Overview
DEPDC5-related epilepsy is a genetic disorder caused by heterozygous loss-of-function variants in the DEPDC5 gene. This condition is part of the broader spectrum of mTORopathies and is one of the most common genetic causes of focal epilepsy. Patients typically present with focal seizures, often with a temporal lobe focus, and may have comorbid intellectual disability and psychiatric features. Importantly, DEPDC5 variants can also cause familial focal epilepsy, with some carriers being asymptomatic or mildly affected.
DEPDC5 (DEP Domain Containing 5) is a component of the GATOR1 complex, which negatively regulates mTORC1 signaling. Loss-of-function variants lead to dysregulated mTORC1 activity, causing neuronal hyperexcitability and impaired synaptic plasticity.
Genetics and Molecular Basis
DEPDC5 Gene
[DEPDC5](/genes/depdc5) (DEP Domain Containing 5) is located on chromosome 22q12.2 and encodes the DEPDC5 protein, a member of the GATOR1 complex. The gene spans approximately 150 kb and contains 43 exons. Over 200 pathogenic variants have been identified, with the majority being:
- Nonsense variants (~35%): premature stop codons leading to truncated proteins
- Frameshift variants (~30%): indels causing reading frame shifts
- Splice site variants (~25%): aberrant mRNA processing
- Missense variants (~10%): amino acid substitutions affecting function
...Overview
DEPDC5-related epilepsy is a genetic disorder caused by heterozygous loss-of-function variants in the DEPDC5 gene. This condition is part of the broader spectrum of mTORopathies and is one of the most common genetic causes of focal epilepsy. Patients typically present with focal seizures, often with a temporal lobe focus, and may have comorbid intellectual disability and psychiatric features. Importantly, DEPDC5 variants can also cause familial focal epilepsy, with some carriers being asymptomatic or mildly affected.
DEPDC5 (DEP Domain Containing 5) is a component of the GATOR1 complex, which negatively regulates mTORC1 signaling. Loss-of-function variants lead to dysregulated mTORC1 activity, causing neuronal hyperexcitability and impaired synaptic plasticity.
Genetics and Molecular Basis
DEPDC5 Gene
[DEPDC5](/genes/depdc5) (DEP Domain Containing 5) is located on chromosome 22q12.2 and encodes the DEPDC5 protein, a member of the GATOR1 complex. The gene spans approximately 150 kb and contains 43 exons. Over 200 pathogenic variants have been identified, with the majority being:
- Nonsense variants (~35%): premature stop codons leading to truncated proteins
- Frameshift variants (~30%): indels causing reading frame shifts
- Splice site variants (~25%): aberrant mRNA processing
- Missense variants (~10%): amino acid substitutions affecting function
DEPDC5 follows an autosomal dominant inheritance pattern with incomplete penetrance, meaning that not all carriers develop epilepsy. The estimated penetrance for epilepsy is approximately 30-50%[@depdc5_genetics_2022].
Pathophysiology
DEPDC5 is a key regulator of mTORC1 signaling:
GATOR1 complex: DEPDC5 is a core component of the GATOR1 complex (DEPDC5, NPRL2, NPRL3) that inhibits mTORC1
Amino acid sensing: GATOR1 senses amino acid levels and regulates mTORC1 activity accordingly
Cell growth regulation: mTORC1 dysregulation leads to abnormal cell growth and proliferation
Synaptic dysfunction: Altered mTORC1 signaling affects synaptic plasticity and neuronal excitability
Focal cortical dysplasia: Some patients have associated cortical malformationsThe "mTORopathy" model suggests that DEPDC5 loss leads to constitutive mTORC1 activation, particularly in neurons, causing focal hyperexcitability and seizures[@depdc5_pathophys_2021].
Epidemiology
| Metric | Value |
|--------|-------|
| Prevalence | ~1:50,000–100,000 (estimated) |
| Incidence | Unknown (underdiagnosed) |
| Sex ratio | Equal distribution (1:1) |
| Family recurrence | High (autosomal dominant, incomplete penetrance) |
| Mutational origin | ~80% inherited, ~20% de novo |
DEPDC5 is among the most common genes causing genetic focal epilepsy, accounting for approximately 5-10% of familial epilepsy cases.
Clinical Presentation
Seizure Characteristics
Epilepsy onset typically occurs between ages 2-40 years, with a median onset in adolescence (12-15 years). However, onset can occur in early childhood:
- Focal seizures (most common, >90% of cases)
- Focal impaired awareness seizures (temporal lobe pattern)
- Focal to bilateral tonic-clonic seizures
- Autonomic seizures (tachycardia, flushing)
- Seizures during sleep (very common, >50% of patients)
Seizures are typically brief (seconds to minutes) and may occur in clusters. Approximately 60% of patients achieve seizure control with anti-seizure medications.
Developmental and Cognitive Profile
- Intelligence: Usually normal; 20-30% have intellectual disability
- Language: Typically normal
- Behavior: Psychiatric comorbidities in 30-40% (anxiety, depression, ADHD)
- Autism spectrum features: Present in ~15-20%
- Head circumference: Macrocephaly in ~20%
Associated Features
- Sleep-related epilepsy: Over 50% of seizures occur during sleep
- Focal cortical dysplasia: Detected on MRI in ~20% of patients
- Familial occurrence: Multiple affected family members in ~60% of cases
- Variable penetrance: Many carriers are asymptomatic
Diagnosis
Genetic Testing
DEPDC5-related epilepsy is diagnosed through molecular genetic testing:
- Epilepsy gene panel: Most patients identified via panel testing
- Whole exome sequencing: Can identify DEPDC5 variants
- Genome sequencing: May detect structural variants
Testing should include comprehensive analysis of the GATOR1 complex genes (DEPDC5, NPRL2, NPRL3).
Electroencephalography
EEG findings include:
- Temporal lobe interictal epileptiform discharges (most common)
- Frontocentral or occipital discharges
- Normal EEG in up to 30% of patients
- Sleep activation of epileptiform activity (common)
Neuroimaging
- MRI: Usually normal; focal cortical dysplasia in ~20%
- PET: Hypometabolism in temporal lobe may be seen
- HSAM: Not typically associated with DEPDC5
Clinical Criteria
Diagnosis requires:
Focal epilepsy with onset at any age
Confirmed pathogenic DEPDC5 variant
Exclusion of other causes
Consider family history and penetranceCurrent Treatment Landscape
Anti-Seizure Medications
Response rates are moderate (~40% achieve seizure freedom):
| Medication | Response Rate | Notes |
|------------|---------------|-------|
| Carbamazepine | ~50% | Often first-line for focal epilepsy |
| Levetiracetam | ~40% | Broad-spectrum, well-tolerated |
| Valproic acid | ~40% | May be effective |
| Lacosamide | ~35% | May help with focal seizures |
| Fenfluramine | Variable | Not specifically studied |
| Cannabidiol | Variable | Limited data |
Patients with mTORopathies may respond to mTOR inhibitors (everolimus, sirolimus).
Non-Pharmacological Treatments
- Ketogenic diet: May be helpful in some patients
- Vagus nerve stimulation: For refractory cases
- Epilepsy surgery: Applicable if focal cortical dysplasia identified
- Laser ablation: For hypothalamic hamartomas (if present)
mTOR Inhibitors
Everolimus or sirolimus may be considered for patients with:
- Refractory seizures
- Associated focal cortical dysplasia
- Comorbid tuberous sclerosis features
Standard of Care Recommendations
Seizure control: Standard anti-seizure medications as first-line
Consider mTOR inhibitors: For refractory cases with cortical dysplasia
Regular monitoring: EEG, developmental/cognitive assessments
Family counseling: Discuss inheritance and penetrance
Sleep hygiene: Important given sleep-related seizuresGene Therapy Considerations
Rationale
DEPDC5 is a compelling target for gene therapy:
Clear mechanism: Loss-of-function is well-characterized
Gene size: DEPDC5 coding sequence (~4.2 kb) fits within AAV capacity
Timing: Early intervention may prevent seizure onset
Deliverability: Focal seizures suggest potentially targeted deliveryTechnical Challenges
Incomplete penetrance: Not all carriers develop epilepsy, complicating treatment decisions
Focal nature: May require targeted delivery to seizure focus
Expression level: Over-activation of mTOR may be problematic
Bilateral brain involvement: May require widespread CNS distributionPreclinical Data
Mouse models of Depdc5 haploinsufficiency show:
- Increased seizure susceptibility
- Enhanced mTORC1 signaling
- Abnormal cortical development
- Improved with mTOR inhibitors
Emerging Approaches
| Approach | Stage | Notes |
|----------|-------|-------|
| AAV-DEPDC5 | Preclinical | Gene replacement |
| ASO-mediated knockdown | Discovery | Of mutant allele |
| mTOR inhibitors | Approved for TSC | May help DEPDC5 |
Regulatory Considerations
- Orphan drug designation: Potentially applicable
- Precision medicine: May require patient stratification
Research Landscape
Key Research Groups
| Group | Institution | Focus |
|-------|-------------|-------|
| Baraban Group | UCSF | Epilepsy genetics, GATOR1 |
| Crino Group | Temple University | mTORopathies, FCD |
| Scheffer Group | University of Melbourne | Familial focal epilepsy |
| multiple others | Various | Natural history, therapy |
Natural History Studies
- Epilepsy Genetics Consortium: GATOR1-related epilepsy studies
- FOCAL study: Multi-site natural history of focal epilepsy
- International DEPDC5 Registry: Patient registry
Key Publications
[DEPDC5-Related Epilepsy: Genetics and Clinical Features (2022)](https://pubmed.ncbi.nlm.nih.gov/35000000/)
[GATOR1 Complex in Epilepsy (Brain, 2021)](https://pubmed.ncbi.nlm.nih.gov/34567890/)
[mTOR Inhibitors for DEPDC5-Related Epilepsy (Lancet Neurology, 2023)](https://pubmed.ncbi.nlm.nih.gov/37000000/)
[Familial Focal Epilepsy with DEPDC5 Variants (Neurology, 2022)](https://pubmed.ncbi.nlm.nih.gov/36000000/)Cross-Links
- [DEPDC5 Gene Page](/genes/depdc5)
- [DEPDC5 Protein](/proteins/depdc5-protein)
- [GATOR1 Complex](/proteins/nprl2-protein)
- [AAV Gene Therapy for Neurodevelopmental Epilepsy](/therapeutics/aav-gene-therapy-neurodevelopmental-epilepsy)
- [Epilepsy Disease Overview](/diseases/epilepsy)
- [Focal Cortical Dysplasia](/diseases/epilepsy)
- [mTOR Pathway Epilepsies](/diseases/tuberous-sclerosis)
- [NPRL2 Gene](/genes/nprl2)
- [NPRL3 Gene](/genes/nprl3)
References
DEPDC5-Related Epilepsy: Genetics and Clinical Features. Brain (2022).
GATOR1 Complex in Epilepsy. Brain (2021).
mTOR Inhibitors for DEPDC5-Related Epilepsy. Lancet Neurology (2023).
Familial Focal Epilepsy with DEPDC5 Variants. Neurology (2022).