Difference between revisions of "Lymphangiectasia"

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==Description==
 
==Description==
'''Lymphangiectasia''' is a disease of the intestinal [[Lymphatic Vessels - Anatomy & Physiology|lymphatic vessels]] that results in the leakage of protein-rich [[Lymph - Anatomy & Physiology|lymph]] into the intestinal lumen, producing a [[Protein Losing Enteropathy|protein-losing enteropathy]](PLE) and severe lipid malabsorption.   
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'''Lymphangiectasia''' is a disease of the [[Lymphatic Vessels - Anatomy & Physiology|lymphatic vessels]] that results in the leakage of protein-rich [[Lymph - Anatomy & Physiology|lymph]].  The term is taken to mean intestinal lymphangiectasia (in which lymph is lost into the intestinal lumen, producing a [[Protein Losing Enteropathy|protein-losing enteropathy]](PLE) and severe lipid malabsorption) but thoracic and generalised lymphangiectasia have been reported.   
  
Lymphangiectasia can be classified into primary or secondary disease.  '''Primary lymphangiectasia''' usually only affects the intestine but it occasionally involve a concurrent [[Chylous Effusion|chylothorax]].  It occurs due to a congenital defect of the lymphatic vessels but it may be associated with inflammation of the lymphatics, so-called '''lipogranulomatous lympangitis'''.  The relationship between lymphangiectasia and lipogranulomatous lymphangitis is currently unclear and it is possible that either condition could result in the development of the other.  '''Secondary lymphangiectasia''' occurs with any pathological process that causes lymphatic obstruction, of which the most common are:
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Lymphangiectasia can be classified into a primary or secondary disease.  '''Primary lymphangiectasia''' usually only affects the intestine but it occasionally involves a concurrent [[Chylous Effusion|chylothorax]].  It occurs due to a congenital defect of the lymphatic vessels but it may be associated with inflammation of the lymphatics, so-called '''lipogranulomatous lympangitis'''.  The relationship between lymphangiectasia and lipogranulomatous lymphangitis is currently unclear and it is possible that either condition could result in the development of the other.  '''Secondary lymphangiectasia''' occurs with any pathological process that causes lymphatic obstruction, of which the most common are:
*'''Inflammation''' and subsequent fibrosis of the lymphatics, obstructing the lumina of the vessels.
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*Direct damage to the lymphatics
*'''Neoplastic infiltration or erosion''' of the walls of lymphatic vessels.
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**'''Inflammation''' and subsequent fibrosis of the lymphatics, obstructing the lumina of the vessels.
*'''Obstruction of the thoracic duct''', the major lymphatic vessel that runs through the chest.  This may occur due to rupture and subsequent inflammation or due to the presence of a neoplastic mass.
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**'''Neoplastic infiltration or erosion''' of the walls of lymphatic vessels.
*'''[[Heart Failure, Right-Sided|Right-sided heat failure]]''' (including cardiac tamponade) causes an increase in central venous pressure, reducing the pressure gradient between the thoracic duct and the subclavian veins with which it anastomoses.
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**'''Obstruction of the thoracic duct''', the major lymphatic vessel that runs through the chest.  This may occur due to traumatic rupture or due to the presence of a neoplastic mass.
 
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*Increased pressure in the systemic veins reducing the pressure gradient from the thoracic duct to the subclavian veins
*caval obstruction?
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**'''[[Heart Failure, Right-Sided|Right-sided heat failure]]''' due to [[Cardiomyopathies|cardiomyopathy]], [[Cardiac Tamponade|cardiac tamponade]] or [[Tricuspid Valve Dysplasia|tricuspid dysplasia]], [[Cor Pulmonale]] or Cor Triatriatum Dexter.
*hepatic disease?
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**Obstruction to venous return by '''intra-thoracic masses''' including thymoma and thymic lymphoma.
  
 
==Signalment==
 
==Signalment==
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====Endoscopy====
 
====Endoscopy====
Grossly, multiple white lipid droplets can be seen to protrude from prominent mucosal blebs.  The mucosa is frequently oedematous.
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Grossly, multiple white lipid droplets can be seen to protrude from prominent mucosal blebs in the intestine.  The mucosa is frequently oedematous.
  
 
===Histopathology===
 
===Histopathology===
Preferably, a full thickness biopsy should be taken to achieve a definitive diagnosis.  Care should be taken as hypoproteinaemic animals are at much greater risk of dehiscence at the biopsy sites, potentially leading to an acute septic peritonitis.  On histological examination of the biopsy sample, accumulation of lipid-laden macrophages may be detected together with a granulomatous response around distended lymphatics.
+
Preferably, a full thickness intestinal biopsy should be taken to achieve a definitive diagnosis.  Care should be taken as hypoproteinaemic animals are at much greater risk of dehiscence at the biopsy sites, potentially leading to an acute septic peritonitis.  On histological examination of the biopsy sample, accumulation of lipid-laden macrophages may be detected together with a granulomatous response around distended lymphatics.
  
 
It is essential to distinguish a true lymphangiectasia from secondary lacteal dilation that occurs with [[Inflammatory Bowel Disease|Inflammatory Bowel Disease ]] (IBD).  In the case of IBD, an inflammatory infiltrate will be seen in the lamina propria but the degree of infiltration may be underestimated if [[Oedema - Pathology|oedema]] is present.
 
It is essential to distinguish a true lymphangiectasia from secondary lacteal dilation that occurs with [[Inflammatory Bowel Disease|Inflammatory Bowel Disease ]] (IBD).  In the case of IBD, an inflammatory infiltrate will be seen in the lamina propria but the degree of infiltration may be underestimated if [[Oedema - Pathology|oedema]] is present.
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===Dietary modification===
 
===Dietary modification===
 
The diet should have a '''low fat content''' to reduce the production of lymph but should have a high calorie content to allow the animal to regain weight.  The fat soluble vitamins (K, E, D and A) should be supplemented.
 
The diet should have a '''low fat content''' to reduce the production of lymph but should have a high calorie content to allow the animal to regain weight.  The fat soluble vitamins (K, E, D and A) should be supplemented.
 
*Anecdotal report of glutamine supplementation
 
  
 
===Immunosuppressive===
 
===Immunosuppressive===

Revision as of 17:41, 20 July 2010




Description

Lymphangiectasia is a disease of the lymphatic vessels that results in the leakage of protein-rich lymph. The term is taken to mean intestinal lymphangiectasia (in which lymph is lost into the intestinal lumen, producing a protein-losing enteropathy(PLE) and severe lipid malabsorption) but thoracic and generalised lymphangiectasia have been reported.

Lymphangiectasia can be classified into a primary or secondary disease. Primary lymphangiectasia usually only affects the intestine but it occasionally involves a concurrent chylothorax. It occurs due to a congenital defect of the lymphatic vessels but it may be associated with inflammation of the lymphatics, so-called lipogranulomatous lympangitis. The relationship between lymphangiectasia and lipogranulomatous lymphangitis is currently unclear and it is possible that either condition could result in the development of the other. Secondary lymphangiectasia occurs with any pathological process that causes lymphatic obstruction, of which the most common are:

  • Direct damage to the lymphatics
    • Inflammation and subsequent fibrosis of the lymphatics, obstructing the lumina of the vessels.
    • Neoplastic infiltration or erosion of the walls of lymphatic vessels.
    • Obstruction of the thoracic duct, the major lymphatic vessel that runs through the chest. This may occur due to traumatic rupture or due to the presence of a neoplastic mass.
  • Increased pressure in the systemic veins reducing the pressure gradient from the thoracic duct to the subclavian veins

Signalment

The disease is relatively common in dogs but rare in cats. Yorkshire terriers, Rottweilers and Norwegian Lundehunds are predisposed to the development of disease.

Diagnosis

Clinical Signs

Clinical signs are related to the loss of lymph and the resultant protein-losing enteropathy and fat malabsorption. The following signs are therefore common:

  • Weight loss in the face of polyphagia due to loss of fat and protein.
  • Chronic diarrhoea or steatorrhoea, the latter occurring due to the high fat content of the faeces. The presence of large quantities of fat in the intestinal lumen provides a substrate for bacteria which produce hydroxy-fatty acids as by-products. Bacterial proliferation may result in concurrent small intestinal bacterial overgrowth (SIBO) and the hydroxy-fatty acids act as potent secretagogues in the colon, leading to the production of diarrhoeic faeces.
  • Effusions may develop for a number of reasons in animals with lymphangiectasia. Ascites composed of a transudate may develop in severely hypoproteinaemic animals but, in animals that develop secondary lymphangiectasia due to right-sided heart failure, a modified transudate may form due to portal hypertension. If the major lymphatic vessels of the abdomen are disrupted (by a neoplastic mass), chylous ascites may develop, although this is very rare. In animals with congenital lymphangiectasia or in those with disruption of the thoracic duct, chylothorax has also been described.
  • Vomiting, lethargy and anorexia are uncommon clinical signs.

Laboratory Tests

The following parameters may be altered on haematological or biochemical analysis of blood samples:

Haematology

  • Lymphopaenia occurs as lymphocytes are the major type of cell present in lymph and they are therefore lost into the intestinal lumen in large numbers.
  • If an inflammatory process (such as lipgranulomatous lymphangitis) has developed, there may be a monocytosis or neutrophilia.

Biochemistry

  • Panhypoproteinaemia occurs in most forms of protein-losing enteropathy and suggests that both plasma albumin and globulin are being lost.
  • Hypocholesterolaemia and a reduction in the circulating concentration of triglycerides occur as these nutrients are lost into the intestinal lumen.
  • Hypocalcaemia occurs due to hypoproteinaemia (reducing the total but not ionised calcium concentration) and due to vitamin D and calcium malabsorption. Hypocalcaemic tetany may be observed in animals which are severely hypocalcaemic and which then become stressed or excited.
  • Hypomagnesaemia may also develop due to malabsorption but this is rarely recognised in clinical practice.
  • Changes associated with SIBO are discussed here.
Lymphangiectasia Endoscopy- Copyright Karin Allenspach's lecture RVC

Other Tests

Further tests may be used to confirm the presence of protein-losing enteropathy, including measurement of faecal alpha-1 protease inhibitor concentration and faecal 51-Chromium albumin concentration after intra-venous injection.

Diagnostic Imaging

Ultrasonography

Ultrasound scans may reveal the presence of effusions (pleural fluid or ascites) and may be used to rule out other causes of PLE. The mucosa of affected intestinal loops may appear to be thickened and may also appear to have 'tiger stripes', although the latter finding is an unreliable indicator of lymphangiectasia.

Endoscopy

Grossly, multiple white lipid droplets can be seen to protrude from prominent mucosal blebs in the intestine. The mucosa is frequently oedematous.

Histopathology

Preferably, a full thickness intestinal biopsy should be taken to achieve a definitive diagnosis. Care should be taken as hypoproteinaemic animals are at much greater risk of dehiscence at the biopsy sites, potentially leading to an acute septic peritonitis. On histological examination of the biopsy sample, accumulation of lipid-laden macrophages may be detected together with a granulomatous response around distended lymphatics.

It is essential to distinguish a true lymphangiectasia from secondary lacteal dilation that occurs with Inflammatory Bowel Disease (IBD). In the case of IBD, an inflammatory infiltrate will be seen in the lamina propria but the degree of infiltration may be underestimated if oedema is present.

Treatment

If the lymphangiectasia is secondary to another disease, the underlying cause should be treated. Otherwise, the following elements should be considered in designing a treatment plan.

Dietary modification

The diet should have a low fat content to reduce the production of lymph but should have a high calorie content to allow the animal to regain weight. The fat soluble vitamins (K, E, D and A) should be supplemented.

Immunosuppressive

Immunosuppressive agents are a key element in the treatment of lymphangiectasia. Corticosteroids such as prednisolone are used most commonly for this pupose at an immunosuppressive dose (~2 mg/kg/day in dogs). These drugs are likely to be of most benefit in those animals that evidence of inflammatory pathology, such as lipogranulomatous lymphangitis and inflammatory infiltration of the lamina propria. If further immunosuppression is considered necessary or if adverse effects occur with corticosteroid therapy, azathioprine or ciclosporin could also be used.

Antimicrobials

Metronidazole or tylosin may be used to control any secondary SIBO. Antibiotics are thought to have effects on both the intestinal immune system and the normal enteric flora.

Fluid therapy

Short term treatment with plasma or colloids can be instituted in severely hypoproteinaemic animals that have begun to develop clinical signs. Diuretics such as frusemide and spironolactone may also be used to manage effusions.

Prognosis

The long-term prognosis is guarded as, although animals may respond to medical therapy initially, they frequently relapse and develop clinical signs associated with hypoproteinaemia.

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.
  • Hall, E.J, Simpson, J.W. and Williams, D.A. (2005) BSAVA Manual of Canine and Feline Gastroenterology (2nd Edition) BSAVA
  • Nelson, R.W. and Couto, C.G. (2009) Small Animal Internal Medicine (Fourth Edition) Mosby Elsevier.