Մասնակից:Erikmamanukyan/Ավազարկղ

Signs and symptoms[խմբագրել | խմբագրել կոդը]

Պարկինսոնի հիվանդության ամենաճանաչելի ախտանիշները կապված են շարժողական համակարգի հետ^[2]։ Ոչ շարժողական ախտանիշները, որոնք ընդգրկում են ինքնավար դիսֆունկցիան, նեյրոհոգեկան խնդիրները (տրամադրության, գիտակցության, վարքի կամ մտածողության խանգարումներ), զգայական խնդիրները(հատկապես խանգարվում է հոտառությունը) և քնի հետ կապված դժվարությունները նույնպես բնորոշ են։ Որոշ ոչ շարժողական խնդիրներ կարող են արտահայտված լինել արդեն ախտորոշման ժամանակ^[2]։

շարժական[խմբագրել | խմբագրել կոդը]

Առանձնացնում ենք 4 հիմնական շարժական ախտանիշներ՝ դող հանգստի ժամանակ, դանդաղաշարժություն, կարկամություն և պոստուռալ անկայունություն^[2]։

Ամենատարածված ախտանիշը ախտահարված ձեռքի դողն է հանգստի ժամանակ, որն անհետանում է կամային շարժումներ կատարելիս, կամ քնի խորը փուլերի ընթացքում^[2]։ Սովորաբար դողը առաջանում է միայն մի ձեռքում, իսկ երկու ձեռքերի միաժամանակյա ախտահարումը խոսում է հիվանդության առաջընթացի մասին^[2]։ Դողի հաճախականությունը կազմում է 4֊6 հերց(պարբերաշրջանը վայրկյանի ըմթացքում )։ Դողը նման է դեղ փաթաթելուն, երբ բութը և ցուցամատը՝ իրար կպած, հակում ունեն պտուտաձև շարժումներ կատարելուն ^[2][3]։ Այս տերմինը եկել է նրանից, որ այս հիվանդների շարժումները նման են նախկինում դեղահաբեր պատրաստելու տեխնիկայի շարժումներին^[3]։

Դանդարաշարժությունը հայտնաբերվում է յուրաքանչուր հիվանդի մոտ, և այն տեղի է ունենում շարժում իրականացնելու գործընթացը պլանավորելու անկարողության պատճառով։ Արդյունքում տուժում է շարժման ամբողջ ընթացքը՝ պլանավորումը, իրականացումը և վերջնարդյունքը։ Դանդաղաշարժությունը կյանքի որակի վրա ամենից շատ ազդող ախտանիշն է, քանի որ դրա պատճառով խանգարվում են կենցաղային գործողությունները, ինչպիսիք են՝ հագնվելը, սնվելը և լոգանք ընդունելը։Այն նաև ազդում է երկու շարժում միաժամանակ կատարելու վրա, և կարող է ավելի ծանր ընթացք ունենալ եթե զուգահեռ դիտվի էմոցիոնալ սթրես, կամ այլ հիվանդություն, սակայն զարմանալիորեն այս հիվանդները կարող են հեծանիվ քշել կամ աստիճանները բարձրանալ ավելի լավ, քան հարթ տեղով քայլել։ Թեև բժիշկները անզեն աչքով նկատում են դանդաղաշարժությունը, այնուամենայնիվ ֆորմալ գնահատելու համար խնդրում են հիվանդին ձեռքի և ոտքի մատերով կրկնվող շարժումներ կատարել ^[4]։

Կարկամությունը դիմադրությունն է վերջույթների շարժման հանդեպ՝ բարձրացած մկանային տոնուսի և մկանների չափից ավել ու շարունակական կրճատման պատճառով^[2]։ Պարկինսոնիզմի ժամանակ կարկամությունը բազմաձև է՝ «ատամնավոր անիվի ֆենոմեն» կամ Կոգվիլիլի կարկամություն^[5][2][6][7]։ Ենթադրվում է, որ Կոգվիլյան կարկամության պատճառը հանգստի դողի և մկանների բարձրացված տոնուսի հետևանք է^[8]։ Կարկամությունը կարող է կապված լինել հոդացավի հետ, և այսպիսի ցավը հաճախ հիվանդության սկզբնական արտահայտման ձևն է^[2]։ Հիվանդության սկզբնական շրջանում կարկամությունը ասիմետրիկ է՝ հիմնականում ախտահարվում են պարանոցի և ուսերի մկանները, և այս մկանների ախտահարումը նախորդում է դեմքի և վերջույթների մկանների ախտահարմանը^[9]։ Հիվանդության առաջընթացի հետ կարկամությունը ընդգրկում է ողջ մարմինը՝ սահմանափակելով շարժման կարողությունը։

Պոստուռալ անկայունությունը բնորոշ է հիվանդության ուշ փուլերին, բերելով հավասարակշռության խախտմանը և հաճախակի ընկնումներին^[10], որն ել պատճառ է դառնում երկրորդային կոտրվածքների, ինքնավստահութան կորստին և շարժվելու սահմանափակմանը^[11]։ Անկայունությունը հաճախ բացակայում է հիվանդության վաղ փուլերում, հատկապես երիտասարդ հիվանդնեի մոտ և հատկապես երկկողմանի ախտանիշներ ունեցողների մոտ Instability^[12]։ Պարկինսոնի հիվանդությամբ տառապողների շուրջ 40% ի մոտ ընկնելու դեպք է գրանցվել, իսկ 10% հիվանդները ունենում են ընկնելու դեպքեր ամեն շաբաթ^[2]։

Այլ հայտնի շարժական նշաններից են խանգարումները կապված դիրքի և քայլելու հետ, ինչպիսիք են մանր քայլքը (արագ,քստքստացող քայլք՝ առաջ թեքված մարմնի դիրքով, դողացող ձեռքով), քայլվածքի սառեցումը(կարճատև քայլելու անկարողություն, երբ թվում է թե ոտքը անհնար է շարժել, հատկապես ուղղությունը փոխելու ժամանակ), մոնոտոն, ցածր ձայնը, դիմականման դեմքի արտահայտությունը և ձեռագիրը,որը գնալով դառնում է ավելի մանր և ոչ հստակ^[13]։

Neuropsychiatric[խմբագրել | խմբագրել կոդը]

Parkinson's disease can cause neuropsychiatric disturbances, which can range from mild to severe. This includes disorders of cognition, mood, behavior, and thought.^[2]

Cognitive disturbances can occur in the early stages of the disease and sometimes prior to diagnosis, and increase in prevalence with duration of the disease.^[2][14] The most common cognitive deficit in PD is executive dysfunction, which can include problems with planning, cognitive flexibility, abstract thinking, rule acquisition, inhibiting inappropriate actions, initiating appropriate actions, working memory, and control of attention.^[14][15] Other cognitive difficulties include slowed cognitive processing speed, impaired recall and impaired perception and estimation of time.^[14][15] Nevertheless, improvement appears when recall is aided by cues.^[14] Visuospatial difficulties are also part of the disease, seen for example when the individual is asked to perform tests of facial recognition and perception of the orientation of drawn lines.^[14][15]

A person with PD has two to six times the risk of dementia compared to the general population.^[2][14] Up to 78% of people with PD have Parkinson's disease dementia.^[16] The prevalence of dementia increases with age and, to a lesser degree, duration of the disease.^[17] Dementia is associated with a reduced quality of life in people with PD and their caregivers, increased mortality, and a higher probability of needing nursing home care.^[14]

Impulse control disorders including pathological gambling, compulsive sexual behavior, binge eating, compulsive shopping and reckless generosity can be caused by medication, particularly orally active dopamine agonists. The dopamine dysregulation syndrome – with wanting of medication leading to overusage – is a rare complication of levodopa use (Giovannoni, et al. 2000).

Behavior and mood alterations are more common in PD without cognitive impairment than in the general population, and are usually present in PD with dementia. The most frequent mood difficulties are depression, apathy, and anxiety.^[2] Establishing the diagnosis of depression is complicated by the fact that the body language of depression may masquerade as PD including a sad expressionless anxious face, a hang dog appearance, slow movement, and monotonous speech. Up to 30% of people with PD may experience symptoms of anxiety, ranging from a generalized anxiety disorder to social phobia, panic disorders and obsessive compulsive disorders. They contribute to impaired quality of life and increased severity of motor symptoms such as on/off fluctuations or freezing episodes.

Punding in which complicated repetitive aimless stereotyped behaviors occur for many hours is another disturbance caused by anti-Parkinson medication.

Hallucinations or delusions occur in approximately 50% of people with PD over the course of the illness, and may herald the emergence of dementia. These range from minor hallucinations – "sense of passage" (something quickly passing beside the person) or "sense of presence" (the perception of something/someone standing just to the side or behind the person) – to full blown vivid, formed visual hallucinations and paranoid ideation. Auditory hallucinations are uncommon in PD, and are rarely described as voices. It is now believed that psychosis is an integral part of the disease. A psychosis with delusions and associated delirium is a recognized complication of anti-Parkinson drug treatment and may also be caused by urinary tract infections (as frequently occurs in the fragile elderly), but drugs and infection are not the only factors, and underlying brain pathology or changes in neurotransmitters or their receptors (e.g., acetylcholine, serotonin) are also thought to play a role in psychosis in PD.^[18][19]

այլ[խմբագրել | խմբագրել կոդը]

Պարկինսոնի հիվանդությունը, բացի շարժողական և նեյրոհոգեկան խնդիրներից,կարող է առաջացնել նաև այլ գործառույթների ախտահարումներ։

Քնի խանգարումները բնորոշ են հիվանդությանը և կարող են ավելի խորանալ դեղերի օգտագործման պատճառով^[2]։ Ախտանիշները կարող են դրսևորվել, որպես ցերեկային քնկոտություն(կարող են դիտվել պատահական քնի նոպաներ, հիշեցնելով նարկոլեպսիան), քնի ակտիվ փուլի խանգարում, կամ անքնություն^[2]։ Արագ քնի վարքային ախտահարման REM behavior disorder (RBD), in which patients act out dreams, sometimes injuring themselves or their bed partner, may begin many years before the development of motor or cognitive features of PD or DLB.^[20]

Alterations in the autonomic nervous system can lead to orthostatic hypotension (low blood pressure upon standing), oily skin and excessive sweating, urinary incontinence, and altered sexual function.^[2] Constipation and impaired stomach emptying (gastric dysmotility) can be severe enough to cause discomfort and even endanger health.^[21] Changes in perception may include an impaired sense of smell, disturbed vision, pain, and paresthesia (tingling and numbness).^[2] All of these symptoms can occur years before diagnosis of the disease.^[2]

Causes[խմբագրել | խմբագրել կոդը]

Environmental factors[խմբագրել | խմբագրել կոդը]

Exposure to pesticides and a history of head injury have each been linked with Parkinson disease (PD), but the risks are modest. Never having smoked cigarettes, and never drinking caffeinated beverages, are also associated with small increases in risk of developing PD.^[22]

Low concentrations of urate in the blood serum is associated with an increased risk of PD.^[23]

Genetics[խմբագրել | խմբագրել կոդը]

Research indicates that PD is the product of a complex interaction of genetic and environmental factors.^[24] Around 15% of individuals with PD have a first-degree relative who has the disease,^[5] and 5–10% of people with PD are known to have forms of the disease that occur because of a mutation in one of several specific genes.^[25] Harboring one of these gene mutations may not lead to the disease; susceptibility factors put the individual at an increased risk, often in combination with other risk factors, which also affect age of onset, severity and progression.^[25]

Genes implicated in the development of PD include SNCA, LRRK2, GBA, PRKN, PINK1, PARK7, VPS35, EIF4G1, DNAJC13 and CHCHD2.^[26]

SNCA gene mutations are important in PD because the protein which this gene encodes, alpha-synuclein, is the main component of the Lewy bodies that accumulate in the brains of people with PD.^[25] Mutations in some genes, including SNCA, LRRK2 and GBA, have been found to be risk factors for "sporadic" (non-familial) PD.^[25] Mutations in the gene LRRK2 are the most common known cause of familial and sporadic PD, accounting for approximately 5% of individuals with a family history of the disease and 3% of sporadic cases.^[27][25] A mutation in GBA presents the greatest genetic risk of developing Parkinsons disease.^[26]

Several Parkinson-related genes are involved in the function of lysosomes, organelles that digest cellular waste products. It has been suggested that some cases of PD may be caused by lysosome dysfunctions that reduce the ability of cells to break down alpha-synuclein.^[28]

Pathophysiology[խմբագրել | խմբագրել կոդը]

The main pathological characteristics of PD are cell death in the brain's basal ganglia (affecting up to 70% of the dopamine secreting neurons in the substantia nigra pars compacta by the end of life)^[27] and the presence of Lewy bodies (accumulations of the protein alpha-synuclein) in many of the remaining neurons. This loss of neurons is accompanied by the death of astrocytes (star-shaped glial cells) and a significant increase in the number of microglia (another type of glial cell) in the substantia nigra.^[29]

There are five major pathways in the brain connecting other brain areas with the basal ganglia. These are known as the motor, oculo-motor, associative, limbic and orbitofrontal circuits, with names indicating the main projection area of each circuit.^[31] All of them are affected in PD, and their disruption explains many of the symptoms of the disease, since these circuits are involved in a wide variety of functions, including movement, attention and learning.^[31] Scientifically, the motor circuit has been examined the most intensively.^[31]

A particular conceptual model of the motor circuit and its alteration with PD has been of great influence since 1980, although some limitations have been pointed out which have led to modifications.^[31] In this model, the basal ganglia normally exert a constant inhibitory influence on a wide range of motor systems, preventing them from becoming active at inappropriate times. When a decision is made to perform a particular action, inhibition is reduced for the required motor system, thereby releasing it for activation. Dopamine acts to facilitate this release of inhibition, so high levels of dopamine function tend to promote motor activity, while low levels of dopamine function, such as occur in PD, demand greater exertions of effort for any given movement. Thus, the net effect of dopamine depletion is to produce hypokinesia, an overall reduction in motor output.^[31] Drugs that are used to treat PD, conversely, may produce excessive dopamine activity, allowing motor systems to be activated at inappropriate times and thereby producing dyskinesias.^[31]

Brain cell death[խմբագրել | խմբագրել կոդը]

There is speculation of several mechanisms by which the brain cells could be lost.^[32] One mechanism consists of an abnormal accumulation of the protein alpha-synuclein bound to ubiquitin in the damaged cells. This insoluble protein accumulates inside neurones forming inclusions called Lewy bodies.^[27][33] According to the Braak staging, a classification of the disease based on pathological findings proposed by Heiko Braak, Lewy bodies first appear in the olfactory bulb, medulla oblongata and pontine tegmentum; individuals at this stage may be asymptomatic or may have early non-motor symptoms (such as loss of sense of smell, or some sleep or automatic dysfunction). As the disease progresses, Lewy bodies develop in the substantia nigra, areas of the midbrain and basal forebrain and, finally, the neocortex.^[27] These brain sites are the main places of neuronal degeneration in PD; however, Lewy bodies may not cause cell death and they may be protective (with the abnormal protein sequestered or walled off). Other forms of alpha-synuclein (e.g., oligomers) that are not aggregated in Lewy bodies and Lewy neurites may actually be the toxic forms of the protein.^[32][33] In people with dementia, a generalized presence of Lewy bodies is common in cortical areas. Neurofibrillary tangles and senile plaques, characteristic of Alzheimer's disease, are not common unless the person is demented.^[29]

Other cell-death mechanisms include proteasomal and lysosomal system dysfunction and reduced mitochondrial activity.^[32] Iron accumulation in the substantia nigra is typically observed in conjunction with the protein inclusions. It may be related to oxidative stress, protein aggregation and neuronal death, but the mechanisms are not fully understood.^[34]

Diagnosis[խմբագրել | խմբագրել կոդը]

A physician will initially assess for Parkinson's disease with a careful medical history and neurological examination.^[2] People may be given levodopa, with any resulting improvement in motor impairment helping to confirm the PD diagnosis. The finding of Lewy bodies in the midbrain on autopsy is usually considered final proof that the person had PD. The clinical course of the illness over time may reveal it is not Parkinson's disease, requiring that the clinical presentation be periodically reviewed to confirm accuracy of the diagnosis.^[2][35]

Other causes that can secondarily produce parkinsonism are stroke and drugs.^[35] Parkinson plus syndromes such as progressive supranuclear palsy and multiple system atrophy must be ruled out.^[2] Anti-Parkinson's medications are typically less effective at controlling symptoms in Parkinson plus syndromes.^[2] Faster progression rates, early cognitive dysfunction or postural instability, minimal tremor or symmetry at onset may indicate a Parkinson plus disease rather than PD itself.^[36] Genetic forms with an autosomal dominant or recessive pattern of inheritance are sometimes referred to as familial Parkinson's disease or familial parkinsonism.^[5]

Medical organizations have created diagnostic criteria to ease and standardize the diagnostic process, especially in the early stages of the disease. The most widely known criteria come from the UK Queen Square Brain Bank for Neurological Disorders and the U.S. National Institute of Neurological Disorders and Stroke. The Queen Square Brain Bank criteria require slowness of movement (bradykinesia) plus either rigidity, resting tremor, or postural instability. Other possible causes of these symptoms need to be ruled out. Finally, three or more of the following supportive features are required during onset or evolution: unilateral onset, tremor at rest, progression in time, asymmetry of motor symptoms, response to levodopa for at least five years, clinical course of at least ten years and appearance of dyskinesias induced by the intake of excessive levodopa.^[37]

When PD diagnoses are checked by autopsy, movement disorders experts are found on average to be 79.6% accurate at initial assessment and 83.9% accurate after they have refined their diagnosis at a follow-up examination. When clinical diagnoses performed mainly by nonexperts are checked by autopsy, average accuracy is 73.8%. Overall, 80.6% of PD diagnoses are accurate, and 82.7% of diagnoses using the Brain Bank criteria are accurate.^[38]

A task force of the International Parkinson and Movement Disorder Society (MDS) has proposed diagnostic criteria for Parkinson’s disease as well as research criteria for the diagnosis of prodromal disease, but these will require validation against the more established criteria.^[39][40]

Imaging[խմբագրել | խմբագրել կոդը]

Computed tomography (CT) scans of people with PD usually appear normal.^[41] MRI has become more accurate in diagnosis of the disease over time, specifically through iron-sensitive T2* and SWI sequences at a magnetic field strength of at least 3T, both of which can demonstrate absence of the characteristic 'swallow tail' imaging pattern in the dorsolateral substantia nigra.^[42] In a meta-analysis, absence of this pattern was 98% sensitive and 95% specific for the disease.^[43] Diffusion MRI has shown potential in distinguishing between PD and Parkinson plus syndromes, though its diagnostic value is still under investigation.^[41] CT and MRI are also used to rule out other diseases that can be secondary causes of parkinsonism, most commonly encephalitis and chronic ischemic insults, as well as less frequent entities such as basal ganglia tumors and hydrocephalus.^[41]

Dopamine-related activity in the basal ganglia can be directly measured with PET and SPECT scans. A finding of reduced dopamine-related activity in the basal ganglia can rule out drug-induced parkinsonism, but reduced basal ganglia dopamine-related activity is seen in both PD and the Parkinson-plus disorders so these scans are not reliable in distinguishing PD from other neurodegenerative causes of parkinsonism.^[41]

Prevention[խմբագրել | խմբագրել կոդը]

Exercise in middle age may reduce the risk of Parkinson's disease later in life.^[44] Caffeine also appears protective with a greater decrease in risk occurring with a larger intake of caffeinated beverages such as coffee.^[45] People who smoke cigarettes or use smokeless tobacco are less likely than non-smokers to develop PD, and the more they have used tobacco, the less likely they are to develop PD. It is not known what underlies this effect. Tobacco use may actually protect against PD, or it may be that an unknown factor both increases the risk of PD and causes an aversion to tobacco or makes it easier to quit using tobacco.^[46]

Antioxidants, such as vitamins C and E, have been proposed to protect against the disease, but results of studies have been contradictory and no positive effect has been proven.^[47] The results regarding fat and fatty acids have been contradictory, with various studies reporting protective effects, risk-increasing effects or no effects.^[47] There have been preliminary indications that the use of anti-inflammatory drugs and calcium channel blockers may be protective.^[24] A 2010 meta-analysis found that nonsteroidal anti-inflammatory drugs (apart from aspirin), have been associated with at least a 15 percent (higher in long-term and regular users) reduction of incidence of the development of Parkinson's disease.^[48]

Management[խմբագրել | խմբագրել կոդը]

There is no cure for Parkinson's disease, but medications, surgery, and physical treatment can provide relief and are much more effective than treatments available for other neurological disorders like Alzheimer’s disease, motor neuron disease, and Parkinson plus syndromes. The main families of drugs useful for treating motor symptoms are levodopa (always combined with a dopa decarboxylase inhibitor and sometimes also with a COMT inhibitor), dopamine agonists and MAO-B inhibitors. The stage of the disease and the age at disease onset determine which group is most useful.^[49]

Three stages may be distinguished: an initial stage in which the individual with PD has already developed some disability requiring pharmacological treatment, a second stage associated with the development of complications related to levodopa usage, and a third stage when symptoms unrelated to dopamine deficiency or levodopa treatment may predominate.^[50]

Treatment in the first stage aims for an optimal trade off between symptom control and treatment side-effects. The start of levodopa treatment may be postponed by initially using other medications such as MAO-B inhibitors and dopamine agonists instead, in the hope of delaying the onset of complications due to levodopa use.^[51] However, levodopa is still the most effective treatment for the motor symptoms of PD and should not be delayed in patients whose quality of life is impaired by those symptoms. Levodopa-related dyskinesias correlate more strongly with duration and severity of the disease than duration of levodopa treatment, so delaying this therapy may not really provide much longer dyskinesia-free time than early use.^[52]

In the second stage the aim is to reduce PD symptoms while controlling fluctuations in the effect of the medication. Sudden withdrawals from medication or overuse have to be managed.^[51] When oral medications are not enough to control symptoms, surgery, deep brain stimulation, subcutaneous waking day apomorphine infusion and enteral dopa pumps can be of use.^[53] The third stage presents many challenging problems requiring a variety of treatments for psychiatric symptoms, orthostatic hypotension, bladder dysfunction, etc.^[53] In the final stages of the disease, palliative care is provided to improve quality of life.^[54]

Medications[խմբագրել | խմբագրել կոդը]

Levodopa[խմբագրել | խմբագրել կոդը]

The motor symptoms of PD are the result of reduced dopamine production in the brain's basal ganglia. Dopamine does not cross the blood-brain barrier, so it cannot be taken as a medicine to boost the brain's depleted levels of dopamine. However a precursor of dopamine, levodopa, can pass through to the brain where it is readily converted to dopamine, and administration of levodopa temporarily diminishes the motor symptoms of PD. Levodopa has been the most widely used PD treatment for over 40 years.^[51]

Only 5–10% of levodopa crosses the blood–brain barrier. Much of the remainder is metabolized to dopamine elsewhere in the body, causing a variety of side effects including nausea, vomiting and orthostatic hypotension.^[55] Carbidopa and benserazide are dopa decarboxylase inhibitors which do not cross the blood-brain barrier and inhibit the conversion of levodopa to dopamine outside the brain, reducing side effects and improving the availability of levodopa for passage into the brain. One of these drugs is usually taken along with levodopa, often combined with levodopa in the same pill.^[56]

Levodopa use leads in the long term to the development of complications: involuntary movements called dyskinesias, and fluctuations in the effectiveness of the medication.^[51] When fluctuations occur, a person can cycle through phases with good response to medication and reduced PD symptoms ("on" state), and phases with poor response to medication and significant PD symptoms ("off" state).^[51] Using lower doses of levodopa may reduce the risk and severity of these levodopa-induced complications.^[57] A former strategy to reduce levodopa-related dyskinesia and fluctuations was to withdraw levodopa medication for some time. This is now discouraged since it can bring on dangerous side effects such as neuroleptic malignant syndrome.^[51] Most people with PD will eventually need levodopa and will later develop levodopa-induced fluctuations and dyskinesias.^[51]

There are controlled-release versions of levodopa. Older controlled-release levodopa preparations have poor and unreliable absorption and bioavailability and have not demonstrated improved control of PD motor symptoms or a reduction in levodopa-related complications when compared to immediate release preparations. A newer extended-release levodopa preparation does seem to be more effective in reducing fluctuations but in many patients problems persist. Intestinal infusions of levodopa (Duodopa) can result in striking improvements in fluctuations compared to oral levodopa when the fluctuations are due to insufficient uptake caused by gastroparesis. Other oral, longer acting formulations are under study and other modes of delivery (inhaled, transdermal) are being developed.^[56]

COMT inhibitors[խմբագրել | խմբագրել կոդը]

Tolcapone inhibits the activity COMT, an enzyme which degrades dopamine.^[51] It has been used to complement levodopa; however, its usefulness is limited by possible complications such as liver damage.^[51] A similarly effective drug, entacapone, has not been shown to cause significant alterations of liver function.^[51] Licensed preparations of entacapone contain entacapone alone or in combination with carbidopa and levodopa.^[51]

Dopamine agonists[խմբագրել | խմբագրել կոդը]

Several dopamine agonists that bind to dopamine receptors in the brain have similar effects to levodopa.^[51] These were initially used as a complementary therapy to levodopa for individuals experiencing levodopa complications (on-off fluctuations and dyskinesias); they are now mainly used on their own as first therapy for the motor symptoms of PD with the aim of delaying the initiation of levodopa therapy and so delaying the onset of levodopa's complications.^[51][58] Dopamine agonists include bromocriptine, pergolide, pramipexole, ropinirole, piribedil, cabergoline, apomorphine and lisuride.

Though dopamine agonists are less effective than levodopa at controlling PD motor symptoms, they are usually effective enough to manage these symptoms in the first years of treatment.^[5] Dyskinesias due to dopamine agonists are rare in younger people who have PD but, along with other complications, become more common with older age at onset.^[5] Thus dopamine agonists are the preferred initial treatment for younger onset PD, and levodopa is preferred for older onset PD.^[5]

Dopamine agonists produce significant, although usually mild, side effects including drowsiness, hallucinations, insomnia, nausea, and constipation.^[51] Sometimes side effects appear even at a minimal clinically effective dose, leading the physician to search for a different drug.^[51] Agonists have been related to impulse control disorders (such as compulsive sexual activity, eating, gambling and shopping) even more strongly than levodopa.^[59] They tend to be more expensive than levodopa.^[5]

Apomorphine, a non-orally administered dopamine agonist, may be used to reduce off periods and dyskinesia in late PD.^[51] It is administered by intermittent injections or continuous subcutaneous infusions.^[51] Since secondary effects such as confusion and hallucinations are common, individuals receiving apomorphine treatment should be closely monitored.^[51] Two dopamine agonists that are administered through skin patches (lisuride and rotigotine) and are useful for people in the initial stages and possibly to control off states in those in the advanced state.^[60]

MAO-B inhibitors[խմբագրել | խմբագրել կոդը]

MAO-B inhibitors (safinamide, selegiline and rasagiline) increase the amount of dopamine in the basal ganglia by inhibiting the activity of monoamine oxidase B (MAO-B), an enzyme which breaks down dopamine.^[51] Like dopamine agonists, their use may delay the commencement of levodopa therapy in early disease, but MAO-B inhibitors produce more adverse effects and are less effective than levodopa at controlling PD motor symptoms. There are few studies of their effectiveness in the advanced stage, although results suggest that they are useful to reduce fluctuations between on and off periods.^[51] An initial study indicated that selegiline in combination with levodopa increased the risk of death, but this was later disproven.^[51]

Other drugs[խմբագրել | խմբագրել կոդը]

Other drugs such as amantadine and anticholinergics may be useful as treatment of motor symptoms. However, the evidence supporting them lacks quality, so they are not first choice treatments.^[51] In addition to motor symptoms, PD is accompanied by a diverse range of symptoms. A number of drugs have been used to treat some of these problems.^[61] Examples are the use of quetiapine for psychosis, cholinesterase inhibitors for dementia, and modafinil for daytime sleepiness.^[61][62] In 2016 pimavanserin was approved for the management of Parkinson's disease psychosis.^[63]

Doxepin and rasagline may reduce physical fatigue in PD.^[64]

Surgery[խմբագրել | խմբագրել կոդը]

Treating motor symptoms with surgery was once a common practice, but since the discovery of levodopa, the number of operations has declined.^[65] Studies in the past few decades have led to great improvements in surgical techniques, so that surgery is again being used in people with advanced PD for whom drug therapy is no longer sufficient.^[65] Surgery for PD can be divided in two main groups: lesional and deep brain stimulation (DBS). Target areas for DBS or lesions include the thalamus, the globus pallidus or the subthalamic nucleus.^[65] Deep brain stimulation is the most commonly used surgical treatment, developed in the 1980s by Alim Louis Benabid and others. It involves the implantation of a medical device called a neurostimulator, which sends electrical impulses to specific parts of the brain. DBS is recommended for people who have PD with motor fluctuations and tremor inadequately controlled by medication, or to those who are intolerant to medication, as long as they do not have severe neuropsychiatric problems.^[66] Other, less common, surgical therapies involve intentional formation of lesions to suppress overactivity of specific subcortical areas. For example, pallidotomy involves surgical destruction of the globus pallidus to control dyskinesia.^[65]

Rehabilitation[խմբագրել | խմբագրել կոդը]

Exercise programs are recommended in people with Parkinson's disease.^[44] There is some evidence that speech or mobility problems can improve with rehabilitation, although studies are scarce and of low quality.^[67][68] Regular physical exercise with or without physical therapy can be beneficial to maintain and improve mobility, flexibility, strength, gait speed, and quality of life.^[68] When an exercise program is performed under the supervision of a physiotherapist, there are more improvements in motor symptoms, mental and emotional functions, daily living activities, and quality of life compared to a self-supervised exercise program at home.^[69] In terms of improving flexibility and range of motion for people experiencing rigidity, generalized relaxation techniques such as gentle rocking have been found to decrease excessive muscle tension. Other effective techniques to promote relaxation include slow rotational movements of the extremities and trunk, rhythmic initiation, diaphragmatic breathing, and meditation techniques.^[70] As for gait and addressing the challenges associated with the disease such as hypokinesia (slowness of movement), shuffling and decreased arm swing; physiotherapists have a variety of strategies to improve functional mobility and safety. Areas of interest with respect to gait during rehabilitation programs focus on, but are not limited to improving gait speed, the base of support, stride length, trunk and arm swing movement. Strategies include utilizing assistive equipment (pole walking and treadmill walking), verbal cueing (manual, visual and auditory), exercises (marching and PNF patterns) and altering environments (surfaces, inputs, open vs. closed).^[71] Strengthening exercises have shown improvements in strength and motor function for people with primary muscular weakness and weakness related to inactivity with mild to moderate Parkinson's disease. However, reports show a significant interaction between strength and the time the medications was taken. Therefore, it is recommended that people with PD should perform exercises 45 minutes to one hour after medications when they are at their best.^[72] Also, due to the forward flexed posture, and respiratory dysfunctions in advanced Parkinson's disease, deep diaphragmatic breathing exercises are beneficial in improving chest wall mobility and vital capacity.^[73] Exercise may improve constipation.^[21] It is unclear if exercise reduces physical fatigue in PD.^[64]

One of the most widely practiced treatments for speech disorders associated with Parkinson's disease is the Lee Silverman voice treatment (LSVT).^[67][74] Speech therapy and specifically LSVT may improve speech.^[67] Occupational therapy (OT) aims to promote health and quality of life by helping people with the disease to participate in as many of their daily living activities as possible.^[67] There have been few studies on the effectiveness of OT and their quality is poor, although there is some indication that it may improve motor skills and quality of life for the duration of the therapy.^[67][75]

Palliative care[խմբագրել | խմբագրել կոդը]

Palliative care is specialized medical care for people with serious illnesses, including Parkinson's. The goal of this speciality is to improve quality of life for both the person with Parkinson's and the family by providing relief from the symptoms, pain, and stress of illnesses.^[76] As Parkinson's is not a curable disease, all treatments are focused on slowing decline and improving quality of life, and are therefore palliative in nature.^[77]

Palliative care should be involved earlier, rather than later in the disease course.^[78][79] Palliative care specialists can help with physical symptoms, emotional factors such as loss of function and jobs, depression, fear, and existential concerns.^[78][79][80]

Along with offering emotional support to both the patient and family, palliative care serves an important role in addressing goals of care. People with Parkinson's may have many difficult decisions to make as the disease progresses such as wishes for feeding tube, non-invasive ventilator, and tracheostomy; wishes for or against cardiopulmonary resuscitation; and when to use hospice care.^[77] Palliative care team members can help answer questions and guide people with Parkinson's on these complex and emotional topics to help them make the best decision based on their own values.^[79][81]

Muscles and nerves that control the digestive process may be affected by PD, resulting in constipation and gastroparesis (food remaining in the stomach for a longer period than normal).^[21] A balanced diet, based on periodical nutritional assessments, is recommended and should be designed to avoid weight loss or gain and minimize consequences of gastrointestinal dysfunction.^[21] As the disease advances, swallowing difficulties (dysphagia) may appear. In such cases it may be helpful to use thickening agents for liquid intake and an upright posture when eating, both measures reducing the risk of choking. Gastrostomy to deliver food directly into the stomach is possible in severe cases.^[21]

Levodopa and proteins use the same transportation system in the intestine and the blood–brain barrier, thereby competing for access.^[21] When they are taken together, this results in a reduced effectiveness of the drug.^[21] Therefore, when levodopa is introduced, excessive protein consumption is discouraged and well balanced Mediterranean diet is recommended. In advanced stages, additional intake of low-protein products such as bread or pasta is recommended for similar reasons.^[21] To minimize interaction with proteins, levodopa should be taken 30 minutes before meals.^[21] At the same time, regimens for PD restrict proteins during breakfast and lunch, allowing protein intake in the evening.^[21]

Prognosis[խմբագրել | խմբագրել կոդը]

PD invariably progresses with time. A severity rating method known as the Unified Parkinson's disease rating scale (UPDRS) is the most commonly used metric for clinical study. A modified version known as the MDS-UPDRS is also sometimes used. An older scaling method known as the Hoehn and Yahr scale (originally published in 1967), and a similar scale known as the Modified Hoehn and Yahr scale, have also been commonly used. The Hoehn and Yahr scale defines five basic stages of progression.

Motor symptoms, if not treated, advance aggressively in the early stages of the disease and more slowly later. Untreated, individuals are expected to lose independent ambulation after an average of eight years and be bedridden after ten years.^[82] However, it is uncommon to find untreated people nowadays. Medication has improved the prognosis of motor symptoms, while at the same time it is a new source of disability, because of the undesired effects of levodopa after years of use.^[82] In people taking levodopa, the progression time of symptoms to a stage of high dependency from caregivers may be over 15 years.^[82] However, it is hard to predict what course the disease will take for a given individual.^[82] Age is the best predictor of disease progression.^[32] The rate of motor decline is greater in those with less impairment at the time of diagnosis, while cognitive impairment is more frequent in those who are over 70 years of age at symptom onset.^[32]

Since current therapies improve motor symptoms, disability at present is mainly related to non-motor features of the disease.^[32] Nevertheless, the relationship between disease progression and disability is not linear. Disability is initially related to motor symptoms.^[82] As the disease advances, disability is more related to motor symptoms that do not respond adequately to medication, such as swallowing/speech difficulties, and gait/balance problems; and also to levodopa-induced complications, which appear in up to 50% of individuals after 5 years of levodopa usage.^[82] Finally, after ten years most people with the disease have autonomic disturbances, sleep problems, mood alterations and cognitive decline.^[82] All of these symptoms, especially cognitive decline, greatly increase disability.^[32][82]

The life expectancy of people with PD is reduced.^[82] Mortality ratios are around twice those of unaffected people.^[82] Cognitive decline and dementia, old age at onset, a more advanced disease state and presence of swallowing problems are all mortality risk factors. On the other hand, a disease pattern mainly characterized by tremor as opposed to rigidity predicts an improved survival.^[82] Death from aspiration pneumonia is twice as common in individuals with PD as in the healthy population.^[82]

In 2013 PD resulted in about 103,000 deaths globally, up from 44,000 deaths in 1990.^[83] The death rate increased from an average of 1.5 to 1.8 per 100,000 during that time.^[83]

Epidemiology[խմբագրել | խմբագրել կոդը]

PD is the second most common neurodegenerative disorder after Alzheimer's disease and affects approximately seven million people globally and one million people in the United States.^[10][47][84] The proportion in a population at a given time is about 0.3% in industrialized countries. PD is more common in the elderly and rates rise from 1% in those over 60 years of age to 4% of the population over 80.^[47] The mean age of onset is around 60 years, although 5–10% of cases, classified as young onset PD, begin between the ages of 20 and 50.^[5] Males are more often affected than females at a ratio of around 3:2.^[24] PD may be less prevalent in those of African and Asian ancestry, although this finding is disputed.^[47] Some studies have proposed that it is more common in men than women, but others failed to detect any differences between the two sexes.^[47] The number of new cases per year of PD is between 8 and 18 per 100,000 person–years.^[47]

Many risk factors and protective factors have been proposed, sometimes in relation to theories concerning possible mechanisms of the disease, however, none have been conclusively related to PD by empirical evidence. When epidemiological studies have been carried out in order to test the relationship between a given factor and PD, they have often been flawed and their results have in some cases been contradictory.^[47] The most frequently replicated relationships are an increased risk of PD in those exposed to pesticides, and a reduced risk in smokers.^[47][85]

History[խմբագրել | խմբագրել կոդը]

Several early sources, including an Egyptian papyrus, an Ayurvedic medical treatise, the Bible, and Galen's writings, describe symptoms resembling those of PD.^[86] After Galen there are no references unambiguously related to PD until the 17th century.^[86] In the 17th and 18th centuries, several authors wrote about elements of the disease, including Sylvius, Gaubius, Hunter and Chomel.^[86][87][88]

In 1817 an English doctor, James Parkinson, published his essay reporting six cases of paralysis agitans.^[89] An Essay on the Shaking Palsy described the characteristic resting tremor, abnormal posture and gait, paralysis and diminished muscle strength, and the way that the disease progresses over time.^[90][91] Early neurologists who made further additions to the knowledge of the disease include Trousseau, Gowers, Kinnier Wilson and Erb, and most notably Jean-Martin Charcot, whose studies between 1868 and 1881 were a landmark in the understanding of the disease.^[89] Among other advances, he made the distinction between rigidity, weakness and bradykinesia.^[89] He also championed the renaming of the disease in honor of James Parkinson.^[89]

In 1912 Frederic Lewy described microscopic particles in affected brains, later named "Lewy bodies".^[89] In 1919 Konstantin Tretiakoff reported that the substantia nigra was the main cerebral structure affected, but this finding was not widely accepted until it was confirmed by further studies published by Rolf Hassler in 1938.^[89] The underlying biochemical changes in the brain were identified in the 1950s, due largely to the work of Arvid Carlsson on the neurotransmitter dopamine and Oleh Hornykiewicz on its role on PD.^[92] In 1997, alpha-synuclein was found to be the main component of Lewy bodies by Spillantini, Trojanowski, Goedert and others.^[33]

Anticholinergics and surgery (lesioning of the corticospinal pathway or some of the basal ganglia structures) were the only treatments until the arrival of levodopa, which reduced their use dramatically.^[87][93] Levodopa was first synthesized in 1911 by Casimir Funk, but it received little attention until the mid 20th century.^[92] It entered clinical practice in 1967 and brought about a revolution in the management of PD.^[92][94] By the late 1980s deep brain stimulation introduced by Alim Louis Benabid and colleagues at Grenoble, France, emerged as a possible treatment.^[95]

Society and culture[խմբագրել | խմբագրել կոդը]

Cost[խմբագրել | խմբագրել կոդը]

The costs of PD to society are high, but precise calculations are difficult due to methodological issues in research and differences between countries.^[96] The annual cost in the UK is estimated to be between Կաղապար:GB£49 million and Կաղապար:GB£3.3 billion, while the cost per patient per year in the U.S. is probably around Կաղապար:US$10,000 and the total burden around Կաղապար:US$23 billion.^[96] The largest share of direct cost comes from inpatient care and nursing homes, while the share coming from medication is substantially lower.^[96] Indirect costs are high, due to reduced productivity and the burden on caregivers.^[96] In addition to economic costs, PD reduces quality of life of those with the disease and their caregivers.^[96]

Advocacy[խմբագրել | խմբագրել կոդը]

11 April, the birthday of James Parkinson, has been designated as World Parkinson's Day.^[89] A red tulip was chosen by international organizations as the symbol of the disease in 2005: it represents the James Parkinson Tulip cultivar, registered in 1981 by a Dutch horticulturalist.^[97] Advocacy organizations include the National Parkinson Foundation, which has provided more than $180 million in care, research and support services since 1982,^[98] Parkinson's Disease Foundation, which has distributed more than $115 million for research and nearly $50 million for education and advocacy programs since its founding in 1957 by William Black;^[99][100] the American Parkinson Disease Association, founded in 1961;^[101] and the European Parkinson's Disease Association, founded in 1992.^[102]

Notable cases[խմբագրել | խմբագրել կոդը]

Actor Michael J. Fox has PD and has greatly increased the public awareness of the disease.^[103] After diagnosis, Fox embraced his Parkinson's in television roles, sometimes acting without medication, in order to further illustrate the effects of the condition. He has written two autobiographies in which his fight against the disease plays a major role,^[104] and appeared before the United States Congress without medication to illustrate the effects of the disease.^[104] The Michael J. Fox Foundation aims to develop a cure for Parkinson's disease.^[104] Fox received an honorary doctorate in medicine from Karolinska Institutet for his contributions to research in Parkinson's disease.^[105]

Professional cyclist and Olympic medalist Davis Phinney, who was diagnosed with young onset Parkinson's at age 40, started the Davis Phinney Foundation in 2004 to support Parkinson's research, focusing on quality of life for people with the disease.^[106][107]

Boxer Muhammad Ali showed signs of Parkinson's when he was 38, but was not diagnosed until he was 42, and has been called the "world's most famous Parkinson's patient".^[108] Whether he had PD or parkinsonism related to boxing is unresolved.^[109][110]

Research[խմբագրել | խմբագրել կոդը]

There is little prospect of significant new PD treatments in the near future.^[111] Currently active research directions include the search for new animal models of the disease and studies of the potential usefulness of gene therapy, stem cell transplants and neuroprotective agents.^[32]

Animal models[խմբագրել | խմբագրել կոդը]

PD is not known to occur naturally in any species other than humans, although animal models which show some features of the disease are used in research. The appearance of parkinsonism in a group of drug addicts in the early 1980s who consumed a contaminated batch of the synthetic opiate MPPP led to the discovery of the chemical MPTP as an agent that causes parkinsonism in non-human primates as well as in humans.^[112] Other predominant toxin-based models employ the insecticide rotenone, the herbicide paraquat and the fungicide maneb.^[113] Models based on toxins are most commonly used in primates. Transgenic rodent models that replicate various aspects of PD have been developed.^[114] Using the neurotoxin 6-hydroxydopamine, also known as 6-OHDA, it creates a model of Parkinson's disease in rats by targeting and destroying dopaminergic neurons in the nigrostriatal pathway when injected into the substantia nigra.^[115]

Gene therapy[խմբագրել | խմբագրել կոդը]

Gene therapy typically involves the use of a non-infectious virus (i.e., a viral vector such as the adeno-associated virus) to shuttle genetic material into a part of the brain. The gene used leads to the production of an enzyme that helps to manage PD symptoms or protects the brain from further damage.^[32][116] In 2010 there were four clinical trials using gene therapy in PD.^[32] There have not been important adverse effects in these trials although the clinical usefulness of gene therapy is still unknown.^[32] One of these reported positive results in 2011,^[117] but the company filed for bankruptcy in March 2012.^[118]

Neuroprotective treatments[խմբագրել | խմբագրել կոդը]

Investigations on neuroprotection are at the forefront of PD research. Several molecules have been proposed as potential treatments.^[32] However, none of them have been conclusively demonstrated to reduce degeneration.^[32] Agents currently under investigation include anti-apoptotics (omigapil, CEP-1347), antiglutamatergics, monoamine oxidase inhibitors (selegiline, rasagiline), promitochondrials (coenzyme Q10, creatine), calcium channel blockers (isradipine) and growth factors (GDNF).^[32] Preclinical research also targets alpha-synuclein.^[111] A vaccine that primes the human immune system to destroy alpha-synuclein, PD01A (developed by Austrian company, Affiris), has entered clinical trials in humans.^[119]

Neural transplantation[խմբագրել | խմբագրել կոդը]

Since early in the 1980s, fetal, porcine, carotid or retinal tissues have been used in cell transplants, in which dissociated cells are injected into the substantia nigra in the hope that they will incorporate themselves into the brain in a way that replaces the dopamine-producing cells that have been lost.^[32] Although there was initial evidence of mesencephalic dopamine-producing cell transplants being beneficial, double-blind trials to date indicate that cell transplants produce no long-term benefit.^[32] An additional significant problem was the excess release of dopamine by the transplanted tissue, leading to dystonias.^[120] Stem cell transplants are a recent research target, because stem cells are easy to manipulate and stem cells transplanted into the brains of rodents and monkeys have been found to survive and reduce behavioral abnormalities.^[32][121] Nevertheless, use of fetal stem cells is controversial.^[32] It has been proposed that effective treatments may be developed in a less controversial way by use of induced pluripotent stem cells taken from adults.^[32]

Other[խմբագրել | խմբագրել կոդը]

Repetitive transcranial magnetic stimulation temporarily improves levodopa-induced dyskinesias.^[122] Its usefulness in PD is an open research topic,^[123] Several nutrients have been proposed as possible treatments; however there is no evidence that vitamins or food additives improve symptoms.^[124] There is no evidence to substantiate that acupuncture and practice of Qigong, or T'ai chi, have any effect on the course of the disease or symptoms.^{[125][126][127]} Fava beans and velvet beans are natural sources of levodopa and are eaten by many people with PD; their intake is not free of risks as life-threatening adverse reactions have been described, such as the neuroleptic malignant syndrome.^[128]

The role of the gut–brain axis and the gut flora in Parkinsons became a topic of study in the 2010s, starting with work in germ-free transgenic mice, in which fecal transplants from people with PD had worse outcomes. Some studies in humans have shown a correlation between patterns of dysbiosis in the gut flora in the people with PD, and these patterns, along with a measure of severity of constipation, could diagnose PD with a 90% specificity but only a 67% sensitivity. As of 2017 some scientists hypothesized that changes in the gut flora might be an early site of PD pathology, or might be part of the pathology.^[129][130]

1. ↑ Photo by Arthur Londe from Nouvelle Iconographie de la Salpètrière, vol. 5, p. 226
2. ↑ ^{2,00 2,01 2,02 2,03 2,04 2,05 2,06 2,07 2,08 2,09 2,10 2,11 2,12 2,13 2,14 2,15 2,16 2,17 2,18 2,19 2,20 2,21 2,22} Jankovic J (April 2008). «Parkinson's disease: clinical features and diagnosis». Journal of Neurology, Neurosurgery, and Psychiatry. 79 (4): 368–76. doi:10.1136/jnnp.2007.131045. PMID 18344392. Արխիվացված է օրիգինալից 19 August 2015-ին. {{cite journal}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
3. ↑ ^{3,0 3,1} Cooper, G.; Eichhorn, G.; Rodnitzky, R. L. (2008). «Parkinson's disease». In Conn, P. Michael (ed.). Neuroscience in medicine. Totowa, NJ: Humana Press. էջեր 508–12. ISBN 978-1-60327-454-8. {{cite book}}: Unknown parameter |name-list-format= ignored (|name-list-style= suggested) (օգնություն)
4. ↑ Lees AJ, Hardy J, Revesz T (June 2009). «Parkinson's disease». Lancet. 373 (9680): 2055–66. doi:10.1016/S0140-6736(09)60492-X. PMID 19524782.
5. ↑ ^{5,0 5,1 5,2 5,3 5,4 5,5 5,6 5,7} Քաղվածելու սխալ՝ Սխալ <ref> պիտակ՝ «pmid15172778» անվանումով ref-երը տեքստ չեն պարունակում:
6. ↑ Banich, Marie T.; Compton, Rebecca J. (2011). «Motor control». Cognitive neuroscience. Belmont, CA: Wadsworth, Cengage learning. էջեր 108–44. ISBN 978-0-8400-3298-0. {{cite book}}: Unknown parameter |name-list-format= ignored (|name-list-style= suggested) (օգնություն)
7. ↑ Longmore, Murray; Wilkinson, Ian B.; Turmezei, Tom; Cheung, Chee Kay (4 January 2007). Oxford Handbook of Clinical Medicine. Oxford University Press. էջ 486. ISBN 978-0-19-856837-7. {{cite book}}: Unknown parameter |name-list-format= ignored (|name-list-style= suggested) (օգնություն)
8. ↑ Fung, Victor S. C.; Thompson, Philip D. (2007). «Rigidity and spasticity». In Tolosa, Eduardo; Jankovic (eds.). Parkinson's disease and movement disorders. Hagerstown, MD: Lippincott Williams & Wilkins. էջեր 504–13. ISBN 978-0-7817-7881-7. {{cite book}}: Unknown parameter |name-list-format= ignored (|name-list-style= suggested) (օգնություն)
9. ↑ O'Sullivan, Susan B; Schmitz, Thomas J (2007). «Parkinson's Disease». Physical Rehabilitation (5th ed.). Philadelphia: F.A. Davis. էջեր 856–57. {{cite book}}: Invalid |ref=harv (օգնություն); Unknown parameter |name-list-format= ignored (|name-list-style= suggested) (օգնություն)
10. ↑ ^{10,0 10,1} Yao, S.C.; Hart, A.D.; Terzella, M.J. (May 2013). «An evidence-based osteopathic approach to Parkinson disease». Osteopathic Family Physician. 5 (3): 96–101. doi:10.1016/j.osfp.2013.01.003.
11. ↑ Mark Hallett; Werner Poewe (13 October 2008). Therapeutics of Parkinson's Disease and Other Movement Disorders. John Wiley & Sons. էջ 417. ISBN 978-0-470-71400-3. Արխիվացված է օրիգինալից 8 September 2017-ին. {{cite book}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
12. ↑ Hoehn MM, Yahr MD (May 1967). «Parkinsonism: onset, progression and mortality». Neurology. 17 (5): 427–42. doi:10.1212/wnl.17.5.427. PMID 6067254.
13. ↑ Rajesh Pahwa; Kelly E. Lyons (25 March 2003). Handbook of Parkinson's Disease (Third ed.). CRC Press. էջ 76. ISBN 978-0-203-91216-4. Արխիվացված է օրիգինալից 8 September 2017-ին. {{cite book}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
14. ↑ ^{14,0 14,1 14,2 14,3 14,4 14,5 14,6} Caballol N, Martí MJ, Tolosa E (September 2007). «Cognitive dysfunction and dementia in Parkinson disease». Movement Disorders. 22 Suppl 17 (Suppl 17): S358–66. doi:10.1002/mds.21677. PMID 18175397.
15. ↑ ^{15,0 15,1 15,2} Parker KL, Lamichhane D, Caetano MS, Narayanan NS (October 2013). «Executive dysfunction in Parkinson's disease and timing deficits». Frontiers in Integrative Neuroscience. 7: 75. doi:10.3389/fnint.2013.00075. PMC 3813949. PMID 24198770.{{cite journal}}: CS1 սպաս․ չպիտակված ազատ DOI (link)
16. ↑ Gomperts SN (April 2016). «Lewy Body Dementias: Dementia With Lewy Bodies and Parkinson Disease Dementia». Continuum (Minneap Minn) (Review). 22 (2 Dementia): 435–63. doi:10.1212/CON.0000000000000309. PMC 5390937. PMID 27042903.
17. ↑ Garcia-Ptacek S, Kramberger MG (September 2016). «Parkinson Disease and Dementia». Journal of Geriatric Psychiatry and Neurology. 29 (5): 261–70. doi:10.1177/0891988716654985. PMID 27502301.
18. ↑ Shergill SS, Walker Z, Le Katona C (October 1998). «A preliminary investigation of laterality in Parkinson's disease and susceptibility to psychosis». Journal of Neurology, Neurosurgery, and Psychiatry. 65 (4): 610–1. doi:10.1136/jnnp.65.4.610. PMC 2170290. PMID 9771806.
19. ↑ Friedman JH (November 2010). «Parkinson's disease psychosis 2010: a review article». Parkinsonism & Related Disorders. 16 (9): 553–60. doi:10.1016/j.parkreldis.2010.05.004. PMID 20538500.
20. ↑ Kim YE, Jeon BS (1 January 2014). «Clinical implication of REM sleep behavior disorder in Parkinson's disease». Journal of Parkinson's Disease. 4 (2): 237–44. doi:10.3233/jpd-130293. PMID 24613864.
21. ↑ ^{21,00 21,01 21,02 21,03 21,04 21,05 21,06 21,07 21,08 21,09} Քաղվածելու սխալ՝ Սխալ <ref> պիտակ՝ «pmid19691125» անվանումով ref-երը տեքստ չեն պարունակում:
22. ↑ Noyce AJ, Bestwick JP, Silveira-Moriyama L, Hawkes CH, Giovannoni G, Lees AJ, Schrag A (December 2012). «Meta-analysis of early nonmotor features and risk factors for Parkinson disease». Annals of Neurology. 72 (6): 893–901. doi:10.1002/ana.23687. PMC 3556649. PMID 23071076.
23. ↑ Chahine LM, Stern MB, Chen-Plotkin A (January 2014). «Blood-based biomarkers for Parkinson's disease». Parkinsonism & Related Disorders. 20 Suppl 1: S99–103. doi:10.1016/S1353-8020(13)70025-7. PMC 4070332. PMID 24262199.
24. ↑ ^{24,0 24,1 24,2} Քաղվածելու սխալ՝ Սխալ <ref> պիտակ՝ «Lancet2015» անվանումով ref-երը տեքստ չեն պարունակում:
25. ↑ ^{25,0 25,1 25,2 25,3 25,4} Lesage S, Brice A (April 2009). «Parkinson's disease: from monogenic forms to genetic susceptibility factors». Human Molecular Genetics. 18 (R1): R48–59. doi:10.1093/hmg/ddp012. PMID 19297401.
26. ↑ ^{26,0 26,1} Kalia LV, Lang AE (August 2015). «Parkinson's disease». Lancet. 386 (9996): 896–912. doi:10.1016/S0140-6736(14)61393-3. PMID 25904081.
27. ↑ ^{27,0 27,1 27,2 27,3} Davie CA (2008). «A review of Parkinson's disease». British Medical Bulletin. 86 (1): 109–27. doi:10.1093/bmb/ldn013. PMID 18398010.
28. ↑ Gan-Or Z, Dion PA, Rouleau GA (2 September 2015). «Genetic perspective on the role of the autophagy-lysosome pathway in Parkinson disease». Autophagy. 11 (9): 1443–57. doi:10.1080/15548627.2015.1067364. PMC 4590678. PMID 26207393.
29. ↑ ^{29,0 29,1} Dickson DV (2007). «Neuropathology of movement disorders». In Tolosa E, Jankovic JJ (eds.). Parkinson's disease and movement disorders. Hagerstown, MD: Lippincott Williams & Wilkins. էջեր 271–83. ISBN 978-0-7817-7881-7.
30. ↑ Jubault T, Brambati SM, Degroot C, Kullmann B, Strafella AP, Lafontaine AL, Chouinard S, Monchi O (December 2009). Gendelman HE (ed.). «Regional brain stem atrophy in idiopathic Parkinson's disease detected by anatomical MRI». PLOS One. 4 (12): e8247. Bibcode:2009PLoSO...4.8247J. doi:10.1371/journal.pone.0008247. PMC 2784293. PMID 20011063.{{cite journal}}: CS1 սպաս․ չպիտակված ազատ DOI (link)
31. ↑ ^{31,0 31,1 31,2 31,3 31,4 31,5} Obeso JA, Rodríguez-Oroz MC, Benitez-Temino B, Blesa FJ, Guridi J, Marin C, Rodriguez M (2008). «Functional organization of the basal ganglia: therapeutic implications for Parkinson's disease». Movement Disorders. 23 Suppl 3 (Suppl 3): S548–59. doi:10.1002/mds.22062. PMID 18781672.
32. ↑ ^{32,00 32,01 32,02 32,03 32,04 32,05 32,06 32,07 32,08 32,09 32,10 32,11 32,12 32,13 32,14 32,15 32,16 32,17 32,18} Obeso JA, Rodriguez-Oroz MC, Goetz CG, Marin C, Kordower JH, Rodriguez M, Hirsch EC, Farrer M, Schapira AH, Halliday G (June 2010). «Missing pieces in the Parkinson's disease puzzle». Nature Medicine. 16 (6): 653–61. doi:10.1038/nm.2165. PMID 20495568.
33. ↑ ^{33,0 33,1 33,2} Schulz-Schaeffer WJ (August 2010). «The synaptic pathology of alpha-synuclein aggregation in dementia with Lewy bodies, Parkinson's disease and Parkinson's disease dementia». Acta Neuropathologica. 120 (2): 131–43. doi:10.1007/s00401-010-0711-0. PMC 2892607. PMID 20563819.
34. ↑ Hirsch EC (December 2009). «Iron transport in Parkinson's disease». Parkinsonism & Related Disorders. 15 Suppl 3 (Suppl 3): S209–11. doi:10.1016/S1353-8020(09)70816-8. PMID 20082992.
35. ↑ ^{35,0 35,1} The National Collaborating Centre for Chronic Conditions, ed. (2006). «Diagnosing Parkinson's Disease». Parkinson's Disease. London: Royal College of Physicians. էջեր 29–47. ISBN 978-1-86016-283-1. Արխիվացված է օրիգինալից 24 September 2010-ին. {{cite book}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
36. ↑ Poewe W, Wenning G (November 2002). «The differential diagnosis of Parkinson's disease». European Journal of Neurology. 9 Suppl 3 (Suppl 3): 23–30. doi:10.1046/j.1468-1331.9.s3.3.x. PMID 12464118.
37. ↑ Gibb WR, Lees AJ (June 1988). «The relevance of the Lewy body to the pathogenesis of idiopathic Parkinson's disease». Journal of Neurology, Neurosurgery, and Psychiatry. 51 (6): 745–52. doi:10.1136/jnnp.51.6.745. PMC 1033142. PMID 2841426.
38. ↑ Rizzo G, Copetti M, Arcuti S, Martino D, Fontana A, Logroscino G (February 2016). «Accuracy of clinical diagnosis of Parkinson disease: A systematic review and meta-analysis». Neurology. 86 (6): 566–76. doi:10.1212/WNL.0000000000002350. PMID 26764028.
39. ↑ Postuma RB, Berg D, Stern M, Poewe W, Olanow CW, Oertel W, Obeso J, Marek K, Litvan I, Lang AE, Halliday G, Goetz CG, Gasser T, Dubois B, Chan P, Bloem BR, Adler CH, Deuschl G (October 2015). «MDS clinical diagnostic criteria for Parkinson's disease». Movement Disorders. 30 (12): 1591–601. doi:10.1002/mds.26424. PMID 26474316.
40. ↑ Berg D, Postuma RB, Adler CH, Bloem BR, Chan P, Dubois B, Gasser T, Goetz CG, Halliday G, Joseph L, Lang AE, Liepelt-Scarfone I, Litvan I, Marek K, Obeso J, Oertel W, Olanow CW, Poewe W, Stern M, Deuschl G (October 2015). «MDS research criteria for prodromal Parkinson's disease». Movement Disorders. 30 (12): 1600–11. doi:10.1002/mds.26431. PMID 26474317.
41. ↑ ^{41,0 41,1 41,2 41,3} Brooks DJ (April 2010). «Imaging approaches to Parkinson disease». Journal of Nuclear Medicine. 51 (4): 596–609. doi:10.2967/jnumed.108.059998. PMID 20351351.
42. ↑ Schwarz ST, Afzal M, Morgan PS, Bajaj N, Gowland PA, Auer DP (2014). «The 'swallow tail' appearance of the healthy nigrosome – a new accurate test of Parkinson's disease: a case-control and retrospective cross-sectional MRI study at 3T». PLOS One. 9 (4): e93814. Bibcode:2014PLoSO...993814S. doi:10.1371/journal.pone.0093814. PMC 3977922. PMID 24710392.{{cite journal}}: CS1 սպաս․ չպիտակված ազատ DOI (link)
43. ↑ Mahlknecht P, Krismer F, Poewe W, Seppi K (April 2017). «Meta-analysis of dorsolateral nigral hyperintensity on magnetic resonance imaging as a marker for Parkinson's disease». Movement Disorders. 32 (4): 619–623. doi:10.1002/mds.26932. PMID 28151553.
44. ↑ ^{44,0 44,1} Քաղվածելու սխալ՝ Սխալ <ref> պիտակ՝ «Neuro2011» անվանումով ref-երը տեքստ չեն պարունակում:
45. ↑ Costa J, Lunet N, Santos C, Santos J, Vaz-Carneiro A (2010). «Caffeine exposure and the risk of Parkinson's disease: a systematic review and meta-analysis of observational studies». Journal of Alzheimer's Disease. 20 Suppl 1 (Suppl 1): S221–38. doi:10.3233/JAD-2010-091525. PMID 20182023.
46. ↑ Ma C, Liu Y, Neumann S, Gao X (2017). «Nicotine from cigarette smoking and diet and Parkinson disease: a review». Translational Neurodegeneration. 6: 18. doi:10.1186/s40035-017-0090-8. PMC 5494127. PMID 28680589.{{cite journal}}: CS1 սպաս․ չպիտակված ազատ DOI (link)
47. ↑ ^{47,0 47,1 47,2 47,3 47,4 47,5 47,6 47,7 47,8} de Lau LM, Breteler MM (June 2006). «Epidemiology of Parkinson's disease». The Lancet. Neurology. 5 (6): 525–35. doi:10.1016/S1474-4422(06)70471-9. PMID 16713924.
48. ↑ Gagne JJ, Power MC (March 2010). «Anti-inflammatory drugs and risk of Parkinson disease: a meta-analysis». Neurology. 74 (12): 995–1002. doi:10.1212/WNL.0b013e3181d5a4a3. PMC 2848103. PMID 20308684.
49. ↑ Connolly BS, Lang AE (23–30 April 2014). «Pharmacological treatment of Parkinson disease: a review». JAMA. 311 (16): 1670–83. doi:10.1001/jama.2014.3654. PMID 24756517.
50. ↑ «The non-motor and non-dopaminergic fratures of PD». Parkinson's Disease : Non-Motor and Non-Dopaminergic Features. Olanow, C. Warren., Stocchi, Fabrizio., Lang, Anthony E. Wiley-Blackwell. 2011. ISBN 978-1405191852. OCLC 743205140.{{cite book}}: CS1 սպաս․ այլ (link)
51. ↑ ^{51,00 51,01 51,02 51,03 51,04 51,05 51,06 51,07 51,08 51,09 51,10 51,11 51,12 51,13 51,14 51,15 51,16 51,17 51,18 51,19 51,20 51,21} The National Collaborating Centre for Chronic Conditions, ed. (2006). «Symptomatic pharmacological therapy in Parkinson's disease». Parkinson's Disease. London: Royal College of Physicians. էջեր 59–100. ISBN 978-1-86016-283-1. Արխիվացված է օրիգինալից 24 September 2010-ին. {{cite book}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
52. ↑ Zhang J, Tan LC (2016). «Revisiting the Medical Management of Parkinson's Disease: Levodopa versus Dopamine Agonist». Current Neuropharmacology. 14 (4): 356–63. doi:10.2174/1570159X14666151208114634. PMC 4876591. PMID 26644151.
53. ↑ ^{53,0 53,1} Pedrosa DJ, Timmermann L (2013). «Review: management of Parkinson's disease». Neuropsychiatric Disease and Treatment. 9: 321–40. doi:10.2147/NDT.S32302. PMC 3592512. PMID 23487540.{{cite journal}}: CS1 սպաս․ չպիտակված ազատ DOI (link)
54. ↑ The National Collaborating Centre for Chronic Conditions, ed. (2006). «Palliative care in Parkinson's disease». Parkinson's Disease. London: Royal College of Physicians. էջեր 147–51. ISBN 978-1-86016-283-1. Արխիվացված է օրիգինալից 24 September 2010-ին. {{cite book}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
55. ↑ Maria, Nord (2017). Levodopa pharmacokinetics -from stomach to brain A study on patients with Parkinson's disease. Linköping: Linköping University Electronic Press. էջ 10. ISBN 9789176855577. OCLC 993068595.
56. ↑ ^{56,0 56,1} Oertel WH (13 March 2017). «Recent advances in treating Parkinson's disease». F1000Research. 6: 260. doi:10.12688/f1000research.10100.1. PMC 5357034. PMID 28357055.{{cite journal}}: CS1 սպաս․ չպիտակված ազատ DOI (link)
57. ↑ Aquino CC, Fox SH (January 2015). «Clinical spectrum of levodopa-induced complications». Movement Disorders. 30 (1): 80–9. doi:10.1002/mds.26125. PMID 25488260.
58. ↑ Goldenberg MM (October 2008). «Medical management of Parkinson's disease». P & T. 33 (10): 590–606. PMC 2730785. PMID 19750042.
59. ↑ Ceravolo R, Frosini D, Rossi C, Bonuccelli U (December 2009). «Impulse control disorders in Parkinson's disease: definition, epidemiology, risk factors, neurobiology and management». Parkinsonism & Related Disorders. 15 Suppl 4 (Suppl 4): S111–5. doi:10.1016/S1353-8020(09)70847-8. PMID 20123548.
60. ↑ Tolosa E, Katzenschlager R (2007). «Pharmacological management of Parkinson's disease». In Tolosa E, Jankovic JJ (eds.). Parkinson's disease and movement disorders. Hagerstwon, MD: Lippincott Williams & Wilkins. էջեր 110–45. ISBN 978-0-7817-7881-7.
61. ↑ ^{61,0 61,1} The National Collaborating Centre for Chronic Conditions, ed. (2006). «Non-motor features of Parkinson's disease». Parkinson's Disease. London: Royal College of Physicians. էջեր 113–33. ISBN 978-1-86016-283-1. Արխիվացված է օրիգինալից 24 September 2010-ին. {{cite book}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
62. ↑ Hasnain M, Vieweg WV, Baron MS, Beatty-Brooks M, Fernandez A, Pandurangi AK (July 2009). «Pharmacological management of psychosis in elderly patients with parkinsonism». The American Journal of Medicine. 122 (7): 614–22. doi:10.1016/j.amjmed.2009.01.025. PMID 19559160.
63. ↑ «Press Announcements - FDA approves first drug to treat hallucinations and delusions associated with Parkinson's disease». www.fda.gov (անգլերեն). Վերցված է 12 October 2018-ին.
64. ↑ ^{64,0 64,1} Elbers RG, Verhoef J, van Wegen EE, Berendse HW, Kwakkel G (October 2015). «Interventions for fatigue in Parkinson's disease». The Cochrane Database of Systematic Reviews (10): CD010925. doi:10.1002/14651858.CD010925.pub2. PMID 26447539.
65. ↑ ^{65,0 65,1 65,2 65,3} The National Collaborating Centre for Chronic Conditions, ed. (2006). «Surgery for Parkinson's disease». Parkinson's Disease. London: Royal College of Physicians. էջեր 101–11. ISBN 978-1-86016-283-1. Արխիվացված է օրիգինալից 24 September 2010-ին. {{cite book}}: Unknown parameter |deadurl= ignored (|url-status= suggested) (օգնություն)
66. ↑ Bronstein JM, Tagliati M, Alterman RL, Lozano AM, Volkmann J, Stefani A, Horak FB, Okun MS, Foote KD, Krack P, Pahwa R, Henderson JM, Hariz MI, Bakay RA, Rezai A, Marks WJ, Moro E, Vitek JL, Weaver FM, Gross RE, DeLong MR (February 2011). «Deep brain stimulation for Parkinson disease: an expert consensus and review of key issues». Archives of Neurology. 68 (2): 165. doi:10.1001/archneurol.2010.260. PMC 4523130. PMID 20937936. {{cite journal}}: Unknown parameter |displayauthors= ignored (|display-authors= suggested) (օգնություն)
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68. ↑ ^{68,0 68,1} Goodwin VA, Richards SH, Taylor RS, Taylor AH, Campbell JL (April 2008). «The effectiveness of exercise interventions for people with Parkinson's disease: a systematic review and meta-analysis». Movement Disorders. 23 (5): 631–40. doi:10.1002/mds.21922. PMID 18181210.
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