Ductal Plate Malformation in the Liver of Boxer Dogs

Author:

Pillai S.1,Center S. A.2,McDonough S. P.3,Demarco J.4,Pintar J.4,Henderson A. K.4,Cooper J.5,Bolton T.6,Sharpe K.7,Hill S.8,Benedict A. G.9,Haviland R.10

Affiliation:

1. Comparative and Genomic Pathology at Memorial Sloan Kettering Cancer Center, Laboratory of comparative pathology, New York, NY, USA

2. Department of Clinical Sciences, College of Veterinary Medicine, Cornell University, Ithaca, NY, USA

3. Department of Biomedical Sciences, College of Veterinary Medicine, Cornell University, Ithaca, NY, USA

4. Garden State Veterinary Specialists, Tinton Falls, NJ, USA

5. Tuft’s Veterinary Emergency Treatment and Specialities, Walpole, MA, USA

6. Internal Medicine Resident, Department of Veterinary Medicine and Biomedical Sciences, Texas A&M University, College Station, TX, USA

7. Blue Pearl Specialty and Emergency Medicine for Pets, Grand Rapids, MI, USA

8. Veterinary Specialty Hospital, San Diego, San Diego, CA, USA

9. VCA Shoreline Veterinary Referral and Emergency Center, Shelton, CT, USA

10. South Carolina Veterinary Specialists, Columbia, SC, USA

Abstract

Ductal plate malformations (DPMs) represent developmental biliary disorders with a wide phenotypic spectrum. This study characterizes DPM in 30 Boxer dogs. Median age was 1.5 (range, 0.3–10.0) years, with 12 dogs <1 year. Clinical features included increased serum levels of liver enzymes (28), gastrointestinal signs (16), poor body condition (14), abdominal effusion (9), and hepatic encephalopathy (2). Additional malformations included gallbladder atresia (8), atrophied left liver (2), absent quadrate lobe with left-displaced gallbladder (1), portal vasculature atresia (left liver, 1), intrahepatic portosystemic shunt (1), and complex intrahepatic arteriovenous malformation (1). All dogs had portal tracts dimensionally expanded by a moderate-to-severe multiple small bile duct phenotype embedded in abundant extracellular matrix; 80% displayed variable portal-to-portal bridging. Quantitative analysis confirmed significantly increased fibrillar collagen and a 3-fold increased portal tract area relative to 6 Boxer and 10 non-Boxer controls. Biliary phenotype was dominated by tightly formed CK19-positive ductules, typically 10 to 15 μm in diameter, with 3 to >30 profiles per portal tract, reduced luminal apertures, and negative Ki-67 immunoreactivity. CK19-positive biliary epithelium intersected directly with zone 1 hepatocytes as a signature feature when considered with other DPM characteristics. Phenotypic variation included a multiple small bile duct phenotype (all dogs), predominantly thin-walled sacculated ducts (4), well-formed saccular ducts (4), and sacculated segmental, interlobular, and intralobular ducts (Caroli malformation, 2 dogs, one with bridging portal fibrosis). Histologic evidence of portal venous hypoperfusion accompanied increased biliary profiles in every case. We propose that this spectrum of disorders be referred to as DPM with appropriate modifiers to characterize the unique phenotypes.

Publisher

SAGE Publications

Subject

General Veterinary

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