Page 741 - Clinical Small Animal Internal Medicine
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65  Cirrhosis and its Consequences  709

               the presence and severity of cirrhosis, but it is crucial   or idiopathic disease, specific treatment may not be
  VetBooks.ir  to  attempt to identify the underlying disease that has   possible. In all cases of cirrhosis, treatment must also
                                                                  include management of any important complications of
               resulted in the development of fibrosis/cirrhosis. This
               will allow for specific treatment to be directed at the
                                                                   Colchicine (0.03 mg/kg/day) is the only specific drug in
               underlying cause.                                  cirrhosis.
                 Due to the risk of coagulopathy in dogs with hepatic   veterinary medicine currently used to stop the formation
                 disease, coagulation testing including PT, PTT, platelet   of fibrosis. It is thought to stimulate collagenase activity,
               count, and possibly buccal mucosal bleeding time (BMBT)   increasing the breakdown and decreasing the formation
               should always be performed prior to liver biopsy.   of collagen. Colchicine is reported to have important and
               Interestingly, results of these parameters do not consist­  common side‐effects, including vomiting, diarrhea, and
               ently predict risk of bleeding after liver biopsy in human   neurologic signs. Additionally, there are no large studies
               patients with chronic liver disease. Fibrinogen concentra­  that have shown positive benefit from this medication, it
               tion should also be evaluated if possible, as it may be   has not been evaluated in cats, and it is currently cost‐
               decreased in cirrhosis. In humans, thromboelastography   prohibitive for many pet owners. As a result of these
               (TEG)    analysis can predict bleeding tendencies in cir­  problems,  most clinicians do not currently recommend
               rhotic patients, but the value of TEG in predicting bleed­  its use, even in documented cases of hepatic cirrhosis.
               ing in our canine and feline patients with liver disease is   Glucocorticoids may be beneficial in some cases of
               unknown. In cases of hypofibrinogenemia or other coagu­  cirrhosis. Steroids interact with TGF‐beta signaling
               lopathy,  transfusion with cryoprecipitate or fresh frozen   pathways and may reduce fibrotic progression, although
               plasma should be performed prior to biopsy. Vitamin K1   this  effect  may  be  relatively  weak.  More  importantly,
               therapy (1–1.5 mg/kg q12–24h for three doses) prior to   prednisone/prednisolone (1 mg/kg/day) may be useful
               biopsy may also be necessary,   especially in cats.Assessment   in inhibiting hepatic inflammation, if present. This
               of coagulation status should, however, not be a substitute   decrease in inflammation will result in decreased activ­
               for proper technique and adequate post­operative care.  ity of hepatic stellate cells, responsible for formation of
                 Biopsy may be obtained through ultrasound‐guided   further fibrosis. Glucocorticoids may be most benefi­
               “Tru‐Cut” needles, laparoscopically, or via exploratory   cial for treatment of dogs and cats with active hepatic
               laparotomy. Each method has practical advantages and   inflammation that have not yet developed fibrosis/cir­
               disadvantages when it comes to cost, time involved,   rhosis. Evidence supporting use of glucocorticoids in
               invasiveness, and availability. But collection of a wedge   the absence of hepatic inflammation is lacking, so their
               biopsy via laparoscopy or exploratory laparotomy is   use may or may not provide additional benefit in treat­
                 generally considered to be a superior method of sample   ment of cirrhosis alone. Moreover, the adverse effects
               collection. It has been shown that morphologic diagnosis   of steroids in animals with advanced fibrosis can be
               of needle biopsy specimens and wedge biopsies (consid­  very significant. Due to their ability to cause gastric
               ered the gold standard) only agreed in 40% of animals   ulceration, they should be used with extreme caution in
               with liver disease. If the “Tru‐Cut” biopsy method is   animals with , as these animals already have a compro­
                 utilized, two or more samples should be collected to   mised GI tract blood flow. Steroids cause muscle break­
               minimize sampling error. Further details on the methods   down so may also potentiate HE.Further details on the
               to collect liver tissue can be found in Chapter 60.  use of corticosteroids in dogs with chronic liver disease
                                                                  can be found in Chapter 62.
                                                                   Losartan is another medication that shows promise for
                 Treatment                                        fibrosis/cirrhosis but has not yet been evaluated for this
                                                                  purpose in small animals. Losartan is an angiotensin II
               Cirrhosis  is  considered  irreversible.  Therefore,  the   receptor antagonist that has been shown in rodent mod­
               most important aspect of treatment is addressing the   els to inhibit hepatic stellate cell activation and attenuate
               underlying cause of liver disease as early as possible to   hepatic fibrosis. It is currently utilized in veterinary
               prevent further development of fibrosis/cirrhosis, and   medicine for its effects on proteinuria. No studies have
               to minimize the risk of cirrhosis‐associated complica­  shown if losartan may be an effective therapy in prevent­
               tions. Corticosteroids have been shown to have positive   ing fibrosis development in dogs or cats.
               long‐term effects in the treatment of idiopathic chronic
                 hepatitis, and may have minor antifibrotic properties   Ascites
               (see Chapter  62). Copper‐chelating medications such
               as D‐penicillamine or trientine should be utilized in   Ascites may spontaneously improve with specific
               cases where primary copper‐associated chronic hepati­  treatment of the underlying liver disease. Reducing
               tis is diagnosed. In cases of previous toxic hepatopathy   hepatic inflammation, when present, may decrease PH
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