Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UMLS:C0023241 (
Legionella
)
6,990
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Innate immune system deficiency may predispose to severe infections such as
Legionnaires' disease
. We have investigated the role of
mannose-binding lectin
(
MBL
) deficiency in the Melbourne Aquarium
Legionnaires' disease
outbreak. Serum samples from patients and controls that were exposed but shown to be uninfected from the Melbourne Aquarium
Legionnaires' disease
outbreak were tested for
MBL
function (C4 deposition) and level (mannan-binding).
MBL
function was lower in
Legionnaires' disease
cases than in age- and sex-matched uninfected, exposed controls. The frequency of
MBL
deficiency with C4 deposition < 0.2 U/microl was significantly higher in
Legionnaires' disease
cases than in controls. This also applied to
Legionnaires' disease
cases requiring hospital care. There was no difference in
MBL
mannan-binding levels between
Legionnaires' disease
patients and controls. There was no significant interval change in
MBL
function or level after a mean of 46 days.
MBL
complement activation functional deficiency appears to predispose to
Legionnaires' disease
.
...
PMID:Low mannose-binding lectin complement activation function is associated with predisposition to Legionnaires' disease. 1742 52
Polymorphisms leading to deficiency of
mannose-binding lectin
(
MBL
) are associated with predisposition to infection. However,
MBL
deficiency can be protective against intracellular pathogens that use
MBL
to enter host cells. The role of
MBL
genotype and activity in infection with the intracellular pathogen
Legionella
pneumophila was studied in a large outbreak of legionellosis at a Dutch flower show. A total of 141 patients, 65 exposed asymptomatic exhibition staff members and 670 unexposed blood bank donors were included for the study of MBL2 genotypes and
MBL
-mediated complement activation. Genotypic
MBL
deficiency was equally prevalent in patients and controls. Deficient
MBL
-mediated complement activation was more prevalent in patients. Even in patients with genotypes that confer
MBL
sufficiency, 20.6% lacked
MBL
-mediated complement activation. In most patients with
MBL
-sufficient genotypes who lacked
MBL
-mediated activation at the acute phase of disease, lectin pathway functionality was restored at convalescence. In conclusion, genotypic
MBL
deficiency was not a risk factor for legionellosis. However, patients with legionellosis displayed deficient
MBL
-mediated complement activation even with
MBL
-sufficient genotypes. Together, these genotypical and functional data suggest that the observed deficiency of lectin pathway activation is an effect of legionellosis rather than a risk factor for acquiring it.
...
PMID:Deficient mannose-binding lectin-mediated complement activation despite mannose-binding lectin-sufficient genotypes in an outbreak of Legionella pneumophila pneumonia. 1907 29
