¶ Cerebral Amyloid Angiopathy: Subtypes and Genetic Variants
Cerebral Amyloid Angiopathy (CAA) is a heterogeneous cerebrovascular disorder with distinct subtypes and strong genetic determinants. Understanding this heterogeneity is crucial for accurate diagnosis, prognosis, and developing targeted therapeutic interventions.
Cerebral Amyloid Angiopathy is characterized by amyloid-beta (Aβ) deposition in the walls of cerebral blood vessels. The clinical presentation, disease progression, and response to therapy vary significantly based on CAA subtype and underlying genetic factors. CAA represents a significant cause of lobar intracerebral hemorrhage and contributes to vascular cognitive impairment in aging and Alzheimer's disease.
Sporadic CAA represents the most common form, accounting for approximately 90% of cases. It typically presents in late adulthood (age >65 years) and is strongly associated with advancing age.
Clinical Features:
- Lobar intracerebral hemorrhages
- Cerebral microbleeds
- Cortical superficial siderosis
- Cognitive decline
- Transient focal neurological episodes
Pathological Characteristics:
- Aβ40 predominance in vascular deposits
- Preference for leptomeningeal and cortical vessels
- Variable involvement of capillaries
- Association with apolipoprotein E ε4 allele
Several autosomal dominant forms of CAA exist, characterized by earlier onset and specific genetic mutations.
Mutations in the amyloid precursor protein (APP) gene on chromosome 21 can cause hereditary cerebral amyloid angiopathies:
| Mutation |
Origin |
Key Features |
| E693Q (Dutch) |
Netherlands |
Early-onset lobar hemorrhages (40-50 years), severe CAA |
| D694N (Iowa) |
Iowa |
Progressive cognitive decline, extensive vascular amyloid |
| K670N/M671L (Flemish) |
Belgian |
Early-onset hemorrhages, AD-like phenotype |
| L705V (Italian) |
Italy |
Early hemorrhagic strokes, Aβ40 vascular amyloid |
| E693G (Arctic) |
Sweden |
Cognitive impairment, parenchymal plaques |
| E22G (Arctic) |
Swedish |
Enhanced Aβ protofibril formation |
| D23N (Iowa) |
Iowa |
Reduced clearance, minimal parenchymal Aβ |
The Dutch mutation (APP E693Q) is particularly noteworthy, causing severe cerebrovascular amyloid with hemorrhagic strokes occurring in the fourth decade of life.
Cystatin C (CST3) is a cysteine protease inhibitor that interacts with Aβ. The Icelandic mutation (CST3 L68P) causes hereditary cerebral hemorrhage with amyloidosis (HCHWA-I):
- Autosomal dominant inheritance
- Severe Aβ deposition in cerebral vessels
- Hemorrhagic strokes in the third to fourth decade
- Additional deposition in systemic vessels
The ITM2B gene encodes the BRI2 protein. Mutations causing familial British dementia (FBD) and familial Danish dementia (FDD) lead to production of abnormal Aβ-like peptides:
- Familial British Dementia (FBD): ITM2B stop codon mutation (W198X) produces BRI-Aβ peptide
- Familial Danish Dementia (FDD): 10-bp deletion produces BRI-J peptide
- Both cause CAA in addition to parenchymal amyloid and neurofibrillary tangles
Individuals with trisomy 21 have three copies of the APP gene, resulting in increased Aβ production. This makes Down syndrome an important genetic risk factor for early-onset CAA:
- CAA develops in the third to fourth decade
- Often coexists with Alzheimer's disease pathology
- Contributes to early-onset cognitive decline
- Represents a genetic model of APP overexpression
This is an inflammatory variant of CAA characterized by:
- Perivascular and intramural lymphocytic inflammation
- Acute onset of headache, cognitive decline, or seizures
- May respond to immunotherapy
- Represents an autoimmune response to vascular Aβ
The coexistence of CAA and Alzheimer's disease is common and represents a distinct subtype:
Features:
- Both parenchymal Aβ plaques and vascular amyloid
- Shared APOE ε4 risk factor
- More severe cognitive impairment
- Higher hemorrhage risk
- Mixed pathology at autopsy
APOE is the strongest genetic determinant of sporadic CAA:
APOE ε4 Allele:
- Dose-dependent increase in CAA risk
- Earlier age of onset
- Greater vascular amyloid burden
- Increased hemorrhage risk
- Reduced Aβ clearance from cerebral vessels
APOE ε2 Allele:
- Associated with hemorrhagic complications
- May increase aneurysm formation
- Interaction with ε4 modifies risk
APOE Risk Table:
| APOE Allele |
Effect on CAA Risk |
| ε4/ε4 |
3-5x increased risk |
| ε4/ε3 |
2-3x increased risk |
| ε3/ε3 |
Baseline risk |
| ε2/ε2 |
May increase hemorrhagic risk |
Presenilin Mutations (PSEN1, PSEN2):
- Cause early-onset AD with CAA
- Alter Aβ42/Aβ40 ratio
- Can present with hemorrhagic strokes
Trem2 Variants:
- Microglial activation gene
- Associated with increased CAA risk
- May affect Aβ clearance
ABCA1:
- Cholesterol transporter
- Modulates APOE function
- Genetic variants influence CAA risk
GWAS-Identified Loci:
- CST3 region: Variants affecting cystatin C levels
- CLU (Clusterin): Associated with CAA-related ICH risk
- PICALM: Linked to cerebral amyloid and AD
Lobar intracerebral hemorrhage is the hallmark of CAA:
Risk Factors:
- Advanced age
- APOE ε4 homozygosity
- Anticoagulant use
- Hypertension (controversial)
- Cerebral microbleeds on MRI
Recurrence Risk:
- Annual recurrence rate: 5-10%
- Higher with multiple hemorrhages
- Reduced with blood pressure control
CAA frequently causes cognitive impairment:
Pattern:
- Executive dysfunction prominent
- Processing speed impairment
- Episodic memory relatively preserved initially
- Progressive decline
CAA can cause brief, recurrent neurological symptoms:
- Duration: minutes to hours
- Recurring stereotyped episodes
- Often sensory or motor
- Associated with cortical superficial siderosis
MRI is essential for CAA diagnosis:
Key Findings:
- Cerebral microbleeds (lobar distribution)
- Cortical superficial siderosis
- White matter hyperintensities
- Recent lobar hemorrhage
- Atrophy patterns
Advanced Techniques:
- SWI (susceptibility-weighted imaging)
- DTI (diffusion tensor imaging)
- Perivascular space enlargement
- Post-contrast leakage imaging
Aβ Analysis:
- Reduced Aβ40 in CSF (vascular removal)
- Aβ40/Aβ42 ratio alterations
- Amyloid PET positivity
Neurodegeneration Markers:
- Elevated neurofilament light chain
- Increased tau proteins
Indications for genetic testing:
- Early-onset CAA (<55 years)
- Family history of CAA or hemorrhagic stroke
- Suspicious pedigree pattern
- Blood pressure control (cautious)
- Avoid anticoagulation when possible
- Surgical considerations (hematoma, location)
- Anticoagulant reversal if needed
- Target blood pressure: <130/80 mmHg
- Avoid nocturnal hypotension
- Smoking cessation
- Moderate alcohol consumption
- Anti-Amyloid Therapies: Immunotherapy targeting Aβ
- Small molecule aggregation inhibitors
- Vascular Protection: smooth muscle cell stabilizers
- PET ligands for vascular amyloid
- CSF Aβ40 as CAA-specific marker
- MRI techniques for vessel wall imaging
- Monoclonal antibodies against Aβ
- Gene therapy for hereditary forms
- Small molecule modulators
- Genotype-guided treatment selection
- Subtype-specific therapies
- Individualized risk assessment
Cerebral Amyloid Angiopathy represents a heterogeneous spectrum of disease with distinct subtypes and genetic determinants. Hereditary forms (APP, CST3, ITM2B mutations) provide insights into disease mechanisms and therapeutic targets, while understanding sporadic genetic risk factors (APOE polymorphism, GWAS loci) enables risk stratification and personalized approaches to management. Integration of genetic classification with clinical and imaging phenotypes will improve diagnosis and guide development of subtype-specific treatments.
- Charidimou et al., Cerebral amyloid angiopathy: emerging concepts (2015)
- van den Brink et al., Hereditary cerebral amyloid angiopathy (2014)
- Prescott et al., Hereditary cerebral amyloid angiopathy (2020)
- Holton et al., Cerebral amyloid angiopathy: updated review (2019)
- Jampana et al., APP mutations in cerebral amyloid angiopathy (2020)
- Ryman et al., Cerebral amyloid angiopathy in Down syndrome (2020)
- Biffi et al., Genetic variants and risk for CAA-related intracerebral hemorrhage (2011)
- Grebe et al., CST3 variants and cerebral amyloid angiopathy (2022)