The Pediatric Infectious Disease Journal
2003; 22(6):524-532
Vaccination of
day-care center attendees reduces carriage of Streptococcus pneumoniae
among their younger siblings
NOGA GIVON-LAVI, MMEDSC; DRORA FRASER, PhD; RON DAGAN, MD
Aim.
We conducted a study to determine whether
administration of a pneumococcal conjugate vaccine to toddlers attending
day-care centers (DCCs) could prevent acquisition of Streptococcus
pneumoniae of the vaccine serotypes (VT) by their younger
siblings.
In a double blind study, 262 DCC attendees
ages 12 to 35 months were randomized to receive a 9-valent pneumococcal
conjugate vaccine (PnCRM9; n = 132), or a control vaccine
(meningococcus C vaccine; n = 130). It was planned to
follow the groups for 2 years with monthly nasopharyngeal pneumococcal
cultures during the first follow-up year and every 2 months during the
second year. Forty-six younger siblings of the above described children,
age <18 months (23 siblings of
the PnCRM9 recipients and 23 of the controls), were also enrolled, and
nasopharyngeal cultures were obtained monthly until the children reached
the age of 18 months or started to attend DCC, if before the age of 18
months. Pneumococcal isolates were serotyped and tested for antibiotic
susceptibility.
Results.
Of the 3748 cultures obtained from the DCC
attendees, 2450 (65%) were positive for S. pneumoniae. Of
306 cultures obtained from the younger siblings, 151 (49%) were positive.
Among the PnCRM9 recipients, cultures were significantly less frequently
positive for the VT S. pneumoniae than among the controls
(13% vs. 21%, respectively; P< 0.001). The same pattern was seen in the younger
siblings of PnCRM9 recipients vs. the siblings of controls (21% vs. 34%,
respectively; P = 0.017). The reverse trend was seen for
non-VT strains in both the DCC attendees (44% vs. 34%, respectively;
P< 0.001) and
their younger siblings (19% vs. 13%, respectively; P =
0.15). There was a significant decrease in the carriage rate of
antibiotic-resistant S. pneumoniae in both the PnCRM9
recipients and their younger siblings. The relative risks (and 95%
confidence intervals) to carry S. pneumoniae
penicillin-nonsusceptible, resistant to ≥1,
≥2 and ≥3 antibiotic categories among younger siblings of PnCRM9
recipients vs. siblings of controls were 0.47 (0.31 to 0.70), 0.49 (0.33
to 0.71), 0.46 (0.30 to 0.73) and 0.49 (0.21 to 1.17), respectively. When
acquired, VT and antibiotic-resistant S. pneumoniae were
carried for a significantly shorter period of time among siblings of
PnCRM9 recipients than in siblings of controls.
Conclusion.
The marked effect of PnCRM9 administration to
DCC attendees on carriage of VT and antibiotic-resistant S.
pneumoniae among their younger household close contacts
demonstrates a herd effect of the vaccine.
From the Pediatric Infectious
Disease Unit (NGL, RD) and the Epidemiology Department (NGL,
DF), Soroka University Medical Center and the Faculty of
Health Sciences, Ben-Gurion University of the Negev,
Beer-Sheva, Israel.
Accepted for publication Feb. 20,
2003.
Reprints not available.
The Pediatric Infectious Disease Journal
2003; 22(6):524-532
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knowledge or opinions of the publisher, and is not to be construed or intended
as providing medical or legal advice. The decision whether or not to vaccinate
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consultation with your health care provider.
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