nal products endometrin should not be recommended for use with other vaginal products (such as antifungal products) as this may alter progesterone release and absorption from the vaginal insert [ see drug interactions (7) ].

0 mg three times daily. the adverse reactions that occurred at a rate greater than or equal to 2% in either endometrin group are summarized in table 1. table 1: number and frequency of reported adverse reactions in women treated with endometrin in an assisted reproductive technology study body system endometrin 100 mg twice daily (n=404) endometrin 100 mg three times daily (n=404) preferred term gastrointestinal disorders abdominal pain 50 (12%) 50 (12%) nausea 32 (8%) 29 (7%) abdominal distension 18 (4%) 17 (4%) constipation 9 (2%) 14 (3%) vomiting 13 (3%) 9 (2%) general disorders and administration site conditions fatigue 7 (2%) 12 (3%) infections and infestations urinary tract infection 9 (2%) 4 (1%) injury, poisoning and procedural complications post-oocyte retrieval pain 115 (28%) 102 (25%) nervous system disorders headache 15 (4%) 13 (3%) reproductive system and breast disorders ovarian hyperstimulation syndrome 30 (7%) 27 (7%) uterine spasm 15 (4%) 11 (3%) vaginal bleeding 13 (3%) 14 (3%) other less common reported adverse reactions included vaginal irritation, itching, burning, discomfort, urticaria, and peripheral edema. 6.2 expected adverse reaction profile seen with progesterone endometrin is also expected to have adverse reactions similar to other drugs containing progesterone that may include breast tenderness, bloating, mood swings, irritability, and drowsiness.

one fetus with spina bifida, three fetuses with congenital heart defects, one fetus with an umbilical hernia, and one fetus with an intestinal anomaly. birth defects reported in the endometrin three times daily group included: one fetus with an esophageal fistula, one fetus with hypospadias and an underdeveloped right ear, one fetus with down syndrome and an atrial septal defect, one fetus with congenital heart anomalies, one fetus with digeorge's syndrome, one fetus with a hand deformity, and one fetus with cleft palate. for additional information on the pharmacology of endometrin and pregnancy outcome information [ see clinical pharmacology (12) and clinical studies sections (14) ]. 8.3 nursing mothers detectable amounts of progesterone have been identified in the milk of nursing mothers. the effect of this on the nursing infant has not been determined. 8.4 pediatric use this drug is not intended for pediatric use and no clinical data have been collected in children. therefore, the safety and effectiveness of endometrin in pediatric patients have not been established. 8.5 geriatric use no clinical data have been collected in patients over age 65.

three fetuses with congenital heart defects, one fetus with an umbilical hernia, and one fetus with an intestinal anomaly. birth defects reported in the endometrin three times daily group included: one fetus with an esophageal fistula, one fetus with hypospadias and an underdeveloped right ear, one fetus with down syndrome and an atrial septal defect, one fetus with congenital heart anomalies, one fetus with digeorge's syndrome, one fetus with a hand deformity, and one fetus with cleft palate. for additional information on the pharmacology of endometrin and pregnancy outcome information [ see clinical pharmacology (12) and clinical studies sections (14) ].

5. the pharmacokinetic results are summarized in table 2. table 2: mean (±standard deviation) serum progesterone pharmacokinetic parameters pharmacokinetic parameter (unit) endometrin 100 mg twice daily (n=6) endometrin 100 mg three times daily (n=6) c max maximum progesterone serum concentration. t max time to maximum progesterone serum concentration. c avg average progesterone serum concentration. auc 0-24 area under the drug concentration versus time curve from 0-24 hours post dose. c min minimum progesterone serum concentration. single dosing c max (ng/ml) 17.0 ± 6.5 19.8 ± 7.2 t max (hr) 24.0 ± 0.0 17.3 ± 7.4 auc 0-24 (ng∙hr/ml) 217 ± 113 284 ± 143 day 5 of multiple dosing c max (ng/ml) 18.5 ± 5.5 24.1 ± 5.6 t max (hr) 18.0 ± 9.4 18.0 ± 9.4 c min (ng/ml) 8.9 ± 4.5 10.9 ± 6.7 c avg (ng/ml) 14.0 ± 4.8 15.9 ± 4.3 auc 0-24 (ng∙hr/ml) 327 ± 127 436 ± 106 distribution progesterone is approximately 96% to 99% bound to serum proteins, primarily to serum albumin and corticosteroid binding globulin. metabolism progesterone is metabolized primarily by the liver, largely to pregnanediols and pregnanolones. pregnanediols and pregnanolones are conjugated in the liver to glucuronide and sulfate metabolites. progesterone metabolites that are excreted in the bile may be deconjugated and may be further metabolized in the gut via reduction, dehydroxylation, and epimerization. excretion progesterone undergoes renal and biliary elimination. following injection of labeled progesterone, 50-60% of the excretion of metabolites occurs via the kidney; approximately 10% occurs via the bile and feces. overall recovery of the labeled material accounts for 70% of an administered dose. only a small portion of unchanged progesterone is excreted in the bile .

ntration versus time curve from 0-24 hours post dose. c min minimum progesterone serum concentration. single dosing c max (ng/ml) 17.0 ± 6.5 19.8 ± 7.2 t max (hr) 24.0 ± 0.0 17.3 ± 7.4 auc 0-24 (ng∙hr/ml) 217 ± 113 284 ± 143 day 5 of multiple dosing c max (ng/ml) 18.5 ± 5.5 24.1 ± 5.6 t max (hr) 18.0 ± 9.4 18.0 ± 9.4 c min (ng/ml) 8.9 ± 4.5 10.9 ± 6.7 c avg (ng/ml) 14.0 ± 4.8 15.9 ± 4.3 auc 0-24 (ng∙hr/ml) 327 ± 127 436 ± 106 distribution progesterone is approximately 96% to 99% bound to serum proteins, primarily to serum albumin and corticosteroid binding globulin. metabolism progesterone is metabolized primarily by the liver, largely to pregnanediols and pregnanolones. pregnanediols and pregnanolones are conjugated in the liver to glucuronide and sulfate metabolites. progesterone metabolites that are excreted in the bile may be deconjugated and may be further metabolized in the gut via reduction, dehydroxylation, and epimerization. excretion progesterone undergoes renal and biliary elimination. following injection of labeled progesterone, 50-60% of the excretion of metabolites occurs via the kidney; approximately 10% occurs via the bile and feces. overall recovery of the labeled material accounts for 70% of an administered dose. only a small portion of unchanged progesterone is excreted in the bile .

n endometrin and the active comparator excluded a difference greater than 10%) to the ongoing pregnancy rate for subjects treated with the active comparator. the results of this study are shown in table 3. table 3: ongoing pregnancy rates ongoing pregnancy defined as the presence of at least one fetal heartbeat seen on ultrasound at 6 weeks post-embryo transfer. in patients receiving endometrin for luteal supplementation and early pregnancy while in an assisted reproductive technology treatment program endometrin 100 mg twice daily endometrin 100 mg three times daily number of subjects 404 404 ongoing pregnancy: n (%) 156 (39%) 171 (42%) 95% confidence interval of pregnancy rate [33.8, 43.6] [37.5, 47.3] pregnancy rate percentage difference between endometrin and comparator -3.6% 0.1% 95% confidence interval for difference vs comparator [-10.3, 3.2] [-6.7, 6.9] subjects participating in the study were stratified at randomization by age and ovarian reserve (as measured by serum fsh levels). the ongoing pregnancy rates for these subgroups are shown in table 4. table 4: ongoing pregnancy rates in age- and ovarian reserve-defined subgroups receiving endometrin for luteal supplementation and early pregnancy while in an assisted reproductive technology treatment program endometrin 100 mg twice daily endometrin 100 mg three times daily subjects age < 35 years (n) 247 247 ongoing pregnancy: n (%) 111 (45%) 117 (47%) pregnancy rate percentage difference between endometrin and comparator 0.5% 2.9% 95% confidence interval for difference vs. comparator [-8.3, 9.3] [-5.9, 11.7] subjects 35-42 years of age (n) 157 157 ongoing pregnancy: n (%) 45 (28%) 54 (34%) pregnancy rate percentage difference between endometrin and comparator -10.1% -4.4% 95% confidence interval for difference vs. comparator [-20.3, 0.3] [-14.9, 6.3] subjects with fsh < 10 iu/l (n) 350 347 ongoing pregnancy: n (%) 140 (40%) 150 (43%) pregnancy rate percentage difference between endometrin and comparator -2.0% 1.2% 95% confidence interval for difference vs. comparator [-9.3, 5.3] [-6.1, 8.5] subjects with fsh between 10 and 15 iu/l (n) 46 51 ongoing pregnancy: n (%) 16 (35%) 20 (39%) pregnancy rate percentage difference between endometrin and comparator -12.2% -7.7% 95% confidence interval for difference vs. comparator [-31.0, 7.7] [-26.6, 11.6] in subjects under the age of 35 or with serum fsh levels less than 10 iu/l, results from both dosing regimens were non-inferior to the results from the comparator with respect to ongoing pregnancy rates. in women age 35 and older and in women with serum fsh levels between 10 and 15 iu/l, the results with respect to ongoing pregnancy rates for both dosing regimens of endometrin did not reach the criteria for non-inferiority. subjects who became pregnant received study medication for a total of 10 weeks. patients over 34 kg/m 2 were not studied. the efficacy of endometrin in this patient group is unknown.

ding that has not been evaluated by a doctor. currently have or have had liver problems or cancer of the breast or genital organs. have or have had blood clots in the legs, lungs, eyes, or elsewhere in your body. endometrin may not be right for you. before starting endometrin, tell your doctor about all your health problems . tell your doctor about all the medicines you take including prescription and nonprescription medicines, vaginal products, vitamins, and herbal supplements. some medicines may affect endometrin. know what medicines you take. keep a list of your medicines to show to the doctor and pharmacist. how should i use endometrin? use endometrin exactly as prescribed. the usual dose of endometrin is one insert placed in your vagina 2 to 3 times a day for up to a total of 10 weeks, unless your healthcare provider advises otherwise. place an endometrin insert in your vagina with the disposable applicator provided. follow the steps below: unwrap the applicator. do not use if the contents or packaging are visibly damaged. put one insert in the space provided at the end of the applicator. the insert should fit snugly and not fall out. place applicator with the insert into the vagina while you are standing, sitting, or when lying on your back with your knees bent. gently place the thin end of the applicator well into the vagina. push the plunger to release the insert. remove the applicator and throw it away in the trash. other information for using endometrin if you forget a dose of endometrin, take the dose as soon as you remember, but do not use more than your daily dose. call your doctor if you use too much endometrin. do not use any other vaginal products when you are using endometrin. what are the possible side effects of endometrin? common side effects seen with art and endometrin included pelvic pain after surgery, abdominal pain, nausea, and swollen ovaries (ovarian hyperstimulation syndrome). other reported side effects included abdominal bloating, headache, urinary infections, uterine cramping, constipation, vomiting, tiredness, and vaginal bleeding. vaginal products with progesterone may also cause vaginal irritation, burning, and discharge. serious risks of progesterone progesterone can increase your chance of getting blood clots. blood clots can be serious and lead to death. serious blood clots include those in the: legs (thrombophlebitis) lungs (pulmonary embolus) eyes (blindness) heart (heart attack) brain (stroke) call your doctor or get medical help right away if you have: persistent pain in the lower leg (calf) sudden shortness of breath coughing up blood sudden blindness, partial or complete severe chest pain sudden, severe headache, vomiting, dizziness, or fainting weakness in an arm or leg, or trouble speaking yellowing of the skin and/or white of the eyes indicating possible liver problem other risks of progesterone use include: headache breast tenderness bloating or fluid retention mood swings and depression irritability drowsiness call your doctor immediately if you have abnormal vaginal bleeding. these are not all the side effects with endometrin. ask your doctor or pharmacist for more information. how should i store endometrin? store endometrin at room temperature, 20 - 25°c (68 - 77°f); excursions permitted between 15 - 30°c (59 - 86°f). do not use endometrin after the expiration date that is printed on the carton. keep endometrin and all medicines out of the reach of children. general information about endometrin medicines are sometimes prescribed for purposes other than those listed in a patient information leaflet. do not use endometrin for a condition for which it was not prescribed. do not give endometrin to other women, even if they have the same condition as you do. it may harm them. this leaflet summarizes the most important information about endometrin. if you would like more information, talk with your doctor. you can ask your doctor or pharmacist for information about endometrin that was written for healthcare professionals. for more information call ferring pharmaceuticals inc. at 1-(888)-ferring or 1-(888)-337-7464. what are the ingredients in endometrin? active ingredient: progesterone inactive ingredients: lactose monohydrate, polyvinylpyrrolidone, adipic acid, sodium bicarbonate, sodium lauryl sulfate, magnesium stearate, pregelatinized starch, and colloidal silicon dioxide manufactured for: ferring pharmaceuticals inc. parsippany, nj 07054 6485-03 revised: 01/2018