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Query: UMLS:C0024312 (
lymphopenia
)
4,859
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Clinical observations of Babesia canis infection in 63 dogs during a 1-year period are summarised, demonstrating the pathogenicity of the Babesia strain endemic in Hungary. Most patients had babesiosis in the spring and autumn, correlating with the seasonal activity of ticks. Male animals appeared in higher numbers, probably due to an overrepresentation of outdoor dogs. Uncomplicated babesiosis was diagnosed in 32 cases. The disease affected dogs of any age in this study. Symptoms were similar to those published from other parts of the world: lethargy, fever, splenomegaly, pallor, icterus, haemoglobinuria and presence of ticks were the most common observations. Thrombocytopenia,
lymphopenia
and neutropenia were frequent haemogram changes. Imidocarb appeared to be highly effective in eliminating the Babesia infection. Thirty-one animals demonstrated babesiosis with complications. Most Rottweilers (7/9) developed complicated disease. Old age was a risk factor for multiple complications. Multiple organ manifestations had poor prognosis. Hepatopathy (44%), pancreatitis (33%), acute renal failure (ARF; 31%) and disseminated intravascular coagulation (DIC; 24%) were frequent complications, while immune-mediated haemolytic anaemia (IMHA; 10%), acute respiratory distress syndrome (ARDS; 6%) and cerebral babesiosis (3%) were rarely observed. There was a significant difference between the mean age of dogs having uncomplicated disease, babesiosis with a single complication and babesiosis with multiple complications (3.4, 4.8 and 8.6 years, respectively, p < 0.001). The recovery rate (78, 68 and 25%, respectively, p = 0.005) and mortality rate (3, 21 and 67%, respectively, p < 0.001) also tended to differ significantly in these groups. Systemic inflammatory response syndrome (SIRS) and DIC are two possible pathways leading to multiple organ dysfunction syndrome (MODS) in babesiosis. DIC was found to predict MODS more sensitively in this study than
SIRS
: there were 6 animals developing MODS out of 11 identified with DIC, while only 5 dogs developed MODS out of 22 having
SIRS
.
...
PMID:Clinical manifestations of canine babesiosis in Hungary (63 cases). 1702 Jan 40
SIRS
is associated with
lymphopenia
, and prolonged
lymphopenia
of septic patients has been associated with increased mortality risk. We hypothesize that elevated adenosine during
SIRS
down-regulates G
i
-coupled A
1
R, which signals an effect that sensitizes a cAMP-dependent lymphotoxic response. In this study, we evaluate the role of adenosine in
SIRS
-mediated
lymphopenia
and impaired IL-15 production. Cecal ligation and puncture was used to induce sepsis-associated
SIRS
in mice. BMDCs were cultured and used to measure the effect of adenosine on IL-15. We found that A
1
R mRNA levels were significantly down-regulated and A
1
R-dependent G
i
activity was abolished in T cells of septic mice. In accordance, cAMP was elevated in isolated T cells from cecal ligation and puncture compared with sham-treated mice. Similar to septic mice, leukopenia was evident in sham A
1
R-KO mice, after treatment with the A
1
R antagonist (8-cyclopentyl-1,3-dipropylxanthine), or after A
1
R desensitization. In contrast, A
2A
R-KO mice were protected from leukopenia. In addition, we observed that septic A
1
R-KO mice exhibited low IL-15 levels. Cultured BMDC agonists of A
2A
R and A
2B
R inhibited IL-15 production and adenosine blocked IL-15-dependent proliferation of cytotoxic T cells that were cocultured with stimulated BMDCs. To conclude, we suggest that
SIRS
-associated
lymphopenia
is initiated by A
1
R desensitization and adenosine-mediated inhibition of IL-15 production is part of the mechanism that accounts for the delay in leukopenia recovery in patients with severe sepsis. Interference with adenosine signaling may thus be potentially beneficial for septic patients with leukopenia.
...
PMID:Systemic inflammatory response syndrome-related lymphopenia is associated with adenosine A
1
receptor dysfunction. 2849 90
