ADACEL  TDAP - clostridium tetani toxoid antigen (formaldehyde inactivated), corynebacterium diphtheriae toxoid antigen (formaldehyde inactivated), bordetella pertussis toxoid antigen (glutaraldehyde inactivated), bordetella pertussis filamentous hemagglutinin antigen (formaldehyde inactivated), bordetella pertussis pertactin antigen and bordetella pertussis fimbriae 2/3 antigen injection, suspension 
Sanofi Pasteur Inc.

Disclaimer: This drug has not been found by FDA to be safe and effective, and this labeling has not been approved by FDA. For further information about unapproved drugs, click here.

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HIGHLIGHTS OF PRESCRIBING INFORMATION
These highlights do not include all the information needed to use Adacel safely and effectively. See full prescribing information for Adacel.

Adacel (Tetanus Toxoid, Reduced Diphtheria Toxoid and Acellular Pertussis Vaccine Adsorbed )
Suspension for Intramuscular Injection
Initial U.S. Approval: 2005


INDICATIONS AND USAGE

  • Adacel is a vaccine indicated for active booster immunization against tetanus, diphtheria and pertussis. Adacel is approved for use as a single dose in persons 11 through 64 years of age. (1)

DOSAGE AND ADMINISTRATION

  • A single Intramuscular injection of 0.5 mL. (2.1)

DOSAGE FORMS AND STRENGTHS

  • Single-dose vials and prefilled syringes containing a 0.5-mL suspension for injection. (3)

CONTRAINDICATIONS

  • Severe allergic reaction (eg, anaphylaxis) to any component of Adacel or any other diphtheria toxoid, tetanus toxoid and pertussis antigen containing vaccine. (4.1)
  • Encephalopathy (e.g., coma, decreased level of consciousness, prolonged seizures) within 7 days of administration of a previous pertussis antigen-containing vaccine. (4.2)

WARNINGS AND PRECAUTIONS

  • The tip caps of the Adacel prefilled syringes may contain natural rubber latex, which may cause allergic reactions in latex sensitive individuals.(5.2, 17)
  • If Guillain-Barré syndrome occurred within 6 weeks of receipt of a prior vaccine containing tetanus toxoid, the risk for Guillain-Barré syndrome may be increased following a subsequent dose of Adacel vaccine.(5.3)
  • Progressive or unstable neurologic conditions are reasons to defer Adacel vaccination (5.4)
  • Persons who experienced an Arthus-type hypersensitivity reaction following a prior dose of a tetanus toxoid-containing vaccine should not receive Adacel unless at least 10 years have elapsed since the last dose of a tetanus toxoid-containing vaccine. (5.5)

ADVERSE REACTIONS

  • The most common solicited injection site reactions occuring within 0-14 days following vaccination with Adacel were
    -
    For Adolescents 11-17 years of age: pain (77.8%), swelling (20.9%), erythema (20.8%).
    -
    For Adults 18-64 years of age: pain (65.7%), swelling (21.0%), erythema (24.7%) (6.1).
  • The most common solicited systemic reactions occurring within 0-14 days following vaccination with Adacel were:
    -
    For Adolescents 11-17 years of age: headache (43.7%), body ache or muscle weakness (30.4%), tiredness (15.1%).
    -
    For Adults 18-64 years of age: headache (33.9%), body ache or muscle weakness (21.9%) (6.1).

To report SUSPECTED ADVERSE REACTIONS, contact Pharmacovigilance Department, Sanofi Pasteur Inc., Discovery Drive, Swiftwater, PA 18370 at 1-800-822-2463 (1-800-VACCINE) or VAERS at 1-800-822-7967 or http://vaers.hhs.gov.


DRUG INTERACTIONS

  • When Adacel vaccine was administered concomitantly with trivalent inactivated influenza vaccine (TIV) to subjects 19-64 years of age, a lower antibody response was observed for pertactin antigen as compared to Adacel vaccine administered alone. (7.1, 14.4)
  • Immunosuppressive therapies may reduce the immune response to Adacel. (7.2)
  • Do not mix Adacel vaccine with any other vaccine in the same syringe or vial.

USE IN SPECIFIC POPULATIONS

  • Safety and effectiveness of Adacel vaccine have not been established in pregnant women (8.1)
  • Pregnancy Surveillance Registry: contact Sanofi Pasteur Inc. at 1-800-822-2463 (1-800-VACCINE) (8.1)


See 17 for PATIENT COUNSELING INFORMATION

Revised: 02/2012

FULL PRESCRIBING INFORMATION: CONTENTS*
* Sections or subsections omitted from the full prescribing information are not listed

1 INDICATIONS AND USAGE

2 DOSAGE AND ADMINISTRATION

2.1 Preparation for Administration

2.2 Administration, Dose and Schedule

2.3 Additional Dosing Information

3 DOSAGE FORMS AND STRENGTHS

4 CONTRAINDICATIONS

4.1 Hypersensitivity

4.2 Encephalopathy

5 WARNINGS AND PRECAUTIONS

5.1 Management of Acute Allergic Reactions

5.2 Latex

5.3 Guillain-Barré Syndrome and Brachial Neuritis

5.4 Progressive or Unstable Neurologic Disorders

5.5 Arthus- Type Hypersensitivity

5.6 Altered Immunocompetence

6 ADVERSE REACTIONS

6.1 Data from Clinical Studies

6.2 Data From Post-Marketing Experience

7 DRUG INTERACTIONS

7.1 Concomitant Vaccine Administration

7.2 Immunosuppressive Treatments

8 USE IN SPECIFIC POPULATIONS

8.1 Pregnancy

8.3 Nursing Mothers

8.4 Pediatric Use

8.5 Geriatric Use

11 DESCRIPTION

12 CLINICAL PHARMACOLOGY

12.1 Mechanism of Action

13 NON-CLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

14 CLINICAL STUDIES

14.1 Immunological Evaluation of Adacel Vaccine

14.2 Immunological Evaluation in Adolescents and Adults 11 Through 64 Years of Age

14.3 Concomitant Hepatitis B Vaccine Administration

14.4 Concomitant Influenza Vaccine Administration

15 REFERENCES

16 HOW SUPPLIED/STORAGE AND HANDLING

17 PATIENT COUNSELING INFORMATION

PRINCIPAL DISPLAY PANEL - 0.5 mL Syringe Label

PRINCIPAL DISPLAY PANEL - 5 Syringe Carton


FULL PRESCRIBING INFORMATION

1 INDICATIONS AND USAGE

Adacel is a vaccine indicated for active booster immunization against tetanus, diphtheria and pertussis. Adacel vaccine is approved for use as a single dose in individuals 11 through 64 years of age.

2 DOSAGE AND ADMINISTRATION

2.1 Preparation for Administration

Just before use, shake the vial or syringe well until a uniform, white, cloudy suspension results.

Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit. If either of these conditions exist, the vaccine should not be administered.

When withdrawing a dose from a stoppered vial, do not remove either the stopper or the metal seal holding it in place. Use a separate sterile needle and syringe for each injection. Using a sterile needle and syringe, withdraw the 0.5 mL dose of vaccine from the single-dose vial and administer the vaccine to the individual. Changing needles between withdrawing the vaccine from the vial and injecting it into a recipient is not necessary unless the needle has been damaged or contaminated.

Adacel vaccine should not be combined through reconstitution or mixed with any other vaccine.

2.2 Administration, Dose and Schedule

Adacel vaccine is administered as a single 0.5 mL intramuscular injection into the deltoid muscle of the upper arm.

Do not administer this product intravenously, subcutaneously or intradermally.

There are no data to support repeat administration of Adacel vaccine.

Five years should have elapsed since the recipient's last dose of tetanus toxoid, diphtheria toxoid and/or pertussis containing vaccine and the administration of Adacel vaccine.

2.3 Additional Dosing Information

Primary series: The safety and effectiveness of Adacel vaccine used as a primary series or to complete the primary series, for diphtheria, tetanus, or pertussis has not been demonstrated.

Wound management: If tetanus prophylaxis is needed for wound management, Adacel may be given if no previous dose of any Tetanus Toxoid, Reduced Diphtheria Toxoid and Acellular Pertussis Vaccine, Adsorbed (Tdap) has been administered.

3 DOSAGE FORMS AND STRENGTHS

ADACEL vaccine is a suspension for injection (0.5mL dose) available in 0.5 mL single-dose vials and prefilled syringes. [See Dosage and Administration (2.2) and How Supplied (16)]

4 CONTRAINDICATIONS

4.1 Hypersensitivity

A severe allergic reaction (eg, anaphylaxis) after a previous dose of any tetanus toxoid, diphtheria toxoid or pertussis containing vaccine or any other component of this vaccine is a contraindication to administration of Adacel vaccine.[See DESCRIPTION (11).] Because of uncertainty as to which component of the vaccine may be responsible, none of the components should be administered. Alternatively, such individuals may be referred to an allergist for evaluation if further immunizations are to be considered.

4.2 Encephalopathy

Encephalopathy (eg, coma , prolonged seizures, or decreased level of consciousness) within 7 days of a previous dose of a pertussis containing vaccine not attributable to another identifiable cause is a contraindication to administration of any pertussis containing vaccine, including Adacel vaccine.

5 WARNINGS AND PRECAUTIONS

5.1 Management of Acute Allergic Reactions

Epinephrine hydrochloride solution (1:1,000) and other appropriate agents and equipment must be available for immediate use in case an anaphylactic or acute hypersensitivity reaction occurs.

5.2 Latex

The tip caps of the Adacel prefilled syringe may contain natural rubber latex, which may cause allergic reactions in latex sensitive individuals. The vial stopper does not contain latex.[ See 16 HOW SUPPLIED/STORAGE AND HANDLING]

5.3 Guillain-Barré Syndrome and Brachial Neuritis

A review by the Institute of Medicine found evidence for acceptance of a causal relation between tetanus toxoid and both brachial neuritis and Guillain-Barré syndrome.(1) If Guillain-Barré syndrome occurred within 6 weeks of receipt of prior vaccine containing tetanus toxoid, the risk for Guillain-Barré syndrome may be increased following a dose of Adacel vaccine.

5.4 Progressive or Unstable Neurologic Disorders

Progressive or unstable neurologic conditions are reasons to defer Adacel. It is not known whether administration of Adacel to persons with an unstable or progressive neurologic disorder might hasten manifestations of the disorder or affect the prognosis. Administration of Adacel to persons with an unstable or progressive neurologic disorder may result in diagnostic confusion between manifestations of the underlying illness and possible adverse effects of vaccination.

5.5 Arthus- Type Hypersensitivity

Persons who experienced an Arthus-type hypersensitivity reaction following a prior dose of a tetanus toxoid-containing vaccine should not receive Adacel unless at least 10 years have elapsed since the last dose of a tetanus toxoid containing vaccine.

5.6 Altered Immunocompetence

If Adacel vaccine is administered to immunocompromised persons, including persons receiving immunosupressive therapy, the expected immune response may not be obtained. [See Drug Interactions (7.2).]

6 ADVERSE REACTIONS

6.1 Data from Clinical Studies

Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a vaccine cannot be directly compared to rates in the clinical trials of another vaccine and may not reflect the rates observed in practice. The adverse reaction information from clinical trials does, however, provide a basis for identifying the adverse events that appear to be related to vaccine use and for approximating rates of those events. As with any vaccine, there is the possibility that broad use of Adacel vaccine could reveal adverse reactions not observed in clinical trials.

The safety of Adacel vaccine was evaluated in 4 clinical studies. A total of 5,841 individuals 11 through 64 years of age inclusive (3,393 adolescents 11- through 17 years of age and, 2,448 adults 18- through 64 years of age) received a single dose of Adacel vaccine.

Clinical study Td506 was a randomized, observer-blind, active controlled trial that enrolled adolescents 11 through 17 years of age (Adacel vaccine N = 1,184; Td vaccine N = 792) and adults 18 through 64 years of age (Adacel vaccine N = 1,752; Td vaccine N = 573). Study participants had not received tetanus or diphtheria containing vaccines within the previous 5 years. Solicited local and systemic reactions and unsolicited adverse events were monitored daily for 14 days post-vaccination using a diary card. From days 14-28 post-vaccination, information on adverse events necessitating a medical contact, such as a telephone call, visit to an emergency room, physician's office or hospitalization, was obtained via telephone interview or at an interim clinic visit. From days 28 to 6 months post-vaccination, participants were monitored for unexpected visits to a physician's office or to an emergency room, onset of serious illness and hospitalizations. Information regarding adverse events that occurred in the 6 month post-vaccination time period was obtained from participants via telephone contact. At least 96% of participants completed the 6-month follow-up evaluation.

Solicited Adverse Events in the US Adolescent and Adult study (Td506)

The frequency of selected solicited adverse events (erythema, swelling, pain and fever) occurring during days 0-14 following vaccination with Adacel vaccine or Td vaccine in adolescents 11 through 17 years of age and adults 18 through 64 years of age are presented in Table 1. Most of these events were reported at a similar frequency in recipients of both Adacel vaccine and Td vaccine. Pain at the injection site was the most common adverse reaction in 62.9% to 77.8% of all vaccinees. In addition, overall rates of pain were higher in adolescent recipients of Adacel vaccine compared to Td vaccine recipients. Rates of moderate and severe pain in adolescents did not significantly differ between the Adacel vaccine and Td vaccine groups. Among adults the rates of pain, after receipt of Adacel vaccine or Td vaccine, did not significantly differ. Fever of 38°C and higher was uncommon, although in the adolescent age group, it occurred significantly more frequently in Adacel vaccine recipients than Td vaccine recipients.

Table 1: Frequencies of Solicited Injection Site Reactions and Fever for Adolescents and Adults, Days 0-14, Following Vaccination with Adacel Vaccine or Td Vaccine in Study Td506
Adverse Event*Adolescents
11-17 years
Adults
18-64 years
Adacel
N = 1,170-1,175 (%)
Td
N = 783-787 (%)
Adacel
N= 1,688-1,698 (%)
Td
N = 551-561(%)
*
The study sample size was designed to detect >10% differences between Adacel and Td vaccines for events of 'Any' intensity.
N = number of participants with available data.
Tetanus and Diphtheria Toxoids Adsorbed for Adult Use manufactured by Sanofi Pasteur Inc., Swiftwater, PA.
§
Adacel vaccine did not meet the non-inferiority criterion for rates of 'Any' Pain in adolescents compared to Td vaccine rates (upper limit of the 95% CI on the difference for Adacel vaccine minus Td vaccine was 10.7% whereas the criterion was <10%). For 'Any' Fever the non-inferiority criteria was met, however, 'Any' Fever was statistically higher in adolescents receiving Adacel vaccine.
Interfered with activities, but did not necessitate medical care or absenteeism.
#
Incapacitating, prevented the performance of usual activities, may have/or did necessitate medical care or absenteeism.
Injection Site PainAny77.8§71.065.762.9
Moderate18.015.615.110.2
Severe#1.50.61.10.9
Injection Site SwellingAny20.918.321.017.3
Moderate
  1.0 to 3.4 cm6.55.77.65.4
Severe#
  ≥3.5 cm6.45.55.85.5
  ≥5 cm (2 inches)2.83.63.22.7
Injection Site ErythemaAny20.819.724.721.6
Moderate
  1.0 to 3.4 cm5.94.68.08.4
Severe#
  ≥3.5 cm6.05.36.24.8
  ≥5 cm (2 inches)2.72.94.03.0
Fever≥38.0°C (≥100.4°F)5.0§2.71.41.1
≥38.8°C to ≤39.4°C
(≥102.0°F to ≤103.0°F)
0.90.60.40.2
≥39.5°C (≥103.1°F)0.20.10.00.2

The frequency of other solicited adverse events (days 0-14) are presented in Table 2. The rates of these events following Adacel vaccine were comparable with those observed with Td vaccine. Headache was the most frequent systemic reaction and was usually of mild to moderate intensity.

Table 2: Frequencies of Other Solicited Adverse Events for Adolescents and Adults, Days 0-14, Following Vaccination with Adacel Vaccine or Td Vaccine in Study Td506
Adverse EventAdolescents 11-17 yearsAdults 18-64 years
Adacel
N* = 1,174-1,175 (%)
Td
N* = 787 (%)
Adacel
N* = 1,697-1,698 (%)
Td
N* = 560-561 (%)
*
N = number of participants with available data.
Tetanus and Diphtheria Toxoids Adsorbed for Adult Use manufactured by Sanofi Pasteur Inc., Swiftwater, PA.
Interfered with activities, but did not necessitate medical care or absenteeism.
§
Incapacitating, prevented the performance of usual activities, may have/or did necessitate medical care or absenteeism.
HeadacheAny43.740.433.934.1
Moderate14.211.111.410.5
Severe§2.01.52.82.1
Body Ache or Muscle WeaknessAny30.429.921.918.8
Moderate8.56.96.15.7
Severe§1.30.91.20.9
TirednessAny30.227.324.320.7
Moderate9.87.56.96.1
Severe§1.21.01.30.5
ChillsAny15.112.68.16.6
Moderate3.22.51.31.6
Severe§0.50.10.70.5
Sore and Swollen JointsAny11.311.79.17.0
Moderate2.62.52.52.1
Severe§0.30.10.50.5
NauseaAny13.312.39.27.9
Moderate3.23.22.51.8
Severe§1.00.60.80.5
Lymph Node SwellingAny6.65.36.54.1
Moderate1.00.51.20.5
Severe§0.10.00.10.0
DiarrheaAny10.310.210.311.3
Moderate1.92.02.22.7
Severe§0.30.00.50.5
VomitingAny4.62.83.01.8
Moderate1.21.11.00.9
Severe§0.50.30.50.2
RashAny2.72.02.02.3

Injection site and systemic solicited reactions occurred at similar rates in Adacel vaccine and Td vaccine recipients in the 3 day post-vaccination period. Most injection site reactions occurred within the first 3 days after vaccination (with a mean duration of less than 3 days). The rates of unsolicited adverse events reported from days 14-28 post-vaccination were comparable between the two vaccine groups, as were the rates of unsolicited adverse events from day 28 through 6 months. There were no spontaneous reports of extensive limb swelling of the injected limb in study Td506, nor in the other three studies which also contributed to the safety database for Adacel vaccine.

Injection Site and Systemic Reactions when Given with Hepatitis B Vaccine

In the concomitant vaccination study with Adacel and Hepatitis B vaccines [See CLINICAL STUDIES (14).], injection site and systemic adverse events were monitored daily for 14 days post-vaccination using a diary card. Injection site adverse events were only monitored at site/arm of Adacel vaccine administration. Unsolicited reactions (including immediate reactions, serious adverse events and events that elicited seeking medical attention) were collected at a clinic visit or via telephone interview for the duration of the trial, ie, up to 6 months post-vaccination.

The rates reported for fever and injection site pain (at the Adacel vaccine administration site) were similar when Adacel and Hep B vaccines were given concurrently or separately. However, the rates of injection site erythema (23.4% for concomitant vaccination and 21.4% for separate administration) and swelling (23.9% for concomitant vaccination and 17.9% for separate administration) at the Adacel vaccine administration site were increased when co-administered. Swollen and/or sore joints were reported by 22.5% for concomitant vaccination and 17.9% for separate administration. The rates of generalized body aches in the individuals who reported swollen and/or sore joints were 86.7% for concomitant vaccination and 72.2% for separate administration. Most joint complaints were mild in intensity with a mean duration of 1.8 days. The incidence of other solicited and unsolicited adverse events were not different between the 2 study groups.

Injection Site and Systemic Reactions when Given with Trivalent Inactivated Influenza Vaccine (TIV)

In the concomitant vaccination study with Adacel vaccine and trivalent inactivated influenza vaccine [See CLINICAL STUDIES (14).], injection site and systemic adverse events were monitored for 14 days post-vaccination using a diary card. All unsolicited reactions occurring through day 14 were collected. From day 14 to the end of the trial, ie, up to 84 days, only events that elicited seeking medical attention were collected.

The rates of fever and injection site erythema and swelling were similar for recipients of concurrent and separate administration of Adacel vaccine and TIV. However, pain at the Adacel vaccine injection site occurred at statistically higher rates following concurrent administration (66.6%) versus separate administration (60.8%). The rates of sore and/or swollen joints were 13% for concurrent administration and 9% for separate administration. Most joint complaints were mild in intensity with a mean duration of 2.0 days. The incidence of other solicited and unsolicited adverse events were similar between the 2 study groups.

Additional Studies

In an additional study, 1,806 adolescents 11 through 17 years of age received Adacel vaccine as part of the lot consistency study used to support Adacel vaccine licensure. This study was a randomized, double-blind, multi-center trial designed to assess lot consistency as measured by the safety and immunogenicity of 3 lots of Adacel vaccine when given as a booster dose to adolescents 11 through 17 years of age inclusive. Local and systemic adverse events were monitored for 14 days post-vaccination using a diary card. Unsolicited adverse events and serious adverse events were collected for 28 days post-vaccination. Pain was the most frequently reported local adverse event occurring in approximately 80% of all participants. Headache was the most frequently reported systemic event occurring in approximately 44% of all participants. Sore and/or swollen joints were reported by approximately 14% of participants. Most joint complaints were mild in intensity with a mean duration of 2.0 days.

An additional 962 adolescents and adults received Adacel vaccine in three supportive Canadian studies used as the basis for licensure in other countries. Within these clinical trials, the rates of local and systemic reactions following Adacel vaccine were similar to those reported in the four principal trials in the US with the exception of a higher rate (86%) of adults experiencing 'any' local injection site pain. The rate of severe pain (0.8%), however, was comparable to the rates reported in four principal trials conducted in the US. There was one spontaneous report of whole-arm swelling of the injected limb among the 277 Td vaccine recipients, and two spontaneous reports among the 962 Adacel vaccine recipients in the supportive Canadian studies.

Serious Adverse Events in All Safety Studies

In all the studies, participants were monitored for serious adverse events throughout the duration of the study.

Throughout the 6-month follow-up period in study Td506, serious adverse events were reported in 1.5% of Adacel vaccine recipients and in 1.4% of Td vaccine recipients. Two serious adverse events in adults were neuropathic events that occurred within 28 days of Adacel vaccine administration; one severe migraine with unilateral facial paralysis and one diagnosis of nerve compression in neck and left arm. Similar or lower rates of serious adverse events were reported in the other trials in participants up to 64 years of age and no additional neuropathic events were reported.

6.2 Data From Post-Marketing Experience

The following adverse events of Adacel have been spontaneously reported in the US and other countries. Because these events are reported voluntarily from a population of uncertain size, it may not be possible to reliably estimate their frequency or establish a causal relationship to vaccine exposure.

The following adverse events were included based on one or more of the following factors: severity, frequency of reporting or strength of evidence for a causal relationship to Adacel vaccine.

  • Immune system disorders
    Anaphylactic reaction, hypersensitivity reaction (angioedema, edema, rash, hypotension)
  • Nervous system disorders
    Paraesthesia, hypoesthesia, Guillain-Barré syndrome, brachial neuritis, facial palsy, convulsion, syncope, myelitis
  • Cardiac disorders
    Myocarditis
  • Skin and subcutaneous tissue disorders
    Pruritus, urticaria
  • Musculoskeletal and connective tissue disorders
    Myositis, muscle spasm
  • General disorders and administration site conditions
    Large injection site reactions (>50 mm), extensive limb swelling from the injection site beyond one or both joints
    Injection site bruising, sterile abscess

7 DRUG INTERACTIONS

7.1 Concomitant Vaccine Administration

When Adacel vaccine is administered concomitantly with other injectable vaccines or Tetanus Immune Globulin, they should be given with separate syringes and at different injection sites. Adacel should not be mixed with any other vaccine in the same syringe or vial.

In clinical studies, Adacel vaccine was administered concomitantly with one of the following US- licensed vaccines: Hepatitis B (10mcg, two dose regimen) or trivalent inactivated influenza vaccines (TIV). [See Adverse Reactions (6.1) and CLINICAL STUDIES (14).]

Hepatitis B Vaccine

Concomitant immunization of Adacel vaccine with Hepatitis B vaccine did not result in reduced antibody responses to any of the antigens from either vaccine.

Trivalent Inactivated Influenza Vaccine (TIV)

No interference in tetanus and diphtheria seroprotection rates and responses to influenza vaccine, detoxified pertussis toxin (PT), fimbriae types 2 and 3 (FIM) or filamentous hemagglutinin (FHA) were observed when Adacel vaccine was administered concomitantly with TIV compared to separate administration. A lower pertactin (PRN) GMC was observed when Adacel vaccine was administered concomitantly with TIV compared to separate administration.

7.2 Immunosuppressive Treatments

Immunosuppressive therapies, including irradiation, antimetabolites, alkylating agents, cytotoxic drugs and corticosteroids (used in greater than physiologic doses), may reduce the immune response to vaccines. [See Warnings And Precautions (5.6).]

8 USE IN SPECIFIC POPULATIONS

8.1 Pregnancy

Pregnancy Category C

Animal reproduction studies have not been conducted with Adacel vaccine. It is also not known whether Adacel vaccine can cause fetal harm when administered to a pregnant woman or can affect reproduction capacity. Adacel vaccine should be given to a pregnant woman only if clearly needed.

Animal fertility studies have not been conducted with Adacel vaccine. The effect of Adacel vaccine on embryo-fetal and pre-weaning development was evaluated in two developmental toxicity studies using pregnant rabbits. Animals were administered Adacel vaccine twice prior to gestation, during the period of organogenesis (gestation day 6) and later during pregnancy on gestation day 29, 0.5 mL/rabbit/occasion (a 17-fold increase compared to the human dose of Adacel vaccine on a body weight basis), by intramuscular injection. No adverse effects on pregnancy, parturition, lactation, embryo-fetal or pre-weaning development were observed. There were no vaccine related fetal malformations or other evidence of teratogenesis noted in this study.

Registry of Receipt of Adacel vaccine during Pregnancy

Sanofi Pasteur Inc. maintains a surveillance registry to collect data on pregnancy outcomes and newborn health status outcomes following vaccination with Adacel vaccine during pregnancy. Women who receive Adacel vaccine during pregnancy are encouraged to contact directly or have their health-care professional contact Sanofi Pasteur Inc. at 1-800-822-2463 (1-800-VACCINE).

8.3 Nursing Mothers

It is not known whether Adacel vaccine is excreted in human milk. Because many drugs are excreted in human milk, caution should be exercised when Adacel vaccine is given to a nursing woman.

8.4 Pediatric Use

Adacel vaccine is not approved for individuals less than 11 years of age. Safety and effectiveness of Adacel vaccine in persons less than 11 years of age have not been established.

8.5 Geriatric Use

Adacel vaccine is not approved for use in individuals 65 years of age and older.

In a clinical study, individuals 65 years of age and older received a single dose of Adacel vaccine. Based on pre-specified criteria, persons 65 years of age and older who received a dose of Adacel vaccine had lower geometric mean concentrations of antibodies to PT, PRN and FIM when compared to infants who had received a primary series of Daptacel vaccine. [See Section 14 for description of Daptacel vaccine.]

11 DESCRIPTION

Adacel vaccine is a sterile isotonic suspension of tetanus and diphtheria toxoids and pertussis antigens adsorbed on aluminum phosphate, for intramuscular injection.

Each 0.5 mL dose contains 5 Lf tetanus toxoid (T), 2 Lf diphtheria toxoid (d), and acellular pertussis antigens [2.5 mcg detoxified pertussis toxin (PT), 5 mcg filamentous hemagglutinin (FHA), 3 mcg pertactin (PRN), 5 mcg fimbriae types 2 and 3 (FIM)].Other ingredients per 0.5 mL dose include 1.5 mg aluminum phosphate (0.33 mg aluminum) as the adjuvant, ≤5 mcg residual formaldehyde, <50 ng residual glutaraldehyde and 3.3 mg (0.6% v/v) 2-phenoxyethanol (not as a preservative). The antigens are the same as those in DAPTACEL®, Diphtheria and Tetanus Toxoids and Acellular Pertussis Vaccine Adsorbed (DTaP); however, Adacel vaccine is formulated with reduced quantities of diphtheria and detoxified PT.

The acellular pertussis vaccine components are produced from Bordetella pertussis cultures grown in Stainer-Scholte medium (2) modified by the addition of casamino acids and dimethyl-beta-cyclodextrin. PT, FHA and PRN are isolated separately from the supernatant culture medium. FIM are extracted and co-purified from the bacterial cells. The pertussis antigens are purified by sequential filtration, salt-precipitation, ultrafiltration and chromatography. PT is detoxified with glutaraldehyde, FHA is treated with formaldehyde, and the residual aldehydes are removed by ultrafiltration. The individual antigens are adsorbed onto aluminum phosphate.

The tetanus toxin is produced from Clostridium tetani grown in modified Mueller-Miller casamino acid medium without beef heart infusion. (3). Tetanus toxin is detoxified with formaldehyde and purified by ammonium sulfate fractionation and diafiltration. Corynebacterium diphtheriae is grown in modified Mueller's growth medium. (4) After purification by ammonium sulfate fractionation, diphtheria toxin is detoxified with formaldehyde and diafiltered.

The adsorbed diphtheria, tetanus and acellular pertussis components are combined with aluminum phosphate (as adjuvant), 2-phenoxyethanol (not as a preservative) and water for injection. Adacel vaccine does not contain a preservative.

In the guinea pig potency test, the tetanus component induces at least 2 neutralizing units/mL of serum and the diphtheria component induces at least 0.5 neutralizing units/mL of serum. The potency of the acellular pertussis vaccine components is evaluated by the antibody response of immunized mice to detoxified PT, FHA, PRN and FIM as measured by enzyme-linked immunosorbent assay (ELISA).

Diphtheria and tetanus toxoids are individually adsorbed onto aluminum phosphate.

12 CLINICAL PHARMACOLOGY

12.1 Mechanism of Action

Tetanus

Tetanus is a disease manifested primarily by neuromuscular dysfunction caused by a potent exotoxin released by C tetani.

Protection against disease is due to the development of neutralizing antibodies to tetanus toxin. A serum tetanus antitoxin level of at least 0.01 IU/mL, measured by neutralization assay is considered the minimum protective level. (5) (6)

Diphtheria

Diphtheria is an acute toxin-mediated disease caused by toxigenic strains of C diphtheriae. Protection against disease is due to the development of neutralizing antibodies to diphtheria toxin. A serum diphtheria antitoxin level of 0.01 IU/mL is the lowest level giving some degree of protection. Antitoxin levels of at least 0.1 IU/mL are generally regarded as protective. (5) Levels of 1.0 IU/mL have been associated with long-term protection. (7)

Pertussis

Pertussis (whooping cough) is a respiratory disease caused by B pertussis. This Gram-negative coccobacillus produces a variety of biologically active components, though their role in either the pathogenesis of, or immunity to, pertussis has not been clearly defined.

13 NON-CLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

Adacel vaccine has not been evaluated for carcinogenic or mutagenic potential, or impairment of fertility.

14 CLINICAL STUDIES

14.1 Immunological Evaluation of Adacel Vaccine

The efficacy of the tetanus toxoid and diphtheria toxoid used in Adacel vaccine was based on the immune response to these antigens compared to a US licensed Tetanus and Diphtheria Toxoids Adsorbed For Adult Use (Td) vaccine manufactured by Sanofi Pasteur Inc., Swiftwater, PA. The primary measures for immune response to the diphtheria and tetanus toxoids were the percentage of participants attaining an antibody level of at least 0.1 IU/mL.

The efficacy of the pertussis antigens used in Adacel vaccine was inferred based on a comparison of pertussis antibody levels achieved in recipients of a single booster dose of Adacel vaccine with those obtained in infants after three doses of DAPTACEL vaccine. In the Sweden I Efficacy Trial, three doses of DAPTACEL vaccine were shown to confer a protective efficacy of 84.9% (95% CI: 80.1%, 88.6%) against WHO defined pertussis (21 days of paroxysmal cough with laboratory-confirmed B pertussis infection or epidemiological link to a confirmed case). The protective efficacy against mild pertussis (defined as at least one day of cough with laboratory-confirmed B pertussis infection) was 77.9% (95% CI: 72.6%, 82.2%).(8)

In addition, the ability of Adacel vaccine to elicit a booster response (defined as rise in antibody concentration after vaccination) to the tetanus, diphtheria and pertussis antigens following vaccination was evaluated. The demonstration of a booster response depended on the antibody concentration to each antigen as established based on the 95th percentile of the pre-vaccination antibody concentrations observed in historical clinical trials with Adacel vaccine.

14.2 Immunological Evaluation in Adolescents and Adults 11 Through 64 Years of Age

Study Td506 was a comparative, multi-center, randomized, observer-blind, controlled trial which enrolled 4,480 participants; 2,053 adolescents (11 through 17 years of age) and 2,427 adults (18 through 64 years of age). Enrollment was stratified by age to ensure adequate representation across the entire age range. Participants had not received a tetanus or diphtheria toxoid containing vaccine within the previous 5 years. After enrollment participants were randomized to receive one dose of either Adacel vaccine or Td vaccine. A total of 4,461 randomized participants were vaccinated. The per-protocol immunogenicity subset included 1,270 Adacel vaccine recipients and 1,026 Td vaccine recipients. Sera were obtained before and approximately 35 days after vaccination. [Blinding procedures for safety assessments are described in ADVERSE REACTIONS (6).]

Demographic characteristics were similar within age groups and between the vaccine groups. A total of 76% of the adolescents and 1.1% of the adults reported a history of receiving 5 previous doses of diphtheria-tetanus-pertussis containing vaccines. Anti-tetanus and anti-diphtheria seroprotection rates (≥0.1 IU/mL) and booster response rates were comparable between Adacel and Td vaccines. (See Table 3 and Table 4.) Adacel vaccine induced pertussis antibody levels that were non-inferior to those of Swedish infants who received three doses of DAPTACEL vaccine. (See Table 5.) Acceptable booster responses to each of the pertussis antigens were also demonstrated, ie, the percentage of participants with a booster response exceeded the pre-defined lower limit. (See Table 6.)

Table 3: Pre-vaccination and Post-vaccination Antibody Responses and Booster Response Rates to Tetanus Toxoid Following Adacel Vaccine as Compared to Td Vaccine in Adolescents and Adults 11 Through 64 Years of Age
Tetanus Antitoxin (IU/mL)
Pre-Vaccination1 Month Post-Vaccination
Age Group
(years)
VaccineN*% ≥0.10
(95% CI)
% ≥1.0
(95% CI)
% ≥0.10
(95% CI)
% ≥1.0
(95% CI)
% Booster
(95% CI)
*
N = number of participants in the per-protocol population with available data.
Booster response is defined as: A four-fold rise in antibody concentration, if the pre-vaccination concentration was equal to or below the cut-off value and a two-fold rise in antibody concentration if the pre-vaccination concentration was above the cut-off value. The cut-off value for tetanus was 2.7 IU/mL.
Seroprotection rates at ≥0.10 IU/mL and booster response rates to Adacel vaccine were non-inferior to Td vaccine (upper limit of the 95% CI on the difference for Td vaccine minus Adacel vaccine <10%).
§
Seroprotection rates at ≥1.0 IU/mL were not prospectively defined as a primary endpoint.
Tetanus and Diphtheria Toxoids Adsorbed for Adult Use manufactured by Sanofi Pasteur Inc., Swiftwater, PA.
11-17Adacel52799.6
(98.6, 100.0)
44.6
(40.3, 49.0)
100.0
(99.3, 100.0)
99.6
(98.6, 100.0)
91.7
(89.0, 93.9)
Td51699.2
(98.0, 99.8)
43.8
(39.5, 48.2)
100.0
(99.3, 100.0)
99.4
(98.3, 99.9)
91.3
(88.5, 93.6)
18-64Adacel742-74397.3
(95.9, 98.3)
72.9
(69.6, 76.1)
100.0
(99.5, 100.0)
97.8§
(96.5, 98.8)
63.1
(59.5, 66.6)
Td50995.9
(93.8, 97.4)
70.3
(66.2, 74.3)
99.8
(98.9, 100.0)
98.2
(96.7, 99.2)
66.8
(62.5, 70.9)
Table 4: Pre-vaccination and Post-vaccination Antibody Responses and Booster Response Rates to Diphtheria Toxoid Following Adacel Vaccine as Compared to Td Vaccine in Adolescents and Adults 11 Through 64 Years of Age
Diphtheria Antitoxin (IU/mL)
Pre-Vaccination1 Month Post-Vaccination
Age Group
(years)
VaccineN*% ≥0.10
(95% CI)
% ≥1.0
(95% CI)
% ≥0.10
(95% CI)
% ≥1.0
(95% CI)
% Booster
(95% CI)
*
N = number of participants in the per-protocol population with available data.
Booster response is defined as: A four-fold rise in antibody concentration, if the pre-vaccination concentration was equal to or below the cut-off value and a two-fold rise in antibody concentration if the pre-vaccination concentration was above the cut-off value. The cut-off value for diphtheria was 2.56 IU/mL.
Seroprotection rates at ≥0.10 IU/mL and booster response rates to Adacel vaccine were non-inferior to Td vaccine (upper limit of the 95% CI on the difference for Td vaccine minus Adacel vaccine <10%).
§
Seroprotection rates at ≥1.0 IU/mL were not prospectively defined as a primary endpoint.
Tetanus and Diphtheria Toxoids Adsorbed for Adult Use manufactured by Sanofi Pasteur Inc., Swiftwater, PA.
11-17Adacel52772.5
(68.5, 76.3)
15.7
(12.7, 19.1)
99.8
(98.9, 100.0)
98.7§
(97.3, 99.5)
95.1
(92.9, 96.8)
Td515-51670.7
(66.5, 74.6)
17.3
(14.1, 20.8)
99.8
(98.9, 100.0)
98.4
(97.0, 99.3)
95.0
(92.7, 96.7)
18-64Adacel739-74162.6
(59.0, 66.1)
14.3
(11.9, 17.0)
94.1
(92.1, 95.7)
78.0§
(74.8, 80.9)
87.4
(84.8, 89.7)
Td506-50763.3
(59.0, 67.5)
16.0
(12.9, 19.5)
95.1
(92.8, 96.8)
79.9
(76.1, 83.3)
83.4
(79.9, 86.5)
Table 5: Ratio of Pertussis Antibody Geometric Mean Concentrations (GMCs)* Observed One Month After a Dose of Adacel Vaccine in Adolescents and Adults 11 Through 64 Years of Age Compared with Those Observed in Infants One Month Following Vaccination at 2, 4 and 6 Months of Age in the Efficacy Trial with DAPTACEL Vaccine
Adolescents 11-17 Years of AgeAdults 18-64 Years of Age
Adacel/DAPTACEL
GMC Ratio
(95% CIs)
Adacel§/DAPTACEL
GMC Ratio
(95% CIs)
*
Antibody GMCs, measured in arbitrary ELISA units were calculated separately for infants, adolescents and adults.
N = 524 to 526, number of adolescents in the per-protocol population with available data for Adacel vaccine.
N = 80, number of infants who received DAPTACEL vaccine with available data post-dose 3 (Sweden Efficacy I).
§
N = 741, number of adults in the per-protocol population with available data for Adacel vaccine.
GMC following Adacel vaccine was non-inferior to GMC following DAPTACEL vaccine (lower limit of 95% CI on the ratio of GMC for Adacel vaccine divided by DAPTACEL vaccine >0.67).
Anti-PT3.6
(2.8, 4.5)
2.1
(1.6, 2.7)
Anti-FHA5.4
(4.5, 6.5)
4.8
(3.9, 5.9)
Anti-PRN3.2
(2.5, 4.1)
3.2
(2.3, 4.4)
Anti-FIM5.3
(3.9, 7.1)
2.5
(1.8, 3.5)
Table 6: Booster Response Rates to the Pertussis Antigens Observed One Month After a Dose of Adacel Vaccine in Adolescents and Adults 11 Through 64 Years of Age
Adolescents 11-17
Years of Age
Adults 18-64
Years of Age
Pre-defined
Acceptable Rates*
%
N%
(95% CI)
N%
(95% CI)
*
The acceptable response rate for each antigen was defined as the lower limit of the 95% CI for the rate being no more than 10% lower than the response rate observed in previous clinical trials.
A booster response for each antigen was defined as a four-fold rise in antibody concentration if the pre-vaccination concentration was equal to or below the cut-off value and a two-fold rise in antibody concentration if the pre-vaccination concentration was above the cut-off value. The cut-off values for pertussis antigens were established based on antibody data from both adolescents and adults in previous clinical trials.
The cut-off values were 85 EU/mL for PT, 170 EU/mL for FHA, 115 EU/mL for PRN and 285 EU/mL for FIM
N = number of participants in the per-protocol population with available data.
Anti-PT52492.0
(89.3, 94.2)
73984.4
(81.6, 87.0)
81.2
Anti-FHA52685.6
(82.3, 88.4)
73982.7
(79.8, 85.3)
77.6
Anti-PRN52594.5
(92.2, 96.3)
73993.8
(91.8, 95.4)
86.4
Anti-FIM52694.9
(92.6, 96.6)
73985.9
(83.2, 88.4)
82.4

14.3 Concomitant Hepatitis B Vaccine Administration

The concomitant use of Adacel vaccine and hepatitis B (Hep B) vaccine (Recombivax HB®, 10 mcg per dose using a two-dose regimen, manufactured by Merck and Co., Inc) was evaluated in a multi-center, open-labeled, randomized, controlled study that enrolled 410 adolescents, 11- through 14 years of age inclusive. One group received Adacel and Hep B vaccines concurrently (N = 206). The other group (N = 204) received Adacel vaccine at the first visit, then 4-6 weeks later received Hep B vaccine. The second dose of Hep B vaccine was given 4-6 weeks after the first dose. Serum samples were obtained prior to and 4-6 weeks after Adacel vaccine administration, as well as 4-6 weeks after the 2nd dose of Hep B for all participants. No interference was observed in the immune responses to any of the vaccine antigens when Adacel and Hep B vaccines were given concurrently or separately. [See Data From Clinical Studies (6.1).]

14.4 Concomitant Influenza Vaccine Administration

The concomitant use of Adacel vaccine and trivalent inactivated influenza vaccine (TIV, Fluzone®, manufactured by Sanofi Pasteur Inc., Swiftwater, PA) was evaluated in a multi-center, open-labeled, randomized, controlled study conducted in 720 adults, 19-64 years of age inclusive. In one group, participants received Adacel and TIV vaccines concurrently (N = 359). The other group received TIV at the first visit, then 4-6 weeks later received Adacel vaccine (N = 361). Sera were obtained prior to and 4-6 weeks after Adacel vaccine, as well as 4-6 weeks after the TIV. The immune responses were comparable for concurrent and separate administration of Adacel and TIV vaccines for diphtheria (percent of participants with seroprotective concentration ≥0.10 IU/mL and booster responses), tetanus (percent of participants with seroprotective concentration ≥0.10 IU/mL), pertussis antigens (booster responses and GMCs except lower PRN GMC in the concomitant group, lower bound of the 90% CI was 0.61 and the pre-specified criterion was ≥0.67) and influenza antigens (percent of participants with hemagglutination-inhibition [HI] antibody titer ≥1:40 IU/mL and ≥4-fold rise in HI titer). Although tetanus booster response rates were significantly lower in the group receiving the vaccines concurrently versus separately, greater than 98% of participants in both groups achieved seroprotective levels of ≥0.1 IU/mL. [See Data From Clinical Studies (6.1).]

15 REFERENCES

1
Stratton KR, et al, editors. Adverse events associated with childhood vaccines; evidence bearing on causality. Washington: National Academy Press; 1994. p. 67-117.
2
Stainer DW, et al. A simple chemically defined medium for the production of phase I Bordetella pertussis. J Gen Microbiol 1970;63:211-20.
3
Mueller JH, et al. Variable factors influencing the production of tetanus toxin. J Bacteriol 1954;67(3):271-7.
4
Stainer DW. Production of diphtheria toxin. In: Manclark CR, editor. Proceedings of an informal consultation on the World Health Organization requirements for diphtheria, tetanus, pertussis and combined vaccines. United States Public Health Service, Bethesda, MD. DHHS 91-1174. 1991. p. 7-11.
5
FDA. Department of Health and Human Services (DHHS). Biological products bacterial vaccines and toxoids; implementation of efficacy review; proposed rule. Fed Reg 1985;50(240):51002-117.
6
Wassilak SGF, et al. Tetanus toxoid. In: Plotkin SA, Orenstein WA, Offit PA, editors. Vaccines. 5th ed. Philadelphia, PA: WB Saunders Company; 2008. p. 805-39.
7
Vitek CR and Wharton M. Diphtheria toxoid. In: Plotkin SA, Orenstein WA, Offit PA, editors. Vaccines. 5th ed. Philadelphia, PA: W.B. Saunders Company; 2008. p. 139-56.
8
Gustafsson L, et al. A controlled trial of a two-component acellular, a five-component acellular and a whole-cell pertussis vaccine. N Engl J Med 1996;334(6):349-55.

16 HOW SUPPLIED/STORAGE AND HANDLING

Syringe, without needle, 1 dose (5 per package) Product No. 49281-400-15 The tip caps of the prefilled syringes may contain natural rubber latex. No other components contain latex.

Vial, 1 dose (5 per package) - Product No. 49281-400-05. Contains no latex.

Vial, 1 dose (10 per package) - Product No. 49281-400-10. Contains no latex.

Adacel vaccine should be stored at 2° to 8°C (35° to 46°F). DO NOT FREEZE. Product which has been exposed to freezing should not be used. Do not use after expiration date shown on the label.

17 PATIENT COUNSELING INFORMATION

Before administration of Adacel vaccine, health-care providers should inform the patient, parent or guardian of the benefits and risks of the vaccine and the importance of receiving recommended booster dose unless a contraindication to further immunization exists.

The health-care provider should inform the patient, parent or guardian about the potential for adverse reactions that have been temporally associated with Adacel vaccine or other vaccines containing similar components. The health-care provider should provide the Vaccine Information Statements (VISs) that are required by the National Childhood Vaccine Injury Act of 1986 to be given with each immunization. The patient, parent or guardian should be instructed to report any serious adverse reactions to their health-care provider.

Pregnancy Exposure Registry [See Pregnancy (8.1).]

Product information as of February 2012
Printed in Canada

Manufactured by:
Sanofi Pasteur Limited
Toronto Ontario Canada
Distributed by:
Sanofi Pasteur Inc.
Swiftwater PA 18370 USA
Adacel® is a registered trademark of the sanofi pasteur group, and its subsidiaries.

R7-0212 USA

PRINCIPAL DISPLAY PANEL - 0.5 mL Vial Label

NDC 49281-400-10

Adolescent/Adult
Tdap

Tetanus Toxoid,
Reduced Diphtheria
Toxoid and Acellular
Pertussis Vaccine
Adsorbed

Adacel®
Rx only

Sanofi Pasteur
Limited

IM only
1 Dose (0.5 mL)

PRINCIPAL DISPLAY PANEL - 0.5 mL Vial Label

PRINCIPAL DISPLAY PANEL - 10 Vial Carton

NDC 49281-400-10

Tetanus Toxoid,
Reduced Diphtheria
Toxoid and Acellular
Pertussis Vaccine
Adsorbed

Adacel®

Tdap

10 VIALS
1 Dose each

Rx only

For adolescent
and adult use.

sanofi pasteur

PRINCIPAL DISPLAY PANEL - 10 Vial Carton

PRINCIPAL DISPLAY PANEL - 0.5 mL Syringe Label

NDC 49281-400-15

0.5 mL Dose
IM only
Tdap

Tetanus Toxoid, Reduced
Diphtheria Toxoid and Acellular
Pertussis Vaccine Adsorbed

Adacel®
Adolescent/Adult
Sanofi Pasteur Limited

Rx only

Principal Display Panel - 0.5 mL Syringe Label

PRINCIPAL DISPLAY PANEL - 5 Syringe Carton

NDC 49281-400-15

Tdap

Tetanus Toxoid, Reduced
Diphtheria Toxoid
and Acellular
Pertussis Vaccine
Adsorbed

5 Prefilled
Syringes
0.5 mL each

Rx only

Adacel®

For adolescent
and adult use.

sanofi pasteur

Principal Display Panel - 5 Syringe Carton

ADACEL   TDAP
clostridium tetani toxoid antigen (formaldehyde inactivated), corynebacterium diphtheriae toxoid antigen (formaldehyde inactivated), bordetella pertussis toxoid antigen (glutaraldehyde inactivated), bordetella pertussis filamentous hemagglutinin antigen (formaldehyde inactivated), bordetella pertussis pertactin antigen, and bordetella pertussis fimbriae 2/3 antigen injection, suspension
Product Information
Product TypeVACCINEItem Code (Source)NDC:49281-400
Route of AdministrationINTRAMUSCULARDEA Schedule    
Active Ingredient/Active Moiety
Ingredient NameBasis of StrengthStrength
CLOSTRIDIUM TETANI TOXOID ANTIGEN (FORMALDEHYDE INACTIVATED) (CLOSTRIDIUM TETANI TOXOID ANTIGEN (FORMALDEHYDE INACTIVATED)) CLOSTRIDIUM TETANI TOXOID ANTIGEN (FORMALDEHYDE INACTIVATED)5 [Lf]  in 0.5 mL
CORYNEBACTERIUM DIPHTHERIAE TOXOID ANTIGEN (FORMALDEHYDE INACTIVATED) (CORYNEBACTERIUM DIPHTHERIAE TOXOID ANTIGEN (FORMALDEHYDE INACTIVATED)) CORYNEBACTERIUM DIPHTHERIAE TOXOID ANTIGEN (FORMALDEHYDE INACTIVATED)2 [Lf]  in 0.5 mL
BORDETELLA PERTUSSIS TOXOID ANTIGEN (GLUTARALDEHYDE INACTIVATED) (BORDETELLA PERTUSSIS TOXOID ANTIGEN (GLUTARALDEHYDE INACTIVATED)) BORDETELLA PERTUSSIS TOXOID ANTIGEN (GLUTARALDEHYDE INACTIVATED)2.5 ug  in 0.5 mL
BORDETELLA PERTUSSIS FILAMENTOUS HEMAGGLUTININ ANTIGEN (FORMALDEHYDE INACTIVATED) (BORDETELLA PERTUSSIS FILAMENTOUS HEMAGGLUTININ ANTIGEN (FORMALDEHYDE INACTIVATED)) BORDETELLA PERTUSSIS FILAMENTOUS HEMAGGLUTININ ANTIGEN (FORMALDEHYDE INACTIVATED)5 ug  in 0.5 mL
BORDETELLA PERTUSSIS PERTACTIN ANTIGEN (BORDETELLA PERTUSSIS PERTACTIN ANTIGEN) BORDETELLA PERTUSSIS PERTACTIN ANTIGEN3 ug  in 0.5 mL
BORDETELLA PERTUSSIS FIMBRIAE 2/3 ANTIGEN (BORDETELLA PERTUSSIS FIMBRIAE 2/3 ANTIGEN) BORDETELLA PERTUSSIS FIMBRIAE 2/3 ANTIGEN5 ug  in 0.5 mL
Inactive Ingredients
Ingredient NameStrength
ALUMINUM PHOSPHATE1.5 mg  in 0.5 mL
FORMALDEHYDE5 ug  in 0.5 mL
GLUTARAL50 ng  in 0.5 mL
PHENOXYETHANOL3.3 ug  in 0.5 mL
Product Characteristics
ColorWHITE (WHITE (CLOUDY)) Score    
ShapeSize
FlavorImprint Code
Contains    
Packaging
#Item CodePackage DescriptionMultilevel Packaging
1NDC:49281-400-1010 VIAL ( VIAL) in 1 PACKAGEcontains a VIAL
10.5 mL in 1 VIALThis package is contained within the PACKAGE (49281-400-10)
2NDC:49281-400-055 VIAL ( VIAL) in 1 PACKAGEcontains a VIAL
20.5 mL in 1 VIALThis package is contained within the PACKAGE (49281-400-05)
3NDC:49281-400-155 SYRINGE ( SYRINGE) in 1 PACKAGEcontains a SYRINGE
30.5 mL in 1 SYRINGEThis package is contained within the PACKAGE (49281-400-15)

Marketing Information
Marketing CategoryApplication Number or Monograph CitationMarketing Start DateMarketing End Date
UNAPPROVED DRUG OTHER06/10/2005

Labeler - Sanofi Pasteur Inc. (086723285)
Establishment
NameAddressID/FEIOperations
Sanofi Pasteur Limited208206623MANUFACTURE

Revised: 02/2012 Sanofi Pasteur Inc.