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Pivot Concepts:
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Target Concepts:
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Query: UMLS:C0038002 (
splenomegaly
)
9,873
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A
Brucella canis
infection, causing recurrent fever with so-called granulomatous hepatitis and
splenomegaly
, was detected serologically in a 30-year-old female patient. The disease originated in an infected dog from Greece which also showed a high titre. Following successful initial treatment with cotrimoxazole and streptomycin the disease broke out again on two further occasions. The infection was finally cured by 4-months continuous cotrimoxazole treatment after which the
Brucella canis
titre dropped from 1:1280 to 1:40 and then to zero. The patient has been symptom-free for the last two years.
...
PMID:[Brucella canis infection in man]. 394 Aug 31
Brucella canis
infects dogs and humans. In dogs, it can cause reproductive failure; in humans, it can cause fever, chills, malaise, peripheral lymphadenomegaly, and
splenomegaly
. B. canis infection in dogs is underrecognized. After evaluating serologic data, transmission patterns, and regulations in the context of brucellosis in dogs as an underrecognized zoonosis, we concluded that brucellosis in dogs remains endemic to many parts of the world and will probably remain a threat to human health and animal welfare unless stronger intervention measures are implemented. A first step for limiting disease spread would be implementation of mandatory testing of dogs before interstate or international movement.
...
PMID:Brucellosis in Dogs and Public Health Risk. 3001 31
Canine brucellosis
, caused by
Brucella canis
, is a disease of dogs and represents a public health concern as it can be transmitted to humans.
Canine brucellosis
is on the rise in the United States and there is currently no vaccine for use in dogs. Mice have been extensively utilized to investigate host-pathogen interactions and vaccine candidates for smooth Brucella species and could serve a similar role for studying B. canis. However, comparatively little is known about B. canis infection in mice. The objective of this study was to characterize the kinetics of colonization and pathogenicity of B. canis in mice in order to evaluate the mouse as a model for studying this pathogen. C57BL/6 mice were inoculated intraperitoneally with 105, 107, or 109 CFU of
Brucella canis
RM6/66 and euthanized 1-, 2-, 4-, 6-, 9-, and 12-weeks post-inoculation. B. canis induced
splenomegaly
in mice infected with 109 CFU at 1- and 2 weeks post-inoculation while no gross lesions were observed in other dose groups. Infection at the two higher doses resulted in dose-dependent granulomatous hepatitis and histiocytic infiltration of the spleen and mesenteric lymph nodes by 1-2 weeks. B. canis was cultured from the liver, spleen, uterus, bone marrow, lung, and kidney in all groups with colonization declining at a slow but steady rate throughout the experiment. Clearance was achieved by 9 weeks 105 CFU group and by 12 weeks in the 107 CFU group, while B. canis persisted in the spleen until 12 weeks in the highest dose group. Although B. canis does not demonstrate significant replication in C57BL/6 mice, it has the ability to establish an infection, induce
splenomegaly
, and persist for several weeks in multiple organs. Moreover, 1 x 107 CFU appears to be a suitable challenge dose for investigating vaccine safety.
...
PMID:Characterization of Brucella canis infection in mice. 3122 Jan 85
