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DEMENTIA & DELIRIUM

DEMENTIA & DELIRIUM. UNC PSYCHIATRY - 2008. DEMOGRAPHICS OF AGING. >85 is fastest growing demographic group 20% of population by 2030 will be over 65 There will be more women than men Life expectancy : (F > M) 1900 47.3 yrs 1985 74.4 yrs 2001 77.0 yrs

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DEMENTIA & DELIRIUM

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  1. DEMENTIA & DELIRIUM UNC PSYCHIATRY - 2008

  2. DEMOGRAPHICS OF AGING • >85 is fastest growing demographic group • 20% of population by 2030 will be over 65 • There will be more women than men • Life expectancy: (F > M) • 1900 47.3 yrs • 1985 74.4 yrs • 2001 77.0 yrs • Psychiatric Disorders LESS prevalent except cognitive impairment

  3. Prevalence of Memory Impairment

  4. Dementia: An acquiredsyndrome characterized by: • Short-term memory impairment AND • At least one of the following: • Aphasia - language impairments • Apraxia - motor memory impairments • Agnosia - sensory memory impairments • Abstract thinking / Exec. function impairments • Impairment in social and/or occupational fn • Not explainable by another disorder

  5. Epidemiology: Prevalence of dementia increases with age *Lower numbers represent moderate to severe dementia

  6. Life Expectancy

  7. Incidence Of Alzheimer’s Disease by Age

  8. Prevalence of AD vs All-cause Dementia By Age

  9. Etiology & Pathogenesis • Dementia results from impaired functioning of multiple brain systems in both cortical and sub-cortical areas that are associated with short-term memory (i.e. learning) and other higher cognitive functions. Generally this is due to structural brain damage that is often progressive and relatively irreversible

  10. Classification of Dementias • Primary versus secondarybased on the pathophysiology leading to damaged brain tissue • Cortical versus sub-corticaldepending on the cerebral location of the primary deficits • Reversible versus irreversibledepending on optimal treatment expectations • Early (before age 65) versus late onset

  11. Most Common Dementias • Alzheimer’s Disease and Lewy Body Dementias (50-75%) • Vascular Dementias (15-20%) • Alcohol-related dementias (including Korsakoff’s (infrequent) and etoh-induced)) • In those under age 65, FTDs may comprise 50% of all dementias • HIV dementia - most common dementia in those under age 55

  12. ALZHEIMER’S Pathophysiology • Neuritic plaques -extracellular - abnormal insoluble amyloid (beta) protein fragments • Neurofibrillary tangles - intracellular - disturbed tau-microtubule complexes (hyperphosphorylated tau) • Cholinergic system degeneration with significant loss of neurons in certain areas (such as Nucleus Basalis of Meynert) • Degeneration often begins in enterorhinal cortex and progresses to other limbic structures

  13. Lewy Body Pathology • Concentric spheres found within vacuoles (eosinophilic cytoplasmic inclusions) • Seen in cortex, midbrain and brainstem neurons in patients with idiopathic parkinsonism, Alzheimer's disease and especially Lewy Body dementias • The main structural component is alpha-synuclein. Ubiquitin is sometimes seen also.

  14. Risk Factors for AD • Age • Family history • Down’s syndrome (trisomy 21) • Head Trauma (esp. late in life) • Female gender (mixed results: age bias and possible higher ‘clinical’ expression in women) • Ethnicity (Caucasians have the lowest risk) • Late-onset depression (after age 65) • Mild Cognitive Impairment (MCI)

  15. Additional Risk Factors for Dementia • Cerebrovascular disease (and the risk factors for CV disease – including smoking, diabetes, hyperlipidemia, hypertension) is associated with vascular dementia risk • Recurrent MDD may be associated with risk of dementia in general.(Kessing and Anderson found risk of dementia to be 6 times higher in patients with 5 or more prior episodes.)1 • Subclinical Hyperthyroidism (especially when antithyroid antibodies are present.2 1Kessing LF, Anderson PK. J Neurol Neurosurg Psychiatry. 2004;75:1662-1666 2Kalmijn S, Mehta KM, Pols HA, et al. Clin Endocrinology (Oxf) 2000;53:733-737

  16. Genetic risk factors • Chromosome 19 - autosomal recessive - Apolipoprotein E-4 allele - associated with late-onset disease (not relevant for non-caucasians) • Chromosome 1, 14, 21 - autosomal dominant mutations - associated with early-onset/familial cases. Amyloid processing genes. • Chromosome 9 – ‘ubiquilin 1’ polymorphisms – needs replication

  17. Protective Factors in AD • Education • Anti-inflammatory agents (those that decrease amyloid production) • Estrogen replacement therapy (+/-) • Smoking (+)[?nicotine/past use](-) [CVD/current use] • APO E-3, CETP VV • Vitamin E & other antioxidants? • Homocysteine reduction • Statin use?

  18. Vascular dementia • Includes Binswanger’s disease, MID, anoxic damage, post-CABG, inflammatory diseases • RISK FACTORS: age, hypertension, diabetes and hyperlipidemia • 2nd most common dementia but incidence drops after the age of 75 (unlike Alzheimer’s disease) • In one study, 87% of ‘vascular dementias’ at autopsy had AD pathology1 1Nolan KA, Lino MM, et al. J Am Geriatr Soc, 1998;46:597-604

  19. Other less common dementias • Primary degenerative dementias • Diffuse Lewy Body dementias (7-26% of dementias) • Frontotemporal dementias (Pick’s, ALS, Huntington’s) • Neurological disordersassociated with dementia • PSP, Parkinson’s dementia, NPH, neoplasms, head trauma, subdurals, demyelinating diseases

  20. Less common dementias (cont.) • Infectious causes • neurosyphilis, Lyme disease • post-encephalitic dementias (esp. herpes) • viral, parasitic, bacterial and fungal meningitidies • opportunistic infections or brain abscess • Human prion disease (transmissible spongiform encephalopathies) - sCJD, ‘Mad-cow disease’(vCJD), Kuru, fatal familial insomnia

  21. General medical causes of dementia • Thyroid and adrenal diseases • Vitamin deficiency states (thiamin, niacin, B12) • Metabolic derangements (hepatic encephalopathy, dialysis dementia, etc.) • Medications(sedatives, antihypertensives, narcotics, anticholinergics) • Whipple’s Disease, sarcoidosis, Wilson’s disease • Toxins (heavy metals, organic poisons)

  22. Rapidly Progressive Dementias • Hashimoto’s Encephalitis (treatable with steroids) • Cerebellar degeneration syndromes • Transmissible spongifrom encepalopathies (prion diseases) • Paraneoplastic syndromes • Postviral encephalitis • Rare cases of AD, DLB, FTD

  23. Clinical Presentation • Always associated with cognitive disturbances and functional impairments • Visuospatial impairments and behavioral disturbances are usually seen as well • Specific symptoms will vary by type of dementia

  24. Memory Impairments • Difficulty learning or retaining new information (repeated conversations) • Information retrieval deficits (can’t recall names, list generation deficits) • Personal episodic memory impairment (misplacing items) • Declarative (semantic) memory (WHAT) > procedural (implicit) memory (HOW)

  25. Language Deficits • List-generation deficits (esp. in AD) • Word-finding difficulties (naming problems) • Verbal fluency deficits • Less complex sentence structure • Relatively preserved auditory comprehension (can understand directions)

  26. Visuospatial impairments • Visual recognition impairments (trouble recognizing familiar faces - CAPGRAS syndrome possible) • Spatial deficits (getting lost in familiar surroundings, 3-D drawing deficits)

  27. Executive Function Impairments • Planning, predicting, correlating, abstracting –> Frontal lobe F’n • Taking multiple threads of information and processing it to make a decision (Trails B testing) • Often the first impairment noticed in highly educated/intelligent people • Pronounced deficits often seen in FTDs before overt memory impairment

  28. Functional Impairments • Deficits appear first in IADLs (managing finances, driving, shopping, working, taking medications, keeping appointments) • Eventually problems with ADLs (feeding, grooming, dressing, eating, toileting) • Rate and specific pattern of loss will vary by individual and somewhat by diagnosis • NB: Functional impairment and performance on cognitive testing may not correlate strongly early in the course of dementia

  29. Behavioral Symptoms • Nearly universal and often the main focus of treatment. Inability to manage these symptoms is highly correlated with institutional placement. • PERSONALITY CHANGE: Occurs early • passivity (apathy, social withdrawal) • disinhibition (inappropriate sexual behavior or language) • self-centered behaviors (childishness, loss of generosity)

  30. Agitation • Very common and frequently worsens as the illness progresses • verbal aggression (25%) • physical aggression (30%) • non-aggressive behaviors such as wandering and pacing (25-50%)

  31. Other Associated Features • Depression (40-50%) - esp. in AD & VD • Psychosis • Delusions (30-60%) • Paranoid type (theft, infidelity) • Misidentification type (Capgras, etc.) • Perceptual disturbances (20-40%) - often visual, common in LBD • Sleep Disturbances (>50%) - insomnia, sleep-wake cycle problems. This plus wandering and aggression are highly correlated with care-giver burnout

  32. Course & Staging of Dementia • Most have insidious onset with progressive decline over many years • Some are fulminate (JCD e.g.) • Some may remit spontaneously or with treatment (e.g. Thyroid disease, B12 def.) • AD - Predictable progression which is the reverse of development. Typically live 4 -10 years after diagnosis and often have symptoms 3-4 years before diagnosis. Women usually outlive men.* • VD - May show step-wise progression. Shorter course than AD. Often see focal findings *Ann Intern Med (2004) Average survival after diagnosis of AD: 5.7 years for women, 4.2 years for men

  33. DIFFERENTIAL DIAGNOSIS • Amnestic syndrome - STM impairments alone • Receptive Aphasia - Impaired cognitive functioning due to failure to understand speech • Mental Retardation - Impaired intellectual abilities but not necessarily memory • Pseudodementia (Dementia Syndrome of Depression). 50% of elderly patients with Depressive Pseudodementia go on to develop irreversible dementia within 3-5 years!

  34. DIFF DX (continued) • Are-related cognitive decline: AKA Age-associated Memory Impairment (AAMI), Benign Senescent Forgetfulness or Mild Cognitive Impairment (MCI). Symptoms not currently associated with functional impairment. However, ~25%-35% progress to dementia within 18 months. • Delirium - Impairments of consciousness and attention. Commonly seen in dementia

  35. DELIRIUM • Acute brain dysfunction characterized by: • Global symptoms (affecting both cerebral hemispheres) including impairment of consciousness and attention • Primary physiological changes with potential for reversibility • ‘waxing and waning’ symptoms – usually worse in evening • Life-threatening conditions underlying the syndrome

  36. Symptoms of Delirium • Common symptoms of a delirium include: • Waxing and waning levels of consciousness • Poor attention and disorientation • Disturbed memory (long and short term) • Psychosis • Sleep dysregulation • Fearfulness with agitation and aggression • Seriously impaired insight and judgment

  37. Epidemiology of Delirium • Very Common - 10-15% med/surg inpatients (30%+ if elderly) • 30% of Adult Burn Patients • 80%of delirious patients have pre-existing dementia • Predisposing Factors: old age, postcardiotomy, s/p burns prexisting brain damage drug withdrawal states AIDS

  38. Causes of Delirium • Often multifactorial • Infections, trauma, brain diseases • Cardiac diseases, lung disease, hypoxia, hypoglycemia • Toxins, or intoxications • Medication effects • Substance withdrawals (e.g. DTs) • Endocrinopathies • In elderly dementia patients: UTI, dehydration and pneumonia are the most common causes

  39. DELIRIUM - TREATMENT • Must look for medical cause(s) and treat • Symptoms can be helped by antipsychotic drugs such as haldoperidol or risperidone (especially psychosis, agitation) • Consider anticholinesterases for anticholinergic delirium • Comfort measures include reorientation strategies, reducing stimulation, frequent reassurance

  40. Delirium vs Dementia(summary) • General rules of thumb: DeliriumDementia acute chronic reversible irreversible physiological structural primary attention primary memory deficits deficits • Delirium and dementia can coexist; in fact delirium is very common in demented patients

  41. Diagnostic ApproachEarly Detection & Screening • Careful history from patient and reliable informant • PE with focus on neurological exam and cognitive testing • Cognitive testing tools such as MMSE are helpful. Score below 24-27 often concerning depending on premorbid abilities • Functional Assessment tools such as the Functional Activities Questionnaire

  42. Cognitive Testing • Serial 7’s (5 answers) - If you can do it, that’s good, but as many as 50% of normal elderly can’t(WORLD backwards is not much better as only 62% of elderly can do it with no errors) • Orientation:If you are disoriented that’s bad, however many early dementia patients are fully oriented (40%) • 3-item recall: Not being able to recall 2/3 is bad as only 19% of dementia patients can do this, but 74% or normal elderly can • MMSE: Sensitivity: 87%, Specificity: 82%

  43. MMSE ‘norms’ by Age and Educational Level Educational level

  44. Diagnostic Work-Up • This is done to • (1) rule out disorders besides dementia, • (2) to identify reversible/treatable dementias (13%) • (3) to clarify the specific dementia syndrome • Routine Assessment: CBC with diff, serum electrolytes, Ca++, glucose, BUN/CR, LFTs, TFTs, B12 & folate, U/A, RPR • When indicated: Sed. rate, HIV, CXR, heavy metals, neuroimaging, LP, EEG, functional imaging, Lyme titers, endocrine studies, rheumatologic studies

  45. Guidelines for use of specialized testing • LP: Suspicion of metastatic CA, CNS infections, neuropsyphilis, hydrocephalus, vasculitis. Also for dementia <55 and rapidly progressive dementias • Neuroimaging - consider in all new cases. However when no focal symptoms or signs, seizures or gait disturbances in an individual over age 60 - consider this optional • Functional Imaging (SPECT, PET, MRS): to clarify type of dementia when necessary • EEG - can help distinguish delirium from dementia, can help with seizure disorder and CJD (periodic slow wave complexes)

  46. Biological Markers • Hyperphosphorylated tau protein in AD • P-tau231 and p-tau181 discriminate AD from non-AD dementias • Elevated p-tau231 in MCI predicts decompensation • Phosphorylation of threonine 231 is an early event in AD, and precedes tangle formation • CSF 14-3-3 protein – elevated in CJD • Neural Thread Protein (NTP) in urine – 60% sensitivity, 91 % specificity. Not helpful yet in mild cases (MCI) because elevations are 50/50 • Pittsburg B Compound (PIB) binds to abnormal B-amyloid fragments and is PET indentifiable

  47. Neuropsychological Testing • Cognitive testing and functional testing are at odds or there is suspicion of early dementia in a high IQ individual with normal MMSE • Mild impairment in a person with: low IQ or limited education, trouble with English, impairments less than 6 months • Determining capacity for legal purposes when deficits are mild

  48. General Treatment Principles For Dementia • Treatment Of Underlying Disease Process (Primary Treatment) • Management Of Behaviors and Symptoms (Secondary Treatment) • Caregiver Support and Education

  49. Reversible Dementias • May become irreversible if not treated soon enough • Many dementias may be arrestible if not fully reversible • Rule out ‘depressive pseduodementia’ and delirium which can mimic dementia • Some reversible dementias include: hypoT4, B12 def., some infections and tumors, drug-induced syndromes, etc.

  50. Primary Treatment Strategies(for progressive dementias) • 1. Prevention • Identify risks and mitigate • Develop neuroprotective strategies for those at risk • 2. Slow or halt progression of illness • Understanding pathophysiology leads to treatment ideas • 5 year delay in onset ---> 1/3 decrease in prevalence • Delaying institutionalization by 1 month saves $1.2 billion/yr • 3. Reverse symptoms • Compensate through augmentation of remaining neurons or other systems • Reversal of destructive processes & regeneration of tissue

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