About The Drug Apidra aka Insulin Glulisine [rDNA origin] Inj

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Find Apidra side effects, uses, warnings, interactions and indications. Apidra is also known as Insulin Glulisine [rDNA origin] Inj.

Apidra

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About Apidra aka Insulin Glulisine [rDNA origin] Inj

What's The Definition Of The Medical Condition Apidra?

Clinical Pharmacology

CLINICAL PHARMACOLOGY Mechanism Of Action Regulation of glucose metabolism is the primary activity of insulins and insulin analogs, including insulin glulisine. Insulins lower blood glucose by stimulating peripheral glucose uptake by skeletal muscle and fat, and by inhibiting hepatic glucose production. Insulins inhibit lipolysis and proteolysis, and enhance protein synthesis. The glucose lowering activities of APIDRA and of regular human insulin are equipotent when administered by the intravenous route. After subcutaneous administration, the effect of APIDRA is more rapid in onset and of shorter duration compared to regular human insulin. [See Pharmacodynamics]. Pharmacodynamics Studies in healthy volunteers and patients with diabetes demonstrated that APIDRA has a more rapid onset of action and a shorter duration of activity than regular human insulin when given subcutaneously. In a study in patients with type 1 diabetes (n= 20), the glucose-lowering profiles of APIDRA and regular human insulin were assessed at various times in relation to a standard meal at a dose of 0.15 Units/kg. (Figure 1.) The maximum blood glucose excursion (ΔGLUmax; baseline subtracted glucose concentration) for APIDRA injected 2 minutes before a meal was 65 mg/dL compared to 64 mg/dL for regular human insulin injected 30 minutes before a meal (see Figure 1A), and 84 mg/dL for regular human insulin injected 2 minutes before a meal (see Figure 1B). The maximum blood glucose excursion for APIDRA injected 15 minutes after the start of a meal was 85 mg/dL compared to 84 mg/dL for regular human insulin injected 2 minutes before a meal (see Figure 1C). Figure 1. Serial mean blood glucose collected up to 6 hours following a single dose of APIDRA and regular human insulin. APIDRA given 2 minutes (APIDRA -pre) before the start of a meal compared to regular human insulin given 30 minutes (Regular -30 min) before start of the meal (Figure 1A) and compared to regular human insulin (Regular -pre) given 2 minutes before a meal (Figure 1B). APIDRA given 15 minutes (APIDRA -post) after start of a meal compared to regular human insulin (Regular -pre) given 2 minutes before a meal (Figure 1C). On the x-axis zero (0) is the start of a 15-minute meal. Figure 1A Figure 1B Figure C In a randomized, open-label, two-way crossover study, 16 healthy male subjects received an intravenous infusion of APIDRA or regular human insulin with saline diluent at a rate of 0.8 milliUnits/kg/min for two hours. Infusion of the same dose of APIDRA or regular human insulin produced equivalent glucose disposal at steady state. Pharmacokinetics Absorption and bioavailability Pharmacokinetic profiles in healthy volunteers and patients with diabetes (type 1 or type 2) demonstrated that absorption of insulin glulisine was faster than that of regular human insulin. In a study in patients with type 1 diabetes (n=20) after subcutaneous administration of 0.15 Units/kg, the median time to maximum concentration (Tmax) was 60 minutes (range 40 to 120 minutes) and the peak concentration (Cmax) was 83 microUnits/mL (range 40 to 131 microUnits/mL) for insulin glulisine compared to a median Tmax of 120 minutes (range 60 to 239 minutes) and a Cmax of 50 microUnits/mL (range 35 to 71 microUnits/mL) for regular human insulin. (Figure 2) Figure 2. Pharmacokinetic profiles of insulin glulisine and regular human insulin in patients with type 1 diabetes after a dose of 0.15 Units/kg. Figure 2 Insulin glulisine and regular human insulin were administered subcutaneously at a dose of 0.2 Units/kg in an euglycemic clamp study in patients with type 2 diabetes (n=24) and a body mass index (BMI) between 20 and 36 kg/m². The median time to maximum concentration (Tmax) was 100 minutes (range 40 to 120 minutes) and the median peak concentration (Cmax) was 84 microUnits/mL (range 53 to 165 microUnits/mL) for insulin glulisine compared to a median Tmax of 240 minutes (range 80 to 360 minutes) and a median Cmax of 41 microUnits/mL (range 33 to 61 microUnits/mL) for regular human insulin. (Figure 3.) Figure 3. Pharmacokinetic profiles of insulin glulisine and regular human insulin in patients with type 2 diabetes after a subcutaneous dose of 0.2 Units/kg. Figure 3 When APIDRA was injected subcutaneously into different areas of the body, the time-concentration profiles were similar. The absolute bioavailability of insulin glulisine after subcutaneous administration is approximately 70%, regardless of injection area (abdomen 73%, deltoid 71%, thigh 68%). In a clinical study in healthy volunteers (n=32) the total insulin glulisine bioavailability was similar after subcutaneous injection of insulin glulisine and NPH insulin (premixed in the syringe) and following separate simultaneous subcutaneous injections. There was 27% attenuation of the maximum concentration (Cmax) of APIDRA after premixing; however, the time to maximum concentration (Tmax) was not affected. No data are available on mixing APIDRA with insulin preparations other than NPH insulin. [See Clinical Studies]. Distribution and Elimination The distribution and elimination of insulin glulisine and regular human insulin after intravenous administration are similar with volumes of distribution of 13 and 21 L and half-lives of 13 and 17 minutes, respectively. After subcutaneous administration, insulin glulisine is eliminated more rapidly than regular human insulin with an apparent half-life of 42 minutes compared to 86 minutes. Clinical Pharmacology In Specific Populations Pediatric patients The pharmacokinetic and pharmacodynamic properties of APIDRA and regular human insulin were assessed in a study conducted in children 7 to 11 years old (n=10) and adolescents 12 to 16 years old (n=10) with type 1 diabetes. The relative differences in pharmacokinetics and pharmacodynamics between APIDRA and regular human insulin in these patients with type 1 diabetes were similar to those in healthy adult subjects and adults with type 1 diabetes. Race A study in 24 healthy Caucasians and Japanese subjects compared the pharmacokinetics and pharmacodynamics after subcutaneous injection of insulin glulisine, insulin lispro, and regular human insulin. With subcutaneous injection of insulin glulisine, Japanese subjects had a greater initial exposure (33%) for the ratio of AUC(0-1h) to AUC(0-clamp end) than Caucasians (21%) although the total exposures were similar. There were similar findings with insulin lispro and regular human insulin. Obesity Insulin glulisine and regular human insulin were administered subcutaneously at a dose of 0.3 Units/kg in a euglycemic clamp study in obese, non-diabetic subjects (n=18) with a body mass index (BMI) between 30 and 40 kg/m². The median time to maximum concentration (Tmax) was 85 minutes (range 49 to 150 minutes) and the median peak concentration (Cmax) was 192 microUnits/mL (range 98 to 380 microUnits/mL) for insulin glulisine compared to a median Tmax of 150 minutes (range 90 to 240 minutes) and a median Cmax of 86 microUnits/mL (range 43 to 175 microUnits/mL) for regular human insulin. The more rapid onset of action and shorter duration of activity of APIDRA and insulin lispro compared to regular human insulin were maintained in an obese non-diabetic population (n= 18). (Figure 4.) Figure 4. Glucose infusion rates (GIR) in a euglycemic clamp study after subcutaneous injection of 0.3 Units/kg of APIDRA, insulin lispro or regular human insulin in an obese population. Figure 4 Renal impairment Studies with human insulin have shown increased circulating levels of insulin in patients with renal failure. In a study performed in 24 non-diabetic subjects with normal renal function (ClCr > 80 mL/min), moderate renal impairment (30-50 mL/min) and severe renal impairment ( < 30 mL/min), the subjects with moderate and severe renal impairment had increased exposure to insulin glulisine by 29% to 40% and reduced clearance of insulin glulisine by 20% to 25% compared to subjects with normal renal function. [See WARNINGS AND PRECAUTIONS]. Hepatic impairment The effect of hepatic impairment on the pharmacokinetics and pharmacodynamics of APIDRA has not been studied. Some studies with human insulin have shown increased circulating levels of insulin in patients with liver failure. [See WARNINGS AND PRECAUTIONS]. Gender The effect of gender on the pharmacokinetics and pharmacodynamics of APIDRA has not been studied. Pregnancy The effect of pregnancy on the pharmacokinetics and pharmacodynamics of APIDRA has not been studied. Smoking The effect of smoking on the pharmacokinetics and pharmacodynamics of APIDRA has not been studied. Clinical Studies The safety and efficacy of APIDRA was studied in adult patients with type 1 and type 2 diabetes (n =1833) and in children and adolescent patients (4 to 17 years) with type 1 diabetes (n=572). The primary efficacy parameter in these trials was glycemic control, assessed using glycated hemoglobin (GHb reported as HbA1c equivalent). Type 1 Diabetes-Adults A 26-week, randomized, open-label, active-controlled, non-inferiority study was conducted in patients with type 1 diabetes to assess the safety and efficacy of APIDRA (n= 339) compared to insulin lispro (n= 333) when administered subcutaneously within 15 minutes before a meal. Insulin glargine was administered once daily in the evening as the basal insulin. There was a 4week run-in period with insulin lispro and insulin glargine prior to randomization. Most patients were Caucasian (97%). Fifty eight percent of the patients were men. The mean age was 39 years (range 18 to 74 years). Glycemic control, the number of daily short-acting insulin injections and the total daily doses of APIDRA and insulin lispro were similar in the two treatment groups (Table 6). Table 6: Type 1 Diabetes Mellitus–Adult Treatment duration Treatment in combination with: 26 weeks Insulin glargine APIDRA Insulin Lispro Glycated hemoglobin (GHb)* (%) Number of patients 331 322 Baseline mean 7.6 7.6 Adjusted mean change from baseline -0.1 -0.1 Treatment difference: APIDRA - Insulin Lispro 0.0 95% CI for treatment difference (-0.1; 0.1) Basal insulin dose (Units/day) Baseline mean 24 24 Adjusted mean change from baseline 0 2 Short-acting insulin dose (Units/day) Baseline mean 30 31 Adjusted mean change from baseline -1 -1 Mean number of short-acting insulin injections per day 3 3 Body weight (kg) Baseline mean 73.9 74.1 Mean change from baseline 0.6 0.3 *GHb reported as HbA1c equivalent Type 2 Diabetes-Adults A 26-week, randomized, open-label, active-controlled, non-inferiority study was conducted in insulin-treated patients with type 2 diabetes to assess the safety and efficacy of APIDRA (n= 435) given within 15 minutes before a meal compared to regular human insulin (n=441) administered 30 to 45 minutes prior to a meal. NPH human insulin was given twice a day as the basal insulin. All patients participated in a 4-week run-in period with regular human insulin and NPH human insulin. Eighty-five percent of patients were Caucasian and 11% were Black. The mean age was 58 years (range 26 to 84 years). The average body mass index (BMI) was 34.6 kg/m². At randomization, 58% of the patients were taking an oral antidiabetic agent. These patients were instructed to continue use of their oral antidiabetic agent at the same dose throughout the trial. The majority of patients (79%) mixed their short-acting insulin with NPH human insulin immediately prior to injection. The reductions from baseline in GHb were similar between the 2 treatment groups (see Table 7). No differences between APIDRA and regular human insulin groups were seen in the number of daily short-acting insulin injections or basal or short-acting insulin doses. (See Table 7.) Table 7: Type 2 Diabetes Mellitus–Adult Treatment duration Treatment in combination with: 26 weeks NPH human insulin APIDRA Regular Human Insulin Glycated hemoglobin (GHb)* (%) Number of patients 404 403 Baseline mean 7.6 7.5 Adjusted mean change from baseline -0.5 -0.3 Treatment difference: APIDRA - Regular Human Insulin 95% CI for treatment difference -0.2 (-0.3; -0.1) Basal insulin dose (Units/day) Baseline mean 59 57 Adjusted mean change from baseline 6 6 Short-acting insulin dose (Units/day) Baseline mean 32 31 Adjusted mean change from baseline 4 5 Mean number of short-acting insulin injections per day 2 2 Body weight (kg) Baseline mean 100.5 99.2 Mean change from baseline 1.8 2.0 *GHb reported as HbA1c equivalent Type 1 Diabetes-Adults: Pre-And Post-Meal Administration A 12-week, randomized, open-label, active-controlled, non-inferiority study was conducted in patients with type 1 diabetes to assess the safety and efficacy of APIDRA administered at different times with respect to a meal. APIDRA was administered subcutaneously either within 15 minutes before a meal (n=286) or immediately after a meal (n=296) and regular human insulin (n= 278) was administered subcutaneously 30 to 45 minutes prior to a meal. Insulin glargine was administered once daily at bedtime as the basal insulin. There was a 4-week run-in period with regular human insulin and insulin glargine followed by randomization. Most patients were Caucasian (94%). The mean age was 40 years (range 18 to 73 years). Glycemic control (see Table 8) was comparable for the 3 treatment regimens. No changes from baseline between the treatments were seen in the total daily number of short-acting insulin injections. (See Table 8.) Table 8: Pre-and Post-Meal Administration in Type 1 Diabetes Mellitus–Adult Treatment duration Treatment in combination with: 12 weeks insulin glargine APIDRA pre meal 12 week sinsulin glargine APIDRA post meal 12 weeksminsulin glargine Regular Human Insulin Glycated hemoglobin (GHb)* (%) Number of patients 268 276 257 Baseline mean 7.7 7.7 7.6 Adjusted mean change from baseline** -0.3 -0.1 -0.1 Basal insulin dose (Units/day) Baseline mean 29 29 28 Adjusted mean change from baseline 1 0 1 Short-acting insulin dose (Units/day) Baseline mean 29 29 27 Adjusted mean change from baseline -1 -1 2 Mean number of short-acting insulin injections per day 3 3 3 Body weight (kg) Baseline mean 79.2 80.3 78.9 Mean change from baseline 0.3 -0.3 0.3 *GHb reported as HbA1c equivalent **Adjusted mean change from baseline treatment difference (98.33% CI for treatment difference): APIDRA pre meal vs. Regular Human Insulin -0.1 (-0.3; 0.0) APIDRA post meal vs. Regular Human Insulin 0.0 (-0.1; 0.2) APIDRA post meal vs. pre meal 0.2 (0.0; 0.3) Type 1 Diabetes-Pediatric Patients A 26-week, randomized, open-label, active-controlled, non-inferiority study was conducted in children and adolescents older than 4 years of age with type 1 diabetes mellitus to assess the safety and efficacy of APIDRA (n= 277) compared to insulin lispro (n= 295) when administered subcutaneously within 15 minutes before a meal. Patients also received insulin glargine (administered once daily in the evening) or NPH insulin (administered once in the morning and once in the evening). There was a 4-week run-in period with insulin lispro and insulin glargine or NPH prior to randomization. Most patients were Caucasian (91%). Fifty percent of the patients were male. The mean age was 12.5 years (range 4 to 17 years). Mean BMI was 20.6 kg/m² . Glycemic control (see Table 9) was comparable for the two treatment regimens. Table 9: Results from a 26-week study in pediatric patients with type 1 diabetes mellitus APIDRA Lispro Number of patients 271 291 Basal Insulin NPH or insulin glargine NPH or insulin glargine Glycated hemoglobin (GHb)* (%) Baseline mean 8.2 8.2 Adjusted mean change from baseline 0.1 0.2 Treatment Difference: Mean (95% confidence interval) -0.1 (-0.2, 0.1) Basal insulin dose (Units/kg/day) Baseline mean 0.5 0.5 Mean change from baseline 0.0 0.0 Short-acting insulin dose (Units/kg/day) Baseline mean 0.5 0.5 Mean change from baseline 0.0 0.0 Mean number of short-acting insulin injections per day 3 3 Baseline mean body weight (kg) 51.5 50.8 Mean weight change from baseline (kg) 2.2 2.2 *GHb reported as HbA1c equivalent Type 1 Diabetes-Adults: Continuous Subcutaneous Insulin Infusion A 12-week randomized, active control study (APIDRA versus insulin aspart) conducted in adults with type 1 diabetes (APIDRA n= 29, insulin aspart n=30) evaluated the use of APIDRA in an external continuous subcutaneous insulin pump. All patients were Caucasian. The mean age was 46 years (range 21 to 73 years). The mean GHb increased from baseline to endpoint in both treatment groups (from 6.8% to 7.0% for APIDRA; from 7.1% to 7.2% for insulin aspart).

Drug Description

Find Lowest Prices on APIDRA (insulin glulisine [rDNA origin]) Solution for Injection DESCRIPTION APIDRA® (insulin glulisine [rDNA origin] injection) is a rapid-acting human insulin analog used to lower blood glucose. Insulin glulisine is produced by recombinant DNA technology utilizing a non-pathogenic laboratory strain of Escherichia coli (K12). Insulin glulisine differs from human insulin in that the amino acid asparagine at position B3 is replaced by lysine and the lysine in position B29 is replaced by glutamic acid. Chemically, insulin glulisine is 3B-lysine29B-glutamic acid-human insulin, has the empirical formula C258H384N64O78S6 and a molecular weight of 5823 and has the following structural formula: APIDRA is a sterile, aqueous, clear, and colorless solution. Each milliliter of APIDRA contains 100 units (3.49 mg) insulin glulisine, 3.15 mg metacresol, 6 mg tromethamine, 5 mg sodium chloride, 0.01 mg polysorbate 20, and water for injection. APIDRA has a pH of approximately 7.3. The pH is adjusted by addition of aqueous solutions of hydrochloric acid and/or sodium hydroxide.

Indications & Dosage

INDICATIONS APIDRA is indicated to improve glycemic control in adults and children with diabetes mellitus. DOSAGE AND ADMINISTRATION Dosage Considerations APIDRA is a recombinant insulin analog that is equipotent to human insulin (i.e. one unit of APIDRA has the same glucose-lowering effect as one unit of regular human insulin) when given intravenously. When given subcutaneously, APIDRA has a more rapid onset of action and a shorter duration of action than regular human insulin. The dosage of APIDRA must be individualized. Blood glucose monitoring is essential in all patients receiving insulin therapy. The total daily insulin requirement may vary and is usually between 0.5 to 1 Unit/kg/day. Insulin requirements may be altered during stress, major illness, or with changes in exercise, meal patterns, or coadministered drugs. Subcutaneous Administration APIDRA should be given within 15 minutes before a meal or within 20 minutes after starting a meal. APIDRA given by subcutaneous injection should generally be used in regimens with an intermediate or long-acting insulin. APIDRA should be administered by subcutaneous injection in the abdominal wall, thigh, or upper arm. Injection sites should be rotated within the same region (abdomen, thigh or upper arm) from one injection to the next to reduce the risk of lipodystrophy [See ADVERSE REACTIONS]. Continuous Subcutaneous Infusion (Insulin Pump) APIDRA may be administered by continuous subcutaneous infusion in the abdominal wall. Do not use diluted or mixed insulins in external insulin pumps. Infusion sites should be rotated within the same region to reduce the risk of lipodystrophy [See ADVERSE REACTIONS]. The initial programming of the external insulin infusion pump should be based on the total daily insulin dose of the previous regimen. The following insulin pumps† have been used in APIDRA clinical trials conducted by sanofiaventis, the manufacturer of APIDRA: Disetronic® H-Tron® plus V100 and D-Tron® with Disetronic catheters (Rapid™, Rapid C™, Rapid D™, and Tender™) MiniMed® Models 506, 507, 507c and 508 with MiniMed catheters (Sof-set Ultimate QR™, and Quick-set™). Before using a different insulin pump with APIDRA, read the pump label to make sure the pump has been evaluated with APIDRA. Physicians and patients should carefully evaluate information on pump use in the APIDRA prescribing information, Patient Information Leaflet, and the pump manufacturer's manual. APIDRA-specific information should be followed for in-use time, frequency of changing infusion sets, or other details specific to APIDRA usage, because APIDRA-specific information may differ from general pump manual instructions. Failure to follow APIDRA-specific instructions may lead to serious adverse events. Patients administering APIDRA by continuous subcutaneous infusion must have an alternative insulin delivery system in case of pump system failure. Based on in vitro studies which have shown loss of the preservative, metacresol and insulin degradation, APIDRA in the reservoir should be changed at least every 48 hours. APIDRA should not be exposed to temperatures greater than 98.6°F (37°C). In clinical use, the infusion sets and the APIDRA in the reservoir must be changed at least every 48 hours [See WARNINGS AND PRECAUTIONS and HOW SUPPLIED/Storage and Handling]. Intravenous Administration APIDRA can be administered intravenously under medical supervision for glycemic control with close monitoring of blood glucose and serum potassium to avoid hypoglycemia and hypokalemia. For intravenous use, APIDRA should be used at concentrations of 0.05 Units/mL to 1 Unit/mL insulin glulisine in infusion systems using polyvinyl chloride (PVC) bags. APIDRA has been shown to be stable only in normal saline solution (0.9% sodium chloride). Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit. Do not administer insulin mixtures intravenously. HOW SUPPLIED Dosage Forms And Strengths APIDRA 100 units per mL (U-100) is available as: 10 mL vials 3 mL SoloStar prefilled pen Storage And Handling APIDRA 100 units per mL (U-100) is available as: 10 mL vials NDC 0088-2500-33 3 mL SoloStar prefilled pen, package of 5 NDC 0088-2502-05 Pen needles are not included in the packs. Solostar is compatible with all pen needles from Becton Dickinson and Company, Ypsomed and Owen Mumford. Storage Do not use after the expiration date (see carton and container). Unopened Vial/SoloStar Unopened APIDRA vials and SoloStar should be stored in a refrigerator, 36°F-46°F (2°C-8°C). Protect from light. APIDRA should not be stored in the freezer and it should not be allowed to freeze. Discard if it has been frozen. Unopened vials/SoloStar not stored in a refrigerator must be used within 28 days. Open (In-Use) Vial Opened vials, whether or not refrigerated, must be used within 28 days. If refrigeration is not possible, the open vial in use can be kept unrefrigerated for up to 28 days away from direct heat and light, as long as the temperature is not greater than 77°F (25°C). Open (In-Use) SoloStar prefilled pen The opened (in-use) SoloStar should NOT be refrigerated but should be kept below 77°F (25°C) away from direct heat and light. The opened (in-use) SoloStar kept at room temperature must be discarded after 28 days. Infusion sets Infusion sets (reservoirs, tubing, and catheters) and the APIDRA in the reservoir must be discarded after 48 hours of use or after exposure to temperatures that exceed 98.6°F (37°C). Intravenous use Infusion bags prepared as indicated under DOSAGE AND ADMINISTRATION are stable at room temperature for 48 hours. Preparation And Handling After dilution for intravenous use, the solution should be inspected visually for particulate matter and discoloration prior to administration. Do not use the solution if it has become cloudy or contains particles; use only if it is clear and colorless. APIDRA is not compatible with Dextrose solution and Ringers solution and, therefore, cannot be used with these solution fluids. The use of APIDRA with other solutions has not been studied and is, therefore, not recommended. sanofi-aventis U.S. LLC Bridgewater, NJ 08807 A Sanofi Company. Date of revision: 05/2014

Medication Guide

PATIENT INFORMATION APIDRA (uh PEE druh) (insulin glulisine [recombinant DNA origin] injection) Solution for Injection Read the Patient Information that comes with APIDRA before you start taking it and each time you get a refill. There may be new information. This leaflet does not take the place of talking with your healthcare provider about your diabetes or treatment. If you have questions about APIDRA or about diabetes, talk with your healthcare provider. What is APIDRA? APIDRA is a man-made insulin used to control high blood sugar in adults and children with diabetes mellitus. It is not known if APIDRA is safe or effective in: children under age 4 with type 1 diabetes children with type 2 diabetes Who should NOT take APIDRA? Do not take APIDRA: when your blood sugar is too low (hypoglycemia). See the section, “What are the possible side effects of APIDRA?” if you are allergic to any of the ingredients in APIDRA. See the end of this leaflet for a complete list of ingredients. Ask your healthcare provider if you are not sure. What should I tell my healthcare provider before taking APIDRA? Medical conditions can affect your insulin needs. Tell your healthcare provider about all of your medical conditions, including if you: have liver or kidney problems. are pregnant, plan to become pregnant, or are breast-feeding. It is not known if APIDRA will harm your unborn baby or nursing child. You and your healthcare provider should talk about the best way to manage your diabetes while you are pregnant or breast-feeding. It is especially important to keep good control of your blood sugar during pregnancy. have heart failure or other heart problems. If you have heart failure, it may get worse while you take TZDs with APIDRA Tell your healthcare provider about all the medicines you take, including prescription and non-prescription medicines, vitamins, and herbal supplements especially ones commonly called TZDs (thiazolidinediones). Know the medicines you take. Keep a list of your medicines with you and show it to your healthcare provider and pharmacist when you get a new medicine. How should I take APIDRA? Take APIDRA exactly as prescribed. Do not make any changes to your dose or type of insulin unless told to do so by your healthcare provider. Know your insulin. Make sure you know: the type and strength of insulin prescribed for you the amount of insulin you take the best time for you to take your insulin. This may change if you take a different type of insulin or if the way you give your insulin changes for example, using an insulin pump instead of giving injections under the skin (subcutaneous injections). APIDRA starts working faster than regular insulin, but does not work as long. APIDRA is usually used with a longer-acting insulin when given by injection under the skin (subcutaneous), or by itself when using an insulin pump. Read the instructions for use that come with your APIDRA. Talk to your healthcare provider if you have any questions. Your healthcare provider should show you how to inject APIDRA before you start taking it. Your healthcare provider will prescribe the best type of APIDRA for you. APIDRA is available in: 3 mL SoloStar® prefilled pen 10 mL vials You need a prescription to get APIDRA. Always be sure you receive the right insulin from the pharmacy. Check your blood sugar level before each use of APIDRA. Ask your healthcare provider what your blood sugars should be and when you should check your blood sugar levels. Check the label to make sure you have the correct insulin type. This is especially important if you also take long-acting insulin. APIDRA should look clear and colorless. Do not use APIDRA if it looks cloudy, colored, or has particles in it. Talk with your pharmacist or healthcare provider if you have any questions. If you take too much APIDRA, your blood sugar may fall low (hypoglycemia). You can treat mild low blood sugar (hypoglycemia) by drinking or eating something sugary right away. Do not share needles, insulin pens or syringes with others. Your dose of APIDRA may need to be changed because of: illness change in diet stress change in physical activity or exercise other medicines you take travel Check your blood sugar and stay on the diet and exercise plan as prescribed by your healthcare provider. What should I consider while taking APIDRA? Alcohol may affect your blood sugar when you take APIDRA Driving and operating machinery. You may have trouble paying attention or reacting if you have low blood sugar (hypoglycemia). Be careful when you drive a car or operate machinery. Ask your healthcare provider if it is alright for you to drive if you have: low blood sugar (hypoglycemia) decreased or no warning signs of low blood sugar What are the possible side effects of APIDRA? APIDRA can cause serious side effects, including: Low blood sugar (hypoglycemia). Symptoms of low blood sugar may include: feeling anxious, or irritable, mood changes trouble concentrating or feeling confused tingling in your hands, feet, lips, or tongue feeling dizzy, light-headed, or drowsy nightmares or trouble sleeping headache blurred vision slurred speech a fast heart beat sweating shakiness walking unsteady Very low blood sugar (hypoglycemia) can cause unconsciousness (passing out), seizures, and death. Talk to your healthcare provider about how to tell if you have low blood sugar and what to do if this happens while taking APIDRA. Know your symptoms of low blood sugar. Follow your healthcare provider's instructions for treating your low blood sugar. Talk to your healthcare provider if low blood sugar is a problem for you. Your dose of APIDRA may need to be changed. Serious allergic reactions. Get medical help right away if you have any of these symptoms of a severe allergic reaction: a rash all over your body shortness of breath trouble breathing (wheezing) fast pulse sweating feel faint (due to low blood pressure) Low potassium in your blood. Your doctor will check you for this. Common side effects include: Reactions at the injection site (local allergic reaction). You may get redness, swelling and itching at the injection site. If you keep having skin reactions or they are serious talk to your healthcare provider. Skin thickening or pits at the injection site. Do not inject insulin into skin where this has happened. Choose an injection area (upper arm, thigh, or stomach area). Change injection sites within the area you choose with each dose. Do not inject into the exact same spot for each injection. Weight gain Heart Failure. Taking certain diabetes pills called thiazolidinediones or “TZDs” with APIDRA may cause heart failure in some people. This can happen even if you have never had heart failure or heart problems before. If you already have heart failure it may get worse while you take TZDs with APIDRA. Your healthcare provider should monitor you closely while you are taking TZDs with APIDRA. Tell your healthcare provider if you have any new or worse symptoms of heart failure including: shortness of breath swelling of your ankles or feet sudden weight gain During treatment with TZDs and APIDRA, the TZD dose may need to be adjusted or stopped by your healthcare provider if you have new or worse heart failure. Tell your healthcare provider about any side effect that bothers you or that does not go away. These are not all of the possible side effects of APIDRA. Call your doctor for medical advice about side effects. You may report side effects to FDA at 1800-332-1088. How should I store APIDRA? See the Patient Instructions for Use that come with your APIDRA for specific storage instructions. Unopened APIDRA: Do not use APIDRA after the expiration date stamped on the label. Keep all unopened APIDRA in the refrigerator between 36°F to 46°F (2°C to 8°C). Do not freeze. Do not use APIDRA if it has been frozen. Keep APIDRA away from direct heat and light. Unopened vials and SoloStar that were not kept in a refrigerator must be used within 28 days after opening. General Information about APIDRA Medicines are sometimes prescribed for conditions that are not mentioned in patient information leaflets. Do not use APIDRA for a condition for which it was not prescribed. Do not give APIDRA to other people, even if they have the same symptoms you have. It may harm them. This leaflet summarizes the most important information about APIDRA. If you would like more information, talk with your healthcare provider. You can ask your healthcare provider for information about APIDRA that is written for healthcare providers. For more information about APIDRA call 1-800-633-1610 or go to www.apidra.com. What are the ingredients in APIDRA? Active ingredient: insulin glulisine Inactive ingredients: metacresol, tromethamine, sodium chloride, polysorbate 20, water for injection, hydrochloric acid or sodium hydroxide ADDITIONAL INFORMATION DIABETES FORECAST is a national magazine designed especially for patients with diabetes and their families and is available by subscription from the American Diabetes Association, (ADA), P.O. Box 363, Mt. Morris, IL 61054-0363, 1-800-DIABETES (1-800-342-2383). You may also visit the ADA website at www.diabetes.org. Another publication, COUNTDOWN, is available from the Juvenile Diabetes Research Foundation International (JDRF), 120 Wall Street, 19th Floor, New York, New York 10005, 1800-JDF-CURE (1-800-533-2873). You may also visit the JDRF website at www.jdf.org. To get more information about diabetes, check with your healthcare provider or diabetes educator or visit www.DiabetesWatch.com. For more information about APIDRA call 1-800-633-1610 or visit www.apidra.com. APIDRA® SoloStar® (insulin glulisine [rDNA origin] injection) 3 mL prefilled pen Patient Instructions for Use Be sure that you read, understand and follow these instructions before you use your APIDRA SoloStar® . Talk with your healthcare provider about the right way to use your APIDRA SoloStar before you use it for the first time. Keep this leaflet in case you need to look at it again later. APIDRA SoloStar should not be used by people who are blind or have severe vision problems, without the help of a person who has good eyesight and who is trained to use the APIDRA SoloStar the right way. APIDRA SoloStar is a disposable prefilled pen used to inject APIDRA. Each APIDRA SoloStar has 300 units of insulin which can be used for many doses. You can select a dose from 1 to 80 units. The pen plunger moves with each dose. The plunger will only move to the end of the cartridge when 300 units of insulin have been given. If you will give yourself subcutaneous injections of APIDRA: You should take APIDRA within 15 minutes before a meal or within 20 minutes after starting a meal. Do not inject APIDRA if you are not going to eat within 15 minutes. Inject APIDRA into the skin of your upper arm, thigh, or stomach area. Do not inject APIDRA into a vein or into a muscle. Choose an injection area (upper arm, thigh, or stomach area). Change injection sites within the area you choose with each dose. Do not inject into the exact same spot for each injection. Important information for use of APIDRA SoloStar: Use a new needle for each injection. APIDRA Solostar may be used with pen needles from Becton Dickinson and Company, Ypsomed and Owen Mumford. Contact your healthcare provider for further information. Do a safety test before each injection. (See step 3.) Do not select a dose or press the injection button without a needle attached. Do not share your APIDRA SoloStar with others even if they have diabetes. If your injection is given by another person, this person must be careful to avoid accidental needle stick injury and prevent passing (transmission of) infection. Do not use APIDRA SoloStar if it is damaged or if you are not sure that it is working correctly. Always carry an extra APIDRA SoloStar prefilled pen in case your APIDRA SoloStar is lost or damaged. Step 1. Preparing for an injection Make sure you have the following items: Apidra SoloStar Pen needles Alcohol swab Puncture resistant container. See “How do I dispose of used needles and APIDRA SoloStar?”. Check the label on your APIDRA SoloStar to make sure you have the right insulin. The APIDRA Solostar is blue. It has a dark blue injection button with a raised ring on the top. Check the expiration date, located on the carton or the label of your APIDRA SoloStar, to make sure the date has not passed. Do not use an APIDRA SoloStar if the date has passed. Take off the pen cap. Look at the insulin in your APIDRA SoloStar. Check to make sure that the insulin looks clear. Do not use this APIDRA SoloStar if the insulin is cloudy, colored, or has particles in it. Step 2. Attaching the needle Always use a new sterile needle for each injection to help prevent contamination, and potential needle blocks. Read the pen needle “Instructions for Use” before you use them. Please note: Pen needles may look different. The pen needles shown are for illustrative purposes only. Wipe the Rubber Seal with alcohol. Remove the protective seal from the new pen needle. Line up the needle with the pen, and keep it straight as you attach it (screw or push on, depending on the needle type). If you do not keep the needle straight while you attach it this can damage the rubber seal, and cause leakage of insulin, or break the needle. Step 3. Doing a Safety test Do a safety test before each injection to make sure that you get the correct dose of APIDRA. The safety test: makes sure that the pen and needle work properly removes air bubbles A. Select a dose of 2 units by turning the dosage selector. B. Take off the outer needle cap and keep it to remove the used needle after injection. Take off the inner needle cap and dispose of it. C. Hold the pen with the needle pointing upwards. D. Tap the insulin reservoir so that any air bubbles rise up towards the needle. E. Press the injection button all the way in. Check if insulin comes out of the needle tip. You may have to do the safety test more than once before you see the insulin. If no insulin comes out, check for air bubbles and repeat the safety test two more times to remove them. If still no insulin comes out, the needle may be blocked. Change the needle and try again. If no insulin comes out after changing the needle, your APIDRA SoloStar may be damaged. Do not use this APIDRA SoloStar. Step 4. Selecting your dose Select the APIDRA dose prescribed by your healthcare provider. You can select the insulin dose in steps of 1 unit, from a minimum of 1 unit to a maximum of 80 units. If you need a dose larger than 80 units, you should give it as two or more injections. A. Check that the dose window shows “0” after the safety test. B. Select your needed dose (in the example below, the selected dose is 30 units). If you turn past your dose, you can turn back down. Do not push the injection button while turning, insulin will come out. You cannot turn the dosage selector passed the number of units left in the pen. Do not force the dosage selector to turn. In this case, either you can inject the amount of insulin that is still in the pen and finish your dose with a new APIDRA SoloStar or you can use a new APIDRA SoloStar for your full dose. Step 5. Giving the injection A. Give the injection exactly as shown to you by your healthcare provider. B. Insert the needle into your skin. C. Inject the dose by pressing the injection button in all the way. Only push the injection button when you are ready to inject. The number in the dose window will return to “0” as you inject. D. Keep the injection button pressed all the way in. Slowly count to 10 before you take the needle out of your skin. This will make sure that the full dose has been given. Step 6. Removing and disposing of the pen needle Always remove the pen needle after each injection and store your APIDRA SoloStar without a needle attached. This helps prevent: Contamination and infection Air from getting into the insulin reservoir and leakage of insulin. This will help to make sure you inject the right dose of insulin. A. Follow the instructions from your healthcare provider when removing and disposing of the needle. For example “scoop” the outer needle cap back on the needle and use it to unscrew the used needle from the pen. To lessen the risk of accidental needle stick injury and passing infection: do not recap needles with your fingers never replace the inner needle cap. If your injection is given by another person, this person must also be careful when removing and disposing of the needles to prevent accidental needle stick injury and passing infection. B. Dispose of the needle the right way into your special puncture resistant container (See “How Do I Dispose of used needles and APIDRA SoloStar?”). C. Always put the pen cap back on the pen, then store the APIDRA SoloStar until your next injection. How do I dispose of used needles and APIDRA SoloStar? Check with your healthcare provider for instructions about the right way to dispose of used needles and APIDRA SoloStar. There may be local or state laws about how to throw away used needles and APIDRA SoloStar. Do not dispose of used needles or APIDRA SoloStar in household trash and do not recycle them. Put used needles and used empty APIDRA SoloStar in a container made specially for disposing of used syringes and needles (called a “sharps” container) or a hard plastic container (such as empty detergent bottles),with a screw-on cap, or metal container with a plastic lid labeled “Used Syringes”. These containers should be sealed and disposed of the right way. How should I Store APIDRA SoloStar? Do not refrigerate APIDRA SoloStar after first use. Keep at room temperature below 77°F (25°C). Dispose of any opened APIDRA SoloStar 28 days after first use. Maintenance Protect your APIDRA SoloStar from dust and dirt. You can clean the outside of your APIDRA SoloStar by wiping it with a damp cloth. Do not soak, wash or lubricate the pen as this may damage it. Handle your APIDRA SoloStar with care. Avoid situations where your APIDRA SoloStar might be damaged. If you are concerned that your APIDRA SoloStar may be damaged, use a new one. If you have any questions about APIDRA SoloStar or about diabetes, ask your healthcare provider, go to www.apidra.com or call sanofi-aventis U.S. at 1-800-633-1610.

Overdosage & Contraindications

Side Effects & Drug Interactions

SIDE EFFECTS The following adverse reactions are discussed elsewhere: Hypoglycemia [See WARNINGS AND PRECAUTIONS] Hypokalemia [See WARNINGS AND PRECAUTIONS] Clinical Trial experience Because clinical trials are conducted under widely varying designs, the adverse reaction rates reported in one clinical trial may not be easily compared to those rates reported in another clinical trial, and may not reflect the rates actually observed in clinical practice. The frequencies of adverse drug reactions during APIDRA clinical trials in patients with type 1 diabetes mellitus and type 2 diabetes mellitus are listed in the tables below. Table 1: Treatment –emergent adverse events in pooled studies of adults with type 1 diabetes (adverse events with frequency ≥ 5%) APIDRA, % (n=950) All comparatorsa, % (n=641) Nasopharyngitis 10.6 12.9 Hypoglycemiab 6.8 6.7 Upper respiratory tract 6.6 5.6 Influenza 4.0 5.0 a Insulin lispro, regular human insulin, insulin aspart b Only severe symptomatic hypoglycemia Table 2: Treatment –emergent adverse events in pooled studies of adults with type 2 diabetes (adverse events with frequency ≥ 5%) APIDRA, % (n=883) Regular human insulin, % (n=883) Upper respiratory tract infection 10.5 7.7 Nasopharyngitis 7.6 8.2 Edema peripheral 7.5 7.8 Influenza 6.2 4.2 Arthralgia 5.9 6.3 Hypertension 3.9 5.3 Pediatrics Table 3 summarizes the adverse reactions occurring with frequency higher than 5% in a clinical study in children and adolescents with type 1 diabetes treated with APIDRA (n=277) or insulin lispro (n=295). Table 3: Treatment –emergent adverse events in children and adolescents with type 1 diabetes (adverse reactions with frequency ≥ 5%) APIDRA, % (n=277) Lispro, % (n=295) Nasopharyngitis 9.0 9.5 Upper respiratory tract infection 8.3 10.8 Headache 6.9 11.2 Hypoglycemic seizure 6.1 4.7 Severe symptomatic hypoglycemia Hypoglycemia is the most commonly observed adverse reaction in patients using insulin, including APIDRA [See WARNINGS AND PRECAUTIONS]. The rates and incidence of severe symptomatic hypoglycemia, defined as hypoglycemia requiring intervention from a third party, were comparable for all treatment regimens (see Table 4). In the phase 3 clinical trial, children and adolescents with type 1 diabetes had a higher incidence of severe symptomatic hypoglycemia in the two treatment groups compared to adults with type 1 diabetes. (see Table 4) [See Clinical Studies]. Table 4: Severe Symptomatic Hypoglycemia* Type 1 Diabetes Adults 12 weeks with insulin glargine Type 1 Diabetes Adults 26 weeks with insulin glargine Type 2 Diabetes Adults 26 weeks with NPH human insulin Type 1 Diabetes Pediatrics 26 weeks APIDRA Pre-meal APIDRA Post-meal Regular Human Insulin APIDRA Insulin Lispro APIDRA Regular Human Insulin APIDRA Insulin Lispro Events per month per patient 0.05 0.05 0.13 0.02 0.02 0.00 0.00 0.09 0.08 Percent of patients (n/total N) 8.4% (24/286) 8.4% (25/296) 10.1% (28/278) 4.8% (16/339) 4.0% (13/333) 1.4% (6/416) 1.2% (5/420) 16.2% (45/277) 19.3% (57/295) * Severe symptomatic hypoglycemia defined as a hypoglycemic event requiring the assistance of another person that met one of the following criteria: the event was associated with a whole blood referenced blood glucose < 36mg/dL or the event was associated with prompt recovery after oral carbohydrate, intravenous glucose or glucagon administration. Insulin initiation and intensification of glucose control Intensification or rapid improvement in glucose control has been associated with a transitory, reversible ophthalmologic refraction disorder, worsening of diabetic retinopathy, and acute painful peripheral neuropathy. However, long-term glycemic control decreases the risk of diabetic retinopathy and neuropathy. Lipodystrophy Long-term use of insulin, including APIDRA, can cause lipodystrophy at the site of repeated insulin injections or infusion. Lipodystrophy includes lipohypertrophy (thickening of adipose tissue) and lipoatrophy (thinning of adipose tissue), and may affect insulin absorption. Rotate insulin injection or infusion sites within the same region to reduce the risk of lipodystrophy. [See DOSAGE AND ADMINISTRATION]. Weight gain Weight gain can occur with insulin therapy, including APIDRA, and has been attributed to the anabolic effects of insulin and the decrease in glucosuria. Peripheral Edema Insulin, including APIDRA, may cause sodium retention and edema, particularly if previously poor metabolic control is improved by intensified insulin therapy. Adverse Reactions with Continuous Subcutaneous Insulin Infusion (CSII) In a 12-week randomized study in patients with type 1 diabetes (n=59), the rates of catheter occlusions and infusion site reactions were similar for APIDRA and insulin aspart treated patients (Table 5). Table 5: Catheter Occlusions and Infusion Site Reactions. 40% APIDRA (n=29) insulin aspart (n=30) Catheter occlusions/month 0.08 0.15 Infusion site reactions 10.3% (3/29) 13.3% (4/30) Allergic Reactions Local Allergy As with any insulin therapy, patients taking APIDRA may experience redness, swelling, or itching at the site of injection. These minor reactions usually resolve in a few days to a few weeks, but in some occasions may require discontinuation of APIDRA. In some instances, these reactions may be related to factors other than insulin, such as irritants in a skin cleansing agent or poor injection technique. Systemic Allergy Severe, life-threatening, generalized allergy, including anaphylaxis, may occur with any insulin, including APIDRA. Generalized allergy to insulin may cause whole body rash (including pruritus), dyspnea, wheezing, hypotension, tachycardia, or diaphoresis. In controlled clinical trials up to 12 months duration, potential systemic allergic reactions were reported in 79 of 1833 patients (4.3%) who received APIDRA and 58 of 1524 patients (3.8%) who received the comparator short-acting insulins. During these trials treatment with APIDRA was permanently discontinued in 1 of 1833 patients due to a potential systemic allergic reaction. Localized reactions and generalized myalgias have been reported with the use of metacresol, which is an excipient of APIDRA. Antibody Production In a study in patients with type 1 diabetes (n=333), the concentrations of insulin antibodies that react with both human insulin and insulin glulisine (cross-reactive insulin antibodies) remained near baseline during the first 6 months of the study in the patients treated with APIDRA. A decrease in antibody concentration was observed during the following 6 months of the study. In a study in patients with type 2 diabetes (n=411), a similar increase in cross-reactive insulin antibody concentration was observed in the patients treated with APIDRA and in the patients treated with human insulin during the first 9 months of the study. Thereafter the concentration of antibodies decreased in the APIDRA patients and remained stable in the human insulin patients. There was no correlation between cross-reactive insulin antibody concentration and changes in HbA1c, insulin doses, or incidence of hypoglycemia. The clinical significance of these antibodies is not known. APIDRA did not elicit a significant antibody response in a study of children and adolescents with type 1 diabetes. Postmarketing Experience The following adverse reactions have been identified during post-approval use of APIDRA. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to estimate reliably their frequency or establish a causal relationship to drug exposure. Medication errors have been reported in which other insulins, particularly long-acting insulins, have been accidentally administered instead of APIDRA [See PATIENT INFORMATION]. DRUG INTERACTIONS A number of drugs affect glucose metabolism and may necessitate insulin dose adjustment and particularly close monitoring. Drugs that may increase the blood glucose-lowering effect of insulins including APIDRA, and therefore increase the risk of hypoglycemia, include oral antidiabetic products, pramlintide, ACE inhibitors, disopyramide, fibrates, fluoxetine, monoamine oxidase inhibitors, propoxyphene, pentoxifylline, salicylates, somatostatin analogs, and sulfonamide antibiotics. Drugs that may reduce the blood-glucose-lowering effect of APIDRA include corticosteroids, niacin, danazol, diuretics, sympathomimetic agents (e.g., epinephrine, albuterol, terbutaline), glucagon, isoniazid, phenothiazine derivatives, somatropin, thyroid hormones, estrogens, progestogens (e.g., in oral contraceptives), protease inhibitors, and atypical antipsychotics. Beta-blockers, clonidine, lithium salts, and alcohol may either increase or decrease the bloodglucose-lowering effect of insulin. Pentamidine may cause hypoglycemia, which may sometimes be followed by hyperglycemia. The signs of hypoglycemia may be reduced or absent in patients taking anti-adrenergic drugs such as beta-blockers, clonidine, guanethidine, and reserpine.

Warnings & Precautions

WARNINGS Included as part of the PRECAUTIONS section. PRECAUTIONS Dosage Adjustment And Monitoring Glucose monitoring is essential for patients receiving insulin therapy. Changes to an insulin regimen should be made cautiously and only under medical supervision. Changes in insulin strength, manufacturer, type, or method of administration may result in the need for a change in insulin dose. Concomitant oral antidiabetic treatment may need to be adjusted. As with all insulin preparations, the time course of action for APIDRA may vary in different individuals or at different times in the same individual and is dependent on many conditions, including the site of injection, local blood supply, or local temperature. Patients who change their level of physical activity or meal plan may require adjustment of insulin dosages. Hypoglycemia Hypoglycemia is the most common adverse reaction of insulin therapy, including APIDRA. The risk of hypoglycemia increases with tighter glycemic control. Patients must be educated to recognize and manage hypoglycemia. Severe hypoglycemia may lead to unconsciousness and/or convulsions and may result in temporary or permanent impairment of brain function or death. Severe hypoglycemia requiring the assistance of another person and/or parenteral glucose infusion or glucagon administration has been observed in clinical trials with insulin, including trials with APIDRA. The timing of hypoglycemia usually reflects the time-action profile of the administered insulin formulations. Other factors such as changes in food intake (e.g., amount of food or timing of meals), injection site, exercise, and concomitant medications may also alter the risk of hypoglycemia [See DRUG INTERACTIONS]. As with all insulins, use caution in patients with hypoglycemia unawareness and in patients who may be predisposed to hypoglycemia (e.g., the pediatric population and patients who fast or have erratic food intake). The patient's ability to concentrate and react may be impaired as a result of hypoglycemia. This may present a risk in situations where these abilities are especially important, such as driving or operating other machinery. Rapid changes in serum glucose levels may induce symptoms similar to hypoglycemia in persons with diabetes, regardless of the glucose value. Early warning symptoms of hypoglycemia may be different or less pronounced under certain conditions, such as longstanding diabetes, diabetic nerve disease, use of medications such as beta-blockers [See DRUG INTERACTIONS], or intensified diabetes control. These situations may result in severe hypoglycemia (and, possibly, loss of consciousness) prior to the patient's awareness of hypoglycemia. Intravenously administered insulin has a more rapid onset of action than subcutaneously administered insulin, requiring closer monitoring for hypoglycemia. Hypersensitivity And Allergic Reactions Severe, life-threatening, generalized allergy, including anaphylaxis, can occur with insulin products, including APIDRA [See ADVERSE REACTIONS]. Hypokalemia All insulin products, including APIDRA, cause a shift in potassium from the extracellular to intracellular space, possibly leading to hypokalemia. Untreated hypokalemia may cause respiratory paralysis, ventricular arrhythmia, and death. Use caution in patients who may be at risk for hypokalemia (e.g., patients using potassium-lowering medications, patients taking medications sensitive to serum potassium concentrations). Monitor glucose and potassium frequently when APIDRA is administered intravenously. Renal Or Hepatic Impairment Frequent glucose monitoring and insulin dose reduction may be required in patients with renal or hepatic impairment [See CLINICAL PHARMACOLOGY]. Mixing Of Insulins APIDRA for subcutaneous injection should not be mixed with insulin preparations other than NPH insulin. If APIDRA is mixed with NPH insulin, APIDRA should be drawn into the syringe first. Injection should occur immediately after mixing. Do not mix APIDRA with other insulins for intravenous administration or for use in a continuous subcutaneous infusion pump. APIDRA for intravenous administration should not be diluted with solutions other than 0.9% sodium chloride (normal saline). The efficacy and safety of mixing APIDRA with diluents or other insulins for use in external subcutaneous infusion pumps have not been established. Subcutaneous Insulin Infusion pumps When used in an external insulin pump for subcutaneous infusion, APIDRA should not be diluted or mixed with any other insulin. APIDRA in the reservoir must be changed at least every 48 hours. APIDRA should not be exposed to temperatures greater than 98.6°F (37°C). Malfunction of the insulin pump or infusion set or handling errors or insulin degradation can rapidly lead to hyperglycemia, ketosis and diabetic ketoacidosis. Prompt identification and correction of the cause of hyperglycemia or ketosis or diabetic ketoacidosis is necessary. Interim subcutaneous injections with APIDRA may be required. Patients using continuous subcutaneous insulin infusion pump therapy must be trained to administer insulin by injection and have alternate insulin therapy available. [See DOSAGE AND ADMINISTRATION, HOW SUPPLIED/Storage and Handling, and PATIENT INFORMATION]. Intravenous Administration When APIDRA is administered intravenously, glucose and potassium levels must be closely monitored to avoid potentially fatal hypoglycemia and hypokalemia. Do not mix APIDRA with other insulins for intravenous administration. APIDRA may be diluted only in normal saline solution. Drug Interactions Some medications may alter insulin requirements and the risk for hypoglycemia or hyperglycemia [See DRUG INTERACTIONS]. Fluid Retention And Heart Failure With Concomitant Use Of PPAR-Gamma Agonists Thiazolidinediones (TZDs), which are peroxisome proliferator-activated receptor (PPAR) gamma agonists, can cause dose-related fluid retention, particularly when used in combination with insulin. Fluid retention may lead to or exacerbate heart failure. Patients treated with insulin, including APIDRA and a PPAR-gamma agonist should be observed for signs and symptoms of heart failure. If heart failure develops, it should be managed according to current standards of care, and discontinuation or dose reduction of the PPAR-gamma agonist must be considered. Patient Counseling Information See FDA-approved patient labeling. Instructions For All Patients Patients should be instructed on self-management procedures including glucose monitoring, proper injection technique, and management of hypoglycemia and hyperglycemia. Patients must be instructed on handling of special situations such as intercurrent conditions (illness, stress, or emotional disturbances), an inadequate or skipped insulin dose, inadvertent administration of an increased insulin dose, inadequate food intake, and skipped meals. Refer patients to the APIDRA Patient Information Leaflet for additional information. Women with diabetes should be advised to inform their doctor if they are pregnant or are contemplating pregnancy. Accidental mix-ups between APIDRA and other insulins, particularly long-acting insulins, have been reported. To avoid medication errors between APIDRA and other insulins, patients should be instructed to always check the insulin label before each injection. For Patients Using Continuous Subcutaneous Insulin Pumps Patients using external pump infusion therapy should be trained appropriately. The following insulin pumps† have been used in APIDRA clinical trials conducted by sanofiaventis, the manufacturer of APIDRA: Disetronic® H-Tron® plus V100 and D-Tron® with Disetronic catheters (Rapid™, Rapid C™, Rapid D™, and Tender™) MiniMed® Models 506, 507, 507c and 508 with MiniMed catheters (Sof-set Ultimate QR™, and Quick-set™). Before using a different insulin pump with APIDRA, read the pump label to make sure the pump has been evaluated with APIDRA. To minimize insulin degradation, infusion set occlusion, and loss of the preservative (metacresol), the infusion sets (reservoir, tubing, and catheter) and the APIDRA in the reservoir must be replaced at least every 48 hours and a new infusion site should be selected. The temperature of the insulin may exceed ambient temperature when the pump housing, cover, tubing or sport case is exposed to sunlight or radiant heat. Insulin exposed to temperatures higher than 98.6°F (37°C) should be discarded. Infusion sites that are erythematous, pruritic, or thickened should be reported to the healthcare professional, and a new site selected because continued infusion may increase the skin reaction or alter the absorption of APIDRA. Pump or infusion set malfunctions or handling errors or insulin degradation can lead to rapid hyperglycemia, and ketosis and diabetic ketoacidosis. This is especially pertinent for rapid-acting insulin analogs that are more rapidly absorbed through skin and have a shorter duration of action. Prompt identification and correction of the cause of hyperglycemia or ketosis or diabetic ketoacidosis is necessary. Problems include pump malfunction, infusion set occlusion, leakage, disconnection or kinking, handling errors and degraded insulin. Less commonly, hypoglycemia from pump malfunction may occur. If these problems cannot be promptly corrected, patients should resume therapy with subcutaneous insulin injection and contact their healthcare professional. Patients administering APIDRA by continuous subcutaneous infusion must have an alternative insulin delivery system in case of pump system failure. [See DOSAGE AND ADMINISTRATION, WARNINGS AND PRECAUTIONS, and HOW SUPPLIED/Storage and Handling]. Nonclinical Toxicology Carcinogenesis, Mutagenesis, Impairment Of Fertility Standard 2-year carcinogenicity studies in animals have not been performed. In Sprague Dawley rats, a 12-month repeat dose toxicity study was conducted with insulin glulisine at subcutaneous doses of 2.5, 5, 20 or 50 Units/kg twice daily (dose resulting in an exposure 1, 2, 8, and 20 times the average human dose, based on body surface area comparison). There was a non-dose dependent higher incidence of mammary gland tumors in female rats administered insulin glulisine compared to untreated controls. The incidence of mammary tumors for insulin glulisine and regular human insulin was similar. The relevance of these findings to humans is not known. Insulin glulisine was not mutagenic in the following tests: Ames test, in vitro mammalian chromosome aberration test in V79 Chinese hamster cells, and in vivo mammalian erythrocyte micronucleus test in rats. In fertility studies in male and female rats at subcutaneous doses up to 10 Units/kg once daily (dose resulting in an exposure 2 times the average human dose, based on body surface area comparison), no clear adverse effects on male and female fertility, or general reproductive performance of animals were observed. Use In Specific Populations Pregnancy Pregnancy Category C Reproduction and teratology studies have been performed with insulin glulisine in rats and rabbits using regular human insulin as a comparator. Insulin glulisine was given to female rats throughout pregnancy at subcutaneous doses up to 10 Units/kg once daily (dose resulting in an exposure 2 times the average human dose, based on body surface area comparison) and did not have any remarkable toxic effects on embryo-fetal development. Insulin glulisine was given to female rabbits throughout pregnancy at subcutaneous doses up to 1.5 Units/kg/day (dose resulting in an exposure 0.5 times the average human dose, based on body surface area comparison). Adverse effects on embryo-fetal development were only seen at maternal toxic dose levels inducing hypoglycemia. Increased incidence of post-implantation losses and skeletal defects were observed at a dose level of 1.5 Units/kg once daily (dose resulting in an exposure 0.5 times the average human dose, based on body surface area comparison) that also caused mortality in dams. A slight increased incidence of post-implantation losses was seen at the next lower dose level of 0.5 Units/kg once daily (dose resulting in an exposure 0.2 times the average human dose, based on body surface area comparison) which was also associated with severe hypoglycemia but there were no defects at that dose. No effects were observed in rabbits at a dose of 0.25 Units/kg once daily (dose resulting in an exposure 0.1 times the average human dose, based on body surface area comparison). The effects of insulin glulisine did not differ from those observed with subcutaneous regular human insulin at the same doses and were attributed to secondary effects of maternal hypoglycemia. There are no well-controlled clinical studies of the use of APIDRA in pregnant women. Because animal reproduction studies are not always predictive of human response, this drug should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus. It is essential for patients with diabetes or a history of gestational diabetes to maintain good metabolic control before conception and throughout pregnancy. Insulin requirements may decrease during the first trimester, generally increase during the second and third trimesters, and rapidly decline after delivery. Careful monitoring of glucose control is essential in these patients. Nursing Mothers It is unknown whether insulin glulisine is excreted in human milk. Because many drugs are excreted in human milk, caution should be exercised when APIDRA is administered to a nursing woman. Use of APIDRA is compatible with breastfeeding, but women with diabetes who are lactating may require adjustments of their insulin doses. Pediatric Use The safety and effectiveness of subcutaneous injections of APIDRA have been established in pediatric patients (age 4 to 17 years) with type 1 diabetes [See Clinical Studies]. APIDRA has not been studied in pediatric patients with type 1 diabetes younger than 4 years of age and in pediatric patients with type 2 diabetes. As in adults, the dosage of APIDRA must be individualized in pediatric patients based on metabolic needs and frequent monitoring of blood glucose. Geriatric Use In clinical trials (n=2408), APIDRA was administered to 147 patients ≥ 65 years of age and 27 patients ≥ 75 years of age. The majority of this small subset of elderly patients had type 2 diabetes. The change in HbA1c values and hypoglycemia frequencies did not differ by age. Nevertheless, caution should be exercised when APIDRA is administered to geriatric patients.

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