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==Diagnosis==
 
==Diagnosis==
 
===Clinical Signs===
 
===Clinical Signs===
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The main route of infection in field cases is oronasal
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by direct or indirect contact with infected pigs or by
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feed which is contaminated with virus, e.g., swill. In
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areas with a high density of pigs, virus spread easily
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occurs between neighbouring pig holdings (Fritzemeierj
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et al., 2000). Disease transmission via the
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semen of infected boars may also occur (Floegel
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et al., 2000). The incubation period in individual
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animals is about one week to 10 days. Under field
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conditions, symptoms may only become evident in a
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holding 2–4 weeks after virus introduction, or even
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later (Laevens et al., 1999). The severity of clinical
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signs mainly depends on the age of the animal and
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the virulence of the virus, and in older breeding pigs
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the course of the infection is often mild or subclinical.
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The virulence of a CSF virus isolate is difficult
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to determine on a rational basis (Mittelholzer
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et al., 2000), as the same CSF virus isolate can cause
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different forms of CSF depending on age, breed and
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immune status of the host animal (Floegel-Niesmann
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et al., unpublished observation).
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Acute, chronic and prenatal forms of CSF can be
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distinguished, and there is no array of classical
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symptoms that is invariably associated with the disease.
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Piglets up to 12 weeks of age most often display
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the acute form. A constant finding is pyrexia, usually
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higher than 40 �C, but in adults the temperature
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may not exceed 39.5 �C. Initial signs are anorexia,
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lethargy, conjunctivitis, enlarged and discoloured
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lymph nodes, respiratory signs and constipation
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followed by diarrhoea. Neurological signs are frequently
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seen, such as a staggering gait with weakness
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of hind legs, incoordination of movement, and
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convulsions (Fig. 1). The typical haemorrhages of
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the skin are usually observed on the ear, tail, abdomen
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and the inner side of the limbs during the
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second and third week after infection until death.
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The virus is shed from the infected animal by saliva,
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urine and faeces (Depner et al., 1994; Laevens et al.,
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1999).
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Pathological changes visible on post mortem examination
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are observed most often in lymph nodes,
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spleen and kidneys. The lymph nodes become swollen,
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oedematous and haemorrhagic (Fig. 2). Haemorrhages
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of the kidney may vary in size from petechiae
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to ecchymotic haemorrhages. Petechiae can also be
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observed in the urinary bladder, larynx, epiglottis and
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heart, and may be widespread over the serosae of the
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abdomen and chest. A non-purulent encephalitis is
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often present (Gruber et al., 1995).
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CSF virus causes severe leukopenia and immunosuppression,
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which often leads to secondary
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Fig. 1. Neurological signs of CSF. The back is hunched
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up and the hind legs are pushed under the abdomen.
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Wasting and haemorrhages on ears and hind legs are
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visible.
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Fig. 2. Swollen lymph nodes of the small intestine and
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necrosis of the ileocaecal valve (centre).
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12 THE VETERINARY JOURNAL, 165, 1
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enteric or respiratory infections. The signs of these
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secondary infections can mask or overlap the most
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typical signs of CSF and may mislead the veterinarian
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(Depner et al., 1999).
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In general, the acute form of African swine fever
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leads to a very similar clinical and pathological picture.
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CSF must also be considered in the differential
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diagnosis of erysipelas, porcine reproductive and
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respiratory syndrome (PRRS), cumarin poisoning,
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purpura haemorragica, post-weaning multisystemic
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wasting syndrome (PWMS), porcine dermatitis and
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nephropathy syndrome (PDNS), Salmonella or
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Pasteurella infections or any enteric or respiratory
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syndrome with fever not responding to antibiotic
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treatment.
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With increasing age of the infected pigs (fattening
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and breeding animals) the clinical signs are less
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specific and recovery with production of antibodies
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can occur. Antibodies against CSF virus become
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detectable 2–3 weeks postexposure to CSF virus
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(Laevens et al., 1998).
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CHRONIC COURSE OF CLASSICAL SWINE
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FEVER VIRUS INFECTION
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The chronic form of CSF is always fatal. It develops
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when pigs are not able to mount an effective immune
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response against the infection. Initial signs
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are similar to die acute infection. Later, predominantly
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non-specific signs are observed, e.g. intermittent
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fever, chronic enteritis and wasting. Animals
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may survive for 2–3 months before they die. CSF
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virus is shed from the onset of clinical signs constantly
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until death. Antibodies may be temporarily
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detected in serum samples, as the immune system
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starts to produce antibodies although they are not
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able to eliminate the virus from the host. Consequently
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the antibodies are neutralised by the virus
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and cease to be detectable (Depner et al., 1996).
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Pathological changes are less typical, especially the
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lack of haemorrhages on organs and serosae. In
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animals displaying chronic diarrhoea, necrotic and
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ulcerative lesions on the ileum, the ileocaecal valve
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and the rectum are common. Since clinical signs of
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chronic CSF are rather non-specific, a broad range
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of other diseases must be considered as part of any
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differential diagnosis.
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PRENATAL COURSE OF INFECTION AND
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LATE ONSET OF DISEASE
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Although the course of infection in the sow is often
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subclinical, CSF virus is able to cross the placenta of
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pregnant animals, thereby infecting fetuses during
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all stages of pregnancy. The outcome of transplacental
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infection of fetuses mainly depends on the
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time of gestation and viral virulence, respectively.
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Infection during early pregnancy may result in
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abortions and stillbirths, mummification and malformations.
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All of this will lead to a reduction in the
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fertility index in the holding.
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Infection of sows from about 50–70 days of pregnancy
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can lead to the birth of persistently viraemic
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piglets, which may be clinically normal at birth and
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survive for several months. After birth, theymay show
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poor growth, wasting or occasionally congenital tremor.
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This course of infection is referred to as �late
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onset CSF�. These piglets constantly shed large
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amounts of virus and are a dangerous virus reservoir,
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spreading the disease and maintaining the infection
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within the pig population (Van Oirschot and Terpstra,
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1977). This situation is comparable to cattle
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persistendy infected with BVD virus.
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CSF must be considered in the differential diagnosis
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of reduced fertility due to parvovirus infection,
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PRRS, leptospirosis and Aujeszky�s disease.
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===Laboratory Tests===
 
===Laboratory Tests===
 
===Pathology===
 
===Pathology===
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