of the management of patients undergoing abortion with Prostodin.
Of those patients experiencing a temperature elevation, approximately one-sixteenth had a clinical diagnosis of endometritis. The remaining temperature elevations returned to normal within several hours after the last injection.
Adverse effects observed during the use of Prostodin for abortion and for hemorrhage, not all of which are clearly drug related, in decreasing order of frequency include:
Vomiting | Nervousness |
Diarrhea | Nosebleed |
Nausea | Sleep disorders |
Flushing or hot flashes | Dyspnea |
Chills or shivering | Tightness in chest |
Coughing | Wheezing |
Headaches | Posterior cervical perforation |
Endometritis | Weakness |
Hiccough | Diaphoresis |
Dysmenorrhea-like pain | Dizziness |
Paresthesia | Blurred vision |
Backache | Epigastric pain |
Muscular pain | Excessive thirst |
Breast tenderness | Twitching eyelids |
Eye pain | Gagging, retching |
Drowsiness | Dry throat |
Dystonia | Sensation of choking |
Asthma | Thyroid storm |
Injection site pain | Syncope |
Tinnitus | Palpitations |
Vertigo | Rash |
Vaso-vagal syndrome | Upper respiratory infection |
Dryness of mouth | Leg cramps |
Hyperventilation | Perforated uterus |
Respiratory distress | Anxiety |
Hematemesis | Chest pain |
Taste alterations | Retained placental fragment |
Urinary tract infection | Shortness of breath |
Septic shock | Fullness of throat |
Torticollis | Uterine sacculation |
Lethargy | Faintness, light-headedness |
Hypertension | Uterine rupture |
Tachycardia | |
Pulmonary edema | |
Endometritis from IUCD |
The most common complications when Prostodin was utilized for abortion requiring additional treatment after discharge from the hospital were endometritis, retained placental fragments, and excessive uterine bleeding, occurring in about one in every 50 patients.
Hypersensitivity reactions (e.g. Anaphylactic reaction, Anaphylactic shock, Anaphylactoid reaction, Angioedema).
An initial dose of 1 mL of Prostodin Sterile Solution is to be administered deep in the muscle with a tuberculin syringe. Subsequent doses of 250 micrograms should be administered at 1½ to 3½ hour intervals depending on uterine response.
An optional test dose of 100 micrograms (0.4 mL) may be administered initially. The dose may be increased to 500 micrograms (2 mL) if uterine contractility is judged to be inadequate after several doses of 250 micrograms (1 mL).
The total dose administered of Prostodin tromethamine should not exceed 12 milligrams and continuous administration of the drug for more than two days is not recommended.
An initial dose of 250 micrograms of Prostodin Sterile Solution (1 mL of Prostodin) is to be given deep, intramuscularly. In clinical trials it was found that the majority of successful cases (73%) responded to single injections. In some selected cases, however, multiple dosing at intervals of 15 to 90 minutes was carried out with successful outcome. The need for additional injections and the interval at which these should be given can be determined only by the attending physicians as dictated by the course of clinical events. The total dose of Prostodin should not exceed 2 milligrams (8 doses).
Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit.
Prostodin Sterile Solution is available in the following packages:
1 mL ampoules | NDC 0009-0856-05 |
10 × 1 mL ampoules | NDC 0009-0856-08 |
Each mL of Prostodin contains Prostodin tromethamine equivalent to 250 mcg of Prostodin.
Prostodin must be refrigerated at 2° to 8° C (36° to 46° F).
This product's label may have been updated. For current full prescribing information, please visit www.pfizer.com
Rx only
LAB-0032-6.0
January 2014
Logo
1 mL
NDC 0009-0856-05
Rx only
Prostodin ®
Prostodin tromethamine
injection, USP
250 mcg*
FOR INTRAMUSCULAR USE ONLY
Refrigerate at 2° to 8°C (36° to 46°F).
DOSAGE AND USE: See accompanying
prescribing information.
*Equivalent to 250 mcg Prostodin.
Distributed by Pharmacia & Upjohn Co
Division of Pfizer Inc, NY, NY 10017
PAA043229
LOT
EXP
Depending on the reaction of the Prostodin after taken, if you are feeling dizziness, drowsiness or any weakness as a reaction on your body, Then consider Prostodin not safe to drive or operate heavy machine after consumption. Meaning that, do not drive or operate heavy duty machines after taking the capsule if the capsule has a strange reaction on your body like dizziness, drowsiness. As prescribed by a pharmacist, it is dangerous to take alcohol while taking medicines as it exposed patients to drowsiness and health risk. Please take note of such effect most especially when taking Primosa capsule. It's advisable to consult your doctor on time for a proper recommendation and medical consultations.
Is Prostodin addictive or habit forming?Medicines are not designed with the mind of creating an addiction or abuse on the health of the users. Addictive Medicine is categorically called Controlled substances by the government. For instance, Schedule H or X in India and schedule II-V in the US are controlled substances.
Please consult the medicine instruction manual on how to use and ensure it is not a controlled substance.In conclusion, self medication is a killer to your health. Consult your doctor for a proper prescription, recommendation, and guidiance.
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Expensive | 1 | 100.0% |
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Once in a day | 1 | 50.0% | |
Twice in a day | 1 | 50.0% |
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> 60 | 2 | 50.0% | |
30-45 | 1 | 25.0% | |
16-29 | 1 | 25.0% |
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The information was verified by Dr. Rachana Salvi, MD Pharmacology