Overview
Children with decompensated cirrhosis are more prone to develop various complications. The pathogenesis of cirrhotic complications (ascites, hyponatremia, acute kidney injury) includes release of vasodilatory molecules like nitric oxide, damage associated molecular pathogens (DAMPs) and pattern associated molecular pathogens (PAMPs) secondary to bacterial translocation, which causes splanchnic bed vasodilation resulting in activation of renin-angiotensin and aldosterone axis (RAAS) causing sodium and water retention and renal vasoconstriction.
The development of complications in these children may result in death or may preclude them from reaching upto liver transplantation.
Midodrine is an α1 adrenergic receptor agonist, which increases vascular tone causing rise in the blood pressure, thereby improving renal perfusion and causes RAAS deactivation. The effects of midodrine is documented in reduction of refractory ascites, hepatorenal syndrome and hyponatremia.
Albumin is a protien that works by both increasing the colloidal oncotic pressure and improving systemic circulation as well as by effecting the body with anti-inflammatory and antioxidant properties.
We have already demonstrated the safety and efficacy of midodrine as well as albumin in cirrhotic children. However, none of these drugs alone provided survival benefit to the patients. Hence, we have planned this study with the ojective to evaluate if combining these 2 drugs (midodrine and albumin) would further reduce the complications and improve the survival in decompensated cirrhotic children.
Description
Aim: To evaluate whether a combination of midodrine and intravenous albumin reduces complications of cirrhosis in decompensated (ascites) cirrhotic children as compared to midodrine alone.
Primary objective: To compare difference in composite incidence of complications of cirrhosis (Acute kidney injury, ascites, hyponatremia, hepatic encephalopathy) in patients receiving midodrine and albumin versus those receiving midodrine alone.
Secondary objectives:
- To compare the rate of control of ascites by 6 months in the 2 groups
- To compare the change in Mean arterial pressure (MAP) at 1 week, 2 weeks, 4 weeks, 3 months, and 6 months in the 2 groups
- To compare the Plasma renin activity at baseline, 4 weeks, 3mo, 6mo in the 2 groups
- Evaluate the change in serum sodium from baseline to 6 months in the 2 groups
- To compare the Creatinine from baseline to 6 months in the 2 groups
- To compare the Frequency of development of drug related adverse effects by 6 months
- To compare the Transplant free survival in the 2 groups
- To compare the Cytokines levels at baseline and 6 months in the 2 groups
- To compare the presence of Minimal Hepatic encephalopathy in the 2 groups Study
population :Children and Adolescents of age group upto 18 years with decompensated
cirrhosis with clinical ascites, following up in the Pediatric Hepatology
Department, ILBS will be prospectively included in this study after informed consent
- Study design: Open-label Randomized Controlled Trial
- Study period: 6 months weeks for each patient; The study will be conducted from the time of ethical approval to June 2025.
Sample size: In a pilot trial done at our center comparing midodrine and SMT the composite incidence of complication was 61.2% in midodrine arm. In absence of a pediatric study we assume a 25% reduction of complication by adding albumin along with midodrine keeping a power of study 80% , the sample size was calculated to be 30 in each arm.
Eligibility
Inclusion Criteria:
- Children (≤ 18 years)
- Cirrhosis based on histological/ radiological + endoscopic evidence
- Clinical ascites (≥ grade 2 ascites)
- Informed consent from parents (Assent > 12 years)
Exclusion Criteria:
- Arterial hypertension (Mean Arterial Pressure ≥ 95th centile for age)
- Presence of Portal vein thrombosis
- Hepatorenal Syndrome
- Congestive Heart failure
- Respiratory failure(PF ratio <200)
- Septic shock
- Presence of Hepatocellular Carcinoma
- Transjugular intrahepatic Porto Systemic Shunt