Immunogenicity, reactogenicity and consistency of production of a Brazilian combined vaccine against diphtheria, tetanus, pertussis and Haemophilus influenzae type b

Martins, Reinaldo de Menezes; Camacho, Luiz Antonio Bastos; Marcovistz, Rugimar; Noronha, Tatiana Guimarães de; Maia, Maria de Lourdes Sousa; Santos, Eliane Matos dos; Barbosa, Glayse Glayde; Silva, Andrea Marques Vieira da; Souza, Patricia Cristina Neves Feliciano de; Lemos, Maria Cristina Ferreira; Homma, Akira

doi:10.1590/S0074-02762008000700014

Abstract

A randomized, double-blinded study evaluating the immunogenicity, safety and consistency of production of a combined diphtheria-tetanus-pertussis-Haemophilus influenzae type b vaccine entirely produced in Brazil by Bio-Manguinhos and Instituto Butantan (DTP/Hib-BM) was undertaken. The reference vaccine had the same DTP vaccine but the Hib component was produced using purified materials supplied by GlaxoSmithKline (DTP/Hib-GSK), which is registered and has supplied the Brazilian National Immunization Program for over more than five years. One thousand infants were recruited for the study and received vaccinations at two, four and six months of age. With respect to immunogenicity, the vaccination protocol was followed in 95.6% and 98.4% of infants in the DTP/Hib-BM and DTP/Hib-GSK groups, respectively. For the Hib component of the study, there was 100% seroprotection (>0.15 µg/mL) with all three lots of DTP/Hib-BM and DTP/Hib-GSK. The geometric mean titer (GMT) was 9.3 µg/mL, 10.3 µg/mL and 10.3 µg/mL for lots 1, 2 and 3 of DTP/Hib-BM, respectively, and the GMT was 11.3 g/mL for DTP/Hib-GSK. For diphtheria, tetanus and pertussis, seroprotection was 99.7%, 100% and 99.9%, respectively, for DTP/Hib-BM, three lots altogether and 99.2%, 100% and 100% for DTP/Hib-GSK. GMTs were similar across all lots and vaccines. Adverse events rates were comparable among the vaccine groups. The Brazilian DTP/Hib vaccine demonstrated an immunogenicity and reactogenicity profile similar to that of the reference vaccine.

vaccines; immunization; combination vaccines; DTP/Hib vaccine

ARTICLES

Immunogenicity, reactogenicity and consistency of production of a Brazilian combined vaccine against diphtheria, tetanus, pertussis and Haemophilus influenzae type b

Reinaldo de Menezes MartinsI, ⁺ + Corresponding author: rmenezes@bio.fiocruz.br ; Luiz Antonio Bastos Camacho^II; Rugimar Marcovistz^III; Tatiana Guimarães de Noronha^I; Maria de Lourdes Sousa Maia^I; Eliane Matos dos Santos^I; Glayse Glayde Barbosa^I; Andrea Marques Vieira da Silva^III; Patricia Cristina Neves Feliciano de Souza^III; Maria Cristina Ferreira Lemos^IV; Akira Homma^V

^IAssessoria Clínica

^IIEscola Nacional de Saúde Pública-Fiocruz

^IIILaboratório de Tecnologia Imunológica

^IVSecretaria Municipal de Saúde do Rio de Janeiro

^VBio-Manguinhos-Fiocruz, Av. Brasil 4365, Pavilhão Rocha Lima, 21040-900 Rio de Janeiro, RJ, Brasil

ABSTRACT

A randomized, double-blinded study evaluating the immunogenicity, safety and consistency of production of a combined diphtheria-tetanus-pertussis-Haemophilus influenzae type b vaccine entirely produced in Brazil by Bio-Manguinhos and Instituto Butantan (DTP/Hib-BM) was undertaken. The reference vaccine had the same DTP vaccine but the Hib component was produced using purified materials supplied by GlaxoSmithKline (DTP/Hib-GSK), which is registered and has supplied the Brazilian National Immunization Program for over more than five years. One thousand infants were recruited for the study and received vaccinations at two, four and six months of age. With respect to immunogenicity, the vaccination protocol was followed in 95.6% and 98.4% of infants in the DTP/Hib-BM and DTP/Hib-GSK groups, respectively. For the Hib component of the study, there was 100% seroprotection (>0.15 µg/mL) with all three lots of DTP/Hib-BM and DTP/Hib-GSK. The geometric mean titer (GMT) was 9.3 µg/mL, 10.3 µg/mL and 10.3 µg/mL for lots 1, 2 and 3 of DTP/Hib-BM, respectively, and the GMT was 11.3 g/mL for DTP/Hib-GSK. For diphtheria, tetanus and pertussis, seroprotection was 99.7%, 100% and 99.9%, respectively, for DTP/Hib-BM, three lots altogether and 99.2%, 100% and 100% for DTP/Hib-GSK. GMTs were similar across all lots and vaccines. Adverse events rates were comparable among the vaccine groups. The Brazilian DTP/Hib vaccine demonstrated an immunogenicity and reactogenicity profile similar to that of the reference vaccine.

Key words: vaccines - immunization - combination vaccines - DTP/Hib vaccine

The combined diphtheria-tetanus-pertussis-Haemophilus influenzae type b (DTP/Hib) vaccine allows for a reduction in the number of required injections, thus improving compliance to the vaccination schedule and higher vaccination coverage. Moreover, the combined vaccine has reduced the logistical costs related to factors such as number of visits to health care centers, number of syringes and needles required and necessary storage space.

In 1998, a technological transfer agreement was established with GlaxoSmithKline (GSK) for the Brazilian production of Hib vaccine (Homma et al. 2005). In 1999, Hib vaccine produced by GSK was introduced in the Brazilian National Immunization Program (NIP) and administered at two, four and six months of age, concomitant to the administration at another site of a DTP vaccine produced by Instituto Butantan. Since 2002, these vaccinations have been administered as a single injection via dilution of the lyophilized vaccine (Hib) with the DTP vaccine at the moment of administration. Reports on the quality, immunogenicity and safety of this combination have been demonstrated in a clinical study (Clemens et al. 2003).

The technology transfer from GSK to Bio-Manguinhos (BM) was a strategic step toward the routine availability of this vaccine by the NIP. This process was concluded in 2005 with the production of the conjugate Hib vaccine by BM.

The present study aimed to determine if the quadrivalent vaccine with the Hib component produced by BM (DTP/Hib-BM) had immunogenicity and reactogenicity similar to that of the Hib vaccine produced by GSK (DTP/Hib-GSK). This was a study for clinical validation of the DTP/Hib-BM vaccine, which was required for its licensure by the Brazilian National Regulatory Agency. The performance of this combined vaccine is extremely important considering its role in the containment of the target diseases and its well-known reactogenicity accounted for by the whole-cell pertussis component.

The combined DTP/Hib vaccine with a cellular pertussis component generally provides good efficacy for all antigens, but in some studies the combination resulted in decreased immunogenicity of the Hib component in comparison to individual administration. Despite this finding, antibody levels against the vaccination components were found to be high and around 95% of immunized children demonstrated high levels of protective antibodies (Decker et al. 2008).

Acellular pertussis (aP) vaccines have been developed that include purified Bordetella pertussis antigens (Sato & Sato 1999, Edwards & Decker 2008). Acellular vaccines are less reactogenic, but the combination of aP with a Hib component is more problematic. With this formulation, the long-term protection against Hib may be lower than with combined vaccines containing whole-cell pertussis (Johnson et al. 2006, Decker et al. 2008). Large-scale immunization against pertussis in developed countries with cellular or acellular vaccinations has altered the epidemiology of the disease. The most prominent changes are a decreased incidence of infection in children and an increased incidence in adolescents and adults, which is most likely secondary to a combination of factors such as waning immunity, less-frequent natural boosters by disease and improved diagnosis (Decker et al. 2008).

SUBJECTS, MATERIALS AND METHODS

This was a double-blinded, randomized study of comparison between three consecutive commercially-available lots of DTP/Hib-BM vaccine and one lot of the reference vaccine, DTP/Hib-GSK. The three lots of DTP/Hib-BM and one lot of DTP/Hib-GSK differed only in the Hib vaccine component, as the DTP lot was the same in all four groups. Comparison of the new combined DTP/Hib-BM vaccine with both the concomitant and separate administration of DTP and Hib was not possible for ethical reasons since the combined vaccine was already in general use.

The study was conducted in five different Health Centers of the Municipal Health Secretary of Rio de Janeiro. Research personnel were trained in good clinical practices, good laboratory practices and on study procedures in compliance with the 1983 revision of the Helsinki Declaration. The study protocol was approved by the National Research Ethics Committee, the Ethical Committees of Fundação Oswaldo Cruz and of the Municipal Health Secretary of Rio de Janeiro, and by the National Regulatory Agency. The protocol was registered with International Standard Randomized Clinical Trial nº 67676353.

Blocked randomization, with block size known only by the statistician, aimed at equal distribution of the four different vaccines stratified by the five health care centers. Vaccine vials were sequentially labeled with numbers and were then assigned to study participants according to their order of arrival for vaccination. Only one of the five doses in each vial was used.

Eligibility for the study included general good health, age between 42 days and three months, birth weight equal to or greater than 2500 g, availability of parents (or guardians) for all of the study procedures and informed consent. Exclusion criteria were: previous vaccination against diphtheria, tetanus, pertussis and Hib; receipt during the study period of a vaccine other than BCG, oral polio, hepatitis B and meningococcal C conjugated to CRM; use of immunosuppressive drugs and blood or blood-derived products since birth or during the study period; any confirmed or suspected immunocompromising condition.

Vaccinations were administered at two, four and six months of age, with an acceptable variation of time between doses of 42-90 days. The interval between the last vaccine dose and the final collection of blood was 30 days, with an acceptable variation of 21-90 days.

Blood was collected for evaluation of antibodies to the vaccine antigens before the first and the third doses, and one month after third dose.

Adverse events following immunization - Study participants were followed for adverse events including local pain, erythema, edema and systemic events (fever, irritability, drowsiness, anorexia) occurring within three days of vaccination (solicited adverse events). Parents (or guardians) received a mercury thermometer, a ruler and a booklet to record any adverse events and were instructed about their utilization. Temperatures were measured in the axilla after placing the thermometer at the site for three minutes. All parents (or guardians) received phone calls and home visits from study personnel in order to improve adherence to the protocol. The number of children with complete records of adverse events (four times) was counted. The axillary temperature was expected to be recorded at six different times (3, 6, 12, 24, 48 and 72 h after each vaccination). At the time of vaccination, none of the children had fever as defined by an axillary temperature of 37.5ºC or greater.

Information about unsolicited adverse events was obtained during the month following each vaccination (an unsolicited adverse event is any adverse event spontaneously reported or reported after questioning). Serious adverse events were closely evaluated by the study investigators and the Coordination Group and followed until their resolution. An Independent Data Monitoring Committee comprised of experts on the evaluation of adverse events discussed each case involving a serious complication and any possible links to the vaccination.

In situations where emergency care was necessary, the parents (or guardians) were asked to go to the reference hospital assigned to each health care center. Two children's hospitals and other specialized services also gave helped support to the study participants. Local coordinators as well as the Coordinating Committee were available at all times to answer questions from parents (or guardians) or to visit the study participant at the hospital.

A meningococcus C conjugate vaccine (Menin-gitec^®) was given at three, five and seven months of age as a reward for the voluntary participation of parents (or guardians) and their children. This vaccination was provided in an ethically acceptable manner and was approved by the ethical committees.

Vaccinations - DTP/Hib was administered intramuscularly in the anterolateral aspect of the thigh. All four vaccines had the same composition. Each dose of 0.5 mL contained sufficient diphtheria and tetanus antigen for the induction of 2 UI of antitoxin in guinea pigs; the pertussis antigen contained an equivalent of 4 UI of the individual dose for humans; the amount of PRP (polyribosilribitol phosphate) conjugated to tetanus toxoid (PRP-T) was 10 g, the amount of aluminum hydroxide was 1.25 mg and thimerosal was 0.01%.

Measurement of antibodies to diphtheria, tetanus, pertussis, and Haemophilus influenzae type b - An enzyme-linked immunosorbent assay (ELISA) was used for antibody measurement. This assay was standardized at the Immunological Technology Laboratory of BM (LATIM) for the four vaccination antigens according to GSK's standard operating procedures (SOPs). For diphtheria and tetanus, LATIM's internal standards were titrated against international standards, which were acquired from the National Institute for Biological Standard Controls in England. For Hib, the internal standards were titrated against standards from GSK. For pertussis, antibody measurement was performed using a kit acquired through GSK (B. pertussis, IgG EIA ASOS). Serum was stored at -20ºC until the time of analysis. The diphtheria, tetanus and PRP antigen for coating ELISA plates were obtained from the Butantan Institute (Brazil) and GSK (Belgium), respectively. Anti-diphtheria and anti-tetanus ELISA titers were considered to be protective if they were equal to or higher than the cut-off of 0.1 IU/mL. B. pertussis antibodies were determined by a cut-off of 15 EL U/mL, while the cut-off for antibodies against PRP was 0.15 µg/mL, according to GSK SOPs. Serum titers were calculated using SoftMax Pro, version 5.2 (Molecular Devices, USA).

Statistical analyses - The three DTP/Hib-BM lots were considered to be consistent if the 95% confidence limit of differences in infants seroprotected by the lots, compared two by two, were within -5% and 5% and if the ratio of geometric mean titers (GMT) of antibodies were within 0.5-2. The pool of three lots of experimental vaccine was considered to be of equal efficacy to the reference vaccine if the difference (DTP/Hib-BM - DTP/Hib-GSK) in seroprotection was within 0 and -5% and if the ratio of GMT of antibodies was higher than 0.5. Analyses by intention to treat (all randomized children) and per protocol (volunteers who followed the protocol) were conducted. A sample size of 250 children in each group was based on the above criteria, a confidence level of 5%, a power of 80% and a 25% loss to follow-up.

For reactogenicity analyses, all children with adverse events registered at any time point were considered. Comparisons with the reference vaccine were made by chi-square analysis with a significance level of 0.05.

Data were analyzed using SPSS^® version15 (SPSS Inc, Chicago, Illinois), Epi-Info^® version 2000 (Centers for Diseases Control, Atlanta, Georgia) and Winpepi version 1.45 (Abramson 2006) programs.

Possible conflict of interest - All authors, with exception of Maria Cristina Ferreira Lemos, are employed by Bio-Manguinhos/Fiocruz, a state-owned Brazilian vaccine producer.

RESULTS

The field work for this study began in January 2006 and concluded in October of the same year. Codes were disclosed after completion of laboratory tests. Of 1,000 randomized children, four in the GSK group and nine in the BM group did not complete all study procedures due to the following: study withdrawal (4), change of address (3), adverse events (3), hydrocephaly diagnosed after randomization (1) and operational errors (2). There was a protocol violation in 30 children. The proportion of children with complete protocols was similar between the comparison groups (95.6%-98.4%). Adverse events were correctly recorded by parents (or guardians) in 92% of the specified time points and, in the case of fever, the event was correctly recorded in about two-thirds of the cases. Analysis of immunogenicity and safety in the total cohort and of adherence to protocol provided similar results.

Immunization allocation groups were homogeneous in their distribution by sex, age, birth weight and weight at the time of recruitment (Table I).

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The time interval between dose administration and blood collection was the same between the experimental groups.

Pre-vaccination levels of antibodies to Hib, diphtheria, tetanus and pertussis were also similar among the groups (Tables II, ^III ).

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Hib - All children were seroprotected against Hib after the third dose of vaccine in the BM group (3 lots) as well as in the GSK group among those study participants who adhered to the protocol (Table II). From 95-98.4% of the participants demonstrated high Hib titers (>1 µg/mL), indicating long-lasting immunity. The 95% confidence intervals of differences in seroprotection rates across DTP-Hib/BM lots were between 2.5% and -1.7%. GMTs were high in all groups and 95% confidence intervals of the ratio of pairs between the DTP/Hib-BM lots were within 0.74-1.21.

Confidence limits of differences in seroprotection rates and ratios of GMT provided evidence to reject the null hypothesis of relevant differences in the immunogenicity of the vaccines. With the intention-to-treat approach, seroprotection rates ranged from 98.4%-99.2% across comparison groups.

The ratio of GMTs for DTP/Hib-BM (pooled results of three lots) and DTP/Hib-GSK after the second dose was 1.11 (95% CI: 0.90:1.35) and after the third dose the ratio was 0.88 (95% CI: 0.74:1.04). The fold increase in titers to Hib after the third dose in comparison to pre-vaccination titers ranged from 19.4-25.9.

The intensity of the immunological response as represented by reverse cumulative distribution of antibodies was similar across the groups.

Tetanus, diphtheria and pertussis - Immunogenicity against the diphtheria, tetanus and pertussis vaccine components was similar across the three lots of DTP/Hib-BM. These results were pooled and compared to those from the DTP/Hib-GSK vaccine (^{Table III} ). After the third dose, more than 99% of infants were seroprotected against all three antigens. Differences in the proportions and GMT ratios were all above the non-inferiority limit. The increase in antibody levels of all antigens following the third dose was also similar for both vaccines.

Reactogenicity - The most frequent adverse events reported were local pain, irritability and an axillary temperature >37.5°C (Table IV). The proportion of children with a high fever (> 39ºC) did not exceed 1.3% in any experimental group or at any vaccine dose. There was no relevant or statistically significant difference (p < 0.05) between the vaccines. In general, solicited adverse events were most common after the first dose and fever was also more frequent and occurred immediately following the first dose (Figure). There were no statistically significant differences between the vaccines when examining the frequency of more severe, objective adverse events: fever > 39ºC, erythema and edema >20 mm.

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Two cases of hypotonic-hyporesponsive episodes (HHE) were reported during the study. One of these cases was confirmed (following the first dose of DTP/Hib-GSK) and one was unconfirmed (following the second dose of DTP/Hib-BM). Both cases underwent complete remission within a few hours. Both children appeared normal in subsequent examinations by a pediatrician and a neurologist.

There were 10 cases of serious adverse events (hospitalizations), all of which were unrelated to administration of the vaccine: bronchiolitis (6), bronchitis (1), idiopatic thrombocytopenic purpura (ITP) (1), dehydration (1) and congenital hydrocephaly which was diagnosed after enrollment in the study (1). No deaths or sequelae were observed, with the exception of the one case of hydrocephaly. There were no significant differences between vaccines with respect to adverse events. The case of ITP occurred in a child with a history of a res-piratory infection the week prior to vaccination, which was 31 days after the first dose of DTP/Hib-BM, 85 and 55 days, respectively, after the first and second doses of hepatitis B vaccine, and around 2 h administration of the meningococcus C vaccine. Since there was suspicion of an underlying disease, after consulting the Independent Data Monitoring Committee, the infant was excluded from the study and was followed up by pediatrician and a hematologist. The ITP resolved spontaneously, without treatment. Afterwards, the infant received a whole-cell DTP/Hib vaccine and the other vaccinations from the regular schedule, including measles, mumps and rubella vaccine with the exception of the hepatitis B vaccine.

Other unsolicited adverse events included common diseases of childhood such as upper respiratory infections, gastroenteritis and bronchitis, and all cases resulted in a good outcome after ambulatory care.

DISCUSSION

Haemophilus influenzae type b vaccine produced by BM has demonstrated high immunogenicity with consistency across lots and with different analytical strategies (intention-to-treat and per protocol). The three lots of Hib vaccine tested were similar ("non-inferior") to the reference vaccine with respect to the proportion of seroprotected infants (titers >0.15 µg/mL), as well as with respect to the intensity of immunological response (GMT) after the third dose of vaccine. The proportion of infants seroprotected after the second dose was also high and similar between both vaccines. Immunogenicity was comparable to a previous study with the same reference vaccine, in which 98% and 100% of infants demonstrated anti-PRP antibody titers >0.15 µg/mL, and GMTs were 4.32 mUI/mL and 9.34 mUI/mL after the second and third doses, respectively (Clemens et al. 2003). The proportion of more intense and possibly long-lasting responses (titers >1 g) was also high for both vaccines, which was also comparable to the previous study. In both groups the average increase in antibody levels indicated that these vaccines are immunogenic even in the presence of high levels of maternal antibodies. Immunogenicity of the diphtheria, tetanus and pertussis components was excellent with both vaccines, and the response to the diphtheria component was superior to that reported in the study by Clemens et al. (2003), possibly accounted for by the concomitant administration of a meningococcus vaccine conjugated to CRM₁₉₇ (MacLennan et al. 2000).

Data analyses emphasized the Hib component of the combined tetravalent DTP/Hib, which was the chief objective of the study. There were no significant differences between vaccine lots with respect to the proportion of seroprotection provided against Hib. Ratios of GMT of lots compared in a two-by-two fashion have shown results within the previously established limits of 0.5-2. Proportions of infants with high responses to the vaccine (>1 g/mL) have also indicated that the Hib-BM lots were equivalent. These results provided empirical evidence of consistency between lot productions, which had also been verified through quality control protocols. Lot consistency authorized pooling of the study results in order to compare the experimental vaccine to the reference vaccine.

For the other antigens (diphtheria, tetanus and pertussis) both the BM and GSK groups have shown seroprotection and geometric mean titer ratios compatible with a conclusion of non-inferiority for the Hib component manufactured by BM. The study design did not permit assessment of the contribution of natural infection to seropositivity, but the reduced incidence of target diseases makes seroprotection secondary to natural infection highly unlikely, as these diseases are under control in Brazil and only a few cases have been reported (MS 2005). The high level of antibodies to Hib in this study permit to foresee long term immunity, but the need for booster doses should be continuously evaluated and decided according to epidemiological data of Hib disease in all age groups.

Regarding long term immunity for diphtheria and tetanus, there should be no problem as long as two additional doses of DTP are given after the three initial DTP/Hib doses and diphtheria and tetanus vaccine, adult type boosters are given each 10 years, for all life. This should avoid waning of immunity and greater risk of disease, as has been determined for diphtheria in Brazil (Pimenta et al. 2006). For pertussis, after three doses of DTP/Hib and two doses of DTP, if available and used as a booster, tetanus, diphtheria and pertussis vaccine, adult type should permit better control of disease at all ages (Edwards & Decker 2008).

As expected, reactogenicity was also similar between vaccines, since the whole-cell pertussis component, which is generally considered the most reactogenic component, was the same in both comparison groups. The large variation in frequencies of adverse events across several studies has been attributed to vaccine peculiarities, but may also reflect other factors such as different vaccination schedules, intensity and duration of ascertainment, type of surveillance (active or passive), greater sensitivity of the surveillance system due to the introduction of a new vaccine, and different definitions or evaluation methods for adverse events (Chen et al. 2004).

In fact, in the study that permitted the introduction of a whole-cell DTP/Hib vaccine in the United States (Black et al. 1993, Centers for Disease Control 1993), the period of observation for adverse events was 24 h, and the information was obtained over the telephone and was recorded as "perceived fever". Moreover, no information was reported about the definition of fever or the site and method of measurement. In an active surveillance study of 20,925 infants from Rio de Janeiro who received the whole-cell DTP/Hib vaccine, information regarding adverse events was obtained via visits or phone calls and was based on information from parents (or guardians) who did not receive thermometers or training for measurement, and the period of observation was 48 h after vaccination (Martins et al. 2007).

In the present study, the detailed observation and recording of adverse events was unprecedented, especially in the case of temperature measurement. Despite detailed instructions and training of parents (or guardians), some data may carry a degree of imprecision, but these variations are expected to be similar across comparison groups. The frequency of adverse events, including fever, showed a decreasing trend from the first to the third dose. Since there was no placebo group, it is not possible to predict the contributions of intercurrent illnesses to the variation in adverse events. In the study by Black et al. (1993), the frequency of fever was similar after each of the three doses (38%, 39.7% and 40%, respectively) and in the active surveillance study of Rio de Janeiro the frequency was 35.4% after the three doses altogether.

In the present study, the high frequency of pain at injection site may be explained by the sensitivity of the definition used ("it hurts when the location of injection is touched by hand"). False positives would be more likely than false negatives given this statement, and a number of actual events may not be clinically significant.

Reactogenicity was evaluated for the infants with events recorded at all pre-established time points and also for those infants with adverse events detected at any time during the study. In both kinds of analyses the vaccine under study demonstrated a reactogenicity profile similar to that of the reference vaccine.

The number of major adverse events that occurred during the study was within the expected number in a 1,000-subject cohort of infants with 3,000 total doses of vaccine. Two cases of HHE made up a rate of 1/1,500 vaccinations. This incidence is comparable to the HHE rates in previous studies of active follow-up after three doses in the first year of life: 1/1,400 doses of the DTP vaccine (Cody et al. 1981) and 1/1,500 doses of the DTP/Hib vaccine as reported, in the Brazilian active surveillance study (Martins et al. 2007).

The causal relationship observed in this project between serious adverse events and the DTP/Hib vaccination was considered to be unlikely after careful investigation. The only established causal association of ITP to vaccines has been shown with measles vaccines and measles-containing vaccines (Farrington et al. 1995, Jonville-Béra et al. 1996, Miller et al. 2001, Black et al. 2003, Jadavji et al. 2003, Jefferson et al. 2004, France et al. 2008), whereas for the hepatitis B vaccine there are only indications of possible causality (Maezono & Escobar 2000, Nuevo et al. 2004, Wang et al. 2006). There is no indication that meningococcal conjugate vaccines are causally associated to ITP (Andrews et al. 2007) and the occurrence of ITP a few hours after administration of the vaccine makes the association unlikely. Sporadic cases of ITP have been temporally associated to the DTP or DTP/Hib vaccine (Jadavji et al. 2003, Wang et al. 2006) but have not been considered as evidence of causal association (Chandran et al. 2008, Edwards & Decker 2008). In our case, the most probable causes of ITP appeared to be a preceding respiratory infection and hepatitis B vaccination.

Hydrocephaly and other serious events which led to hospitalization for greater than 12 h have been reported in infants regardless of vaccination.

The Brazilian DTP/Hib vaccine, with local production of all of its components, demonstrated immunogenicity and reactogenicity profiles similar to those of the DTP/Hib vaccine with the Hib component produced using purified materials supplied by GSK. The data for this study was obtained with strict methodological procedures in conditions similar to those expected in all health care centers and supports the use of the vaccine in routine immunizations.

ACKNOWLEDGEMENTS

To Independent Data Monitoring Committee: José Cássio de Moraes, MD, PhD, Departamento de Medicina Social da Faculdade de Ciências Médicas da Santa Casa de São Paulo, Helena Keico Sato, MD, PhD, Divisão de Imunização, Secretaria de Saúde de São Paulo and José Geraldo Leite Ribeiro, MD, MSc, Faculdade de Ciências Médicas de Minas Gerais; to Camilla Bayer and Alessandro Fonseca de Souza, LATIM/Bio-Manguinhos-Fiocruz, Instituto Fernandes Figueira-Fiocruz, Hospital Jesus, Secretaria de Saúde, Rio de Janeiro, the five Health Centers participating in the study, District Health Councils, mothers and guardians, for their cooperation and good will, to other collaborators inside and outside of Bio-Manguinhos-Fiocruz and all partners.

Received 26 June 2008

Accepted 29 September 2008

Financial support: FINEP, Ministério da Ciência e Tecnologia, Bio-Manguinhos-Fiocruz

Andrews N, Stowe J, Miller E, Taylor B 2007. Post-licensure safety of the meningococcal group C conjugate vaccine. Hum Vaccin 3: 59-63.
Black C, Kaye JA, Jick H 2003. MMR vaccine and idiopathic thrombocytopenic purpura. Br J Clin Pharmacol 55: 107-111.
Black SB, Shinefield HR, Ray P, Lewis EM, Fireman B, Hiatt R 1993. Safety of combined oligosaccharide conjugate Haemophilus influenzae type b (HbOC) and whole-cell diphtheria-tetanus-toxoids-pertussis vaccine in infancy. Pediatr Infect Dis J 12: 981-985.
Centers for Disease Control 1993. Recommendations for use of Haemophilus b conjugate vaccines and a combined diphtheria, tetanus, pertussis and Haemophilus b vaccine. Morb Mortal Wkly Rep 42: No. RR-13, 1-6.
Chandran A, Watt JP, Santosham M 2008. Haemophilus influenzae vaccines. In S Plotkin, W Orenstein, P Offit (eds.), Vaccines, 5th ed., Saunders, China, p. 157-176.
Chen RT, Davis RL, Sheedy KM 2004. Safety of immunizations. In SA Plotkin, WA Orenstein (eds.) Vaccines, 4th ed., Saunders, Philadelphia, p. 1557-1581.
Clemens SC, Azevedo T, Homma A 2003. Feasibility study of the immunogenicity and safety of a novel DTPw/Hib (PRP-T) Brazilian combination compared to a licensed vaccine in healthy children at 2, 4 and 6 months of age. Rev Soc Bras Med Trop 36: 321-330.
Cody CL, Baraff LJ, Cherry JD, Marcy SM, Manclark CR 1981. Nature and rates of adverse reactions associated with DTP and DT immunizations in infants and children. Pediatrics 68: 650-660.
Decker MD, Edwards KM, Bogaerts HH 2008. Combination vaccines. In S Plotkin, W Orenstein, P Offit (eds.), Vaccines, 5th ed, Saunders, China, p. 1069-1101.
Edwards KM, Decker MD 2008. Pertussis. In S Plotkin, W Orenstein, P Offit (eds.), Vaccines, 5th ed., Saunders, China, p. 467-517.
Farrington P, Pugh S, Colville A, Flower A, Nash J, Morgan-Capner P, Rush M, Miller E 1995. A new method for active surveillance of adverse events from diphtheria/tetanus/pertussis and measles/mumps/rubella vaccines. Lancet 345: 567-569.
France FK, Glanz J, Xu S, Hambidge S, Yamasaki K, Black SB, Marcy M, Mullooly JP, Jackson LA, Nordin J, Belongia FA, Hohman K, Chen RT, Davis R 2008. Risk of immune thrombocytopenic purpura after measles-mumps-rubella immunization in children. Pediatrics 121: 625-626.
Homma A, Leal MLF, Moreira MS, Pina FO, Baetas RBG, Pizarro APB, Couto AR 2005. Desenvolvimento e produção de vacinas no Instituto de Tecnologia em Imunobiológicos (Bio-Manguinhos) da Fiocruz. In PM Buss, JG Temporão, JR Carvalheiro (eds.), Vacinas, soros e imunizações no Brasil, Editora Fiocruz, Rio de Janeiro, p. 349-378.
Jadavji T, Scheifele D, Halperin S 2003. Thrombocytopenia after immunization of Canadian children, 1992 to 2001. Pediatr Infect Dis J 22: 119-122.
Jefferson T, Price D, Demicheli V, Bianco E 2004. Unintended events following immunization with MMR: a systematic review. Vaccine 22: 4135-4136.
Johnson NG, Ruggeberg JU, Balfour GF, Chen Lee Y, Liddy H, Irving D, Sheldon J, SlackMPE, Pollard AJ, Heath PT 2006. Haemo-philus influenzae type b reemergence after combination immunization. Emerg Infect Dis 12: 937-941.
Jonville-Béra AP, Autret E, Galy-Eyraud C, Hessel L 1996. Thrombocytopenic purpura after measles, mumps and rubella vaccination: a retrospective survey by the French regional pharmacovigilance centres and Pasteur-Mérieux serums et vaccines. Pediatr Infect Dis J 15: 44-48.
MacLennan JM, Shackley F, Heath PT, Deeks JJ, Flamank C, Herbert M, Griffiths H, Hatzmann E, Goilav C, Moxon ER 2000. Safety, immunogenicity and induction of immunologic memory by a serogroup C meningococcal conjugate vaccine in infants. JAMA 283: 2795-2801.
Maezono R, Escobar AMU. Púrpura trombocitopênica após vacina contra hepatite B 2000. J Pediatr (Rio J) 76: 395-398.
Martins RM, Camacho LAB, Lemos MCF, Noronha TG, Carvalho MHC, Greffe N, Silva MM, Périssé AR, Maia MLS, Homma A 2007. Incidence of hypotonic-hyporesponsive episodes associated to the combined DTP/Hib vaccine used in Brazilian National Immunizations Program. J Pediatr (Rio J) 83: 523-528.
Miller E, Waight P, Farrington CP, Andrews N, Stowe J, Taylor B 2001. Idiopathic thrombocytopenic purpura and MMR vaccine. Arch Dis Child 84: 227-229.
MS - Ministério da Saúde, Secretaria de Vigilância em Saúde 2005. Guia de Vigilância Epidemiológica, 6ª ed., Brasília, Ministério da Saúde, 816 pp.
Nuevo H, Nascimento-Carvalho CMC, Athayde-Oliveira C, Lyra I 2004. Thrombocytopenic purpura after hepatitis B vaccine: case report and review of literature. Pediatr Infect Dis J 23: 183-184.
Pimenta FP, Damasco PV, Cerbino Neto J, Lopes GS, Hirata Jr R, Milagres LG, Mattos-Guaraldi AL 2006. Diphtheria-neutralizing antibody levels in healthy adults from Rio de Janeiro, Brazil. Mem Inst Oswaldo Cruz 101: 459-462.
Sato Y, Sato H 1999. Development of acellular pertussis vaccines. Biologicals 27: 61-69.
Wang JD, Huang FL, Chin PY, Wang TM, Chi CS, Chang TK 2006. Acute immune thrombocytopenic purpura in infants: associated factors, clinical features, treatment and long term outcome. Eur J Haematol 77: 334-337.

+

Corresponding author:

rmenezes@bio.fiocruz.br

Publication Dates

Publication in this collection
02 Dec 2008
Date of issue
Nov 2008

History

Accepted
29 Sept 2008
Received
26 June 2008

This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

[1] Andrews N, Stowe J, Miller E, Taylor B 2007. Post-licensure safety of the meningococcal group C conjugate vaccine. Hum Vaccin 3: 59-63.

[2] Black C, Kaye JA, Jick H 2003. MMR vaccine and idiopathic thrombocytopenic purpura. Br J Clin Pharmacol 55: 107-111.

[3] Black SB, Shinefield HR, Ray P, Lewis EM, Fireman B, Hiatt R 1993. Safety of combined oligosaccharide conjugate Haemophilus influenzae type b (HbOC) and whole-cell diphtheria-tetanus-toxoids-pertussis vaccine in infancy. Pediatr Infect Dis J 12: 981-985.

[4] Centers for Disease Control 1993. Recommendations for use of Haemophilus b conjugate vaccines and a combined diphtheria, tetanus, pertussis and Haemophilus b vaccine. Morb Mortal Wkly Rep 42: No. RR-13, 1-6.

[5] Chandran A, Watt JP, Santosham M 2008. Haemophilus influenzae vaccines. In S Plotkin, W Orenstein, P Offit (eds.), Vaccines, 5th ed., Saunders, China, p. 157-176.

[6] Chen RT, Davis RL, Sheedy KM 2004. Safety of immunizations. In SA Plotkin, WA Orenstein (eds.) Vaccines, 4th ed., Saunders, Philadelphia, p. 1557-1581.

[7] Clemens SC, Azevedo T, Homma A 2003. Feasibility study of the immunogenicity and safety of a novel DTPw/Hib (PRP-T) Brazilian combination compared to a licensed vaccine in healthy children at 2, 4 and 6 months of age. Rev Soc Bras Med Trop 36: 321-330.

[8] Cody CL, Baraff LJ, Cherry JD, Marcy SM, Manclark CR 1981. Nature and rates of adverse reactions associated with DTP and DT immunizations in infants and children. Pediatrics 68: 650-660.

[9] Decker MD, Edwards KM, Bogaerts HH 2008. Combination vaccines. In S Plotkin, W Orenstein, P Offit (eds.), Vaccines, 5th ed, Saunders, China, p. 1069-1101.

[10] Edwards KM, Decker MD 2008. Pertussis. In S Plotkin, W Orenstein, P Offit (eds.), Vaccines, 5th ed., Saunders, China, p. 467-517.

[11] Farrington P, Pugh S, Colville A, Flower A, Nash J, Morgan-Capner P, Rush M, Miller E 1995. A new method for active surveillance of adverse events from diphtheria/tetanus/pertussis and measles/mumps/rubella vaccines. Lancet 345: 567-569.

[12] France FK, Glanz J, Xu S, Hambidge S, Yamasaki K, Black SB, Marcy M, Mullooly JP, Jackson LA, Nordin J, Belongia FA, Hohman K, Chen RT, Davis R 2008. Risk of immune thrombocytopenic purpura after measles-mumps-rubella immunization in children. Pediatrics 121: 625-626.

[13] Homma A, Leal MLF, Moreira MS, Pina FO, Baetas RBG, Pizarro APB, Couto AR 2005. Desenvolvimento e produção de vacinas no Instituto de Tecnologia em Imunobiológicos (Bio-Manguinhos) da Fiocruz. In PM Buss, JG Temporão, JR Carvalheiro (eds.), Vacinas, soros e imunizações no Brasil, Editora Fiocruz, Rio de Janeiro, p. 349-378.

[14] Jadavji T, Scheifele D, Halperin S 2003. Thrombocytopenia after immunization of Canadian children, 1992 to 2001. Pediatr Infect Dis J 22: 119-122.

[15] Jefferson T, Price D, Demicheli V, Bianco E 2004. Unintended events following immunization with MMR: a systematic review. Vaccine 22: 4135-4136.

[16] Johnson NG, Ruggeberg JU, Balfour GF, Chen Lee Y, Liddy H, Irving D, Sheldon J, SlackMPE, Pollard AJ, Heath PT 2006. Haemo-philus influenzae type b reemergence after combination immunization. Emerg Infect Dis 12: 937-941.

[17] Jonville-Béra AP, Autret E, Galy-Eyraud C, Hessel L 1996. Thrombocytopenic purpura after measles, mumps and rubella vaccination: a retrospective survey by the French regional pharmacovigilance centres and Pasteur-Mérieux serums et vaccines. Pediatr Infect Dis J 15: 44-48.

[18] MacLennan JM, Shackley F, Heath PT, Deeks JJ, Flamank C, Herbert M, Griffiths H, Hatzmann E, Goilav C, Moxon ER 2000. Safety, immunogenicity and induction of immunologic memory by a serogroup C meningococcal conjugate vaccine in infants. JAMA 283: 2795-2801.

[19] Maezono R, Escobar AMU. Púrpura trombocitopênica após vacina contra hepatite B 2000. J Pediatr (Rio J) 76: 395-398.

[20] Martins RM, Camacho LAB, Lemos MCF, Noronha TG, Carvalho MHC, Greffe N, Silva MM, Périssé AR, Maia MLS, Homma A 2007. Incidence of hypotonic-hyporesponsive episodes associated to the combined DTP/Hib vaccine used in Brazilian National Immunizations Program. J Pediatr (Rio J) 83: 523-528.

[21] Miller E, Waight P, Farrington CP, Andrews N, Stowe J, Taylor B 2001. Idiopathic thrombocytopenic purpura and MMR vaccine. Arch Dis Child 84: 227-229.

[22] MS - Ministério da Saúde, Secretaria de Vigilância em Saúde 2005. Guia de Vigilância Epidemiológica, 6ª ed., Brasília, Ministério da Saúde, 816 pp.

[23] Nuevo H, Nascimento-Carvalho CMC, Athayde-Oliveira C, Lyra I 2004. Thrombocytopenic purpura after hepatitis B vaccine: case report and review of literature. Pediatr Infect Dis J 23: 183-184.

[24] Pimenta FP, Damasco PV, Cerbino Neto J, Lopes GS, Hirata Jr R, Milagres LG, Mattos-Guaraldi AL 2006. Diphtheria-neutralizing antibody levels in healthy adults from Rio de Janeiro, Brazil. Mem Inst Oswaldo Cruz 101: 459-462.

[25] Sato Y, Sato H 1999. Development of acellular pertussis vaccines. Biologicals 27: 61-69.

[26] Wang JD, Huang FL, Chin PY, Wang TM, Chi CS, Chang TK 2006. Acute immune thrombocytopenic purpura in infants: associated factors, clinical features, treatment and long term outcome. Eur J Haematol 77: 334-337.