Abstract
Strokes within pediatric populations are considered to be the 10th leading cause of death in the United States of America, with over half of such events occurring in children younger than one year of life. The multifactorial etiopathology that has an influence on stroke development and occurrence signify the importance of the timely recognition of both modifiable and non-modifiable factors for adequate diagnostic and treatment approaches. The early recognition of a stroke and stroke risk in children has the potential to advance the application of neuroprotective, thrombolytic, and antithrombotic interventions and rehabilitation strategies to the earliest possible timepoints after the onset of a stroke, improving the outcomes and quality of life for affected children and their families. The recent development of molecular genetic methods has greatly facilitated the analysis and diagnosis of single-gene disorders. In this review, the most significant single gene disorders associated with pediatric stroke are presented, along with specific therapeutic options whenever they exist. Besides monogenic disorders that may present with stroke as a first symptom, genetic polymorphisms may contribute to the risk of pediatric and perinatal stroke. The most frequently studied genetic risk factors are several common polymorphisms in genes associated with thrombophilia; these genes code for proteins that are part of the coagulation cascade, fibrolysis, homocystein metabolism, lipid metabolism, or platelets. Single polymorphism frequencies may not be sufficient to completely explain the stroke causality and an analysis of several genotype combinations is a more promising approach. The recent steps forward in our understanding of the disorders underlying strokes has given us a next generation of therapeutics and therapeutic targets by which to improve stroke survival, protect or rebuild neuronal connections in the brain, and enhance neural function. Advances in DNA sequencing and the development of new tools to correct human gene mutations have brought genetic analysis and gene therapy into the focus of investigations for new therapeutic options for stroke patients.
Highlights
Strokes within the pediatric population are considered to be the 10th leading cause of death in the United States of America (USA), with over half of such events occurring in children younger than one year of life [1]
Besides the above-mentioned monogenic disorders that may present with stroke as a first symptom, numerous studies indicate that genetic polymorphisms may contribute to the risk of pediatric and perinatal stroke
A slightly increased risk of childhood arterial ischemic stroke (AIS) was identified in some studies [128], no significant differences in allele distribution or genotype were reported, and a recent meta-analysis of 358 children with stroke and 451 controls from different populations confirmed no association between the FXIII polymorphism 34L allele and CAIS [142]
Summary
Strokes within the pediatric population are considered to be the 10th leading cause of death in the United States of America (USA), with over half of such events occurring in children younger than one year of life [1]. Strokes within the pediatric population can be classified as ischemic or hemorrhagic based on the cause of the stroke. Ischemic stroke can be further classified as AIS or venous infarction, where a venous infarction can be caused by cerebral sinovenous thrombosis (CSVT) or cortical vein thrombosis [4]. The aim of this review is to summarize and discuss recent knowledge regarding the classification, genetic basis, and therapeutic options of strokes within a pediatric population
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