Haemophilus influenzae type B and Hib Vaccine

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Presentation transcript:

Haemophilus influenzae type B and Hib Vaccine Epidemiology and Prevention of Vaccine-Preventable Diseases National Immunization Program Centers for Disease Control and Prevention Revised March 2002

Haemophilus influenzae type b Severe bacterial infection, primarily in infants During late 19th century believed to cause influenza Immunology and microbiology clarified in 1930s

Haemophilus influenzae Aerobic gram-negative bacteria Polysaccharide capsule Six different serotypes (a-f) of polysaccharide capsule 95% of invasive disease caused by type b

Haemophilus influenzae type b Pathogenesis Organism colonizes nasopharynx In some persons organism invades bloodstream and cause infection at distant site Antecedent URI may be a contributing factor

Haemophilus influenzae type b Clinical Manifestations* *prevaccination era

Haemophilus influenzae type b Meningitis Accounted for approximately 50%-65% of cases Hearing impairment or neurologic sequelae in 15-30% Case fatality rate 2-5% in spite of effective antimicrobial therapy

Haemophilus influenzae type b Medical Management Treatment with chloramphenicol or an effective 3rd generation cephalosporin Ampicillin-resistant strains now common throughout the United States Hospitalization required

Haemophilus influenzae type b Epidemiology Reservoir Human Asymptomatic carriers Transmission Respiratory droplets Temporal pattern Peaks in Sept-Dec and March-May Communicability Generally limited but higher in some circumstances Limited communicability implied from lack of secondary cases in household settings. Secondary cases may occur in some situations, such as day care settings.

Estimated Incidence* of Invasive Hib Disease, 1987-2000 *Rate per 100,000 children <5 years of age

Hemophilus influenzae type b, 1986 Incidence by age group

Haemophilus influenzae type b – United States, 1996-2000 Incidence has fallen 99% since prevaccine era 341 confirmed Hib cases reported during 1996-2000 (average of 68 cases per year) Most recent cases in unvaccinated or incompletely vaccinated children

Hemophilus influenzae type b Risk factors for invasive disease Exposure factors household crowding large household size day care attendance low socioeconomic status low parental education school-aged siblings Host factors race/ethnicity chronic disease

Haemophilus influenzae type b Polysaccharide Vaccine Available 1985-1988 Not effective in children <18 months of age Effectiveness in older children variable

Polysaccharide Vaccines Age-related immune response Not consistently immunogenic in children 2 years old No booster response Antibody with less functional activity

Polysaccharide Conjugate Vaccines Stimulates T-dependent immunity Enhanced antibody production, especially in young children Repeat doses elicit booster response Antibody is biologically active in vitro

Haemophilus influenzae type b Conjugate Vaccines Pure polysaccharide vaccines (1985-1989) not effective in infants 3 conjugate vaccines licensed for use in infants Chemically and immunologically different

Conjugate Hib Vaccines PRP-D ProHIBIT HbOC Hibtiter PRP-T ActHIB, OmniHIB, TriHIBit PRP-OMP PedvaxHIB, COMVAX

Haemophilus influenzae type b Vaccine Routine Schedule Vaccine 2 mo 4 mo 6 mo 12-18 mo HbOC x PRP-T PRP-OMP

Haemophilus influenzae type b Vaccine Vaccination at <6 weeks of age may induce immunologic tolerance to Hib antigen Minimum age 6 weeks Minimum interval 4 weeks for primary series doses

Haemophilus influenzae type b Vaccine Interchangeability All conjugate Hib vaccines interchangeable for primary series and booster dose 3 dose primary series if more than one brand of vaccine used

Haemophilus influenzae type b Vaccine Delayed Vaccination Schedule Children starting late may not need entire 3 or 4 dose series Number of doses child requires depends on current age All children 15-59 months of age need at least 1 dose

Haemophilus influenzae type b Vaccine Detailed Schedule for Unimmunized Children Age at 1st Dose (months) Primary series Booster HbOC/PRP-T PRP-OMP PRP-D 2-6 7-11 12-14 15-59 3 doses, 2 m apart 2 doses, 2 m apart 1 dose 12-15 months 12-18 months 2 months later -- --

Lapsed Immunization* Doses Needed Prior Vaccination Age (mos) 1 + booster 1 2 Age (mos) 7-11 12-14 15-59 Prior Vaccination 1 dose 2 doses (not PRP-OMP) 2 doses before 12 mos 1 dose before 12 mos Any incomplete schedule *adapted from 2000 Red Book (AAP)

Haemophilus influenzae type b Vaccine Vaccination following invasive disease Children <24 months may not develop protective antibody after invasive disease Vaccinate during convalescence Complete series for age

Haemophilus influenzae type b Vaccine Use in older children and adults Generally not recommended for persons >59 months of age Consider for high risk persons: asplenia, immunodeficiency, HIV infection, HSCT One pediatric dose of any conjugate vaccine

Combination Vaccines Containing Hib DTaP – Hib TriHIBit Hepatitis B – Hib COMVAX

TriHIBit® ActHIB reconstituted with Tripedia Not approved for the primary series at 2, 4, or 6 months of age Approved for the fourth dose of the DTaP and Hib series only Primary series Hib doses given as TriHIBit should be disregarded

TriHIBit® May be used as the booster dose of the Hib series at >12 months of age following any Hib vaccine series* Should not be used if child has receive no prior Hib doses *booster dose should follow prior dose by >2 months

COMVAX Hepatitis B-Hib combination Use when either or both antigens indicated >6 weeks of age Not licensed for use if mother HBsAg+ Spacing and timing rules same as for individual antigens

Haemophilus influenzae type b Vaccine Adverse Reactions Swelling, redness, and/or pain in 5%-30% of recipients Systemic reactions infrequent Serious adverse reactions rare

Moderate to severe acute illness Age <6 weeks Haemophilus influenzae type b Vaccine Contraindications and Precautions Severe allergic reactions to vaccine component or following previous dose Moderate to severe acute illness Age <6 weeks

National Immunization Program Hotline 800.232.2522 Email nipinfo@cdc.gov Website www.cdc.gov/nip