1. Hepatorenal Syndrome (HRS)� & HRS secrets
3. HRS - the Classical Era Treatment of ascites known since ancient times (description of paracentesis by Hippokrates)
300 B.C.: Erasitratus of Cappadocia postulates connection of ascites with liver disease
100 B.C.: Celsus recognizes the role of renal function in the pathogenesis of ascites:
Urine volume exceeds drinking volume: hope for recovery
Urine volume declines: no hope
7. Hepatorenal syndrome is a circulatory disorder
8. Milestones in HRS Pathophysiology�19th century Friedrich Theodor von Frerichs
[Clinics of Liver disease] Berlin 1858-1861:
Increased congestion of portal vein causes arterial underfilling
Arterial underfilling: responsible for decrease in urinary output
Austin Flint (1863)
Clinical report on hydro-peritoneum, based on analysis of forty-six cases. Am J Med Sci 45,306
Renal histology described as normal in all patients [!]
Patients died rapidly
No specific treatment available
9. With current treatment, renal histology is abnormal �in most patients
10. Renal comorbidities Acute tubular necrosis
Causes
Prolonged hypoperfusion
vasoconstriction
Low serum albumin
Molecular dysfunction of albumin
Hypoxia, mitochondrial damage
Radiographic contrast agents
Sepsis
Diuretic therapy
Drugs - NSAIDs, antibiotics
IgA- nephritis
11. Heyd CG (1924): The liver and its relation to chronic abdominal infection. Ann Surg 79:55-77
Helwig & Schutz (1932): A liver-kidney syndrome. Surg Gynecol Obstet 55:570-80
1950/60: landmark studies
Isolation of aldosterone 1953
Kowalski, Cardiac output in Laennec's cirrhosis, J Clin Invest 1953
Papper et al., Renal failure in Laennec‘s cirrhosis, Ann Int Med 1959
Hecker & Sherlock, Electrolyte and circulatory changes in terminal liver failure. Lancet 1956
Milestones in HRS Pathophysiology�20th century
14. Epstein M, et al. Renal failure in the patient with cirrhosis. The role of active vasoconstriction. Am J Med 49:175-185, 1970
intravital
post mortem
Liver transplantation Milestones in Pathophysiology�20th century
15. HRS is a potentially reversible syndrome that occurs in patients with cirrhosis, ascites and liver failure, as well as in patients with acute liver failure or alcoholic hepatitis.
It is characterised by impaired renal function, marked alterations in cardiovascular function and overactivity of the sympathetic nervous and renin–angiotensin systems.
Portal hypertension is required to develop HRS
Severe renal vasoconstriction leads to a decrease of GFR.
16. Doppler ultrasound in HRS: high RI predicts HRS 2 yrs in advance
17. Type-2 HRS is characterised by moderate renal failure (serum creatinine from 1.5 to 2.5 mg/dl), with a steady or slowly progressive course.
It appears spontaneously, but can also follow a precipitating event.
Type-2 HRS is typically associated with refractory ascites. Survival of patients with type-2 HRS is shorter than that of non-azotaemic cirrhotic patients with ascites but better than that of patients with type-1 HRS
19. Type-1 HRS is characterised by rapid progressive renal failure defined by doubling of the initial serum creatinine concentrations to >2.5 mg/dl in <2 weeks.
It may appear spontaneously, but often develops after a precipitating event, particularly SBP.
Type-1 HRS usually occurs within the setting of an acute deterioration of circulatory function characterised by arterial hypotension and activation of endogenous vasoconstrictor systems, and may be associated with impaired cardiac and liver functions as well as encephalopathy.
Prognosis is poor
20. What is the incidence of HRS?
Prospective study - Ginés et al, n=234
Cirrhotic patients with normal renal function
Incidence of HRS at 1 yr follow up 18%
Incidence of HRS at 5 yrs 39%
Greates risk for HRS and death:
Low serum osmolality
Low urinary sodium (<5mVal/L)
Independent risk factors:
Absence of hepatomegaly
Plasma renin activity >3.5 ng/ml/h
MAP < 85 mm Hg
21. gut barrier dysfunction�plays a key role in the development of renal dysfunction
25. Correlation of exhaled NO and hyperdynamic ciculation in cirrhosis
26. HRS secret #4 „Hyperdynamic“ circulation is restricted to splanchnic vessels, shifting blood away from kidneys and brain.
The concept of “splanchnic steal“ appears more adequate.
30. Current treatment of HRS �depends on pathophysiology Treat central hypovolemia
Albumin 20% solution (initial dose 1 g/kg, then 20-40 g/day until improvement)
Remove nephrotoxic drugs
Diuretics, NSAIDs, Antihypertensives, ACE-Inhib.
Aminoglycosides and other nephrotoxic ABs
Treat infection
UTI
SBP
Pneumonia
Sepsis, endocarditis
31. Vasodilators in HRS:�usually catastrophic results !!! No chance in afferent renal Vasoconstriction
systemic hypotension -> INCREASE of renal vasokonstriktion
32. Vasodilators in HRS: No success
AT-II Antagonists
ACE - Inhibitors
alpha1-Antagonists
Ca - Antagonists
Prostaglandine analogues (PgE1, PgI2, Misoprostol)
Questionable
N-Acetylcysteine (n=6)
Endothelin-A-Antagonists (n=3)
Dopamine
33. Vasoconstrictors in HRS��caution in CAD, arterial stenosis, intestinal vasculopathy, NOMI Vasopressin
No studies, Thrombozytopenia, DIC, liver toxicity
Ornipressin
Infusion 1-4 U/h
Too cheap - killed by industry
Noradrenaline
Infusion 0.03-0.5 µg/kg/min
Midodrin
Oral drug available: outcome not improved
Terlipressin
Pro-drug (Triglycyl-Lysin-Vasopressin)
Bolus 0.5-2 in 4-8 hours interval
Larger experience
34. Terlipressin: effects on �HRS resolution
37. HRS secret #5 Prophylaxis is best therapy of HRS
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