te amount of giapreza in a normal saline (0.9% sodium chloride) infusion bag to achieve the desired final concentration of 5,000 ng/ml or 10,000 ng/ml. discard vial and any unused portion of the drug product after use. diluted solution may be stored at room temperature (20°c to 25°c [68°f to 77°f]) or under refrigeration (2°c to 8°c [36°f to 46°f]). discard prepared solution after 24 hours at room temperature or under refrigeration. 2.2. administration the recommended starting dosage of giapreza is 20 nanograms (ng)/kg/min via continuous intravenous infusion. administration through a central venous line is recommended. monitor blood pressure response and titrate giapreza as frequently as every 5 minutes by increments of up to 15 ng/kg/min as needed to achieve or maintain target blood pressure. do not exceed 80 ng/kg/min during the first 3 hours of treatment. maintenance dose should not exceed 40 ng/kg/min. doses as low as 1.25 ng/kg/min may be used. once the underlying shock has sufficiently improved, down-titrate every 5 to 15 minutes by increments of up to 15 ng/kg/min based on blood pressure.

a than with placebo. table 1: adverse reactions occurring in ≥ 4% of patients treated with giapreza and ≥ 1.5% more often than in placebo-treated patients in athos-3 adverse event giapreza n=163 placebo n=158 thromboembolic events including arterial and venous thrombotic events 21 (12.9%) 8 (5.1%) deep vein thrombosis 7 (4.3%) 0 (0.0%) thrombocytopenia 16 (9.8%) 11 (7.0%) tachycardia 14 (8.6%) 9 (5.7%) fungal infection 10 (6.1%) 2 (1.3%) delirium 9 (5.5%) 1 (0.6%) acidosis 9 (5.5%) 1 (0.6%) hyperglycemia 7 (4.3%) 4 (2.5%) peripheral ischemia 7 (4.3%) 4 (2.5%)

tality. 8.2. lactation risk summary it is not known whether giapreza is present in human milk. no data are available on the effects of angiotensin ii on the breastfed child or the effects on milk production. 8.4. pediatric use the safety and efficacy of giapreza in pediatric patients have not been established. 8.5. geriatric use in athos-3, 48% of the total patient population was aged 65 years and older. there was no significant difference in safety or efficacy between patients less than 65 and those 65 years or older when treated with giapreza .

y approximately 40%. distribution: no specific studies were conducted that examined the distribution of giapreza. metabolism and excretion: no specific studies were conducted that examined the metabolism and excretion of giapreza. the plasma half-life of iv administered angiotensin ii is less than one minute. it is metabolized by aminopeptidase a and angiotensin converting enzyme 2 to angiotensin-(2-8) [angiotensin iii] and angiotensin-(1-7), respectively in plasma, erythrocytes and many of the major organs (i.e., intestine, kidney, liver and lung). angiotensin ii type 1 receptor (at1) mediated activity of angiotensin iii is approximately 40% of angiotensin ii; however, aldosterone synthesis activity is similar to angiotensin ii. angiotensin-(1-7) exerts the opposite effects of angiotensin ii on at1 receptors and causes vasodilation. specific populations no formal pharmacokinetic studies were conducted with giapreza in the following specific populations. renal impairment the clearance of angiotensin ii is not dependent on renal function. therefore, the pharmacokinetics of giapreza are not expected to be influenced by renal impairment. hepatic impairment the clearance of angiotensin ii is not dependent on hepatic function. therefore, the pharmacokinetics of giapreza are not expected to be influenced by hepatic impairment. age the effect of age was analyzed in the 163 patients receiving giapreza in athos-3. there were no significant differences in pharmacokinetics between age groups (< 65 years / ≥ 65 years). male and female patients the effect of sex was analyzed in the 163 patients receiving giapreza in athos-3. there were no significant differences in pharmacokinetics between male and female patients.

sin ii; however, aldosterone synthesis activity is similar to angiotensin ii. angiotensin-(1-7) exerts the opposite effects of angiotensin ii on at1 receptors and causes vasodilation. specific populations no formal pharmacokinetic studies were conducted with giapreza in the following specific populations. renal impairment the clearance of angiotensin ii is not dependent on renal function. therefore, the pharmacokinetics of giapreza are not expected to be influenced by renal impairment. hepatic impairment the clearance of angiotensin ii is not dependent on hepatic function. therefore, the pharmacokinetics of giapreza are not expected to be influenced by hepatic impairment. age the effect of age was analyzed in the 163 patients receiving giapreza in athos-3. there were no significant differences in pharmacokinetics between age groups (< 65 years / ≥ 65 years). male and female patients the effect of sex was analyzed in the 163 patients receiving giapreza in athos-3. there were no significant differences in pharmacokinetics between male and female patients.

e time of study drug administration, 97% of subjects were receiving norepinephrine, 67% vasopressin, 15% phenylephrine, 13% epinephrine, and 2% dopamine. 83% of subjects had received two or more vasopressors and 47% three or more vasopressors prior to study drug administration. 61% of subjects were male, 80% were white, 10% were black, and 10% were other races. the median age of subjects was 64 years (range: 22-89 years). patients requiring high doses of steroids, patients with a history of asthma or bronchospasm, and patients with raynaud's syndrome were not included. the primary endpoint was achieved by 70% of patients randomized to giapreza compared to 23% of placebo patients; p < 0.0001 (a treatment effect of 47%). figure 1 shows the results in all patients and in selected subgroups. figure 1: athos-3: primary endpoint – overall result and results in selected subgroups ne equiv = norepinephrine equivalent dose: the sum of all vasopressor doses with each vasopressor dose converted to the clinically equivalent norepinephrine dose. note: the figure above presents effects in various subgroups, all of which are baseline characteristics. the 95% confidence limits that are shown do not take into account the number of comparisons made and may not reflect the effect of a particular factor after adjustment for all other factors. apparent homogeneity or heterogeneity among groups should not be over-interpreted. in the giapreza-treated group, the median time to reach the target map endpoint was 5 minutes. the effect on map was sustained for at least the first three hours of treatment. the median dose of giapreza was 10 ng/kg/min at 30 minutes. of the 114 responders at hour 3, only 2 (1.8%) received more than 80 ng/kg/min. patients were not necessarily on maximum doses of other vasopressors at the time of randomization. the effect of giapreza when added to maximum doses of other vasopressors is unknown. mortality through day 28 was 46% on giapreza and 54% on placebo (hazard ratio 0.78; 95% confidence interval 0.57 – 1.07). giapreza-forest-plot