AHFS Category 80:08
Diphtheria and Tetanus
Toxoids and Acellular
Pertussis Vaccine Adsorbed
DAPTACEL?
DESCRIPTION
DAPTACEL™, Diphtheria and Tetanus Toxoids and Acellular Pertussis Vaccine
Adsorbed, for intramuscular use, manufactured by Aventis
Pasteur Limited, is a sterile suspension of pertussis antigens and
diphtheria and tetanus toxoids adsorbed on aluminum phosphate in a
sterile isotonic sodium chloride solution. After shaking, the vaccine is a
white homogeneous cloudy suspension. Each dose of
DAPTACEL™ contains the following active ingredients:
pertussis toxoid 10 µg
filamentous hemagglutinin (FHA) 5 µg
pertactin (PRN) 3 µg
fimbriae types 2 and 3 5 µg
diphtheria toxoid 15 Lf
tetanus toxoid 5 Lf
Other ingredients per dose include 3.3 mg (0.6% v/v) 2-phenoxyethanol as the
preservative, 0.33 mg of aluminum as the adjuvant,
≤0.1 mg residual formaldehyde and <50 ng residual glutaraldehyde.
The acellular pertussis vaccine components are produced from Bordetella
pertussis cultures grown in Stainer-Scholte medium1modified by the addition of casamino acids and dimethyl-beta-cyclodextrin.
The fimbriae types 2 and 3 are extracted from the bacterial
cells and the pertussis toxin, FHA and PRN are prepared from the
supernatant. These proteins are purified by sequential filtration,
saltprecipitation,
ultrafiltration and chromatography. Pertussis toxin is inactivated with
glutaraldehyde and FHA is treated with
formaldehyde. The individual antigens are adsorbed separately onto aluminum
phosphate.
Corynebacterium diphtheriae is grown in modified Mueller’s growth medium.2
After ammonium sulfate fractionation, the diphtheria toxin
is detoxified with formalin and diafiltered. Clostridium tetani is grown in
modified Mueller-Miller casamino acid medium without beef
heart infusion.3 Tetanus toxin is detoxified with formalin and purified by
ammonium sulfate fractionation and diafiltration. Diphtheria and
tetanus toxoids are individually adsorbed onto aluminum phosphate.
The adsorbed diphtheria, tetanus and acellular pertussis components are
combined in a sterile isotonic sodium chloride solution
containing 2-phenoxyethanol as preservative.
Both diphtheria and tetanus toxoids induce at least 2 units of antitoxin per
mL in the guinea pig potency test. The potency of the
acellular pertussis vaccine components is evaluated by the antibody response
of immunized mice to pertussis toxin, FHA, PRN and
fimbriae types 2 and 3 measured by enzyme-linked immunosorbent assay
(ELISA).
CLINICAL PHARMACOLOGY
Simultaneous immunization of infants and children against diphtheria,
tetanus and pertussis with conventional whole-cell pertussis DTP
vaccine (Diphtheria and Tetanus Toxoids and Pertussis Vaccine Adsorbed - For
Pediatric Use) has been a routine practice in the US since
the late 1940s. This has played a major role in markedly reducing disease
and deaths from these infections.4 DTaP (Diphtheria and
Tetanus Toxoids and Acellular Pertussis Vaccine Adsorbed) vaccines were
first available for use in infants in the US in 1996 and have
been routinely recommended for all doses of the vaccination series for
infants and children <7 years of age since 1997.5
Diphtheria
Corynebacterium diphtheriae may cause both localized and generalized
disease. The systemic intoxication is caused by diphtheria
exotoxin, an extracellular protein of toxigenic strains of C. diphtheriae.
Protection against disease is due to the development of
neutralizing antibody to diphtheria toxin.
Both toxigenic and nontoxigenic strains of C. diphtheriae can cause disease
but only strains that produce diphtheria toxin cause severe
manifestations such as myocarditis and neuritis. Diphtheria is a serious
disease, with the highest case-fatality rates among infants and
the elderly.4,6
Prior to the widespread use of diphtheria toxoid in the late 1940s,
diphtheria disease was common in the US. More than 200,000 cases,
primarily among children, were reported in 1921. Approximately 5% – 10% of
cases were fatal; the highest case-fatality rates were in the
very young and the elderly. More recently, reported cases of diphtheria of
all types declined fro m 306 in 1975 to 59 in 1979; most were
cutaneous diphtheria reported from a single state. After 1979, cutaneous
diphtheria was no longer reportable.4 From 1980 through 2000,
only 50 cases of diphtheria were reported in the US. During the period
1980–1996, six fatal cases of diphtheria were reported. Only 1 case
of diphtheria was reported each year in 1998–2000 with no fatalities.7 Of 40
reported cases with known age in 1982-1998, 63% were in
persons ≥20 years of age. Most cases have occurred in unimmunized or
inadequately immunized persons. Although diphtheria disease is
rare in the US, it appears that C. diphtheriae continues to circulate in
areas of the country with previously endemic diphtheria.8
Page 2 of 12
Diphtheria continues to occur in other parts of the world. A major epidemic
of diphtheria occurred in the newly Independent States of
the former Soviet Union beginning in 1990. This epidemic resulted in
approximately 150,000 cases and 5,000 deaths during the years
1990-1997.9 This outbreak is believed to be due to several factors,
including a lack of routine immunization of adults in these
countries.10
Complete immunization significantly reduces the risk of developing
diphtheria and immunized persons who develop disease have
milder illness. Following adequate immunization with diphtheria toxoid,
protection is thought to last for at least 10 years. Immunization
does not, however, eliminate carriage of C. diphtheriae in the pharynx, nose
or on the skin.
4
Tetanus
Tetanus manifests systemic toxicity primarily by neuromuscular dysfunction
caused by a potent exotoxin elaborated by Clostridium tetani.
Spores of C. tetani are ubiquitous. Serological tests indicate that
naturally acquired immunity to tetanus toxin does not occur in the US.
Thus, universal primary immunization, with subsequent maintenance of
adequate antitoxin levels by means of appropriately timed
boosters, is necessary to protect all age groups. Tetanus toxoid is a highly
effective antigen and a completed primary series generally
induces protective levels of serum antitoxin that persist for 10 years or
more.4
Following routine use of tetanus toxoid in the US, the occurrence of tetanus
disease decreased dramatically from 560 reported cases in
1947 to an average of 50-100 cases reported annually from the mid 1970s
through the late 1990s to 35 cases in 2000.7 The casefatality
rate has been relatively constant at approximately 30%. During the years
1982-1998, 52% of reported cases were among
persons 60 years of age or older. In the mid to late 1990s, the age
distribution of reported cases shifted to a younger age group, in part
due to an increased number of cases among injection drug users in
California. From 1995-1997, persons 20-59 years of age accounted
for 60% of all cases, with persons 60 years of age or older accounting for
only 35%. In the US, tetanus occurs almost exclusively
among unvaccinated or inadequately vaccinated persons.8
Pertussis
Pertussis (whooping cough) is a disease of the respiratory tract caused by
Bordetella pertussis. This gram-negative coccobacillus
produces a variety of biologically active components. The role of the
different components produced by B. pertussis in either the
pathogenesis of, or immunity to, pertussis is not well understood.6
Pertussis is highly communicable (attack rates of 90% have been reported for
susceptible individuals exposed to a case in the home11)
and can cause severe disease, particularly among young infants. Since
pertussis became a nationally reportable disease in the US in
1922, the highest number of pertussis cases (approximately 260,000) was
reported in 1934. Following the introduction and widespread
use of whole-cell pertussis DTP vaccine among infants and children in the
mid to late 1940s, pertussis incidence gradually declined,
reaching a historical low of 1,010 cases reported in 1976.12
During the 1980s and 1990s, the number of reported pertussis cases in the US
has gradually increased, particularly among adolescents
and adults.12,13 Improvements in the diagnosis and reporting of pertussis in
older age groups is thought to have contributed, at least in
part, to the increase in reported cases. The number of cases of pertussis
reported among children aged 6 months to 4 years has remained
stable throughout the 1990s, suggesting that protection offered by
vaccination has continued with the introduction of DTaP vaccines.12
During 1997-2000, a total of 29,134 cases were reported, for an estimated
average annual incidence rate of 2.7 per 100,000 population.12
Among 29,048 cases for whom age was known, 29% were aged < 1 year, 12% were
aged 1-4 years, 10% were aged 5–9 years, 29%
were aged 10-19 years and 20% were ≥20 years of age.12 Average annual
incidence rates during 1997-2000 were highest among infants
aged <1 year (55.5 cases per 100,000 population) and lower in children aged
1–4 years (5.5), children aged 5–9 years (3.6), persons aged
10-19 years (5.5) and persons aged ≥20 years (0.8).12
The severity of pertussis remains highest in infants. Of 7,203 infants <6
months of age reported as having pertussis during the period
1997-2000, 63% were hospitalized, 12% had pneumonia, 1.4% had one or more
seizures, 0.2% had encephalopathy and 0.8% died.12
Atypical infection, including nonspecific symptoms of bronchitis or upper
respiratory tract infection, may occur at any age but more
commonly in older children and adults, including some who were previously
immunized. In these cases, pertussis may not be
diagnosed because classic signs, particularly the inspiratory whoop, may be
absent. Older preschool-aged and school-aged children, as
well as adolescents and adults who develop pertussis, may play a role in
transmission to young infants.8
Concerns about the safety of whole-cell pertussis DTP vaccines prompted the
development of less reactogenic DTaP vaccines that
contain purified antigens of B. pertussis. The pertussis component of DTaP
vaccines contains inactivated pertussis toxin and may
contain one or more of FHA, PRN and fimbriae types 2 and 3. DTaP vaccines
were first available for use in infants in the US in 1996 and
have been routinely recommended by the Advisory Committee on Immunization
Practices (ACIP) for all doses of the vaccination series
for infants and children <7 years of age since 1997.5
Since 1991, 7 studies conducted in Europe and Africa have evaluated the
efficacy of 8 DTaP vaccines administered to infants. The
vaccines, produced by different manufacturers, contained a varying number
and quantity of antigens. The derivation and formulation of
the individual antigens also varied among different vaccines. The studies
differed in study design and 3, including the Sweden I Efficacy
Trial (1992–1995), were randomized placebo-controlled clinical trials.
Because of these and other differences, comparisons among
studies should be made with caution. Within individual studies, however, the
efficacy of acellular pertussis vaccines can be compared
directly with that of a placebo control or whole-cell pertussis DTP. The
efficacy of 3 doses of acellular pertussis vaccines in preventing
moderate to severe pertussis disease was within the range expected for most
whole-cell pertussis DTP vaccines. Point estimates of the
efficacy of DTaP vaccines ranged from 59% - 89%.5
The effectiveness of pertussis vaccine among US children aged 7–18 months in
1998 and 1999 was calculated using the screening
method. During this time, the National Immunization Survey reported 66% of
children aged ≤18 months received DTaP rather than wholecell
pertussis DTP.12 The screening estimate of 88% reflects the effectiveness of
the overall vaccination program that used approximately
two thirds DTaP and one third whole-cell pertussis DTP in children aged 7–18
months. This estimate is similar to that observed in clinical
trials for acellular pertussis vaccines. During 1997–2000, the incidence
rates were highest among infants aged <1 year, lower in children
aged 1–4 years and remained stable among children aged 5-9 years.12
Page 3 of 12
Efficacy of DAPTACEL™
Pertussis
A randomized, double-blinded, placebo-controlled efficacy and safety study
was conducted in Sweden from 1992-1995 (Sweden I
Efficacy Trial) under the sponsorship of the National Institute of Allergy
and Infectious Diseases (NIAID). A total of 9,829 infants
received 1 of 4 vaccines: DAPTACEL™ (n = 2,587); another investigational
acellular pertussis vaccine (n = 2,566); whole-cell
pertussis DTP vaccine (n = 2,102); or DT vaccine as placebo (Swedish
National Bacteriological Laboratory, n = 2,574). Infants were
immunized at 2, 4 and 6 months of age. The mean length of follow-up was 2
years after the third dose of vaccine. The protective
efficacy of DAPTACEL™ against pertussis after 3 doses of vaccine using the
World Health Organization (WHO) case definition
(≥21 consecutive days of paroxysmal cough with culture or serologic
confirmation or epidemiologic link to a confirmed case) was
84.9% (95% confidence interval [CI] 80.1 to 88.6).14 The protective efficacy
of DAPTACEL™ against mild pertussis (≥1 day of cough
with laboratory confirmation) was 77.9% (95% CI 72.6 to 82.2).15 Protection
against pertussis by DAPTACEL™ was sustained for the
2-year follow-up period.14,15
In order to assess the antibody response to the pertussis antigens of
DAPTACEL™ in the US population, 2 lots of DAPTACEL™, including
the lot used in the Sweden I Efficacy Trial, were administered to US infants
in the US Bridging Study.15 In this study, antibody responses
following 3 doses of DAPTACEL™ given to US children at 2, 4 and 6 months of
age were compared to those from a subset of the infants
enrolled in the Sweden I Efficacy Trial. Assays were performed in parallel
on the available sera from the US and Swedish infants. Antibody
responses to all the antigens were similar except for those to the PRN
component. For both lots of DAPTACEL™, the geometric mean
concentration (GMC) and percent response to PRN in US infants (Lot 006, n =
107; Lot 009, n = 108) were significantly lower after 3 doses
of vaccine than in Swedish infants (n = 83). In a separate study performed
in Canada (Phase II), in which children received 4 doses of
DAPTACEL™ at 2, 4, 6 and 17–18 months of age, antibody responses following
the fourth dose (n = 275) were equivalent or higher than
those seen in the Swedish infants after 3 doses. While a serologic correlate
of protection for pertussis has not been established, the
antibody response to all antigens in North American infants after 4 doses of
DAPTACEL™ at 2, 4, 6 and 17-20 months of age was
comparable to that achieved in Swedish infants in whom efficacy was
demonstrated after 3 doses of DTaP at 2, 4 and 6 months of age.15
Diphtheria and Tetanus
In a Canadian clinical study, 324 children were enrolled to receive DAPTACEL™
at 2, 4, 6 and 17–18 months of age. The proportion of
children with post-dose 3 diphtheria (n = 313) and tetanus (n = 313)
antitoxin levels ≥0.01 IU/mL was 100% and ≥0.10 IU/mL was
85% and 100%, respectively.15 The proportion with post-dose 4 diphtheria (n
= 296) and tetanus (n = 296) antitoxin levels ≥0.10 IU/mL
was 100%.15 The efficacy of the diphtheria and tetanus toxoids used in
DAPTACEL™ was determined on the basis of immunogenicity
studies with a comparison to a serological correlate of protection (0.01
antitoxin units/mL) established by the Panel on Review of
Bacterial Vaccines and Toxoids.16
In the US Bridging Study, for which data are only available following 3
doses, 99.2% (n = 261) achieved diphtheria antitoxin levels of
≥0.01 IU/mL, 80.6% (n = 261) achieved levels of ≥0.10 IU/mL and 100% (n =
260) achieved tetanus antitoxin levels of 0.01 U/mL and
0.10 U/mL.15
Concurrently Administered Vaccines
In a clinical trial conducted in the US, DAPTACEL™ was given simultaneously
with Haemophilus influenzae type b vaccine and with live
oral poliovirus vaccine (OPV) at 2, 4 and 6 months of age according to local
practices. Two hundred eighty-one infants received 3 doses
of Haemophilus influenzae type b vaccine and 305 received 3 doses of OPV.
Immune responses to these vaccines were evaluated in a
subset of 258 children. One month after the third dose, 96.9% (n = 253)
achieved anti-PRP antibody levels of at least 0.15 µg/mL,
82.7% (n = 216) achieved antibody levels of at least 1.0 µg/mL; and 100% (n
= 178), had protective neutralizing antibody of ≥1:8 for
poliovirus types 1 and 2 and 98.3% (n = 175) for poliovirus type 3.15
In the same study, hepatitis B vaccine (supplied by different manufacturers)
was also given to children by different schedules. Hepatitis B
vaccine was given concurrently with DAPTACEL™ at 2 and 6 months of age to a
subset of infants who received a birth dose of hepatitis
B vaccine. Of infants with adequate serum available for serology testing (n
= 82), 97% achieved anti-HBs antibody levels ≥10 mIU/mL
post dose 3.15
No immunogenicity data are available for concurrent administration of
DAPTACEL™ with IPV; pneumococcal conjugate vaccine;
measles, mumps and rubella vaccine (MMR) or varicella vaccine.
INDICATIONS AND USAGE
DAPTACEL™ is indicated for active immunization against diphtheria, tetanus
and pertussis in infants and children 6 weeks through 6 years
of age (prior to seventh birthday).
Children who have had well-documented pertussis (culture positive for B.
pertussis or epidemiologic linkage to a culture positive case)
should complete the vaccination series with DT; some experts recommend
including acellular pertussis vaccine as well. Although welldocumented
pertussis disease is likely to confer immunity, the duration of protection
is unknown.17
DAPTACEL™ is not to be used for the treatment of B. pertussis, C.
diphtheriae or C. tetani infections.
When passive protection is required, Tetanus Immune Globulin and/or
Diphtheria Antitoxin may also be administered at separate sites
with separate needles and syringes.4 (See DOSAGE AND ADMINISTRATION.)
As with any vaccine, vaccination with DAPTACEL™ may not protect 100% of
susceptible individuals.
CONTRAINDICATIONS
This vaccine is contraindicated in children and adults seven years of age
and older.
Hypersensitivity to any component of the vaccine is a contraindication to
further administration.5
Page 4 of 12
The following events after receipt of DAPTACEL™ are contraindications to
further administration of any pertussis-containing vaccine:5
• An immediate anaphylactic reaction. Because of uncertainty as to which
component of the vaccine may be responsible, no further
vaccination with diphtheria, tetanus or pertussis components should be
carried out. Alternatively, such individuals may be referred to
an allergist for evaluation if further immunizations are to be considered.
• Encephalopathy not attributable to another identifiable cause (e.g., an
acute, severe central nervous system disorder occurring within
7 days after vaccination and consisting of major alterations in
consciousness, unresponsiveness or generalized or focal seizures that
persist more than a few hours, without recovery within 24 hours). In such
cases, DT vaccine should be administered for the
remaining doses in the vaccination schedule.
The decision to administer or delay vaccination because of a current or
recent febrile illness depends on the severity of symptoms and
on the etiology of the disease. According to the ACIP, all vaccines can be
administered to persons with mild illness such as diarrhea,
mild upper-respiratory infection with or without low-grade fever, or other
low-grade febrile illness.17,18 However, children with moderate
or serious illness should not be immunized until recovered.4
Elective immunization procedures should be deferred during an outbreak of
poliomyelitis because of the risk of provoking
paralysis.19,20,21
WARNINGS
The stopper to the vial of this product contains dry natural latex rubber
that may cause allergic reactions.
If any of the following events occur within the specified period after
administration of a whole-cell pertussis DTP or DTaP vaccine,
providers and parents should evaluate the risks and benefits of subsequent
doses of whole-cell pertussis DTP or DTaP vaccines:5
• Temperature of ≥40.5°C (105°F) within 48 hours, not attributable to
another identifiable cause.
• Collapse or shock-like state (hypotonic-hyporesponsive episode) within 48
hours.
• Persistent crying lasting ≥3 hours within 48 hours.
• Convulsions with or without fever within 3 days.
When a decision is made to withhold pertussis vaccine, immunization with DT
vaccine should be continued.4
Because of the risk of hemorrhage, DAPTACEL™ should not be given to children
with any coagulation disorder, including
thrombocytopenia, which would contraindicate intramuscular injection unless
the potential benefit clearly outweighs the risk of
administration.
Studies suggest that, when given whole-cell pertussis DTP vaccine, infants
and children with a history of convulsions in first-degree
family members have a 2.4-fold increased risk for neurologic events.22
However, ACIP has concluded that a history of convulsions or
other central nervous system disorders in parents or siblings is not a
contraindication to pertussis vaccination and that children with
such family histories should receive DTaP vaccines according to the
recommended schedule.4,17,18
If an infant or young child with a personal or family history of febrile or
non-febrile convulsions is to be immunized,
acetaminophen or other appropriate antipyretic should be given at the time
of DTaP vaccination and for the ensuing 24 hours
according to the respective package insert recommended dosage to reduce the
possibility of post-vaccination fever.4,17,18
A committee of the Institute of Medicine (IOM) has concluded that the
evidence is consistent with a causal relationship between wholecell
pertussis DTP vaccine and acute neurologic illness and, under special
circumstances, between whole-cell pertussis DTP vaccine
and chronic neurologic disease in the context of the National Childhood
Encephalopathy Study (NCES) report.23,24 However, the IOM
committee concluded that the evidence was insufficient to determine whether
whole-cell pertussis DTP vaccine increased the overall
risk of chronic neurologic disease.24 Acute encephalopathy (with or without
permanent neurological injury) or permanent neurological
injury has not been reported following administration of DAPTACEL™ but the
experience with this vaccine is insufficient to rule this out.
(See ADVERSE REACTIONS.)
Infants and children with recognized possible or potential underlying
neurologic conditions seem to be at enhanced risk for the
appearance of manifestations of the underlying neurologic disorder within 2
or 3 days following whole-cell pertussis DTP vaccine
immunization.4 Whether to administer DAPTACEL™ to children with proven or
suspected underlying neurologic disorders must be
decided on an individual basis after consideration of the risks and
benefits. An important consideration includes the current local
incidence of pertussis. The ACIP has issued guidelines for such children.25
PRECAUTIONS
General
Care is to be taken by the health-care provider for the safe and effective
use of this vaccine.
Epinephrine Hydrochloride Solution (1:1,000), other appropriate agents and
equipment must be available for immediate use in case an
anaphylactic or acute hypersensitivity reaction occurs. Health-care
providers must be familiar with current recommendations for the
initial management of anaphylaxis in non-hospital settings, including proper
airway management.17,26
Before an injection of any vaccine, all known precautions should be taken to
prevent adverse reactions. This includes a review of the
patient’s history with respect to possible sensitivity to the vaccine,
similar vaccines or to dry natural latex rubber (see WARNINGS),
previous immunization history, current health status (see CONTRAINDICATIONS)
and a current knowledge of the literature concerning
the use of the vaccine under consideration including the nature of adverse
events that may follow its use.
The expected immune response to DAPTACEL™ may not be obtained in
immunosuppressed persons.4 Pertussis-containing vaccines
are not contraindicated in persons with HIV infection.17
Special care should be taken to ensure that the injection does not enter a
blood vessel.
A separate, sterile syringe and needle or a sterile disposable unit should
be used for each patient to prevent transmission of hepatitis or other
infectious agents from person to person. Needles should not be recapped but
should be disposed of according to biohazard waste guidelines.
Page 5 of 12
Information for Vaccine Recipients and Parents/Guardians
Before administration of this vaccine, health-care personnel should inform
the parent, guardian or other responsible adult of the
benefits and risks of the vaccine and the importance of completing the
immunization series unless a contraindication to further
immunization exists. (See ADVERSE REACTIONS and WARNINGS.)
The physician should inform the parent or guardian about the potential for
adverse reactions that have been temporally associated with
DAPTACEL™ and other pertussis-containing vaccines. The health-care provider
should provide the Vaccine Information Statements
(VIS) which are required by the National Childhood Vaccine Injury Act of
1986 to be given with each immunization. The parent or
guardian should be instructed to report any serious adverse reactions to
their health-care provider.
IT IS EXTREMELY IMPORTANT WHEN A CHILD RETURNS FOR THE NEXT DOSE IN THE
SERIES THAT THE PARENT OR GUARDIAN SHOULD
BE QUESTIONED CONCERNING ANY SYMPTOMS AND/OR SIGNS OF AN ADVERSE REACTION
AFTER THE PREVIOUS DOSE OF VACCINE.
(See CONTRAINDICATIONS and ADVERSE REACTIONS.)
Adverse events following immunization should be reported by health-care
providers to the Vaccine Adverse Events Reporting System
(VAERS). (See ADVERSE REACTIONS, Reporting of Adverse Events.)
Drug Interactions
As with other intramuscular (I.M.) injections, use with caution in patients
on anticoagulant therapy.
Immunosuppressive therapies, including irradiation, antimetabolites,
alkylating agents, cytotoxic drugs and corticosteroids (used in
greater than physiologic doses), may reduce the immune response to vaccines.
Although no specific studies with pertussis vaccine are
available, if immunosuppressive therapy is to be soon discontinued, it seems
reasonable to defer immunization until the patient has
been off therapy for one month; otherwise, the patient should be vaccinated
while still on therapy.4
If DAPTACEL™ is administered to persons with an immunodeficiency disorder,
on immunosuppressive therapy or after a recent
injection of immune globulin, an adequate immunologic response may not
occur.
For information regarding simultaneous administration with other vaccines
refer to DOSAGE AND ADMINISTRATION.
If passive immunization is needed for tetanus or diphtheria prophylaxis,
Tetanus Immune Globulin (Human) (TIG), or Diphtheria Antitoxin,if used, should be given in a separate site, with a separate needle and
syringe.18
Carcinogenesis, Mutagenesis, Impairment of Fertility DAPTACEL™ has not been evaluated for its carcinogenic or mutagenic potential
or impairment of fertility.
Pregnancy Category C
Animal reproduction studies have not been conducted with DAPTACEL™. It is
not known whether DAPTACEL™ can cause fetal harm
when administered to a pregnant woman or can affect reproductive capacity.
DAPTACEL™ is NOT recommended for use in a pregnant
woman.
Geriatric Use
This product is NOT recommended for use in adult populations.
Pediatric Use
SAFETY AND EFFECTIVENESS OF DAPTACEL™ IN INFANTS BELOW 6 WEEKS OF AGE HAVE
NOT BEEN ESTABLISHED. (See DOSAGE AND
ADMINISTRATION.)
THIS VACCINE IS NOT RECOMMENDED FOR PERSONS 7 YEARS OF AGE OR OLDER. Tetanus
and Diphtheria Toxoids Adsorbed For Adult
Use (Td) is to be used in individuals 7 years of age or older.
ADVERSE REACTIONS
Over 11,400 doses of DAPTACEL™ have been administered to infants and
toddlers in 6 clinical studies. In all, 3,694 children received a
total of 3 doses and 476 children received 4 doses of DAPTACEL™.14,15,27,28,29,30,31
In the Sweden I Efficacy Trial, DAPTACEL™ was compared with DT and a
whole-cell pertussis DTP vaccine. A standard diary card was
kept for 14 days after each dose and follow-up telephone calls were made 1
and 14 days after each injection. Telephone calls were
made monthly to monitor the occurrence of severe events and/or
hospitalizations for the 2 months after the last injection. There were
fewer of the common local and systemic reactions following DAPTACEL™ than
following the whole-cell pertussis DTP vaccine. As
shown in Table 1, the 2,587 infants who enrolled to receive DAPTACEL™ at 2,
4 and 6 months of age had similar rates of reactions
within 24 hours as recipients of DT and significantly lower rates than
infants receiving whole-cell pertussis DTP.14
The rates of local reactions reported 1 day after any dose were lower in the
DAPTACEL™ and DT groups than in the whole-cell
pertussis DTP vaccine group.
Page 6 of 12
TABLE 114,15 PERCENTAGE OF INFANTS FROM SWEDEN I EFFICACY TRIAL WITH LOCAL
OR SYSTEMIC REACTIONS WITHIN
24 HOURS POST-DOSE 1, 2 AND 3 OF DAPTACEL™ COMPARED WITH DT AND WHOLE-CELL
PERTUSSIS DTP
VACCINES
Dose 1 Dose 2 Dose 3
(2 MONTHS) (4 MONTHS) (6 MONTHS)
EVENT DAPTACEL™ DT DTP DAPTACEL™ DT DTP DAPTACEL™ DT DTP
N = 2,587 N = 2,574 N = 2,102 N = 2,563 N = 2,555 N = 2,040 N = 2,549 N =
2,538 N = 2,001
Local
Tenderness
(Any) 8.0* 8.4 59.5 10.1* 10.3 60.2 10.8* 10.0 50.0
Redness
≥2 cm 0.3* 0.3 6.0 1.0* 0.8 5.1 3.7* 2.4 6.4
Swelling
≥2 cm 0.9* 0.7 10.6 1.6* 2.0 10.0 6.3*§ 3.9 10.5
Systemic
Fever? ≥38°C
(100.4°F) 7.8* 7.6 72.3 19.1* 18.4 74.3 23.6* 22.1 65.1
Fretfulness?? 32.3 33.0 82.1 39.6 39.8 85.4 35.9 37.7 73.0
Anorexia 11.2* 10.3 39.2 9.1* 8.1 25.6 8.4* 7.7 17.5
Drowsiness 32.7* 32.0 56.9 25.9* 25.6 50.6 18.9* 20.6 37.6
Crying
≥1 hour 1.7* 1.6 11.8 2.5* 2.7 9.3 1.2* 1.0 3.3
Vomiting 6.9* 6.3 9.5 5.2** 5.8 7.4 4.3 5.2 5.5
N = Number of evaluable subjects
* p<0.001: DAPTACEL™ versus whole-cell pertussis DTP
** p<0.003: DAPTACEL™ versus whole-cell pertussis DTP
§ p<0.0001: DAPTACEL™ versus DT
? Rectal temperature
?? Statistical comparisons were not made for this variable
DT: Swedish National Biologics Laboratories
DTP: Aventis Pasteur Inc.
The incidence of serious and less common selected systemic events in this
trial are summarized in Table 2.14,15
TABLE 214,15 SELECTED SYSTEMIC EVENTS: RATES PER 1,000 DOSES AFTER
VACCINATION AT 2, 4, AND 6 MONTHS OF AGE
IN SWEDEN I EFFICACY TRIAL
Dose 1 Dose 2 Dose 3
(2 MONTHS) (4 MONTHS) (6 MONTHS)
EVENT DAPTACEL™ DT DTP DAPTACEL™ DT DTP DAPTACEL™ DT DTP
N = 2,587 N = 2,574 N = 2,102 N = 2,565 N = 2,556 N = 2,040 N = 2,551 N =
2,539 N = 2,002
Rectal temperature 0.39 0.78 3.33 0 0.78 3.43 0.39 1.18 6.99
≥40°C (104°F) within
48 hours of vaccination
Hypotonic- 0 0 1.9 0 0 0.49 0.39 0 0
hyporesponsive
episode within 24 hours
of vaccination
Persistent crying ≥3 1.16 0 8.09 0.39 0.39 1.96 0 0 1.0
hours within 24 hours
of vaccination
Seizures within 72 0 0.39 0 0 0.39 0.49 0 0.39 0
hours of vaccination
N = Number of evaluable subjects
One case of whole limb swelling and generalized symptoms, with resolution
within 24 hours, was observed following dose 2 of
DAPTACEL™. No episodes of anaphylaxis or encephalopathy were observed. No
seizures were reported within 3 days of vaccination
with DAPTACEL™. Over the entire study period, 6 seizures were reported in
the DAPTACEL™ group, 9 in the DT group and 3 in the
whole-cell pertussis DTP group, for overall rates of 2.3, 3.5 and 1.4 per
1,000 vaccinees, respectively. One case of infantile spasms was
reported in the DAPTACEL™ group. There were no instances of invasive
bacterial infection or death.14,15
Rates of serious adverse events that are less common than those reported in
the Sweden I Efficacy Trial are not known at this time.
Table 3 summarizes the safety results from the Phase II Study in Canada in
children who were immunized at 2, 4, 6 and 17–18 months
of age with DAPTACEL™. For adverse events, parents recorded information for
72 hours post-immunization in a diary card. Local
reactions of redness and swelling were assessed and measured by the parents
using a template with graded size markings. Study staff
collected the information from the parents during a structured telephone
interview at 2–6, 8–12, 24, 48 and 72 hours and 7 days postimmunization
and recorded the information in the case report form.15,29
Local and systemic adverse events were consistently less common in DAPTACEL™
recipients at 2, 4 and 6 months of age than in those
who received whole-cell pertussis DTP vaccine. Following the fourth dose,
the same trends were observed, except for rates of severe
redness and swelling which did not differ between the 2 vaccine groups.
Rates of local reactions of redness and swelling were increased
following the fourth dose compared with the first 3 doses as was mild
tenderness but there was no increase in severe tenderness.
TABLE 315,29 PERCENTAGE OF CHILDREN FROM PHASE II STUDY IN CANADA WITH LOCAL
OR SYSTEMIC REACTIONS
WITHIN 72 HOURS OF VACCINATION WITH DAPTACEL™ AND WHOLE-CELL PERTUSSIS DTP
VACCINE AT 2, 4,
6 AND 17–18 MONTHS OF AGE
Dose 1 Dose 2 Dose 3 Dose 4
(2 MONTHS) (4 MONTHS) (6 MONTHS) (18 MONTHS)
EVENT DAPTACEL™ DTP# DAPTACEL™ DTP# DAPTACEL™ DTP# DAPTACEL™ DTP#
N = 324 N = 108 N = 321 N = 106 N = 320 N = 104 N = 301 N = 97
Local
Redness
Any 12.7* 44.4 20.6* 57.5 22.2* 51.9 36.5* 55.7
≥10 mm 1.2* 13.9 7.8* 22.6 10.0* 17.3 27.9 36.1
≥35 mm 0.3* 3.7 0.3* 5.7 1.6 1.9 21.9 20.6
Swelling
Any 4.3* 23.1 4.3* 32.1 4.7* 25.0 18.6* 28.9
≥10 mm 1.9* 15.7 2.2* 21.7 3.8* 14.4 15.9* 25.8
≥35 mm 0.3* 6.5 0* 5.7 0.9* 4.8 11.3 15.5
Tenderness†
Any 10.2* 37.0 7.5* 51.9 8.8* 48.1 23.9* 86.6
Moderate + Severe 0.9* 13.0 1.2* 20.8 1.3* 17.3 3.0* 53.6
Severe 0* 4.6 0.3* 7.5 0* 4.8 0.3* 12.4
Systemic
Fever†§
Any ≥37.5°C (99.5°F) 12.0* 43.7 7.7* 50.0 14.8* 53.2 14.5* 67.9
≥38°C (100.4°F) 0.7 1.9 0* 7.8 1.2* 11.7 1.9* 17.9
≥40°C (104°F) 0.3 0 0 1.0 0 1.1 0 0
Irritabilityϒ
Any 41.0* 65.7 41.4* 68.9 40.9* 67.3 36.9* 79.4
Moderate + Severe 9.0* 18.5 6.9* 22.6 5.0* 22.1 5.0* 24.7
Severe 0 1.9 0.3 0 0 1.0 0 2.1
AnorexiaΩ
Any 16.0 22.2 9.0* 16.0 11.6* 23.1 17.6* 41.2
Moderate + Severe 1.5 3.7 0.9 2.8 1.3 1.9 2.0* 13.4
Severe 0 0 0.3 0 0 0 0 2.1
Drowsiness∇
Any 43.2 52.8 21.8* 33.0 14.4* 32.7 13.3* 29.9
Moderate + Severe 7.7 8.3 2.8* 7.5 1.3 0 1.0* 6.2
Severe 0.3 0 0 0 0 0 0 0
Crying ≥3 Hours 0.6 0.9 0.3 0.9 0 1.0 0 1.0
N = Number of evaluable subjects
# DTP: whole-cell pertussis DTP vaccine (Aventis Pasteur Limited)
* Significantly less reactogenic than whole-cell DTP vaccine, p<0.05
† Moderate = sustained cry with gentle pressure at injection site; Severe =
cries when leg is moved
‡ Temperature measurements were axillary
§ Number of evaluable subjects for DAPTACEL™/DTP = 301/103, 298/102, 257/94
and 207/78 at 2, 4, 6 and 18 months, respectively
ϒ Moderate = more difficulty with settling, even with cuddling; Severe =
persistent crying/screaming and inability to console
Ω Moderate = missed one or two feeds; Severe = little or no intake for more
than two feeds
∇ Moderate = sleeping much more than normal; Severe = sleeping most of the
time with difficulty arousing
The US Bridging Study was designed, in part, to assess the safety of
DAPTACEL™ in infants at 2, 4 and 6 months of age, with routinely
recommended, concurrently given childhood vaccines (Haemophilus influenzae
type b vaccine, OPV and hepatitis B). For adverse events,
parents recorded information for 72 hours post-immunization in a diary card.
Local reactions were assessed and measured by the parents.
Study staff collected the information from the parents during a structured
telephone interview on days 4 and 14 post-immunization and
recorded the information in the case report form.15 The incidence of
redness, swelling, pain or tenderness at the injection site and systemic
symptoms after each dose is shown as pooled data from 2 lots of DAPTACEL™
(Lots 006 and 009) in Table 4. Fever ≥38°C (100.4°F) was
observed in 9.9% – 11.9% of subjects. The incidence of severe systemic
symptoms including irritability, tiredness, anorexia, rash and
vomiting ranged from 0.3% – 0.6%. One afebrile seizure occurred within 24
hours post dose 2 immunization (n = 321).15
Page 7 of 12
Page 8 of 12
In an ongoing study (P3T06) initiated in May 2001 and anticipated to be
completed in 2004, which was designed to assess the safety of
DAPTACEL™ given with routinely recommended vaccines (Haemophilus influenzae
type b vaccine, IPV, hepatitis B and pneumococcal
conjugate vaccine) in the US (in which 777 children have received their
first dose, 350 have received their second dose and 86 their third
dose with safety data still being collected from children in this study),
one afebrile seizure was reported within 24 hours of receipt of dose 1.
TABLE 415 PERCENTAGE OF CHILDREN FROM US BRIDGING STUDY WITH ANY LOCAL AND
SYSTEMIC REACTIONS WITHIN
72 HOURS OF VACCINATION WITH DAPTACEL™ AT 2, 4 AND 6 MONTHS OF AGE (LOTS 006
AND 009 POOLED)
Dose 1 Dose 2 Dose 3
EVENT (2 MONTHS) (4 MONTHS) (6 MONTHS)
N = 321 N = 317 N = 315
Local
Redness
Any 12.5 15.8 19.7
<1 inch 11.8 15.1 18.7
≥1 inch 0.6 0.6 1.0
Swelling
Any 14.3 15.4 17.8
<1 inch 13.7 15.1 16.2
≥1 inch 0.6 0.3 1.6
Tenderness
Any 30.5 19.6 15.9
Moderate + Severe 8.1 4.4 1.0
Severe 0 0 0
Systemic
Fever*†
Any ≥38°C (100.4°F) 11.9 9.9 9.9
≥39°C (102.2°F) 0.3 0.3 0.6
≥40°C (104°F) 0 0 0
Irritability
Any 72.0 61.2 56.2
Moderate + Severe 33.6 25.2 18.7
Severe 0.3 0.3 0
Anorexia
Any 26.2 14.8 17.8
Moderate + Severe 5.6 3.8 4.8
Severe 0 0.3 0
Drowsiness
Any 62.0 44.8 35.6
Moderate + Severe 24.0 8.5 7.3
Severe 0.6 0.3 0
Crying ≥3 Hours 0.3 0 0
N = Number of evaluable subjects
* Rectal temperature
† N = 319, 314 and 313 at 2, 4 and 6 months respectively
Moderate = discomforting enough to interfere with or limit usual daily
activity
Severe = disabling, unable to perform daily activities
NIAID sponsored a multicenter Phase I/II clinical trial to compare the
safety and immunogenicity of 13 acellular pertussis vaccines with
a conventional whole-cell pertussis DTP vaccine in infants in the US. The
common local and systemic adverse experiences, after all 3
doses, for DAPTACEL™ and the participating acellular vaccines that have
subsequently been licensed in the US were generally similar
in type and frequency and were reduced in comparison to the whole-cell
pertussis DTP vaccine.28
Additional adverse reactions evaluated in conjunction with pertussis,
diphtheria and tetanus vaccination are as follows:
• As with other aluminum-containing vaccines, a nodule may be palpable at
the injection sites for several weeks. Sterile abscess
formation at the site of injection has been reported.4,32
• Rarely, anaphylactic reactions (i.e., hives, swelling of the mouth,
difficulty breathing, hypotension or shock) have been reported after
receiving preparations containing diphtheria, tetanus and/or pertussis
antigens.4
Arthus-type hypersensitivity reactions, characterized by severe local
reactions (generally starting 2-8 hours after an injection), may
follow receipt of tetanus toxoid. A few cases of peripheral neuropathy have
been reported following tetanus toxoid administration,
although the evidence is inadequate to accept or reject a causal relation.33
Page 9 of 12
A review by the Institute of Medicine (IOM) found a causal relation between
tetanus toxoid and brachial neuritis and Guillain-Barré
syndrome.34 The following illnesses have been reported as temporally
associated with some vaccines containing tetanus toxoid:
neurological complications35,36 including cochlear lesion, brachial plexus
neuropathies,37 paralysis of the radial nerve,33 paralysis of the
recurrent nerve, accommodation paresis and EEG disturbances with
encephalopathy (with or without permanent intellectual or motor
function impairment).38,39 In the differential diagnosis of
polyradiculoneuropathies following administration of a vaccine containing
tetanus toxoid, tetanus toxoid should be considered as a possible
etiology.39
Onset of infantile spasms has occurred in infants who have recently received
whole-cell pertussis DTP or DT. Analysis of data from the
National Childhood Encephalopathy Study (NCES) on children with infantile
spasms failed to demonstrate that receipt of DT or whole-cell
pertussis DTP vaccines was causally related to infantile spasms.23,40 The
incidence of onset of infantile spasms increases at 3-9 months
of age, the time period in which the second and third doses of whole-cell
pertussis DTP are generally given. Therefore, some cases of
infantile spasms can be expected to be related by chance alone to recent
receipt of whole-cell pertussis DTP.4
Persistent, inconsolable crying lasting ≥3 hours and high-pitched, unusual
screaming, 1% and 0.1% respectively, after 15,752 doses of
whole-cell pertussis DTP vaccine have been reported.38 Convulsions and
hypotonic-hyporesponsive episodes (HHE) have each been
reported to occur at a frequency of about 1:1,750 injections of whole-cell
pertussis DTP.17,26,38 Most convulsions are brief, generalized
and self-limited and are usually associated with fever. Neither febrile nor
afebrile convulsions associated with whole-cell pertussis DTP
vaccine have been shown to be associated with subsequent seizure disorder.17
Persistent, inconsolable crying ≥3 hours, convulsions
and HHE have also been reported following DTaP vaccines, including DAPTACEL™.5
In another large study (Sweden II Efficacy Trial), 3 DTaP vaccines and a
whole-cell pertussis DTP vaccine, none of which are licensed in the
US, were evaluated to assess relative safety and efficacy.41 This study
included HCPDT, a vaccine made of the same components as
DAPTACEL™ but containing twice the amount of PT and four times the amount of
FHA (20 µg pertussis toxoid and 20 µg FHA). Hypotonichyporesponsive
episodes (HHE) were observed following 29 (0.047%) of 61,220 doses of HCPDT;
16 (0.026%) of 61,219 doses of an
acellular pertussis vaccine made by another manufacturer; and 34 (0.056%) of
60,792 doses of a whole-cell pertussis DPT vaccine. There
were 4 additional cases of HHE in other studies using HCPDT vaccine for an
overall rate of 33 (0.047%) in 69,525 doses.15,41 (See
CONTRAINDICATIONS and PRECAUTIONS.)
Sudden Infant Death Syndrome (SIDS) has occurred in infants following
administration of whole-cell pertussis DTP and DTaP. Large
case-control studies of SIDS in the US have shown that receipt of whole-cell
pertussis DTP was not causally related to SIDS.42,43 It
should be recognized that the first 3 immunizing doses of whole-cell
pertussis DTP and DTaP (including DAPTACEL™) are usually
administered to infants 2-6 months of age and that approximately 85% of SIDS
cases occur at ages 1-6 months with the peak
incidence occurring at 6 weeks to 4 months of age. By chance alone, some
cases of SIDS can be expected to follow receipt of wholecell
pertussis DTP17 and acellular pertussis vaccines. A review by a committee of
the IOM concluded that available evidence did not
indicate a causal relation between whole-cell pertussis DTP vaccine and
SIDS.23
Whole-cell pertussis DTP vaccine has been associated with acute
encephalopathy.23 A 10-year follow-up to the National Childhood
Encephalopathy Study (NCES) of children who experienced acute neurologic
disorders in infancy concluded that serious acute neurologic
illness increased the risk of chronic neurologic disease or death.44 A
committee of the Institute of Medicine (IOM) has concluded that,
because whole-cell pertussis DTP may cause acute neurologic illness,
whole-cell pertussis DTP may also cause chronic neurologic
disease in the context of the NCES report.24 However, the IOM committee
concluded that the evidence was insufficient to indicate
whether or not whole-cell pertussis DTP increased the overall risk of
chronic neurologic disease.24
A bulging fontanel associated with increased intracranial pressure which
occurred within 24 hours following whole-cell pertussis DTP
immunization has been reported, although a causal relationship has not been
established.45,46,47
Reporting of Adverse Events
The National Vaccine Injury Compensation Program, established by the
National Childhood Vaccine Injury Act of 1986, requires
physicians and other health-care providers who administer vaccines to
maintain permanent vaccination records of the manufacturer and
lot number of the vaccine administered in the vaccine recipient’s permanent
medical record along with the date of administration of the
vaccine and the name, address and title of the person administering the
vaccine. The Act (or statute) further requires the health-care
professional to report to the Secretary of the US Department of Health and
Human Services the occurrence following immunization of
any events set forth in the statute or the Vaccine Injury Table, including
anaphylaxis or anaphylactic shock within 7 days; encephalopathy
or encephalitis within 7 days, brachial neuritis within 28 days; or an acute
complication or sequelae (including death) of an illness,
disability, injury, or condition referred to above, or any events that would
contraindicate further doses of vaccine, according to this
DAPTACEL™ package insert.17,48
Reporting by parents or guardians of all adverse events after vaccine
administration should be encouraged. Adverse events following
immunization with vaccine should be reported by health-care providers to
VAERS. Reporting forms and information about reporting
requirements or completion of the form can be obtained from VAERS through a
toll-free number 1-800-822-7967.48,49
Health-care providers should also report these events to the
Pharmacovigilance Department, Aventis Pasteur Inc., Discovery
Drive, Swiftwater, PA 18370 or call 1-800-822-2463.
DOSAGE AND ADMINISTRATION
DAPTACEL™ is a sterile white homogenous cloudy suspension of acellular
pertussis vaccine components and diphtheria and tetanus
toxoids adsorbed on aluminum in a sterile isotonic sodium chloride solution
and containing 2-phenoxyethanol as preservative. Inspect
the vial visually for extraneous particulate matter and/or discoloration
before administration. If these conditions exist, the product should
not be administered.
JUST BEFORE USE, SHAKE THE VIAL WELL, until a uniform, cloudy suspension
results. WITHDRAW AND INJECT A 0.5 mL DOSE. When
administering a dose from a rubber-stoppered vial, do not remove either the
rubber stopper or the metal seal holding it in place. Aseptic
technique must be used for withdrawal of each dose.
Page 10 of 12
Before injection, the skin over the site to be injected should be cleansed
with a suitable germicide. After insertion of the needle into the
muscle, aspirate to ensure that the needle has not entered a blood vessel.
Administer the vaccine intramuscularly (I.M.). In children younger than 1
year (i.e., infants), the anterolateral aspect of the thigh
provides the largest muscle and is the preferred site of injection. In older
children, the deltoid muscle is usually large enough for I.M.
injection. The vaccine should not be injected into the gluteal area or areas
where there may be a major nerve trunk.17
Fractional doses (doses <0.5 mL) should not be given. The effect of
fractional doses on the frequency of serious adverse events and on
efficacy has not been determined.
Do NOT administer this product intravenously or subcutaneously.
Immunization Series
A 0.5 mL dose of DAPTACEL™ is approved for administration as a 4 dose series
at 2, 4 and 6 months of age, at intervals of 6–8 weeks
and at 17–20 months of age. (See CLINICAL PHARMACOLOGY.) The customary age
for the first dose is 2 months of age, but it may be
given as early as 6 weeks of age and up to the seventh birthday. The
interval between the third and fourth dose should be at least
6 months. It is recommended that DAPTACEL™ be given for all doses in the
series because no data on the interchangeability of
DAPTACEL™ with other DTaP vaccines exist. At this time, data are
insufficient to establish the frequency of adverse events following a
fifth dose of DAPTACEL™ in children who have previously received 4 doses of
DAPTACEL™.50
DAPTACEL™ may be used to complete the immunization series in infants who
have received 1 or more doses of whole-cell pertussis
DTP. However, the safety and efficacy of DAPTACEL™ in such infants have not
been fully demonstrated.5
PERSONS 7 YEARS OF AGE AND OLDER SHOULD NOT BE IMMUNIZED WITH DAPTACEL™ OR
ANY OTHER PERTUSSIS-CONTAINING
VACCINES.18
DAPTACEL™ should not be combined through reconstitution or mixed with any
other vaccine.If any recommended dose of pertussis vaccine cannot be given, DT (For
Pediatric Use) should be given as needed to complete the series.
Pre-term infants should be vaccinated according to their chronological age
from birth.17
Interruption of the recommended schedule with a delay between doses should
not interfere with the final immunity achieved with
DAPTACEL™. There is no need to start the series over again, regardless of
the time between doses.
Simultaneous Vaccine Administration
In clinical trials, DAPTACEL™ was routinely administered, at separate sites,
concomitantly with one or more of the following vaccines:
OPV, hepatitis B vaccine and Haemophilus influenzae type b vaccine.15 No
safety and immunogenicity data are currently available on
the simultaneous administration of pneumococcal conjugate vaccine, MMR
vaccine and varicella vaccine and no immunogenicity data
are currently available on the simultaneous administration of IPV. Two
afebrile seizures, occurring within 24 hours of immunization, have
been reported from 2 US trials where DAPTACEL™ was given with other
concomitant vaccines. (See ADVERSE REACTIONS.) When
concomitant administration of other vaccines is required, they should be
given with different syringes and at different injection sites.
ACIP encourages routine simultaneous administration of DTaP, IPV,
Haemophilus influenzae type b vaccine, pneumococcal conjugate
vaccine, MMR, varicella vaccine and hepatitis B vaccine for children who are
the recommended age to receive these vaccines and for
whom no specific contraindications exist at the time of the visit, unless,
in the judgment of the provider, complete vaccination of the
child will not be compromised by administering different vaccines at
different visits. Simultaneous administration is particularly
important if the child might not return for subsequent vaccinations.18 (See
CLINICAL PHARMACOLOGY.)
If passive immunization is needed for tetanus prophylaxis, Tetanus Immune
Globulin (Human) (TIG) is the product of choice. It provides
longer protection than antitoxin of animal origin and is associated with few
adverse reactions. The currently recommended prophylactic
dose of TIG for wounds of average severity is 250 units intramuscularly.
When tetanus toxoid-containing vaccines and TIG and/or
Diphtheria Antitoxin are administered concurrently, separate syringes and
separate sites should be used.
HOW SUPPLIED
Vial, 1 x 1 Dose - Product No. 49281-286-01
Vial, 5 x 1 Dose - Product No. 49281-286-05
STORAGE
DAPTACEL™ 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.
REFERENCES
1. Stainer DW, Scholte MJ. A simple chemically defined medium for the
production of phase I Bordetella pertussis. J Gen Microbiol
1970;63:211-220.
2. Stainer DW. Production of diphtheria toxin. In: Manclark CR, ed.
Proceeding 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 Publication No. (FDA) 91-1174. 1991:7-11.
3. Mueller JH, Miller PA. Variable factors influencing the production of
tetanus toxin. J Bacteriol 1953;67:271-277.
4. Recommendations of the Advisory Committee on Immunization Practices (ACIP).
Diphtheria, Tetanus, and Pertussis:
Recommendations for vaccine use and other preventive measures. MMWR
1991;40(RR-10):1-28.
5. Recommendations of the Advisory Committee on Immunization Practices (ACIP).
Pertussis vaccination: Use of acellular pertussis
vaccines among infants and young children. MMWR 1997;46(RR-7):1-25.
6. Plotkin SA, et al. Vaccines. 3rd ed. Philadelphia,W. B. Saunders Company.
1999:140-157,293-344,441-474.
7. Centers for Disease Control and Prevention (CDC). Notice to readers:
Final 2000 reports of notifiable diseases. MMWR
2001;50(33):1-10.
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8. Atkinson W, et al, editors. Epidemiology and Prevention of
Vaccine-Preventable Diseases. 6th ed.Centers for Disease Control and
Prevention (CDC); Public Health Foundation. 2000:51-72.
9. American Public Health Association (APHA). Control of Communicable
Diseases Manual. 2000;(17):166-167.
10. Hardy IRB, et al. Current situation and control strategies for
resurgence of diphtheria in newly independent states of the former
Soviet Union. Lancet 1996;347:1739-1744.
11. Bedson SP, et al.The prevention of whooping-cough by vaccination. A
Medical Research Council Investigation. Br Med J
1951;1:1463-1471.
12. Centers for Disease Control and Prevention (CDC). Pertussis-United
States,1997-2000. MMWR 2002;51(4):1-92.
13. Güris D, et al. Changing epidemiology of pertussis in the United States:
Increasing reported incidence among adolescents and
adults, 1990-1996. Clin Infect Dis 1999;28:1230-1237.
14. 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;6:349-355.
15. Aventis Pasteur Limited: Data on File.
16. Department of Health and Human Services, Food and Drug Administration.
Biological Products; Bacterial Vaccines and Toxoids;
Implementation of Efficacy Review; Proposed Rule. Federal Register 1985;
50(240):51002-51117.
17. American Academy of Pediatrics. In: Pickering LK, ed. 2000 Red Book:
Report on the Committee of Infectious Diseases. 25th ed.
Elk Grove Village, IL: American Academy of Pediatrics
2000:17,31-35,51-53,54,65,68,442-443,759-765.
18. Recommendations of the Advisory Committee on Immunization Practices (ACIP).
General recommendations on immunization.
MMWR 1994;43(RR-1):1-38.
19. Expanded programme on immunization, injection and paralytic
poliomyelitis. Wkly Epidem Rec 1980;5:38-40.
20. Sutter RW, et al. Attributable risk of DTP (diphtheria and tetanus
toxoids and pertussis vaccine) injection in provoking paralytic
poliomyelitis during a large outbreak in Oman. J Infect Dis
1992;165:444-449.
21. Christie AB. Infectious diseases: Epidemiology and Clinical Practice.
4th ed. Edinburgh, Churchill Livingstone. 1987;2:817-825.
22. Livengood JR, et al. Family history of convulsion and use of pertussis
vaccine. J Pediatr 1989;115(4):527-531.
23. Howson CP, et al. Adverse Effects of Pertussis and Rubella Vaccines,
Pertussis Vaccines and CNS Disorders. Institute of Medicine
(IOM). National Academy Press,Washington, DC, 1991:7-169.
24. Institute of Medicine (IOM). DTP vaccine and chronic nervous system
dysfunction: A new analysis. National Academy Press,
Washington, DC, 1994;Supplement:1-17.
25. Recommendations of the Advisory Committee on Immunization Practices (ACIP).
Update: Vaccine side effects, adverse reactions,
contraindications, and precautions. MMWR 1996;45(RR-12):1-35.
26. National Advisory Committee on Immunization (NACI): Canadian
Immunization Guide, 5th ed. Minister of Public Works and
Government Services Canada. 1998:9-13,133-139.
27. Edwards KM, et al. Comparison of 13 acellular pertussis vaccines:
Overview and serologic response. American Academy of
Pediatrics 1995;Supplement:548-557.
28. Decker MD, et al. Comparison of 13 acellular pertussis vaccines: Adverse
reactions. Pediatr 1995;96:557-566.
29. Halperin SA et al. Adverse reactions and antibody response to four doses
of acellular or whole-cell pertussis combined with
diphtheria and tetanus toxoids in the first 19 months of life. Vaccine
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Manufactured by: Product information
Aventis Pasteur Limited as of May 2002.
Toronto Ontario Canada
Distributed by:
Aventis Pasteur Inc.
Swiftwater PA 18370 USA Printed in Canada.
US Patents: 4500639, 4687738, 4784589, 4997915, 5444159, 5667787, 5877298.
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