Difference between revisions of "Cholangitis, Lymphocytic"
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− | Also known as: | + | |
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+ | {| cellpadding="10" cellspacing="0" border="1" | ||
+ | | Also known as: | ||
+ | | '''Lymphocytic-plasmacytic cholangitis<br> | ||
+ | '''Cholangiohepatitis''' | ||
+ | |||
+ | '''Lymphocytic portal hepatitis''' | ||
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+ | '''Non-suppurative cholangitis''' | ||
+ | |-} | ||
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+ | |||
+ | ==Description== | ||
+ | '''Lymphocytic cholangitis''' is a slowly progressive chronic disease characterised by infiltration of the portal areas of the liver with inflammatory cells, mostly [[Lymphocytes|lymphocytes]] and [[B cell differentiation - WikiBlood#Plasma cells|plasma cells]]. Bile duct hypertrophy and [[Liver Fibrosis|fibrosis]] are present. However, lymphocytic cholangitis does not progress to biliary [[Cirrhosis|cirrhosis]]. An immune-mediated aetiology has been postulated but this has not been substantiated to date. It is rarely associated with [[Pancreatitis - Dog and Cat|pancreatitis]], compared to [[Cholangitis, Neutrophilic]] | ||
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==Signalment== | ==Signalment== | ||
− | Young to middle-aged cats, 50% are under 4 years old. | + | Young to middle-aged cats, 50% are under 4 years old. |
+ | |||
==Diagnosis== | ==Diagnosis== | ||
===Clinical Signs=== | ===Clinical Signs=== | ||
History of chronic waxing and waning low-grade illness. | History of chronic waxing and waning low-grade illness. | ||
− | Vague clinical signs which may include anorexia, depression, weight loss, intermittent [[ | + | Vague clinical signs which may include anorexia, depression, weight loss, intermittent [[Stomach and Abomasum Consequences of Gastric Disease - Pathology|vomiting]] and [[Diarrhoea|diarrhoea]], [[Icterus|jaundice]],lymphadenomegaly. Severe illness and pyrexia is less likely compared to [[Cholangitis, Neutrophilic]]. |
− | Some cats in the UK are polyphagic and are frequently presented with ascites and/or jaundice. | + | Some cats in the UK are polyphagic and are frequently presented with ascites and/or jaundice. |
+ | |||
===Laboratory Tests=== | ===Laboratory Tests=== | ||
====Haematology==== | ====Haematology==== | ||
− | [[Neutrophilia|Neutrophilia]] is less common than with [[Cholangitis, Neutrophilic]] | + | [[Changes in Inflammatory Cells Circulating in Blood - Pathology#Neutrophilia|Neutrophilia]] is less common than with [[Cholangitis, Neutrophilic]] |
====Biochemistry==== | ====Biochemistry==== | ||
Increased alkaline phosphatase (ALP), alanine aminotransferase (ALT), Hyperbilirubinaemia and Hyperglobulinaemia. | Increased alkaline phosphatase (ALP), alanine aminotransferase (ALT), Hyperbilirubinaemia and Hyperglobulinaemia. | ||
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===Diagnostic Imaging=== | ===Diagnostic Imaging=== | ||
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====Ultrasonography==== | ====Ultrasonography==== | ||
Ultrasonography is more helpful. Biliary tract dilation can be seen in all cases. Common bile duct is normally dilated and the [[Gall Bladder - Anatomy & Physiology|gall bladder]] may also be dilated with "sludge". Main differential is extrahepatic biliary obstruction. | Ultrasonography is more helpful. Biliary tract dilation can be seen in all cases. Common bile duct is normally dilated and the [[Gall Bladder - Anatomy & Physiology|gall bladder]] may also be dilated with "sludge". Main differential is extrahepatic biliary obstruction. | ||
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===Histopathology=== | ===Histopathology=== | ||
Liver biopsy is important to rule out [[Feline Infectious Peritonitis|Feline Infectious Peritonitis]] . It is vital to obtain a haemostasis profile prior to biopsy due to risk of prolonged coagulation with liver disease. It is unnecessary to obtain a bile sample unless the presentation is acute, in which case [[Cholangitis, Neutrophilic]] needs to be ruled out. | Liver biopsy is important to rule out [[Feline Infectious Peritonitis|Feline Infectious Peritonitis]] . It is vital to obtain a haemostasis profile prior to biopsy due to risk of prolonged coagulation with liver disease. It is unnecessary to obtain a bile sample unless the presentation is acute, in which case [[Cholangitis, Neutrophilic]] needs to be ruled out. | ||
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==Treatment== | ==Treatment== | ||
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Antibiotic may be given at early stages of treatment until an infectious cause has been ruled out. | Antibiotic may be given at early stages of treatment until an infectious cause has been ruled out. | ||
− | + | Ursodeoxycholic acid may be given as it has hepatoprotective (anti-inflammatory, immunomodulatory and antifibrotic effects) properties and choleretic effect. The latter promotes increased fluidity of biliary secretions for treating or preventing sludging. Additionally antioxidants such as S-adenosylmethionine and vitamin E can be given to counteract the potent oxidising property of bile. | |
+ | |||
==Prognosis== | ==Prognosis== | ||
Poor due to the waxing and waning feature of this disease. In cats, this disease does not usually progress to end-stage cirrhosis and therefore it does not usually result in death, which is in contrast to dogs. | Poor due to the waxing and waning feature of this disease. In cats, this disease does not usually progress to end-stage cirrhosis and therefore it does not usually result in death, which is in contrast to dogs. | ||
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==References== | ==References== | ||
Ettinger, S.J. and Feldman, E. C. (2000) '''Textbook of Veterinary Internal Medicine Diseases of the Dog and Cat Volume 2''' (Fifth Edition) ''W.B. Saunders Company''. | Ettinger, S.J. and Feldman, E. C. (2000) '''Textbook of Veterinary Internal Medicine Diseases of the Dog and Cat Volume 2''' (Fifth Edition) ''W.B. Saunders Company''. | ||
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Nelson, R.W. and Couto, C.G. (2009) '''Small Animal Internal Medicine (Fourth Edition)''' ''Mosby Elsevier''. | Nelson, R.W. and Couto, C.G. (2009) '''Small Animal Internal Medicine (Fourth Edition)''' ''Mosby Elsevier''. | ||
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Marks, S.L. (2003). '''Update on the Diagnosis and Management of Feline Cholangiohepatitis''' ''Waltham Feline Medicine Symposium''. | Marks, S.L. (2003). '''Update on the Diagnosis and Management of Feline Cholangiohepatitis''' ''Waltham Feline Medicine Symposium''. | ||
− | + | [[Category:Gall_Bladder_and_Tract_-_Pathology]][[Category:To_Do_-_Caz]] | |
− | + | [[Category:Cat]][[Category:Dog]] | |
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− | [[Category:Gall_Bladder_and_Tract_-_Pathology]] | ||
− | [[Category: | ||
− | [[Category: |
Revision as of 12:08, 23 July 2010
This article is still under construction. |
Description
Lymphocytic cholangitis is a slowly progressive chronic disease characterised by infiltration of the portal areas of the liver with inflammatory cells, mostly lymphocytes and plasma cells. Bile duct hypertrophy and fibrosis are present. However, lymphocytic cholangitis does not progress to biliary cirrhosis. An immune-mediated aetiology has been postulated but this has not been substantiated to date. It is rarely associated with pancreatitis, compared to Cholangitis, Neutrophilic
Signalment
Young to middle-aged cats, 50% are under 4 years old.
Diagnosis
Clinical Signs
History of chronic waxing and waning low-grade illness. Vague clinical signs which may include anorexia, depression, weight loss, intermittent vomiting and diarrhoea, jaundice,lymphadenomegaly. Severe illness and pyrexia is less likely compared to Cholangitis, Neutrophilic. Some cats in the UK are polyphagic and are frequently presented with ascites and/or jaundice.
Laboratory Tests
Haematology
Neutrophilia is less common than with Cholangitis, Neutrophilic
Biochemistry
Increased alkaline phosphatase (ALP), alanine aminotransferase (ALT), Hyperbilirubinaemia and Hyperglobulinaemia.
Diagnostic Imaging
Radiography
Radiographic signs are non specific. Hepatomegaly due to enlargement of biliary ducts and in some cases ascites is also seen.
Ultrasonography
Ultrasonography is more helpful. Biliary tract dilation can be seen in all cases. Common bile duct is normally dilated and the gall bladder may also be dilated with "sludge". Main differential is extrahepatic biliary obstruction.
Histopathology
Liver biopsy is important to rule out Feline Infectious Peritonitis . It is vital to obtain a haemostasis profile prior to biopsy due to risk of prolonged coagulation with liver disease. It is unnecessary to obtain a bile sample unless the presentation is acute, in which case Cholangitis, Neutrophilic needs to be ruled out.
Treatment
- Immunosuppressives
Glucocorticoid at initial immunosuppressive dose for 6-12 weeks. This should be tapered gradually to alternate day dosing. However, recurrence is common following initial amelioration of clinical signs. Response to therapy is hard to assess due to the slowly progressive nature of this disease. A persistent rise in ALT and/or increasing total serum bilirubin indicates an inadequate control of the disease.
Azathioprine has been trialled but this is not recommended due to its side effects which include inappetence and leucopaenia. Methotrexate at low weekly dose has also been used in a few affected cats.
Antibiotic may be given at early stages of treatment until an infectious cause has been ruled out.
Ursodeoxycholic acid may be given as it has hepatoprotective (anti-inflammatory, immunomodulatory and antifibrotic effects) properties and choleretic effect. The latter promotes increased fluidity of biliary secretions for treating or preventing sludging. Additionally antioxidants such as S-adenosylmethionine and vitamin E can be given to counteract the potent oxidising property of bile.
Prognosis
Poor due to the waxing and waning feature of this disease. In cats, this disease does not usually progress to end-stage cirrhosis and therefore it does not usually result in death, which is in contrast to dogs.
References
Ettinger, S.J. and Feldman, E. C. (2000) Textbook of Veterinary Internal Medicine Diseases of the Dog and Cat Volume 2 (Fifth Edition) W.B. Saunders Company. Nelson, R.W. and Couto, C.G. (2009) Small Animal Internal Medicine (Fourth Edition) Mosby Elsevier. Marks, S.L. (2003). Update on the Diagnosis and Management of Feline Cholangiohepatitis Waltham Feline Medicine Symposium.
Also known as: | Lymphocytic-plasmacytic cholangitis Cholangiohepatitis Lymphocytic portal hepatitis Non-suppurative cholangitis |