Relationships between congenital peritoneopericardial diaphragmatic hernia or congenital central diaphragmatic hernia and ductal plate malformations in dogs and cats

Laura M. Seibert Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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Sharon A. Center Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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John F. Randolph Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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Meredith L. Miller Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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Andrew D. Miller Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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Eunju Choi Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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James A. Flanders Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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H. Jay Harvey Frpm the Departments of Clinical Sciences (Seibert, Center, Randolph, ML Miller, Flanders, Harvey) and Biomedical Sciences (AD Miller, Choi), College of Veterinary Medicine, Cornell University, Ithaca, NY 14853.

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Abstract

OBJECTIVE

To characterize the association between peritoneopericardial diaphragmatic hernia (PPDH) or congenital central diaphragmatic hernia (CCDH) and ductal plate malformations (DPMs) in dogs and cats.

ANIMALS

18 dogs and 18 cats with PPDH or CCDH and 19 dogs and 18 cats without PPDH or CCDH.

PROCEDURES

Evaluation of clinical details verified PPDH or CCDH and survival times. Histologic features of nonherniated liver samples were used to categorize DPM. Immunohistochemical staining for cytokeratin-19 distinguished bile duct profiles per portal tract and for Ki-67–assessed cholangiocyte proliferation. Histologic features of herniated liver samples from PPDH or CCDH were compared with those of pathological controls (traumatic diaphragmatic hernia, n = 6; liver lobe torsion, 6; ischemic hepatopathy, 2).

RESULTS

DPM occurred in 13 of 18 dogs with the proliferative-like phenotype predominating and in 15 of 18 cats with evenly distributed proliferative-like and Caroli phenotypes. Congenital hepatic fibrosis DPM was noted in 3 dogs and 2 cats and renal DPM in 3 dogs and 3 cats. No signalment, clinical signs, or clinicopathologic features discriminated DPM. Kaplan Meier survival curves were similar in dogs and cats. Bile duct profiles per portal tract in dogs (median, 5.0; range, 1.4 to 100.8) and cats (6.6; 1.9 to 11.0) with congenital diaphragmatic hernias significantly exceeded those in healthy dogs (1.4; 1.2 to 1.6) and cats (2.3; 1.7 to 2.6). Animals with DPM lacked active cholangiocyte proliferation. Histologic features characterizing malformative bile duct profiles yet without biliary proliferation were preserved in herniated liver lobes in animals with DPM.

CONCLUSIONS AND CLINICAL RELEVANCE

DPM was strongly associated with PPDH and CCDH. Because DPM can impact health, awareness of its coexistence with PPDH or CCDH should prompt biopsy of nonherniated liver tissue during surgical correction of PPDH and CCDH.

Abstract

OBJECTIVE

To characterize the association between peritoneopericardial diaphragmatic hernia (PPDH) or congenital central diaphragmatic hernia (CCDH) and ductal plate malformations (DPMs) in dogs and cats.

ANIMALS

18 dogs and 18 cats with PPDH or CCDH and 19 dogs and 18 cats without PPDH or CCDH.

PROCEDURES

Evaluation of clinical details verified PPDH or CCDH and survival times. Histologic features of nonherniated liver samples were used to categorize DPM. Immunohistochemical staining for cytokeratin-19 distinguished bile duct profiles per portal tract and for Ki-67–assessed cholangiocyte proliferation. Histologic features of herniated liver samples from PPDH or CCDH were compared with those of pathological controls (traumatic diaphragmatic hernia, n = 6; liver lobe torsion, 6; ischemic hepatopathy, 2).

RESULTS

DPM occurred in 13 of 18 dogs with the proliferative-like phenotype predominating and in 15 of 18 cats with evenly distributed proliferative-like and Caroli phenotypes. Congenital hepatic fibrosis DPM was noted in 3 dogs and 2 cats and renal DPM in 3 dogs and 3 cats. No signalment, clinical signs, or clinicopathologic features discriminated DPM. Kaplan Meier survival curves were similar in dogs and cats. Bile duct profiles per portal tract in dogs (median, 5.0; range, 1.4 to 100.8) and cats (6.6; 1.9 to 11.0) with congenital diaphragmatic hernias significantly exceeded those in healthy dogs (1.4; 1.2 to 1.6) and cats (2.3; 1.7 to 2.6). Animals with DPM lacked active cholangiocyte proliferation. Histologic features characterizing malformative bile duct profiles yet without biliary proliferation were preserved in herniated liver lobes in animals with DPM.

CONCLUSIONS AND CLINICAL RELEVANCE

DPM was strongly associated with PPDH and CCDH. Because DPM can impact health, awareness of its coexistence with PPDH or CCDH should prompt biopsy of nonherniated liver tissue during surgical correction of PPDH and CCDH.

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