Congenital heart defects (CHDs) are the most common congenital malformations in pediatric pathology. Psychomotor development is impaired in 10-50% of the patients with CHD.1 Several biomolecules are used as diagnostic or prognostic markers for impaired psychomotor developmental; however, neuromarkers have been the most efficient. Our study aimed to evaluate serum glial acidic fibrillary protein (GFAP) as a predictor of impaired early psychomotor development (in the first postoperative year) in patients with CHD who had cardiac surgery.
This was a prospective, controlled study, including 80 pediatric patients (< 6 years of age) with CHD, who needed elective surgical intervention. Each patient was evaluated using the Denver Developmental Screening Test II (DDST II) scale before surgery and 4-6 months after surgery. DDST II includes 125 items grouped into four categories: fine-motor adaptive function, gross motor function, personal-social behavior, and language. GFAP levels were checked preoperatively: 1) in the operating room after induction of anesthesia, but before starting cardiopulmonary bypass, and 2) 24 h after surgery.
GFAP value was significantly higher (p = 0.0046) during the postoperative phase than the preoperative phase. Significant correlations between GFAP and neurodevelopmental scores were obtained in two domains: personal-social behavior and fine motor function. To establish the role of GFAP as a marker of brain development, receiver operating characteristic analysis was conducted and a good area under the curve of 0.75 was obtained (Figure 1). The analysis yielded a cut-off of 0.688.
GFAP constitutes the cytoskeleton of astrocytes. GFAP is present in the central nervous system but reaches the serum upon astrocyte injury or death. Therefore, it is used as a neuromarker for brain injury. In studies on children who had cardiovascular surgery, a significant increase in serum GFAP was observed after surgical intervention; moreover, GFAP levels correlated with factors that induce neurologic risk, including total by-pass time, aortic cross clamping time, and low temperature.2 In our study, correlations between these risk factors and GFAP levels or neurodevelopmental scores were not found.
Studies on neurodevelopmental dynamics have reported contrasting results. In a study by Sanchez-de-Toledo including 39 patients, no significant difference was found in serum GFAP in the immediate postoperative period between children with normal and abnormal neurodevelopment.3 A study by Graham on 97 patients showed that lower neurodevelopmental scores in early childhood are associated with higher levels of serum GFAP during surgery in neonates.4 Vedovelli et al.5 reported that GFAP could predict deficits in communication skills of infants and children.Vergine suggested that cardiopulmonary by-pass due to body temperature changes leads to nervous system injury, and high GFAP levels during surgery correlate with delays in psychomotor scores after 4-8 years.6 They demonstrated that GFAP > 0.49 ng/ml is an important risk factor for poor neurologic function in the long-term. In our study, a cut-off value of 0.68 ng/ml was associated with neurodevelopmental delay in the short-term, that is, 4-6 months after surgery.
According to studies, GFAP is as good neuromarker for identifying early acute nervous system injury and long-term psychomotor impairment.7
In conclusion, we demonstrated that GFAP > 0.68 ng/ml is associated with impairment in neurodevelopmental scores of children with CHD requiring cardiovascular surgery. GFAP can serve as a good marker for short-term neurodevelopmental impairment. In addition, GFAP can prognose neurological outcomes long after the neurological insult. This neuromarker should be used in protocols for neuroprotective perioperative strategies to decrease neurological injury in patients with CHD after cardiovascular surgery.