cirrhosis

CIRRHOSISDr akhondei

cirrhosis

Cirrhosis is a pathologically defined entity that is associated with a spectrum of characteristic clininical manifestation

1-Irreversible chronic injury of the hepatic parenchyma

2-Extensive fibrosis 3-formation of regenerative

nodules

Normal liver

Cirrhosis of the liver is the third leading cause of death in people between the ages of 25 and 65 years, exceeded only by cardiovascular disease and cancer.

The cost of cirrhosis in terms of human suffering, financial burden, and loss of productive life is devastating.

Patients with cirrhosis may present in a variety of ways.

Variceal bleeding New onset of ascites Hepatomegaly and/or splenomegaly


Incidental Discovery Of Abnormal Laboratory Tests

Serum Aminotransferases, Hypoalbuminemia, Prolonged Prothrombin Time, Hrombocytopenia)


Detection of the peripheral stigmata ofchronic liver disease such as

Jaundice, Dupuytren's contracture, Manifestations related to hyperestrogenemia

such as o Spider angiomata, o Palmar erythema,o Gynecomastia, and testicular atrophy which

may also be related to low testosterone concentrations


hepatic encephalopathy or one or more complications or systemic manifestations of hepatocellular carcinoma

Some patients never come to clinical attention. In older reviews, cirrhosis was diagnosed at autopsy in up to 30 to 40 percent of patients

Cirrhosis represents the terminal stage of a number of chronic liver diseases including those caused by

excessive ethanol consumption Viral hepatitis Drugs and toxins, Vascular Autoimmune Metabolic disorders Cryptogenic. In some cases, no cause can be determined and the cirrhosis is

Early cirrhosis may be asymptomatic and undetectable except by biopsy.

However, by the time cirrhosis becomes clinically apparent, hepatic functional reserve is markedly impaired.

If liver injury cannot be arrested, the prognosis without intervention is poor

The onset of complications (eg, ascites, encephalopathy, variceal

hemorrhage) indicates a more advanced stage of disease and a poorer prognosis, with median survival of about 5 years or less.

CIRRHOSIS & PORTAL HYPERTENSION

CIRRHOSIS

Term was 1st coined by Laennec in 1826

Many definitions but common theme is injury, repair, regeneration and scarring

NOT a localized process; involves entire liver

Primary histologic features:1. Marked fibrosis2. Destruction of vascular & biliary elements3. Regeneration4. Nodule formation

Cirrhosis: Pathophysiology

Primary event is injury to hepatocellular elements

Initiates inflammatory response with cytokine release->toxic substances

Destruction of hepatocytes, bile duct cells, vascular endothelial cells

Repair thru cellular proliferation and regeneration

Formation of fibrous scar


Primary cell responsible for fibrosis is stellate cell

Become activated in response to injury and lead to ed expression of fibril-forming collagen

Above process is influenced by Kupffer cells which activate stellate cells by eliciting production of cytokines

Sinusoidal fenestrations are obliterated because of ed collagen and EC matrix synthesis


Prevents normal flow of nutrients to hepatocytes and increases vascular resistance

Initially, fibrosis may be reversible if inciting events are removed

With sustained injury, process of fibrosis becomes irreversible and leads to cirrhosis

Causes of Cirrhosis

Alcohol Viral hepatitis Biliary obstruction Veno-occlusive disease Hemochromatosis Wilson’s disease Autommune Drugs and toxins Metabolic diseases Idiopathic

Classification of Cirrhosis

WHO divided cirrhosis into 3 categories based on morphological characteristics of the hepatic nodules

1. Micronodular2. Macronodular3. Mixed

Micronodular Cirrhosis

Nodules are <3 mm in diameter Relatively uniform in size Distributed throughout the liver Rarely contain portal tracts or efferent

veins Liver is of uniform size or mildly

enlarged Reflect relatively early disease

Macronodular & Mixed Cirrhosis Nodules are >3 mm in diameter and vary

considerably in size Usually contain portal tracts and efferent

veins Liver is usually normal or reduced in size Mixed pattern if both type of nodules are

present in equal proportions

Cirrhosis - Alcohol

Also known as Laennec’s cirrhosis >50% of pts. with alcoholic cirrhosis die

within 4 yrs of diagnosis Develops in only 10% to 30% of heavy

drinkers Morphologically, micronodular pattern Multifactorial - genetic, nutritional, drug

use and viral

Cirrhosis - Alcohol

Fatty liver, alcoholic hepatitis Histology - megamitochondria, Mallory

bodies, inflammation, necrosis, fibrosis Key mediator is acetaldehyde (ADH), the

product of alcohol metabolism by alcohol dehydrogenase

ADH directly activates stellate cells, inhibits DNA repair and damage microtubules

NAFLD/NASH

Nonalcoholic Fatty Liver Disease and Steatohepatitis

Becoming more common Infiltration of the liver with fat ±

inflammation Pathologically similar to alcoholic liver but

in absence of alcohol Associated with obesity, hyperlipidemia,

NIDDM,

Viral Hepatitis

Most common cause of cirrhosis worldwide (>50% of cases)

Incidence of cirrhosis in Hepatitis B pts. is 1% and 10% in Hepatitis C pts.

Incidence increases to 70-80% in HBV +ve pts. who are superinfected with HDV

DIAGNOSIS

Can be asymptomatic for decades History Physical findings: Hepatomegaly,

jaundice, ascites, spider angioma, splenomegaly, palmar erythema, fetor hepaticus, purpura etc.

Elevated LFTs, thrombocytopenia,

DIAGNOSIS

Definitive diagnosis is by biopsy or gross inspection of liver

Noninvasive methods include US, CT scan, MRI

Indirect evidence - esophageal varices seen during endoscopy

Manifestations of Cirrhosis

Hepatorenal syndrome Hepatic encephalopathy Portal hypertension Water retention Hematologic Hepatocellular carcinoma

Portal Hypertension (PH)

Portal vein pressure above the normal range of 5 to 8 mm Hg

Portal vein - Hepatic vein pressure gradient greater than 5 mm Hg (>12 clinically significant)

Represents an increase of the hydrostatic pressure within the portal vein or its tributaries

Pathophysiology of PH

Cirrhosis results in scarring (perisinusoidal deposition of collagen)

Scarring narrows and compresses hepatic sinusoids (fibrosis)

Progressive increase in resistance to portal venous blood flow results in PH

Portal vein thrombosis, or hepatic venous obstruction also cause PH by increasing the resistance to portal blood flow

Pathophysiology of PH

As pressure increases, blood flow decreases and the pressure in the portal system is transmitted to its branches

Results in dilation of venous tributaries Increased blood flow through collaterals

and subsequently increased venous return cause an increase in cardiac output and total blood volume and a decrease in systemic vascular resistance

With progression of disease, blood pressure usually falls

Portal Vein Collaterals Coronary vein and short gastric veins ->

veins of the lesser curve of the stomach and the esophagus, leading to the formation of varices

Inferior mesenteric vein -> rectal branches which, when distended, form hemorrhoids

Umbilical vein ->epigastric venous system around the umbilicus (caput medusae)

Retroperitoneal collaterals ->gastrointestinal veins through the bare areas of the liver

Etiology of PH

Causes of PH can be divided into1. Pre-hepatic

2. Intra-hepatic

3. Post-hepatic

Pre-hepatic PH

Caused by obstruction to blood flow at the level of portal vein

Examples: congenital atresia, extrinsic compression, schistosomiasis, portal, superior mesenteric, or splenic vein thrombosis

Post-hepatic

Caused by obstruction to blood flow at the level of hepatic vein

Examples: Budd-Chiari syndrome, chronic heart failure, constrictive pericarditis, vena cava webs

Budd-Chiari Syndrome

Caused by hepatic venous obstruction At the level of the inferior vena cava, the

hepatic veins, or the central veins within the liver itself

result of congenital webs (in Africa and Asia), acute or chronic thrombosis (in the West), and malignancy


Acute symptoms include hepatomegaly, RUQ abdominal pain, nausea, vomiting, ascites

Chronic form present with the sequelae of cirrhosis and portal hypertension, including variceal bleeding, ascites, spontaneous bacterial peritonitis, fatigue, and encephalopathy

Diagnosis is most often made by US evaluation of the liver and its vasculature

Cross-sectional imaging using contrast-enhanced CT or MRI


Gold standard for the diagnosis has been angiography

Management has traditionally been surgical intervention (surgical decompression with a side-to-side portosystemic shunt)

Minimally invasive treatment using TIPS may be first-line therapy now

Response rates to medical therapy are poor

Portal Vein Thrombosis

Most common cause in children (fewer than 10% of adult pts.)

Normal liver function and not as susceptible to the development of complications, such as encephalopathy

Diagnosis by sonography, CT and MRI Often, the initial manifestation of portal

vein thrombosis is variceal bleeding in a noncirrhotic patient with normal liver function

Portal Vein Thrombosis - Causes Umbilical vein infection (the most common

cause in children) Coagulopathies (protein C and

antithrombin III deficiency), Hepatic malignancy, myeloproliferative

disorders Inflammatory bowel disease pancreatitis trauma Most cases in adults are idiopathic

Portal Vein Thrombosis

Therapeutic options are esophageal variceal ligation and sclerotherapy

Distal splenorenal shunt Rex shunt in patients whose intrahepatic

portal vein is patent (most commonly children)

Splenic Vein Thrombosis

Most often caused by disorders of the pancreas (acute and chronic pancreatitis, trauma, pancreatic malignancy, and pseudocysts)

Related to the location of the splenic vein Gastric varices are present in 80% of

patients Occurs in the setting of normal liver function Readily cured with splenectomy (variceal

hemorrhage), although observation for asymptomatic patients is acceptable.

Complications of PH

GI bleeding due to gastric and esophageal varices

Ascites Hepatic encephalopathy

Varices

Most life threatening complication is bleeding from esophageal varices

Distal 5 cm of esophagus Usually the portal vein-hepatic vein

pressure gradient >12 mm Hg Bleeding occurs in 25-35% of pts. With

varices and risk is highest in 1st yr.

Prevention of Varices

Primary prophylaxis: prevent 1st episode of bleeding

Secondary prophylaxis: prevent recurrent episodes of bleeding

Include control of underlying cause of cirrhosis and pharmacological, surgical interventions to lower portal pressure

Prevention of Varices

Beta blockade: Beta blockade (Nadolol, Propranolol)

Nitrates:Organic nitrates Surgery: No longer performed*

Endoscopy: Sclerotherapy (no longer used*) and variceal ligation

* Refers to primary prophylaxis

Treatment of Varices

Initial Management:1. Airway control2. Hemodynamic monitoring3. Placement of large bore IV lines4. Full lab investigation (Hct, Coags, LFTs,)5. Administration of blood products6. ICU monitoring

Pharmacologic Treatment of Varices Decreases the rate of bleeding Enhances the endoscopic ability to

visualize the site of bleeding Vasopressin - potent splanchnic

vasoconstrictor; decreases portal venous blood flow and pressure

Somatostatin: decrease splanchnic blood flow indirectly; fewer side effects

Octreotide: Initial drug of choice for acute variceal bleeding

Endoscopic Therapy for Varices Endoscopic Sclerotherapy: complications

occur in 10-30% and include fever, retrosternal chest pain, dysphagia, perforation

Endoscopic variceal ligation: becoming the initial intervention of choice; success rates range from 80-100%

Balloon Tamponade

Sengstaken-Blakemore tube Minnesota tube Alternative therapy for pts. who fail

pharmacologic or endoscopic therapy Complications: aspiration, perforation,

necrosis Limited to 24 hrs; works in 70-80%

TIPS

Transjugular inrahepatic portasystemic shunt

1st line treatment for bleeding esophageal varices when earlier-mentioned methods fail

Performed in IR Success rates 90-100% Significant complication is hepatic

encephalopathy

Surgical Intervention

Liver transplantation: only definitive procedure for PH caused by cirrhosis

Shunts Totally diverting (end-side portacaval) Partially diverting (side-side portacaval) Selective (distal splenorenal shunt)

Devascularization

Severe complications

such as spontaneous bacterial peritonitis or ascites that is refractory to diuretic therapy, occur in the most advanced disease and are associated with a median life expectancy of less than 1 year.

Cirrhosis, even if early and stable, predisposes to development of primary hepatocellular carcinoma in as many as 3% of patients per year.

Until recently, little could be done to alter the prognosis of patients with cirrhosis and most died of complications. Today, the outlook has begun to change because of advances in orthotopic liver transplantation and development of therapies to prevent and treat complications.

Biologic Basis of hepatic fibrosis

Hepatic fibrosis is a wound-healing

response The same cell type produce hepatic

fibrosis regardless of the underling cause.

hepatic fibrosis follows chronic,but not self-limited,injury.

Fibrosis occurs earliest in regions where injury is most severe.

Antifibrotic therapies :Rationale and specific Agent

The paradigm of satellite cell activation provides an important framework to define potential sites of antifibrotic therapy follows

1.Cure the primary disease to prevent injury.

2.Reduce inflammation or the host response to avoid stimulating satellite cells.

3.Directly down –regulate stellate cell activation

Antifibrotic therapies :Rationale and specific Agent

4.Neutralize the proliferative,fibrogenic,contractile,and proinflammatory responses of stellate cells.

5.Stimulate apoptosis of stellate cells. 6.Increase the degradation of scar

martix,either by stimulating cells that produce matrix proteases,down-regulating their inhibitors ,or directly administering matrix proteases.

DIAGNOSTIC APPROACH

Unless the diagnosis is already established, specific serologic tests and often a liver biopsy are required to establish the cause of the cirrhosis .

DIAGNOSTIC APPROACH

In addition, patients should undergo laboratory testing to document the severity of the disease and assessment of whether ascites or hepatic encephalopathy is present ..

DIAGNOSTIC APPROACH

Obtaining this information helps to determine prognosis, the possibility of specific therapy, and the possible necessity for screening family members for inherited diseases or chronic viral hepatitis

specific therapy may be indicated

Antiviral therapy for chronic hepatitis C and B,

Corticosteroids (with or without immunosuppressive therapy) for autoimmune hepatitis,

Phlebotomy for hereditary hemochromatosis,

Penicillamine for Wilson's disease.

In some cases, even hepatic fibrosis can be reversed; examples include abstinence from alcohol in alcoholic liver disease and immunosuppressive therapy in autoimmune hepatitis

30 - 50 Years30 - 50 Years

Progression of Hepatitis B Infection

Short-termShort-termInfectionInfection

Long-termLong-termHepatitisHepatitis

CirrhosisCirrhosis LiverLiverCancerCancer

DeathDeath

Long-termLong-termCarrierCarrier

ResolutionResolution

CirrhosisCirrhosis

ResolutionResolution

DeathDeath

SilentSilentCirrhosisCirrhosis

initial testing should consist of the following

Measurement of serum aminotransferases, bilirubin, alkaline phosphatase, albumin, creatinine, and sodium (otherwise unexplained hyponatremia is a marker of severe disease), the blood urea nitrogen, platelet count, and prothrombin time

.

initial testing should consist of the following

• Abdominal ultrasonography to assess the portal circulation. In one study, the severity of liver disease correlated with portal vein blood velocity as determined by ultrasound

Portal hypertension is the most common and lethal complication of chronic liver disease

Esophageal varices and hemorrhage ascites renal dysfunction hypersplenism portal-systemic encephalopathy

P H.. PPG>5mmHg

Hepatocellular carcinoma The issue of periodic surveillance of

such patients with serum alpha-fetoprotein (AFP) measurements (values above 20 µg/L being abnormal) and ultrasound examinations remains a contentious issue from the viewpoint of cost-effectiveness since an improvement in survival has not yet been demonstrate

All patients with cirrhosis should be evaluated for the presence of varices because of the beneficial effect of prophylaxis with propranolol or nadolol

Patients with most forms of cirrhosis, particularly due to hepatitis B and C, hereditary hemochromatosis, and alcoholic liver disease, are at high risk (1 to 6 percent per year) for the development of hepatocellular carcinoma

A.Cure the primary diseaseClear chronic viral infectionAbstinence from alcohol,stop toxic drugsRemove iron ,copper in overload diseaseEradicate schistosomiasisReverse biliary obstructionRevers jejunoileal bypass

Nonalcoholic steatohepatitis NASH

NASH is a disorder diagnosed by liver biopsy. The biopsy findings are indistinguishable from those of alcoholic hepatitis described above but the patient lacks a history of significant alcohol consumption. The liver disease is stable in most patients but a minority progress to cirrhosis

CIRRHOSIS & PORTAL HYPERTENSION

SURGICAL COMPLICATIONS

Turner Lisle

Resident Teaching Conference

May 2008

Cirrhosis

End result of anything that causes hepatocellular

injury Toxins, viruses, prolonged cholestasis,

autoimmunity, metabolic disorders

Pathologic response is uniform Hepatocellular necrosis Fibrosis Nodular regeneration

Cirrhosis - why do we care

Hepatic failure Portal hypertension - variceal bleeding

Ischemia & autoimmune factors thoughtto play a role, although mechanism is notclear

Anatomy

Dual blood supply Hepatic arterial Portal venous

Total hepatic blood flow ~1500 mL/min or 25% of cardiac output

Portal vein 2/3 of total hepatic blood flow

Hepatic artery >1/2 of O2

Portal Hypertension

Usually due to increased portal venous resistance

Classification based on site of increased resistance Prehepatic Intrahepatic

Prehepatic Portal HTN

Portal vein thrombosis most common Isolated splenic vein thrombosis

Usually caused by pancreatic inflammation or neoplasm

Results in gastrosplenic HTN with ensuing formation of gastric varices

Normal superior mesenteric & portal vein pressure

Easily reversed by splenectomy alone

Intrahepatic Portal HTN

Often a combination of pre-, intra-, or post-sinusoidal

Presinusoidal Schistosomiasis Nonalcoholic cirrhosis

Sinusoidal EtOH

Postsinusoidal - overall rare EtOH Budd-Chiari syndrome (hepatic vein thrombosis) Constrictive pericarditis Heart failure

Portal Hypertension

Portal pressure > 5 mmHg Portal pressure > 8 mmHg needed for

collateralization

Collateralization

Evaluation of the Cirrhotic

1) Dx of underlying liver disease2) Estimation of fxn hepatic reserve3) Definition of portal venous anatomy4) Hepatic hemodynamic evaluation5) If present, identification of site of UGI

bleeding

Evaluation of the Cirrhotic

Physical Exam Jaundice Ascites Caput medusae Asterixis Spider angiomas Palmer erythema Testicular atrophy Gynecomastia +/- Palpable spleen

(portal HTN)

Lab tests Anemia Thrombocytopenia Coagulopathy Hypoalbuminemia AST/ALT Bili Alk Phos GGT Hepatitis serologies -fetoprotein

Liver biopsy

Cause of cirrhosis Activity of liver disease Approaches

Percutaneous (avoid with ascites or INR) Transjugular venous Laparoscopic Open

Hepatic Functional Reserve

CHILD-PUGH Encephalopathy grade Amount of ascites Bilirubin Albumin PT (INR)

Operative mortality A (5%) B (10-15%) C (25%)

Subjective……

MELD Bilirubin INR Creatinine Cr Max = 4.0 mg/dL On dialysis → calculate

with CR = 4.0 mg/dL

Calculators on the web

MELD 5-201% increase in mortality with each integer rise inMELD score

MELD >20Additional 2% increase in mortality with each integerrise in MELD score

Diagnosis of bleeding

NGT decompression & lavage Endoscopy - key procedure for UGIB UGIB with portal HTN

90% due to varices 10% other causes (Mallory-Weiss tears, ulcers,

etc) Majority are esophagogastric varices Isolated gastric varices

Likely splenic vein thrombosis

Variceal Hemmorrhage

Single most life threatening complication of portal HTN

Risk of death is related to the underlying hepatic functional reserve

Pathogenesis of rupture incompletely understood Multifactorial Portal pressure >12mmHg

Treatment Control the bleeding Control the portal HTN

Treatment of acute variceal bleeding

Emergency tx should be non-operative Resuscitation first Endoscopy

Successful in >85% Pharmacotherapy

Vasopressin +/- NTG Somatostatin/Octreotide (fewer complications)

Balloon tamponade (rare) TIPS

Endoscopic treatment

Most common treatment modality for acute bleeding as well as prevention

Sclerosis Ligation Complications

Esophageal ulceration Perforation Worsening hemorrhage Aspiration

Failure after two unsuccessful attempts

•Equally efficacious (80-90%)

•Potentially lethal complications

•as pharmacotherapy and endoscopy

•Has been shown to be as effective

•-esophageal perforation•-ischemic necrosis of esophagus

•May be life saving

•Deflation followed by

•high re-bleeding rate

•Sengstaken-Blakemore tube

TIPS

Portal decompression without surgery (nonselective shunt)

Not recommended as initial therapy for acute variceal bleeding

Preferred tx when pharmacotherapy and endoscopic means have failed

Best when used as a bridge to transplant Problems include shunt stenosis/occlusion,

encephalopathy (50% at 1-year)

•Transjugular Intrahepatic Portosystemic Shunt

Emergency surgery Indications

Failure of acute endoscopic tx Failure of TIPS placement Hemorrhage from gastric varices

Esophageal transection rapid/simple Portacaval shunt or splenorenal shunt Operative mortality >25% in most series

Prevention of recurrent hemorrhage

Likelihood of repeat episodes >70% Goals

Prevention of recurrent bleeding Maintenance of satisfactory hepatic function

Options Pharmacotherapy (-blockers +/- nitrates) Chronic endoscopy (successful in 2/3) TIPS (less bleeding, more encephalopathy) Operative shunts Transplantation

Portosystemic shunts

Most effective means of preventing recurrent bleeding in patients with portal hypertension

Problems Encephalopathy Accelerated hepatic failure

Types Nonselective - End-to-end/side portocaval Selective - Distal splenorenal Partial - Small diameter PTFE

Nonshunt procedures

Objectives Ablation of varices Extensive interruption of collateral vessels

Options Transection and reanastamosis of the distal

esophagus Extensive esophagogastric devascularization +

esophageal transection and splenectomy

Rebleeding rates similar to endoscopicexperience

Ascites Usually an indicator of advanced cirrhosis Initiated by altered hepatic and splanchnic

hemodynamics Intravascular volume deficit resulting in

increased aldosterone….. Central goal is to achieve a NEGATIVE

sodium balance

Ascites treatment

Dietary restriction Dietary restriction + Diuretics

spironolactone +/- lasix 5-10% are refractory

Intermittent paracentesis TIPS Peritoneovenous “Denver” shunt (rarely used)

SBP PMN >250/mm3 or positive culture

Encephalopathy

Variety of manifestations Pathogenesis - circulating cerebral toxins

Ammonia Mercaptans -aminobutyric acid

Precipitated by multiple factors Shunts, hemorrhage, excessive diuresis, azotemia,

infection, increased dietary protein, sedatives Management

Eliminate/treat precipitating factors Lactulose, neomycin (decrease absorption of intestinal

ammonia)

Questions

cirrhosis

Documents

cirrhosis isearly cirrhosis

time cirrhosis

cost of cirrhosis

percent of patients

liver injury

variety of ways

irreversible chronic

hrombocytopenia patients