Diff: Frontotemporal dementia
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Frontotemporal dementia (FTD), also known as frontotemporal lobar degeneration, is a group of [[Neurodegenerative disorder|neurodegenerative disorders]] characterized by progressive changes in behaviour, personality, language, and executive functions. It is the second most common cause of dementia in individuals under the age of 65, after Alzheimer's disease. |
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'''Frontotemporal dementia''' ('''FTD''') is a group of disorders that damage the frontal and temporal lobes of the brain. These areas are important for personality, social judgement, language, planning and behaviour. |
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== Overview == |
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Frontotemporal dementia primarily affects the frontal and temporal lobes of the brain, leading to the degeneration and loss of neurons in these regions. The symptoms of FTD can vary widely depending on the specific subtype and areas of the brain affected. |
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FTD often begins earlier than more common forms of dementia. It may first appear as changes in behaviour, personality or language rather than memory loss. |
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== Types of Frontotemporal Dementia == |
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== Types == |
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The main clinical groups are behavioural variant frontotemporal dementia, primary progressive aphasia and FTD associated with movement disorders. |
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=== Behavioural Variant Frontotemporal Dementia (bvFTD) === |
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Behavioural variant frontotemporal dementia (bvFTD) is the most common subtype of FTD, accounting for approximately 50% to 60% of cases. It is characterized by changes in behaviour, personality, and social cognition. Common symptoms include: |
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Behavioural variant FTD can cause social disinhibition, apathy, loss of empathy, repetitive behaviour, poor judgement, changes in eating habits and difficulty planning. |
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* Social disinhibition and inappropriate behaviours |
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* Loss of empathy and sympathy |
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* Emotional blunting or apathy |
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* Impulsivity and lack of judgment |
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* Changes in eating habits and food preferences |
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* Language difficulties (less prominent compared to other subtypes) |
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Primary progressive aphasia mainly affects language. A person may lose word meaning, have difficulty naming objects, speak more slowly, make grammatical errors, or struggle to understand speech. |
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=== Semantic Variant Primary Progressive Aphasia (svPPA) === |
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Semantic variant primary progressive aphasia (svPPA) is characterized by progressive language impairment, specifically affecting word comprehension and semantic knowledge. Individuals with svPPA may have difficulty finding words, understanding the meaning of words and objects, and maintaining coherent conversations. Other features may include: |
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Movement-related forms can overlap with motor neuron disease, corticobasal syndrome or progressive supranuclear palsy. These may involve weakness, stiffness, falls, swallowing difficulty or abnormal eye movements. |
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* Naming difficulties |
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* Word-finding pauses and substitutions |
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* Impaired object recognition |
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* Reading and writing impairments |
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== Causes == |
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FTD is associated with abnormal protein build-up inside nerve cells, commonly involving tau or TDP-43. The protein changes damage neurons and lead to loss of brain tissue in the frontal and temporal lobes. |
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=== Nonfluent/Agrammatic Variant Primary Progressive Aphasia (nfvPPA) === |
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Nonfluent/agrammatic variant primary progressive aphasia (nfvPPA) is characterized by difficulties in speech production and grammar. Individuals with nfvPPA may exhibit the following symptoms: |
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There is often a genetic link. Some cases are caused by inherited changes in genes such as C9orf72, MAPT or GRN, but many cases occur without a known family history. |
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* Speech hesitations, effortful speech, and slow rate of speech |
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* Grammatical errors and difficulties forming sentences |
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* Apraxia of speech (difficulty coordinating the movements for speech) |
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* Preservation (repetitive behaviours or words) |
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== Symptoms == |
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Symptoms vary by subtype. Behavioural symptoms may include loss of inhibition, reduced empathy, compulsive routines, apathy, poor judgement and changes in food preference. Language symptoms may include word-finding problems, loss of word meaning, effortful speech or grammar problems. |
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=== Other Subtypes === |
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There are additional subtypes of FTD that are less common but still recognized: |
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Memory may be relatively preserved early on, which can make FTD look different from Alzheimer's disease. As the condition progresses, symptoms broaden and daily support needs usually increase. |
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* Frontotemporal dementia with motor neuron disease (FTD-MND): This subtype combines features of frontotemporal dementia and motor neuron disease, such as ALS (amyotrophic lateral sclerosis). |
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* [[Corticobasal syndrome|Corticobasal syndrome (CBS)]]: CBS is characterized by asymmetric motor symptoms, including limb rigidity, dystonia, and apraxia, as well as cognitive impairments. |
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* Progressive supranuclear palsy (PSP): PSP involves impairments in balance, eye movements, and coordination, along with cognitive changes. |
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== Diagnosis == |
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Diagnosis is based on the pattern of symptoms, neurological examination, cognitive and language testing, brain imaging and sometimes genetic testing. MRI or PET imaging may show changes in the frontal or temporal lobes. |
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== Genetics and Pathology == |
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Frontotemporal dementia can have both genetic and sporadic causes. Approximately 40% to 50% of cases have a family history of the disease, suggesting a genetic component. Mutations in several genes, including C9orf72, MAPT, and GRN, have been associated with familial forms of FTD. |
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FTD can be mistaken for depression, bipolar disorder, other mental health conditions or Alzheimer's disease, especially early in the illness. |
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The underlying pathology of FTD involves the accumulation of abnormal protein aggregates in the brain. In some cases, these aggregates are composed of tau protein (tauopathy), while in others, they consist of TDP-43 protein (TDP-43 pathology). |
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== Treatment and Care == |
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There is currently no cure for FTD. Care focuses on symptoms, communication, safety, daily structure and support for family or carers. |
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== Diagnosis and Treatment == |
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The diagnosis of frontotemporal dementia can be challenging due to its diverse clinical presentations and overlap with other neurodegenerative disorders. It often requires a comprehensive evaluation, including neurological examination, neuropsychological testing, brain imaging (MRI or PET scans), and genetic testing. |
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Speech and language therapy can help with communication strategies. Occupational therapy may help with routines and safety. Some medicines may be used for distressing symptoms, but treatment is individual and should be reviewed carefully. |
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Currently, there is no cure for FTD, and treatment focuses on managing symptoms and providing supportive care. This may involve a multidisciplinary approach, including medication, behavioural interventions, and therapy to address specific cognitive and behavioural symptoms. |
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Planning is important because FTD is progressive. Financial, legal and care arrangements often need to be discussed earlier than families expect. |
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== Notable Individuals Affected by Frontotemporal Dementia == |
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== Notable People == |
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Publicly reported cases have included author Terry Pratchett, who was diagnosed with posterior cortical atrophy, and actor Bruce Willis, whose family announced a diagnosis of frontotemporal dementia in 2023. Public reports about individual diagnoses should be handled cautiously and sourced clearly. |
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* Alberto Lattuada: Italian film director who was diagnosed with frontotemporal dementia in 2011. |
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* Peter Falk: American actor known for his role as Columbo, who battled FTD in the later years of his life. |
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* Terry Pratchett: British author famous for his Discworld series, who was diagnosed with posterior cortical atrophy, a subtype of FTD. |
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* Robin Williams: American actor and comedian who experienced behavioral and cognitive changes associated with FTD before his death. |
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== See Also == |
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* [[Neurodegenerative_disorder]] |
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* [[C9orf72]] |
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* [[Amyotrophic_Lateral_Sclerosis_(ALS)]] |
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== References == |
== References == |
* [https://www.nhs.uk/conditions/frontotemporal-dementia/ NHS: Frontotemporal dementia] |
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* [https://www.nhs.uk/conditions/frontotemporal-dementia/symptoms/ NHS: Frontotemporal dementia symptoms] |
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* [https://www.alzheimers.gov/alzheimers-dementias/frontotemporal-dementia Alzheimers.gov: What is frontotemporal dementia?] |
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* [https://www.alzheimers.org.uk/about-dementia/types-dementia/frontotemporal-dementia Alzheimer's Society: Frontotemporal dementia] |
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# Rademakers R, et al. (2012). Common variation in the C9orf72 gene is associated with frontotemporal dementia. Acta Neuropathol, 124(1), 77-87. |
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# Rohrer JD, et al. (2011). The heritability and genetics of frontotemporal lobar degeneration. Neurology, 77(10), 903-908. |
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# Piguet O, et al. (2011). Frontotemporal dementia. Handb Clin Neurol, 100, 521-535. |
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# Rascovsky K, et al. (2011). Sensitivity of revised diagnostic criteria for the behavioural variant of frontotemporal dementia. Brain, 134(Pt 9), 2456-2477. |
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[[Category:Medicine]] |
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[[Category:Neurology]] |
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[[Category:Dementia]] |