Dementia with Lewy bodies

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Dementia with Lewy bodies
Classification and external resources
Lewy Koerperchen.JPG
Lewy bodies are the pathomorphological characteristic of the disease
ICD-10 G31.8
ICD-9 331.82
OMIM 127750
DiseasesDB 3800
eMedicine neuro/91
MeSH D020961

Dementia with Lewy bodies (DLB), also known under a variety of other names including Lewy body dementia, diffuse Lewy body disease, cortical Lewy body disease, and senile dementia of Lewy type, is a type of dementia closely associated with Parkinson's disease. It is characterized anatomically by the presence of Lewy bodies, clumps of alpha-synuclein and ubiquitin protein in neurons, detectable in post mortem brain histology.[1] Lewy body dementia affects 1.3 million individuals in the United States alone.

Classification[edit]

Lewy body dementia (LBD) is a progressive degenerative dementia of the elderly. Its primary feature is cognitive decline, particularly of executive functioning. The patient will display an inability to plan, or a loss of analytical or abstract thinking. Persons with LBD will show markedly fluctuating cognition. Wakefulness will vary from day to day, and alertness and short term memory will rise and fall. Persistent or recurring visual hallucinations with vivid and detailed pictures are often an early diagnostic symptom. REM sleep behavior disorder (RBD) is a symptom often first recognized by the patient's caretaker. RBD includes vivid dreaming, with persistent dreams, purposeful or violent movements, and falling out of bed.[2] LBD symptoms overlap clinically with Alzheimer's disease and Parkinson's disease, but are more associated with the latter.[1] Because of this overlap, Lewy Body Dementia is often misdiagnosed in its early years

In LBD, loss of cholinergic (acetylcholine-producing) neurons is thought to account for degeneration of cognitive function (similar to Alzheimer's), while the death of dopaminergic (dopamine-producing) neurons appears to be responsible for degeneration of motor control (similar to Parkinson's) – in some ways, therefore, it resembles both diseases. The overlap of neuropathologies and presenting symptoms (cognitive, emotional, and motor) can make an accurate differential diagnosis difficult. In fact, it is often confused in its early stages with Alzheimer's disease and/or vascular dementia (multi-infarct dementia), although, where Alzheimer’s disease usually begins quite gradually, DLB often has a rapid or acute onset, with especially rapid decline in the first few months. DLB tends to progress more quickly than Alzheimer’s disease.[3] Despite the difficulty, a prompt diagnosis of DLB is important because of the risks of sensitivity to certain neuroleptic drugs and because appropriate treatment of symptoms can improve life for both the person with DLB and their caregivers.[3]

Benzodiazepines, anticholinergics, surgical anesthetics, some antidepressants, and OTC cold remedies can cause acute confusion, delusions and hallucinations.

DLB is distinguished from the dementia that sometimes occurs in Parkinson's disease by the time frame in which dementia symptoms appear relative to Parkinson symptoms.[4] Parkinson's disease with dementia (PDD) would be the diagnosis when dementia onset is more than a year after the onset of Parkinson's. DLB is diagnosed when cognitive symptoms begin at the same time or within a year of Parkinson symptoms.

Signs and symptoms[edit]

While the specific symptoms in a person with DLB will vary, core features of DLB are: fluctuating cognition with great variations in attention and alertness from day to day and hour to hour, recurrent visual hallucinations (observed in 75% of people with DLB), and motor features of Parkinson's. Suggestive symptoms are rapid eye movement(REM)-sleep behavior disorder and abnormalities detected in PET or SPECT scans.[5]

Parkinson's features could include shuffling gait, reduced arm-swing during walking, blank expression (reduced range of facial expression), stiffness of movements, ratchet-like cogwheeling movements; low speech volume, sialorrhea and difficulty swallowing. Tremors are less common in DLB than in Parkinson's disease.[6] DLB patients also often experience problems with orthostatic hypotension, including repeated falls, syncope (fainting), and transient loss of consciousness.

One of the most critical and distinctive clinical features is hypersensitivity to neuroleptic and antiemetic medications that affect dopaminergic and cholinergic systems.[7] In the worst cases, a patient treated with these drugs could become catatonic, lose cognitive function and/or develop life-threatening muscle rigidity. Some commonly used drugs which should be used with great caution, if at all, for people with DLB are chlorpromazine, haloperidol, or thioridazine.[3]

Visual hallucinations in people with DLB most commonly involve perception of people or animals that are not there. Delusions may include reduplicative paramnesia and other elaborate misperceptions or misinterpretations.[8] These hallucinations are not necessarily disturbing and in some cases, the person with DLB may have insight into the hallucinations and even be amused by them or conscious they are not really there. People with DLB may also have problems with vision, including double vision[3] and misinterpretation of what they see, for example, mistaking a pile of socks for snakes or a clothes closet for the bathroom.[8]

Causes[edit]

The causes are not yet well understood, but a genetic link with the PARK11 gene has been described.[9] As with Alzheimer's and Parkinson's diseases, most cases of DLB appear sporadically and DLB is not thought to be a strongly hereditary disease.[7] As with Alzheimer's, DLB risk is heightened with inheritance of the ε4 allele of the apolipoprotein E (APOE).[10]

Pathophysiology[edit]

Photomicrographs of regions of substantia nigra in a patient showing Lewy bodies and Lewy neurites in various magnifications

Pathologically, DLB is characterized by the development of abnormal proteinaceous (alpha-synuclein) cytoplasmic inclusions, called Lewy bodies, throughout the brain. These inclusions have similar structural features to "classical" Lewy bodies seen subcortically in Parkinson's disease. Additionally, a loss of dopamine-producing neurons (in the substantia nigra) occurs, similar to that seen in Parkinson's disease, and a loss of acetylcholine-producing neurons (in the basal nucleus of Meynert and elsewhere) similar to that seen in Alzheimer's disease. Cerebral atrophy (or shrinkage) also occurs as the cerebral cortex degenerates. Autopsy series have revealed the pathology of DLB is often concomitant with the pathology of Alzheimer's disease. That is, when Lewy body inclusions are found in the cortex, they often co-occur with Alzheimer's disease pathology found primarily in the hippocampus, including senile plaques (deposited beta-amyloid protein), and granulovacuolar degeneration (grainy deposits within and a clear zone around hippocampal neurons). Neurofibrillary tangles (abnormally phosphorylated tau protein) are less common in DLB, although they are known to occur, and astrocyte abnormalities are also known to occur.[11][12][13][14] It is presently not clear whether DLB is an Alzheimer's variant or a separate disease entity.[1][15][16][17] Unlike Alzheimer's disease, the brain may appear grossly normal with no visible signs of atrophy.[18]

Management[edit]

Although a cure for DLB is not available, treatments offer relatively small symptomatic benefit, but remain palliative in nature. Current treatments can be divided into pharmaceutical and caregiving.

Pharmaceutical[edit]

Pharmaceutical management, as with Parkinson's disease, involves striking a balance between treating the motor and emotive/cognitive symptoms. Motor symptoms appear to respond somewhat to the drugs used to treat Parkinson's disease (e.g. levodopa.) while cognitive issues may improve with drugs for Alzheimer's disease such as (Aricept). Drugs used in the treatment of Attention deficit/hyperactivity disorder (e.g. Ritalin) might improve cognition or daytime sleepiness, however drugs for both Parkinson's disease and ADHD increase levels of the chemical dopamine in the brain and so increase the risk of hallucinations with those classes of pharmaceuticals.[19][20]

Treatment of the movement and cognitive portions of the disease can worsen hallucinations and psychosis, while treatment of hallucinations and psychosis with anti-psychotics can worsen parkinsonian or ADHD symptoms in DLB such as tremor or rigidity & lack of concentration or impulse control.[21][22] Doctors may find the use of cholinesterase inhibitors represents the treatment of choice for cognitive problems and donepezil (Aricept), rivastigmine (Exelon) and galantamine (Reminyl) may be recommended as a means to help with these problems and to slow or prevent the decline of cognitive function.[3] Reports indicate Lewy body dementia may be more responsive to donepezil than Alzheimer's disease.[23] Memantine may also be useful.[24] Levocarb may help with movement problems, but in some cases, like dopamine agonists, may tend to aggravate psychosis in people with DLB. Clonazepam may help with rapid eye movement behavior disorder; table salt or antihypotensive medications may help with fainting and other problems associated with orthostatic hypotension. Botulinum toxin injections in the parotid glands may help with sialorrhea. Other medications, especially stimulants such as the ADHD drug methylphenidate (Ritalin) and modafinil, may improve daytime alertness but as with the anti-parkinsonian drug Levocarb, anti-hyperkinetics like Ritalin increase the risk of psychosis.[1][20] Experts advise extreme caution in the use of antipsychotic medication in people with DLB because of their sensitivity to these agents. When these medications must be used, atypical antipsychotics are preferred to typical antipsychotics; a very low dose should be tried initially and escalated only slowly, and patients should be carefully monitored for bad reactions to the drugs.

Due to hypersensitivity to neuroleptics, prevention of DLB patients taking these drugs is of great importance. People with DLB are at risk for neuroleptic malignant syndrome, a life-threatening illness, because of their sensitivity to these medications, especially the older typical antipsychotics, such as haloperidol. Other medications, including drugs for urinary incontinence and the antihistamine medication Benadryl can also exacerbate dementia.

Caregiving[edit]

Because DLB has no cure, it gradually renders people incapable of tending to their own needs. Caregiving is thus very important and must be carefully managed over the course of the disease. Caring for people with DLB involves adapting the home environment, schedule, activities, and communications to accommodate declining cognitive skills and parkinsonian symptoms.[8]

People with DLB may swing dramatically between good days—high alertness and few cognitive or movement problems—and bad days, and the level of care they need may thus vary widely and unpredictably. Sharp changes in behavior may be due to the day-to-day variability of DLB, but they may also be triggered by changes in the schedule or home environment, or by physical problems, such as constipation, dehydration, bladder infection, injuries from falls, and other problems the person with DLB may not be able to convey to caregivers. Potential physical problems should always be checked out when a person with DLB becomes agitated.

Especially when hallucinations and delusions are not dangerous or troubling to the person with DLB, it may be best for caregivers not to disabuse patients of them. Often the best approach may be benign neglect - acknowledging, but not encouraging or agreeing. Trying to talk the DLB patient out of his delusion may be frustrating to caregivers and discouraging to patients, sometimes provoking anger or dejection. When misperceptions, hallucinations, and the behaviors stemming from these become troublesome, caregivers should try to identify and eliminate environmental triggers, and perhaps offer cues or "therapeutic white lies" to steer patients out of trouble. Doctors may prescribe low doses of atypical antipsychotics, such as quetiapine, for psychosis and agitation in DLB. A small clinical trial found about half of DLB patients treated with low doses of quetiapine experienced significant reduction in these symptoms. Unfortunately, several participants in the study had to discontinue treatment because of side effects such as excessive daytime sleepiness or orthostatic hypotension.[4]

Changes in the schedule or environment, delusions, hallucinations, misperceptions, and sleep problems may also trigger behavior changes. It can help people with DLB to encourage exercise, simplify the visual environment, stick to a routine, and avoid asking too much (or too little) of them. Speaking slowly and sticking to essential information improves communication. The potential for visual misperception and hallucinations, in addition to the risk of abrupt and dramatic swings in cognition and motor impairment, should put families on alert to the dangers of driving with DLB.[10]

Epidemiology[edit]

Currently, an estimated 60 to 75% of diagnosed dementias are of the Alzheimer's and mixed (Alzheimer's and vascular dementia) type, 10 to 15% are Lewy body type, with the remaining types being of an entire spectrum of dementias, including frontotemporal lobar degeneration, alcoholic dementia, pure vascular dementia, etc. It is slightly more prevalent in men than women.[10]

History[edit]

Frederic Lewy (1885–1950) was first to discover the abnormal protein deposits ("Lewy body inclusions") in the early 1900s.[25] Dementia with Lewy bodies was first described by Japanese psychiatrist and neuropathologist Kenji Kosaka in 1976.[26] DLB only started to be diagnosed in the mid-1990s after the discovery of alpha-synuclein staining first highlighted Lewy bodies in the cortex of post mortem brains of a subset of dementia patients.[7] Because it was only recently discovered, DLB is not a recognized diagnosis in DSM-IV, which was published in 1994. It is, however, briefly mentioned in the DSM-IV-TR (published in 2000) under "Dementia Due to Other General Medical Conditions". In 1996, a consortium of scientists initially proposed and later revised diagnostic guidelines.

Attention was drawn to LBD following the 2008 death of actress Estelle Getty, who had previously been diagnosed with both Parkinson's and Alzheimer's diseases before her true condition was discovered. Fellow Golden Girls cast members noted, years earlier, Getty had severe trouble remembering her lines during the filming of the show. Another victim of DLB was William Stiles Bennet II, 1934-2009, a grandson and a son of US Congressmen who represented the area that includes Orange County, NY. Known as "Billo" to his friends, the younger Bennet was a successful businessman, and was one of the original developers of the Yoplait yogurt line.

Cultural reference[edit]

  • Writer and artist Mervyn Peake died from the disease in 1968.
  • Kelsey Grammer's lead character, mayor of Chicago Tom Kane in the television series Boss, suffers from early-stage Lewy body dementia.
  • In the Japanese anime series Ghost Hound, psychiatrist Atsushi Hirata emails an MRI scan image of a brain to colleague neurologist Reika Ōtori, who initially diagnoses the brain in the image as showing signs of Lewy body dementia. He shocks her by saying the brain in the image is his own brain, and recent apparitions and altered states of consciousness experienced by him may be related to the depicted condition of his brain.
  • Estelle Getty died from the disease in 2008.
  • Norman Winter, 80s, American publicist (Bob Dylan, Michael Jackson, Neil Diamond), died from it in 2013.[27]

See also[edit]

References[edit]

  1. ^ a b c d Van Gerpen, Jay A.; Assn, Lewy Body Dementia (2007), New Trends in Lewy Body Dementia, from "The Many Faces of Lewy Body Dementia" series at Coral Springs Medical Center, FL, YouTube 
  2. ^ Lewy Body Dementia Association (lbda.org)
  3. ^ a b c d e Scotland, Alzheimer; Dementia, Action on, Dementia with Lewy Bodies 
  4. ^ a b Weintraub, Daniel; Hurtig, Howard I. (2007), "Presentation and Management of Psychosis in Parkinson's Disease and Dementia with Lewy Bodies", American Journal of Psychiatry 164 (10): 1491–1498, doi:10.1176/appi.ajp.2007.07040715, PMC 2137166, PMID 17898337 
  5. ^ Association Inc., Lewy Body Dementia (2007), "What is Lewy Body Dementia", Slideshare 
  6. ^ Lennox, Graham; Lewy-net, Nottingham Medical School, Dementia with Lewy Bodies 
  7. ^ a b c Stewart, Jonathan T.; Assn, Lewy Body Dementia (2007), Difficulties in Diagnosing Lewy Body Dementia, from "The Many Faces of Lewy Body Dementia" series at Coral Springs Medical Center, FL, YouTube 
  8. ^ a b c Ferman, Tanis J.; Assn, Lewy Body Dementia (2007), Behavioral Challenges in Dementia with Lewy Bodies, from "The Many Faces of Lewy Body Dementia" series at Coral Springs Medical Center, FL, YouTube 
  9. ^ Bogaerts V, Engelborghs S, Kumar-Singh S, et al. (September 2007), "A novel locus for dementia with Lewy bodies: a clinically and genetically heterogeneous disorder", Brain 130 (Pt 9): 2277–91, doi:10.1093/brain/awm167, PMID 17681982. 
  10. ^ a b c Crystal, Howard A. (2008), "Dementia with Lewy Bodies", E-Medicine from WebMD 
  11. ^ Hishikawa N, Hashizume Y, Yoshida M, Niwa J, Tanaka F, Sobue G. (April 2005), "Tuft-shaped astrocytes in Lewy body disease", Acta Neuropathol 109 (4): 373–80, doi:10.1007/s00401-004-0967-3, PMID 15668789 
  12. ^ Iseki E, Togo T, Suzuki K, Katsuse O, Marui W, de Silva R, Lees A, Yamamoto T, Kosaka K. (March 2003), "Dementia with Lewy bodies from the perspective of tauopathy", Acta Neuropathol. 105 (3): 265–70, doi:10.1007/s00401-002-0644-3 (inactive 2014-03-22), PMID 12557014 
  13. ^ Marla Gearing, PhD; Michael Lynn, MS; Suzanne S. Mirra, MD (February 1999), "Neurofibrillary Pathology in Alzheimer Disease With Lewy Bodies", Archives of Neurology 56 (2) 
  14. ^ Hiroshige Fujishiro, MD, PhD,1 Tanis J. Ferman, PhD,2 Bradley F. Boeve, MD,3 Glenn E. Smith, PhD,4 Neill R. Graff-Radford, MBBCh, FRCP,5 Ryan J. Uitti, MD,5 Zbigniew K. Wszolek, MD,5 David S. Knopman, MD,3 Ronald C. Petersen, MD,3 Joseph E. Parisi, MD,6 and Dennis W. Dickson, MD1 (July 2008), "Validation of the neuropathologic criteria of the third consortium for dementia with Lewy bodies for prospectively diagnosed cases.", J Neuropathol Exp Neurol. 67 (7): 649–56, doi:10.1097/NEN.0b013e31817d7a1d, PMC 2745052, PMID 18596548 
  15. ^ Uchikado H, Lin WL, DeLucia MW, Dickson DW Uchikado, H; Lin, WL; Delucia, MW; Dickson, DW (2006), "Alzheimer disease with amygdala Lewy bodies: a distinct form of alpha-synucleinopathy", Journal of neuropathology and experimental neurology 65 (7): 685–97, doi:10.1097/01.jnen.0000225908.90052.07, PMID 16825955 
  16. ^ Kotzbauer PT, Trojanowsk JQ, Lee VM (2001), "Lewy body pathology in Alzheimer's disease", Journal of molecular neuroscience : MN 17 (2): 225–32, doi:10.1385/JMN:17:2:225, PMID 11816795 
  17. ^ http://www.oumedicine.com/body.cfm?id=844&action=detail&aeproductid=Adam2004_1&aearticleid=000739
  18. ^ http://jnnp.bmj.com/content/76/suppl_5/v8.full
  19. ^ http://www.ncbi.nlm.nih.gov/pubmed/8555378
  20. ^ a b Stimulant psychosis
  21. ^ http://www.nlm.nih.gov/medlineplus/ency/article/000759.htm
  22. ^ http://www.healthy.net/scr/News.aspx?Id=8976
  23. ^ Neef, Doug; Walling, Anne D (2006-04-01), "Dementia with Lewy Bodies: an Emerging Disease", American Family Physician 73 (7): 1223–1229, PMID 16623209, retrieved 2010-01-29. 
  24. ^ Aarsland, D; Ballard, C; Walker, Z; Bostrom, F; Alves, G; Kossakowski, K; Leroi, I; Pozo-Rodriguez, F et al. (2009), "Memantine in patients with Parkinson's disease dementia or dementia with Lewy bodies: a double-blind, placebo-controlled, multicentre trial", Lancet neurology 8 (7): 613–8, doi:10.1016/S1474-4422(09)70146-2, PMID 19520613 
  25. ^ Lewy body dementia at Who Named It?
  26. ^ Kosaka K, Oyanagi S, Matsushita M, and Hori A. (1976), "Presenile dementia with Alzheimer-, Pick- and Lewy-body changes", Acta Neuropathol 36 (3): 221–233, PMID 188300 
  27. ^ Music Publicist Norman Winter, Who Repped Michael Jackson and Bob Dylan, Dies

External links[edit]