CompletedNot Applicable

Impact of Vaccines on Antimicrobial Microbial Resistance

Malawi13,200 participantsStarted 2021-03-15

Plain-language summary

Vaccination is a potentially critical component of efforts to arrest development and dissemination of antimicrobial resistance (AMR), though little is known about vaccination impact within low-income and middle-income countries. This study will evaluate the impact of vaccination on reducing carriage prevalence of resistant Streptococcus pneumoniae and extended spectrum beta-lactamase-producing Escherichia coli and Klebsiella species. We will leverage two large ongoing cluster-randomised vaccine evaluations in Malawi assessing; first, adding a booster dose to the 13-valent pneumococcal conjugate vaccine (PCV13) schedule, and second, introduction of the RTS,S/AS01 malaria vaccine. Six cross-sectional surveys will be implemented within primary healthcare centres (n=3000 users of outpatient facilities per survey) and their local communities (n=700 healthy children per survey): three surveys in Blantyre district (PCV13 component) and three surveys in Mangochi district (RTS,S/AS01 component). We will evaluate antibiotic prescription practices and AMR carriage in children ≤3 years. For the PCV13 component, surveys will be conducted 9, 18 and 33 months following a 3+0 to 2+1 schedule change. For the RTS,S/AS01 component, surveys will be conducted 32, 44 and 56 months post-RTS,S/AS01 introduction. Six health centres in each study component will be randomly selected for study inclusion. Between intervention arms, the primary outcome will be the difference in penicillin non-susceptibility prevalence among S. pneumoniae nasopharyngeal carriage isolates in healthy children. The study is powered to detect an absolute change of 13 percentage points (ie, 35% vs 22% penicillin non-susceptibility). This study has been approved by the Kamuzu University of Health Sciences (Ref: P01-21-3249), University College London (Ref: 18331/002) and University of Liverpool (Ref: 9908) Research Ethics Committees. Parental/caregiver verbal or written informed consent will be obtained prior to inclusion or recruitment in the health centre-based and community-based activities, respectively. Results will be disseminated via the Malawi Ministry of Health, WHO, peer-reviewed publications and conference presentations.

Who can participate

Age range5 Months – 3 Years

SexALL

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Inclusion Criteria: * Permanent residence in Blantyre (PCV cohort) or Mangochi (RTS,S/AS01 cohort) * Parent/legal guardian consent * Evidence of having received an initial 2 or 3 doses of the PCV13 vaccine (survey 1) or the full PCV13 schedule (surveys 2 and 3: Either 2+1 or 3+0 depending on cluster) or full initial (+/- booster) course of the RTS,S/SA01 vaccine (in Mangochi intervention cluster). Exclusion Criteria: * Current tuberculosis (TB) treatment * Terminal illness (Defined as a condition that cannot be cured and it is likely to lead to the individual's death) * Having received antibiotic treatment \<14 days before study enrolment * Hospitalisation for pneumonia \<14 days before study enrolment * Presence of gross respiratory tract pathology For the HC audits, we will request to review the health information from attendees that comply with the following characteristics: * \<3 years of age * HC attendance for investigation and/or treatment of ill health

What they're measuring

The antibiotic resistance profile of S. pneumoniae carriage isolates from children <3 years following a PCV13 schedule that extends protection (2+1 vs. 3+0) or the introduction of malaria vaccine (RTS,S/AS01)

Timeframe: less than 3 years

Trial details

NCT IDNCT06450379

SponsorMalawi Liverpool Wellcome Programme

Sponsor typeOTHER

Study typeOBSERVATIONAL

Primary completion2024-04-26