Cirrhosis Clinical Trial
Official title:
Immune-inflammatory and Metabolic Effects of High Dose Furosemide Plus Hypertonic Saline Solution (HSS) Treatment in Cirrhotic Subjects With Refractory Ascite
Introduction: Patients with chronic liver diseases are usually thin as a result of
hypermetabolism and malnutrition expressed by reduced levels of leptin and impairment of
other adyponectins such as visfatin.
Aims: To evaluate the metabolic and inflammatory effects of intravenous high-dose furosemide
plus hypertonic saline solutions (HSS) compared with repeated paracentesis and a standard
oral diuretic schedule, in patients with cirrhosis and refractory ascites.
Methods; All consecutive cirrhotic patients with refractory ascites unresponsive to
outpatient treatment will be enrolled . Enrolled subjects will be randomized to treatment
with intravenous infusion of furosemide (125-250mg⁄bid) plus small volumes of HSS from the
first day after admission until 3 days before discharge (Group A ), or repeated paracentesis
from the first day after admission until 3 days before discharge (Group B, ).
Plasma levels of ANP, BNP, Leptin, visfatin, IL-1β, TNF-a, IL-6 were measured before and
after the two type of treatment.
Cirrhosis and congestive heart failure (CHF) are major clinical disease states characterized
by renal sodium and water retention with edema formation. Abnormalities of circulatory and
volume homeostasis in these diseases elicit neuro-hormonal responses influencing renal
function and leading to retention of sodium and water.Cytokines constitute a complex network
of molecules involved in the regulation of the inflammatory response and the homeostasis of
organ functions. Moreover cytokines coordinate physiologic and pathologic processes in the
liver, such as liver growth and regeneration, as well as inflammatory processes including
viral liver disease, liver fibrosis and cirrhosis .
Furthermore, patients with chronic liver diseases are usually thin as a result of
hypermetabolism, diminished food intake, and malnutrition, and leptin is thought to be
involved in this process. Furthermore, other adipocytokines play an important role in lipid
metabolism and liver disease progression. Visfatin a 52-kDa protein that has been cloned as
pre-B cell colony-enhancing factor (PBEF), and liver and muscle have been reported to be the
tissues with the highest expression levels of this protein. Recently, visfatin has also been
proposed as an adipokine secreted by adipose tissue.
A recent study reported that patients with chronic HBV infection have significantly higher
serum levels of adiponectin and visfatin, but lower leptin levels than healthy controls, and
that serum adipocytokine levels independently correlate with HBV viremia, HBsAg levels, and
liver fibrosis stages.
Another recent study reported that in subjects with alcoholic cirrhosis following adjustment
for fat mass, visfatin levels were significantly higher from Child-Pugh Class A to Class C.
Furthermore, leptin, the first described adipokine, interplays with hepatic metabolism, and
data from a small study suggest that recombinant leptin administration has a possibly
beneficial effect on steatosis, but not fibrosis, in NAFLD patients with hypo-leptinemia and
a very recent study reported that in non-alcoholic steatohepatitis (NASH), leptin is
upregulated, and promotes liver fibrosis by directly activating hepatic stellate cells (HSC)
via the hedgehog pathway and the hedgehog-regulated osteopontin (OPN).
Nevertheless, to the best of knowledge, no study has addressed the effectiveness of
treatment of complications of cirrhosis such as ascites and fluid overload on these
inflammatory and metabolic abnormalities.
According to the International Ascites Club, refractory ascites is defined by the lack of
response to high doses of diuretics (spironolactone 400mg⁄day and furosemide 160mg⁄day) or
the development of adverse effects (hyperkalemia, hyponatremia, hepatic encephalopathy or
renal failure) that prohibit further use of diuretics.
A recent clinical trial reported that intravenous hypertonic saline solutions (HSS) plus
high-dose furosemide is a safe and effective alternative to repeated paracentesis when
treating hospitalized patients with cirrhosis and refractory ascites.
Specific objective and hypothesis:
On this basis, the hypothesis of this trial was that the clinical effectiveness of high dose
furosemide + HSS could be accomplished by parallel effects on inflammatory, natriuretic and
metabolic pathways expressed by changes of cytokines, natriuretic peptides, leptin and
visfatin serum levels after treatment.
Thus the aim of this trial will be to evalute the metabolic and inflammatory effects of
intravenous high-dose furosemide plus HSS compared with repeated paracentesis and a standard
oral diuretic schedule, in patients with cirrhosis and refractory ascites, evaluating their
effects on a panel of serum biomarkers such as some inflammatory cytokines, ANP/BNP, leptin
and visfatin serum levels by means of analysis of differences of their serum levels before
and after treatment with high dose furosemide + HSS.
Materials and methods All consecutive cirrhotic patients presenting with ascites
unresponsive to ambulatory treatment at Palermo University Hospital (Azienda Ospedaliera
Policlinico 'Paolo Giaccone') who will be admitted to the Internal Medicine Ward from
December 2013 to December 2015 will be offered enrolment in the study protocol after a
diagnosis of ascites had been made and all potential contraindications excluded.
Refractory ascites was defined according to the International Ascites Club criteria 1 as
either: (a) diuretic-resistant refractory ascites: <1.5kg ⁄week weight loss while being
treated with furosemide (160mg⁄day) and spironolactone (400mg⁄day) or an equivalent dose of
a loop-acting and distal-acting diuretic; or (b) diuretic-intractable refractory ascites:
<1.5kg⁄week weight loss as a result of the inability to use an effective dose of diuretic
because of development of diuretic-induced hyponatremia (sodium level <125mEq⁄ L),
hyperkalemia (potassium level >5.5mEq⁄L), renal failure (doubling of serum creatinine or
values >2.5g⁄dL) or encephalopathy; (c) previous dietary restriction of sodium between
50-66mEq ⁄day.
Exclusion criteria were: inability to obtain informed consent, possible non-cirrhotic
ascites, congestive heart failure (defined by clinical exam and echocardiogram), acute renal
failure, hepatocellular carcinoma based on the Barcelona Clinic liver Cancer (BCLC) criteria
, complete portal vein thrombosis, active sepsis or other incurable cancers. The study was
approved by the institutional Ethics Committee and written informed consent was obtained for
all patients.
Daily clinical and laboratory evaluation Treatment protocol Group A: treatment with
intravenous infusion of furosemide (doses 125-250mg⁄ bid) plus small volumes of HSS (150mL
1.4-4.6% NaCl), from the first day after admission until 3 days before discharge ( 8 days of
treatment) , with water restriction and a normal sodium diet.
Group B: repeated paracentesis (4-6L daily) from the first day after admission until 3 days
before discharge with albumin reinfusion at a rate of 5-8g⁄ L of removed ascites. The last
paracentesis (at 3 days from admission after 8 days was a total paracentesis (8.1±2.7L) plus
iv albumin infusion (8g per liter of ascitic fluid removed) following a method previously
described.
Blood sample collection Blood samples from each subject enrolled wil, be drawn after at
least 30 minutes of bed rest in a supine position, within 24h of admission and after 8 days
of active treatment. Blood samples were centrifuged (10,000g) and the resulting supernatant
was immediately frozen at -80°C until analysis was completed.
Metabolic and immune-inflammatory biochemical evaluation Will be evaluate plasma levels of
ANP, BNP, Leptin, visfatin, and IL-1β, TNF-a, IL-6 that will be measured using a sandwich
ELISA (Human IL-1β, TNF-a, IL-6 6 Diaclone). ANP and BNP plasma concentration was measured
in duplicate by a solid phase sandwich immune-radiometric assay for human BNP (IRMA, ANP and
BNP, Shering cis bio int). The minimum detectable concentrations for the diagnostic tests
are: TNF-a: 8pg/mL; IL-1β: <1pg/mL; IL-6: <0.81pg/mL; ANP: 3.1pg/mL; BNP: 5pg/mL.
Leptin and visfatin will be measured by ELISA Sandwich (leptin Mediagnost and visfatin
Phoenix Pharmaceticals Inc); the minimum detectable concentration for these diagnostic teste
were: leptin 0.8ng/ml; visfatin: 1.8ng/ml.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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