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Brucellosis

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Title: Brucellosis


1
Brucellosis
  • (Malta fever, undulant fever)

2
  • Definition
  • Brucellosis is a bacterial zoonosis transmitted
    directly or indirectly to humans from infected
    animals
  • It is caused by the Brucella group of organisms,
    which are small, non motile, Gram-negative rods.
  • Its distribution is worldwide apart from the few
    countries where it has been eradicated from the
    animal reservoir.

3
  • Although Marsten described the disease first in
    1863, it is known after Bruce who described it in
    1886 and discovered B. melitensis. Later on,
    other species were discovered.

4
  • PATHOLOGY
  • Causative agents
  • Brucella group of organisms, which are small, non
    motile, Gram-negative rods.
  • Species of Brucella group of organisms
  • B. abortus is distributed   Worldwide, except for
    Japan and Northern Europe , and its Host are
    Cattle.

5
  • 2-B. melitensis is distributed in Mediterranean
    region and Middle East , and its Host are Goats,
    sheep, camel.
  • 3-B. suis is distributed in Far East, USA and its
    Host are Pigs.
  • The organisms usually gain entry into the human
    body via the mouth less frequently they may
    enter via the respiratory tract, genital tract or
    abraded skin.
  • The bacilli travel in the lymphatics and infect
    lymph nodes.

6
  • This is followed by haematogenous spread with
    ultimate localization in the reticulo-endothelial
    system.
  • Spread is usually by the ingestion of raw milk
    from infected cattle or goats, although
    occupational exposure(abbatoir workers, meat
    inspectors)is also common.
  • Person-to-person transmission is rare.

7
Clinical features
  • The incubation period of acute brucellosis is 1-3
    weeks.
  • The onset is insidious, with malaise, headache,
    weakness, generalized myalgia and night sweats.
  • The fever pattern is classically undulant,
    although continuous and intermittent patterns are
    also seen.
  • Lymphadenopathy, hepatosplenomegaly and spinal
    tenderness, sacro-iliitis (20-30) may be
    present arthritis, osteomyelitis,
    epididymo-orchitis (up to 40),
    meningoencephalitis and endocarditis have all
    been described.

8
  • Untreated brucellosis can give rise to chronic
    infection, lasting a year or more.
  • This is characterized by easy fatiguability,
    myalgia, and occasional bouts of fever and
    depression.
  • Splenomegaly is usually present.
  • Occasionally infection can lead to localized
    brucellosis. Bones and joints, spleen,
    endocardium, lungs, urinary tract and nervous
    system may be involved.
  • Systemic symptoms occur in less than one-third.

9
complications
10
  • Although several diseases have a similar
    symptomatology, prolonged pyrexia with a history
    of contact with animals or animal products and
    without any specific diagnosis should arouse a
    suspicion of brucellosis.

11
  • Diagnosis
  • Blood (or bone marrow) cultures are positive
    during the acute phase of illness in 50 of
    patients (higher in B. melitensis), but prolonged
    culture is needed.
  • In chronic disease serological tests are of
    greater value. The brucella agglutination test,
    which demonstrates a four fold or greater rise in
    titre (gt 1 in 160) over a 4-week period, is
    highly suggestive of brucellosis.

12
  • Non-agglutinating IgG and IgA molecules can block
    the agglutinating reaction (prozone phenomenon)
    and the test should be carried out to a high
    dilution to avoid this.
  • An elevated serum IgG level is evidence of
    current or recent infection a negative test
    excludes chronic brucellosis.
  • In localized brucellosis antibody titres are
    low, and diagnosis is usually established by
    culturing the organisms from the involved site.

13
  • PCR for detection of Brucella in blood gives a
    rapid diagnosis, and along with measurement of
    IgG or IgM antibodies by ELISA, are highly
    sensitive and specific.
  • Management and prevention
  • Brucellosis is treated with a combination of
    doxycycline 200 mg daily and rifampicin 600-900
    mg daily for 6 weeks, the relapse/failure rate is
    10.

14
  • Alternatively, tetracycline can be combined with
    streptomycin, which is usually given for only the
    first 2 weeks of treatment. Relapse follows such
    treatment in 510 of patients
  • Prevention and control involve careful attention
    to hygiene when handling infected animals,
    vaccination with the eradication of infection in
    animals, and pasteurization of milk.
  • No vaccine is available for use in humans.

15
Salmonellosis
  • Enteric (typhoid) fever

16
  • Bacteria of the genus Salmonella (Gram-negative,
    motile, non lactose fermenting bacilli) are
    highly adapted for growth in both humans and
    animals and cause a wide spectrum of disease.
  • The growth of serotypes S. Typhi and S.
    Paratyphi is restricted to human hosts, in whom
    these organisms cause enteric (typhoid) fever.
  • More than 200 serotypes are pathogenic to humans,
    in whom they often cause gastroenteritis and can
    be associated with localized infections and/or
    bacteremia.

17
  • AETIOPATHOGENESIS
  • Humans are the only reservoir of S. typhi.
    Organisms therefore originate from patients with
    typhoid, or from convalescent or chronic carriers
    excreting organisms in their stools.
  • Human hands, flies, or insects then transfer
    these organisms to food or drink. Since S. typhi
    survive freezing and drying, infection can also
    occur through ice or canned food. Shellfish from
    polluted waters may transmit the disease.

18
  • Typhoid bacilli traversing the small intestine
    produce little epithelial cell damage, but gain
    access to the blood stream from intestinal
    lymphatics and Peyers patches.
  • Bacilli are engulfed by reticulo-endothelial
    cells, but some multiply intra cellularly and
    then re-enter the blood stream to produce
    bacteraemia.
  • Multiplication of organisms also takes place
    regularly in the gall bladder.

19
CLINICAL FEATURES
  • The incubation period averages 10 to 14 days.
  • The onset of the disease is insidious, with
    headache, malaise, anorexia and fever.
  • The fever is intermittent, sometimes increasing
    in a step-like manner to reach a peak towards the
    end of the first week. There after it plateaus
    and remains mildly remittent (38C to 40C) for
    two to three weeks.
  • Accompanying chills are common but frank rigors
    are rare.

20
  • Headache is present and often disabling.
  • Some cases progresses to mental dullness and
    delirium.
  • Other symptoms in the early phase of the disease
    are dry cough and occasionally sore throat.
  • Abdominal discomfort with mild bloating and
    constipation also occurs, but gives way during
    the second week to diarrhoea with pea soup
    stools.
  • The spleen is usually palpable by the end of the
    first week.

21
  • The liver is mildly enlarged and tender and mild
    jaundice may be present.
  • Acute renal failure and disseminated
    intravascular coagulation(DIC) are rare
    complications. The typical rash of typhoid
    develops in the second week "Rose spots" are
    macules which occur in small crops on the chest
    and abdomen they blanch on pressure and last for
    just 2-3 days.
  • In the absence of complications, after 3-4 weeks
    the fever of typhoid disappears.

22
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23
Complications of typhoid
24
  • After clinical recovery 5-10 of patients will
    continue to excrete S. typhi for several months
    these are termed convalescent carriers.
  • Between 1 and 4 will continue to carry the
    organism for more than one year this is chronic
    carriers.
  • The usual site of carriage is the gall bladder,
    and chronic carriage is associated with the
    presence of gallstones.
  • However, in parts of the Middle East and Africa
    where urinary schistosomiasis is prevalent,
    chronic carriage of S. typhi in the urinary
    bladder is also common.

25
  • Diagnosis
  • Blood culture is the investigation of choice. In
    the first week of disease 70 to 90 of patients
    are culture-positive, but only 30 to 40 in the
    third week.
  • Occasionally only bone marrow cultures may be
    positive, when antibiotics have been given.
    However all this depends on good laboratory
    facilities.
  • Other clues to diagnosis are leucopenia of 2000
    to 4000/cumm and platelet count of under
    100,000/cumm.

26
  • Positive yields from stool and urine cultures
    increase with time and in stool is 70 by the end
    of the third week.
  • The Widal test requires the demonstration of a
    four-fold rise in serum agglutinins against the
    somatic (O) antigen of the bacillus. Titres
    against the flagellar (H) antigen are less
    specific.
  • Early antimicrobial therapy may alter the
    immunologic response.

27
  • Management
  • Increasing antibiotic resistance is seen in
    isolates of S. typhi, especially in the Indian
    subcontinent.
  • Chloramphenicol, co-trimoxazole and amoxicillin
    may all still be effective in some cases, but
    quinolones (e.g. ciprofloxacin 500 mg twice
    daily) are now the treatment of choice, although
    increased resistance to these agents is being
    seen in such cases azithromycin may be effective.

28
  • The patient's temperature may remain elevated for
    several days after starting antibiotics, and this
    alone is not a sign of treatment failure.
  • Prolonged antibiotic therapy may eliminate the
    carrier state, but in the presence of gall
    bladder disease it is rarely effective.
  • Cholecystectomy is not usually justified on
    clinical or public health grounds.

29
Prevention
  • good environmental sanitation and above all a
    ready supply of clean piped water.
  • Immunization with two doses of traditional TAB
    vaccine affords limited protection for up to one
    year and is associated with local pain and fever.
  • A live oral vaccine has been introduced which in
    three spaced doses provides protection for
    several years, but it requires refrigeration and
    a cold chain.
  • By contrast the new injectable Vi polysaccharide
    vaccine is effective for about three years in a
    single dose.
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