P T Heath1, R Booy2,
J McVernon3, J Bowen-Morris3,
H Griffiths3, M P E Slack4,
A C Moloney5, M E Ramsay6 and
E R Moxon3
1 Department of Child Health and St Georges
Vaccine Institute, St Georges Hospital Medical School, London, UK 2 Department of Child Health, Queen Mary College, University of
London, UK 3 Oxford Vaccine Group, John Radcliffe Hospital, Oxford, UK 4 PHLS Haemophilus Reference Unit, John Radcliffe Hospital, Oxford,
UK 5 Regional Pathology Laboratory, Waterford Regional Hospital,
Waterford, Republic of Ireland 6 Communicable Disease Surveillance Centre, Colindale, London, UK
Correspondence to:
Dr P T Heath, Department of Child Health and St Georges Vaccine Institute, St
Georges Hospital Medical School, Cranmer Terrace, London SW17 ORE, UK; pheath@sghms.ac.uk
Aims: To document the immunogenicity and persistence of
antibodyto polyribosyl-ribitol phosphate (PRP) as well as the
clinicalprotection against invasive Haemophilus influenzae
type b (Hib)disease in premature infants immunised at the routine
schedule.
Methods: Blood was obtained at 2, 5, 12, and 64 months of agefrom a cohort of prematurely born infants (32
weeks gestation).Anti-PRP antibody concentrations were compared with
those ofa control cohort of infants born at full term and vaccinatedat the same schedule. Hib vaccine failures occurring between
October 1992 and October 2000 were reported by paediatriciansthrough
an active, prospective, national survey in the UK andRepublic of
Ireland. The number of prematurely born childrenwith vaccine failure
was compared with the corresponding numberborn at term.
Results: Twenty seven prematurely born infants were followedto 5 years of age. Compared with term infants they had a significantlylower geometric mean concentration of anti-PRP antibody and/or
a significantly lower proportion above one or both of the conventionalprotective antibody concentrations (0.15 and 1.0 µg/ml)at all
ages. A total of 165 cases of invasive Hib disease wereidentified
over eight years of national surveillance. Eighteenwere premature
(<37 weeks); approximately 12 would be expected.The relative risk of
UK premature infants developing diseasecompared with term infants
was 1.5 (95% CI 0.9 to 2.6).
Conclusions: Premature infants develop lower antibody concentrationsthan term infants following Hib conjugate vaccination. Prematureinfants may also have an increased risk of clinical vaccine
failure, but interpretation is limited by the small number of
premature infants developing invasive Hib disease over eightyears of
national surveillance. Overall, vaccination with Hibconjugate
vaccines affords a high level of protection to prematurebabies.
Keywords: Haemophilus influenzae; vaccine; preterm; risk group
Abbreviations: DTP, diphtheria/tetanus/pertussis vaccine;
HbOC, PRP conjugated to mutant diphtheria toxoid (CRM197) vaccine; Hib,
Haemophilus influenzae type b; PRP, polyribosyl-ribitol phosphate; PRP-OMP,
PRP conjugated to outer membrane protein of Neisseria meningitidis
vaccine; PRP-T, PRP conjugated to tetanus toxoid vaccine; ROI, Republic of
Ireland; TVF, true vaccine failure
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MATERIAL CONTAINED, PRESENTED, OR PROVIDED HERE IS FOR GENERAL INFORMATION
PURPOSES ONLY AND IS NOT TO BE CONSTRUED AS REFLECTING THE KNOWLEDGE OR OPINIONS
OF THE PUBLISHER, AND IS NOT TO BE CONSTRUED OR INTENDED AS PROVIDING MEDICAL OR
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