diabetic patients should be carefully observed while receiving progestin therapy.

dy col1620-f01 (n = 139) body as a whole abdominal pain 12% perineal pain female 17% central and peripheral nervous system headache 17% gastro-intestinal system constipation 27% diarrhea 8% nausea 22% vomiting 5% musculo-skeletal system arthralgia 8% psychiatric depression 11% libido decreased 10% nervousness 16% somnolence 27% reproductive, female breast enlargement 40% dyspareunia 6% urinary system nocturia 13% secondary amenorrhea in three studies, 127 women with secondary amenorrhea received estrogen replacement therapy and crinone 4% or 8% every other day for six doses. treatment-emergent adverse events during estrogen and crinone treatment that occurred in 5% or more of women are shown in table 5. table 5 treatment-emergent adverse events in ≥ 5% of women receiving estrogen treatment and crinone every other day studies col1620-004us, col1620-005us, col1620-009us estrogen + crinone 4% n = 62 estrogen + crinone 8% n = 65 body as a whole abdominal pain 3 (5%) 6 (9%) appetite increased 3 (5%) 5 (8%) bloating 8 (13%) 8 (12%) cramps nos 12 (19%) 17 (26%) fatigue 13 (21%) 14 (22%) central and peripheral nervous system headache 12 (19%) 10 (15%) gastro-intestinal system nausea 5 (8%) 4 (6%) musculo-skeletal system back pain 5 (8%) 2 (3%) myalgia 5 (8%) 0 (0%) psychiatric depression 12 (19%) 10 (15%) emotional lability 14 (23%) 14 (22%) sleep disorder 11 (18%) 12 (18%) reproductive, female vaginal discharge 7 (11%) 2 (3%) resistance mechanism upper respiratory tract infection 3 (5%) 5 (8%) skin and appendages pruritus genital 1 (2%) 4 (6%)

rinone 8% once daily beginning within 24 hours of embryo transfer and continuing through day 30 post-transfer. clinical pregnancies assessed at day 90 post-transfer were seen in 36 (26%) of women. thirty-two women (23%) delivered newborns and four women (3%) had spontaneous abortions. of the 47 newborns delivered, one had a teratoma associated with a cleft palate; one had respiratory distress syndrome; 44 were apparently normal and one was lost to follow-up.

approximately 25 to 50 hours, and an elimination half-life of 5 to 20 minutes. therefore, the pharmacokinetics of crinone are rate-limited by absorption rather than by elimination. the bioavailability of progesterone in crinone was determined relative to progesterone administered intramuscularly. in a single dose crossover study, 20 healthy, estrogenized postmenopausal women received 45 mg or 90 mg progesterone vaginally in crinone 4% or crinone 8%, or 45 mg or 90 mg progesterone intramuscularly. the pharmacokinetic parameters (mean ± standard deviation) are shown in table 1. table 1 single dose relative bioavailability crinone 4% 45 mg intramuscular progesterone crinone 8% 90 mg intramuscular progesterone c max (ng/ml) 13.15 ± 6.49 39.06 ± 13.68 14.87 ± 6.32 53.76 ± 14.9 c avg 0-24 (ng/ml) 6.94 ± 4.24 22.41 ± 4.92 6.98 ± 3.21 28.98 ± 8.75 auc 0-96 (ng∙hr/ml) 288.63 ± 273.72 806.26 ± 102.75 296.78 ± 129.90 1378.91 ± 176.39 t max (hr) 5.6 ± 1.84 8.2 ± 6.43 6.8 ± 3.3 9.2 ± 2.7 t 1/2 (hr) 55.13 ± 28.04 28.05 ± 16.87 34.8 ± 11.3 19.6 ± 6.0 f (%) 27.6 19.8 c max - maximum progesterone serum concentration c avg 0-24 - average progesterone serum concentration over 24 hours auc 0-96 - area under the drug concentration versus time curve from 0-96 hours post dose t max - time to maximum progesterone concentration t 1/2 - elimination half-life f - relative bioavailability the multiple dose pharmacokinetics of crinone 4% and crinone 8% administered every other day and crinone 8% administered daily or twice daily for 12 days were studied in 10 healthy, estrogenized postmenopausal women in two separate studies. steady state was achieved within the first 24 hours after initiation of treatment. the pharmacokinetic parameters (mean ± standard deviation) after the last administration of crinone 4% or 8% derived from these studies are shown in table 2. table 2 multiple dose pharmacokinetics assisted reproductive technology secondary amenorrhea daily dosing 8% twice daily dosing 8% every other day dosing 4% every other day dosing 8% c max (ng/ml) 15.97± 5.05 14.57 ± 4.49 13.21± 9.46 13.67 ± 3.58 c avg (ng/ml) 8.99 ± 3.53 11.6 ± 3.47 4.05 ± 2.85 6.75 ± 2.83 t max (hr) 5.40 ± 0.97 3.55 ± 2.48 6.67 ± 3.16 7.00 ± 2.88 auc 0-t (ng∙hr/ml) 391.98 ±153.28 138.72 ± 41.58 242.15 ± 167.88 438.36 ± 223.36 t 1/2 (hr) 45.00 ± 34.70 25.91 ± 6.15 49.87 ± 31.20 39.08 ± 12.88 c max -maximum progesterone serum concentration c avg -average progesterone serum concentration t max -time to maximum progesterone concentration auc 0-t -area under the drug concentration versus time curve t 1/2 -elimination half-life distribution progesterone is extensively bound to serum proteins (~ 96-99%), primarily to serum albumin and corticosteroid binding globulin. metabolism the major urinary metabolite of oral progesterone is 5β-pregnan-3α, 20α-diol glucuronide which is present in plasma in the conjugated form only. plasma metabolites also include 5β-pregnan-3α-ol-20-one (5β-pregnanolone) and 5α-pregnan-3α-ol-20-one (5α-pregnanolone). excretion progesterone undergoes both biliary and renal elimination. following an injection of labeled progesterone, 50-60% of the excretion of progesterone metabolites occurs via the kidney; approximately 10% occurs via the bile and feces, the second major excretory pathway. overall recovery of labeled material accounts for 70% of an administered dose, with the remainder of the dose not characterized with respect to elimination. only a small portion of unchanged progesterone is excreted in the bile.

8 ± 3.21 28.98 ± 8.75 auc 0-96 (ng∙hr/ml) 288.63 ± 273.72 806.26 ± 102.75 296.78 ± 129.90 1378.91 ± 176.39 t max (hr) 5.6 ± 1.84 8.2 ± 6.43 6.8 ± 3.3 9.2 ± 2.7 t 1/2 (hr) 55.13 ± 28.04 28.05 ± 16.87 34.8 ± 11.3 19.6 ± 6.0 f (%) 27.6 19.8 c max - maximum progesterone serum concentration c avg 0-24 - average progesterone serum concentration over 24 hours auc 0-96 - area under the drug concentration versus time curve from 0-96 hours post dose t max - time to maximum progesterone concentration t 1/2 - elimination half-life f - relative bioavailability the multiple dose pharmacokinetics of crinone 4% and crinone 8% administered every other day and crinone 8% administered daily or twice daily for 12 days were studied in 10 healthy, estrogenized postmenopausal women in two separate studies. steady state was achieved within the first 24 hours after initiation of treatment. the pharmacokinetic parameters (mean ± standard deviation) after the last administration of crinone 4% or 8% derived from these studies are shown in table 2. table 2 multiple dose pharmacokinetics assisted reproductive technology secondary amenorrhea daily dosing 8% twice daily dosing 8% every other day dosing 4% every other day dosing 8% c max (ng/ml) 15.97± 5.05 14.57 ± 4.49 13.21± 9.46 13.67 ± 3.58 c avg (ng/ml) 8.99 ± 3.53 11.6 ± 3.47 4.05 ± 2.85 6.75 ± 2.83 t max (hr) 5.40 ± 0.97 3.55 ± 2.48 6.67 ± 3.16 7.00 ± 2.88 auc 0-t (ng∙hr/ml) 391.98 ±153.28 138.72 ± 41.58 242.15 ± 167.88 438.36 ± 223.36 t 1/2 (hr) 45.00 ± 34.70 25.91 ± 6.15 49.87 ± 31.20 39.08 ± 12.88 c max -maximum progesterone serum concentration c avg -average progesterone serum concentration t max -time to maximum progesterone concentration auc 0-t -area under the drug concentration versus time curve t 1/2 -elimination half-life distribution progesterone is extensively bound to serum proteins (~ 96-99%), primarily to serum albumin and corticosteroid binding globulin. metabolism the major urinary metabolite of oral progesterone is 5β-pregnan-3α, 20α-diol glucuronide which is present in plasma in the conjugated form only. plasma metabolites also include 5β-pregnan-3α-ol-20-one (5β-pregnanolone) and 5α-pregnan-3α-ol-20-one (5α-pregnanolone). excretion progesterone undergoes both biliary and renal elimination. following an injection of labeled progesterone, 50-60% of the excretion of progesterone metabolites occurs via the kidney; approximately 10% occurs via the bile and feces, the second major excretory pathway. overall recovery of labeled material accounts for 70% of an administered dose, with the remainder of the dose not characterized with respect to elimination. only a small portion of unchanged progesterone is excreted in the bile.

time they were administered only leuprolide acetate to suppress remaining ovarian function. the pre-pilot cycle, pilot cycle, pre-donor egg cycle, and donor egg cycle each lasted approximately 34 days. the third phase of the study consisted of a 10-week treatment period to maintain a pregnancy until placental autonomy was achieved. sixty-one women received crinone 8% as part of the pilot cycle to determine their endometrial response. of the 55 evaluable endometrial biopsies in the crinone 8% group performed on day 25 to 27, all were histologically "in-phase", consistent with luteal phase biopsy specimens of menstruating women at comparable time intervals. fifty-four women who received crinone 8% and had a histologically "in-phase" biopsy received a donor oocyte transfer. among these 54 crinone-treated women, clinical pregnancies (assessed about week 10 after transfer by clinical examination, ultrasound and/or ß-hcg levels) occurred in 26 women (48%). seventeen women (31%) delivered a total of 25 newborns, seven women (13%) had spontaneous abortions and two women (4%) had elective abortions. in a second study (col1620-f01), crinone 8% was used in luteal phase support of women with tubal or idiopathic infertility due to endometriosis and normal ovulatory cycles, undergoing in vitro fertilization ("ivf") procedures. all women received a gnrh analog to suppress endogenous progesterone, human menopausal gonadotropins, and human chorionic gonadotropin. in this multi-center, open-label study, 139 women (aged 22-38 years) received crinone 8% once daily beginning within 24 hours of embryo transfer and continuing through day 30 post-transfer. clinical pregnancies assessed at day 90 post-transfer were seen in 36 (26%) of women. thirty-two women (23%) delivered newborns and four women (3%) had spontaneous abortions. (see precautions, pregnancy ) secondary amenorrhea in three parallel, open-label studies (col1620-004us, col1620-005us, col1620-009us), 127 women (aged 18-44) with hypothalamic amenorrhea or premature ovarian failure were randomized to receive either crinone 4% (n = 62) or crinone 8% (n = 65). all women were treated with either conjugated estrogens 0.625 mg daily (n = 100) or transdermal estradiol (delivering 50 mcg/day) twice weekly (n = 27). estrogen therapy was continuous for the entire three 28-day cycle studies. at day 15 of the second cycle (six weeks after initiating estrogen replacement), women who demonstrated adequate response to estrogen therapy (by ultrasound) and who continued to be amenorrheic received crinone every other day for six doses (day 15 through day 25 of the cycle). in cycle 2, crinone 4% induced bleeding in 79% of women and crinone 8% induced bleeding in 77% of women. in the third cycle, estrogen was continued and crinone was administered every other day beginning on day 15 for six doses. on day 24 an endometrial biopsy was performed. in 53 women who received crinone 4%, biopsy results were as follows: 7% proliferative, 40% late secretory, 19% mid secretory, 13% early secretory, 7% atrophic, 6% menstrual endometrium, 6% inactive endometrium and 2% negative endometrium. in 54 women who received crinone 8%, biopsy results were as follows: 44% late secretory, 19% mid secretory, 11% early secretory, 19% atrophic, 5% menstrual endometrium and 2% "oral contraceptive like" endometrium.

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ormones that helps to prepare the lining of your uterus so that it is ready to receive and nourish a fertilized egg and to continue a pregnancy. if you are undergoing art treatment and your doctor has determined your body does not produce enough progesterone on its own, crinone may be prescribed to increase your progesterone. if pregnancy occurs, crinone may be supplemented for 10 to 12 weeks until production of progesterone by the placenta is adequate. who should not use crinone? do not start using crinone if you: are allergic to progesterone, progesterone-like drugs, or any of the inactive ingredients in the gel (ask a pharmacist if you are not sure about the inactive ingredients in crinone). have unusual vaginal bleeding which has not been evaluated by a doctor. have or have had a liver disease. have or have had cancer of the breast or genital organs. have had a miscarriage and your physician suspects some tissue is still in the uterus. have or have had blood clots in the legs, lungs, eyes, or elsewhere. what are the possible side effects of crinone? serious side effects include: blood clots. progestational drug products may increase your chance of having blood clots in your blood vessels. blood clots can cause: blood vessel problems (thrombophlebitis) stroke loss of your arm or leg blood clot in your lungs (pulmonary embolus) heart attack death birth defects. abdominal wall defect and cleft palate have been reported with crinone use in early pregnancy. it is not known if these defects were caused by crinone. call your healthcare provider right away if you get any of the following warning signs or any other unusual symptoms that concern you: pains in the calves or chest, a sudden shortness of breath or coughing blood indicating possible clots in the legs, heart, or lungs. severe headache or vomiting, dizziness, faintness, or changes in vision or speech, weakness or numbness of an arm or leg indicating possible clots in the brain or eye. common side effects include: abdominal pain perineal pain (the perineum is the area between the vagina and the rectum) cramps bloating headache fatigue increased appetite constipation diarrhea nausea joint pain depression mood swings sleep disorder nervousness decreased libido breast enlargement excessive urination at night vaginal discharge upper respiratory tract infection these are not all the possible side effects of crinone. for more information, ask your healthcare provider or pharmacist for advice about side effects. to report suspected adverse reactions, contact allergan at 1-800-678-1605 or fda at 1-800-fda-1088 or www.fda.gov/medwatch . how should i use crinone? use as directed by your healthcare provider. read the instructions for use included in this leaflet for information on the right way to use crinone. additional information about crinone you may see a small amount of white discharge that may look like a vaginal discharge. this discharge may be caused by gel that can remain in your vagina, even several days after use. gel discharge from your vagina is normal, but if you are concerned, talk to your healthcare provider. if you miss a dose of crinone, use it as soon as you remember. do not use more crinone than the dose prescribed by your doctor. talk to your healthcare provider about whether to use other vaginal medicines when you are using crinone. general information about the safe and effective use of crinone medicines are sometimes prescribed for purposes other than those listed in a patient information leaflet. do not use crinone for another condition. your doctor has prescribed this drug for you and you alone. do not give this drug to anyone else, even if they have the same condition. keep crinone out of the reach of children this leaflet provides the most important information about crinone. if you would like more information, talk with your healthcare provider or pharmacist. you can ask for information about crinone that is written for health professionals. you can get more information by calling the toll free number 1-888-776-4358 or visit www.crinoneusa.com . what are the ingredients in crinone? crinone contains either 45 mg (4% gel) or 90 mg (8% gel) of progesterone in a base containing glycerin, light mineral oil, polycarbophil, carbomer homopolymer type b, hydrogenated palm oil glyceride, sorbic acid, purified water and may contain sodium hydroxide. how should i store crinone? store crinone at room temperature between 68°f to 77°f (20°c to 25°c). do not use crinone after the expiration date printed on the box.