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Important changes to the childhood immunisation programme

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Title: Important changes to the childhood immunisation programme


1
Important changes to the childhood immunisation
programme
2
Changes from 4th September 2006
  • The addition of a pneumococcal conjugate vaccine
    (PCV) at 2, 4 and 13 months of age
  • A dose of MenC vaccine at 3 and 4 months
  • A booster dose of Hib and MenC vaccine (given as
    a combined Hib/MenC vaccine) at 12 months of age.

3
The childhood immunisation schedule
4
Why are these changes being made?
  • to protect children lt 2 years of age who are at
    increased risk of pneumococcal disease
  • to boost childrens protection against Hib and
    MenC infections through their early childhood
    years

5
Facts about pneumococcal disease
6
What is pneumococcal disease?
  • Describes infections caused by the bacterium
    S.pneumoniae
  • Over 90 serotypes identified
  • 20 30 serotypes responsible for majority of
    disease
  • 7 serotypes responsible for 82 of disease in
    children under 5 years of age

7
Pneumococcal infection
  • Major cause of serious disease
  • meningitis, septicaemia and severe pneumonia
    (invasive pneumococcal disease - IPD)
  • Less serious, but commoner diseases
  • otitis media, milder pneumonia and bronchitis
    (non invasive)

8
Severity of disease
  • dependent on which part of the body is affected

9
http//www.hpa.org.uk/infections/topics_az/pneumoc
occal/pneumo_powerpoint_2006.ppt366,4,Slide 4
10
Pneumococcal infection
  • Most common in
  • the very young babies and children under 2
    years of age
  • the very old over 65 years of age
  • younger age groups with concurrent medical
    conditions

11
Invasive pneumococcal disease rates by age per
100,000 population per year
12
Pneumococcal infection
  • 5000 cases of invasive pneumococcal disease (IPD)
    per year
  • 530 children IPD lt 2 years (England Wales)
  • Around 50 children lt 2yrs die from IPD per yr1
  • 2 thirds from pneumococcal meningitis
  • 50 who survive pneumococcal meningitis have
    disabilities2

1. IspahaniP, Slack RC, Donald FE, et al (2004)
Twenty-year surveillance of invasive pneumococcal
disease in Nottingham serogroups responsible and
implication for immunisation. Arch Dis Child 89
757-62 2. Bedford H, de Louvois J, Halket et al
(2001) Meningitis in infancy in England and
Wales follow-up at 5 years. BMJ 323 533-6
13
Why change the Hib and MenC immunisation schedule?
14
Evidence for changes
  • Regular reviews of immunisation programmes to
    ensure all children have the best possible
    protection against preventable diseases
  • Research shows that longer-term protection
    against Hib and meningococcal C disease is
    achieved by modifying the existing programme

15
Evidence for changes
  • Studies show two doses of MenC in the first year
    of life provides the same level of protection as
    three doses
  • No additional or increased protection from giving
    three doses of MenC in the first year of life
  • An additional dose in the second year of life
    gives longer-term protection against
    meningococcal C disease

16
Evidence for changes
  • Studies show an additional booster dose of Hib
    vaccine is needed in the second year of life to
    ensure that
  • Hib disease levels remain low
  • protection given to children continues well into
    their childhood

17
What do the changes mean?
  • No additional visits in the first year of life
  • Infants will be offered different combinations of
    vaccines at the 2, 3 and 4 month visits
  • Three injections will be offered to infants at 4
    months of age
  • A new 12 month vaccination visit will be
    introduced

18
Three injections for infants
  • Its been done before during the Hib booster
    campaign 2003
  • Infant anterolateral thigh can accommodate two
    injections along the length of the thigh
  • At least 2.5cms (1 inch) apart so that reactions
    dont overlap
  • Record which vaccine was injected at which point
    on limb
  • Common practice in United States where e.g. DTaP,
    Hep B, Hib and PCV may all be given in same visit

19
Simultaneous administration
DTaP/IPV/Hib
PCV
MenC
World Health Organisation (2004)
20
Why keep PCV separate?
  • To allow any localised reaction to be easily
    linked to the particular vaccine

21
Order of injections given
  • Prepare all 3 injections immediately prior to
    immunising
  • 2 in 1 leg, PCV in other
  • DH do not specify which leg
  • Local decisions - may consider recommending
    always using the same leg

22
Can the deltoid be used?
  • It is not recommended that immunisations be
    given in the arm of infants under one year of age
    because
  • Risk of hitting radial nerve
  • Muscle mass not properly developed

23
Can one vaccine be delayed?
  • DH recommends all three vaccines be given at the
    same time to ensure children are fully protected
    from serious disease as early as possible
  • Parents have the right to refuse one or all
    injections
  • HCW should never recommend delaying
  • Could leave HCW open to criticism if relevant
    vaccine preventable infection occurred in the
    interim

24
12 month visit
  • A single dose of Hib/MenC
  • No catch-up for Hib/MenC booster
  • Cannot be administered (at the moment) with PCV
    MMR at 13 months as no data to show compatibility

25
13 month visit
  • 1st MMR and booster PCV
  • Cannot be administered (at the moment) with
    combined Hib/MenC vaccine as no data to show
    compatibility
  • PCV catch-up for all children aged gt 2 months and
    lt 2 years of age

26
Pneumococcal catch-up programme

27
Children over 2 months and under 8 months of age
at the start of the programme.
  • Children born 04.02.06 - 03.07.06
  • (gt 2 months but lt 8 months of age)
  • Two doses of PCV two months apart with booster at
    13 months

28
Children over 8 months of age at the start of the
programme.
  • Children born 04.08.05 - 03.02.06 (8 months
    13 months of age)
  • A single dose of PCV at 13 months of age

29
Children over 12 months of age at the start of
the programme.
  • Children born 05.09.04 - 03.08.05 (gt 13 months -
    lt 2 years of age)
  • A single dose of PVC

30
(No Transcript)
31
At-risk children
  • Asplenia or dysfunction of the spleen
  • Chronic respiratory disease
  • Chronic heart disease
  • Chronic renal disease
  • Chronic liver disease
  • Diabetes
  • Immunosuppression
  • Cochlear implants
  • CSF leaks
  • lt 5s with previous history of invasive disease

32
At-risk children
  • It is important that at-risk children of any
    age up to 5 years receive a complete course of
    PCV vaccination as soon as possible (regardless
    of catch-up scheduling)

33
At-risk children
  • PCV routinely at 2, 4 and 13 months of age
  • At-risk children lt 12 months of age2 doses of
    PCV (one month apart if necessary) before 12
    months and one at 13 months of age
  • At-risk children gt 12 months and lt 5 years of age
    should be offered a single dose of PCV
  • All at-risk children should be offered a single
    dose of pneumococcal polysaccharide vaccine (PPV)
    when they are two years of age or over and at
    least 2 months after the final dose of PCV

34
At-risk children
  • Children aged 2 months and under 5 years of age
    with asplenia, splenic dysfunction or who are
    immunocompromised, require a second dose 2 months
    after the first dose as they may have a
    sub-optimal immunological response to the first
    dose of vaccine
  • All children lt 5 years with previous history of
    IPD should have PCV irrespective of previous
    vaccination history
  • At-risk children presenting for first
    pneumococcal immunisation aged 5 years and over
    should be offered a single dose of PPV

35
Vaccination of children with unknown or
incomplete vaccination status
  • Following completion of the catch-up
    programme, children who have not completed the
    routine programme require
  • Children lt 12 months of age
  • 2 doses of PCV, 2 months apart and further dose
    at 13 months of age
  • Children gt 12 months and lt 2 years of age
  • should be offered a single dose of PCV

36
Supplies
  • Week commencing 7th and 14th August 2006first
    allocated delivery of two week supply on usual
    delivery date
  • Week commencing 21st and 28th Augustno
    deliveries
  • Week commencing 4th September 2006 campaign
    starts
  • Week commencing 4th and 11th September
    2006second allocated delivery of two week supply
  • Free ordering from midday 13th September 2006

37
Further information
  • CMO Letters
  • www.dh.gov.uk/PublictionsAndStatistics/LettersAndC
    irculars/DearColleagueLetters/fs/en
  • www.dh.gov.uk/AboutUs/MinistersAndDepartmentLeader
    s/ChiefMedicalOfficer/CMOPublications/CMOLetters/f
    s/en
  • NHS Immunisation website
  • www.immunisation.nhs.uk
  • The Green Book
  • www.dh.gov.uk/PolicyAndGuidance/HealthAndSocialCar
    eTopics/GreenBook/fs/en
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