Meningococcus

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pathogen

Neisseria meningitidis
gram negative diplococci
carriage in nasopharynx
12 identified capsular serogroups
common pathogenic serogroup A, B, C, W, X, Y
seasonal epidemics by group A, C
- meningitis belt
sporadic cases by e.g. group B
- Latin America
- Norway
- New Zealand
immunity generated by polysaccharide capsule except B
- may be the reason that herd immunity development relatively slow and sporadic outbreaks continue in above countries

epidemiology

highest < 2 y/o and adolescent
annual outbreak during dry season in meningitis belt
- dry winds make people's nose drier resulting in easier capture and membrane breakthrough
wide range difference of nasopharynx carriage between countries
- reason totally unknown
- NZ & 3%
- Nigeria muslim boarding school 30-40%
日本で戦後急速に発生が減ったのは，抗菌薬の導入普及と発熱早期での過剰投与，および住宅環境の改善による小児の集蔟が減少したためかもしれない

transmission

aerosol
fomite
adolescent activity

clinical picture

fever
distinctive petechiae anywhere in whole body
- apparent pain accompanies with petechia in contrast to dengue
- in earlier stage rashes are inflammation, not petechiae
no fading by pressure with glass tumbler - "tumbler test"
resulting in purple bruising of skin
photophobia
headache, neck stiffness, vomiting
irritability and/or confusion

vaccine

development history

1960s - purified PS vaccines for A and C
- immunity short term due to lack of T-cell involvement
1990s - conjugated vaccines for A and C after success of Hib conjugate vaccine
2000s - monovalent A vaccine for Africa
- "MenAfriVac"

current vaccines

A polysaccharide
- MenAfriVac
C conjugate
A,C,Y,W135 conjugate
- Menactra (Sanofi Pasteur)
- Menveo (GSK)
- Nimenrix (Pfizer)
B protein (not polysaccharide)
- Bexsero (GSK)
- Trumenba (Pfizer)
- VA-MENGOC-BC (Finlay Institute of Cuba)

issues of men B vaccine

polysaccharide of B is relatively low immunogenic
- the reason is considered because of interaction between B polysaccharide and fetal brain tissue, resulting in possible immunotolerance
  - interaction is observed as antibodies against B-PS have also affinity to fetal brain tissue
- it means B-PS vaccine has potential of neurological damage for young infants
currently available men B vaccines are protein-based vaccine, not PS vaccine
- proteins expressed on the surface of N. meningitidis group B are purified through bacterial culture