Gene expression patterns in the progression of canine copper-associated chronic hepatitis

Dirksen, Karen; Spee, Bart; Penning, Louis C.; Ingh, T.S.G.A.M. van den; Burgener, Iwan; Watson, Adrian; Koerkamp, Marian J. A. Groot; Rothuizen, J.; Steenbeek, Frank G. van; Fieten, Hille

doi:10.1371/journal.pone.0176826

Cited by 17 publications

(16 citation statements)

References 97 publications

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“…Serum concentrations of TGFβ‐1 were increased in dogs with moderate‐to‐severe hepatic fibrosis . Increased TIMP‐1 mRNA expression also has been demonstrated in liver from dogs with CH …”

Section: Pathogenesismentioning

confidence: 91%

Hepatic Fibrosis in Dogs

Eulenberg

Lidbury

2017

Veterinary Internal Medicne

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Hepatic fibrosis is commonly diagnosed in dogs, often as a sequela to chronic hepatitis (CH). The development of fibrosis is a crucial event in the progression of hepatic disease that is of prognostic value. The pathophysiology of hepatic fibrosis in human patients and rodent models has been studied extensively. Although less is known about this process in dogs, evidence suggests that fibrogenic mechanisms are similar between species and that activation of hepatic stellate cells is a key step. Diagnosis and staging of hepatic fibrosis in dogs requires histopathological examination of a liver biopsy specimen. However, performing a liver biopsy is invasive and assessment of fibrotic stage is complicated by the absence of a universally accepted staging scheme in veterinary medicine. Serum biomarkers that can discriminate among different fibrosis stages are used in human patients, but such markers must be more completely evaluated in dogs before clinical use. When successful treatment of its underlying cause is feasible, reversal of hepatic fibrosis has been shown to be possible in rodent models and human patients. Reversal of fibrosis has not been well documented in dogs, but successful treatment of CH is possible. In human medicine, better understanding of the pathomechanisms of hepatic fibrosis is leading to the development of novel treatment strategies. In time, these may be applied to dogs. This article comparatively reviews the pathogenesis of hepatic fibrosis, its diagnosis, and its treatment in dogs.

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Section: Pathogenesismentioning

confidence: 91%

Hepatic Fibrosis in Dogs

Eulenberg

Lidbury

2017

Veterinary Internal Medicne

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“…metallothionein 1A is upregulated in high copper conditions but down-regulated in chronic hepatitis. Gene expression analysis also demonstrates up-regulation of amyloid precursor protein genes in high copper chronic hepatitis and up-regulation of COMMD1 in early disease (Dirksen et al 2017).…”

Section: Hepatic Diseasementioning

confidence: 93%

“…Gene expression analysis also demonstrates up‐regulation of amyloid precursor protein genes in high copper chronic hepatitis and up‐regulation of COMMD1 in early disease (Dirksen et al . ).…”

Section: Larger Mammal Modelsmentioning

confidence: 97%

Animal models of Wilson disease

Reed

Lutsenko²,

Bandmann

2018

Journal of Neurochemistry

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Wilson disease (WD) is an autosomal recessive disorder of copper metabolism manifesting with hepatic, neurological and psychiatric symptoms. The limitations of the currently available therapy for WD (particularly in the management of neuropsychiatric disease), together with our limited understanding of key aspects of this illness (e.g. neurological vs. hepatic presentation) justify the ongoing need to study WD in suitable animal models. Four animal models of WD have been established: the Long-Evans Cinnamon rat, the toxic-milk mouse, the Atp7b knockout mouse and the Labrador retriever. The existing models of WD all show good similarity to human hepatic WD and have been helpful in developing an improved understanding of the human disease. As mammals, the mouse, rat and canine models also benefit from high homology to the human genome. However, important differences exist between these mammalian models and human disease, particularly the absence of a convincing neurological phenotype. This review will first provide an overview of our current knowledge of the orthologous genes encoding ATP7B and the closely related ATP7A protein in C. elegans, Drosophila and zebrafish (Danio rerio) and then summarise key characteristics of rodent and larger mammalian models of ATP7B-deficiency.

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“…A urina, após centrifugação por 10 min a 1.500 rpm, não mudou de cor e nem demonstrou sedimento significativo. No hemograma observou-se anemia macrocítica hipocrômica com policromasia e anisocitose (eritrócitos 1,52 x10 6 /µL [5,[5][6][7][8]5 Nos rins, havia um material grosseiramente granular e vermelho-alaranjado obstruindo parcial ou totalmente grande parte dos túbulos renais (cilindros de hemoglobina) (Figura 4B). No interior de muitos desses túbulos notava-se grande quantidade de células epiteliais necróticas, caracterizadas por citoplasma encolhido, homogêneo e fortemente eosinofílico, contendo núcleos compostos por cromatina condensada (picnose) ou fragmentos nucleares (cariorrexia).…”

Section: Casounclassified

“…A intoxicação por cobre tem sido relatada tanto em humanos como em animais, principalmente na espécie ovina, a mais suscetível e frequentemente acometida [7,11,12]. Em cães, as manifestações clinicopatológicas da intoxicação por cobre são caracterizadas, basicamente, por um quadro de insuficiência hepática crônica, fazendo da crise hemolítica, tão comum em ovinos intoxicados por cobre, uma síndrome raramente associada à intoxicação na espécie canina, existindo apenas ocasionais descrições na literatura veterinária a cerca dessa manifestação [2,3,6,11,17]. O objetivo deste relato é descrever um caso de crise hemolítica em um cão com hepatite crônica associada ao cobre.…”

Section: Introductionunclassified

Vaginal Squamous Cell Carcinoma in a Nelore cow

Paula

Pupin

2019

Acta Scientiae. Vet.

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Background:Copper is an essential micronutrient for the body to function properly. However, although it is a vital element, an excess of copper in the body is extremely toxic. Copper toxicity has been reported mainly in sheep. In dogs, clinicopathological signs of toxicity are characterized by chronic liver failure. This means that the hemolytic crisis so common in sheep is a condition rarely associated with toxicity in dogs, so there are very few descriptions of this condition in the veterinary literature. The purpose of this report is to describe a case of hemolytic crisis in a dog with copper-associated chronic hepatitis. Case: A medium-sized 6-year-old bitch was brought to the Veterinary Hospital of the Federal University of Santa Maria, with clinical presentation of apathy, anorexia and red urine. A physical examination revealed mildly jaundiced mucosa and dark brown urine. A urinalysis indicated the presence of protein, bilirubin and occult blood. The blood count revealed hypochromic macrocytic anemia, leukocytosis due to left shift neutrophilia and thrombocytopenia. Serum biochemistry showed elevated levels of alanine aminotransferase and alkaline phosphatase. The animal was given a blood transfusion due to the severity of her anemia, but her clinical condition worsened and she died, whereupon her body was sent for necropsy. This necropsy revealed conspicuous signs of jaundice, splenomegaly and altered liver and kidney color. The liver was brownish, with its natural surface firm and slightly irregular. The kidneys were diffusely blackened. The urine was dark brown. Fragments of different organs were collected, fixed in 10% buffered formalin solution, routinely processed for histopathology and stained with hematoxylin and eosin. A histological dissection of the liver showed the hepatic lobes dissected by fibrosis, forming islands of hepatocytes and numerous lymphocytes and plasmocytes. Brown granular pigment was observed in periportal hepatocytes. Perls Prussian blue and rubeanic acid staining techniques were performed to characterize this pigment.

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Gene expression patterns in the progression of canine copper-associated chronic hepatitis

Cited by 17 publications

References 97 publications

Hepatic Fibrosis in Dogs

Hepatic Fibrosis in Dogs

Animal models of Wilson disease

Vaginal Squamous Cell Carcinoma in a Nelore cow

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