NeuroLearn NeuroHelp Bacteria @ Acute meningitis

Background Histopathology & Immunohistochemistry

BACKGROUND AND CLINICAL INFORMATION: Head

Definition: Neonatal period is defined as the first 30 days of life. This is the period in which risk for acquiring meningitis is greater than any time thereafter. In reality, the risk factors and treatment may extend to infants who are several months old.

Clinical features:

Early onset (less than 48 hr old): obstetric complications are common; transmission is usually mother to infant; infants are usually mature and usually present as sepsis clinically with only one third with CNS dysfunction; common agents include Group B streptococci (especially group III) and E. coli but nosocomial pathogens are rare; mortality is about 35%.
Late onset (later than 7 days after birth) group: obstetric complications are rare but babies are often premature; transmission is from mother or other adults to infants; fever is more prominent; CNS manifestation is more striking and seizures is present in about half the cases; common agents include Group B strepptococci and nosocomial pathogens but E. coli is uncommon; mortality is about 15%.

Incidence and risk factors: 0.5% of all life birth.

Risk factors:

Low birth weight: Infants below 2,500 grams have a three times increased risk.
Metabolic: Risk factors specific for E. coli sepsis include galactosemia, excess free iron (administer to prevent iron deficiency anemia in some situations) and excess vitamin E (adminstered to prevent retinopathy in premature babies).
Other risk factors: premature rupture of membrane, resuscitation at birth and babys born to mothers with a temperature greater than 37.8 øC postpartum.

Pathogenesis: lack of transplacentally acquired antibodies against potential meningeal pathogens, absence of alveolar macrophages at birth, a small PMN pool with chemothactic deficiencies compared with adults, and inefficient synthesis of antibodies during the neonatal stages all add to the increased susceptibility of neonates to meningitis.

Amniotic fluid is inhibitory to the growth of E. coli and certain other organisms because of the presence of lysozyme, transferrin, and certain immunoglobulins. The amniotic fluid is no longer a hostile environment for E. coli if it contains meconium or vernix. In contrast, Group B Streptococcus can grow in "normal" amniotic fluid. Macrophages in the amniotic fluid are derived from the maternal circulation.

Infectious agents: almost half of the cases are caused by streptococci (especially group B), followed by Staphylococcus (S. epidermis, S. aureus, and S. pneumoniae), Klebsiella-Enterobacter species and then Escherichia coli (most commonly type K1).

Common pathogens and route of infection:

Group B Streptococcus: early onset disease acquired in the birth canal; late onset disease- contamination.
Staphylococcus epidermidis: comtaminated intravascular cannulae.
Staphylococcus aureus: usually a primary focus of infection is evident, with heel punctures and intravenous cannula entry sites as most common foci.
Escherichia coli: multiple pathways including acquisition through the birth canal and contaminated nursary personals.
Listeria monocytogenes: the source is genital tract or subclinical infection of the mother.

HISTOPATHOLOGY AND IMMUNOHISTOCHEMISTRY: Head

Arachnoiditis around the base of the brain may be particularly prominent, alternatively, the exudate may be distributed over the cerebral cortex surface.

Vasculitis is an invariable component of neonatal meningitis. Perivascular inflammatory infiltration in the adventitia with the intima spared is common in arteries; phlebitis with thrombosis and complete occlusion is common in veins; this may lead to thrombotic hemorrhagic infarction.

Pathogenesis: One of the explanation for the increase in severity of neonatal meningitis is the relatively paucity and functional immaturity of arachnoid villi in the newborn. Thus, the egress of bacteria is slower, which can lead to bacterial accumulation in the CSF. The inflammatiory exudate in the ventricular CSF drains into and "Plugs" the arachnoid villi, producing dysfunction of this exit valve and transiently increasing intracranial pressure. Choroid plexitis, ventriculitis, and glial tufts and bridges formation within the ventricles will lead to obstructive hydrocephalus.

Rhombencephalitis often associate with meningitis due to Listeria in both pediatric and adult cases [Uldry PA et al., J Neurol 1993 24:235-42]