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Not Yet RecruitingNCT07464522

Non-invasive Predictors of Esophageal Varices and Their Correlation to Upper Endoscopic Findings

Non-invasive Predictors of Esophageal Varices in Pediatric Portal Hypertension and Their Correlation to Upper Endoscopic Findings

Summary

The goal of this observational study: * To evaluate the diagnostic accuracy of non-invasive markers in predicting the presence and grading of esophageal varices in children with portal hypertension. * To correlate these non-invasive markers with the severity of portal hypertension and the grade of esophageal varices to identify patients at high risk of bleeding. * To propose a defined protocol for screening esophageal varices in those children.

Detailed description

Portal hypertension in children represents a major hepatobiliary disorder characterized by abnormally elevated pressure within the portal venous system, typically defined as a clinically significant increase in portal venous pressure leading to the formation of portosystemic collaterals and complications such as splenomegaly, hypersplenism, gastroesophageal varices, and portal hypertensive gastropathy. Although direct portal pressure measurement is rarely performed in pediatrics, portal hypertension is generally inferred when clinical, laboratory, and radiologic findings indicate increased resistance to portal blood flow. Doppler ultrasonography demonstrating reduced portal vein velocity, increased portal vein diameter, or reversal of flow is widely accepted as a non-invasive surrogate of elevated portal pressure in children. The true global incidence of pediatric portal hypertension remains difficult to determine, partly because of variations in underlying etiologies across different regions. Nevertheless, portal hypertension is a major cause of upper gastrointestinal bleeding in childhood, accounting for a significant proportion of variceal hemorrhage admissions in tertiary pediatric gastroenterology units. In developing countries, extrahepatic portal vein obstruction (EHPVO) constitutes the leading cause, whereas intrahepatic diseases dominate in high-income nations. With increasing survival of children with chronic liver diseases and improved neonatal care, the burden of pediatric portal hypertension has been rising over the past two decades, underscoring the need for improved strategies for early diagnosis and prevention of complications. Causes of portal hypertension in children are traditionally divided into extrahepatic and intrahepatic categories. EHPVO is among the most frequent etiologies in many low- and middle-income countries and is commonly associated with neonatal umbilical vein catheterization, sepsis, dehydration, thrombophilia, abdominal surgery, and congenital portal vein malformations. These children often present at a young age with splenomegaly and hypersplenism despite preserved liver synthetic function. Intrahepatic causes include cholestatic liver diseases such as biliary atresia-which remains a leading indication for pediatric liver transplantation-congenital hepatic fibrosis, autoimmune hepatitis, Wilson disease, alpha-1-antitrypsin deficiency, metabolic disorders, and chronic viral hepatitis. Progressive hepatocellular injury, fibrosis, and architectural distortion increase resistance to portal flow and lead to portal hypertension in these conditions. Diagnosis of portal hypertension in children relies on a combination of clinical evaluation, laboratory abnormalities, and imaging findings. Splenomegaly is the most common and often earliest clinical manifestation. Laboratory markers such as thrombocytopenia reflect hypersplenism secondary to splenic sequestration. Doppler ultrasound is the first-line diagnostic tool, providing information on portal vein diameter, patency, flow velocity, degree of congestion, presence of cavernous transformation, and detection of portosystemic collaterals. Additional imaging modalities such as contrast-enhanced CT, MR angiography, and elastography may assist in defining the underlying cause and assessing liver stiffness. Endoscopy remains the gold standard for confirming and grading esophageal varices; however, its invasive nature and the need for anesthesia in children limit its use as a routine screening tool. Consequently, numerous non-invasive predictors such as platelet count, spleen size, platelet-to-spleen ratio, APRI, liver stiffness, and composite scores have been investigated to reduce reliance on endoscopy. Complications of pediatric portal hypertension vary according to etiology and disease stage. Esophageal and gastric varices represent the most feared sequelae, with variceal hemorrhage contributing significantly to morbidity and mortality. Other complications include portal hypertensive gastropathy, hypersplenism, ascites, growth failure, minimal hepatic encephalopathy, and portal biliopathy in cases of long-standing EHPVO. Extrahepatic consequences such as portopulmonary hypertension and hepatopulmonary syndrome are increasingly recognized in children with chronic liver disease and may adversely affect prognosis, transplant eligibility, and overall quality of life. The early diagnosis of portal hypertension and timely identification of esophageal varices are crucial components of pediatric care. Early screening enables risk stratification, facilitates timely initiation of primary prophylaxis, and significantly reduces the incidence of first variceal bleeding episodes-events associated with substantial morbidity in children. In addition, early detection of the underlying cause allows for more effective medical, surgical, or interventional radiologic management and may prevent long-term complications. Improved non-invasive models and imaging markers continue to support safer, more accessible strategies for monitoring children at risk and reducing dependence on endoscopy. Given the lifelong implications of chronic portal hypertension and the potential for life-threatening bleeding, establishing reliable early predictors of esophageal varices remains a central goal in pediatric hepatology and is essential for optimizing long-term outcomes in affected children.

Conditions

• Esophageal Varices
• Portal Hypertension

Timeline

Start date

2026-03-20

Primary completion

2028-03-20

Completion

2028-05-20

First posted

2026-03-11

Last updated

2026-03-23

Source: ClinicalTrials.gov record NCT07464522. Inclusion in this directory is not an endorsement.