Alzheimer's Disease in Brazil: Symptoms, Causes & Treatment

Alzheimer's Disease in Brazil: Symptoms, Causes & Treatment | aihealz

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How you might notice it

01Progressive short-term memory loss — forgetting recent conversations, repeating questions within minutes, misplacing items, and missing appointments — is the earliest and most reliable symptom in 80-90% of typical cases.

02Word-finding difficulty with hesitations, circumlocutions ('the thing you write with'), and substitutions; reading and reading comprehension decline later than speech production.

03Executive dysfunction: trouble planning meals, managing finances, following multi-step instructions, and adapting to new situations. Often noticed first by family during travel or financial tasks.

04Visuospatial impairment producing getting lost in familiar places, difficulty judging distances when driving, and trouble using familiar tools — sometimes mistaken for vision loss.

05Disorientation to time and place, beginning with date confusion and progressing to inability to identify season, year, or the home address.

06Loss of insight into the deficit (anosognosia) — patients often deny memory problems even when objective testing is clearly abnormal. Family members are usually a more reliable source of history.

07Apraxia — difficulty performing learned motor sequences such as dressing, using cutlery, or operating familiar appliances despite preserved motor strength.

08Behavioral and psychological symptoms (BPSD): apathy in over 70% of patients, depression in 40-50%, anxiety, irritability, paranoid ideation, agitation, and night-time wandering as disease progresses.

09Aphasia and agnosia in moderate stages — failure to recognise faces of relatives, name common objects, or understand complex sentences.

10Incontinence, immobility, dysphagia, and mutism in severe stages, ultimately rendering the patient bedbound and dependent for all care.

early warning signs

•Repeated short-term memory lapses noticed by family members that the patient denies or minimises
•New difficulty handling personal finances, taxes, or online banking that the person previously managed without help
•Subtle word-finding pauses and reliance on filler phrases such as 'that thing' or 'whatchamacallit' in a previously articulate person
•Getting briefly lost driving familiar routes or missing a familiar exit
•Withdrawal from hobbies, social events, or conversations that require following multiple speakers

● emergency signs

•Sudden severe confusion or rapid worsening over hours to days — suggests delirium from infection, medication, metabolic derangement, or stroke, not Alzheimer's progression
•First-ever seizure in a patient with known or suspected dementia — warrants brain imaging and neurology review
•Sudden focal weakness, slurred speech, or facial droop — stroke until proven otherwise, regardless of background cognitive impairment
•Headache, vomiting, or new gait disturbance with cognitive decline — rule out subdural haematoma, hydrocephalus, or mass lesion with urgent CT or MRI
•Severe agitation with risk of harm to self or carer — emergency assessment for delirium, pain, infection, or medication adverse effect before antipsychotics are added

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How it’s diagnosed

diagnosis

Diagnosis follows a stepwise workflow combining clinical assessment, structured cognitive testing, screening laboratory studies, structural brain imaging, and increasingly, fluid and PET biomarkers. The decisive history is taken from both the patient and a knowledgeable informant — the informant usually provides the most accurate picture of functional change. Structured cognitive testing with the Mini-Mental State Examination (MMSE) or Montreal Cognitive Assessment (MoCA) quantifies global cognition; the MoCA is more sensitive for mild cognitive impairment. A standard work-up screens for treatable mimics with TSH, vitamin B12, comprehensive metabolic panel, depression assessment, and brain imaging (MRI preferred over CT) to rule out subdural haematoma, normal-pressure hydrocephalus, vascular disease, and structural lesions. MRI in Alzheimer's typically shows medial temporal lobe atrophy with relatively preserved frontal and motor regions. The 2024 NIA-AA Revised Criteria established Alzheimer's as a biological diagnosis defined by core biomarkers. Cerebrospinal fluid testing for the Aβ42/40 ratio plus phosphorylated tau (p-tau181 or p-tau217) is sensitive and specific; amyloid PET imaging with florbetapir, florbetaben, or flutemetamol can confirm cerebral amyloid in vivo. Tau PET is now used to stage disease. Plasma p-tau217 assays have emerged as a high-accuracy blood test (positive and negative predictive values exceeding 90% in specialist clinics) and are being introduced as a first-line biomarker. Differential diagnosis must exclude vascular dementia, dementia with Lewy bodies, frontotemporal dementia, depression-related pseudodementia, and normal-pressure hydrocephalus — each has distinct features and management implications.

Key tests

Structured cognitive testing (MoCA, MMSE) with informant historyQuantifies severity of cognitive impairment, establishes baseline for tracking, and identifies the cognitive domains affected. The MoCA is more sensitive than MMSE for mild cognitive impairment and early Alzheimer's.

Screening blood panel (CBC, CMP, TSH, vitamin B12, folate)Excludes reversible contributors to cognitive decline — hypothyroidism, B12 deficiency, hepatic or renal encephalopathy, anaemia. Recommended in every dementia work-up by AAN and NICE.

Brain MRI (or CT if MRI contraindicated)Identifies medial temporal lobe atrophy supporting Alzheimer's; rules out vascular dementia, normal-pressure hydrocephalus, subdural haematoma, tumours, and other structural causes.

Cerebrospinal fluid Aβ42/40 ratio and phosphorylated tau (p-tau181 or p-tau217)Core biomarker confirmation per the 2024 NIA-AA Revised Criteria. A low Aβ42/40 ratio plus elevated p-tau is highly specific for Alzheimer's pathology.

Plasma p-tau217Emerging blood-based biomarker with diagnostic accuracy comparable to CSF and PET in specialist settings; expected to become the first-line screening test before confirmatory CSF or PET.

Amyloid PET imaging (florbetapir, florbetaben, or flutemetamol)Visualises cerebral amyloid plaques in vivo. Required for confirming amyloid positivity before initiating anti-amyloid antibody therapy (lecanemab, donanemab).

Tau PET imagingVisualises tau tangle distribution and burden; useful for staging disease and assessing response to therapy. Predicts rate of clinical decline more accurately than amyloid PET.

APOE genotyping (with genetic counselling)Identifies APOE-ε4 homozygotes who carry markedly higher risk of amyloid-related imaging abnormalities (ARIA) on anti-amyloid therapy; informs treatment risk-benefit discussion.

Outlook

Median survival from clinical diagnosis of Alzheimer's dementia is 8-10 years, with substantial variation depending on age at diagnosis, sex, comorbidities, and disease stage. Patients diagnosed in their late 60s often live 10-15 years; those diagnosed after 80 typically 4-6 years. Progression follows a relatively predictable trajectory: 2-4 years from MCI to mild dementia, 4-7 years through moderate stage, and 1-3 years in severe dementia. Death is most often from pneumonia, urinary tract infection with sepsis, malnutrition, pressure injuries, or pulmonary embolism rather than the dementia itself. Anti-amyloid antibody therapy (lecanemab, donanemab) slows decline by 25-35% over 18-24 months in early disease; longer-term effects are still being characterised. Prognosis is improved by treating coexisting vascular risk factors, depression, sleep apnoea, hearing loss, and pain. Predictors of faster decline include APOE-ε4 homozygosity, higher tau burden on PET, early age at onset, prominent neuropsychiatric symptoms, and significant comorbid vascular disease.

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Causes & risk factors

known causes

Amyloid-beta plaque accumulation: Cleavage of amyloid precursor protein (APP) by beta- and gamma-secretases produces amyloid-beta peptides, particularly Aβ42, that misfold and aggregate into extracellular plaques. Plaques begin in the neocortex 15-25 years before symptoms and disrupt synaptic function, inflame surrounding microglia, and seed downstream tau pathology.
Hyperphosphorylated tau and neurofibrillary tangles: Tau, a microtubule-stabilising protein, becomes abnormally phosphorylated, detaches from microtubules, and aggregates into intracellular neurofibrillary tangles. Tangles begin in the entorhinal cortex and hippocampus and spread cortically along the Braak staging pattern. Tau burden correlates more closely with cognitive decline than amyloid burden.
Synaptic loss and neurodegeneration: Soluble Aβ oligomers and tau drive failure of glutamatergic and cholinergic synapses, the latter explaining the rationale for cholinesterase inhibitor therapy. Bulk neuronal loss follows, producing the medial temporal and parietal atrophy visible on MRI.
Neuroinflammation: Reactive microglia and astrocytes around plaques release pro-inflammatory cytokines that amplify neuronal injury. Genetic risk variants in TREM2, CR1, and CLU implicate innate immunity in disease initiation.
Cerebral amyloid angiopathy and vascular contribution: Amyloid-beta also deposits in cerebral vessel walls, causing microbleeds and lobar haemorrhage. Mixed Alzheimer's and vascular pathology accounts for the majority of dementia cases in older adults at autopsy.
Genetic mutations in APP, PSEN1, or PSEN2 (autosomal dominant early-onset disease): Pathogenic variants in any of these three genes cause overproduction of Aβ42 and produce highly penetrant early-onset Alzheimer's disease, typically with onset in the 30s-50s. Each child of an affected parent has 50% risk.
APOE-ε4 risk allele: The APOE-ε4 variant on chromosome 19 is the strongest common genetic risk factor for late-onset disease. ε4 reduces clearance of Aβ from the brain. One copy raises lifetime risk roughly 3-fold; two copies raise it 9-15 fold.

risk factors

Age over 65non-modifiable: The strongest risk factor by far. Prevalence is ~3% at age 65-74, ~17% at 75-84, and ~32% at 85+ (Alzheimer's Association 2024). Most cases occur in those over 75.
Family history and APOE-ε4 genotypegenetic: One APOE-ε4 allele raises lifetime risk ~3x; two copies raise risk 9-15x and lower mean onset age by 10-15 years. Autosomal dominant APP, PSEN1, PSEN2 mutations confer near-100% risk.
Female sexnon-modifiable: Women account for roughly two-thirds of US Alzheimer's cases. Part of the difference reflects greater life expectancy, but biological factors (oestrogen withdrawal, APOE-ε4 interaction) may also contribute.
Untreated hypertension in midlifemodifiable: Systolic blood pressure ≥140 mmHg in midlife increases late-life dementia risk by 60%. SPRINT-MIND showed intensive blood pressure control reduced MCI incidence by 19% (PMID 30688979).
Type 2 diabetes and insulin resistancemodifiable: Diabetes raises Alzheimer's risk roughly 1.5-2x. Brain insulin resistance impairs Aβ clearance and energy metabolism; midlife glycaemic control reduces late-life dementia risk.
Hearing lossmodifiable: Untreated hearing loss approximately doubles dementia risk. The 2024 Lancet Commission identifies hearing loss as the largest single modifiable contributor (~7% of population-attributable risk). Hearing aids reduce risk in at-risk populations (ACHIEVE trial 2023).

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Living with it

01Control blood pressure to under 130/80 mmHg in mid-life and early late-life — SPRINT-MIND showed a 19% reduction in MCI incidence with intensive control

02Treat hearing loss with appropriately fitted hearing aids — the ACHIEVE trial demonstrated 48% slowing of cognitive decline in at-risk older adults

03Maintain at least 150 minutes per week of moderate aerobic activity plus twice-weekly resistance training to reduce dementia risk by 30-40%

04Manage type 2 diabetes, LDL cholesterol, and avoid smoking — combined modifiable factors account for ~45% of population-attributable dementia risk (Lancet Commission 2024)

05Stay cognitively and socially engaged — continued learning, social activity, and a varied occupation build cognitive reserve that delays clinical onset

06Limit alcohol to under 14 units per week and treat depression promptly when it appears

recommended foods

•Mediterranean or MIND (Mediterranean-DASH Intervention for Neurodegenerative Delay) eating pattern — observational reduction in incident Alzheimer's of 35-53% in highest adherence groups
•Leafy green vegetables daily — spinach, kale, lettuce; one serving daily linked to slower cognitive decline
•Berries 2-3 times weekly — blueberries and strawberries; associated with delayed cognitive ageing
•Olive oil as the primary cooking fat; fatty fish (salmon, sardines, mackerel) at least twice weekly
•Nuts, whole grains, beans, and poultry over red meat
•Adequate hydration — older adults are prone to chronic dehydration that worsens confusion

foods to avoid

•Heavy intake of processed and red meat, fried foods, pastries, and sweets — linked to faster cognitive decline
•Sugar-sweetened beverages and ultra-processed foods high in added sugar and sodium
•Excessive alcohol — keep within 14 units/week or less; binge drinking accelerates cognitive loss
•Saturated and trans fats from butter, margarine, and processed foods in large amounts
•Crash diets and prolonged calorie restriction — increase frailty risk and may worsen cognition in late-stage disease
•Anticholinergic-heavy supplement regimens — many over-the-counter sleep, allergy, and bladder products carry anticholinergic burden that worsens cognition

Living with Alzheimer's Disease

Timeline

Alzheimer's is progressive and not reversible with current therapy, so 'recovery' applies to the timeline of disease control rather than cure. Cholinesterase inhibitors typically deliver their measurable benefit within 3-6 months of titration; about 25-50% of patients show a clear response. Anti-amyloid antibody therapy clears amyloid plaques within 12-18 months in most responders, often allowing donanemab to be stopped once PET is plaque-clear. ARIA, if it occurs, is usually within the first 6 months of therapy and typically resolves over 4-12 weeks after pausing or discontinuing treatment. Functional decline continues despite therapy — at a slowed rate — across all stages.

Lifestyle

01Establish a predictable daily routine — fixed wake, meal, activity, and sleep times reduce confusion and behavioural symptoms
02Simplify the home environment with clear signage, removed trip hazards, locked-out hot taps and stove controls, and a single accessible toilet
03Use a single calendar, whiteboard, or smartphone reminder system shared with carers to track appointments and medication
04Maintain regular physical exercise — walking, swimming, or chair-based exercise 5 days a week — adapted to ability
05Engage in social and cognitive activities the patient enjoys (music, reading aloud, light gardening, family meals) at intensities matched to current ability
06Prioritise sleep hygiene — consistent bedtime, daylight exposure, and treatment of sleep apnoea if present
07Plan financial, legal, and healthcare decisions early — lasting power of attorney, advance directives, and care preferences are easier to capture in mild stages

Daily management

01Set medications in a weekly pill organiser and link doses to fixed daily events (breakfast, lights-out) to support adherence
02Carry an ID card or wear a medical bracelet noting the diagnosis, emergency contact, and current medications
03Schedule regular check-ins with the primary care team for blood pressure, diabetes, vision, hearing, dental, and foot care
04Track behaviour, sleep, and any new symptoms in a simple diary — patterns help clinicians distinguish disease progression from delirium
05Plan respite for the primary carer at least monthly; carer burnout drives premature nursing home admission
06Review medication list at least annually for anticholinergic burden and unnecessary sedatives

Exercise

Aim for 150 minutes per week of moderate aerobic activity (walking, cycling, swimming) plus twice-weekly resistance training and balance work. In moderate dementia, supervised group programmes or chair-based routines are safer. Falls prevention becomes a priority as the disease advances — physiotherapy review for gait, footwear, and home hazards is recommended at least annually.

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Frequently asked

Is Alzheimer's disease the same as dementia?

No. Dementia is the broader syndrome of progressive cognitive decline severe enough to impair daily function. Alzheimer's disease is the most common cause of dementia, accounting for 60-70% of cases worldwide. Other causes include vascular dementia, dementia with Lewy bodies, and frontotemporal dementia. Distinguishing them matters because treatment, prognosis, and family counselling differ.

What is the first sign of Alzheimer's disease?

Progressive short-term memory loss is the earliest reliable sign in 80-90% of typical cases. Family members usually notice the change before the patient does, and the patient may deny or minimise the deficit. Word-finding difficulty and trouble managing finances often appear alongside memory change.

How is Alzheimer's disease diagnosed?

Diagnosis combines history from the patient and a relative, structured cognitive testing (MoCA or MMSE), basic blood work to rule out reversible causes, and brain MRI. Confirmation now uses biomarkers — CSF Aβ42/40 ratio with phosphorylated tau, plasma p-tau217 blood tests, or amyloid PET imaging.

Can a blood test diagnose Alzheimer's?

Yes, in specialist settings. Plasma p-tau217 is a newer blood biomarker with diagnostic accuracy comparable to cerebrospinal fluid testing and amyloid PET in research and memory-clinic cohorts. Positive results are typically confirmed with CSF or PET before starting disease-modifying therapy.

What causes Alzheimer's disease?

Two pathologies are central: extracellular plaques of beta-amyloid peptide and intracellular tangles of hyperphosphorylated tau, which together produce synaptic loss, neuroinflammation, and neuronal death over 15-25 years. Genetic factors (APOE-ε4 most importantly) interact with vascular and lifestyle risk factors to determine when symptoms appear.

Is Alzheimer's disease hereditary?

Most Alzheimer's is not directly inherited but has a strong heritable component. The APOE-ε4 allele raises risk roughly 3x with one copy and 9-15x with two copies. Rare autosomal-dominant mutations in APP, PSEN1, or PSEN2 cause early-onset disease with near-100% penetrance; each child of an affected parent has 50% risk.

Can Alzheimer's disease be prevented?

It cannot be guaranteed prevented, but roughly 45% of dementia cases worldwide are linked to 14 modifiable risk factors per the Lancet Commission 2024. Treating hypertension, hearing loss, depression, diabetes, and high LDL; staying physically and socially active; avoiding smoking; and limiting alcohol all measurably lower risk. Prevention is most effective when started in midlife.

What is lecanemab and how effective is it?

Lecanemab (Leqembi) is a monoclonal antibody that clears beta-amyloid from the brain. It received traditional FDA approval in July 2023. In the CLARITY-AD trial it slowed cognitive and functional decline by 27% over 18 months in early Alzheimer's. It is given by IV infusion every 2 weeks and requires MRI surveillance for ARIA.

What is donanemab and how is it different from lecanemab?

Donanemab (Kisunla) is a monoclonal antibody targeting an N-terminal pyroglutamate epitope of amyloid plaques. It received FDA traditional approval in July 2024. TRAILBLAZER-ALZ 2 showed a 35% slowing of decline over 76 weeks. Donanemab is dosed every 4 weeks and can be stopped once amyloid PET shows plaque clearance.

What is ARIA and why does it matter?

ARIA (amyloid-related imaging abnormalities) refers to MRI changes seen with anti-amyloid antibodies: ARIA-E (oedema) and ARIA-H (microhaemorrhages). Most cases are asymptomatic and detected only on surveillance MRI; a minority cause headache, confusion, or seizure. APOE-ε4 homozygotes have 2-3x higher rates.

Do cholinesterase inhibitors really work?

Yes, modestly. Donepezil, rivastigmine, and galantamine produce small but consistent improvements in cognition, function, and behaviour averaging 2-3 points on the ADAS-Cog at 6 months, and delay nursing home placement by 4-6 months in meta-analyses. About 25-50% of patients show a clinically meaningful response.

How long do people live after an Alzheimer's diagnosis?

Median survival from clinical diagnosis is 8-10 years, with wide variation. Patients diagnosed in their late 60s often live 10-15 years; those diagnosed after 80 typically 4-6 years. Death is most often from pneumonia, infection, or complications of immobility rather than the dementia itself.

What are the stages of Alzheimer's disease?

Five stages are commonly recognised: preclinical (biomarker-positive, no symptoms), mild cognitive impairment due to Alzheimer's (objective decline, function preserved), mild dementia (trouble with complex tasks), moderate dementia (help with basic care), and severe dementia (total dependence). Average progression from MCI to severe dementia is 8-12 years.

What is APOE-ε4 and should I get tested?

APOE-ε4 is a variant on chromosome 19 that raises lifetime Alzheimer's risk roughly 3x with one copy and 9-15x with two copies. Testing is recommended before starting anti-amyloid antibody therapy because homozygotes have higher ARIA risk. Predictive testing in asymptomatic adults should be done with genetic counselling.

Can young people get Alzheimer's disease?

Yes. Early-onset Alzheimer's (under age 65) accounts for 5-10% of all cases. Most early-onset disease is sporadic, but a small minority is caused by autosomal-dominant mutations in APP, PSEN1, or PSEN2, often presenting in the 40s or 50s. Atypical presentations such as posterior cortical atrophy are over-represented.

What is the difference between Alzheimer's and Lewy body dementia?

Lewy body dementia features early visual hallucinations, fluctuating cognition, REM sleep behaviour disorder, and parkinsonism appearing within a year of cognitive change. Severe sensitivity to typical antipsychotics is a hallmark. Alzheimer's begins with amnestic decline, lacks early hallucinations and parkinsonism, and shows medial temporal atrophy on MRI.

Can lifestyle changes slow Alzheimer's once diagnosed?

Yes, modestly. Multidomain lifestyle programmes combining Mediterranean-style diet, regular exercise, cognitive engagement, social activity, and tight vascular risk control slow cognitive decline in at-risk older adults. Treating hearing loss, depression, sleep apnoea, and pain measurably improves cognition.

How much does anti-amyloid antibody therapy cost?

Lecanemab costs approximately USD 26,500 per year for the drug alone in the United States; donanemab pricing is similar. Total annual cost including infusions, baseline and surveillance MRI scans, biomarker confirmation, and clinic visits typically runs USD 40,000-60,000. Medicare in the US covers therapy for biomarker-confirmed patients in approved registries.

Are antipsychotics safe in Alzheimer's-related agitation?

Typical and atypical antipsychotics carry a class warning for increased mortality in older adults with dementia and should be avoided where possible. Brexpiprazole received FDA approval in 2023 specifically for Alzheimer's-related agitation when non-pharmacological measures fail. Citalopram and other SSRIs have modest evidence for agitation.

Why was aducanumab withdrawn?

Aducanumab (Aduhelm) received controversial accelerated FDA approval in 2021 based on amyloid clearance rather than clinical benefit, with split trial data. Coverage restrictions, weak clinical evidence, and the arrival of lecanemab and donanemab — both with positive phase 3 trials — led the manufacturer Biogen to discontinue aducanumab in early 2024.

When should a person with Alzheimer's stop driving?

Most patients with mild dementia can drive safely for a limited period, but skills decline within 1-3 years. Stop driving when there are getting-lost episodes, near-misses, decline on a formal driving assessment, or family concern about safety. Many jurisdictions require notification of a dementia diagnosis to the licensing authority.

What support is available for caregivers?

National associations such as the Alzheimer's Association (US), Alzheimer's Society (UK), and Alzheimer's Disease International provide 24/7 helplines, online communities, local support groups, and care-navigation services. Practical respite, day-centre attendance, home aides, and structured caregiver education reduce burnout and delay nursing home admission.

Alzheimer's Disease.Care & specialists in Brazil

What it is

How you might notice it

How it’s diagnosed

Treatment & cost

Causes & risk factors

Living with it

When to seek help

Related conditions

Easily confused with

Often appears alongside

Types and stages

Living with Alzheimer's Disease

Complementary approaches

Patient support resources

Frequently asked

Sources & references

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