ABSTRACT. Twenty-two sudden infant death syndrome (SIDS) cases and 22 controls were examined immunohistochemically with regard to IgA, IgM, and IgG plasma cells in tracheal wall and duodenal mucosa. Furthermore, the presence of secretory component in tracheal surface and gland epithelium as well as in duodenal crypt and villus epithelium were evaluated. The examined specimens were obtained at autopsies. The control groups consisted of 11 infants who died of noninfectious causes and 11 who died of infections. In the tracheal wall, the SIDS group had higher IgM cell numbers than the control group that died of noninfectious causes ( p < 0.01), whereas the SIDS Among the Scandinavian countries, Norway has the highest incidence of SIDS, and the incidence seems to be increasing (1). Both the etiology and the pathogenesis of SIDS are at present unclear. We have, however, recently published data that indicate that hypoxia precedes death in approximately 80% of the SIDS cases (2, 3). There are several factors that might initiate respiratory inhibition and hypoxia. Because SIDS is more common in colder climates and an increased incidence correlates with the season of respiratory tract infections (4), an immune response in the respiratory tract might be one possible "trigger mechanism." Adaptive immunity at mucosal surfaces of children and adults is mainly exerted by secretory IgA and IgM antibodies, which represent the quantitatively most important humoral immune system of the body (5-8). SC, the poly-Ig receptor, is imperative for the secretion of secretory IgA and secretory IgM (9). Increased concentrations of IgM, IgG, and to a lesser extent IgA in lung lavage fluid from SIDS victims (10) and raised numbers of IgA, IgM, and IgG producing cells in salivary glands (1 1) indicate a stimulation of the secretory immune system in the upper airways and lungs. Furthermore, lack of SC in the tracheal epithelium preventing the transport of dimeric IgA and pentameric IgM has been suggested as an etiologic factor in SIDS (12).The purpose of this study was to investigate the humoral immune response and the expression of epithelial SC in the wall of the upper respiratory tract and the duodenal mucosa in SIDS. MATERIALS AND METHODSTissue specimens. Tracheal wall and duodenal mucosa specimens were obtained from 22 infants who died from SIDS (15 males and seven females; median age 4 mo, range 1-7 mo). Tracheal wall samples were taken from the canna; one sample was rejected because of bacterial growth.The control group consisted of 22 specimens from tracheal wall and from duodenal mucosa. The median age of the control group was 4 mo (range 1-12 mo). Eleven infants died of the following causes: congenital heart disease (n = 4), head injury (n = 2), infanticide (n = I), CO intoxication (n = I), drowning (n = I), battered child syndrome (n = l), and accidental suffocation (n = 1). None of these infants had clinical evidence of an infection. Eleven infants died of a specific infection: sepsis (n = 4), pneumonia (n = 6), or meningitis (n = 1...
Seventeen sudden infant death syndrome (SIDS) cases and 9 controls, were examined immunohistochemically with regard to the presence of IgA-, IgM-, IgD, and IgG, as well as for the subtypes IgG1-, IgG2-, IgG3-, and IgG4-immunocytes. Differences in compartmentalization were also investigated. Differences were demonstrated between SIDS and controls in total number of IgG cells per 0.1 mm2 tissue area (median: 18.3, range: 12.3-30.2 versus median: 6.3, range: 2.0-14.6) (p < 0.01), and for IgA immunocytes (median: 3.9, range: 2.4-5.0 versus median: 1.5, range: 1.1-3.7) (p < 0.05), while no differences were demonstrated for IgM cells (median: 1.8, range: 1.2-3.3 versus median: 1.8, range: 0.7-5.6) or IgD cells (median: 1.9, range: 0.8-2.9 versus median: 1.6, range: 0.7-2.4). Differences were demonstrated between SIDS and control IgG plasma cells in all the four palatine tonsillar compartments; germinal centre (p < 0.01), mantle zone (p < 0.05), interfollicular area (p < 0.01) and reticular epithelium (p < 0.01). Furthermore, the number of IgA cells was higher in SIDS vs. controls in both the germinal centre (median: 1.4, range: 0.6-2.1 versus median: 0.6, range: 0.3-1.3) (p < 0.05) and in the interfollicular area (median: 2.2, range: 1.1-3.1 versus median: 0.5, range: 0.4-2.0) (p < 0.01).(ABSTRACT TRUNCATED AT 250 WORDS)
Intravenous and intrathecal injection of IL-1 beta prolong the duration of apnea and modifies autoresuscitation.
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