Analysis Tools
mortality/aging
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• homozygotes begin to die within a few weeks after birth
• Background Sensitivity: homozygotes display a higher death rate on a 129/Sv background, with ~80% dying within 6 weeks
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• homozygotes display a sharp decline in postnatal survival during the first 3 weeks after birth
• survival can extended for a few days by draining the chylous effusion by thoracocentesis
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respiratory system
chylothorax
(
J:71816
)
|
• homozygotes with respiratory distress exhibit congenital chylothorax
|
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• mutant pleural tissues are filled by chylous effusion and lungs become compressed
|
|
• homozygotes typically exhibit signs of respiratory distress at P6 and die 2 days later
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• homozygotes die from respiratory failure due to compression of lungs by chyle
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cardiovascular system
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• homozygotes exhibit upregulation of Egr1 (an immediate early gene implicated in vascular stenosis) in restricted parts of the thoracic vasculature, in the atrial wall of the heart at E16.5, in pulmonary arteries at E18.5 and in lung arteries after birth
• Egr1 dysfunction may be associated with obstructions that ultimately affect the lymphatics
|
immune system
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• homozygotes with a developing chylothorax show extremely dilated thoracic lymphatic vessels while pericardial and chest skin lymphatic vessels remain unaffected
• notably, dilated thoracic lymphatics are observed as early as E16.5, prior to the onset of respiratory distress and chylothorax
• no signs of edema or inflammation surrounding the lymphatics are observed
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behavior/neurological
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• homozygotes become physically inactive prior to death
|
homeostasis/metabolism
chylothorax
(
J:71816
)
|
• homozygotes with respiratory distress exhibit congenital chylothorax
|
Mouse Models of Human Disease |
DO ID | OMIM ID(s) | Ref(s) | |
| congenital chylothorax | DOID:0060646 |
OMIM:603523 |
J:71816 | |
