FTD Subtype Comparison Matrix

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disease1622 wordssynced 2026-04-02

Frontotemporal Dementia (FTD) encompasses a spectrum of clinically and pathologically heterogeneous disorders. This comparison matrix provides a detailed analysis of the four primary FTD subtypes: behavioral variant FTD (bvFTD), semantic variant primary progressive aphasia (svPPA), nonfluent/agrammatic variant PPA (nfvPPA), and logopenic variant primary progressive aphasia (lvPPA).

> See Also: [Frontotemporal Dementia Overview](/diseases/frontotemporal-dementia), [TDP-43 Proteinopathy](/mechanisms/tdp-43-proteinopathy), [GRN Gene](/genes/grn), [MAPT Gene](/genes/mapT), [C9orf72 Gene](/genes/c9orf72)

Overview Comparison

| Feature | bvFTD | svPPA | nfvPPA | lvPPA |
|---------|-------|-------|--------|-------|
| Core Syndrome | Behavioral variant | Language variant | Language variant | Language variant |
| Primary Deficit | Behavior/social cognition | Word meaning/object knowledge | Speech production | Word retrieval/repetition |
| Typical Age of Onset | 45-65 years | 50-70 years | 50-70 years | 60-75 years |
| Disease Duration | 6-12 years | 8-15 years | 6-12 years | 6-10 years |
| Prevalence (of FTD) | ~60% | ~20% | ~15% | ~5% |

Clinical Features

Behavioral Variant FTD (bvFTD)

Core Diagnostic Features (Rascovsky criteria):

...

FTD Subtype Comparison Matrix

Overview Comparison

Clinical Features

Behavioral Variant FTD (bvFTD)

Core Diagnostic Features (Rascovsky criteria):

Disinhibition — Socially inappropriate behavior, loss of manners, impulsive actions

Apathy — Loss of initiative, decreased interest, reduced emotional expression

Loss of Empathy — Reduced concern for others, failure to recognize others' needs

Compulsive Behaviors — Ritualistic, repetitive movements, hoarding, utilization behaviors

Supporting Features:

Executive dysfunction (planning, organization, mental flexibility)
Social cognition deficits (recognizing emotions, social cues)
Motor behaviors (fidgeting, pacing, wandering)
Dietary changes (binge eating, food preferences)
Loss of insight (unawareness of changes)

Differential: Can mimic psychiatric disorders (bipolar, depression, OCD), AD, or vascular dementia.

Semantic Variant PPA (svPPA)

Core Features:

Anomia — Word-finding difficulty, particularly for low-frequency items
Single-word Comprehension Deficit — Loss of word meaning, especially for objects
Surface Dyslexia — Reading words with irregular pronunciation
Object Agnosia — Inability to recognize objects despite intact vision
Preserved Speech Fluency — Fluent, grammatically correct speech with empty content
Preserved Repetition — Normal repetition ability

Behavior Changes (later stage):

Loss of knowledge about people and objects
Behavioral features similar to bvFTD in later stages
Rigid food preferences (sweet foods)

Nonfluent/Agrammatic Variant PPA (nfvPPA)

Core Features:

Agrammatism — Omission of function words, simplified grammar, short phrases
Hesitant/Slow Speech — Effortful, halting speech production
Phonological Errors — Sound substitutions, omissions, distortions
Motor Speech Impairment — Apraxia of speech
Preserved Word Comprehension — Understanding of single words relatively intact
Preserved Object Knowledge — Object recognition maintained

Supporting Features:

Reading/writing impairment (spelling errors)
Impaired sentence comprehension for complex sentences
Aprosodia (monotone speech)
Mildbehavioral changes possible

Logopenic Variant PPA (lvPPA)

Core Features:

Word-finding Pauses — Frequent pauses during speech to retrieve words
Phonological Errors — Sound-level errors (substitutions, transpositions)
Impaired Repetition — Particularly for sentences, phrases
Spared Comprehension — Single-word and sentence comprehension intact
Spared Speech Fluency — Generally fluent, not halting like nfvPPA
Preserved Grammar — Grammatical structure preserved

Note: lvPPA is most commonly associated with underlying AD pathology rather than FTLD.

Imaging Patterns

Structural MRI (Typical Patterns)

| Subtype | Key Findings | Regions Affected |
|---------|-------------|------------------|
| bvFTD | Symmetric or asymmetric frontal/temporal atrophy | Orbitofrontal, dorsolateral prefrontal, anterior temporal |
| svPPA | Left anterior temporal lobe atrophy (often asymmetric) | Left anterior temporal pole, inferior temporal |
| nfvPPA | Left posterior frontal/inferior parietal atrophy | Left inferior frontal gyrus, premotor, insular |
| lvPPA | Left posterior temporal/parietal atrophy | Left temporoparietal junction, superior temporal |

FDG-PET Patterns

| Subtype | Hypometabolism Pattern |
|---------|----------------------|
| bvFTD | Frontal and anterior temporal lobes, anterior cingulate |
| svPPA | Left anterior temporal and inferior frontal |
| nfvPPA | Left inferior frontal and premotor |
| lvPPA | Left posterior temporal and parietal |

Tau PET (Flortaucipir)

bvFTD: Variable uptake — positive in tauopathy (CBD, PSP), negative in TDP-43 cases
svPPA: Typically negative (TDP-43 pathology)
nfvPPA: May show uptake in some cases (tauopathy)
lvPPA: Often positive (underlying AD pathology in majority of cases)

Genetic Associations

Known Genetic Causes

| Gene | Protein | Inheritance | Subtype Association | Pathology |
|------|---------|-------------|---------------------|-----------|
| MAPT | Tau protein | Autosomal dominant | bvFTD, PSP | FTLD-tau (3R/4R tau) |
| GRN | Progranulin | Autosomal dominant | bvFTD, CBD, PNFA | FTLD-TDP type A |
| C9orf72 | Dipeptide repeats | Autosomal dominant | bvFTD, ALS-FTD | FTLD-TDP type B |
| VCP | Valosin-containing protein | Autosomal dominant | bvFTD, IBM | FTLD-TDP type IV |
| FUS | Fused in sarcoma | Autosomal dominant | bvFTD | FTLD-FUS |
| CHCHD10 | Coiled-coil-helix-coiled-coil-helix domain 10 | Autosomal dominant | bvFTD, ALS-FTD | FTLD-TDP |

Frequency by Subtype

| Subtype | Familial % | Most Common Genes |
|---------|------------|-------------------|
| bvFTD | 30-40% | MAPT, GRN, C9orf72 |
| svPPA | 20-30% | GRN, MAPT |
| nfvPPA | 30-40% | GRN, MAPT |
| lvPPA | ~10% | Usually sporadic (APP/PSEN mutations rare) |

Pathological Classification

FTLD Subtypes

| Clinical Syndrome | Most Common Pathology | Other Possible Pathologies |
|-----------------|----------------------|---------------------------|
| bvFTD | FTLD-TDP (45%), FTLD-tau (40%) | FTLD-FUS (10%) |
| svPPA | FTLD-TDP type C (90%) | FTLD-tau, AD |
| nfvPPA | FTLD-tau type A (70%) | FTLD-TDP, AD |
| lvPPA | AD pathology (70-80%) | FTLD-TDP, FTLD-tau |

TDP-43 Subtypes

| FTLD-TDP Type | Clinical Correlates |
|--------------|--------------------|
| Type A (neuronal intranuclear inclusions) | bvFTD, nfvPPA, CBD |
| Type B (neuronal cytoplasmic inclusions) | bvFTD, ALS-FTD |
| Type C (DNR — dystrophic neurites) | svPPA |
| Type IV (VIP) | VCP-mutation FTD |

Treatment Approaches

Current Symptomatic Management

| Approach | bvFTD | svPPA | nfvPPA | lvPPA |
|----------|-------|-------|--------|-------|
| SSRIs | First-line for disinhibition, compulsions | Limited benefit | Limited benefit | Not effective |
| Antipsychotics | For severe agitation (off-label) | Not recommended | Not recommended | Not recommended |
| Stimulants | For apathy (low-dose) | Not used | Not used | Not used |
| Speech Therapy | Limited | Communication strategies | Speech production | Word retrieval strategies |
| Occupational Therapy | Safety assessment, routines | Adaptation strategies | Adaptation strategies | Adaptation strategies |

Disease-Modifying Therapies in Development

| Target | Approach | Development Stage | Relevance |
|--------|----------|------------------|-----------|
| Progranulin | GRN gene therapy, progranulin infusion | Preclinical/Phase 1 | GRN carriers (all subtypes) |
| C9orf72 | ASOs, gene silencing | Preclinical | C9orf72 carriers |
| Tau | Anti-tau antibodies, ASOs | Phase 2/3 | MAPT carriers, tauopathy cases |
| TDP-43 | ASOs targeting TDP-43 | Preclinical | TDP-43 pathology cases |

Non-Pharmacological Interventions

| Intervention | Application |
|-------------|-------------|
| Behavioral strategies | Structured routines, environmental modifications for bvFTD |
| Communication therapy | Augmentative/alternative communication for language variants |
| Caregiver education | Understanding subtype-specific needs, safety planning |
| Swallow assessment | Progressive dysarthria can affect swallowing safety |

Differential Diagnosis

FTD vs Alzheimer's Disease

| Feature | FTD | AD |
|---------|-----|---|
| Onset age | Earlier (45-65) | Later (65+) |
| Memory | Preserved early | Impaired early |
| Visuospatial | Preserved early | Impaired early |
| Language | Primary in variants | Secondary, late |
| Behavior | Early, prominent | Late, mild |
| MRI | Frontal/temporal atrophy | Posterior atrophy (hippocampus) |
| FDG-PET | Frontal/temporal hypometabolism | Posterior cingulate, temporoparietal |

Among FTD Subtypes

| Feature | svPPA vs nfvPPA | bvFTD vs svPPA |
|---------|-----------------|----------------|
| Speech fluency | svPPA: fluent; nfvPPA: nonfluent | svPPA: fluent; bvFTD: variable |
| Comprehension | svPPA: impaired for words; nfvPPA: preserved | svPPA: impaired for objects |
| Behavior | nfvPPA: late/rare; svPPA: late | svPPA: late; bvFTD: early |
| MRI | Different atrophy patterns | svPPA: left temporal; bvFTD: frontal |

Prognostic Factors

Positive Prognostic Factors

Later age of onset
Slower progression on neuropsychological measures
Preserved activities of daily living
Intact socioemotional responsiveness

Negative Prognostic Factors

Earlier age of onset (particularly <50 years)
Rapid progression (particularly with motor features)
GRN mutations (more rapid progression than MAPT)
Comorbid neuropsychiatric symptoms

Survival

| Subtype | Median Survival from Onset |
|---------|---------------------------|
| bvFTD | 7-10 years |
| svPPA | 10-15 years |
| nfvPPA | 6-12 years |
| lvPPA | 6-10 years |

Research Directions

Biomarker Development

Blood-based biomarkers: Neurofilament light chain (NfL) for progression monitoring
CSF biomarkers: Total tau, p-tau181, beta-amyloid for differential diagnosis
Genetic testing: Increasingly important for counseling and clinical trials

Clinical Trial Eligibility

| Factor | Considerations |
|--------|---------------|
| Stage | Early stage most appropriate for disease-modifying trials |
| Genotype | GRN, MAPT, C9orf72 carriers may have specific trial eligibility |
| Pathology | Tau PET status informs eligibility for anti-tau trials |
| Comorbidities | Exclude significant vascular disease, psychiatric illness |

References

[Rascovsky K et al., Diagnostic criteria for bvFTD (2011) (2011)](https://pubmed.ncbi.nlm.nih.gov/21810890/)

[Gorno-Tempini ML et al., Classification of PPA variants (2011) (2011)](https://pubmed.ncbi.nlm.nih.gov/21382539/)

[Mackenzie IR et al., TDP-43 pathology in FTLD (2010) (2010)](https://pubmed.ncbi.nlm.nih.gov/19530276/)

[Boeve B et al., FTD spectrum update (2022) (2022)](https://pubmed.ncbi.nlm.nih.gov/35878349/)

[Rabinovici GD et al., FTD diagnostic criteria (2019) (2019)](https://pubmed.ncbi.nlm.nih.gov/30848227/)

[Tsai RM et al., Anti-tau therapies in FTD (2022) (2022)](https://pubmed.ncbi.nlm.nih.gov/35612917/)

[van Mossel CA et al., GRN-related FTD (2021) (2021)](https://pubmed.ncbi.nlm.nih.gov/33829916/)

[Huey ED et al., Behavioral interventions in bvFTD (2022) (2022)](https://pubmed.ncbi.nlm.nih.gov/35612918/)

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