Sturge-Weber Syndrome: A Review of Pathophysiology, Genetics, Clinical Features, and Current Management Approache

The Sturge-Weber syndrome is a sporadic congenital neurocutaneous disorder characterized by a port-wine stain affecting the skin in the distribution of the ophthalmic branch of the trigeminal nerve, abnormal capillary venous vessels in the leptomeninges of the brain and choroid, glaucoma, seizures, stroke, and intellectual disability. It has been hypothesized that somatic mosaic mutations disrupting vascular development cause both the Sturge-Weber syndrome and port-wine stains, and the severity and extent of presentation are determined by the developmental time point at which the mutations occurred. To date, no such mutation has been identified. We performed whole-genome sequencing of DNA from paired samples of visibly affected and normal tissue from 3 persons with the Sturge-Weber syndrome. We tested for the presence of a somatic mosaic mutation in 97 samples from 50 persons with the Sturge-Weber syndrome, a port-wine stain, or neither (controls), using amplicon sequencing and SNaPshot assays, and investigated the effects of the mutation on downstream signaling, using phosphorylation-specific antibodies for relevant effectors and a luciferase reporter assay. We identified a nonsynonymous single-nucleotide variant (c.548G→A, p.Arg183Gln) in GNAQ in samples of affected tissue from 88% of the participants (23 of 26) with the Sturge-Weber syndrome and from 92% of the participants (12 of 13) with apparently nonsyndromic port-wine stains, but not in any of the samples of affected tissue from 4 participants with an unrelated cerebrovascular malformation or in any of the samples from the 6 controls. The prevalence of the mutant allele in affected tissues ranged from 1.0 to 18.1%. Extracellular signal-regulated kinase activity was modestly increased during transgenic expression of mutant Gαq. The Sturge-Weber syndrome and port-wine stains are caused by a somatic activating mutation in GNAQ. This finding confirms a long-standing hypothesis. (Funded by the National Institutes of Health and Hunter's Dream for a Cure Foundation.).

Exposure of young animals to commonly used anesthetics causes neurotoxicity including impaired neurocognitive function and abnormal behavior. The potential neurocognitive and behavioral effects of anesthesia exposure in young children are thus important to understand.

In laboratory animals, exposure to most general anaesthetics leads to neurotoxicity manifested by neuronal cell death, and abnormal behaviour and cognition. Some, large human cohort studies demonstrate an association between general anaesthesia at a young age and subsequent neurodevelopmental deficits, but are prone to bias. Others have found no evidence for an association. We aimed to establish whether general anaesthesia in early infancy has an effect on neurodevelopmental outcomes in a randomised controlled trial (RCT). In this international assessor-masked equivalence RCT, infants less than 60 weeks’ postmenstrual age and born at greater than 26 weeks gestation undergoing inguinal herniorraphies without prior exposure to general anaesthesia or risk factors for neurologic injury were recruited. They were randomly assigned to receive either an awake-regional or sevoflurane-based general anaesthetic. The primary outcome measure was the Wechsler Preschool and Primary Scale of Intelligence-Third Edition (WPPSI-III) Full Scale Intelligence Quotient (FSIQ) at 5 years of age. The primary analysis was as-per-protocol adjusted for gestational age at birth and country using multiple imputation to deal with missing data. An intention-to-treat analysis was also performed. A difference in means of five points was predefined as the clinical equivalence margin. This trial is registered with ANZCTR, number ACTRN12606000441516 and ClinicalTrials.gov , number NCT007566000 . Between Feb 2007 and Jan 2013, 722 infants were randomised, 363 to the awake-regional and 359 to general anaesthesia. The median duration of anaesthesia in the general anaesthetic group was 54 minutes. There were 74 protocol violations in the awake-regional group and 2 in the general anaesthesia group. Primary outcome data for the as-per-protocol analysis were obtained from 205 children in the awake-regional group and 242 in the general anaesthesia group. The FSIQ score (mean [standard deviation (SD)]) was 99.08 (18.35) in the awake-regional group and 98.97 (19.66) in the general anaesthesia group, with a difference in means (awake-regional minus general anaesthesia) of 0.23, 95% Confidence Intervals −2.59 to 3.06) showing strong evidence of equivalence. The results with the intention-to-treat analysis were similar to the as-per-protocol analysis. We found strong evidence that just under an hour of general anaesthesia in early infancy does not alter neurodevelopmental outcome compared to awake-regional anaesthesia in a predominantly male study population.