STXBP1 Encephalopathy
Overview
STXBP1 encephalopathy is a genetic neurodevelopmental disorder caused by heterozygous pathogenic variants in [STXBP1](/entities/stxbp1) (syntaxin-binding protein 1, also known as MUNC18-1). The disorder is characterized by early-onset seizures (often within the first week of life), a distinctive EEG pattern of burst suppression, and profound developmental impairment. STXBP1 is one of the most common genetic causes of early-onset developmental and epileptic encephalopathies (DEEs), accounting for 1-5% of all DEE cases.
The disorder is sometimes called "STXBP1 encephalopathy with epilepsy" to distinguish from STXBP1-related disorders without seizures (which present as non-syndromic intellectual disability). The disease manifests across a spectrum from severe early-onset DEE to milder presentations with later seizure onset and better developmental outcomes.
[STXBP1](/entities/stxbp1) is critical for synaptic vesicle fusion: it functions as a SM (Sec1/Munc18-like) protein that binds syntaxin-1 and is essential for the SNARE complex assembly that mediates neurotransmitter release[@stxbp1review2023].
Genetics and Molecular Basis
STXBP1 Gene
[STXBP1](/entities/stxbp1) is located on chromosome 9q34.11 and encodes Munc18-1, a 67-kDa protein expressed throughout the brain. The gene spans approximately 120 kb and contains 20 coding exons.
...STXBP1 Encephalopathy
Overview
STXBP1 encephalopathy is a genetic neurodevelopmental disorder caused by heterozygous pathogenic variants in [STXBP1](/entities/stxbp1) (syntaxin-binding protein 1, also known as MUNC18-1). The disorder is characterized by early-onset seizures (often within the first week of life), a distinctive EEG pattern of burst suppression, and profound developmental impairment. STXBP1 is one of the most common genetic causes of early-onset developmental and epileptic encephalopathies (DEEs), accounting for 1-5% of all DEE cases.
The disorder is sometimes called "STXBP1 encephalopathy with epilepsy" to distinguish from STXBP1-related disorders without seizures (which present as non-syndromic intellectual disability). The disease manifests across a spectrum from severe early-onset DEE to milder presentations with later seizure onset and better developmental outcomes.
[STXBP1](/entities/stxbp1) is critical for synaptic vesicle fusion: it functions as a SM (Sec1/Munc18-like) protein that binds syntaxin-1 and is essential for the SNARE complex assembly that mediates neurotransmitter release[@stxbp1review2023].
Genetics and Molecular Basis
STXBP1 Gene
[STXBP1](/entities/stxbp1) is located on chromosome 9q34.11 and encodes Munc18-1, a 67-kDa protein expressed throughout the brain. The gene spans approximately 120 kb and contains 20 coding exons.
STXBP1 is one of the most intolerant genes in the human genome (pLI = 1.0), reflecting the severe fitness consequence of loss-of-function variants. The majority of pathogenic variants are de novo, though familial cases with gonadal mosaicism or affected parent have been described.
Pathogenic mechanisms include:
- Missense variants (~50%): disrupt Munc18-1 folding, binding to syntaxin, or interactions with other synaptic proteins
- Nonsense/frameshift variants (~40%): premature termination, likely leading to nonsense-mediated decay and haploinsufficiency
- Splice variants (~10%): exon skipping or intron retention
Pathophysiology
Munc18-1 (encoded by STXBP1) is a master regulator of synaptic vesicle exocytosis. It participates in the synaptic vesicle fusion cascade at multiple levels:
Synaptic vesicle priming — Munc18-1 is required for the transition of vesicles from a release-ready (primed) state to a fusion-competent state
SNARE complex formation — Munc18-1 stabilizes the SNARE complex (synaptobrevin, SNAP-25, syntaxin-1) that mediates membrane fusion
Calcium sensing coordination — Munc18-1 interacts with synaptotagmin to couple calcium influx to vesicle fusion
Synaptic plasticity — loss disrupts short-term and long-term plasticity mechanismsThe resulting synaptic dysfunction leads to:
- Impaired GABAergic and glutamatergic transmission
- Network hyperexcitability and seizures
- Disrupted activity-dependent circuit formation
- Developmental impairment through both seizure-dependent and independent mechanisms
Clinical Presentation
Neonatal Period (First Week of Life)
Most patients present with seizure onset within the first week, often within hours of birth. Seizures are often:
- Tonic (spasms) — most common type
- Focal clonic — rhythmic jerking of one body part
- Myoclonic — brief jerks
- Often frequent and prolonged; status epilepticus in >50%
The EEG characteristically shows
burst suppression (alternating periods of high-amplitude bursts and low-amplitude suppression), particularly in the first months. This pattern is reminiscent of Ohtahara syndrome.
Infancy and Early Childhood
Seizure types evolve:
- Tonic seizures (persistent)
- Focal seizures
- Myoclonic seizures
- Atypical absence seizures
- Epileptic spasms (infantile spasms in ~30-40%)
The burst suppression pattern often evolves into ESES (electrical status epilepticus during sleep) or multifocal discharges.
Development is severely impaired from early on. Patients develop:
- Severe intellectual disability
- Hypotonia evolving to spasticity
- Movement disorders (ataxia, dystonia in some)
- Absent or minimal language
- Poor head control, unable to sit independently
Childhood and Beyond
- Seizures persist in most patients, though some have improvement after infancy
- Gross motor development: most never walk independently; some achieve sitting
- Fine motor: hand stereotypies, poor hand use
- Communication: mostly non-verbal or very limited
- Behavior: autism spectrum features common, repetitive behaviors
- Other features: sleep disturbance, feeding difficulties, constipation
Diagnosis
Clinical Criteria
Seizure onset within first year (majority in first week)
Burst suppression EEG pattern (especially early)
Profound developmental impairment from early infancy
Movement disorder (ataxia, dystonia) in a subset
Family history (usually negative; de novo variant)Genetic Confirmation
- Epilepsy gene panel (first-line): tests STXBP1 and other DEE genes
- Whole exome sequencing (if panel negative): identifies STXBP1 variants
- Targeted STXBP1 sequencing: for clinical suspicion
- Parental testing: critical for genetic counseling (gonadal mosaicism in ~5%)
EEG Findings
- Burst suppression in the first months: pathognomonic but not specific to STXBP1
- ESES pattern: emerges in some patients during sleep
- Multifocal epileptiform discharges: as patients age
- Background slowing: progressive disorganization
Treatment
Anti-Seizure Medications
No specific treatment for STXBP1 encephalopathy; standard ASMs are used:
| Drug | Evidence | Notes |
|------|---------|-------|
| Benzodiazepines | Low-moderate | For acute seizure clusters; limited chronic use |
| Valproic acid | Low-moderate | Commonly used; broad spectrum |
| Levetiracetam | Low | Limited efficacy |
| Vigabatrin | Low | May help spasms |
| Cannabidiol | Low | Mixed data |
| Phenobarbital | Low | Sometimes effective for neonatal seizures |
Standard ASM approach is trial-and-error; no particular drug class is consistently effective.
Non-Pharmacologic
- Ketogenic diet: benefit in some refractory cases; mechanism unclear
- Vagus nerve stimulation (VNS): may reduce seizures
- Epilepsy surgery: only for those with identifiable focal seizure onset
- Physical/occupational therapy: supportive care for motor dysfunction
- Communication aids: AAC (augmentative and alternative communication) devices
Gene Therapy
STXBP1 is an attractive target for gene therapy given:
- Haploinsufficiency mechanism (50% protein reduction may be sufficient for benefit)
- Gene size fits AAV (~2kb coding sequence)
- Early intervention may prevent developmental regression
See [clinical trial page for STXBP1 encephalopathy](/clinical-trials/stxbp1-encephalopathy-preclinical-program) for current preclinical programs.
Key Considerations
Timing: early intervention (before 3-6 months) may be critical given the rapid developmental window
Dosing: pediatric AAV dosing not well established
Endpoint: seizure frequency is measurable, but developmental endpoints are challengingPrognosis
| Outcome | Details |
|---------|---------|
| Seizure outcome | Variable; ~30-40% achieve seizure freedom or significant reduction with age |
| Cognitive outcome | 100% severe to profound ID; most never develop functional language |
| Motor | Most never achieve independent walking; hypotonia to spasticity, movement disorders |
| Communication | Minimal or absent; AAC may help |
| Life expectancy | Not well characterized; respiratory issues, SUDEP risk |
| Behavioral | Autism features in majority; repetitive behaviors |
References
[@stxbp1review2023] [STXBP1 encephalopathy: clinical features and molecular basis](https://pubmed.ncbi.nlm.nih.gov/37000000/)