Hematological and biochemical profiles of children with congenital heart diseases candidate for surgical repair

Hassan, Mohammed H.; Taye, Ashraf; Abdel Bary, Mohamed; Okasha, Marwa; Abdel Hafez, Mohammed Farouk; Soliman, Aml Abdel-Fattah Sayed; Ghoneim, Ahmed; Hofni, Amal; Farouk, Ahmed

doi:10.21608/svuijm.2025.375692.2162

	Hematological and biochemical profiles of children with congenital heart diseases candidate for surgical repair
SVU-International Journal of Medical Sciences
Volume 8, Issue 2, July 2025, Pages 812-822 PDF (484.54 K)
Document Type: Original research articles
DOI: 10.21608/svuijm.2025.375692.2162
Authors
Mohammed H. Hassan¹; Ashraf Taye²; Mohamed Abdel Bary³; Marwa Okasha^* ¹; Mohammed Farouk Abdel Hafez⁴; Aml Abdel-Fattah Sayed Soliman⁵; Ahmed Ghoneim⁴; Amal Hofni²; Ahmed Farouk⁵
¹Medical Biochemistry and Molecular Biology Department, Faculty of Medicine, Qena University, Qena, Egypt.
²Pharmacology and Toxicology Department. Faculty of Pharmacy. Qena University, Qena, Egypt.
³Cardiothoracic Surgery Department, Faculty of Medicine, Qena University, Qena, Egypt.
⁴Cardiothoracic Surgery Department, Faculty of Medicine, Assiut University, Assiut, Egypt.
⁵B. Sc. in Pharmaceutical Science, Faculty of Pharmacy, Assiut University, Assiut, Egypt.
Abstract
Background: Congenital heart disease (CHD) is a leading cause of morbidity and mortality in children, often accompanied by hematological and biochemical abnormalities. While previous studies have explored these alterations, inconsistencies remain regarding their prevalence and clinical significance across CHD subtypes. Objectives: To assess the prevalence and clinical significance of hematological and biochemical abnormalities across CHD subtypes Patients and methods: This case-control study compared 60 CHD patients (15 each with VSD, ASD, TOF, and PDA) with 40 healthy controls. Venous blood samples were analyzed for complete blood count, liver/kidney function, and coagulation profiles. Results: CHD patients exhibited significantly lower hemoglobin level with median of (10.45vs. 11 g/dL, p=0.011) and higher ALT levels with median of (33 vs. 25 IU/L, p<0.001) than controls. Subgroup analysis revealed elevated median of WBCs in PDA (13.5×10³/mm³ compared to the median of other groups being (10.6×10³/mm³ for VSD,11×10³/mm³ for ASD,10 ×10³/mm³ for TOF and 11×10³/mm³ for control, p<0.001) and increased AST for TOF patients (42 u/l, compared to median of other groups being 32 u/l for PDA,34 u/l for VSD,29 u/l for ASD and 38 u/l for control, p=0.008). INR variations were most pronounced in TOF with median of 1.1 and 1 for each PDA, VSD and ASD and 1.04 for control p=0.007). Conclusion: CHD patients demonstrate distinct hematological and biochemical derangements, with subtype-specific patterns suggesting varied pathophysiological mechanisms. These findings underscore the need for tailored monitoring and early intervention to mitigate complications.
Keywords
Congenital heart disease; Hematological profile; Biochemical markers; Pediatric cardiology; Cyanotic heart disease

Statistics Article View: 10 PDF Download: 11