Rapid reduction in invasive pneumococcal disease after introduction of PCV7 into the National Immunization Plan in Israel

S. Ben-Shimol, D. Greenberg, N. Givon-Lavi, N. Elias, D. Glikman, U. Rubinstein, R. Dagan, Jacob Amir, Galia Barkai, Diana Averbuch, Shraga Aviner, Bachinski Ahuva, Maskit Bar-Meir, Avihu Bar-Yochai, Ilana Benedikt, Rita Bernstein, Nael Elias, Dan Engelhard, Moshe Ephros, Daniel GlikmanGiora Gottesman, Galia Grisaru-Soen, Alex Guri, Imad Kasis, Nathan Keller, Orli Megged, Dan Miron, Meirav Mor, Hana Ofir-Mintzer, Avi Peretz, Uri Rubinstein, Yechiel Schlesinger, David Schwartz, Itamar Shalit, Eli Somekh, Isaac Srugo, Alvira Zbriger, Miriam Zucker

Research output: Contribution to journalArticlepeer-review

67 Scopus citations

Abstract

Background: The 7-valent conjugated vaccine (PCV7) was introduced into the Israeli National Immunization Program (NIP) in July 2009 (2, 4, 12 months schedule; 2 dose catch-up in second year of life). Nationwide active prospective surveillance on invasive pneumococcal disease (IPD) has been conducted in children since 1989. In the current study, IPD epidemiology in children <5 years during the 20 years before and 18 months after PCV7 NIP initiation, is reported. Methods: All 27 centers performing blood/cerebrospinal fluid (CSF) cultures in children reported monthly IPD cases. Capture-recapture approach was used for completeness. Results: During 1989-2010, 6022 IPD cases were reported in children <5 years; PCV7 serotypes (7VST) caused ∼50% of all episodes. In 2009 and 2010, 7VST IPD incidences <5 years of age (per 100,000) were 15.9 and 5.4, respectively (a 43% and 81% decrease, respectively) compared to 2003-2007 (mean incidence 27.8). Serotype 6A dynamics resembled those of 7VST. The respective overall IPD incidence decreases were 23% and 42%. The incidence dynamics of serotypes 1, 3, 5, 7F and 19A IPD were characterized by considerable fluctuations over the study period without any upwards or downwards trend in any of the age groups. The overall incidence of serotypes not included in the 13-valent pneumococcal conjugate vaccine (PCV13) did not vary significantly during the study period. By the end of 2010, 72% of the remaining IPD was caused by pneumococcal serotypes included in PCV13. Conclusions: An active prospective long-term surveillance, showed a rapid and sharp decline in IPD in children <5 years following initiation of NIP with PCV7. No serotype replacement has been observed so far. The transition from PCV7 to PCV13 initiated in October 2010 may lead to a further substantial decrease in IPD. Follow-up is needed to better determine the long-term PCV effects.

Original languageEnglish
Pages (from-to)6600-6607
Number of pages8
JournalVaccine
Volume30
Issue number46
DOIs
StatePublished - 12 Oct 2012

Bibliographical note

Funding Information:
Shalom Ben Shimol: None. David Greenberg has received a grant from MSD. Noga Givon Lavi: None. Nael Elias: None. Uri Rubinstein: None. Daniel. Glikman: None. Ron Dagan: In the last five years, Prof. Ron Dagan has received grants/research support from Berna/Crucell, Wyeth/Pfizer, MSD, Protea; has been a scientific consultant for Berna/Crucell, GlaxoSmithKline, Novartis, Wyeth/Pfizer, Protea, MSD and a speaker for Berna/Crucell, GlaxoSmithKline, Wyeth/Pfizer; he is a shareholder of Protea/NASVAX.

Funding Information:
The study was supported in part by Wyeth (Pfizer) Grant No. 0887X1-4603.

Funding

Shalom Ben Shimol: None. David Greenberg has received a grant from MSD. Noga Givon Lavi: None. Nael Elias: None. Uri Rubinstein: None. Daniel. Glikman: None. Ron Dagan: In the last five years, Prof. Ron Dagan has received grants/research support from Berna/Crucell, Wyeth/Pfizer, MSD, Protea; has been a scientific consultant for Berna/Crucell, GlaxoSmithKline, Novartis, Wyeth/Pfizer, Protea, MSD and a speaker for Berna/Crucell, GlaxoSmithKline, Wyeth/Pfizer; he is a shareholder of Protea/NASVAX. The study was supported in part by Wyeth (Pfizer) Grant No. 0887X1-4603.

FundersFunder number
Pfizer0887X1-4603
Meso Scale Diagnostics

    Keywords

    • Children
    • Dynamics
    • Invasive pneumococcal disease
    • PCV - pneumococcal conjugate vaccine
    • Streptococcus pneumoniae
    • Surveillance

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