Analysis Tools
digestive/alimentary system
|
• after 6 months, acinar cells exhibit loss of cell height, enlargement of central lumen, and failure to stain uniformly for the acinar-specific marker amylase unlike wild-type cells
|
|
• after 6 months, acinar cells exhibit increased proliferation compared to in wild-type cells
|
endocrine/exocrine glands
|
• at 7 weeks of age, mice develop regions of progressive acinar cell damage with characteristics of necrosis unlike in wild-type mice
• however, duct and islet cells are not effected
|
|
• after 6 months, acinar cells exhibit loss of cell height, enlargement of central lumen, and failure to stain uniformly for the acinar-specific marker amylase unlike wild-type cells
|
|
• after 6 months, acinar cells exhibit increased proliferation compared to in wild-type cells
|
|
• at 4 to 7 months, 24% of mice exhibit fibrotic inflammation in the pancreas unlike wild-type mice
• at 24 weeks, fibrosis in the form of collagen deposition and pancreatic stellate cell activation is evident unlike in wild-type mice
• at 1 year, 40% of mice exhibit pancreatic fibrosis
|
|
• pancreatic inflammatory infiltrate is composed of T cells, B cells, and macrophages
• mice older than 6 months exhibit chronic pancreatic inflammatory lesions
|
|
• treatment with cerulein after 1 week produces an inflammatory response in the pancreas unlike in wild-type mice
|
immune system
|
• pancreatic inflammatory infiltrate is composed of T cells, B cells, and macrophages
• mice older than 6 months exhibit chronic pancreatic inflammatory lesions
|
|
• treatment with cerulein after 1 week produces an inflammatory response in the pancreas unlike in wild-type mice
|
cellular
|
• at 7 weeks of age, mice develop regions of progressive acinar cell damage with characteristics of necrosis unlike in wild-type mice
• however, duct and islet cells are not effected
|
