Streptococcus pneumoniae: Difference between revisions
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Streptococcus pneumoniae
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== |
==Background== |
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=== |
===Microbiology=== |
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* [[Stain::Gram-positive]], lancet-shaped [[Cellular shape::coccus|diplococcus]] |
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* 90+ serotypes, based on capsular polysaccharide that is bound to peptidoglycan |
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* Lab identification is based on [[Catalase test::catalase-negative]], [[Hemolysis pattern::α-hemolysis]] of blood agar (from pneumolysin), [[Susceptible to::optochin]] susceptibility, and bile salt solubility |
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* Via transformation, bacteria can exchange genetic material with each other |
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*[[Stain::Gram-positive]], lancet-shaped [[Cellular shape::coccus|diplococcus]] |
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==== Susceptibility testing ==== |
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*90+ serotypes, based on capsular polysaccharide that is bound to peptidoglycan |
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* CLSI penicillin breakpoints for susceptibility changed in 2008 |
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*Lab identification is based on [[Catalase test::catalase-negative]], [[Hemolysis pattern::α-hemolysis]] of blood agar (from pneumolysin), [[Susceptible to::optochin]] susceptibility, and bile salt solubility |
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** For meningitis: ≤0.06 μg/mL |
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*Via transformation, bacteria can exchange genetic material with each other |
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** For other infections: ≤2 μg/mL |
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====Susceptibility testing==== |
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==== Antibiotic resistance ==== |
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* '''[[Penicillin]]''' resistance |
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** ''S. pneumoniae'' has 6 PBPs: 1A, 1B, 2A, 2B, 2X, and 3 |
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** Resistance in any of the PBPs can increase the MIC |
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** Mutations in PBP 2B are associated with low-level resistance |
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** Mutations in PBP 2X are associated with high-level resistance |
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* '''[[Macrolides|Macrolide]]''' resistance |
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** ''ermB'' encodes an enzyme that methylates the 23S subunit, blocking macrolides and giving very high MIC ≥64 |
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** ''mefA'' encodes an efflux pump that gives a relatively lower MIC ≤16 |
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*CLSI penicillin breakpoints for susceptibility changed in 2008 |
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=== Epidemiology === |
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**For meningitis: ≤0.06 μg/mL |
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* Present worldwide |
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**For other infections: ≤2 μg/mL |
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* Major cause of morbidity and mortality in children |
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** Leading cause of under-5 mortality worldwide |
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=== |
====Antibiotic resistance==== |
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* Acquired by coughing and sneezing |
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* Asymptomatic carriage or colonization in the nasopharynx |
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* Invasion through epithelial cells into the bloodstream, using the PAF and pIg receptors |
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* Capsule and various proteins help it to evade immune system |
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*'''[[Penicillin]]''' resistance |
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== Clinical Manifestations == |
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**''S. pneumoniae'' has 6 PBPs: 1A, 1B, 2A, 2B, 2X, and 3 |
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**Resistance in any of the PBPs can increase the MIC |
|||
**Mutations in PBP 2B are associated with low-level resistance |
|||
**Mutations in PBP 2X are associated with high-level resistance |
|||
*'''[[Macrolides|Macrolide]]''' resistance |
|||
**''ermB'' encodes an enzyme that methylates the 23S subunit, blocking macrolides and giving very high MIC ≥64 |
|||
**''mefA'' encodes an efflux pump that gives a relatively lower MIC ≤16 |
|||
=== |
===Epidemiology=== |
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*Present worldwide |
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* 4-10% in the general adult population, usually lasting several weeks |
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*Major cause of morbidity and mortality in children |
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* Highest in children, up to 30-60% depending on the situation, lasting up to 6 months |
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**Leading cause of under-5 mortality worldwide |
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=== |
===Pathophysiology=== |
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*Acquired by coughing and sneezing |
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=== Sinusitis === |
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*Asymptomatic carriage or colonization in the nasopharynx |
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*Invasion through epithelial cells into the bloodstream, using the PAF and pIg receptors |
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*Capsule and various proteins help it to evade immune system |
|||
==Clinical Manifestations== |
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=== Bacteremia === |
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=== |
===Asymptomatic carriage=== |
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*4-10% in the general adult population, usually lasting several weeks |
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* Acute onset of cough (92%), fatigue (63%), shortness of breath (47%), and dyspnea (23%) with documented or subjective fever (92%), chills (77%), sweats, purulent sputum, and pleuritic chest pain (79%) |
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*Highest in children, up to 30-60% depending on the situation, lasting up to 6 months |
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=== |
===Otitis media=== |
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===Sinusitis=== |
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* Most common cause of meningitis in adults |
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* Acquired by hematogenous spread from nasopharynx, or direct invasion from sinuses |
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* May be secondary to otitis media or sinusitis |
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* CSF leaks and other defects predispose to infection |
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* Diagnostic yield in CSF decrease significantly 4 hours after administration of antibiotics |
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===Bacteremia=== |
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===Pneumonia=== |
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*Acute onset of cough (92%), fatigue (63%), shortness of breath (47%), and dyspnea (23%) with documented or subjective fever (92%), chills (77%), sweats, purulent sputum, and pleuritic chest pain (79%) |
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===Meningitis=== |
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*Most common cause of meningitis in adults |
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*Acquired by hematogenous spread from nasopharynx, or direct invasion from sinuses |
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*May be secondary to otitis media or sinusitis |
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*CSF leaks and other defects predispose to infection |
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*Diagnostic yield in CSF decrease significantly 4 hours after administration of antibiotics |
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== Prevention == |
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=== Vaccination === |
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* Essentially two forms of vaccine available in Canada |
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** 13-valent pneumococcal conjugate vaccine (Pneu-C-13), which is more immunogenic |
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*** Includes serotypes 4, 9V, 6B, 14, 18C, 19F, 23F, 1, 5, 7F, 3, 6A, and 19A |
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** 23-valent pneumococcal polysaccharide vaccine (Pneu-C-23), which includes more strains |
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*** Includes above serotypes except 6A, plus 2, 8, 9N, 10A, 11A, 12F, 15B, 17F, 20, 22F, and 33F |
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* Pneu-C-13 is part of routine childhood immunizations, which Pneu-P-23 is used for most adults |
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{| class="wikitable" |
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!Age |
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!Status |
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!Vaccine |
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|- |
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|18-64 |
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|high risk for invasive disease |
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|PP-23 ± booster at 5 years |
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|- |
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|18-64 |
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|smoking, alcohol, homeless, LTC |
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|PP-23 |
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|- |
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|≥65 |
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|regardless of prior vaccination |
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|PP-23 at least 5 years after last dose and 8 weeks after a dose of PC-13 |
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|- |
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|≥18 |
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|immunocompromised |
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|PC-13 followed by PP-23 with booster at 5 years |
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|- |
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|≥18 |
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|HSCT recipient |
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|PC-13 x3 q4wk starting 3-9 months post-transplant, followed by PP-23 6-12 months later ± booster at 1 year |
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|} |
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* Conditions with high risk for invasive disease include (highest risk are bolded): |
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** [[CSF leak]], chronic neurologic conditions that impair clearance of oral secretions, cochlear implants, chronic heart disease, [[diabetes mellitus]], '''[[chronic kidney disease]]''', '''[[chronic liver disease]]''' including [[cirrhosis]], and chronic lung disease including [[asthma]] requiring medical care within past 12 months |
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** '''Immunocompromising conditions''', including [[hyposplenia]] (including [[sickle cell disease]], [[asplenia]], or splenic dysfunction), [[primary immunodeficiency]], therapeutic immune suppression (including [[corticosteroids]], [[chemotherapy]], [[radiation therapy]], and transplantation), [[HIV]], [[HSCT]], [[malignancy]], [[nephrotic syndrome]], [[solid organ transplantation]] |
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{{DISPLAYTITLE:''Streptococcus pneumoniae''}} |
{{DISPLAYTITLE:''Streptococcus pneumoniae''}} |
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[[Category:Gram-positive cocci]] |
[[Category:Gram-positive cocci]] |
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Revision as of 09:54, 14 August 2020
Background
Microbiology
- Gram-positive, lancet-shaped diplococcus
- 90+ serotypes, based on capsular polysaccharide that is bound to peptidoglycan
- Lab identification is based on catalase-negative, α-hemolysis of blood agar (from pneumolysin), optochin susceptibility, and bile salt solubility
- Via transformation, bacteria can exchange genetic material with each other
Susceptibility testing
- CLSI penicillin breakpoints for susceptibility changed in 2008
- For meningitis: ≤0.06 μg/mL
- For other infections: ≤2 μg/mL
Antibiotic resistance
- Penicillin resistance
- S. pneumoniae has 6 PBPs: 1A, 1B, 2A, 2B, 2X, and 3
- Resistance in any of the PBPs can increase the MIC
- Mutations in PBP 2B are associated with low-level resistance
- Mutations in PBP 2X are associated with high-level resistance
- Macrolide resistance
- ermB encodes an enzyme that methylates the 23S subunit, blocking macrolides and giving very high MIC ≥64
- mefA encodes an efflux pump that gives a relatively lower MIC ≤16
Epidemiology
- Present worldwide
- Major cause of morbidity and mortality in children
- Leading cause of under-5 mortality worldwide
Pathophysiology
- Acquired by coughing and sneezing
- Asymptomatic carriage or colonization in the nasopharynx
- Invasion through epithelial cells into the bloodstream, using the PAF and pIg receptors
- Capsule and various proteins help it to evade immune system
Clinical Manifestations
Asymptomatic carriage
- 4-10% in the general adult population, usually lasting several weeks
- Highest in children, up to 30-60% depending on the situation, lasting up to 6 months
Otitis media
Sinusitis
Bacteremia
Pneumonia
- Acute onset of cough (92%), fatigue (63%), shortness of breath (47%), and dyspnea (23%) with documented or subjective fever (92%), chills (77%), sweats, purulent sputum, and pleuritic chest pain (79%)
Meningitis
- Most common cause of meningitis in adults
- Acquired by hematogenous spread from nasopharynx, or direct invasion from sinuses
- May be secondary to otitis media or sinusitis
- CSF leaks and other defects predispose to infection
- Diagnostic yield in CSF decrease significantly 4 hours after administration of antibiotics
Prevention
Vaccination
- Essentially two forms of vaccine available in Canada
- 13-valent pneumococcal conjugate vaccine (Pneu-C-13), which is more immunogenic
- Includes serotypes 4, 9V, 6B, 14, 18C, 19F, 23F, 1, 5, 7F, 3, 6A, and 19A
- 23-valent pneumococcal polysaccharide vaccine (Pneu-C-23), which includes more strains
- Includes above serotypes except 6A, plus 2, 8, 9N, 10A, 11A, 12F, 15B, 17F, 20, 22F, and 33F
- 13-valent pneumococcal conjugate vaccine (Pneu-C-13), which is more immunogenic
- Pneu-C-13 is part of routine childhood immunizations, which Pneu-P-23 is used for most adults
| Age | Status | Vaccine |
|---|---|---|
| 18-64 | high risk for invasive disease | PP-23 ± booster at 5 years |
| 18-64 | smoking, alcohol, homeless, LTC | PP-23 |
| ≥65 | regardless of prior vaccination | PP-23 at least 5 years after last dose and 8 weeks after a dose of PC-13 |
| ≥18 | immunocompromised | PC-13 followed by PP-23 with booster at 5 years |
| ≥18 | HSCT recipient | PC-13 x3 q4wk starting 3-9 months post-transplant, followed by PP-23 6-12 months later ± booster at 1 year |
- Conditions with high risk for invasive disease include (highest risk are bolded):
- CSF leak, chronic neurologic conditions that impair clearance of oral secretions, cochlear implants, chronic heart disease, diabetes mellitus, chronic kidney disease, chronic liver disease including cirrhosis, and chronic lung disease including asthma requiring medical care within past 12 months
- Immunocompromising conditions, including hyposplenia (including sickle cell disease, asplenia, or splenic dysfunction), primary immunodeficiency, therapeutic immune suppression (including corticosteroids, chemotherapy, radiation therapy, and transplantation), HIV, HSCT, malignancy, nephrotic syndrome, solid organ transplantation
