Skip to main content
Erschienen in:

Open Access 04.01.2020 | Review

Pathophysiologic Approach to Pain Therapy for Complex Pain Entities: A Narrative Review

verfasst von: Martina Rekatsina, Antonella Paladini, Alba Piroli, Panagiotis Zis, Joseph V. Pergolizzi, Giustino Varrassi

Erschienen in: Pain and Therapy | Ausgabe 1/2020

Abstract

Pain management is challenging for both clinicians and patients. In fact, pain patients are frequently undertreated or even completely untreated. Optimal treatment is based on targeting the underlying mechanisms of pain and tailoring the management modality for each patient using a personalized approach. This narrative review deals with pain conditions that have a complex underlying mechanism and need an individualized and frequently multifactorial approach to pain management. The research is based on previously conducted studies, and does not contain any studies with human participants or animals performed by any of the authors. This is not an exhaustive review of the current evidence. However, it provides the clinician with a perspective on pain therapy targeting the underlying pain mechanism(s). When dealing with complex pain conditions, the prudent physician benefits from having a deep knowledge of various underlying pain mechanisms in order to provide a plan for optimal pharmacological pain relief to patients.
Hinweise
The original version of this article was revised to correct the Figure 1 caption.

Enhanced Digital Features

To view enhanced digital features for this article go to https://​doi.​org/​10.​6084/​m9.​figshare.​11341664.
A correction to this article is available online at https://​doi.​org/​10.​1007/​s40122-020-00152-w.
Key Summary Points
The pathophysiology of pain may be very different from patient to patient.
Personalized medicine is the keystone of efficacious and safe therapy. This is especially true in some difficult pain syndromes.
The authors try to analyze the relevant literature in order to suggest the best therapy in complex patients.

Introduction

According to recent data, pain occurs in all demographics of the general population, with higher prevalence in some clusters such as the elderly [1]. Pain can be either acute or chronic; the latter refers to pain that persists past the normal healing time, and usually lasts or recurs for more than 3–6 months [2]. Pain may be nociceptive (somatic and visceral), neuropathic, nociplastic, or mixed [3]. Nociplastic is a new term, introduced by the International Association for the Study of Pain (IASP), and describes pain of unknown origin that arises from altered nociception, despite no clear evidence of actual or threatened tissue damage causing the activation of peripheral nociceptors or evidence of disease or lesion of the somatosensory system causing the pain [3]. Before an effective pain treatment plan can be established, recognizing the origin of the symptoms is crucial. Inflammation is the most frequent cause, but there is also pain of mechanistic origin, such as chronic osteoarthritis of the knee where the cartilage has eroded. However, the source of pain can also be obscured, which occurs in fibromyalgia, and is classified as chronic primary pain according to the IASP classification of pain for the International Classification of Diseases (ICD) 11 [4]. The classification system of chronic pain has evolved. The main overarching categories of chronic pain are primary and secondary pain. Secondary chronic pain is further divided into six categories: cancer-related pain, postsurgical or posttraumatic pain, secondary headache or orofacial pain, secondary visceral pain, and secondary musculoskeletal pain [5].

Participation of the Central Nervous System

Regardless of the origin of the pain or its duration, the central nervous system (CNS) is always involved. The CNS detects and interprets a wide range of thermal and mechanical stimuli as well as environmental and endogenous chemical irritants. Intense stimuli provoke acute pain, but recurrent stimuli, should protective reflexes fail, can lead to chronic pain through plasticity of the peripheral nervous system (PNS) and CNS as well as signal enhancement [6].

Personalized Management of Pain

Personalized management is a very important approach to pain management. In 2016, the National Health Service of England (NHS England) published its vision on personalized medicine [7]. According, they noted: “Personalized medicine is a move away from a ‘one size fits all’ approach to the treatment and care of patients with a particular condition, to one which uses new approaches to better manage patients’ health and targets therapies to achieve the best outcomes in the management of a patient’s disease or predisposition to disease” [7]. However, the concept of personalized medicine is not new. Clinicians throughout the history of medicine have been working on tailoring care based on patients’ individual needs. Specifically, in 2014, Hui and Bruera published their article on a personalized approach for managing cancer pain [8]. They stated: “Impeccable management of pain begins with appropriate assessment, which includes documentation of pain characteristics, determination of pain mechanism, identification of modulating factors, clarification of a personalized pain goal, and regular reassessments over time.” According to the authors, the first step in the successful management of pain is the identification of its likely sources [8].

Suggestions for Developing Strategies Against Pain

According to the previous statements, it is well understood that the management of pain needs to target all of the different pathophysiological mechanisms that may cause pain. Several pain specialists have also stressed this [9]. Throughout the years, an initiative called CHANGE PAIN has evolved. The major objectives of the CHANGE PAIN International Advisory Board were to enhance the understanding of chronic pain and to develop strategies for improving pain management [9]. CHANGE PAIN conducted a survey which, among others, pointed out a basic lack of knowledge among physicians regarding the differences between nociceptive and neuropathic pain [10]. Moreover, Varrassi et al. stated: “Increasing physicians’ knowledge of the pharmacological options available to manage these different pain mechanisms offers the promise of better treatment decisions and more widespread adoption of a multimechanistic approach” [11]. In their opinion, managing pain could include the use of two agents from different medication classes or one agent acting through different mechanisms. When physicians do not address the mechanisms responsible for pain, there is an increased risk of initiating a “vicious circle,” where both doses and their side effects progressively increase [10]. A cross-sectional study in Europe revealed that medical schools still provide little education regarding pain, which could be responsible for the continued high prevalence of pain [12]. A close examination of the pathophysiological mechanisms of pain would include all of the cells of the CNS, and would offer new perspectives on pain control [13, 14] and open the possibility for the development of new pharmacological substances [15, 16] or lead to the novel use of existing agents for different types of pain.
It is also important for clinicians to become aware of the multifactorial nature of chronic pain in order to make pharmacological decisions based on the underlying mechanistic factors of the pain [15]. Therefore, it is crucial that clinicians who treat patients with chronic pain are knowledgeable regarding current theories of the development of chronic pain, and understand the differences between nociceptive and neuropathic pain and how they develop. An understanding of peripheral sensitization and the local release of inflammatory mediators that attract immune cells after injury is crucial, as well as an understanding of the process of central sensitization. The latter is the result of persistent transmission of pain signals from the periphery to the spinal cord [17].

Different Mechanisms of Pain and Central Sensitization

A number of different mechanisms are involved in central sensitization, which involves the peripheral input of a nociceptive stimulus to a dorsal horn synapse and the concomitant release of substance P and glutamate into the synaptic cleft. These include presynaptic N-methyl d-aspartate (NMDA) receptors and a-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) receptors, and the signal is transmitted to the thalamus. There, microglial cells release inflammatory modulators, after activation of the toll-like receptor 4 (TLR4). The role of the NMDA receptors is crucial, because their prolonged activation after repetitive stimuli leads to their increasing density, which in turn enhances the signal to the thalamus [18, 19]. Allodynia, hyperalgesia, spontaneous pain, and secondary hyperalgesia indicate central sensitization. Another characteristic of central sensitization is the wind-up phenomenon, where the same unchanged stimulus causes increasingly intense sensations of pain [20]. Wind-up can be prevented up to a point by ketamine, an NMDA antagonist [21]. However, ketamine cannot fully reverse central sensitization [22, 23]. Another cause of central sensitization could be a defect of the descending inhibitory control (DIC) system, which is present in various pain conditions [24, 25] Therefore, knowledge of the multiple causative mechanisms of pain and pain syndromes, along with their molecular components, is fundamental in creating proper treatment plans, especially in complex patients [11, 17, 26].

Objectives

Because a very important task for clinicians is the effective management of pain in their patients by targeting the causative triggering mechanisms, this review aims to bring together published work that has shed light on the above mechanisms and, at the same time, offers insight into current or promising pain-relieving pharmacological treatments.

Methods

We searched relevant articles within the PubMed, Scopus, and Cochrane databases, considering publications up to May 2019. All searches used the following research key words: (pathophysiology OR underlying mechanism OR cause) AND (pain OR painful OR pain syndromes) AND (pharmacological therapy OR pharmacological approach OR pharmacological treatment OR pharmacological strategy). The primary search was supplemented with a secondary search using the bibliographies of the articles retrieved. Only full-length original articles were accepted, and the search was limited to English-language publications. Because knowledge regarding pain mechanisms is evolving so rapidly, the primary search focused on articles within the last 15 years. All retrieved articles were reviewed by title, abstract, and the article itself when its content was not clearly indicated by the title and abstract. The inclusion criteria were as follows: (1) the article referred to acute or chronic pain, and a specific pathophysiological mechanism was suggested in the article, and (2) the authors suggested a treatment plan or a medication therapy that would target the underlying mechanism. We tried to focus on the main complex categories of pain, such as neuropathic pain, and special populations such as the elderly. The perspective suggested here can be used by clinicians to guide their efforts in dealing with pain experienced by their patients. This article is based on previously conducted studies and does not contain any studies with human participants or animals performed by any of the authors.

Results

The article selection process is shown in Fig. 1. According to the new classifications of chronic pain [5], we attempted to cover as many clinical conditions as possible, indicating a possible representative for each category. As a result, we elaborated on the pathophysiological mechanisms and the proposed pharmacological approach for the following: chronic neuropathic pain, chronic primary pain and more specifically fibromyalgia, chronic visceral pain, central post-stroke pain, pain in complex regional pain syndrome, and low back pain. Finally, a group of patients that is continually growing and, in our opinion, needs particular attention is the elderly population, who were included in our review.

Pathophysiological Approach and Pharmacological Pain Management

Chronic Neuropathic Pain

Mechanism of Pain

Neuropathic pain can have multiple causes and be peripheral, central, or mixed. It arises as the direct result of a disease or lesion of the central and/or peripheral somatosensory nervous system, and it should be distinguished from nociceptive pain and treated differently [27]. These lesions produce and maintain spontaneous ectopic activity by way of voltage-gated neuronal sodium channels and transient receptor potential channels, which manifests as thermal hyperalgesia and pain attacks [27]. These channels can be modulated with medicines such as carbamazepine, lidocaine, and capsaicin, with resulting pain relief [28]. An important aspect of neuropathic pain is central sensitization, which manifests as intensified spontaneous pain, mechanical allodynia, or hyperalgesia, all of which can be modulated with medicines including gabapentin, pregabalin, and opioids, with resulting pain relief [28]. Moreover, in healthy individuals there is a descending system in the CNS that can modulate nociceptive impulse transmission [27]. By inhibiting the reuptake of the neurotransmitters needed for this path, antidepressants can lead to pain relief [28]. Treatment of this type of pain is extremely important, considering its influence on patients’ quality of life [29].

Treatment Plan

Therefore, the suggested pharmacotherapy for neuropathic pain is as follows:
(a)
Tricyclic antidepressants (TCAs) and selective serotonin-norepinephrine reuptake inhibitors (SNRIs) such as duloxetine, which act through the potentiation of the descending nociceptive inhibitory pathways by presynaptic inhibition of the reuptake of serotonin and norepinephrine, two monoaminergic neurotransmitters. TCAs also block voltage-dependent sodium channels and have sympatholytic properties, and should be given in an individually titrated dose [30]. Both are considered first-line medications. The last update of the relevant Cochrane review also supports this, pinpointing diabetic neuropathy and postherpetic neuralgia as benefiting the most from this category of medication [31].
 
(b)
Gabapentinoids, which act on the α2-d-subunit and inhibit the activation of calcium influx [30], and are recommended as a first-line medication. The evidence suggests that although they are not expected to benefit more than half of the patients, this category of medications should always be considered [32].
 
(c)
Weak (e.g., tramadol) or strong opioids (e.g., morphine, buprenorphine) for resistant pain. Opioids act as agonists primarily at the µ-opioid receptors, which are located in both the CNS and PNS. Tramadol exerts an additional effect on the descending pain-suppressing system by inhibiting the reuptake of norepinephrine and serotonin [30]. The use of opioids, although controversial, is being reserved for occasions when either more rapid relief is necessary or when pain is significantly resistant, leaving them as a second-line recommendation. The 2013 Cochrane review regarding opioids for neuropathic pain does not conclude that opioids are better than placebo for long-term use and highlights their multiple side effects [33].
 
(d)
µ-Opioid receptor agonist norepinephrine reuptake inhibitors such as tapentadol should also be used wisely, like high-potency opioids [30].
 
(e)
Topical treatments such as lidocaine patches, which block sodium channels, or the capsaicin 8% patch, which leads to reversible degeneration of nociceptive afferent fibers in the skin, are being recommended as a second-line option for the treatment of painful peripheral neuropathy [30]. However, the relevant Cochrane remains inconclusive regarding the efficacy, awaiting for newer evidence [34].
 
Vranken [35] proposed several other treatments for neuropathic pain for patients who cannot tolerate the side effects of the first-line pharmacological treatment. For example, the muscle relaxant baclofen exerts its analgesic effect via an agonistic effect on the inhibitory GABAβ receptors, while mexiletine, an oral analog of lidocaine, can be used if a trial lidocaine infusion has been effective for the patient [35]. Moreover, clonidine, as an α2-adrenoceptor agonist, can be used in neuropathic pain [35], as well as ketamine [35]. Transdermal buprenorphine has also been used successfully for central neuropathic pain [36]. Palmitoylethanolamide (PEA) has been recommended for chronic neuropathic pain, as well [15, 16].
For the effective management of neuropathic pain a combination medication therapy might be of utmost importance. However, a Cochrane systematic review did not succeed to suggest the value of any specific combination [37].

Chronic Primary Pain (Fibromyalgia)

Mechanism of Pain

It has been suggested that fibromyalgia is the result of two different mechanisms affecting the CNS: on the one hand, hyperreactivity of the CNS, and on the other hand the decreased capacity of the CNS to modulate pain [38]. A probable cause for the latter could be the decreased activity of the serotonergic/noradrenergic pathways [39]. Hauser et al. suggested that “the cerebrospinal fluid levels of the main noradrenaline metabolites, as well as the serum levels of serotonin, tryptophan, and 5-hydroxyindoleacetic acid are lower in fibromyalgia patients, whereas those of pronociceptive neurotransmitters such as glutamate, nerve growth factor, and substance P are increased” [39]. Emerging evidence also shows that glial cells may play a role in maintaining central sensitization by producing various chemokines and cytokines [40]. PNS abnormalities seem to have their own role in the pathogenesis as well. Fibromyalgia patients have functional impairment of small nerve fibers and reduced small fiber density [41]. It has been suggested that certain interventions to limit peripheral input might improve pain, allodynia, and hyperalgesia. Moreover, it is important to note that other sources of comorbid pain can increase central sensitization; therefore, comorbidities should be properly treated [42]. Finally, Calandre et al. mention other factors that may lead to fibromyalgia, including polymorphisms in the catechol-O-methyltransferase (COMT) gene or alterations in the hypothalamic–pituitary–adrenal axis, abnormal autonomic nervous system functioning, disruptions of sleep architecture, and dysfunctional dopaminergic neurotransmission. In addition, certain psychological or physical factors may play a role in fibromyalgia [43]. This topic was recently reviewed, and a new hypothesis has been proposed [44].

Treatment Plan

The main categories proposed are as follows: antidepressants, antipsychotic medications, dopaminergic agonists, anticonvulsants, muscle relaxants, cannabinoids, opioids, melatonin and its analogs, NMDA antagonists, and 5-HT3 receptor antagonists such as modafinil and armodafinil (non-amphetamine stimulants that release dopamine and noradrenaline in the CNS and histamine in the hypothalamus) [45].
Among the above-mentioned agents, pregabalin and gabapentin are currently mainly used to treat chronic pain, improve sleep, and enhance health-related quality of life, and the TCA amitriptyline is widely used as first-line treatment for fibromyalgia [46]. It is important to note that the combinations of amitriptyline plus fluoxetine or pregabalin plus duloxetine have been shown to be more effective than either medicine alone [46], and tramadol administered alone or together with paracetamol has been shown to reduce pain by 30% [45].
The most recent recommendations from the European League Against Rheumatism (EULAR) regarding pharmacological therapy for pain in fibromyalgia included duloxetine, pregabalin, and tramadol (with or without paracetamol) for severe pain. When severe sleep problems were also present, low-dose amitriptyline was suggested, as were cyclobenzaprine or pregabalin to be taken at night [47].
However, many patients do not respond to the above treatments, indicating the need for developing new medicines or reformulating older ones in order to target the pathogenesis of fibromyalgia [45]. It is worth mentioning that some new potential agents are being investigated, including IMC-1 (a fixed-dose combination of the anti-herpes virus nucleoside analog famciclovir and the anti-herpes virus active COX-2 inhibitor celecoxib), neurotrophins, mast cell stabilizers, and mirogabalin (which is more specific for calcium channels than pregabalin or gabapentin) [45]. An interesting study from Del Giorno et al. [48] evaluated the therapeutic efficacy of duloxetine combined with pregabalin in patients suffering from fibromyalgia, and the possible added benefit of the lipid-signaling molecule PEA. The combination of duloxetine and pregabalin had previously been suggested [49], and was well documented to exert anti-inflammatory, analgesic, and pain-relieving effects in both preclinical and clinical studies. The authors concluded that adding PEA to an initial combination therapy of pregabalin plus duloxetine improved the outcome of fibromyalgia, and that when an additional medication is needed, PEA could serve as an optimal option [48]. Non-pharmacological treatments for fibromyalgia may also be appropriate, for example postural counseling [50].

Chronic Visceral Pain

Mechanism of Pain

Identifying the specific underlying causes of chronic visceral pain is very important for its proper management. The inflammatory process begins in the gastrointestinal (GI) tract and is then transmitted through various receptors and ion channels to the CNS. Therefore, targeting those portions of the GI tract could be ideal in terms of reducing side effects and providing novel opportunities for the pharmacological treatment of chronic visceral pain. Moreover, in chronic visceral pain, the aforementioned receptors and ion channels have undergone pathological changes, and as a result there is enhanced nociceptive signaling [51].
A significant correlation has been demonstrated between serotonin polymorphisms and chronic visceral pain severity. For example, in patients with irritable bowel syndrome, it was observed that plasma serotonin concentrations were reduced in patients with constipation but elevated in those with diarrhea [52]. Therefore, there has been considerable interest in these receptors as possible therapeutic targets [52]. A possible role of genetic polymorphisms coding for anti-inflammatory and proinflammatory interleukins (IL), α-2 adrenergic receptors, and serotonin and cholecystokinin (CCK) receptors has also been suggested [52].

Treatment Plan

An effective treatment plan might target pronociceptive mechanisms by blocking sodium channels with lidocaine, potassium channels with retigabine, or voltage-gated calcium channels with gabapentin or pregabalin. Protease-activated receptor 2 blockers could also be useful, as well as histamine receptor blockers such as ebastine. Agonists against serotonin, tachykinin, or purine, and glutamate receptor antagonists such as ketamine have also been shown to reduce visceromotor pain. Additionally, recent evidence highlights increases in antinociceptive mechanisms in models of chronic visceral pain, which present novel targets for pharmacological treatment of this condition. These mechanisms are up-regulated during inflammatory or chronic visceral hypersensitivity states. Potential targets include the receptors for oxytocin, GABA, cannabinoids, opioids, and TRPM8, along with protease-activated receptor 4 (PAR4) and guanylate cyclase-C receptors [51]. The physician should be aware of all of the different mechanisms that may apply in each individual case and which agents may be effective when pharmacotherapy must switch from an agonist to an antagonist (e.g., against serotonin receptors), which is necessary for individualized treatment. The clinician has several options in the armamentarium against chronic visceral pain, including laxatives, antidiarrheals, antispasmodics (mebeverine hydrochloride, hyoscine butylbromide, and peppermint oil), probiotics, fecal microbiota transplantation, and serotonin receptor agonists (tegaserod, prucalopride, renzapride) and antagonists (alosetron, ramosetron). In addition, anti-inflammatory therapies such as rifaximin, corticosteroids, mast cell stabilizers, and mesalazine may be used [52].

Central Post-Stroke Pain

Mechanism of Pain

Central post-stroke pain is caused by CNS lesions. Although the pathogenesis of central post-stroke pain remains unknown, the suggested underlying causes include hyperexcitation of the damaged sensory pathways, damage to the central inhibitory pathways, or a combination of the two. It is likely that various neurotransmitters are involved in this process [53]. Initially, the thalamus was believed to be the cause of pain by failing in its inhibitory role. However, there is also evidence suggesting that various cortical structures such as the anterior cingulate cortex are involved, leading to allodynia. The pathways that mediate cold sensation or other impairments in the spinothalamic paths could also account for the generation of the pain [53].

Treatment Plan

For pharmacological treatment, the first-line medication is the adrenergic antidepressant agent amitriptyline. However, its effect is frequently incomplete, and many patients do not tolerate high doses. Lamotrigine, an antiepileptic, was also found to be effective and can be used as an alternative or add-on therapy. GABAergic medicines with potential calcium channel-blocking effects, such as gabapentin or pregabalin, have also recently emerged as a potentially useful therapy. Fluvoxamine and mexiletine may be used adjunctively in some patients [53]. Transdermal buprenorphine may also be useful in some cases [36].

Pain in Complex Regional Pain Syndrome

Mechanism of Pain

Complex regional pain syndrome (CRPS) is frequently seen as a post-traumatic disorder characterized by a non-dermatomal, severe, continuous pain in the affected limb and is associated with sensory, motor, vasomotor, sudomotor, and trophic disturbances. CRPS is usually precipitated by trauma or surgery [54]. The pathophysiology of CRPS is multifactorial, with recent studies suggesting it may be an exaggerated inflammatory response to trauma or surgery. Both peripheral and central mechanisms are thought to play a role in the initiation and maintenance of CRPS [55, 56]. Recent studies focusing on inflammatory processes in CRPS found higher levels of proinflammatory cytokines in blister fluid in the form of tumor necrosis factor alpha (TNFα) of the affected extremity compared with the unaffected extremity, and this could suggest a role for local inflammatory processes in CRPS [56]. Elevated levels of proinflammatory cytokines have also been found in the serum, plasma, and cerebrospinal fluid of patients with CRPS [57], which may be involved in peripheral nociceptor activation and sensitization [58].
Another explanation for the pathogenic mechanisms of CRPS is neurogenic inflammation mediated by calcitonin gene-related peptide (CGRP) and substance P. This is thought to be an underlying mechanism for such symptoms as edema, vasodilation, and increased sweating [55].
CRPS is also described as an autoantibody-mediated autoimmune disease, where immunoglobulin G mediates inflammation [59]. According to Bharwani et al., deep-tissue microvascular ischemia–reperfusion injury along with various human leukocyte antigen (HLA) associations and cortical reorganization could play an important role in CRPS and pain [54]. It has also been proposed that CRPS is a small fiber neuropathy, as it has many similarities to other generalized small fiber-predominant polyneuropathies [60].

Treatment Plan

Accordingly, as additives to physiotherapy and invasive treatments, the choice of medication is based on the mechanism deemed most prominent in each specific CRPS case/patient [54]. The different medications that can be used include free radical scavengers, immunomodulating medications (bisphosphonates, glucocorticoids, TNFα antagonists, thalidomide), and immunoglobulin to fight against inflammation. Achieving a change in pain perception is an important aspect of care. Gabapentin has been shown to lead to a reduction in pain symptoms in CRPS and may be used in the treatment of neuropathic pain. If intractable pain persists, treatment with intravenous administration of low-dose ketamine in long-standing cases may be considered. Should the patient suffer from so-called cold CRPS caused by vasomotor changes, a calcium channel blocker, α-sympathetic blocker, or phosphodiesterase-5 (PDE5) inhibitor can be considered. Finally, muscle relaxants or antispasmodics offer another approach, as intrathecal baclofen has been shown to have a positive effect on dystonia in patients with CRPS [54].

Low Back Pain (LBP)

Mechanism of Pain

Low back pain (LBP) encompasses three distinct sources: axial lumbosacral, radicular, and referred pain. For that reason, there are many different pathophysiological mechanisms in play [61]. Despite the fact that LBP has been the subject of much study and clinical effort, no clear-cut effective treatment has yet emerged. Continuing efforts should be made to understand the pathology, diagnosis, and method of treatment for LBP [62]. The source(s) of pain should be identified and specifically targeted. The most common causes of LBP are myofascial pain [63], facet-mediated pain due to either degeneration [64] or OA [61], discogenic pain [65, 66, 67], failed back surgery syndrome (FBSS) [68, 69], spinal stenosis pain [70], and sacroiliac joint pain [71].

Treatment Plan

Treatment in LBP should be specific and should target the main cause of pain, which is usually inflammation. Paracetamol and nonsteroidal anti-inflammatory drugs (NSΑΙDs) have been shown to provide short-term pain relief [72]. While tramadol has shown limited analgesia, with mild functional improvement for chronic LBP, strong opioids may offer significant analgesia and improved function at 3 and 6 months, as shown in selected randomized trials [73]. Recent guidelines from the National Institute for Health and Care Excellence (NICE) for the treatment of low back pain recommend exercise as a key part of any treatment program, and a “cautious, stepwise approach” to pharmacological therapy [74]. The use of TCAs has shown beneficial effects for LBP treatment by exerting analgesia primarily through serotonin and norepinephrine reuptake inhibition, sodium channel blockade, and NMDA antagonism [72]. Additionally, serotonin norepinephrine reuptake inhibitors (SNRIs) offer another pharmacological treatment for chronic LBP, as they inhibit serotonin and norepinephrine reuptake, which is important for descending pain inhibition [72]. Lastly, pharmacological treatment of LBP may include antiepileptics. While gabapentin has shown analgesic efficacy for chronic LBP with radiculopathy, only topiramate has been studied for chronic axial LBP with evidence of effective analgesia and improved quality of life [75].
At this point, it is worth mentioning that some authors have suggested the addition of PEA to a multimodal therapeutic regimen for the treatment of FBSS in treatment-resistant patients [69]. In that study, treatment with PEA was found to significantly decrease pain intensity. PEA is a mechanism-modifying approach in pain management and was shown in earlier studies to exert anti-inflammatory, analgesic, and neuroprotective action [76] through inhibition of mast cell and microglial activation [13, 77].

Pain in the Elderly

Mechanism of Pain

The world's population is aging, and the elderly endure a great variety of pain due to the physiological changes associated with growing old [13, 14]. In the elderly, peripheral nerves display functional, structural, and biochemical changes mainly involving the Aδ fibers. Persistent neuroinflammation is promoted in older individuals by mast cells and microglia, which become more sensitive to noxious stimuli and less capable of regulation by homeostatic endogenous systems (primed microglia) (Fig. 2) [15]. Another characteristic of aging is an overall increase in central sensitization, due to limited descending inhibitory capacity and altered responses to heat pain in the middle insular cortex and primary somatosensory cortex. In general, the pain threshold increases with age, while the threshold for pain tolerance remains unchanged or decreases [15].

Treatment Plan

When treating pain in the elderly, physicians should never forget the physiological modifications (Table 1) significantly affecting pharmacological consequences of drug administration, including the potential side effects. Nausea and vomiting, bowel dysfunction, and somnolence are the main treatment-limiting symptoms in seniors [78]. Positive results in the treatment of pain for the aged can only be achieved by using innovative therapeutic strategies based on a knowledge of the patient’s real needs and in consideration of age-related changes in pain perception, pain processing, and the immune system which may modify responsiveness to painful stimuli [13, 14, 79]. As stated previously, microglia, mast cells, and astrocytes are very important to pain perception, so they can serve as targets for the control of persistent pain. Because PEA has a high ratio of efficacy to risk, it may be an excellent co-treatment for the burgeoning elderly population with chronic pain [15].
Table 1
Physiological modifications in the elderly, and their influence on pharmacological therapy
Parameter modification
Pharmacological effect
Example medications affected
Increased fat mass
Reduced lean mass
Reduced body water
Increased duration of lipophilic drugs effects
Increased plasma concentration of water-soluble drugs
Local anesthetics
Opioids
Reduced serum albumin
Increased free-medication availability
Anticonvulsants
NSAIDs
Reduced hepatic and renal clearance
Increased medicine half-life and increased dose-related side effects from medications that undergo first-pass metabolism
Local anesthetics
Opioids
Reduced cytochrome P-450 function
Possible toxic medicine-medicine interactions
Local anesthetics
Opioids
SNRIs
SSRIs
Increased reactivity of glia [74]
Increased need for anti-inflammatory medications
Corticosteroids
NSAIDs
SSRIs selective serotonin reuptake inhibitors
Patients with cognitive decline constitute an important geriatric subpopulation [80]. For instance, in Alzheimer’s disease (AD), neuropathological changes selectively impact the affective-motivational component of pain (medial pathway) more than the sensory-discriminative dimension (lateral pathway), which impairs the patient’s ability to assess a painful experience. Combined with an unchanged pain threshold and a higher tolerance of painful stimuli typical of the elderly, AD patients have been observed to have a higher tolerance for intense pain that alters their experience of chronic pain [80]. However, in other studies these changes were inconsequential, indicating no selective reduction in the emotional aspects of the pain experience in these patients [81]. Another key point for AD patients is their altered response to analgesic medicines, in that they have little to no placebo effect, requiring a higher dose of pain medication to obtain an analgesic effect [82]. Moreover, changes in the blood–brain barrier in AD patients can influence the effect of centrally acting pain medications such as opioids. For example, pain perception in vascular dementia may increase because of white matter lesions in pathways ascending to the thalamus, such as the spinothalamic tract, while pain perception in Lewy body dementia may be altered due to brain atrophy and damage caused by Lewy bodies [80].
Of paramount importance is that both underreported or underestimated pain and comorbidities and polypharmacy are formidable barriers to effective pain control in the elderly. Avoiding potentially dangerous medications such as neuroleptics and benzodiazepines as pain relievers, and initiating treatment with non-opioid analgesics or gradual titration of pain regimens are crucial. SNRIs can be considered as adjuvants and/or as an alternative to NSAIDs and opioids [80].
One additional obstacle in the elderly is compliance to therapy. This may be reduced when fixed-dose combinations of medicines are prescribed [83]. Pain is always multifactorial. Hence, considering a multimodal approach to therapy is essential, especially in complex patients with many comorbid conditions.

Limitations

This is not an exhaustive review of the current evidence. However, it provides the clinician with a perspective on pain therapy targeting the underlying pain mechanism(s) in complex pain syndromes. A further limiting aspect is that the review focuses on just a few complex pain syndromes. Further reviews on other pain syndromes will be necessary, using the same methodology.

Conclusions

When pain is complex, a multimechanistic approach to pain control may be required in order to address the different pain mechanisms involved. Clinicians treating patients with chronic pain in such complex painful conditions must understand the underlying pathophysiology and appropriate treatment regimens, which likely involve combination therapy using analgesic and adjuvant agents. The optimal modality will be found by tailoring the right therapy for the right patient, ensuring the best possible compliance with therapy.

Acknowledgements

The views expressed are those of the authors, and not necessarily coincide with those of the NHS of any of the countries of the authors.

Funding

This research was funded in part by the Paolo Procacci Foundation and a research grant from the Salvatore Maugeri Foundation. This study was part of the joint project “Modello di Unità di Terapia del Dolore e Cure Palliative, Integrate con Associazioni di Volontariato” with the Department of MESVA of the University of L’Aquila. No Rapid Service Fee was received by the journal for the publication of this article.

Editorial Assistance

The authors acknowledge editorial services by Jo Ann LeQuang of LeQ Medical, which was funded by Paolo Procacci Foundation, including the permission to reproduce one of the figures in the paper, initially draw by Luca Di Giacomo.

Authorship

All named authors meet the International Committee of Medical Journal Editors (ICMJE) criteria for authorship for this article, take responsibility for the integrity of the work as a whole, and have given their approval for this version to be published.

Authorship Contributions

Martina Rekatsina carried out most of the selection of the articles and drafted the initial manuscript. All the authors contributed to review and critical revision to improve the quality of the paper. All authors have reviewed and approved the final draft of the submitted manuscript.

Disclosures

Martina Rekatsina, Alba Piroli, and Panagiotis Zis have nothing to disclose. Antonella Paladini, Joseph V. Pergolizzi, and Giustino Varrassi are members of the Journal Editorial Board.

Compliance with Ethics Guidelines

This article is based on previously published studies and does not contain any original data derived from studies on humans or animals performed by the authors.
Open Access This article is distributed under the terms of the Creative Commons Attribution-NonCommercial 4.0 International License (http://​creativecommons.​org/​licenses/​by-nc/​4.​0/​), which permits any non-commercial use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
Literatur
1.
Zurück zum Zitat Del Giorno R, Frumento P, Varrassi G, Paladini A, Coaccioli S. Assessment of chronic pain and access to pain therapy: a cross-sectional population-based study. J Pain Res. 2017;10:2577–84.CrossRefPubMedPubMedCentral Del Giorno R, Frumento P, Varrassi G, Paladini A, Coaccioli S. Assessment of chronic pain and access to pain therapy: a cross-sectional population-based study. J Pain Res. 2017;10:2577–84.CrossRefPubMedPubMedCentral
2.
Zurück zum Zitat Merskey H, Bogduk N. Classification of Chronic Pain. Seattle: IASP Press; 1994. Merskey H, Bogduk N. Classification of Chronic Pain. Seattle: IASP Press; 1994.
3.
Zurück zum Zitat Kosek E, Cohen M, Baron R, Gebhart GF, Mico JA, Rice AS, et al. Do we need a third mechanistic descriptor for chronic pain states? Pain. 2016;157(7):1382–6.CrossRefPubMed Kosek E, Cohen M, Baron R, Gebhart GF, Mico JA, Rice AS, et al. Do we need a third mechanistic descriptor for chronic pain states? Pain. 2016;157(7):1382–6.CrossRefPubMed
4.
Zurück zum Zitat Nicholas M, Vlaeyen JWS, Rief W, Barke A, Aziz Q, Benoliel R, et al. The IASP classification of chronic pain for ICD-11: chronic primary pain. Pain. 2019;160(1):28–37.CrossRefPubMed Nicholas M, Vlaeyen JWS, Rief W, Barke A, Aziz Q, Benoliel R, et al. The IASP classification of chronic pain for ICD-11: chronic primary pain. Pain. 2019;160(1):28–37.CrossRefPubMed
5.
9.
Zurück zum Zitat Varrassi G, Collett B, Morlion B, et al. Proceedings of the CHANGE PAIN Expert Summit in Rome, June 2010. Curr Med Res Opin. 2011;27:2061–2.CrossRefPubMed Varrassi G, Collett B, Morlion B, et al. Proceedings of the CHANGE PAIN Expert Summit in Rome, June 2010. Curr Med Res Opin. 2011;27:2061–2.CrossRefPubMed
10.
Zurück zum Zitat Muller-Schwefe G, Jaksch W, Morlion B, Kalso E, Schafer M, Coluzzi F, et al. Make a change: optimising communication and pain management decisions. Curr Med Res Opin. 2011;27(2):481–8.CrossRefPubMed Muller-Schwefe G, Jaksch W, Morlion B, Kalso E, Schafer M, Coluzzi F, et al. Make a change: optimising communication and pain management decisions. Curr Med Res Opin. 2011;27(2):481–8.CrossRefPubMed
11.
Zurück zum Zitat Varrassi G, Muller-Schwefe G, Pergolizzi J, et al. Pharmacological treatment of chronic pain the need for change. Curr Med Res Opin. 2010;26(5):1231–45.CrossRefPubMed Varrassi G, Muller-Schwefe G, Pergolizzi J, et al. Pharmacological treatment of chronic pain the need for change. Curr Med Res Opin. 2010;26(5):1231–45.CrossRefPubMed
13.
Zurück zum Zitat Varrassi G, Fusco M, Coaccioli S, Paladini A. Chronic pain and neurodegenerative processes in elderly people. Pain Pract. 2015;15(1):1–3.CrossRefPubMed Varrassi G, Fusco M, Coaccioli S, Paladini A. Chronic pain and neurodegenerative processes in elderly people. Pain Pract. 2015;15(1):1–3.CrossRefPubMed
15.
Zurück zum Zitat Paladini A, Fusco M, Coaccioli S, Skaper S, Varrassi G. Chronic pain in the elderly: the case for new therapeutic strategies. Pain Physician. 2015;18:E863–E876876.PubMed Paladini A, Fusco M, Coaccioli S, Skaper S, Varrassi G. Chronic pain in the elderly: the case for new therapeutic strategies. Pain Physician. 2015;18:E863–E876876.PubMed
16.
Zurück zum Zitat Paladini A, Fusco M, Cenacchi T, Schievano C, Piroli A, Varrassi G. Palmitoylethanolamide, a special food for medical purposes, in the treatment of chronic pain: a pooled data meta-analysis. Pain Physician. 2016;19(2):11–24PubMed Paladini A, Fusco M, Cenacchi T, Schievano C, Piroli A, Varrassi G. Palmitoylethanolamide, a special food for medical purposes, in the treatment of chronic pain: a pooled data meta-analysis. Pain Physician. 2016;19(2):11–24PubMed
17.
Zurück zum Zitat Pergolizzi J, Ahlbeck K, Aldington D, Alon E, Coluzzi F, Dahan A, et al. The development of chronic pain: physiological change necessitates a multidisciplinary approach to treatment. Curr Med Res Opin. 2013;29(9):1127–35.CrossRefPubMedPubMedCentral Pergolizzi J, Ahlbeck K, Aldington D, Alon E, Coluzzi F, Dahan A, et al. The development of chronic pain: physiological change necessitates a multidisciplinary approach to treatment. Curr Med Res Opin. 2013;29(9):1127–35.CrossRefPubMedPubMedCentral
18.
Zurück zum Zitat Mannion RJ, Woolf CJ. Pain mechanisms and management: a central perspective. Clin J Pain. 2000;16(3 Suppl):S144–S156156.CrossRefPubMed Mannion RJ, Woolf CJ. Pain mechanisms and management: a central perspective. Clin J Pain. 2000;16(3 Suppl):S144–S156156.CrossRefPubMed
19.
Zurück zum Zitat Larssen M. Ionotropic glutamate receptors in spinal nociceptive processing. Mol Neurobiol. 2009;40:260–88.CrossRef Larssen M. Ionotropic glutamate receptors in spinal nociceptive processing. Mol Neurobiol. 2009;40:260–88.CrossRef
20.
Zurück zum Zitat Pedersen JL, Andersen OK, Arendt-Nielsen L, Kehlet H. Hyperalgesia and temporal summation of pain after heat injury in man. Pain. 1998;74(2–3):189–97.CrossRefPubMed Pedersen JL, Andersen OK, Arendt-Nielsen L, Kehlet H. Hyperalgesia and temporal summation of pain after heat injury in man. Pain. 1998;74(2–3):189–97.CrossRefPubMed
21.
Zurück zum Zitat Guirimand F, Dupont X, Brasseur L, Chauvin M, Bouhassira D. The effects of ketamine on the temporal summation (wind-up) of the R(III) nociceptive flexion reflex and pain in humans. Anesth Analg. 2000;90(2):408–14.CrossRefPubMed Guirimand F, Dupont X, Brasseur L, Chauvin M, Bouhassira D. The effects of ketamine on the temporal summation (wind-up) of the R(III) nociceptive flexion reflex and pain in humans. Anesth Analg. 2000;90(2):408–14.CrossRefPubMed
22.
Zurück zum Zitat Noppers I, Niesters M, Aarts L, Smith T, Sarton E, Dahan A. Ketamine for the treatment of chronic non-cancer pain. Exp Opin Pharmacother. 2010;11(14):2417–29.CrossRef Noppers I, Niesters M, Aarts L, Smith T, Sarton E, Dahan A. Ketamine for the treatment of chronic non-cancer pain. Exp Opin Pharmacother. 2010;11(14):2417–29.CrossRef
23.
Zurück zum Zitat Correll GE, Maleki J, Gracely EJ, Muir JJ, Harbut RE. Subanesthetic ketamine infusion therapy: a retrospective analysis of a novel therapeutic approach to complex regional pain syndrome. Pain Med (Malden, Mass). 2004;5(3):263–75.CrossRef Correll GE, Maleki J, Gracely EJ, Muir JJ, Harbut RE. Subanesthetic ketamine infusion therapy: a retrospective analysis of a novel therapeutic approach to complex regional pain syndrome. Pain Med (Malden, Mass). 2004;5(3):263–75.CrossRef
24.
Zurück zum Zitat Song GH, Venkatraman V, Ho KY, Chee MW, Yeoh KG, Wilder-Smith CH. Cortical effects of anticipation and endogenous modulation of visceral pain assessed by functional brain MRI in irritable bowel syndrome patients and healthy controls. Pain. 2006;126(1–3):79–90.CrossRefPubMed Song GH, Venkatraman V, Ho KY, Chee MW, Yeoh KG, Wilder-Smith CH. Cortical effects of anticipation and endogenous modulation of visceral pain assessed by functional brain MRI in irritable bowel syndrome patients and healthy controls. Pain. 2006;126(1–3):79–90.CrossRefPubMed
25.
Zurück zum Zitat Pertovaara A, Almeida A. Descending inhibitory systems. In: Cervero F, Jensen T, editors. Handbook of clinical neurology. Amsterdan: Elsevier; 2006. p. 179–192. Pertovaara A, Almeida A. Descending inhibitory systems. In: Cervero F, Jensen T, editors. Handbook of clinical neurology. Amsterdan: Elsevier; 2006. p. 179–192.
26.
Zurück zum Zitat Woolf CJ. Pain: moving from symptom control toward mechanism-specific pharmacologic management. Ann Int Med. 2004;140(6):441–51.CrossRefPubMed Woolf CJ. Pain: moving from symptom control toward mechanism-specific pharmacologic management. Ann Int Med. 2004;140(6):441–51.CrossRefPubMed
27.
Zurück zum Zitat Baron R, Binder A, Wasner G. Neuropathic pain: diagnosis, pathophysiological mechanisms, and treatment. Lancet Neurol. 2010;9(8):807–19.CrossRefPubMed Baron R, Binder A, Wasner G. Neuropathic pain: diagnosis, pathophysiological mechanisms, and treatment. Lancet Neurol. 2010;9(8):807–19.CrossRefPubMed
28.
Zurück zum Zitat Finnerup NB, Attal N, Haroutounian S, McNicol E, Baron R, Dworkin RH, et al. Pharmacotherapy for neuropathic pain in adults: a systematic review and meta-analysis. Lancet Neurol. 2015;14(2):162–73.CrossRefPubMedPubMedCentral Finnerup NB, Attal N, Haroutounian S, McNicol E, Baron R, Dworkin RH, et al. Pharmacotherapy for neuropathic pain in adults: a systematic review and meta-analysis. Lancet Neurol. 2015;14(2):162–73.CrossRefPubMedPubMedCentral
30.
Zurück zum Zitat Binder A, Baron R. The pharmacological therapy of chronic neuropathic pain. Dtsch Arztebl Int. 2016;113(37):616–25.PubMedPubMedCentral Binder A, Baron R. The pharmacological therapy of chronic neuropathic pain. Dtsch Arztebl Int. 2016;113(37):616–25.PubMedPubMedCentral
31.
Zurück zum Zitat Saarto T, Wiffen PJ. Antidepressants for neuropathic pain. Cochrane Database Syst Rev. 2007;96:399–409. Saarto T, Wiffen PJ. Antidepressants for neuropathic pain. Cochrane Database Syst Rev. 2007;96:399–409.
33.
Zurück zum Zitat McNicol ED, Midbari A, Eisenberg E. Opioids for neuropathic pain. Cochrane Database Syst Rev. 2013;11:3013–25. McNicol ED, Midbari A, Eisenberg E. Opioids for neuropathic pain. Cochrane Database Syst Rev. 2013;11:3013–25.
35.
Zurück zum Zitat Vranken JH. Elucidation of pathophysiology and treatment of neuropathic pain. Cent Nerv Syst Agents Med Chem. 2012;12(4):304–14.CrossRefPubMed Vranken JH. Elucidation of pathophysiology and treatment of neuropathic pain. Cent Nerv Syst Agents Med Chem. 2012;12(4):304–14.CrossRefPubMed
36.
Zurück zum Zitat Guetti C, Angeletti C, Marinangeli F, Ciccozzi A, Baldascino G, Paladini A, et al. Transdermal buprenorphine for central neuropathic pain: clinical reports. Pain Pract. 2011;11(5):446–52.CrossRefPubMed Guetti C, Angeletti C, Marinangeli F, Ciccozzi A, Baldascino G, Paladini A, et al. Transdermal buprenorphine for central neuropathic pain: clinical reports. Pain Pract. 2011;11(5):446–52.CrossRefPubMed
38.
Zurück zum Zitat Yarnitsky D. Conditioned pain modulation (the diffuse noxious inhibitory control-like effect): its relevance for acute and chronic pain states. Curr Opin Anaesthesiol. 2010;23(5):611–5.CrossRefPubMed Yarnitsky D. Conditioned pain modulation (the diffuse noxious inhibitory control-like effect): its relevance for acute and chronic pain states. Curr Opin Anaesthesiol. 2010;23(5):611–5.CrossRefPubMed
39.
Zurück zum Zitat Hauser W, Ablin J, Fitzcharles MA, Littlejohn G, Luciano JV, Usui C, et al. Fibromyalgia. Nat Rev Dis Primers. 2015;1:15022.CrossRefPubMed Hauser W, Ablin J, Fitzcharles MA, Littlejohn G, Luciano JV, Usui C, et al. Fibromyalgia. Nat Rev Dis Primers. 2015;1:15022.CrossRefPubMed
40.
41.
Zurück zum Zitat Uceyler N, Zeller D, Kahn AK, Kewenig S, Kittel-Schneider S, Schmid A, et al. Small fibre pathology in patients with fibromyalgia syndrome. Brain. 2013;136(Pt 6):1857–67.CrossRefPubMed Uceyler N, Zeller D, Kahn AK, Kewenig S, Kittel-Schneider S, Schmid A, et al. Small fibre pathology in patients with fibromyalgia syndrome. Brain. 2013;136(Pt 6):1857–67.CrossRefPubMed
42.
Zurück zum Zitat Staud R. Peripheral pain mechanisms in chronic widespread pain. Best Pract Res Clin Rheuamtol. 2011;25(2):155–64.CrossRef Staud R. Peripheral pain mechanisms in chronic widespread pain. Best Pract Res Clin Rheuamtol. 2011;25(2):155–64.CrossRef
43.
Zurück zum Zitat Calandre EP, Hidalgo J, Rico-Villademoros F. Use of ziprasidone in patients with fibromyalgia: a case series. Rheumatol Int. 2007;27(5):473–6.CrossRefPubMed Calandre EP, Hidalgo J, Rico-Villademoros F. Use of ziprasidone in patients with fibromyalgia: a case series. Rheumatol Int. 2007;27(5):473–6.CrossRefPubMed
44.
Zurück zum Zitat Perrot S. Fibromyalgia: a misconnection in a multiconnected world? Eur J Pain. 2019;23(5):866–73.CrossRefPubMed Perrot S. Fibromyalgia: a misconnection in a multiconnected world? Eur J Pain. 2019;23(5):866–73.CrossRefPubMed
45.
Zurück zum Zitat Atzeni F, Gerardi MC, Masala IF, Alciati A, Batticciotto A, Sarzi-Puttini P. An update on emerging drugs for fibromyalgia treatment. Exp Opin Emerg Drugs. 2017;22(4):357–67.CrossRef Atzeni F, Gerardi MC, Masala IF, Alciati A, Batticciotto A, Sarzi-Puttini P. An update on emerging drugs for fibromyalgia treatment. Exp Opin Emerg Drugs. 2017;22(4):357–67.CrossRef
46.
Zurück zum Zitat Macfarlane GJ, Kronisch C, Atzeni F, Hauser W, Choy EH, Amris K, et al. EULAR recommendations for management of fibromyalgia. Ann Rheum Dis. 2017;76(12):e54.CrossRefPubMed Macfarlane GJ, Kronisch C, Atzeni F, Hauser W, Choy EH, Amris K, et al. EULAR recommendations for management of fibromyalgia. Ann Rheum Dis. 2017;76(12):e54.CrossRefPubMed
47.
Zurück zum Zitat Macfarlane GJ, Kronisch C, Dean LE, Atzeni F, Hauser W, Fluss E, et al. EULAR revised recommendations for the management of fibromyalgia. Ann Rheum Dis. 2017;76(2):318–28.CrossRefPubMed Macfarlane GJ, Kronisch C, Dean LE, Atzeni F, Hauser W, Fluss E, et al. EULAR revised recommendations for the management of fibromyalgia. Ann Rheum Dis. 2017;76(2):318–28.CrossRefPubMed
48.
Zurück zum Zitat Del Giorno R, Skaper S, Paladini A, Varrassi G, Coaccioli S. Palmitoylethanolamide in fibromyalgia: results from prospective and retrospective observational studies. Pain Ther. 2015;4(2):169–78.CrossRefPubMedPubMedCentral Del Giorno R, Skaper S, Paladini A, Varrassi G, Coaccioli S. Palmitoylethanolamide in fibromyalgia: results from prospective and retrospective observational studies. Pain Ther. 2015;4(2):169–78.CrossRefPubMedPubMedCentral
49.
Zurück zum Zitat Angeletti C, Guetti C, Piroli A, Angeletti PM, Paladini A, Ciccozzi A, et al. Duloxetine and pregabalin for pain management in multiple rheumatic diseases associated with fibromyalgia. Pain Pract. 2013;13(8):657–62.CrossRefPubMed Angeletti C, Guetti C, Piroli A, Angeletti PM, Paladini A, Ciccozzi A, et al. Duloxetine and pregabalin for pain management in multiple rheumatic diseases associated with fibromyalgia. Pain Pract. 2013;13(8):657–62.CrossRefPubMed
50.
Zurück zum Zitat Galvani C, Caramaschi P, Mura P, Paladini A, Piroli A, Arnaudo E, et al. Postural counseling represents a novel option in pain management of fibromyalgia patients. J Pain Res. 2019;12:327–37.CrossRefPubMedPubMedCentral Galvani C, Caramaschi P, Mura P, Paladini A, Piroli A, Arnaudo E, et al. Postural counseling represents a novel option in pain management of fibromyalgia patients. J Pain Res. 2019;12:327–37.CrossRefPubMedPubMedCentral
51.
Zurück zum Zitat Sadeghi M, Erickson A, Castro J, Deiteren A, Harrington AM, Grundy L, et al. Contribution of membrane receptor signalling to chronic visceral pain. Int J Biochem Cell Biol. 2018;98:10–23.CrossRefPubMed Sadeghi M, Erickson A, Castro J, Deiteren A, Harrington AM, Grundy L, et al. Contribution of membrane receptor signalling to chronic visceral pain. Int J Biochem Cell Biol. 2018;98:10–23.CrossRefPubMed
52.
Zurück zum Zitat Radovanovic-Dinic B, Tesic-Rajkovic S, Grgov S, Petrovic G, Zivkovic V. Irritable bowel syndrome from etiopathogenesis to therapy. Biomed Pap Med Fac Univ Palacky Olomouc Czech Repub. 2018;162(1):1–9.CrossRefPubMed Radovanovic-Dinic B, Tesic-Rajkovic S, Grgov S, Petrovic G, Zivkovic V. Irritable bowel syndrome from etiopathogenesis to therapy. Biomed Pap Med Fac Univ Palacky Olomouc Czech Repub. 2018;162(1):1–9.CrossRefPubMed
53.
Zurück zum Zitat Kim JS. Pharmacological management of central post-stroke pain: a practical guide. CNS Drugs. 2014;28(9):787–97.CrossRefPubMed Kim JS. Pharmacological management of central post-stroke pain: a practical guide. CNS Drugs. 2014;28(9):787–97.CrossRefPubMed
55.
Zurück zum Zitat Birklein F, Schlereth T. Complex regional pain syndrome-significant progress in understanding. Pain. 2015;156(Suppl 1):S94–103.CrossRefPubMed Birklein F, Schlereth T. Complex regional pain syndrome-significant progress in understanding. Pain. 2015;156(Suppl 1):S94–103.CrossRefPubMed
56.
Zurück zum Zitat Huygen FJ, De Bruijn AG, De Bruin MT, Groeneweg JG, Klein J, Zijlstra FJ. Evidence for local inflammation in complex regional pain syndrome type 1. Mediat Inflamm. 2002;11(1):47–51.CrossRef Huygen FJ, De Bruijn AG, De Bruin MT, Groeneweg JG, Klein J, Zijlstra FJ. Evidence for local inflammation in complex regional pain syndrome type 1. Mediat Inflamm. 2002;11(1):47–51.CrossRef
57.
Zurück zum Zitat Alexander GM, Peterlin BL, Perreault MJ, Grothusen JR, Schwartzman RJ. Changes in plasma cytokines and their soluble receptors in complex regional pain syndrome. J Pain. 2012;13(1):10–20.CrossRefPubMed Alexander GM, Peterlin BL, Perreault MJ, Grothusen JR, Schwartzman RJ. Changes in plasma cytokines and their soluble receptors in complex regional pain syndrome. J Pain. 2012;13(1):10–20.CrossRefPubMed
58.
Zurück zum Zitat Sommer C, Kress M. Recent findings on how proinflammatory cytokines cause pain: peripheral mechanisms in inflammatory and neuropathic hyperalgesia. Neurosci Lett. 2004;361(1–3):184–7.CrossRefPubMed Sommer C, Kress M. Recent findings on how proinflammatory cytokines cause pain: peripheral mechanisms in inflammatory and neuropathic hyperalgesia. Neurosci Lett. 2004;361(1–3):184–7.CrossRefPubMed
59.
Zurück zum Zitat Blaes F, Schmitz K, Tschernatsch M, Kaps M, Krasenbrink I, Hempelmann G, et al. Autoimmune etiology of complex regional pain syndrome (M. Sudeck). Neurology. 2004;63(9):1734–6.CrossRefPubMed Blaes F, Schmitz K, Tschernatsch M, Kaps M, Krasenbrink I, Hempelmann G, et al. Autoimmune etiology of complex regional pain syndrome (M. Sudeck). Neurology. 2004;63(9):1734–6.CrossRefPubMed
60.
Zurück zum Zitat Oaklander AL, Fields HL. Is reflex sympathetic dystrophy/complex regional pain syndrome type I a small-fiber neuropathy? Ann Neurol. 2009;65(6):629–38.CrossRefPubMed Oaklander AL, Fields HL. Is reflex sympathetic dystrophy/complex regional pain syndrome type I a small-fiber neuropathy? Ann Neurol. 2009;65(6):629–38.CrossRefPubMed
61.
Zurück zum Zitat Urits I, Burshtein A, Sharma M, Testa L, Gold PA, Orhurhu V, et al. Low back pain, a comprehensive review: pathophysiology, diagnosis, and treatment. Curr Pain Headache Rep. 2019;23(3):23.CrossRefPubMed Urits I, Burshtein A, Sharma M, Testa L, Gold PA, Orhurhu V, et al. Low back pain, a comprehensive review: pathophysiology, diagnosis, and treatment. Curr Pain Headache Rep. 2019;23(3):23.CrossRefPubMed
63.
Zurück zum Zitat Partanen JV, Ojala TA, Arokoski JP. Myofascial syndrome and pain: a neurophysiological approach. Pathophysiology. 2010;17(1):19–28.CrossRefPubMed Partanen JV, Ojala TA, Arokoski JP. Myofascial syndrome and pain: a neurophysiological approach. Pathophysiology. 2010;17(1):19–28.CrossRefPubMed
64.
Zurück zum Zitat Kalichman L, Hunter DJ. Lumbar facet joint osteoarthritis: a review. Semin Arthritis Rheum. 2007;37(2):69–80.CrossRefPubMed Kalichman L, Hunter DJ. Lumbar facet joint osteoarthritis: a review. Semin Arthritis Rheum. 2007;37(2):69–80.CrossRefPubMed
65.
Zurück zum Zitat Bogduk N. Evidence-informed management of chronic low back pain with facet injections and radiofrequency neurotomy. Spine J. 2008;8(1):56–64.CrossRefPubMed Bogduk N. Evidence-informed management of chronic low back pain with facet injections and radiofrequency neurotomy. Spine J. 2008;8(1):56–64.CrossRefPubMed
66.
Zurück zum Zitat Comer C, Conaghan PG. Tackling persistent low back pain in primary care. Practitioner. 2009;253(1721):32–4.PubMed Comer C, Conaghan PG. Tackling persistent low back pain in primary care. Practitioner. 2009;253(1721):32–4.PubMed
67.
Zurück zum Zitat Aprill C, Bogduk N. High-intensity zone: a diagnostic sign of painful lumbar disc on magnetic resonance imaging. Br J Radiol. 1992;65(773):361–9.CrossRefPubMed Aprill C, Bogduk N. High-intensity zone: a diagnostic sign of painful lumbar disc on magnetic resonance imaging. Br J Radiol. 1992;65(773):361–9.CrossRefPubMed
69.
Zurück zum Zitat Paladini A, Varrassi G, Bentivegna G, Carletti S, Piroli A, Coaccioli S. Palmitoylethanolamide in the treatment of failed back surgery syndrome. Pain Res Treat. 2017;2017:1486010.PubMedPubMedCentral Paladini A, Varrassi G, Bentivegna G, Carletti S, Piroli A, Coaccioli S. Palmitoylethanolamide in the treatment of failed back surgery syndrome. Pain Res Treat. 2017;2017:1486010.PubMedPubMedCentral
70.
Zurück zum Zitat Koc Z, Ozcakir S, Sivrioglu K, Gurbet A, Kucukoglu S. Effectiveness of physical therapy and epidural steroid injections in lumbar spinal stenosis. Spine. 2009;34(10):985–9.CrossRefPubMed Koc Z, Ozcakir S, Sivrioglu K, Gurbet A, Kucukoglu S. Effectiveness of physical therapy and epidural steroid injections in lumbar spinal stenosis. Spine. 2009;34(10):985–9.CrossRefPubMed
71.
Zurück zum Zitat Foley BS, Buschbacher RM. Sacroiliac joint pain: anatomy, biomechanics, diagnosis, and treatment. Am J Phys Med Rehabil. 2006;85(12):997–1006.CrossRefPubMed Foley BS, Buschbacher RM. Sacroiliac joint pain: anatomy, biomechanics, diagnosis, and treatment. Am J Phys Med Rehabil. 2006;85(12):997–1006.CrossRefPubMed
72.
Zurück zum Zitat Chou R. In the clinic. Low back pain. Ann Intern Med. 2014;160(11):6.CrossRef Chou R. In the clinic. Low back pain. Ann Intern Med. 2014;160(11):6.CrossRef
73.
Zurück zum Zitat Koes BW, Backes D, Bindels PJE. Pharmacotherapy for chronic non-specific low back pain: current and future options. Exp Opin Pharmacother. 2018;19(6):537–45.CrossRef Koes BW, Backes D, Bindels PJE. Pharmacotherapy for chronic non-specific low back pain: current and future options. Exp Opin Pharmacother. 2018;19(6):537–45.CrossRef
74.
Zurück zum Zitat O'Sullivan K, O'Keeffe M, O'Sullivan P. NICE low back pain guidelines: opportunities and obstacles to change practice. Br J Sports Med. 2017;51(22):1632–3.CrossRefPubMed O'Sullivan K, O'Keeffe M, O'Sullivan P. NICE low back pain guidelines: opportunities and obstacles to change practice. Br J Sports Med. 2017;51(22):1632–3.CrossRefPubMed
75.
Zurück zum Zitat Gofeld M, Jitendra J, Faclier G. Radiofrequency denervation of the lumbar zygapophysial joints: 10-year prospective clinical audit. Pain Physician. 2007;10(2):291–300.CrossRefPubMed Gofeld M, Jitendra J, Faclier G. Radiofrequency denervation of the lumbar zygapophysial joints: 10-year prospective clinical audit. Pain Physician. 2007;10(2):291–300.CrossRefPubMed
76.
Zurück zum Zitat Alhouayek M, Muccioli GG. Harnessing the anti-inflammatory potential of palmitoylethanolamide. Drug Discov Today. 2014;19(10):1632–9.CrossRefPubMed Alhouayek M, Muccioli GG. Harnessing the anti-inflammatory potential of palmitoylethanolamide. Drug Discov Today. 2014;19(10):1632–9.CrossRefPubMed
77.
Zurück zum Zitat Bettoni I, Comelli F, Colombo A, Bonfanti P, Costa B. Non-neuronal cell modulation relieves neuropathic pain: efficacy of the endogenous lipid palmitoylethanolamide. CNS Neurol Disord Drug Targets. 2013;12(1):34–44.CrossRefPubMed Bettoni I, Comelli F, Colombo A, Bonfanti P, Costa B. Non-neuronal cell modulation relieves neuropathic pain: efficacy of the endogenous lipid palmitoylethanolamide. CNS Neurol Disord Drug Targets. 2013;12(1):34–44.CrossRefPubMed
78.
Zurück zum Zitat Varrassi G, Muller-Schwefe GH. The international CHANGE PAIN physician survey: does specialism influence the perception of pain and its treatment? Curr Med Res Opin. 2012;28(5):823–31.CrossRefPubMed Varrassi G, Muller-Schwefe GH. The international CHANGE PAIN physician survey: does specialism influence the perception of pain and its treatment? Curr Med Res Opin. 2012;28(5):823–31.CrossRefPubMed
79.
Zurück zum Zitat Fusco M, Paladini A, Skaper S, Varrassi G. Chronic and neuropathic pain syndrome in the elderly: pathophysiological basis and perspectives for a rational therapy. Pain Nurs Mag. 2014;3:94–104. Fusco M, Paladini A, Skaper S, Varrassi G. Chronic and neuropathic pain syndrome in the elderly: pathophysiological basis and perspectives for a rational therapy. Pain Nurs Mag. 2014;3:94–104.
81.
Zurück zum Zitat Benedetti F, Arduino C, Costa S, Vighetti S, Tarenzi L, Rainero I, et al. Loss of expectation-related mechanisms in Alzheimer's disease makes analgesic therapies less effective. Pain. 2006;121(1–2):133–44.CrossRefPubMed Benedetti F, Arduino C, Costa S, Vighetti S, Tarenzi L, Rainero I, et al. Loss of expectation-related mechanisms in Alzheimer's disease makes analgesic therapies less effective. Pain. 2006;121(1–2):133–44.CrossRefPubMed
82.
Zurück zum Zitat Banks WA. Drug delivery to the brain in Alzheimer's disease: consideration of the blood-brain barrier. Adv Drug Deliv Rev. 2012;64(7):629–39.CrossRefPubMed Banks WA. Drug delivery to the brain in Alzheimer's disease: consideration of the blood-brain barrier. Adv Drug Deliv Rev. 2012;64(7):629–39.CrossRefPubMed
83.
Zurück zum Zitat Varrassi G, Hanna M, Macheras G, et al. Multimodal analgesia in moderate-to-severe pain: a role for a new fixed combination of dexketoprofen and tramadol. Curr Med Res Opin. 2017;33:1165–73.CrossRefPubMed Varrassi G, Hanna M, Macheras G, et al. Multimodal analgesia in moderate-to-severe pain: a role for a new fixed combination of dexketoprofen and tramadol. Curr Med Res Opin. 2017;33:1165–73.CrossRefPubMed
Metadaten
Titel
Pathophysiologic Approach to Pain Therapy for Complex Pain Entities: A Narrative Review
verfasst von
Martina Rekatsina
Antonella Paladini
Alba Piroli
Panagiotis Zis
Joseph V. Pergolizzi
Giustino Varrassi
Publikationsdatum
04.01.2020
Verlag
Springer Healthcare
Erschienen in
Pain and Therapy / Ausgabe 1/2020
Print ISSN: 2193-8237
Elektronische ISSN: 2193-651X
DOI
https://doi.org/10.1007/s40122-019-00147-2

Kompaktes Leitlinien-Wissen Innere Medizin (Link öffnet in neuem Fenster)

Mit medbee Pocketcards schnell und sicher entscheiden.
Leitlinien-Wissen kostenlos und immer griffbereit auf ihrem Desktop, Handy oder Tablet.

Neu im Fachgebiet Innere Medizin

Duale Checkpointhemmung gegen Melanome verlängert langfristig das Leben

Im Vergleich zu den Überlebenschancen vor der Einführung von Immuncheckpointhemmern (ICI) ist der Fortschritt durch eine ICI-Kombination mit unterschiedlichen Tagets bei fortgeschrittenem Melanom erstaunlich. Das belegen die finalen Ergebnisse der CheckMate-067-Studie und geben Betroffenen "Hoffnung auf Heilung".

Knochenmarktransplantat als Chance für ältere AML-Patienten

Lange Zeit ist die Transplantation von hämatopoetischen Stammzellen nur bei jüngeren Patienten mit akuter myeloischer Leukämie praktiziert worden. Inzwischen profitieren auch Ältere davon. Ergebnisse einer Studie unterstützen dieses Vorgehen.

Nierenzellkarzinom: Kein Nachteil durch subkutan appliziertes Nivolumab

Die subkutane Applikation von Nivolumab ist nach Daten einer Phase-3-Studie ähnlich gut wirksam wie die intravenöse: Die Pharmakokinetik ist vergleichbar, die objektive Response war in der Studie sogar leicht besser als in der Gruppe mit Infusionen.

Vorteile für Androgenentzug plus Androgenrezeptorblockade

Für Männer mit metastasiertem hormonsensitivem Prostata-Ca. (mHSPC), die keine Hormonchemotherapie wollen oder vertragen, ist der Androgenentzug plus Darolutamid eine Alternative: Das Progressionsrisiko wird im Vergleich zum alleinigen Androgenentzug fast halbiert.

EKG Essentials: EKG befunden mit System (Link öffnet in neuem Fenster)

In diesem CME-Kurs können Sie Ihr Wissen zur EKG-Befundung anhand von zwölf Video-Tutorials auffrischen und 10 CME-Punkte sammeln.
Praxisnah, relevant und mit vielen Tipps & Tricks vom Profi.

Update Innere Medizin

Bestellen Sie unseren Fach-Newsletter und bleiben Sie gut informiert.