, vaginal discharge is the most frequently reported treatment-emergent adverse reaction in the intrarosa treatment group with an incidence of ≥ 2 percent and greater than reported in the placebo treatment group. there were 38 cases in 665 participating postmenopausal women (5.71 percent) in the intrarosa treatment group compared to 17 cases in 464 participating postmenopausal women (3.66 percent) in the placebo treatment group. in a 52-week non-comparative clinical trial [92% - white caucasian non-hispanic women, 6% - black or african american women, and 2% - "other" women, average age 57.9 years of age (range 43 to 75 years of age)], vaginal discharge and abnormal pap smear at 52 weeks were the most frequently reported treatment-emergent adverse reaction in women receiving intrarosa with an incidence of ≥ 2 percent. there were 74 cases of vaginal discharge (14.2 percent) and 11 cases of abnormal pap smear (2.1 percent) in 521 participating postmenopausal women. the eleven (11) cases of abnormal pap smear at 52 weeks include one (1) case of low-grade squamous intraepithelial lesion (lsil), and ten (10) cases of atypical cells of undetermined significance (ascus).

% - white caucasian non-hispanic women, 6% - black or african american women, and 2% - "other" women, average age 57.9 years of age (range 43 to 75 years of age)], vaginal discharge and abnormal pap smear at 52 weeks were the most frequently reported treatment-emergent adverse reaction in women receiving intrarosa with an incidence of ≥ 2 percent. there were 74 cases of vaginal discharge (14.2 percent) and 11 cases of abnormal pap smear (2.1 percent) in 521 participating postmenopausal women. the eleven (11) cases of abnormal pap smear at 52 weeks include one (1) case of low-grade squamous intraepithelial lesion (lsil), and ten (10) cases of atypical cells of undetermined significance (ascus).

of prasterone has not been studied.

intrarosa (n=10) prasterone c max (ng/ml) 1.60 (±0.95) 4.42 (±1.49) auc 0-24 (ng·h/ml) 24.82 (±14.31) 56.17 (±28.27) testosterone c max (ng/ml) 0.12 (±0.04) 1 0.15 (±0.05) auc 0-24 (ng·h/ml) 2.58 (±0.94) 1 2.79 (±0.94) estradiol c max (pg/ml) 3.33 (±1.31) 5.04 (±2.68) auc 0-24 (pg·h/ml) 66.49 (±20.70) 96.93 (±52.06) figure 1. serum concentrations of prasterone (a), testosterone (b), and estradiol (c) measured over a 24h period on day 7 following daily administration of placebo or intrarosa (mean ± sd). in two primary efficacy trials, daily administration of intrarosa vaginal insert for 12 weeks increased mean serum c trough of prasterone and its metabolites testosterone and estradiol by 47%, 21% and 19% from baseline, respectively. this comparison based on c trough may underestimate the magnitude of increase in prasterone and metabolites’ exposure because it does not take into account the overall concentration-time profile following administration of intrarosa. metabolism exogenous prasterone is metabolized in the same manner as endogenous prasterone. human steroidogenic enzymes such as hydroxysteroid dehydrogenases, 5α-reductases and aromatases transform prasterone into androgens and estrogens. figure 1

) 3.33 (±1.31) 5.04 (±2.68) auc 0-24 (pg·h/ml) 66.49 (±20.70) 96.93 (±52.06) figure 1. serum concentrations of prasterone (a), testosterone (b), and estradiol (c) measured over a 24h period on day 7 following daily administration of placebo or intrarosa (mean ± sd). in two primary efficacy trials, daily administration of intrarosa vaginal insert for 12 weeks increased mean serum c trough of prasterone and its metabolites testosterone and estradiol by 47%, 21% and 19% from baseline, respectively. this comparison based on c trough may underestimate the magnitude of increase in prasterone and metabolites’ exposure because it does not take into account the overall concentration-time profile following administration of intrarosa. metabolism exogenous prasterone is metabolized in the same manner as endogenous prasterone. human steroidogenic enzymes such as hydroxysteroid dehydrogenases, 5α-reductases and aromatases transform prasterone into androgens and estrogens. figure 1

eunia, the percentage of vaginal superficial cells, the percentage of parabasal cells, and vaginal ph. the second clinical trial (trial 2) was a 12-week randomized, double-blind and placebo-controlled trial that enrolled 558 generally healthy postmenopausal women between 40 to 80 years of age (mean 59.5 years) who, at baseline, had identified moderate to severe dyspareunia as their most bothersome symptom of vulvar and vaginal atrophy. in addition to dyspareunia, women had ≤ 5% superficial cells on vaginal smear and a vaginal ph > 5. women were randomized in a 2:1 ratio to receive once daily vaginal insert containing 6.5 mg intrarosa (n=376) or placebo (n=182). the primary endpoints and study conduct were the same or similar to those in trial 1. the primary efficacy results obtained in the intent-to-treat (itt) population in trial 1 are shown in table 2. table 2: efficacy summary in primary 12-week trial 1: itt population (locf) 1 difference from placebo =intrarosa (week 12 mean – baseline mean) – placebo (week 12 mean – baseline mean). 2 ancova: treatment as the main factor and baseline value as the covariate. placebo n = 77 intrarosa n = 81 dyspareunia baseline mean severity week 12 mean severity mean change in severity (sd) difference from placebo 1 p-value 2 2.58 1.71 -0.87 (0.95) - - 2.63 1.36 -1.27 (0.99) -0.40 0.0132 % superficial cells baseline mean week 12 mean mean change (sd) difference from placebo 1 p-value 2 0.73 1.64 0.91 (2.69) - - 0.68 6.30 5.62 (5.49) 4.71 <0.0001 % parabasal cells baseline mean week 12 mean mean change (sd) difference from placebo 1 p-value 2 68.48 66.86 -1.62 (28.22) - - 65.05 17.65 -47.40 (42.50) -45.77 <0.0001 vaginal ph baseline mean week 12 mean mean change (sd) difference from placebo 1 p-value 2 6.51 6.31 -0.21 (0.69) - - 6.47 5.43 -1.04 (1.00) -0.83 <0.0001 the primary efficacy results obtained in the intent-to-treat (itt) population in trial 2 are shown in table 3. table 3: efficacy summary in primary 12-week trial 2: itt population (locf) 1 difference from placebo =intrarosa (week 12 mean – baseline mean) – placebo (week 12 mean – baseline mean). 2 ancova: treatment as the main factor and baseline value as the covariate. placebo n = 157 intrarosa n = 325 dyspareunia baseline mean severity week 12 mean severity mean change in severity (sd) difference from placebo 1 p-value 2 2.56 1.50 -1.06 (1.02) - - 2.54 1.13 -1.42 (1.00) -0.35 0.0002 % superficial cells baseline mean week 12 mean mean change (sd) difference from placebo 1 p-value 2 1.04 2.78 1.75 (3.33) - - 1.02 11.22 10.20 (10.35) 8.46 <0.0001 % parabasal cells baseline mean week 12 mean mean change (sd) difference from placebo 1 p-value 2 51.66 39.68 -11.98 (29.58) - - 54.25 12.74 -41.51 (36.26) -29.53 <0.0001 vaginal ph baseline mean week 12 mean mean change (sd) difference from placebo 1 p-value 2 6.32 6.05 -0.27 (0.74) - - 6.34 5.39 -0.94 (0.94) -0.67 <0.0001

ast menopause. it is not known if intrarosa vaginal inserts will harm your unborn baby. are breastfeeding or plan to breastfeed. intrarosa vaginal inserts are only for use in women who are past menopause. it is not known if intrarosa passes into your breast milk. tell your healthcare provider about all the medicines you take, including prescription and over-the-counter medicines, vitamins, and herbal supplements. how should i use intrarosa vaginal inserts? see the instructions for use at the end of this patient information for detailed instructions about the right way to use intrarosa vaginal inserts. use intrarosa vaginal inserts exactly how your healthcare provider tells you to use it. place 1 intrarosa vaginal insert in your vagina one time each day at bedtime, using the applicator that comes with intrarosa vaginal inserts. what are the possible side effects of intrarosa vaginal inserts? the most common side effects of intrarosa vaginal inserts are vaginal discharge and changes on pap smear. these are not all of the possible side effects of intrarosa vaginal inserts. call your doctor for medical advice about side effects. you may report side effects to fda at 1-800-fda-1088. how should i store intrarosa vaginal inserts? store intrarosa vaginal inserts between 41°f to 86°f (5°c to 30°c). intrarosa vaginal inserts can be stored at room temperature or in the refrigerator. keep intrarosa vaginal inserts and all medicines out of the reach of children. general information about the safe and effective use of intrarosa vaginal inserts. medicines are sometimes prescribed for purposes other than those listed in a patient information leaflet. do not use intrarosa vaginal inserts for a condition for which it was not prescribed. do not give intrarosa vaginal inserts to other people, even if they have the same symptoms that you have. it may harm them. you can ask your pharmacist or healthcare provider for information about intrarosa vaginal inserts that is written for health professionals. what are the ingredients in intrarosa vaginal inserts? active ingredient: prasterone inactive ingredient: off-white hard fat (witepsol) for more information, go to www.intrarosa.com or call millicent u.s. inc at 1-877-810-2101.