AKA Pancreatic Acinar Athropy (PAA)
- Degeneration of acinar cells ccurs as a sequel to
- Starvation - loss of zymogen granules
- Maldigestion
- Obstruction of the pancreatic ducts by
- Neoplasm
- Chronic inflammation and associated fibrosis
- Foreign bodies (parasites, pancreoliths
- Specific nutritional deficiencies include: essential amino acids, zinc, copper, selenium
Clinical signs
- By the time clinical signs of exocrine pancreatic insufficiency (EPI) appear, the pancreas is usually almost totally destroyed
- Chronic diarrhoea with steatorrhoea and undigested muscle fibres. Large quantities of pale faeces are passed (due to dilution of bile pigment and the presence of undigested fats). The faeces have a characteristic rancid or cheesy odour.
- Loss of condition despite marked increase in appetite
Macroscopic appearance
- The pancreas is extremely thin and almost lace-like
- Primarily acinar tissue affected; the ducts and Islets of Langerhans are relatively normal
Microscopic appearance
- In these cases the parenchyma is replaced by atypical parenchyma and adipose tissue
- Irregular, shrunken acini composed of cells with little cytoplasm
- Some cases show a few areas of apparently normal glandular tissue or foci of cellular infiltraton which have been interpreted as suggesting degenerative changes
Aetiology
- The underlying cause is not known, possibly due to nutritional imbalances
- Chronic pancreatitis is a rare cause of EPI
- Possible hereditary EPI in GSDs and rough coated collies
Diagnosis
- Low serum trypsin-like immunoreactivity is an early, preclinical diagnostic test for EPI
Extra information for Exocrine Pancreatic Atrophy
Exocrine pancreatic atrophy in GSDs and rough coated collies: an end result of lymphocytic pancreatitis. Wiberg ME et al. Vet Path (1999) 36 530-41
- Histological changes in EPI dogs
- Histological changes in the subclinical pancreas (ie; just TLI):
- Patchy areas of normal and abnormal exocrine parenchyma
- Consistently a marked lymphoid infiltrate (lesser numbers of plasma cells seen, occasional eosinophils), starting in the border zone with gradual loss of the pancreatic parenchyma
- Mainly CD3+ T cells, with fewer CD3+ lymphocytes.
- Some lymphoid follicles (mainly B cells) scattered throughout.
- No associated increase in fibrous connective tissue
- Some intra-acinar lymphocytes seen
- As tissue destruction continued, ductal structures became more obvious
- Apoptosis seen in the acini often in normal looking acini.
- Ultrastructure
- Degenerative changes in acinar cells – dilation of rER, swelling of mitochondria, nuclear pyknosis, aptotitic bodies
- Histology of clinical EPI:
- Totally atrophied exocrine pancreas
- Some dogs had areas of normal acinar structures
- Little inflammation in the border zone
- Most of the remaining exocrine pancreas was disorganized, prominent ducts, increased amounts of adipose tissue.
- Slight increase in fibrous tissue compared to subclinical phase, but replacement with fat was more prominent than fibrosis.
- No ductular epithelial hyperplasia evident
- Ultrastructure
- Often no remaining acinar cells
- Suggests and immune-mediated destruction - ?hereditary
- Islet cells usually well preserved in the atrophied pancreas.