The pancreas has two separate functions within the body, often referred to as the exocrine and endocrine pancreata. The endocrine pancreas secretes hormones, including insulin and glucagon, which regulate blood glucose metabolism. The exocrine pancreas secretes zymogens and active enzymes that, ultimately, aid in digestion. Exocrine pancreatic insufficiency (EPI) is a condition of maldigestion and usually doe not involve the endocrine pancreas. In this article, we review the etiologic factors, diagnostic tools, and management recommendations for dogs with EPI.
NORMAL EXOCRINE PANCREATIC FUNCTION
Carbohydrate digestion is facilitated by pancreatic amylase secretion, which hydrolyzes most carbohydrates into disaccharides and some trisaccharides. Finally, the exocrine pancreas facilitates fat digestion by releasing the enzymes pancreatic lipase, cholesterol esterase, and phospholipase and the zymogen procolipase, which is activated by trypsin to form colipase.
Exocrine pancreatic secretions contain digestive enzymes and sodium bicarbonate in an aqueous solution. Acetylcholine and cholecystokinin stimulate the release of digestive enzymes, while secretin stimulates the release of large quantities of bicarbonate and water. The digestive enzymes are produced and secreted by the pancreatic acinar cells, while epithelial cells of the pancreatic ductules secrete bicarbonate. Once within the duodenum, sodium bicarbonate neutralizes gastric secretions.1
EXOCRINE PANCREATIC INSUFFICIENCY
In patients with EPI, inadequate production of digestive enzymes by the pancreatic acinar cells leads to maldigestion and malabsorption of nutrients. The persistence of undigested food within the small intestine often results in bacterial overgrowth, further compromising intestinal function. Fortunately, the pancreas has a high reserve capacity, so signs of maldigestion do not occur until 90% of the exocrine pancreatic function is lost.2 In rare cases of EPI in people, there is selective deficiency of individual pancreatic enzymes. Isolated lipase deficiency has been described in a single dog.3
CAUSES OF EPI
Causes of EPI include pancreatic acinar atrophy, chronic pancreatitis, pancreatic hypoplasia, and neoplasia.
Pancreatic acinar atrophy
The most common cause of EPI in dogs is pancreatic acinar atrophy. The severity of this condition ranges from subclinical disease to a complete absence of secretory capacity.2 Pancreatic acinar atrophy is thought to be an immune-mediated condition that begins with lymphocytic pancreatitis.4 Selective destruction of acinar cells with replacement by atypical parenchyma, ductal structures, and adipose tissue is seen in the late stages of the disease.
Immunohistochemical analysis of pancreatic biopsy samples from dogs with subclinical EPI reveals a predominance of intra-acinar CD4+ and CD8+ T lymphocytes, supporting an immune-mediated cause.5 Other histologic characteristics include piecemeal tissue destruction, large groups of lymphocytes that resemble lymphoid follicle germinal centers, and necrotic and apoptotic acinar cell death.4
In people, most cases of EPI are secondary to chronic pancreatitis,1 but the prevalence of cases of EPI that develop secondary to chronic pancreatitis in dogs is still unclear.2 Pancreatic fibrosis can affect the islet cells of the endocrine pancreas and the acinar cells of the exocrine pancreas.2 In one study, two of four dogs with EPI resulting from chronic pancreatitis also had diabetes mellitus.6 In people and dogs with EPI resulting from chronic pancreatitis, diabetes mellitus usually precedes the development of EPI.6
A potential cause of EPI is congenital hypoplasia of the pancreas. This cause has been proposed in puppies in particular, although published data lack histologic evidence to support this theory.2,7
Rarely, pancreatic neoplasia can occlude the pancreatic duct, prohibiting release of pancreatic enzymes into the duodenum. Although the ability of the pancreatic acinar cells to produce pancreatic enzymes may not be affected, clinical signs of EPI may result.2
In a recent case report, pancreatic atrophy was described for the first time in several racing greyhound puppies. It is unclear whether environmental factors contributed to the development of EPI in these dogs or whether a true breed predisposition to this condition exists.11
The median age of dogs with EPI is variable, depending on the cause (Table 1).
Dogs with EPI present with signs of maldigestion, primarily weight loss despite an increased appetite and diarrhea or loosely formed feces. Feces are usually yellow or gray, are increased in volume, and may appear undigested or pulpy. In most cases, fecal consistency is loosely formed, but dogs may experience severe watery diarrhea initially. The diarrhea is usually accompanied by steatorrhea, flatulence, and borborygmi. Some dogs with EPI also experience vomiting. Along with the weight loss, these dogs may have a poor coat. They may also seem nervous, aggressive, or irritable as a result of abdominal discomfort.2,12,13
EPI rarely affects serum chemistry profile and complete blood count results. Amylase and lipase activities are not useful in diagnosing EPI. Occasionally, a serum chemistry profile may reveal hypocholesterolemia due to fat maldigestion. Elevation of alanine transaminase (ALT) activity has been documented uncommonly, although the cause of this is unknown. One theory is that an increased uptake of hepatotoxins occurs through the compromised small intestinal wall.2
Dogs with marked weight loss and loss of intra-abdominal fat secondary to EPI may have decreased serosal detail on abdominal radiographs. No specific ultrasonographic abnormalities have been reported in dogs with EPI.14
Pancreatic biopsies are rarely necessary for diagnosing EPI, and the results may be misleading if acinar atrophy, fibrosis, or hypoplasia is not diffuse.2 Pathologic findings within the pancreas may help you determine the cause of EPI, but a diagnosis of EPI must be based on findings from tests of pancreatic function rather than histologic appearance.
Specific diagnostic tests
A diagnosis of EPI is most reliably based on clinical signs and pancreatic function test results. The gold standard for diagnosing EPI in people is in vitro analysis of pancreatic secretions obtained from the duodenum following stimulation by cholecystokinin and secretin.15 This technique has proved to be difficult and impractical in dogs.16 The recommended test for diagnosing EPI in dogs is the canine serum trypsin-like immunoreactivity (cTLI) by radioimmunoassay.
Canine serum trypsin-like immunoreactivity. This test measures the trypsinogen that has entered the bloodstream directly from the pancreas. Enzymes that originated or were activated within the intestinal lumen are not measured, which eliminates any interference by intestinal inflammation.2 The test is also not affected by exogenous sources of pancreatic enzymes because it is species-specific.16 The reference range for cTLI is 5.7 to 45.2 µg/L, with values below 2.5 µg/L being highly diagnostic for EPI when concurrent clinical signs exist.2
Although not affected by intestinal inflammation, the cTLI test may be affected by pancreatic inflammation.6,17 Pancreatitis affecting any residual functioning acinar cells may falsely elevate cTLI concentrations.17 Dogs with EPI may have normal cTLI concentrations in the presence of kidney disease because trypsinogen is renally excreted.2,18 The cTLI concentrations could be normal in animals with EPI secondary to pancreatic duct obstruction.16 Postprandial samples may also result in falsely elevated cTLI results.2,18 Thus, the sample should be obtained in a patient that has been fasted for 12 to 18 hours, and the sample should be nonhemolyzed. Despite these potential interferences, the cTLI test is considered 100% sensitive and specific for EPI with results below 1.9 µg/L.16
Canine TLI testing by radioimmunoassay is available through commercial laboratories such as the Texas A&M University College of Veterinary Medicine's Gastrointestinal Laboratory, Antech Diagnostic Laboratory, or Idexx Laboratories. An in-house ELISA test kit to detect cTLI has been investigated.19
Serum pancreatic lipase immunoreactivity. Serum pancreatic lipase immunoreactivity (PLI), used to detect pancreatitis, is also a sensitive test for diagnosing EPI. Unfortunately, poor specificity makes it inferior to the cTLI test for this purpose.20 The newest version of the PLI test, the Spec cPL Test (Idexx Laboratories), has been optimized for diagnosing pancreatitis but may not be useful for diagnosing EPI. In general, all available forms of pancreatic lipase testing should be used for diagnosing pancreatitis rather than pancreatic insufficiency.
Fecal pancreatic elastase 1. Fecal pancreatic elastase 1 is a zymogen produced exclusively within pancreatic acinar cells.21 It survives intestinal transit unchanged and is unaffected by intestinal inflammation.21 An ELISA test for fecal pancreatic elastase 1 (Elastase 1 Canine—ScheBo Biotech AG) in dogs is available and is marketed as a screening tool for EPI. A fecal pancreatic elastase 1 value < 10 µg/g feces indicates a diagnosis of EPI. Values > 40 µg/g feces indicate normal exocrine pancreatic function, while values between 10 and 40 µg/g feces are borderline results. In borderline cases, further testing is recommended.22 This test is species-specific, so it is unaffected by pancreatic enzyme supplementation. Fecal pancreatic elastase 1 measurement has been used extensively in diagnosing EPI in people.21
Other tests. Several tests for EPI have been rendered nearly obsolete by the advent of the cTLI test. These include tests for fecal proteolytic activity, which should be low in dogs with EPI, including the x-ray film method, the azocasein method, and the radial enzyme diffusion method.2,16 The bentiromide test, also known as the serum n-benzoyl-L-tyrosine-p-aminobenzoic acid test (BT-PABA), is an indirect method of assessing the presence of chymotrypsin in the blood.16-18,23
Other tests that are no longer actively used include the starch tolerance test, the D-xylose absorption test, and the oral fat absorption test.21 None of these tests are as sensitive and specific as the cTLI test for diagnosing EPI.
As previously discussed, clinical EPI does not result until 90% of the secretory capacity of the exocrine pancreas is lost. Mild decreases in pancreatic function have been detected in clinically normal dogs. This condition has been termed subclinical EPI and may reflect partial pancreatic acinar atrophy. In affected dogs, repeated cTLI results fall between 2.5 and 5 µg/L; a single subnormal value is not diagnostic for subclinical EPI.2 In one study, 20 of 35 (57%) of dogs with subnormal results had normal cTLI concentrations when retested.23 Further, the detection of reduced pancreatic function should not be mistaken for progressive disease. The length of the subclinical phase is highly variable, and some dogs never develop clinical EPI.24
Dogs with borderline fasting cTLI results can be further tested by using the TLI stimulation test, in which cTLI is measured before and after pancreatic stimulation.23 Food is usually used for pancreatic stimulation. Endogenous stimulation by intravenous administration of cholecystokinin and secretin has also been effective experimentally in one study.23 A diagnosis of EPI is confirmed if there is no response to stimulation. Dogs with subclinical EPI typically have low fasting cTLI results but normal post-stimulation results.23,24
Dogs with subclinical EPI do not require treatment. In cases of suspected pancreatic acinar atrophy, the efficacy of immunosuppressive therapy has been studied in hopes of slowing or preventing the development of clinical EPI. Because of the unpredictable progression of subclinical EPI, the use of immunosuppressive medications is not recommended.2,24
Pancreatic enzyme replacement
The mainstay of treatment in dogs with clinical EPI of any cause is pancreatic enzyme replacement. Commercially available preparations are generally derived from porcine pancreas and contain lipase, amylase, and protease for digestion of fats, carbohydrates, and proteins, respectively. The veterinary products come in powdered and uncoated tablet forms (e.g. Viokase-V—Fort Dodge Animal Health; Pancrezyme—Virbac Animal Health), and products approved for use in people are available in all forms and can be used instead if needed. Alternatively, chopped, raw bovine or porcine pancreas can be fed directly.
Pancreatic enzyme supplementation doses are listed in Table 2. Patients that respond poorly to supplementation may improve with dose increases, alternate forms of enzyme replacement, incubation of food with enzymes for 20 to 30 minutes before feeding, or concurrent administration of H2 blockers.2 Theoretically, H2 blockers such as cimetidine or famotidine would reduce gastric acidity and better preserve the enzymes for intestinal use.12 Administration of these drugs could begin during initiation of treatment in all dogs or may be reserved for those with suboptimal response to treatment. Given the cost of treatment, pancreatic enzyme dose reduction can be attempted. Some dogs have been managed adequately with a 50% dose reduction.13
Pancreatic enzyme supplementation may cause gastrointestinal distress (including diarrhea, cramping, and nausea) at high doses.27 Additionally, oral ulceration and bleeding have been reported, presumably the result of digestive enzymes contacting the oral mucosa. Ulcerations may be alleviated by reducing the dose28,29 or by incubating the enzymes in the food for longer periods.28
Alternative sources of pancreatic enzymes have been investigated. Fungal lipase, derived from Aspergillus species, is acid-resistant, so it survives gastric transit but, unfortunately, is deactivated by proteases and bile acids within the small intestine, making it inferior to traditional supplementation.30,31 Bacterial lipase, derived from Burkholderia plantarii, survives gastric and intestinal transit. It has been proved to correct steatorrhea more effectively than porcine pancreatic enzyme supplements and requires much lower doses.30,32 Bacterial-derived enzymes may be ideal for treating EPI, but high cost and reduced availability may limit their use.
Dietary modification may improve clinical signs in dogs with EPI. In most cases, trial and error is needed to discern the appropriate diet for a patient.33 In people with EPI, high-fat diets are used to maximize weight gain.34 This type of diet may be helpful in dogs, but it can worsen diarrhea and may increase the requirement for enzyme supplementation.33 In most cases, a moderate-fat diet is recommended.2 Low-fat diets have not been shown to improve clinical signs over moderate-fat diets.13
Replacing diets rich in long-chain fatty acids with those containing more medium-chain fatty acids, such as Purina Veterinary Diet EN (Nestlé Purina), also does not seem to improve clinical signs, although this may increase intestinal absorption of cholesterol and fat-soluble vitamins, which can be decreased in patients with EPI.35 High-fiber diets are generally not recommended because they increase fecal mass, are poorly digestible, and can inhibit the absorption of other nutrients.33 However, some dogs can show improvement in fecal firmness and a decrease in flatulence and borborygmi when receiving high-fiber diets.33 Finally, hydrolyzed protein diets have resulted in improved body condition in some dogs with EPI.36
We typically recommend initiating therapy with an easily digestible diet such as Purina Veterinary Diet EN or Iams Veterinary Formula Intestinal—Low-Residue (Iams). If no response is seen, the dosage of pancreatic enzyme supplementation is usually adjusted before alternative diets are used. In general, treats are not recommended since it is impractical to administer enzyme supplementation with each treat to aid in digestion. If clients insist upon giving treats, we recommend waiting until signs of EPI are well-controlled.
EPI should be included in the differential list for any dog with small bowel diarrhea. With the advent of more sensitive and specific testing, EPI has become relatively simple for clinicians to diagnose. Treatment is generally rewarding but can be expensive and may present a management challenge in certain cases. Given the multitude of concurrent and secondary diseases that develop, it is also important to remain open to these possible conditions even after EPI has been diagnosed (see the sidebar titled "Canine EPI: Concurrent and secondary diseases").
Jessica A. Morgan, DVM
Lisa E. Moore, DVM, DACVIM
Affiliated Veterinary Specialists
9905 South U.S. Highway 17/92
Maitland, FL 32751
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