Determinants of delayed or incomplete diphtheria-tetanus-pertussis vaccination in parallel urban and rural birth cohorts of 30,956 infants in Tanzania

BMC Infectious Diseases, Volume 19, No. 1, Year 2019

Interpretation

Background: Delayed vaccination increases the time infants are at risk for acquiring vaccine-preventable diseases. Factors associated with incomplete vaccination are relatively well characterized in resource-limited settings; however, few studies have assessed immunization timeliness. Methods: We conducted a prospective cohort study examining Diphtheria-Tetanus-Pertussis (DTP) vaccination timing among newborns enrolled in a Neonatal Vitamin A supplementation trial (NEOVITA) conducted in urban Dar es Salaam (n = 11,189) and rural Morogoro Region (n = 19,767), Tanzania. We used log-binomial models to assess the relationship of demographic, socioeconomic, healthcare access, and birth characteristics with late or incomplete DTP1 and DTP3 immunization. Results: The proportion of infants with either delayed or incomplete vaccination was similar in Dar es Salaam (DTP1 11.5% and DTP3 16.0%) and Morogoro (DTP1 9.2% and DTP3 17.3%); however, the determinants of delayed or incomplete vaccination as well as their magnitude of association differed by setting. Both maternal and paternal education were more strongly associated with vaccination status in rural Morogoro region as compared to Dar es Salaam (p-values for heterogeneity < 0.05). Infants in Morogoro who had fathers and mothers with no education had 36% (95% CI: 22-52%) and 22% (95% CI: 10-34%) increased risk of delayed or incomplete DTP3 vaccination as compared to those with primary school education, respectively. In Dar es Salaam, mothers who attended their first antenatal care (ANC) visit in the 3rd trimester had 1.55 (95% CI: 1.36-1.78) times the risk of delayed or not received vaccination as compared to those with a 2nd trimester booking, while there was no relationship in Morogoro. In rural Morogoro, infants born at home had 17% (95% CI: 8-27%) increased risk for delayed or no receipt of DTP3 vaccination. In both settings, younger maternal age and poorer households were at increased risk for delayed or incomplete vaccination. Conclusion: We found some risk factors for delayed and incomplete vaccination were shared between urban and rural Tanzania; however, we found several context-specific risk factors as well as determinants that differed in their magnitude of risk between contexts. Immunization programs should be tailored to address context-specific barriers and enablers to improve timely and complete vaccination. This study utilized data from a randomized, double-blind controlled trial of Neonatal Vitamin A supplementation (NEOVITA). This trial enrolled 31,999 children in urban Dar es Salaam and rural Morogoro, Tanzania from August 2010 to March 2014 (ACTRN12610000636055). Briefly, newborns born at home or at a health facility were randomized to receive a mega-dose of vitamin A (50,000 IU) or placebo on the day of birth or within 3 days; trial recruitment and detailed data collection procedures have been presented elsewhere [7]. Newborns whose mothers were younger than 15 years old or older than 49 years were excluded from participation in the trial. In urban Dar es Salaam, 11,895 participants were enrolled at antenatal clinics and in labor wards of public health facilities in Kinondoni, Ilala, and Temeke districts. In Morogoro Region, 20,104 participants were recruited within a rural Health and Demographic Surveillance System (HDSS) that covers approximately 2400 km2 and allowed for enrollment of both health facility and home births in Kilombero, Ulanga and Kilosa districts. Newborns were eligible for randomization if they were able to feed orally, were born within the past three days, were not previously enrolled in other clinical trials, intended to stay in the study area for at least six months post-delivery, and the parents provided written informed consent to participate. At the baseline visit, trained study staff administered a baseline questionnaire to mothers in order to collect information on demographic, socioeconomic, and health factors. Trained fieldworkers visited the infants 1 and 3 days after enrollment, as well as 1, 3, 6, and 12 months after birth. During these visits, fieldworkers assessed the morbidity and mortality of the infants and ascertained information about the infants’ recent nutrition intake and any immunizations the infant received since the last visit [7, 8]. All newborns enrolled in the trial were given a child health card at the time of randomization. DTP vaccination status was determined by field workers who reviewed the child health card recorded dates of vaccination at each study visit (1 day, 3 days, and then 1, 3, 6, and 12 months). Child health cards were not available at less than 0.1% of all study visits and in these few cases the date of vaccination was reported by the mother or infant caregiver. In this study, we analyzed DTP1 and DTP3 vaccination timing. Tanzania Mainland recommended DTP1 vaccination at 4 weeks of age; however, during the trial in 2012, the pentavalent DTP + Haemophilus influenza type B (Hib) + Hepatitis B (HepB) vaccine was introduced and the recommended age at vaccination was increased to 6 weeks [9]. Tanzania recommended DTP3 at 14 weeks of age throughout the study. There is no universal definition of delayed vaccination for DTP vaccine, although most, including the Pan American Health Organization, define late vaccination as one month or more after the recommended age of vaccination [10]. At the time of the study, LMICs were advised to set their recommended age at DTP1 vaccination at 6 weeks (4 weeks–2 months) [11, 12]. As a result, in the primary analysis we define delayed DTP1 vaccination as receipt > 90 days of age based on the upper recommended age for DTP1 (2 months or 60 days) plus 30 days late. In a sensitivity analysis, we define delayed vaccination as > 72 days based on the Tanzanian recommended age for the first pentavalent vaccine dose (6 weeks or 42 days) plus 30 days late. Due to the staggered roll-out of the pentavalent vaccine program during the study, we were not able to determine if infants were due for their first DTP vaccination at 4 weeks or 6 weeks and therefore we only present the conservative definition of 72 days late in the sensitivity analysis. Infants who were lost to follow up, died or were vaccinated before 15 days were excluded from the DTP1 analysis. The standard recommended age range for DTP3 vaccination in LMICs was 14 weeks [12 weeks–6 months]) [11, 12]. As a result, we defined delayed DTP3 vaccination as receipt > 210 days (7 months) of age in the main analysis. In a sensitivity analysis, we defined delayed DTP3 vaccination as > 128 days of age based on the Tanzanian recommended age of 14 weeks (98 days) plus 30 days late. Infants who were lost to follow up, died or were vaccinated before 60 days were excluded from the DTP3 analysis. Univariate and multivariate relative risks of delayed or incomplete DTP1 and DTP3 vaccination (> 90 days and > 210 days, respectively) were calculated using log-binomial models stratified by Dar es Salaam and Morogoro region [13]. We also present sensitivity analyses using delayed vaccination definitions of > 72 days and > 128 days for DTP1 and DTP3, respectively. Log-binomial models did not converge in a few instances and in these cases log-Poisson models, which provide consistent but not fully efficient estimates of the relative risk and its confidence intervals, were used [14]. Preterm birth was defined as delivery at < 37 weeks gestation as assessed by maternal report of last menstrual period. Small-for-gestational-age (SGA) was defined, with the use of Oken standards, as birth weight < 10th percentile for gestational age and sex [15]. A wealth index was generated based on household ownership of assets, and households were categorized into wealth quintiles stratified by Dar es Salaam and Morogoro residence [16]. Due to collinearity, low birth weight was modeled separately from preterm birth and small-for-gestational age. P-values for trend in categorical analyses were calculated by treating the median value of each category as a continuous variable. The log-rank test was used to assess the statistical significance of potential effect modification of predictors of interest by study site (Dar es Salaam versus Morogoro). Missing data were retained with use of the missing indicator method. All P values were 2-sided with a P < 0.05 considered statistically significant. All of the analyses for this study were conducted using R version 3.3.1.

AI Digest

Study Justification:

This study aimed to investigate the factors associated with delayed or incomplete diphtheria-tetanus-pertussis (DTP) vaccination in Tanzania. Understanding these factors is crucial for improving immunization programs and reducing the risk of vaccine-preventable diseases in infants.

Study Highlights:

– The study examined DTP vaccination timing among 30,956 infants enrolled in a Neonatal Vitamin A supplementation trial in urban Dar es Salaam and rural Morogoro, Tanzania.
– The proportion of infants with delayed or incomplete vaccination was similar in both settings.
– The determinants of delayed or incomplete vaccination differed between urban and rural areas.
– Maternal and paternal education were more strongly associated with vaccination status in rural Morogoro.
– In Dar es Salaam, mothers who attended their first antenatal care visit in the 3rd trimester had a higher risk of delayed or no vaccination.
– Infants born at home in Morogoro had an increased risk of delayed or no vaccination.
– Younger maternal age and poorer households were associated with delayed or incomplete vaccination in both settings.

Recommendations for Lay Reader and Policy Maker:

– Immunization programs should be tailored to address context-specific barriers and enablers to improve timely and complete vaccination.
– Strategies should be developed to improve education levels among parents, especially in rural areas.
– Efforts should be made to encourage early antenatal care visits to ensure timely vaccination.
– Interventions should be implemented to increase vaccination coverage among infants born at home.
– Additional support should be provided to younger mothers and families from poorer households to ensure timely and complete vaccination.

Key Role Players:

– Ministry of Health: Responsible for implementing and coordinating immunization programs.
– Health Facilities: Provide vaccination services and ensure timely delivery of vaccines.
– Community Health Workers: Educate and mobilize communities to promote vaccination.
– Non-Governmental Organizations: Support immunization programs through advocacy, funding, and implementation of interventions.
– Education Authorities: Promote education initiatives to improve literacy rates and knowledge about vaccination.

Cost Items for Planning Recommendations:

– Training and Capacity Building: Budget for training healthcare workers and community health workers on immunization strategies and communication skills.
– Vaccine Supply and Distribution: Allocate funds for the procurement, storage, and transportation of vaccines to ensure availability in both urban and rural areas.
– Outreach and Awareness Campaigns: Set aside funds for community engagement activities, including awareness campaigns, community meetings, and educational materials.
– Monitoring and Evaluation: Allocate resources for monitoring and evaluating the implementation and impact of immunization programs.
– Research and Data Collection: Budget for conducting further research and data collection to inform evidence-based decision-making in immunization programs.

Strength of Evidence

The strength of evidence for this abstract is 8 out of 10.
The evidence in the abstract is strong because it is based on a large prospective cohort study with a sample size of 30,956 infants in Tanzania. The study used log-binomial models to assess the relationship between various factors and delayed or incomplete DTP vaccination. The findings provide valuable insights into the determinants of vaccination timing in both urban and rural settings. To improve the evidence, the abstract could include more specific information about the methodology, such as the duration of the study, the data collection procedures, and the statistical analysis methods used. Additionally, it would be helpful to provide a summary of the key findings and their implications for immunization programs in Tanzania.

Abstract

Materials

https://efashare.b-cdn.net/materials/4f969839ade74b3c9fd9779a18903d64276306d97a5b754acf0fc9910439364f/12879_2019_3828_MOESM1_ESM.docx

Innovations

The study “Determinants of delayed or incomplete diphtheria-tetanus-pertussis vaccination in parallel urban and rural birth cohorts of 30,956 infants in Tanzania” focused on identifying factors associated with delayed or incomplete DTP vaccination in infants in Tanzania. The study found several determinants of delayed or incomplete vaccination, including maternal and paternal education, timing of the first antenatal care visit, place of birth, maternal age, and household wealth.

Based on this study, here are some potential innovations that could improve access to maternal health:

1. Education programs: Implementing educational programs for both mothers and fathers on the importance of timely vaccination and the benefits of maternal health care. This could help increase awareness and understanding of the importance of vaccination and encourage parents to prioritize their child’s immunization.

2. Antenatal care promotion: Promote early and regular attendance of antenatal care visits. This could be done through community outreach programs, providing incentives for early attendance, and improving the availability and accessibility of antenatal care services.

3. Mobile health (mHealth) interventions: Utilize mobile technology to send reminders and educational messages to pregnant women and new mothers about the importance of timely vaccination. This could help improve awareness and adherence to vaccination schedules.

4. Community-based vaccination programs: Establish community-based vaccination programs that bring immunization services closer to rural areas. This could involve mobile vaccination clinics or outreach teams that visit remote communities to provide vaccinations and maternal health services.

5. Socioeconomic support: Implement interventions to address socioeconomic barriers to vaccination, such as providing financial support for transportation to health facilities, reducing out-of-pocket costs for vaccinations, and improving access to healthcare services in low-income areas.

6. Health worker training: Provide training and support for healthcare workers to improve their knowledge and skills in maternal health and vaccination. This could include training on counseling techniques, communication skills, and the importance of timely vaccination.

These innovations have the potential to improve access to maternal health by addressing the specific determinants identified in the study and tailoring interventions to the context of urban and rural areas in Tanzania.

AI Innovations Description

The study mentioned focuses on the determinants of delayed or incomplete diphtheria-tetanus-pertussis (DTP) vaccination in urban and rural areas of Tanzania. The findings of the study highlight several factors that contribute to delayed or incomplete vaccination, including demographic, socioeconomic, healthcare access, and birth characteristics.

Based on the study’s results, here is a recommendation that can be developed into an innovation to improve access to maternal health:

1. Tailored Immunization Programs: The study found that there were context-specific risk factors and determinants that differed in their magnitude of risk between urban and rural settings. Therefore, it is recommended to develop immunization programs that are tailored to address the specific barriers and enablers in each setting. This could involve targeted interventions and strategies to improve access to vaccination services, such as mobile clinics or outreach programs in rural areas, and ensuring timely antenatal care visits in urban areas.

By implementing tailored immunization programs, healthcare providers can address the unique challenges faced by different communities and improve the timely and complete vaccination coverage for infants. This innovation can contribute to reducing the risk of vaccine-preventable diseases and improving maternal and child health outcomes.

AI Innovations Methodology

Based on the provided information, here are some potential recommendations to improve access to maternal health:

1. Strengthening Antenatal Care (ANC) Services: Focus on increasing the number of ANC visits and promoting early initiation of ANC, as this has been shown to be associated with timely and complete vaccination.

2. Community-Based Education and Awareness Programs: Implement community-based programs to educate and raise awareness among pregnant women and their families about the importance of maternal health and vaccination. This can be done through community health workers, local leaders, and mass media campaigns.

3. Mobile Health (mHealth) Interventions: Utilize mobile technology to provide information and reminders about maternal health services and vaccination schedules. This can include SMS reminders, mobile apps, and telemedicine consultations.

4. Improving Healthcare Access: Address barriers to healthcare access, such as distance to health facilities, transportation, and cost. This can be done by expanding the availability of health facilities, improving transportation infrastructure, and implementing financial support programs for maternal health services.

To simulate the impact of these recommendations on improving access to maternal health, a methodology could include the following steps:

1. Define the indicators: Determine the specific indicators that will be used to measure access to maternal health, such as the number of ANC visits, vaccination coverage rates, and timeliness of vaccination.

2. Collect baseline data: Gather data on the current status of access to maternal health services and vaccination in the target population. This can be done through surveys, interviews, and analysis of existing data sources.

3. Develop a simulation model: Create a simulation model that incorporates the various factors influencing access to maternal health, such as demographic characteristics, socioeconomic status, healthcare infrastructure, and the recommended recommendations. This model should be based on the available data and evidence.

4. Implement the recommendations: Introduce the recommended interventions and track their implementation over a specified period of time. This can include implementing ANC strengthening programs, community-based education initiatives, mHealth interventions, and improvements in healthcare access.

5. Simulate the impact: Use the simulation model to estimate the impact of the recommendations on access to maternal health. This can be done by comparing the indicators before and after the implementation of the interventions.

6. Evaluate the results: Analyze the simulation results to assess the effectiveness of the recommendations in improving access to maternal health. This can include comparing the indicators between the baseline and simulation scenarios, as well as conducting statistical analyses to determine the significance of the changes.

7. Refine and iterate: Based on the evaluation results, refine the recommendations and simulation model as needed. Iterate the process by implementing the refined recommendations and conducting further simulations to continuously improve access to maternal health.

It is important to note that the methodology described above is a general framework and the specific details may vary depending on the context and available resources.

Authors & Co-Authors

Statistics:

Citations: 5

Authors: 7

Identifiers:

DOI: 10.1186/s12879-019-3828-3

Research Areas:

Disability, Disparities, Food Security, Genetics and Genomics, Health System and Policy, Infectious Diseases, Maternal Access, Maternal and Child Health, Quality of Care, Sexual and Reproductive Health, Social Determinants

Study Countries:

Tanzania

Study Design:

Cohort Study, Grounded Theory, randomised-control-trial

Study Approach:

Quantitative