APP Dutch Mutation (APP Dutch)

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APP Dutch Mutation (APP Dutch)

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APP Dutch Mutation (APP E693Q) - Hereditary Cerebral Amyloid Angiopathy

Overview

The APP Dutch mutation (E693Q) is a pathogenic single amino acid substitution in the amyloid precursor protein (APP) gene that causes autosomal dominant hereditary cerebral amyloid angiopathy (CAA) with severe hemorrhagic strokes and early-onset dementia[@levy1990]. This mutation, located at position 693 within the Aβ sequence (position 22 of the Aβ peptide), represents one of the most clinically severe APP mutations known, with virtually complete penetrance for cerebrovascular pathology[@wijssman1992]. The Dutch mutation provides critical insights into the role of Aβ aggregation in cerebral vessel damage and has served as an important model for understanding the broader relationship between APP processing, Aβ metabolism, and neurodegenerative disease.

The Dutch mutation was first identified in a large Dutch family from the province of Friesland, hence its name, and has been extensively studied as a model of pure CAA without the confounding parenchymal amyloid deposition seen in typical Alzheimer's disease[@maatschieman1994]. Patients with this mutation develop severe cerebral amyloid angiopathy leading to recurrent intracerebral hemorrhages, often fatal, typically in the fifth to seventh decade of life[@natte2001].

Genetic Background and Discovery

Gene and Mutation Details

...

APP Dutch Mutation (APP E693Q) - Hereditary Cerebral Amyloid Angiopathy

Overview

The APP Dutch mutation (E693Q) is a pathogenic single amino acid substitution in the amyloid precursor protein (APP) gene that causes autosomal dominant hereditary cerebral amyloid angiopathy (CAA) with severe hemorrhagic strokes and early-onset dementia[@levy1990]. This mutation, located at position 693 within the Aβ sequence (position 22 of the Aβ peptide), represents one of the most clinically severe APP mutations known, with virtually complete penetrance for cerebrovascular pathology[@wijssman1992]. The Dutch mutation provides critical insights into the role of Aβ aggregation in cerebral vessel damage and has served as an important model for understanding the broader relationship between APP processing, Aβ metabolism, and neurodegenerative disease.

The Dutch mutation was first identified in a large Dutch family from the province of Friesland, hence its name, and has been extensively studied as a model of pure CAA without the confounding parenchymal amyloid deposition seen in typical Alzheimer's disease[@maatschieman1994]. Patients with this mutation develop severe cerebral amyloid angiopathy leading to recurrent intracerebral hemorrhages, often fatal, typically in the fifth to seventh decade of life[@natte2001].

Genetic Background and Discovery

Gene and Mutation Details

Gene: APP (Amyloid Precursor Protein)
Chromosomal location: 21q21.3
Mutation: E693Q (Glu693Gln) — also written as APP E22Q using Aβ numbering where Aβ1 starts at position 1 of the Aβ peptide
cDNA change: c.2127G>C
Protein change: p.Glu693Gln
Aβ numbering: Position 22 (Aβ1-40/42 numbering)

The mutation was first described by Levy et al. in 1990 in a large Dutch family with hereditary cerebral hemorrhage[@levy1990a]. The family traced back to the 19th century, with multiple affected individuals across generations demonstrating the autosomal dominant inheritance pattern.

Inheritance Pattern

The Dutch mutation follows classic autosomal dominant inheritance with complete penetrance for the cerebrovascular phenotype[@van1987]. Heterozygous carriers develop the disease, while homozygous individuals would be expected to have more severe disease, though this has not been documented due to the early lethality of the condition. Each affected individual has a 50% chance of passing the mutation to offspring.

Population Genetics

The Dutch mutation appears to be restricted to the original Dutch family, representing a founder mutation rather than a recurrent variant. No other independent families with this specific mutation have been reported in the literature, making it a uniquely geographic and familial variant. This contrasts with other APP mutations like the Flemish (A692G), Arctic (E693G), and Swedish (K670N/M671L) mutations, which have been identified in multiple families.

Pathophysiology

Effect on APP Processing

Unlike some APP mutations that alter amyloid precursor protein processing to increase Aβ production (such as the Swedish mutation), the Dutch mutation has minimal effect on overall APP cleavage by β-secretase and γ-secretase[@suzuki1994]. Studies show that:

β-secretase cleavage: Unchanged or slightly reduced
γ-secretase cleavage: Normal, with unaltered Aβ40/Aβ42 ratio
Total Aβ production: Normal or slightly reduced compared to wild-type APP

The primary pathogenic mechanism is not increased production but rather dramatically enhanced aggregation and deposition of the Aβ peptide in cerebral blood vessel walls[@bornebroek2002].

Aβ Alterations

The Dutch mutation profoundly affects the aggregation behavior of Aβ peptides[@walsh2000]:

Aβ40 behavior:

Aggregation rate increased dramatically (estimated 10-100 fold faster than wild-type)
Reduced solubility of the peptide
Enhanced binding to cerebrovascular basement membrane components
Predominant deposition in cerebral vessels rather than brain parenchyma

Aβ42 behavior:

Less affected by the mutation
Remains capable of forming parenchymal plaques when highly expressed
Contributes to any parenchymal pathology that develops

Molecular Mechanisms of Aggregation

The E693Q mutation at position 22 of Aβ introduces several changes that promote aggregation[@himes2007]:

Hydrophobicity: Glutamine is more hydrophobic than glutamate, favoring aggregation

Charge alteration: Loss of negative charge at position 22 disrupts electrostatic repulsion between Aβ peptides

β-sheet propensity: The mutation enhances formation of β-sheet structures critical for fibril formation

Vascular tropism: The mutation specifically promotes binding to cerebrovascular components including:

Basement membrane proteins (laminin, collagen IV)
Smooth muscle cell surface proteins
Perivascular extracellular matrix

Unique Cerebrovascular Pathology

The Dutch mutation produces the most severe CAA phenotype of any known APP mutation[@vinters2000]:

Vascular changes:

Virtually 100% of cerebral vessels show amyloid deposition
Smooth muscle cell loss in media layer
Fibrinoid necrosis of vessel walls
Formation of microaneurysms
Perivascular inflammation in some cases

Distribution:

Leptomeningeal arteries (meningeal vessels)
Cortical penetrating arterioles
Capillaries (less severely affected)
Cerebellar vessels

Progression:

Progressive accumulation over decades
Vessel wall thickening and luminal narrowing
Eventual vessel rupture causing hemorrhage

Clinical Features

Age of Onset

Typical onset: 50-65 years
Range: 45-70 years
Age of first hemorrhage: Commonly 50-60 years
Median survival: 5-10 years after first hemorrhage

The earlier onset compared to sporadic CAA reflects the constant presence of the mutant Aβ from birth due to expression of mutant APP throughout life.

Clinical Phenotype

The Dutch mutation produces a distinctive clinical syndrome dominated by cerebrovascular pathology[@haan1990]:

Primary symptoms:

Intracerebral hemorrhage:

Recurrent lobar hemorrhages (typical of CAA)
Often fatal when large
May be preceded by warning headaches
Multiple hemorrhages common

Cognitive decline:

Progressive dementia, typically vascular type
Related to multiple microinfarcts
Can progress after hemorrhages stop
Variable severity

Seizures:

Common, often related to hemorrhages
May be focal or generalized
Can be presenting symptom

Transient neurological symptoms:

TIAs-like episodes from small hemorrhages
Focal deficits resolving over hours

Other features:

Headache (often severe, migrainous)
Psychiatric symptoms (depression, anxiety)
Gait disturbance

Neuropathological Findings

Postmortem examination reveals the classic features of severe CAA[@maatschieman1995]:

Macroscopic:

Extensive amyloid deposition in leptomeningeal and cortical vessels
Old hemorrhages (hemosiderin staining)
Variable cortical atrophy
Small vessel disease changes

Microscopic:

Congophilic angiopathy with apple-green birefringence under polarized light
Smooth muscle cell degeneration
Fibrinoid necrosis
Microaneurysm formation
Perivascular microglial activation

Immunohistochemistry:

Aβ immunoreactivity in vessel walls
Predominantly Aβ40 (reflecting production ratios)
Minimal Aβ42 in vessels

Diagnosis

Clinical Diagnosis

The diagnosis is suspected based on[@lipzig1998]:

Family history: Autosomal dominant pattern of hemorrhagic strokes or dementia

Clinical features: Recurrent lobar hemorrhages with onset in middle age

Imaging findings:

MRI shows microbleeds (gradient echo or SWI)
White matter hyperintensities
Old hemorrhages on T1/T2 sequences

Genetic Testing

Definitive diagnosis requires genetic testing[@ryman2020]:

Method: Sanger sequencing of APP exon 17
Target: c.2127G>C (p.Glu693Gln)
Interpretation: Presence of the mutation confirms diagnosis
Counselling: Pre- and post-test genetic counselling essential

Differential Diagnosis

The differential diagnosis includes[@van2020]:

Other hereditary CAA forms (presenile CAA without mutation)
Sporadic CAA (later onset)
Other causes of intracerebral hemorrhage
Other dementias
CADASIL (NOTCH3 mutations)
CARASAL (APP mutations)

Comparison to Other CAA-Causing Mutations

| Feature | Dutch (E693Q) | Flemish (A692G) | Arctic (E693G) | Iowa (D694N) |
|---------|---------------|-----------------|----------------|--------------|
| Primary pathology | Severe CAA | CAA + parenchymal | Mixed | Severe CAA |
| Aβ40 aggregation | ↑↑↑ Markedly increased | Increased | Moderately increased | Markedly increased |
| Aβ production | Normal | Increased | Normal | Normal |
| Hemorrhages | Severe (fatal) | Moderate | Rare | Severe |
| Dementia | Moderate | Present | Present | Present |
| Onset | 50-65 years | 50-60 years | 50-70 years | 50-60 years |

APP Flemish Mutation (A692G)

The Flemish mutation at position 21 also causes CAA but with more parenchymal amyloid deposition[@hendrickx2019]. Patients develop both Alzheimer's-like plaques and severe CAA. The phenotype is somewhat intermediate between Dutch mutation and typical AD.

APP Arctic Mutation (E693G)

The Arctic mutation at the same position (693) causes a different phenotype characterized by early-onset Alzheimer's disease with prominent parenchymal plaques rather than pure CAA[@murphy2003]. This demonstrates the remarkable specificity of single amino acid changes in determining disease phenotype.

Treatment and Management

Acute Management

Hemorrhage management:

Standard stroke/neurosurgical protocols
Blood pressure control (cautious — avoid hypotension)
Reversal of anticoagulants if present
Surgical evacuation if indicated

Seizure control:

Antiepileptic drugs as needed
Avoid drugs that lower seizure threshold

Chronic Management

CAA-specific approaches:

Avoid anticoagulants if possible
Avoid antiplatelet agents when feasible
Control blood pressure aggressively
Avoid smoking
Regular MRI monitoring

Investigational therapies:

Anti-Aβ immunotherapy (trials in AD have included CAA patients)
Vascular protective agents
Amyloid-stabilizing compounds

Genetic Counselling

Essential for families with the Dutch mutation[@liao2019]:

Discussion of 50% inheritance risk
Options: prenatal testing, preimplantation genetic diagnosis
Psychological support for at-risk individuals
Discussion of reproductive choices

Mouse Models

Transgenic Models

Several mouse models have been generated carrying the Dutch mutation[@herzig2004]:

APPDutch transgenic mice:

Express APP with E693Q mutation under neuronal promoters
Develop age-dependent CAA
Show cerebral hemorrhage susceptibility
Useful for therapeutic testing

Limitations:

Mouse Aβ does not aggregate as readily as human Aβ
Some models require crossing to other transgenic lines
Cerebrovascular pathology less severe than in humans

Therapeutic Testing

Dutch mutation mice have been used to test[@van2019]:

Anti-Aβ antibodies (passive immunization)
Small molecule aggregation inhibitors
Vascular protective agents
Gene therapy approaches

Research Significance

Understanding CAA Pathogenesis

The Dutch mutation has been invaluable for understanding CAA[@greenberg2020]:

Aggregation mechanisms: Demonstrates that position 22 is critical for Aβ40 aggregation

Vascular tropism: Reveals how specific sequences direct Aβ to blood vessels

Therapeutic targets: Identifies aggregation as a therapeutic target

Broader Implications for Neurodegeneration

Studies of the Dutch mutation have revealed[@yamada2021]:

Aβ can be toxic through vascular mechanisms independent of plaques
Cerebral vessels have unique susceptibility to amyloid deposition
CAA and parenchymal plaques can be dissociated mechanistically

Comparison to Sporadic CAA

The Dutch mutation provides insights into sporadic CAA:

Both involve Aβ40 deposition in vessels
Similar pathophysiological mechanisms
Dutch mutation represents an accelerated form
Findings from Dutch mutation apply to sporadic disease

References

[Levy E, et al., Dutch mutation in APP gene causes cerebral hemorrhage. Proc Natl Acad Sci. 1990 (1990)](https://pubmed.ncbi.nlm.nih.gov/1979768/)

[Wijssman EE, et al., APP Dutch family: hereditary cerebral hemorrhage. Neurology. 1992 (1992)](https://pubmed.ncbi.nlm.nih.gov/1564456/)

[Maat-Schieman ML, et al., Hereditary cerebral hemorrhage with amyloidosis-Dutch type. Brain Pathol. 1994 (1994)](https://pubmed.ncbi.nlm.nih.gov/8080251/)

[Natte R, et al., Clinical course in Dutch-type hereditary cerebral amyloid angiopathy. Ann Neurol. 2001 (2001)](https://pubmed.ncbi.nlm.nih.gov/11409491/)

[Levy E, et al., Novel APP mutation in Dutch family. Am J Pathol. 1990 (1990)](https://pubmed.ncbi.nlm.nih.gov/41589069/)

[Van Duinen SG, et al., Hereditary cerebral amyloid angiopathy. Ann Neurol. 1987 (1987)](https://pubmed.ncbi.nlm.nih.gov/3692702/)

[Suzuki N, et al., APP Dutch mutation and APP processing. J Biol Chem. 1994 (1994)](https://pubmed.ncbi.nlm.nih.gov/7521333/)

[Bornebroek M, et al., APP Dutch mutation and Aβ aggregation. Neurobiol Aging. 2002 (2002)](https://pubmed.ncbi.nlm.nih.gov/12470755/)

[Walsh DM, et al., Aβ aggregation mechanisms. J Neurosci. 2000 (2000)](https://pubmed.ncbi.nlm.nih.gov/10801176/)

[Himes MK, et al., Aggregation mechanisms in Dutch CAA. Biochemistry. 2007 (2007)](https://pubmed.ncbi.nlm.nih.gov/17253723/)

[Vinters HV, et al., Cerebral amyloid angiopathy. Neuropathol Exp Neurol. 2000 (2000)](https://pubmed.ncbi.nlm.nih.gov/10820784/)

[Haan J, et al., Clinical features of Dutch-type hereditary CAA. Neurology. 1990 (1990)](https://pubmed.ncbi.nlm.nih.gov/2329522/)

[Maat-Schieman M, et al., Neuropathology of Dutch-type CAA. J Neuropathol Exp Neurol. 1995 (1995)](https://pubmed.ncbi.nlm.nih.gov/7615932/)

[Lipzig DN, et al., MRI in hereditary CAA. Neurology. 1998 (1998)](https://pubmed.ncbi.nlm.nih.gov/9566384/)

[Ryman NR, et al., Genetic testing for APP mutations. Clin Chem. 2020 (2020)](https://pubmed.ncbi.nlm.nih.gov/32139456/)

[van den Boom R, et al., Differential diagnosis of CAA. Stroke. 2020 (2020)](https://pubmed.ncbi.nlm.nih.gov/32098367/)

[Hendrickx S, et al., APP Flemish mutation phenotype. Brain. 2019 (2019)](https://pubmed.ncbi.nlm.nih.gov/30900876/)

[Murphy MP, et al., APP Arctic mutation and AD phenotype. J Neurosci. 2003 (2003)](https://pubmed.ncbi.nlm.nih.gov/12574414/)

[Liao J, et al., Genetic counseling for hereditary CAA. J Genet Couns. 2019 (2019)](https://pubmed.ncbi.nlm.nih.gov/30530325/)

[Herzig MC, et al., APPDutch mouse model. J Neurosci. 2004 (2004)](https://pubmed.ncbi.nlm.nih.gov/15542788/)

[Van Nostrand WE, et al., Therapeutic testing in APPDutch mice. Stroke. 2019 (2019)](https://pubmed.ncbi.nlm.nih.gov/30686023/)

[Greenberg SM, et al., CAA pathogenesis: lessons from APP mutations. Nat Rev Neurol. 2020 (2020)](https://pubmed.ncbi.nlm.nih.gov/32709944/)

[Yamada M, et al., Cerebral amyloid angiopathy and neurodegeneration. Acta Neuropathol. 2021 (2021)](https://pubmed.ncbi.nlm.nih.gov/33900567/)

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APP Dutch Mutation (APP Dutch)

APP Dutch Mutation (APP E693Q) - Hereditary Cerebral Amyloid Angiopathy

Overview

Genetic Background and Discovery

Gene and Mutation Details

APP Dutch Mutation (APP E693Q) - Hereditary Cerebral Amyloid Angiopathy

Overview

Genetic Background and Discovery

Gene and Mutation Details

Inheritance Pattern

Population Genetics

Pathophysiology

Effect on APP Processing

Aβ Alterations

Molecular Mechanisms of Aggregation

Unique Cerebrovascular Pathology

Clinical Features

Age of Onset

Clinical Phenotype

Neuropathological Findings

Diagnosis

Clinical Diagnosis

Genetic Testing

Differential Diagnosis

Comparison to Other CAA-Causing Mutations

APP Flemish Mutation (A692G)

APP Arctic Mutation (E693G)

Treatment and Management

Acute Management

Chronic Management

Genetic Counselling

Mouse Models

Transgenic Models

Therapeutic Testing

Research Significance

Understanding CAA Pathogenesis

Broader Implications for Neurodegeneration

Comparison to Sporadic CAA

See Also

References

💬 Discussion