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 Is the replacement of a diseased liver with a healthy liver allograft.  Used technique is orthotopic transplantation, in which the native liver is.

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Presentation on theme: " Is the replacement of a diseased liver with a healthy liver allograft.  Used technique is orthotopic transplantation, in which the native liver is."— Presentation transcript:

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2  Is the replacement of a diseased liver with a healthy liver allograft.  Used technique is orthotopic transplantation, in which the native liver is removed and replaced by the donor organ in the same anatomic location as the original liver.  Liver transplantation nowadays is a well accepted treatment option for end-stage liver disease and acute liver failure.

3 The first human liver transplant was performed in 1963 by a surgical team led by Dr. Thomas Starzl of Denver, Colorado, United States.Thomas StarzlDenver, ColoradoUnited States The first short-term success was achieved in 1967 with the first one-year survival post transplantation. Despite the development of viable surgical techniques, liver transplantation remained experimental through the 1970s, with one year patient survival in the vicinity of 25%.

4  The introduction of ciclosporin by Sir Roy Calne markedly improved patient outcomes,ciclosporinRoy Calne  in 1980s saw recognition of liver transplantation as a standard clinical treatment for both adult and pediatric patients with appropriate indications.  Liver transplantation is now performed at over one hundred centers in the USA, as well as numerous centres in Europe and elsewhere. One-year patient survival is 80– 85%, and outcomes continue to improveUSA

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6  Fulminant hepatic failure  Complications of cirrhosis Ascites Encephalopathy Synthetic dysfunction Liver cancer Refractory variceal hemorrhage Chronic gastrointestinal blood loss due to portal hypertensive  Systemic complications of chronic liver disease Hepatopulmonary syndrome Portopulmonary hypertension  Liver-based metabolic conditions causing systemic disease Primary oxaluria Familial amyloidosis 1-antitrypsin deficiency Wilson’s disease Urea cycle enzyme deficiencies Glycogen storage disease Tyrosemia

7 Absolute  Active extrahepatic malignancy  Hepatic malignancy with macrovascular or diffuse tumor invasion  Active and uncontrolled infection outside of the hepatobiliary system  Active substance or alcohol abuse  Severe cardiopulmonary or other comorbid conditions  Psychosocial factors that would likely preclude recovery after transplantation  Technical and/or anatomical barriers  Brain death

8  Age  Cholangiocarcinoma  Portal vein thrombosis  Chronic or refractory infections  Human immunodeficiency virus infection  Previous malignancy  Active psychiatric illness  Poor social support

9  Deceased donor brain dead cardiac dead  Living donor right lobe left lobe left lateral segment posterior sector graft

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11 Parameter1 Point2 Points3 Points EncephalopathyNoneGrade 1-2Grade 3-4 AscitesNoneMedically controlled Uncontrolled Albumin, g/dL>3.52.8-3.5< 2.8 Bilirubin, mg/dL < 22-3> 3 International normalized ratio < 1.71.7-2.3>2.3

12  MELD score = 0.957 x Log e (creatinine mg/dL) + 0. 378 x Log e (bilirubin mg/dL) + 1.120 x Log e (INR) + 0.643.  MELD >14 is an indication for liver transplantation  Its used for patient listing

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14  Liver will regenerate up to 80% of its size after 14 days of removing 70 % of its mass.

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16  ICU care  Following LT, the function of the new liver is monitored closely in an ICU setting. Elevations of liver enzymes, notoriously transaminases (ie, aspartate aminotransferase, alanine aminotransferase), early on are reflective of preservation injury (cold preservation). On occasion, these enzyme levels rise sharply. If they are higher than 2000, the overall viability function of the liver should be monitored carefully to assess the need for retransplantation.

17  Usually, the liver enzyme levels normalize very quickly, typically within a week of transplantation. The bilirubin level follows a similar pattern of early rise and delayed clearing. However, if the preservation injury is severe, this elevation can persist for 2-3 weeks and can be accompanied by a significant rise in alkaline phosphatase levels.

18  Platelet counts usually decrease in the first week after LT and recover during the second week. This may be caused by platelet sequestration in the liver and spleen due to preservation injury. Once the liver has recovered, as manifested by the return of bilirubin to normal levels, the platelet count increases.  Recovery in a typical patient is rapid, as is discharge to the floor, usually within 2-3 days.  However, if the graft has suffered severe preservation injury, return to normality may lag..

19  Treatment is mostly supportive, with the goal of maintaining stable hemodynamics while the liver recovers. In extreme cases, termed primary graft nonfunction, the new liver never recovers and urgent retransplantation is required

20  After the patient's medical condition has stabilized and graft function is stable, he or she is transferred from the ICU to the floor transplant unit. At this time, tests are performed to assure adequacy of the new connections.  A duplex Doppler ultrasound helps check for patency of the vascular anastomoses and the presence of abnormal fluid collections. leaks.

21  During the patient's stay on the floor unit, his or her laboratory studies, medications, nutritional status, and exercise tolerance are monitored. As soon as patients are able, discharge instructions begin to prepare them for going home.  Most patients with severe ESLD have a very low albumin level prior to transplantation. After successful LT, the albumin level slowly rises to normal levels. This explains the generalized edema that patients may experience following transplantation, which begins to disappear once albumin levels start to normalize.

22  Patients should be kept on lifelong immunosuppressant to prevent rejection.

23 – Bacterial; related to procedure → pneumonia; - biliary sepsis; wound infection; - catheter related, c. difficile PMC – Viral: HSV stomatitis, - HCV, Hepatitis B, if without prophylaxis – Fungal: Pneumocystis, - Aspergillus, Cryptococcus, - Hystoplasma, Coccidioides, – Parasites: Toxoplasma, - Strongyloides, Leishmania, - Trypanosoma

24 Allograft dysfunction: – PNF in first two weeks – Acute cellular rejection – Small-for-size Syndrome Biliary tract: – Bile leaks – Anastomosis disruption – Hepatic duct stricture/hepatic artery thrombosis Disease recurrence

25  Rejection (acute and chronic)  Post transplant lymphoprolifrative disorder

26  Xenotransplantation  hepatocyte cell transplantation  use of bioartificial liver devices (ie, extracorporeal liver-assist devices).

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