Cirrhosis, Liver Clinical Trial
Official title:
Randomized Control Trial of Rifaximin and Norfloxacin in Primary and Secondary Prophylaxis of Spontaneous Bacterial Peritonitis(SBP) in Cirrhotic Patients
Spontaneous bacterial peritonitis (SBP) is a frequent and severe complication of cirrhotic
patients with ascites.Early diagnosis and prompt treatment with effective antibiotics
significantly improves the prognosis of this complication. The recommended treatment is a
third generation cephalosporin given intravenously for five days.Following recovery patients
should receive secondary prophylaxis with a quinolone such as oral norfloxacin 400
mg/day.Also all patients should be assessed for liver transplantation.
Most commonly used antibiotic for both primary and secondary prophylaxis is norfloxacin 400
mg once daily.Other antibiotics like cotrimoxazole,ceftriaxone,ciprofloxacin and rifaximin
have also been evaluated in various studies.Use of antibiotic prophylaxis has been evaluated
to decrease recurrence of SBP in treated groups than in control groups.
Rifaximin is an oral antimicrobial agent with broad-spectrum activity that is gut-selective
and nonsystemic. Rifaximin appears to have a low level of selection for resistant bacterial
mutants. Intestinal decontamination is known to increase peripheral blood counts by
suppressing endotoxemia and inhibiting the effects of cytokines and nitric oxide on blood
counts.
With this mechanisms rifaximin has been already proven to decrease recurrence of hepatic
encephalopathy.The most important mechanism for development of SBP is bacterial translocation
(BT).Translocation of enteric flora occurs via defective mucosal barrier.BT is considered the
key step in pathogenesis of SBP and cirrhotic patients.It is also the critical factor that is
responsible for host immune response and secreation of inflammatory mediators that is
responsible for hemodynamic changes in cirrhotics.Three most important mechanism of bacterial
translocation include bacterial overgrowth,physical disruption of gut mucosal barrier and
impaired host defence.
Rifaximin by mechanism of gut decontamination may reduce translocation of intestinal bacteria
into mesenteric lymph nodes then into ascitic fluid.Thus it may prove useful in preventing
recurrence of SBP.There was no study till date that has compared efficacy of Norfloxacin and
rifaximin to prevent development of SBP.This pilot study was done to compare the efficacy of
rifaximin with norfloxacin in both primary and secondary prophylaxis of SBP in a prospective
randomized open-label and non-inferiority trial
Ascites is the most common complication of cirrhosis, and 60% of patients with compensated
cirrhosis develop ascites within 10 years during the course of their disease . Ascites occurs
only when portal hypertension has developed and is related to inability to excrete an
adequate amount of sodium into urine, leading to a positive sodium balance.Evidence suggests
that renal sodium retention in patients with cirrhosis is secondary to arterial splanchnic
vasodilation. This causes a decrease in effective arterial blood volume with activation of
arterial and cardiopulmonary volume receptors, and homeostatic activation of vasoconstrictor
and sodium-retaining systems (i.e., the sympathetic nervous system and the
(renin-angiotensin-aldosterone system). Renal sodium retention leads to expansion of the
extracellular fluid volume and formation of ascites and edema . The development of ascites is
associated with a poor prognosis and impaired quality of life in patients with cirrhosis .
Thus, patients with ascites should generally be considered for referral for liver
transplantation. There is a clear rationale for the management of ascites in patients with
cirrhosis, as a successful treatment may improve the outcome and symptoms.
Spontaneous bacterial peritonitis (SBP) is a frequent and severe complication of cirrhotic
patients with ascites.Early diagnosis and prompt treatment with effective antibiotics
significantly improves the prognosis of this complication. The recommended treatment is a
third generation cephalosporin given intravenously for five days. The most commonly used is
cefotaxime, up to 4 g/day in 2-4 divided doses because of its proven efficacy and safety3.
Repeat diagnostic paracentesis to document response by a greater than 25% decrease in ascitic
fluid neutrophil count at 48 hours after commencement of antibiotic is recommended. With this
regimen, recovery from SBP is higher than 80-90% and 30-day survival is at least
80%.Following recovery patients should receive secondary prophylaxis with a quinolone such as
oral norfloxacin 400 mg/day.Also all patients should be assessed for liver transplantation
.Most commonly used antibiotic for both primary and secondary prophylaxis is norfloxacin 400
mg once daily.Other antibiotics like cotrimoxazole,ceftriaxone,ciprofloxacin and rifaximin
have also been evaluated in various studies.Use of antibiotic prophylaxis has been evaluated
to decrease recurrence of SBP in treated groups than in control groups.
Rifaximin is an oral antimicrobial agent with broad-spectrum activity that is gut-selective
and nonsystemic. Rifaximin appears to have a low level of selection for resistant bacterial
mutants and may not confer the same risks as those associated with systemic antibiotics. A
study in patients with alcohol-related decompensated cirrhosis reported that rifaximin
treatment reduced endotoxin levels and resulted in significantly decreased hepatic venous
pressure gradient values, which decreased the occurrence of complications in advanced liver
disease.13Intestinal decontamination with rifaximin has been shown to increase platelet count
significantly in thrombocytopenic patients with cirrhosis.This benefit is thought to be
achieved through a concomitant reduction of endotoxemia.Improvements in platelet counts in
patients with thrombocytopenia could decrease bleeding risks and complications of medical
procedures, and help stabilize underlying liver disease. Intestinal decontamination is also
known to increase peripheral blood counts by suppressing endotoxemia and inhibiting the
effects of cytokines and nitric oxide on blood counts.
With this mechanisms rifaximin has been already proven to decrease recurrence of hepatic
encephalopathy.The most important mechanism for development of SBP is bacterial translocation
(BT) which refers to entry of bacteria or their products into regional lymph nodes,systemic
circulation and extraintestinal organs.Translocation of enteric flora occurs via defective
mucosal barrier.BT is considered the key step in pathogenesis of SBP and cirrhotic
patients.It is also the critical factor that is responsible for host immune response and
secreation of inflammatory mediators that is responsible for hemodynamic changes in
cirrhotics.Three most important mechanism of bacterial translocation include bacterial
overgrowth,physical disruption of gut mucosal barrier and impaired host defence.
Rifaximin by mechanism of gut decontamination may reduce translocation of intestinal bacteria
into mesenteric lymph nodes then into ascitic fluid.Thus it may prove useful in preventing
recurrence of SBP.There is no study till date that has compared efficacy of Norfloxacin and
rifaximin to prevent development of SBP.This pilot study was done to compare the efficacy of
rifaximin with norfloxacin in both primary and secondary prophylaxis of SBP in a prospective
randomized open-label and non-inferiority trial
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