Introduction
Parkinsons disease (PD) is a chronic process that may affect the patient for many years and goes through various stages1. Most authors divide the diseases natural history into a premotor or prodromal stage, an early stage, an intermediate stage, and an advanced stage. During the early stage, dopaminergic drugs at low doses provide good control for the whole day. In the intermediate stage, frequent drug adjustments are needed to control the symptoms. The advanced stage occurs when conventional therapy (see below) does not provide the patient with an adequate disease control2.
Although the term advanced PD has been widely used, it is still not very well-defined3. Identifying it clearly is a key issue since we have specific treatments for this stage.
In this review, we try to analyze the advanced PD fundamentals. First of all, we divide the parkinsonian symptoms according to their response to dopaminergic medication, the only available. Both conventional and device-aided treatments only act on dopaminergic symptoms. The failure of the first group marks the onset of advanced PD. This should lead to a switch to device-aided therapies. Unfortunately, this is not always the case. Not infrequently, patients are referred to surgery or infusion therapies after years with poor control on conventional therapy. We describe the works of different groups searching for criteria to identify patients with advanced PD and their limitations, in our opinion. Finally, we propose some keys to improve the identification of this stage. We consider it critical the decline of the functional impact in daily activities with conventional treatment, no matter whether the symptoms are motor, non-motor or both. The patients judgment about this decline is essential to establish the advanced stage. This judgment does not always match with the rating scales used by the neurologist. We also think that the presence of invalidating non-dopaminergic symptoms, such as dementia, on-freezing gait or orthostatic hypotension, should define a stage different from the advanced.
Relevant issues in advanced PD. Treatments and symptomatic response
PD is, in fact, a multiple system degenerative condition. Apart from the substantia negra pars compacta, there is neuronal loss in areas such as the olfactory system, autonomic nerves, peduncle pontine nuclei, locus coeruleus, and raphe nuclei nucleus basalis of Meynert, limbic system or the associative cortex4. This broad degeneration explains many PD symptoms different from tremor, ridigity, and bradykinesia, the classic triad. Any therapy currently available only acts on the pathways modulated by dopamine, either binding the dopaminergic receptor or modifying the subthalamic nucleus hyperactivity, as in the case of surgery.
Over the last years, much attention has been paid to PDs non-motor symptoms5,6. Nevertheless, from a practical point of view, it could be more useful to divide PD symptoms into dopaminergic and non-dopaminergic. The first group responds to dopaminergic drugs, while the second group does not. The Sydney study followed up a cohort of PD patients for 15 years. After this time, non-dopaminergic symptoms become much more disabling than dopaminergic ones for most patients7.
It is very important to learn which symptoms respond to dopaminergic medication. In this way, the neurologist may design the best possible therapeutic strategy, and the patient knows what to expect from the treatment.
In table 1, we have divided the Parkinsonian symptoms into dopaminergic and non-dopaminergic. The most troublesome non-dopaminergic symptoms are on-freezing gait, autonomic disorders, particularly orthostatic hypotension, and cognitive decline, which progresses to dementia in 80% of the cases7,8.
Dopaminergic symptoms | Non-dopaminergic symptoms | ||
---|---|---|---|
Motor | Non-motor | Motor | Non -motor |
Bradykinesia | Pain* | On-state freezing | Dementia |
Rigidity | Depression* | On-state balance disturbance | Psychosis |
Apathy* | |||
Tremor | Anxiety * | On-state dysphagia | Autonomic disfunction |
Urinary urgency* | |||
Lack of concentration |
*These symptoms may also have a non-dopaminergic origin and, therefore, fail to respond to dopaminergic drugs.
Invalidating non-dopaminergic symptoms occur in later stages of PD and dramatically constrain the patients daily activities. Before reaching this step, our current therapeutic capacity, properly applied, may extend the patients functionality for a long period, even when the oral dopaminergic medication starts to fail.
Nowadays, the available PD therapy can be divided into two groups, conventional2 and device-aided treatment9. The first group includes oral drugs and the rotigotine patch. The second one is formed by deep brain stimulation (DBS), continuous apomorphine infusion (APO), and intrajejunal levodopa (DUO).
When only conventional treatment was available, the patient got into a very disabling situation once it failed. The term advanced PD was coined to describe this situation, meaning a terrible and progressive life quality loss until death.
With the advent of device-aided therapies, the picture has completely changed. Several studies10-12 have shown that either DBS or infusion treatments allow for reasonable control of PD symptoms for many years.
Since these device-aided therapies have been available, a reliable way to identify the advanced PD stages onset has become crucial. The neurologist must be aware when the disease control starts to decline with conventional therapy and change to device-aided therapies. Hence, a definition for advanced PD should not be academic but operational, as it should give rise to a shift of therapeutic paradigm.
Another important issue is whether to call advanced stage to the whole period when conventional therapy is not sufficient for a good PD control. The patients management is quite different when dopaminergic symptoms are dominant or when invalidating non-dopaminergic symptoms play the clinical pictures central role.
Due to the negative connotations the term advanced evokes, some authors have proposed different names, for instance, complex stage3.
The search for criteria of advanced PD
The availability of device-aided therapies has prompted the search for operative criteria to define advanced PD. Some pitfalls complicate this search, such as the absence of biomarkers, the disease heterogeneity, the patients personal experience with the disease, the patients employment status or the presence of non-dopaminergic symptoms, sometimes overlooked.
The NAVIGATE-PD study13 interviewed 103 experts from 13 countries about operative criteria to consider device-aided therapies, DBS, APO, and DUO. They concluded that loss in quality of life was the critical point. They proposed that (1) taking levodopa 5 or more times per day, (2) daily troublesome off-time over 1 or 2 h, or (3) severe dyskinesia, with no specific duration, were red flags for possible advanced PD.
A group of Spanish neurologists carried on the CEPA (Consensus about the definition of advanced PD), also called CDEPA (Questionnaire for advanced PD), study14,15. They administered a questionnaire to other 240 Spanish neurologists, with a preferential dedication to PD, about possible advanced stage criteria, applying the Delphi method. The panellists considered as definitive symptoms (1) the need for aid in the daily activities, (2) severe motor fluctuations, (3) severe dysphagia, (4) falls, and (5) dementia. The critical factor to the advanced stage was the disease duration.
Another study, with the Delphi method, involved experts from ten European countries16. The goals were to define clinical indicators for advanced PD, criteria for device-aided therapies, and the patients more suitable for each one of them. The panellists regarded the following clinical characteristics as suggestive of advanced PD. They are divided into three categories and ranked by order of importance.
Motor symptoms: moderate level of troublesome motor fluctuations, at least 2 h of the waking day with off-symptoms, at least 1 h of the day with troublesome dyskinesia, moderate level of dyskinesia, troublesome dysphagia, and daily oral levodopa at least 5 times a day
Non-motor symptoms: mild level of dementia, non-transitory troublesome hallucinations, moderate level of psychosis, non-motor fluctuations, and moderate level of nighttime sleep disturbances
Functional impact: repeated falls despite optimal treatment, need for help with the activities of daily life at least some of the time, inability to perform complex tasks at least some of the time, and moderate impaired mobility.
In the case of patients with advanced PD candidates for device-aided therapies, the clinical characteristics were reduced to:
Motor symptoms: troublesome dyskinesia and off-periods, at least 2 h of off-time, off-period postural instability, dystonia with pain, and freezing of gait during off
Non-motor symptoms: nighttime sleep disturbances, with no other specification
Functional impact: limited activities of daily life.
The OBSERVE-PD study17 tried to correlate these clinical indicators with the neurologists global assessment for advanced PD. It included 2615 patients from 18 countries. The correlation obtained was moderate (K=0.430; 95% IC 0.406-0.473). According to their neurologists, within the patients diagnosed with advanced PD, 66% met the criteria for device-aided therapies. The authors highlighted that not all the patients treated with these therapies had advanced PD. As no more information was available, the authors speculate about the possible indications, such as poor levodopa tolerability, refractory non-motor symptoms, uncontrollable tremor, or functional needs in younger patients. Curiously, they did not consider these three latter situations as advanced PD.
The recent MANAGE-PD study has attempted to rank the criteria to identify advanced PD18. The authors split the patients into three categories. Category 1 encompasses patients adequately controlled on conventional therapy. In Category 2, conventional therapy must be optimized to improve PD control. Finally, in Category 3, the disease control with this medication is not adequate, despite the optimization. To screen the patients, they applied two filters. The first one consists of checking whether the patients have at least one of these criteria: (1) 5 or more daily levodopa doses, (2) daily off-time of at least 2 h, (3) unpredictable motor fluctuations, (4) troublesome dyskinesia, and (5) limitation in at least one activity of daily life. Meeting one or more of these problems should lead to a second filter to determine whether the patients need optimization or device-aided therapy. To validate these criteria, the authors presented ten clinical pictures with the three categories to 20 neurologists.
The importance of the patients judgment for the early identification of the advanced stage
The aim for the early identification of advanced PD and the consequent shift in the therapeutic paradigm is to maintain the best possible patients functionality. To achieve this, the neurologist must apply the appropriate therapy for each stage. The critical point is the change from intermediate to advanced PD since this should mean different disease management.
The recent study Euroinf 2 presents the characteristics of a cohort of 173 patients treated with device-aided therapies. It results quite striking that many patients start with some of these therapies in very advanced stages or even with remarkable axial symptoms19. Sometimes patients are on conventional therapy when they should have been on a device-aided therapy long before. For this reason, it is essential to identify when conventional therapy optimization is no longer the best option.
Most authors agree that the advanced stage commences when conventional treatment optimization does not provide adequate control for the disease2,14,15,18. The term adequate control may be too vague as it depends on the neurologists judgment and, mainly, on the patients perception, demands, and expectations. Although there are some general recommendations, both conventional and device-aided PD therapies should always be personalized. The division of PD into different stages is not an abstraction. It must be adapted to each patients reality, being, therefore, an operational definition.
The need for personalizing each case is well underlined in the aforementioned OBSERVE-PD study17. The correlation between the patients neurologists judgment and the criteria from a group of experts is only moderate. In the validation of the CEPA study15, the authors remark that the neurologist clinical judgment is the gold standard to determine the PD stage.
A point regarded as key in some study is the PD duration14. However, this condition is not always related to the disease stage. In our personal experience, the average disease duration before the onset of device-aided treatments has been eight and a ½ years. Out of them, 30% were on these therapies after 6 years of PD (personal data not published). At the opposite end, there are patients with PD for over 20 years with sufficient autonomy had no dementia20,21. Although after 5 years, half of the patients get motor fluctuations22, a minority remains in good condition with no need for drug adjustments or significant non-motor symptoms after over 10 years23. Hence, we think that the PD duration is not a reliable indicator of the advanced stage.
As mentioned above, the MANAGE-PD study18 considers three red flags for possible advanced PD, daily off-state over 2 h, troublesome dyskinesia and 5 or more daily levodopa doses. Many levodopa doses mean several adjustments, but patients may have a reasonable control on 5 daily levodopa dose. If these adjustments do not avoid troublesome dyskinesia, the patient has bad PD control and advanced PD. The issue of the off-state is not so straight. Although a daily 2-h off-state is a red flag in PD, we must consider as well how the patient experiences this problem and how it affects their functional situation. Patients with demanding jobs may feel significantly limiting an off-state of 1 h a day. In contrast, more aged patients with no job responsibilities may tolerate better off-periods even over 2 hours. Hence, the patients judgment may be more valuable than a score on a rating scale when both do not match.
Besides, we have to take into account the off-period duration and intensity, and not only motor but also non-motor symptoms. Pain, anxiety, apathy, depression, or lack of concentration may be very disabling during the off-state with or without motor symptoms. At our site, we have seen patients with episodes of severe off-state pain lasting < 1 h, only responsive to infusion treatments. We also think that we should include within the advanced stage cases with disabling tremor, even if the other Parkinsonian symptoms do appropriately respond to conventional medication. Finally, we must not forget the patients with faltering on-state, even without important fluctuations. As this is mainly due to gastroparesis, a treatment skipping the oral route is usually effective.
A stage beyond the advanced stage
Nowadays, the advanced PD stage encompasses the whole period from the onset of the conventional treatment failure to the disabling non-dopaminergic symptoms dominance. However, this is not a homogeneous period with similar management. Many patients with device-aided treatments carry on an independent life. This does not happen with disabling non-dopaminergic symptoms.
Some studies searching for advanced PD criteria give the same defining value for advanced PD to dopaminergic symptoms refractory to conventional treatment and disabling non-dopaminergic symptoms. Both the CEPA study14,15 and the 2018 consensus study16 include as advanced PD criteria dementia, falls or on-state dysphagia, non-responsive to dopaminergic medication, along with dopaminergic symptoms, such as off-time pain, depression, and dyskinesia, all of them responsive to device-aided therapies. The patients functionality is different enough to consider these situations as two distinct stages of PD.
The presence of disabling non-dopaminergic symptoms is not a contraindication for device-aided therapies but diminish their efficiency dramatically. Only infusion treatments, with low doses and close follow-up, are to try.
We suggest keeping the name advanced stage for the situation in which dopaminergic symptoms dominate the clinical picture but do not respond sufficiently to conventional treatment. Conversely, we consider a new PD stage for the situation in which disabling non-dopaminergic symptoms are dominant. In this case, the patients functional state is severely diminished, and the therapeutic options significantly reduced. We propose calling this phase post-advanced stage. Something in this respect has been previously suggested15. In this study, the authors divide the advanced stage into advanced and late. Their criteria are the response to conventional therapy, partial in the first case, absent in the second. They do not mention refractory non-dopaminergic symptoms.
Table 2 shows the keys to advanced PD.
Conventional therapy does not provide adequate Parkinsons disease control |
The term adequate control encompasses both motor and non-motor symptoms |
The term adequate control must be personalized. It is very important the patients perception of the treatments functional impact |
The identification of this stage should involve a shift to device-aided therapy |
The earlier we identify this stage, the earlier we will be able to improve the patients quality of life |
Device-aided therapy only alleviates dopaminergic symptoms, either motor or non-motor |
The term advanced Parkinsons disease should be restricted to the situation in which dopaminergic symptoms do not respond to conventional drugs, and non-dopaminergic symptoms are not disabling |
If non-dopaminergic symptoms are disabling, we should speak of post-advanced stage |
Conclusions
The key to advanced PDs definition stems from the lack of disease adequate control on conventional therapy. The early identification of this phase allows switching to device-aided therapies, which alleviate dopaminergic symptoms, either motor or non-motor. To determine advanced PD, a key point is the worsening of the patients functional state. We must consider the off-period duration and its intensity, faltering on without fluctuations or disabling non-motor symptoms. The patients judgment about their situation is essential to assess this stage. Sometimes it does not match with the rating scales.
The patients functionality in the advanced stage will depend on the presence of disabling non-dopaminergic symptoms. These symptoms usually appear in a later phase. We propose, therefore, differentiating two situations within what is called now advanced state. We should restrict this name advanced stage to the phase in which dopaminergic symptoms are dominant and respond to device-aided therapies. If disabling non-dopaminergic symptoms are present, we should speak of post-advanced stage.
Figure 1 shows a picture of the EP natural history, including the post-advanced stage.