Havrix

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Havrix uses


1 INDICATIONS AND USAGE

Havrix is a vaccine indicated for the prevention of disease caused by Havrix virus in persons 12 months of age and older. The primary dose should be given at least 2 weeks prior to expected exposure to HAV. (1.1)

1.1 Indications and Use

Havrix® [Hepatitis A Vaccine, Inactivated] is indicated for the prevention of disease caused by Havrix virus (HAV) in persons 12 months of age and older. The primary dose should be given at least 2 weeks prior to expected exposure to HAV.

2 DOSAGE AND ADMINISTRATION

FOR INTRAMUSCULAR ADMINISTRATION ONLY.

2.1 Dosage and Schedule

Children/Adolescents (12 months through 18 years of age): The vaccination schedule consists of a primary 0.5-mL dose administered intramuscularly, and a 0.5-mL booster dose administered intramuscularly 6 to 18 months later.

Adults (19 years of age and older): The vaccination schedule consists of a primary 1-mL dose administered intramuscularly, and a 1-mL booster dose administered intramuscularly 6 to 18 months later.

Booster Immunization Following Another Manufacturer's Havrix Vaccine: A booster dose of Havrix may be given at 6 to 12 months following a primary dose of HAVRIX .

2.2 Preparation and Administration

Shake the single-dose vial or single-dose prefilled syringe well to obtain a slightly opaque, white suspension before withdrawal and use. Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit. Discard if the suspension does not appear homogenous or if extraneous particulate matter remains or discoloration is observed.

For single-dose vials, withdraw and administer entire dose of Havrix intramuscularly using a sterile needle and syringe.

For single-dose prefilled syringes, securely attach a needle by twisting in a clockwise direction and administer dose of Havrix intramuscularly.

For adults, adolescents, and children older than 2 years of age, the deltoid muscle is the preferred site for intramuscular injection. For children 12 through 23 months of age, the anterolateral area of the thigh is the preferred site for intramuscular injection.

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3 DOSAGE FORMS AND STRENGTHS

Suspension for injection available in four presentations:



Suspension supplied in four presentations:

4 CONTRAINDICATIONS

Do not administer Havrix to individuals with a history of immediate and/or severe allergic or hypersensitivity reactions (e.g., anaphylaxis) after a previous dose of any Havrix vaccine, or to individuals who have had an anaphylactic reaction to any component of Havrix, including neomycin .

Do not administer Havrix to individuals with a history of immediate and/or severe allergic or hypersensitivity reactions (e.g., anaphylaxis) after a previous dose of any Havrix vaccine or with an anaphylactic reaction to neomycin. (4, 11)

5 WARNINGS AND PRECAUTIONS

5.1 Prevention and Management of Allergic Vaccine Reactions

Appropriate medical treatment and supervision must be available to manage possible anaphylactic reactions following administration of the vaccine .

5.2 Hypersensitivity to Latex

The vial stopper and the syringe plunger stopper and tip cap contain dry natural latex rubber that may cause allergic reactions in latex-sensitive individuals.

5.3 Altered Immunocompetence

Immunocompromised persons, including individuals receiving immunosuppressive therapy, may have a diminished immune response to Havrix and may not be protected against HAV infection after vaccination .

5.4 Limitations of Vaccine Effectiveness

Havrix virus has a relatively long incubation period (approximately 20 to 50 days). Havrix may not prevent Havrix infection in individuals who have an unrecognized Havrix infection at the time of vaccination. Vaccination with Havrix may not result in a protective response in all susceptible vaccinees.

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6 ADVERSE REACTIONS

The most common local adverse reactions and systemic adverse events reported in different clinical trials across different age groups when Havrix was administered alone or concomitantly were:


To report SUSPECTED ADVERSE REACTIONS, contact Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc., at 1-877-888-4231 or VAERS at 1-800-822-7967 or www.vaers.hhs.gov.

6.1 Clinical Trials Experience

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 safety of Havrix has been evaluated in over 10,000 subjects 1 year to 85 years of age. Subjects were given one or two doses of the vaccine. The second (booster dose) was given 6 months or more after the first dose.

The most common local adverse reactions and systemic adverse events (≥15%) reported in different clinical trials across different age groups when Havrix was administered alone or concomitantly were:


Allergic Reactions

Local and/or systemic allergic reactions that occurred in <1% of over 10,000 children/adolescents or adults in clinical trials regardless of causality included: injection-site pruritus and/or rash; bronchial constriction; asthma; wheezing; edema/swelling; rash; generalized erythema; urticaria; pruritus; eye irritation/itching; dermatitis .

Children - 12 through 23 Months of Age

Across five clinical trials, 4374 children 12 to 23 months of age received one or two 25U doses of Havrix, including 3885 children who received 2 doses of Havrix and 1250 children who received Havrix concomitantly with one or more other vaccines, including Measles, Mumps, and Rubella Virus Vaccine, Live (M-M-R II®), Varicella Vaccine, Live (VARIVAX®), Diphtheria and Tetanus Toxoids and Acellular Pertussis Vaccine, Adsorbed (Tripedia or INFANRIX), Measles, Mumps, Rubella, and Varicella Vaccine, Live (ProQuad®), Pneumococcal 7-valent Conjugate Vaccine (Diphtheria CRM197, Prevnar), or Haemophilus B Conjugate Vaccine (Meningococcal Protein Conjugate, PedvaxHIB®). Overall, the race distribution of study subjects was as follows: 64.7% Caucasian; 15.7% Hispanic-American; 12.3% Black; 4.8% other; 1.4% Asian; and 1.1% Native American. The distribution of subjects by gender was 51.8% male and 48.2% female.

In an open-label clinical trial, 653 children 12 to 23 months of age were randomized to receive a first dose of Havrix with ProQuad and Prevnar concomitantly (N=330) or a first dose of ProQuad and pneumococcal 7-valent conjugate vaccine concomitantly, followed by a first dose of Havrix 6 weeks later (N=323). Approximately 6 months later, subjects received either the second doses of ProQuad and Havrix concomitantly or the second doses of ProQuad and Havrix separately. The race distribution of the study subjects was as follows: 60.3% Caucasian; 21.6% African-American; 9.5% Hispanic-American; 7.2% other; 1.1% Asian; and 0.3% Native American. The distribution of subjects by gender was 50.7% male and 49.3% female.

Table 1 presents rates of solicited local reactions at the Havrix injection site and rates of elevated temperatures (≥100.4°F and ≥102.2°F) that occurred within 5 days following each dose of Havrix and elevated temperatures >98.6°F for a total of 14 days after vaccination; occurrences of these events were recorded daily on diary cards. Table 2 presents rates of unsolicited systemic adverse events that occurred within 14 days at ≥5% in any group following each dose of Havrix.

Dose 1 Dose 2
Adverse reaction: Days 1-5 unless noted Havrix alone Havrix + ProQuad + Prevnar concomitantly Havrix alone Havrix + ProQuad concomitantly
N=number of subjects for whom data are available.
Injection site adverse reactions N=274 N=311 N=251 N=263
Injection site erythema 11.7% 9.6% 12.7% 9.5%
Injection site pain/tenderness 15.3% 20.9% 20.3% 17.5%
Injection site swelling 9.5% 6.8% 7.6% 6.1%
Temperature > 98.6°F or feverish (Days 1-14) 12.4% 35.7% 10.8% 10.3%
N=243 N=285 N=221 N=237
Temperature ≥ 100.4°F 10.3% 16.8% 10% 4.2%
Temperature ≥ 102.2 °F 2.1% 3.5% 2.3% 2.5%
Dose 1 Dose 2
Adverse Event: Days 1-14 Havrix alone Havrix + ProQuad + PREVNAR concomitantly Havrix alone Havrix + ProQuad concomitantly
N=274 N=311 N=251 N=263
General Disorders and Administration Site Conditions
Irritability 3.6% 6.1% 2.8% 2.7%
Infections and Infestations
Upper respiratory tract infection 3.3% 6.1% 4.8% 5.7%
Skin and Subcutaneous Tissue Disorders
Dermatitis diaper 1.1% 6.1% 2.4% 3.4%

In Stage I of an open, multicenter, randomized study, children 15 months of age were randomized to receive the first dose of Havrix alone (N=151) or concomitantly with PedvaxHIB and INFANRIX (N=155); another group of children 15 months of age were randomized to receive the first dose of Havrix alone (N=152) or concomitantly with PedvaxHIB (N=159). All groups received the second dose of Havrix alone at least 6 months following the first dose. The race distribution of Stage I study subjects was: 63.9% Caucasian; 17.5% Hispanic-American; 14.7% Black; 2.6% other; and 1.3% Asian. The distribution of subjects by gender was 54.0% male and 46.0% female. In Stage II of this study, an additional 654 children 12-17 months of age received the first dose of Havrix alone followed by the second dose of Havrix 6 months later. The race distribution of Stage II of the study subjects was: 66.1% Caucasian; 10.6% Hispanic-American; 16.8% Black; 4.7% other; and 1.5% Asian. The distribution of subjects by gender was 51.2% male and 48.8% female.

Table 3 presents rates of solicited local reactions at the Havrix injection-site and rates of elevated temperatures (≥100.4°F and ≥102.2°F) that occurred within 5 days following each dose of Havrix and elevated temperatures >98.6°F for a total of 14 days following each dose of Havrix. Occurrences of these events were recorded daily on diary cards. Table 4 presents rates of unsolicited systemic adverse events that occurred within 14 days at ≥5% following each dose of Havrix.

Stage I Stage II
Dose 1 Dose 2 Dose 1 Dose 2
Adverse Reaction: Days 1-5 unless noted Havrix alone Havrix + PedvaxHIB and Infanrix or Havrix + PedvaxHIB concomitantly Havrix alone Havrix alone Havrix alone
N= number of subjects for whom data is available
Injection site adverse reactions N=256 N=302 N=503 N=647 N=599
Injection site erythema 18.0% 19.9% 21.5% 11.7% 16.2%
Injection site pain/tenderness 21.9% 36.4% 27.4% 20.1% 22.9%
Injection site swelling 10.2% 14.2% 10.1% 7.1% 7.0%
Temperature > 98.6°F or feverish (Days 1-14) 10.2% 17.2% 10.7% 10.0% 8.2%
N=234 N=290 N=473 N=631 N=591
Temperature ≥ 100.4°F 9.0% 16.9% 9.1% 9.4% 8.6%
Temperature ≥ 102.2 °F 3.8% 3.1% 3.2% 2.9% 2.4%
Stage I Stage II
Dose 1 Dose 2 Dose 1 Dose 2
Adverse Event:

Days 1-14

Havrix alone Havrix + PedvaxHIB and Infanrix or

Havrix + PedvaxHIB concomitantly

Havrix alone Havrix alone Havrix alone
N=256 N=302 N=503 N=647 N=599
Gastrointestinal Disorders
Diarrhea 3.9% 8.3% 3.8% 4.6% 3.8%
Teething 3.1% 2.3% 1.4% 5.7% 4.3%
General Disorders and Administration Site Conditions
Irritability 6.3% 9.6% 4.0% 8.8% 6.5%
Infections and Infestations
Upper respiratory tract infection 2.3% 3.3% 3.0% 4.9% 5.2%
Respiratory, Thoracic and Mediastinal Disorders
Rhinorrhea 2.0% 4.0% 3.8% 6.2% 3.8%

Data presented in Tables 1 through 4 on solicited local reactions, and solicited and unsolicited systemic adverse events with incidence ≥5% following each dose of Havrix are representative of other clinical trials of Havrix in children 12 through 23 months of age. Across the five studies conducted in children 12-23 months of age, ≥39.9% of subjects experienced local adverse reactions and ≥55.7% of subjects experienced systemic adverse events. The majority of local and systemic adverse events were mild to moderate in intensity.

The following additional unsolicited local adverse reactions and systemic adverse events were observed at a common frequency of ≥1% to <10% in any individual clinical study. This listing includes only the adverse reactions not reported elsewhere in the label. These local adverse reactions and systemic adverse events occurred among recipients of Havrix alone or Havrix given concomitantly within 14 days following any dose of Havrix across four clinical studies.


Serious Adverse Events (Children 12 through 23 Months of Age): Across the five studies conducted in subjects 12-23 months of age, 0.7% (32/4374) of subjects reported a serious adverse event following any dose of Havrix, and 0.1% (5/4374) of subjects reported a serious adverse event judged to be vaccine related by the study investigator. The serious adverse events were collected over the period defined in each protocol (14, 28, or 42 days). Vaccine-related serious adverse events which occurred following any dose of Havrix with or without concomitant vaccines included febrile seizure (0.05%), dehydration (0.02%), gastroenteritis (0.02%), and cellulitis (0.02%).

Children/Adolescents - 2 Years through 18 Years of Age

In 11 clinical trials, 2615 healthy children 2 years through 18 years of age received at least one dose of Havrix. These studies included administration of Havrix in varying doses and regimens (1377 children received one or more 25U doses). The race distribution of the study subjects who received at least one dose of Havrix in these studies was as follows: 84.7% Caucasian; 10.6% American Indian; 2.3% African-American; 1.5% Hispanic-American; 0.6% other; 0.2% Oriental. The distribution of subjects by gender was 51.2% male and 48.8% female.

In a double-blind, placebo-controlled efficacy trial (i.e. The Monroe Efficacy Study), 1037 healthy children and adolescents 2 through 16 years of age were randomized to receive a primary dose of 25U of Havrix and a booster dose of Havrix 6, 12, or 18 months later, or placebo (alum diluent). All study subjects were Caucasian: 51.5% were male and 48.5% were female. Subjects were followed days 1 to 5 postvaccination for fever and local adverse reactions and days 1 to 14 for systemic adverse events. The most common adverse events/reactions were injection-site reactions, reported by 6.4% of subjects. Table 5 summarizes local adverse reactions and systemic adverse events reported in ≥1% of subjects. There were no significant differences in the rates of any adverse events or adverse reactions between vaccine and placebo recipients after Dose 1.

Adverse Event Havrix

(N=519)

Placebo (Alum Diluent)No statistically significant differences between the two groups. , Second injection of placebo not administered because code for the trial was broken. , Placebo (Alum diluent) = amorphous aluminum hydroxyphosphate sulfate.

(N=518)

Rate (Percent)

Dose 1

Rate (Percent)

Booster

Rate (Percent)

N=Number of subjects enrolled/randomized.
Percent=percentage of subjects for whom data are available with adverse event
n=number of subjects for whom adverse events available
Injection SiteAdverse Reactions at the injection site (VAQTA) Days 1-5 after vaccination with Havrix n=515 n=475 n=510
Pain 6.4% 3.4% 6.3%
Tenderness 4.9% 1.7% 6.1%
Erythema 1.9% 0.8% 1.8%
Swelling 1.7% 1.5% 1.6%
Warmth 1.7% 0.6% 1.6%
SystemicSystemic adverse events reported Days 1-15 after vaccination, regardless of causality. n=519 n=475 n=518
Abdominal pain 1.2% 1.1% 1.0%
Pharyngitis 1.2% 0% 0.8%
Headache 0.4% 0.8% 1.0%

Adults - 19 Years of Age and Older

In an open-label clinical trial, 240 healthy adults 18 to 54 years of age were randomized to receive either Havrix (50U/1-mL) with Typhim Vi (Typhoid Vi polysaccharide vaccine) and YF-Vax (yellow fever vaccine) concomitantly (N=80), typhoid Vi polysaccharide and yellow fever vaccines concomitantly (N=80), or Havrix alone (N=80). Approximately 6 months later, subjects who received Havrix were administered a second dose of Havrix. The race distribution of the study subjects who received Havrix with or without typhoid Vi polysaccharide and yellow fever vaccine was as follows: 78.3% Caucasian; 14.2% Oriental; 3.3% other; 2.1% African-American; 1.7% Indian; 0.4% Hispanic-American. The distribution of subjects by gender was 40.8% male and 59.2% female. Subjects were monitored for local adverse reactions and fever for 5 days and systemic adverse events for 14 days after each vaccination. In the 14 days after the first dose of Havrix, the proportion of subjects with adverse events was similar between recipients of Havrix given concomitantly with typhoid Vi polysaccharide and yellow fever vaccines compared to recipients of typhoid Vi polysaccharide and yellow fever vaccines without Havrix. Table 6 summarizes solicited local adverse reactions and Table 7 summarizes unsolicited systemic adverse events reported in ≥5% in adults who received one or two doses of Havrix alone and for subjects who received Havrix concomitantly with typhoid Vi polysaccharide and yellow fever vaccines. There were no solicited systemic complaints reported at a rate ≥5%. Fever ≥101°F occurred in 1.3% of subjects in each group.

Adverse Event Havrix administered alone

(N=80)

Havrix + ViCPSViCPS=Typhoid Vi polysaccharide vaccine. and Yellow Fever vaccines administered concomitantlyHavrix administered concomitantly with typhoid Vi polysaccharide (ViCPS) and yellow fever vaccines.

(N=80)

Rate (Percent)
N=Number of subjects enrolled/randomized.
Percent=percentage of subjects with adverse event.
Injection-site Adverse Reactions at the injection site (VAQTA) Days 1-5 after vaccination
Pain/tenderness/soreness 78.8% 70.3%
Warmth 23.7% 23.7%
Swelling 16.2% 8.8%
Erythema 17.5% 6.3%
Body System Havrix administered alone

(N=80)

Havrix + ViCPSViCPS=Typhoid Vi polysaccharide vaccine. and Yellow Fever vaccines administered concomitantlyHavrix administered concomitantly with typhoid Vi polysaccharide (ViCPS) and yellow fever vaccines.

(N=80)

Adverse Event
Rate (Percent)
N=Number of subjects enrolled/randomized with data available.
Percent=percentage of subjects with adverse event for whom data are available.
General disorders and administration site reactions Systemic Adverse Events reported Days 1-15 after vaccination, regardless of causality.
Asthenia/fatigue 7.5% 11.3%
Chills 1.3% 7.5%
Gastrointestinal disorders
Nausea 7.5% 12.5%
Musculoskeletal and connective tissue disorders
Myalgia 5.0% 10.0%
Arm pain 0.0% 6.3%
Nervous system disorders
Headache 23.8% 26.3%
Infections and infestations
Upper respiratory infection 7.5% 3.8%
Pharyngitis 2.5% 6.3%

In four clinical trials involving 1645 healthy adults 19 years of age and older who received one or more 50U doses of Havrix vaccine, subjects were followed for fever and local adverse reactions 1 to 5 days postvaccination and for systemic adverse events 1 to 14 days postvaccination. One single-blind study evaluated doses of Havrix with varying amounts of viral antigen and/or alum content in healthy adults ≥170 pounds and ≥30 years of age (N=210 adults administered 50U/1-mL dose). One open-label study evaluated Havrix given with immune globulin (IG) or alone (N=164 adults who received Havrix alone). A third study was single-blind and evaluated 3 different lots of Havrix (N=1112). The fourth study that was also single-blind evaluated doses of Havrix with varying amounts of viral antigen in healthy adults ≥170 pounds and ≥30 years of age (N=159 adults administered the 50U/1-mL dose). Overall, the race distribution of the study subjects who received at least one dose of Havrix was as follows: 94.2% Caucasian; 2.2% Black; 1.5% Hispanic; 1.5% Oriental; 0.4% other; 0.2% American Indian. 47.6% of subjects were male and 52.4% were female. The most common adverse event/reaction was injection-site pain/soreness/tenderness reported by 67.0% of subjects. Of all reported injection-site reactions 99.8% were mild (i.e., easily tolerated with no medical intervention) or moderate (i.e., minimally interfered with usual activity possibly requiring little medical intervention). Listed below in Table 8 are the local adverse reactions and systemic adverse events reported by ≥5% of subjects, in decreasing order of frequency within each body system.

Body System Havrix (Any Dose)

(N=1645)

Adverse Events Rate (n/total n)
N=Number of subjects enrolled/randomized.
n=Number of subjects in each category with data available.
Percent=percentage of subjects for whom data are available with adverse event.
Nervous system disorders Systemic Adverse Events reported Days 1 to 14 after vaccination, regardless of causality. n=1641
Headache 16.1%
General disorders and administration site reactions Adverse Reactions at the injection site (VAQTA) and measured fever Days 1 to 5 after vaccination. n=1640
Injection-site pain/tenderness/soreness 67.0%
Injection-site warmth 18.2%
Injection-site swelling 14.7%
Injection-site erythema 13.7%

The following additional unsolicited systemic adverse events were observed among recipients of Havrix that occurred within 14 days at a common frequency of ≥1% to <10% following any dose not reported elsewhere in the label. These adverse reactions have been reported across 4 clinical studies.

6.2 Post-Marketing Experience

The following additional adverse events have been reported with use of the marketed vaccine. Because these reactions are reported voluntarily from a population of uncertain size, it is not possible to reliably estimate their frequency or establish a causal relationship to a vaccine exposure.

Blood and lymphatic disorders: Thrombocytopenia.

Nervous system disorders: Guillain-Barré syndrome; cerebellar ataxia; encephalitis.

Post-Marketing Observational Safety Study

In a post-marketing, 60-day safety surveillance study, conducted at a large health maintenance organization in the United States, a total of 42,110 individuals ≥2 years of age received 1 or 2 doses of Havrix (13,735 children/adolescents and 28,375 adult subjects). Safety was passively monitored by electronic search of the automated medical records database for emergency room and outpatient visits, hospitalizations, and deaths. Medical charts were reviewed when an event was considered to be possibly vaccine-related by the investigator. None of the serious adverse events identified were assessed as being related to vaccine by the investigator. Diarrhea/gastroenteritis, resulting in outpatient visits, was determined by the investigator to be the only vaccine-related nonserious adverse reaction in the study. There was no vaccine-related adverse reaction identified that had not been reported in earlier clinical trials with Havrix.

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7 DRUG INTERACTIONS

7.1 Use with Other Vaccines

Do not mix Havrix with any other vaccine in the same syringe or vial. Use separate injection sites and syringes for each vaccine. Please refer to package inserts of coadministered vaccines.

In clinical trials in children, Havrix was concomitantly administered with one or more of the following US licensed vaccines: Measles, Mumps, and Rubella Virus Vaccine, Live; Varicella Vaccine, Live; Diphtheria and Tetanus Toxoids and Acellular Pertussis Vaccine, Adsorbed; Measles, Mumps, Rubella, and Varicella Vaccine, Live; Pneumococcal 7-valent Conjugate Vaccine (Diphtheria CRM197); and Haemophilus B Conjugate Vaccine (Meningococcal Protein Conjugate). Safety and immunogenicity were similar for concomitantly administered vaccines compared to separately administered vaccines.

In clinical trials in adults, Havrix was concomitantly administered with typhoid Vi polysaccharide and yellow fever vaccines . Safety and immunogenicity were similar for concomitantly administered vaccines compared to separately administered vaccines.

7.2 Use with Immune Globulin

Havrix may be administered concomitantly with Immune Globulin, human, using separate sites and syringes. The recommended vaccination regimen for Havrix should be followed. Consult the manufacturer's product circular for the appropriate dosage of Immune Globulin. A booster dose of Havrix should be administered at the appropriate time as outlined in the recommended regimen for Havrix .

7.3 Immunosuppressive Therapy

If Havrix is administered to a person receiving immunosuppressive therapy, an adequate immunologic response may not be obtained.

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8 USE IN SPECIFIC POPULATIONS

8.1 Pregnancy

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

8.3 Nursing Mothers

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

8.4 Pediatric Use

The safety of Havrix has been evaluated in 4374 children 12 through 23 months of age, and 2615 children/adolescents 2 through 18 years of age who received at least one 25U dose of Havrix .

Safety and effectiveness in infants below 12 months of age have not been established.

8.5 Geriatric Use

In the post-marketing observational safety study which included 42,110 persons who received Havrix , 4769 persons were 65 years of age or older and 1073 persons were 75 years of age or older. There were no adverse events judged by the investigator to be vaccine-related in the geriatric study population. In other clinical studies, 68 subjects 65 years of age or older were vaccinated with Havrix, 10 of whom were 75 years of age or older. No overall differences in safety and immunogenicity were observed between these subjects and younger subjects; however, greater sensitivity of some older individuals cannot be ruled out. Other reported clinical experience has not identified differences in responses between the elderly and younger subjects.

8.6 Immunocompromised Individuals

Immunocompromised persons may have a diminished immune response to Havrix and may not be protected against HAV infection.

11 DESCRIPTION

Havrix is an inactivated whole virus vaccine derived from Havrix virus grown in cell culture in human MRC-5 diploid fibroblasts. It contains inactivated virus of a strain which was originally derived by further serial passage of a proven attenuated strain. The virus is grown, harvested, purified by a combination of physical and high performance liquid chromatographic techniques developed at the Merck Research Laboratories, formalin inactivated, and then adsorbed onto amorphous aluminum hydroxyphosphate sulfate.

Havrix is a sterile suspension for intramuscular injection. One milliliter of the vaccine contains approximately 50U of Havrix virus antigen, which is purified and formulated without a preservative. Within the limits of current assay variability, the 50U dose of Havrix contains less than 0.1 mcg of non-viral protein, less than 4 × 10–6 mcg of DNA, less than 10–4 mcg of bovine albumin, and less than 0.8 mcg of formaldehyde. Other process chemical residuals are less than 10 parts per billion (ppb), including neomycin.

Each 0.5-mL pediatric dose contains 25U of Havrix virus antigen and adsorbed onto approximately 0.225 mg of aluminum provided as amorphous aluminum hydroxyphosphate sulfate, and 35 mcg of sodium borate as a pH stabilizer, in 0.9% sodium chloride.

Each 1-mL adult dose contains 50U of Havrix virus antigen and adsorbed onto approximately 0.45 mg of aluminum provided as amorphous aluminum hydroxyphosphate sulfate, and 70 mcg of sodium borate as a pH stabilizer, in 0.9% sodium chloride.

12 CLINICAL PHARMACOLOGY

12.1 Mechanism of Action

Havrix has been shown to elicit antibodies to Havrix as measured by ELISA.

Protection from Havrix disease has been shown to be related to the presence of antibody. However, the lowest titer needed to confer protection has not been determined.

13 NONCLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

Havrix has not been evaluated for its carcinogenic or mutagenic potential, or its potential to impair fertility.

14 CLINICAL STUDIES

14.1 Efficacy of Havrix: The Monroe Clinical Study

The immunogenicity and protective efficacy of Havrix were evaluated in a randomized, double-blind, placebo-controlled study involving 1037 susceptible healthy children and adolescents 2 through 16 years of age in a U.S. community with recurrent outbreaks of Havrix. All of these children were Caucasian, and there were 51.5% male and 48.5% female. Each child received an intramuscular dose of Havrix (25U) (N=519) or placebo (alum diluent) (N=518). Among those individuals who were initially seronegative (measured by a modification of the HAVAB radioimmunoassay [RIA]), seroconversion was achieved in >99% of vaccine recipients within 4 weeks after vaccination. The onset of seroconversion following a single dose of Havrix was shown to parallel the onset of protection against clinical Havrix disease.

Because of the long incubation period of the disease (approximately 20 to 50 days, or longer in children), clinical efficacy was based on confirmed casesThe clinical case definition included all of the following occurring at the same time: 1) one or more typical clinical signs or symptoms of Havrix (e.g., jaundice, malaise, fever ≥38.3°C); 2) elevation of Havrix IgM antibody (HAVAB-M); 3) elevation of alanine transferase (ALT) ≥2 times the upper limit of normal. of Havrix occurring ≥50 days after vaccination in order to exclude any children incubating the infection before vaccination. In subjects who were initially seronegative, the protective efficacy of a single dose of Havrix was observed to be 100% with 21 cases of clinically confirmed Havrix occurring in the placebo group and none in the vaccine group (p<0.001). The number of clinically confirmed cases of Havrix ≥30 days after vaccination were also compared. In this analysis, 28 cases of clinically confirmed Havrix occurred in the placebo group while none occurred in the vaccine group ≥30 days after vaccination. In addition, it was observed in this trial that no cases of clinically confirmed Havrix occurred in the vaccine group after day 16.One vaccinee did not meet the pre-defined criteria for clinically confirmed Havrix but did have positive Havrix IgM and borderline liver enzyme (ALT) elevations on days 34, 50, and 58 after vaccination with mild clinical symptoms observed on days 49 and 50. Following demonstration of protection with a single dose and termination of the study, a booster dose was administered to a subset of vaccinees 6, 12, or 18 months after the primary dose.

No cases of clinically confirmed Havrix disease ≥50 days after vaccination have occurred in those vaccinees from The Monroe Efficacy Study monitored for up to 9 years.

14.2 Other Clinical Studies

The efficacy of Havrix in other age groups was based upon immunogenicity measured 4 to 6 weeks following vaccination. Havrix was found to be immunogenic in all age groups.

Children - 12 through 23 Months of Age

In a clinical trial, children 12 through 23 months of age were randomized to receive the first dose of Havrix with or without M-M-R II and VARIVAX (N=617) and the second dose of Havrix with or without Tripedia and optionally either oral poliovirus vaccine (no longer licensed in the US) or IPOL (N=555). The race distribution of study subjects who received at least one dose of Havrix was as follows: 56.7% Caucasian; 17.5% Hispanic-American; 14.3% African-American; 7.0% Native American; 3.4% other; 0.8% Oriental; 0.2% Asian; and 0.2% Indian. The distribution of subjects by gender was 53.6% male and 46.4% female. In the analysis population, there were 471 initially seronegative children 12 through 23 months of age, who received the first dose of Havrix with (N=237) or without (N=234) M-M-R II and VARIVAX of whom 96% (95% CI: 93.7%, 97.5%) seroconverted (defined as having an anti-HAV titer ≥10 mIU/mL) post dose 1 with an anti-HAV geometric mean titer (GMT) of 48 mIU/mL (95% CI: 44.7, 51.6). There were 343 children in the analysis population who received the second dose of Havrix with (N=168) or without (N=175) Tripedia and optional oral poliovirus vaccine or IPOL of whom 100% (95% CI: 99.3%, 100%) seroconverted post dose 2 with an anti-HAV GMT of 6920 mIU/mL (95% CI: 6136, 7801). Of children who received only Havrix at both visits, 100% (n=97) seroconverted after the second dose of Havrix.

In a clinical trial involving 653 healthy children 12 to 15 months of age, 330 were randomized to receive Havrix, ProQuad, and pneumococcal 7-valent conjugate vaccine concomitantly, and 323 were randomized to receive ProQuad and pneumococcal 7-valent conjugate vaccine concomitantly followed by Havrix 6 weeks later. The race distribution of the study subjects was as follows: 60.3% Caucasian; 21.6% African-American; 9.5% Hispanic-American; 7.2% other; 1.1% Asian/Pacific; and 0.3% Native American. The distribution of subjects by gender was 50.7% male and 49.3% female. In the analysis population, the seropositivity rate for Havrix antibody (defined as the percent of subjects with an anti-HAV titer ≥10 mIU/mL) was 100% (n=182; 95% CI: 98.0%, 100%) post dose 2 with an anti-HAV GMT of 4977 mIU/mL (95% CI: 4068, 6089) when Havrix was given with ProQuad and pneumococcal 7-valent conjugate vaccine and 99.4% (n=159, 95% CI: 96.5%, 100%) post dose 2 with an anti-HAV GMT of 6123 mIU/mL (95% CI: 4826, 7770) when Havrix alone was given. These seropositivity rates were similar whether Havrix was administered with or without ProQuad and pneumococcal 7-valent conjugate vaccine.

In an open, multicenter, randomized study involving 617 children 15 months of age, 306 were randomized to receive Havrix with or without PedvaxHIB and INFANRIX, and 311 were randomized to receive Havrix with or without PedvaxHIB. The race distribution of the study subjects was as follows: 63.9% Caucasian; 17.5% Hispanic-American; 14.7% Black; 2.6% other; and 1.3% Asian. The distribution of subjects by gender was 54.0% male and 46.0% female. The seropositivity rate for Havrix antibody (defined as the percent of subjects with an anti-HAV titer ≥ 10 mIU/mL) 4 weeks post dose 2 was 100% (n=208, 95% CI: 98.2%, 100.0%) in those who received Havrix concomitantly with PedvaxHIB and INFANRIX or concomitantly with PedvaxHIB. In those subjects who received Havrix alone, the seropositivity rate for Havrix antibody was 100% (n=183, 95% CI: 98.0%, 100.0%), regardless of baseline Havrix serostatus. Overall, the anti-HAV GMT in the concomitant groups was 3616.5 mIU/mL (95% CI: 3084.5, 4240.2). The anti-HAV GMT in the nonconcomitant groups was 4712.6 mIU/mL (95% CI: 3996.8, 5556.8). Comparable responses were observed in both the initially seronegative and seropositive subjects.

In three combined clinical studies 1022 initially seronegative subjects received 2 doses of Havrix alone or concomitantly with other vaccines. Of the seronegative subjects, 99.9% achieved an anti-HAV titer ≥10 mIU/mL (95% CI: 99.5%, 100%) and an anti-HAV GMT of 5392.1 mIU/mL (95% CI: 4996.5, 5819.0) 4 weeks following dose 2 of Havrix.

Children/Adolescents - 2 Years through 18 Years of Age

Immunogenicity data were combined from eleven randomized clinical studies in children and adolescents 2 through 18 years of age who received Havrix (25U/0.5 mL). These included administration of Havrix in varying doses and regimens (N=404 received 25U/0.5 mL), the Monroe Efficacy Study (N=973), and comparison studies for process and formulation changes (N=1238). The race distribution of the study subjects who received at least one dose of Havrix in these studies was as follows: 84.8% Caucasian; 10.6% American Indian; 2.3% African-American; 1.5% Hispanic-American; 0.6% other; 0.2% Oriental. The distribution of subjects by gender was 51.2% male and 48.8% female. The proportions of subjects who seroconverted 4 weeks after the first and second doses administered 6 months apart were 97% (n=1230; 95% CI: 96%, 98%) and 100% (n=1057; 95% CI: 99.5%, 100%) of subjects with anti-HAV GMTs of 43 mIU/mL (95% CI: 40, 45) and 10,077 mIU/mL (95% CI: 9394, 10,810), respectively.

Adults - 19 Years of Age and Older

Immunogenicity data were combined from five randomized clinical studies in adults 19 years of age and older who received Havrix (50U/1-mL). One single-blind study evaluated doses of Havrix with varying amounts of viral antigen and/or alum content in healthy adults ≥170 pounds and ≥30 years of age (N=208 adults administered 50U/1-mL dose). One open-label study evaluated Havrix given with immune globulin or alone (N=164 adults who received Havrix alone). A third study was single-blind and evaluated 3 different lots of Havrix (N=1112). The fourth study was single-blind and evaluated doses of Havrix with varying amounts of viral antigen in healthy adults ≥170 pounds and ≥30 years of age (N=159 adults administered the 50U/1-mL dose). The fifth study was an open-label study to evaluate various regimens for time of administration of the booster dose of Havrix (6, 12, and 18 months post dose 1, N=354). The race distribution of the study subjects who received at least one dose of Havrix in these studies was as follows: 93.2% Caucasian; 2.5% African-American; 2.1% Hispanic-American; 1.4% Oriental; 0.5% other; 0.3% American Indian. The distribution of subjects by gender was 44.8% male and 55.2% female. The proportion of subjects who seroconverted 4 weeks after the first and second doses administered 6 months apart was 95% (n=1411; 95% CI: 94%, 96%) and 99.9% (n=1244; 95% CI: 99.4%, 100%) with GMTs of 37 mIU/mL (95% CI: 35, 38) and 6013 mIU/mL (95% CI: 5592, 6467), respectively. Furthermore, at 2 weeks postvaccination, 69.2% (n=744; 95% CI: 65.7%, 72.5%) of adults seroconverted with an anti-HAV GMT of 16 mIU/mL after a single dose of Havrix.

14.3 Timing of Booster Dose Administration

Children/Adolescents - 2 through 18 Years of Age

In the Monroe Efficacy Study, children were administered a second dose of Havrix 6, 12, or 18 months following the initial dose. For subjects who received both doses of Havrix, the GMTs and proportions of subjects who seroconverted 4 weeks after the booster dose administered 6, 12, and 18 months after the first dose are presented in Table 9.

Months Following Initial 25U Dose CohortBlood samples were taken at prebooster and postbooster time points. (n=960)

0 and 6 Months

Cohort (n=35)

0 and 12 Months

Cohort (n=39)

0 and 18 Months

Seroconversion Rate

GMT (mIU/mL) (95% CI)

6 97%

107 (98, 117)

- -
7 100%

10433 (9681, 11243)

- -
12 - 91%

48 (33, 71)

-
13 - 100%

12308 (9337, 16226)

-
18 - - 90%

50 (28, 89)

19 - - 100%

9591 (7613, 12082)


Adults - 19 years of age and older

Among the 5 randomized clinical studies in adults 19 years of age and older described in Section 14.2, there were additional data in which a booster dose of Havrix (50U/1-mL) was administered 12 or 18 months after the first dose. For subjects in these studies who received both doses of Havrix, the proportions who seroconverted 4 weeks after the booster dose administered 6, 12, and 18 months after the first dose were 100% of 1201 subjects, 98% of 91 subjects, and 100% of 84 subjects, respectively. GMTs in mIU/mL one month after the subjects received the booster dose at 6, 12, or 18 months after the primary dose were 5987 mIU/mL (95% CI: 5561, 6445), 4896 mIU/mL (95% CI: 3589, 6679), and 6043 mIU/mL (95% CI: 4687, 7793), respectively.

14.4 Duration of Immune Response

In follow-up of subjects in The Monroe Efficacy Study, in children (≥2 years of age) and adolescents who received two doses (25U) of Havrix, detectable levels of anti-HAV antibodies (≥10 mIU/mL) were present in 100% of subjects for at least 10 years postvaccination. In subjects who received Havrix at 0 and 6 months, the GMT was 819 mIU/mL (n=175) at 2.5 to 3.5 years and 505 mIU/mL (n=174) at 5 to 6 years, and 574 mIU/mL (n=114) at 10 years postvaccination. In subjects who received Havrix at 0 and 12 months, the GMT was 2224 mIU/mL (n=49) at 2.5 to 3.5 years, 1191 mIU/mL (n=47) at 5 to 6 years, and 1005 mIU/mL (n=36) at 10 years postvaccination. In subjects who received Havrix at 0 and 18 months, the GMT was 2501 mIU/mL (n=53) at 2.5 to 3.5 years, 1614 mIU/mL (n=56) at 5 to 6 years, and 1507 mIU/mL (n=41) at 10 years postvaccination.

In adults that were administered Havrix at 0 and 6 months, the Havrix antibody response to date has been shown to persist at least 6 years. Detectable levels of anti-HAV antibodies (≥10 mIU/mL) were present in 100% (378/378) of subjects with a GMT of 1734 mIU/mL at 1 year, 99.2% (252/254) of subjects with a GMT of 687 mIU/mL at 2 to 3 years, 99.1% (219/221) of subjects with a GMT of 605 mIU/mL at 4 years, and 99.4% (170/171) of subjects with a GMT of 684 mIU/mL at 6 years postvaccination.

The total duration of the protective effect of Havrix in healthy vaccinees is unknown at present.

14.5 Concomitant Administration of Havrix and Immune Globulin

The concurrent use of Havrix and immune globulin (IG, 0.06 mL/kg) was evaluated in an open-label, randomized clinical study involving 294 healthy adults 18 to 39 years of age. Adults were randomized to receive 2 doses of Havrix 24 weeks apart (N=129), the first dose of Havrix concomitant with a dose of IG followed by the second dose of Havrix alone 24 weeks later (N=135), or IG alone (N=30). The race distribution of the study subjects who received at least one dose of Havrix or IG in this study was as follows: 92.3% Caucasian; 4.0% Hispanic-American; 3.0% African-American; 0.3% Native American; 0.3% Asian/Pacific. The distribution of subjects by gender was 28.7% male and 71.3% female. Table 10 provides seroconversion rates and GMTs at 4 and 24 weeks after the first dose in each treatment group and at one month after a booster dose of Havrix (administered at 24 weeks) .

Havrix plus IG Havrix IG
Weeks Seroconversion Rate

GMT (mIU/mL) (95% CI)

N/A = Not Applicable.
4 100%

42 (39, 45)

(n=129)

96%

38 (33, 42)

(n=135)

87%

19 (15, 23)

(n=30)

24 92%

83 (65, 105)

(n=125)

97%The seroconversion rate and the GMT in the group receiving Havrix alone were significantly higher than in the group receiving Havrix plus IG (p=0.05, p<0.001, respectively).

137 (112, 169)

(n=132)

0%

UndetectableUndetectable is defined as <10mIU/mL.

(n=28)

28 100%

4872 (3716, 6388)

(n=114)

100%

6498 (5111, 8261)

(n=128)

N/A

14.6 Interchangeability of the Booster Dose

A randomized, double-blind clinical study in 537 healthy adults, 18 to 83 years of age, evaluated the immune response to a booster dose of Havrix and HAVRIX given at 6 or 12 months following an initial dose of HAVRIX. Subjects were randomized to receive Havrix (50U) as a booster dose 6 months (N=232) or 12 months (N=124) following an initial dose of HAVRIX or HAVRIX (1440 EL. U) as a booster dose 6 months (N=118) or 12 months (N=63) following an initial dose of HAVRIX. The race distribution of the study subjects who received the booster dose of Havrix or HAVRIX in this study was as follows: 87.2% Caucasian; 8.0% African-American; 1.9% Hispanic-American; 1.3% Oriental; 0.9% Asian; 0.4% Indian; 0.4% other. The distribution of subjects by gender was 44.9% male and 55.1% female. When Havrix was given as a booster dose following HAVRIX, the vaccine produced an adequate immune response .

First Dose Booster Dose Seropositivity Rate Booster Response Rate Geometric Mean Titer
HAVRIX

1440 EL.U.

Havrix

50 U

99.7% (n=313) 86.1% (n=310) 3272 (n=313)
HAVRIX

1440 EL.U.

HAVRIX

1440 EL.U.

99.3% (n=151) 80.1% (n=151) 2423 (n=151)

14.7 Immune Response to Concomitantly Administered Vaccines

Clinical Studies of Havrix with M-M-R II, VARIVAX, and Tripedia

In the clinical trial in which children 12 months of age received the first dose of Havrix concomitantly with M-M-R II and VARIVAX described in Section 14.2, rates of seroprotection to Havrix were similar between the two groups who received Havrix with or without M-M-R II and VARIVAX. Measles, mumps, and rubella immune responses were tested in 241 subjects, 263 subjects, and 270 subjects, respectively. Seropositivity rates were 98.8% [95% CI: 96.4%, 99.7%] for measles, 99.6% [95% CI: 97.9%, 100%] for mumps, and 100% [95% CI: 98.6%, 100%] for rubella, which were similar to observed historical rates (seropositivity rates 99% for all three antigens, with lower bound of the 95% CI >89%) following vaccination with a first dose of M-M-R II in this age group. Data from this study were insufficient to adequately assess the immune response to VARIVAX administered concomitantly with Havrix. In this same study, the second dose of Havrix at 18 months of age was given with or without Tripedia (DTaP). Seropositivity rates for diphtheria and tetanus were similar to those in historical controls. However, data from this study were insufficient to assess the pertussis response of DTaP when administered with Havrix. Rates of seroprotection to Havrix were similar between the two groups who received Havrix with or without M-M-R II and VARIVAX, and between the two groups who received Havrix with or without DTaP.

Clinical Studies of Havrix with ProQuad and Prevnar

In the clinical trial of concomitant use of Havrix with ProQuad and pneumococcal 7-valent conjugate vaccine in children 12 to 15 months of age described in Section 14.2, the antibody GMTs for S. pneumoniae types 4, 6B, 9V, 14, 18C, 19F, and 23F 6 weeks after vaccination with pneumococcal 7-valent conjugate vaccine administered concomitantly with ProQuad and Havrix were non-inferior as compared to GMTs observed in the group given pneumococcal 7-valent conjugate vaccine with ProQuad alone (the lower bounds of the 95% CI around the fold-difference for the 7 serotypes excluded 0.5). For the varicella component of ProQuad, in subjects with baseline antibody titers <1.25 gpELISA units/mL, the proportion with a titer ≥5 gpELISA units/mL 6 weeks after their first dose of ProQuad was non-inferior (defined as -10 percentage point change) when ProQuad was administered with Havrix and pneumococcal 7-valent conjugate vaccine as compared to the proportion with a titer ≥5 gpELISA units/mL when ProQuad was administered with pneumococcal 7-valent conjugate vaccine alone (difference in seroprotection rate -5.1% [95% CI: -9.3, -1.4%]). Havrix responses were similar when compared between the two groups who received Havrix with or without ProQuad and pneumococcal 7-valent conjugate vaccine. Seroconversion rates and antibody titers for varicella and S. pneumoniae types 4, 6B, 9V, 14, 18C, 19F, and 23F were similar between groups at 6 weeks postvaccination.

Clinical Studies of Havrix with INFANRIX and PedvaxHIB

In the clinical trial of concomitant administration of Havrix with INFANRIX and PedvaxHIB in children 15 months of age, described in Section 14.2, when the first dose of Havrix was administered concomitantly with either INFANRIX and PedvaxHIB or PedvaxHIB, there was no interference in immune response to Havrix as measured by seropositivity rates after dose 2 of Havrix compared to administration of both doses of Havrix alone. When dose 1 of Havrix was administered concomitantly with either PedvaxHIB and INFANRIX or PedvaxHIB, there was no interference in immune response to Haemophilus influenzae b (as measured by the proportion of subjects who attained an anti-polyribosylribitol phosphate antibody titer >1.0 mcg/mL at 4 weeks after vaccination), compared to subjects receiving either PedvaxHIB and INFANRIX or PedvaxHIB. When Havrix was administered concomitantly with INFANRIX and PedvaxHIB, there was no interference in immune responses at 4 weeks after vaccination to the pertussis antigens (PT, FHA, or pertactin, as measured by GMTs) and no interference in immune responses to diphtheria toxoid or tetanus toxoid (as measured by the proportion of subjects achieving an antibody titer >0.1 IU/mL) compared to administration of INFANRIX and PedvaxHIB.

Clinical Studies of Havrix with Typhoid Vi Polysaccharide Vaccine and Yellow Fever Vaccine, Live Attenuated

In the clinical trial of concomitant use of Havrix with typhoid Vi polysaccharide and yellow fever vaccines in adults 18-54 years of age described in Section 6.1, the antibody response rates for typhoid Vi polysaccharide and yellow fever were adequate when typhoid Vi polysaccharide and yellow fever vaccines were administered concomitantly with (N=80) and nonconcomitantly without Havrix (N=80). The seropositivity rate for Havrix when Havrix, typhoid Vi polysaccharide, and yellow fever vaccines were administered concomitantly was generally similar to when Havrix was given alone .

Data are insufficient to assess the immune response to Havrix and poliovirus vaccine when administered concomitantly.

16 HOW SUPPLIED/STORAGE AND HANDLING

Havrix is available in single-dose vials and prefilled Luer-Lok® syringes.

Pediatric/Adolescent Formulations

25U/0.5 mL in single-dose vials and prefilled Luer-Lok® syringes.

NDC 0006-4831-41 – box of ten 0.5-mL single dose vials.

NDC 0006-4095-02 – carton of ten 0.5-mL prefilled single-dose Luer-Lok® syringes with tip caps.

NDC 0006-4095-09 – carton of six 0.5-mL prefilled single-dose Luer-Lok® syringes with tip caps.

Adult Formulations

50U/1-mL in single-dose vials and prefilled Luer-Lok® syringes.

NDC 0006-4841-00 – 1-mL single dose vial.

NDC 0006-4841-41 – box of ten 1-mL single dose vials.

NDC 0006-4096-02 – carton of ten 1-mL prefilled single-dose Luer-Lok® syringes with tip caps.

NDC 0006-4096-09 – carton of six 1-mL prefilled single-dose Luer-Lok® syringes with tip caps.

Store vaccine at 2-8°C (36-46°F).

DO NOT FREEZE since freezing destroys potency.

17 PATIENT COUNSELING INFORMATION

Information for Vaccine Recipients and Parents or Guardians


Manuf. and Dist. by: Merck Sharp & Dohme Corp., a subsidiary of

MERCK & CO., INC., Whitehouse Station, NJ 08889, USA

For patent information: www.merck.com/product/patent/home.html

The trademarks depicted herein are owned by their respective companies.

Copyright ©1996-2014 Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc.

All rights reserved.

uspi-v251-i-1402r016

Printed in USA

PRINCIPAL DISPLAY PANEL - 10 Single-Dose 0.5 mL Vial Carton

NDC 0006-4831-41

10 Single-dose ~25U/0.5-mL Vials

(HEPATITIS A VACCINE, INACTIVATED)

Havrix®

PEDIATRIC/ADOLESCENT

0.5 mL vial contains approximately 25U of Havrix virus antigen on an Amorphous aluminum

hydroxyphosphate sulfate adjuvant. Havrix virus is grown in cell culture in human MRC-5

diploid fibroblasts.

Rx only

PRINCIPAL DISPLAY PANEL - 10 Single-Dose 0.5 mL Vial Carton

PRINCIPAL DISPLAY PANEL - 10 Single-Dose 0.5 mL Syringe Carton

NDC 0006-4095-02

10 Single-Dose 0.5-mL Syringes

(HEPATITIS A VACCINE,

INACTIVATED)

Havrix ®

PEDIATRIC/ADOLESCENT

FORMULATION

This package contains 10 single-dose syringes.

Each 0.5-mL syringe contains approximately 25U of Havrix virus antigen

on an amorphous aluminum hydroxyphosphate sulfate adjuvant.

Havrix virus is grown in cell culture in human MRC-5 diploid fibroblasts.

Rx only

PRINCIPAL DISPLAY PANEL - 10 Single-Dose 0.5 mL Syringe Carton

PRINCIPAL DISPLAY PANEL - Single-Dose 1 mL Vial Carton

NDC 0006-4841-00

1 Single-dose

~50U/1-mL Vial

(HEPATITIS A

VACCINE,

INACTIVATED)

Havrix ®

ADULT

FORMULATION

1 mL contains approximately 50U

of Havrix virus antigen on an

Amorphous aluminum hydroxyphos-

phate sulfate adjuvant.

Havrix virus is grown in cell

culture in human MRC-5 diploid

fibroblasts.

Rx only

PRINCIPAL DISPLAY PANEL - Single-Dose 1 mL Vial Carton

PRINCIPAL DISPLAY PANEL - 10 Single-Dose 1 mL Syringe Carton

NDC 0006-4096-02

10 Single-Dose 1-mL Syringes

(HEPATITIS A VACCINE,

INACTIVATED)

Havrix ®

ADULT FORMULATION

This package contains 10 single-dose syringes.

Each 1-mL syringe contains approximately 50U of Havrix virus antigen

on an amorphous aluminum hydroxyphosphate sulfate adjuvant.

Havrix virus is grown in cell culture in human MRC-5 diploid fibroblasts.

Rx only

PRINCIPAL DISPLAY PANEL - 10 Single-Dose 1 mL Syringe Carton

Havrix pharmaceutical active ingredients containing related brand and generic drugs:

Active ingredient is the part of the drug or medicine which is biologically active. This portion of the drug is responsible for the main action of the drug which is intended to cure or reduce the symptom or disease. The other portions of the drug which are inactive are called excipients; there role is to act as vehicle or binder. In contrast to active ingredient, the inactive ingredient's role is not significant in the cure or treatment of the disease. There can be one or more active ingredients in a drug.


Havrix available forms, composition, doses:

Form of the medicine is the form in which the medicine is marketed in the market, for example, a medicine X can be in the form of capsule or the form of chewable tablet or the form of tablet. Sometimes same medicine can be available as injection form. Each medicine cannot be in all forms but can be marketed in 1, 2, or 3 forms which the pharmaceutical company decided based on various background research results.
Composition is the list of ingredients which combinedly form a medicine. Both active ingredients and inactive ingredients form the composition. The active ingredient gives the desired therapeutic effect whereas the inactive ingredient helps in making the medicine stable.
Doses are various strengths of the medicine like 10mg, 20mg, 30mg and so on. Each medicine comes in various doses which is decided by the manufacturer, that is, pharmaceutical company. The dose is decided on the severity of the symptom or disease.


Havrix destination | category:

Destination is defined as the organism to which the drug or medicine is targeted. For most of the drugs what we discuss, human is the drug destination.
Drug category can be defined as major classification of the drug. For example, an antihistaminic or an antipyretic or anti anginal or pain killer, anti-inflammatory or so.


Havrix Anatomical Therapeutic Chemical codes:

A medicine is classified depending on the organ or system it acts [Anatomical], based on what result it gives on what disease, symptom [Therapeutical], based on chemical composition [Chemical]. It is called as ATC code. The code is based on Active ingredients of the medicine. A medicine can have different codes as sometimes it acts on different organs for different indications. Same way, different brands with same active ingredients and same indications can have same ATC code.


Havrix pharmaceutical companies:

Pharmaceutical companies are drug manufacturing companies that help in complete development of the drug from the background research to formation, clinical trials, release of the drug into the market and marketing of the drug.
Researchers are the persons who are responsible for the scientific research and is responsible for all the background clinical trials that resulted in the development of the drug.


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Frequently asked Questions

Can i drive or operate heavy machine after consuming Havrix?

Depending on the reaction of the Havrix after taken, if you are feeling dizziness, drowsiness or any weakness as a reaction on your body, Then consider Havrix not safe to drive or operate heavy machine after consumption. Meaning that, do not drive or operate heavy duty machines after taking the capsule if the capsule has a strange reaction on your body like dizziness, drowsiness. As prescribed by a pharmacist, it is dangerous to take alcohol while taking medicines as it exposed patients to drowsiness and health risk. Please take note of such effect most especially when taking Primosa capsule. It's advisable to consult your doctor on time for a proper recommendation and medical consultations.

Is Havrix addictive or habit forming?

Medicines are not designed with the mind of creating an addiction or abuse on the health of the users. Addictive Medicine is categorically called Controlled substances by the government. For instance, Schedule H or X in India and schedule II-V in the US are controlled substances.

Please consult the medicine instruction manual on how to use and ensure it is not a controlled substance.In conclusion, self medication is a killer to your health. Consult your doctor for a proper prescription, recommendation, and guidiance.

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Review

sdrugs.com conducted a study on Havrix, and the result of the survey is set out below. It is noteworthy that the product of the survey is based on the perception and impressions of the visitors of the website as well as the views of Havrix consumers. We, as a result of this, advice that you do not base your therapeutic or medical decisions on this result, but rather consult your certified medical experts for their recommendations.

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