Shar-Pei Fever

An accumulation of excess hyaluronic acid in the upper dermis is the reason for the Shar-Pei's extremely wrinkled skin. A mutation of the hyaluronic acid synthase gene (HAS2) has resulted in its overexpression in dermal fibroblasts. In the US, ~23% of Shar-Peis are estimated to have this mutation and thus have large quantities of hyaluronic acid in their skin, resulting in extensive and thick skin folding. This hyaluronic acid can accumulate in cutaneous vesicles.

Hyaluronic acid also acts as an alarm that activates the innate immune system. It stimulates macrophages to produce excessive amounts of two cytokines: IL-1beta and IL-6. When they reach the circulation, these cytokines act on the brain to trigger a fever.

Dogs with highly folded skin are the most susceptible to developing fever syndromes. IL-1beta and IL-6 also act on hepatocytes to stimulate their production of acute phase proteins such as serum amyloid A (SAA). As a result, when hyaluronic acid escapes into their bloodstream, Shar-Peis develop episodes of fever and inflammation.

Dogs with Shar-Pei fever experience episodes of high fever that last 12–48 hours and are accompanied by arthritis, especially in the tibiotarsal joints. These episodes may occur as often as every few weeks.

SAA concentrations remain high between episodes of Shar-Pei fever, so SAA is deposited in tissues to form insoluble amyloid. Amyloid, in turn, is deposited in organs such as the kidneys, liver, spleen, GI tract, and myocardium. These amyloid deposits can result in kidney or liver failure, leading to early death.

Diagnosis of Shar-Pei fever is based on the presence of compatible clinical signs in a Shar-Pei or cross. Other causes of fever must be ruled out.

The presence of amyloid deposits can be detected in renal biopsy by staining with Congo red. The detection of these deposits is required for a definitive diagnosis of Shar-Pei fever.

A genetic test is available to identify dogs at risk for Shar-Pei fever.

Routine screening for urinary protein loss is recommended in all Shar-Peis because it may result from renal amyloidosis, an important consequence of Shar-Pei fever.

The administration of colchicine (0.025 mg/kg, PO, every 48 hours for 1 week, then every 24 hours longterm) has been recommended for the treatment of Shar-Pei fever. Although the mechanism of action for this drug has not been determined, colchicine has anti-inflammatory effects, reduces neutrophil chemotaxis, and is considered the treatment of choice for Shar-Pei fever. Azole antifungals, macrolide antimicrobials, calcium channel blockers, and P-glycoprotein pump inhibitors increase blood concentrations of colchicine, potentially causing multiorgan failure due to colchicine toxicosis. Therefore, drug interactions should be considered before any drugs are added to colchicine treatment.

Maintaining good general health is also important in treating Shar-Pei fever. Vitamin supplementation has also been recommended (1).

Corticosteroids can be used to treat severe vesicular cutaneous hyaluronosis or lymphedema.

• Dr. Linda Tintle (dedicated to the health of Chinese Shar-Pei)

• Cornell University, College of Veterinary Medicine, Animal Health Diagnostic Center: Shar-Pei Autoinflammatory Disease (SPAID)

1. Tintle LJM. Hyaluronosis, Shar-Pei autoinflammatory disease (SPAID), familial Shar-Pei fever and amyloidosis. Unpublished paper; May 2016.