Diagnosis of complex regional pain syndrome

Article information

Ann Clin Neurophysiol. 2022;24(2):35-45
Publication date (electronic) : 2022 October 31
doi : https://doi.org/10.14253/acn.2022.24.2.35
Department of Neurology, Incheon St. Mary’s Hospital, The Catholic University of Korea College of Medicine, Incheon, Korea
Correspondence to Young-Do Kim Department of Neurology, Incheon St. Mary’s Hospital, The Catholic University of Korea College of Medicine, 56 Dongsu-ro, Bupyeong-gu, Incheon 21431, Korea Tel: +82-32-510-5010 Fax: +82-32-280-6390 E-mail: limbic@catholic.ac.kr
Received 2022 July 30; Revised 2022 August 28; Accepted 2022 August 31.

Abstract

Complex regional pain syndrome (CRPS) is a chronic regional pain disorder that most frequently affects the limbs. It is characterized by hyperalgesia, allodynia, edema, motor disturbance, and vasomotor instability, and typically occurs following surgery or trauma. In type-I CRPS there is no confirmed nerve injury, while peripheral nerve injury is present in type-II CRPS. The multifactorial pathophysiological etiology of CRPS includes inflammation, autoimmune responses, abnormal cytokine production, autonomic dysfunction, altered blood flow, psychological factors, and central cortical reorganization. There are no specific laboratory diagnostic tools for CRPS, and so it is diagnosed clinically. The Budapest criteria are currently the most-accepted diagnostic criteria.

INTRODUCTION

Complex regional pain syndrome (CRPS) is a chronic pain disorder that frequently causes allodynia (disproportionately increased pain response to a nonnoxious stimulus) and hyperalgesia (disproportionately increased pain response to a mildly noxious stimulus) in the extremities and other body regions. It occurs most frequently after trauma or surgery, and the pain experienced is excessive relative to the severity of the event and the amount of tissue damage.1 Clinical manifestations include autonomic dysfunction, hyperalgesia, edema, vasomotor instability, and spontaneous pain. Changes in the understanding of the illness over time have made diagnosing and managing CRPS challenging. Furthermore, a CRPS diagnosis cannot be confirmed by a single test, and so clinical diagnostic criteria for CRPS have been developed by clinicians and researchers based on the existing knowledge in the absence of information on the precise cause of CRPS. The clinical presentation and disease course of CRPS both vary. Despite receiving treatment, many patients have a poor prognosis, and their quality of life can be severely impacted. Reducing disease progression and improving the quality of life require early diagnosis and initiation of treatment.2 This review provides an update on the current literature related to the epidemiology, pathophysiology, clinical manifestations, and diagnosis of CRPS.

DEFINITION AND TERMINOLOGY

The definition of and diagnosis methods for CRPS have evolved over time. There are now more than 100 names for this disorder in the literature, depending on the triggering event, the predominating symptoms, the specialty and country of origin of the treating physician, and the hypothesized pathogenic mechanism.3 “Reflex sympathetic dystrophy,” “causalgia,” “algoneurodystrophy,” and “Sudeck’s atrophy” were historically used as names for this syndrome (Table 1),4 with “reflex sympathetic dystrophy” (RSD) being the most frequently accepted one. The term RSD was introduced by Evans in 1946 in an attempt to unify both causalgia and similar entities being due to a hyperactive sympathetic nervous system.5 The general consensus regarding CRPS has been reported as follows: “CRPS describes an array of painful conditions that are characterized by continuing (spontaneous and/or evoked) regional pain that is seemingly disproportionate in time or degree to the usual course of any known trauma or other lesion. The pain is regional (not in a specific nerve territory or dermatome) and usually has a distal predominance of abnormal sensory, motor, sudomotor, vasomotor, and/or trophic findings. The syndrome shows variable progression over time.”6 CRPS can be classified into two categories: (1) type-I CRPS (CRPS-I, the form also known as RSD), which is when there is no confirmed nerve injury, and (2) type-II CRPS (CRPS-II, formerly termed “causalgia”), which is associated with nerve injury.1 Some researchers additionally distinguish between “warm” and “cold” CRPS subtypes:7 increased skin temperature at outset of symptoms distinguishes warm CRPS, further indicating that it is an inflammatory form, while decreased skin temperature at the onset of symptoms distinguishes cold CRPS.

Synonyms for CRPS

EPIDEMIOLOGY

There are obviously variations among practitioners because CRPS is diagnosed clinically based on the medical history, and physical and neurological examinations. This has resulted in the estimated annual incidence varying significantly between studies, from 5 to 26 per 100,000.8,9 The largest CRPS population-based study to date in the USA was reported on in 2016. Among the 33,406,123 patients included in that study from a sample database spanning from 2007 to 2011 revealed, 22,533 patients (i.e., 0.07%) were discharged with a diagnosis of CRPS.10 CRPS-I is more common than CRPS-II. The reported incidence of CRPS-II in the presence of peripheral nerve damage in different data sets has ranged from 2% to 14%, with a mean of approximately 4%.8

The reported female-to-male ratio of patients with CRPS has ranged from 2:1 to 4:1.9,11 The incidence appears to be highest in females who are postmenopausal.12 It is particularly interesting that a slight male preponderance in the sex distribution was found in two different Korean patient groups,13 while females made up nearly two-thirds of the patients in a Japanese cohort.14 The prevalence of CRPS varies with age, with the mean age at diagnosis peaking at 40-50 years and the incidence peaking at 61-70 years, and CRPS being very uncommon in childhood and adolescence.9

Polytrauma, fractures, crush injuries, and surgery are the most commonly recognized risk factors for CRPS.6,15 However, in up to 10% of patients there are no known triggering factors.9,11,12 The most frequent primary causes of CRPS in a recent review of 1,043 patients were fractures (42%), blunt traumatic injuries excluding fractures (e.g., sprains), surgery (12%), and carpal tunnel syndrome (7%).11 CRPS-I was found significantly more often in patients with ankle fractures than in those with hand, wrist, or foot fractures.16 Significantly higher incidence rates of CRPS-I were also related to intra-articular fractures and dislocated fractures.16 Nevertheless, the overall prevalence of CRPS associated with these triggering events is quite low. Crijns et al.17 found that 0.19% of 59,765 patients received treatment for distal radius fractures also had CRPS. In a similar more-recent study, 0.64% of 172,194 patients with distal radius fractures who underwent surgical treatment experienced CRPS.18 Among 113 cases that were analyzed retrospectively, the symptoms manifested on the right side in 47% of cases, on the left in 51%, and bilaterally in 2%.9,14 The upper extremities are more likely than the lower extremities to be affected.19 Two Korean cohorts represent a significant exception, where a lower limb was affected more frequently than an upper extremity, and 7% of patients had multiple extremities affected.20

A diagnosis of CRPS is strongly and independently correlated with fibromyalgia, which increases the risk up to 2.5-fold compared with controls.17,21 The risk may also be increased by other musculoskeletal diseases, including rheumatoid arthritis.19 An unexpectedly finding is that lower rates of CRPS-1 were related to diabetes, obesity, and hypothyroidism.15

PATHOPHYSIOLOGY

While the pathophysiology of CRPS is still unknown, it is considered to involve dysfunction of both the central and peripheral nerve systems (Fig. 1).22 Despite scientific progress, the pathophysiological etiology of CRPS has still not been established (Table 2). CRPS is characterized by an inappropriate tissue response to injury as well as increased sensitization of the peripheral and central nervous systems along with accompanying inflammatory alterations and autonomic dysfunction.23 It is also thought that genetic and psychological factors contribute of CRPS.23

Fig. 1.

Hypothetical model of mechanisms interacting in the development of complex regional pain syndrome. PTSD, post-traumatic stress disorder; CGRP, calcitonin-gene-related peptide; IL, interleukin; TNF, tumor necrosis factor.

The various pathophysiologies of CRPS

The warm or acute phase is defined by the release of proinflammatory modulators, while the cold or chronic phase is characterized by the activation of keratinocytes, fibroblasts, and osteoclasts.2 Both a proinflammatory immune response and impaired neuropeptide signaling are characteristics of CRPS.24 Inflammation is a normal natural consequence of a stroke, surgery, or tissue trauma, and the response of the innate immune system is both amplified and persistent in CRPS patients.2 Cytokines of the innate immune system trigger an immune cascade that results in histamine-induced vasodilation, which in turn results in the redness, swelling, pain, and warmth typical of the acute phase of CRPS.25 Numerous investigations have found increased CD4 and CD8 lymphocyte populations in CRPS patients, suggesting an antigen-mediated T-cell response.26 Neuropathic inflammation is also considered a major factor in the progression of CRPS. The activation of peripheral nociceptors of C-fibers results in the transmission of pain signals afferently toward the dorsal ganglia and efferently toward the affected tissue.27 An investigation of skin biopsies from CRPS patients found that the binding of substance P and calcitonin-gene-related peptide (CGRP) to keratinocyte receptors led to keratinocyte proliferation, neurogenic inflammatory alterations, and subsequent hyperalgesia and allodynia.28 It was believed that depolarization of afferent C-fibers could lead in neurogenic inflammation and the release of substance P and CGRP.29

Previous research has found that autoantibody levels in the serum, skin, and tissues are higher in CRPS patients and animal models, which supports CRPS being an autoimmune disorder.30 Autoantibodies are thought to cause pain in CRPS by sensitizing nociceptors.31 Additionally, CRPS induced elevations of IgM antibody levels in the skin and spinal tissue of rats, which were assumed to cause increased nociceptive sensitization.32

Abnormal activity of the autonomic nervous system was initially believed to be the cause of CRPS. Clinical symptoms such as skin-color changes, elevated heart rate, decreased heart-rate variability, low cardiac output, and excessive sweating are frequently caused by an imbalance in the autonomic nervous system in CRPS patients.33

Postganglionic sympathetic neurons and afferent neurons are connected via the sympathetic nervous system, and so it is thought that upregulation of alpha-adrenergic receptors causes inflammation of the skin of CRPS patients.34 Patients with CRPS were found to have higher systemic catecholamine expression but lower norepinephrine levels in the affected limb.34 Prolonged proinflammatory cytokine release during the chronic cold phase of CRPS causes hyperactivity of the sympathetic nervous system, which increases norepinephrine levels, decreases α-1 adrenergic receptor expression, and culminates in vasoconstriction and the development of a cold, blue, and clammy limb.2

Another suggested underlying mechanism is abnormal cortical reorganization, which has also been described as a form of maladaptive plasticity. Studies utilizing functional magnetic resonance imaging (MRI) and magnetoencephalography have revealed this brain reorganization.35 Somatosensory cortex reorganization may cause various CRPS manifestations, such as the glove- or stocking-like distribution of sensory signs,36 the extension of sensory deficits over an entire quadrant or even one entire side of the body,37 referral or mislocalization of tactile sensations,38 and the perception of the affected limb as being distorted or larger than it actually is.39 Similar to this, reorganization of the motor cortex definitely plays a significant role in the majority of motor abnormalities experienced by patients with CRPS-I or CRPS-II.40

There is abundant evidence that hereditary factors contribute to the propensity to develop CRPS. There have been reports of familial cases of CRPS, and these patients frequently have severe disease with early onset, recurrences, spreading to many sites, and/or dystonia.41 HLA-DQ1 was substantially more prevalent in 52 Dutch CRPS patients than in 295 local controls.42 A pilot study produced indirect relationship between CRPS and the closely linked DR2.43 CRPS manifestations are potentially related to genetic abnormalities in mitochondrial DNA.44

Psychosocial factors and pain outcomes are correlated in CRPS patients.45 It has been proposed that psychological conditions including depression play a role in the emergence of CRPS.4 Most (86%) of 58 CRPS patients who met the criteria for posttraumatic stress disorder (PTSD) had symptoms of PTSD before being diagnosed as CRPS, with the remaining 14% of patients developing PTSD during the course of CRPS.46 However, research findings on how psychological factors contribute to the development of CRPS are controversial.

CLINICAL MANIFESTATIONS

The main characteristics of CRPS include spontaneous pain, hyperalgesia, allodynia, and abnormal vasomotor and sudomotor activities.36 Psychological dysfunction frequently manifests during the course of CRPS. The signs and symptoms of CRPS can vary widely between patients and over the course of the disease (Table 3).47

Signs and symptoms of CRPS

Most adult patients diagnosed with CRPS-I or CRPS-II exhibit a combination of sensory gain and loss.48 Patients with CRPS may complain of localized, intense somatic tissue pain that is burning, throbbing, squeezing, aching, or shooting.49 The pain typically progresses from the site of the initial injury, and may affect the entire limb in its most-extreme manifestation, or even the limb on the opposite side in rare cases.50 One-third of CRPS patients have severe allodynia, which is more common in the chronic stage and is considered to be caused by central nociceptive sensitization.51 Patients who have allodynia frequently adopt a protective posture to safeguard the injured extremity. Many CRPS patients are unable to use the affected extremity due to movement exacerbating the pain. CRPS-related pain does not have a dermatomal or nerve root distribution, and typically is not related to a distinct nerve lesion. Most CRPS patients experience some type of motor dysfunction,36,52,53 such as tremor, restricted range of motion, muscle weakness, or the affected limb being fixed in a long-term position (dystonia).52 Additionally, CRPS patients frequently move more slowly or more inaccurately when performing specific movements with the affected limb.54-56 Trophic changes such as osteoporosis, fibrosis, thin or shiny skin, aberrant nail growth, and changes in hair growth may be present, especially in the chronic stage. Sudomotor dysfunction (hyperhidrosis or hypohidrosis) can also occur in CRPS patients.36,48 Vasomotor or sudomotor dysfunction is a sign of an unstable sympathetic nervous system. Significant changes in skin temperature and (in particular) color occur over time and are not constant manifestations,57 with the limb initially having a dry, hot, and pink appearance in the classic presentation, but later becoming blue, cold, and hyperhydrotic.58 Usually the skin temperature differs by more than 1°C between the affected and unaffected limbs.59 Regardless of the skin color or temperature, edema is observable in almost all patients at the initiation of symptoms.36 This occurs less frequently as the disease becomes present for longer, but at least 40% of patients with chronic diseases still experience edema.51

It has long been believed that CRPS develops in three separate phases: (1) an acute phase characterized by the predominance of pain, sensory abnormalities, edema, sudomotor dysfunction, and possible motor function symptoms; (2) a dystrophic phase when trophic and substantial motor alterations arise, pain and sensory dysfunction become more pronounced, and vasomotor abnormalities persist; and (3) an atrophic phase where motor and trophic changes progress, vasomotor disturbances persist, and pain and sensory problems lessen.60

DIAGNOSTIC CRITERIA

Reflex sympathetic dystrophy was first identified using the Veldman criteria in 1993 (Table 4).36 There are no specific tools or equipment required to fulfill these criteria. The International Association for the Study of Pain (IASP) published the first CRPS diagnostic criteria in 1994. These criteria later became known as the Orlando criteria (Table 4),61 and the subsequent establishment of the Budapest criteria followed further work by a consensus group.6

Criteria for diagnosing CRPS

The Budapest Research Criteria were established by Harden et al.,62 and were subsequently adopted as new criteria for diagnosing CRPS. Sensory abnormalities, temperature asymmetry, color changes, edema, sweating, and motor dysfunction were the most important contributing factors. These criteria closely reflected criteria proposed by Harden and Bruehl in 1999.63,64 A consensus meeting was convened by the IASP in 2003 with the goal of improving the IASP diagnostic criteria for CRPS, which yielded new criteria known as the Budapest criteria.6 The Budapest criteria are currently the most widely used diagnostic criteria since they have recently been validated as having higher specificity than the earlier criteria (Table 4).15 The Budapest criteria were compared with the IASP criteria in order to distinguish between CRPS-I and other types of neuropathic pain during the initial validation of these criteria in 2010.15 That study found excellent diagnostic sensitivity for both the IASP criteria (100%) and the Budapest criteria (99%), but the specificity was higher for the Budapest criteria (68%) than for the IASP criteria (41%).15 The diagnostic validity of the Budapest criteria has been assessed in four studies, which have produced varying results, with the sensitivity ranging from 45% to 99% and the specificity ranging from 68% to 85%.11,14,64 Despite broad agreement on its application, the Budapest criteria for clinically diagnosing CRPS-I and CRPS-II might not be applicable to all populations or all neurological disorders, including poststroke CRPS.64

EVALUATION

There are no specific laboratory diagnostic tools for CRPS, and so it is diagnosed clinically. However, various diagnostic tools are frequently used to support the diagnosis of CRPS (Table 5). Additionally, several tests are used to evaluate autonomic function and aid in excluding other diseases. Careful physical and neurological examinations should be applied to patients with suspected CRPS. To help rule out infection and rheumatological problems, general laboratory tests such a full blood count, C-reactive protein, erythrocyte sedimentation rate, and serum autoantibodies are recommended. To rule out nerve lesions, nerve conduction velocity tests and electromyography should be performed. Somatosensory evoked potential studies and transcranial magnetic stimulation of motor pathways should be additionally used to assess central pathways. Bedside sensory testing or even quantitative sensory testing may be useful for identifying small-fiber impairment. These include the quantitative sudomotor axon reflex test (QSART), thermography, and laser Doppler flowmetry for testing sudomotor function and peripheral vasoconstrictor responses. The use of thermography is predicated on the existence of unilateral vasomotor disruption, which causes detectable temperature differences between limbs.36 However, normal symmetrical thermographic findings do not rule out a CRPS diagnosis. In both the acute and chronic stages of the disease, quantitative analysis of sudomotor activity may reveal abnormal sweat production of the affected extremity.65 A provocative test called the QSART measures the amount of sweat produced in response to a cholinergic challenge, such as acetylcholine.

Diagnostic tests for CRPS

Numerous imaging methods including plain radiography, bone scintigraphy, computed tomography, MRI, positron-emission tomography, and single-photon-emission computed tomography are the most beneficial for ruling out alternative diagnoses. Although three-phase bone scintigraphy has long been regarded as an objective diagnosis method, it is insufficient for diagnosing CRPS.66 However, CRPS is considered to be characterized by a pattern of increased uptake in all three phases, particularly diffuse periarticular uptake in and around the joints of the affected extremity during the delayed phase, especially during the first 6 months of CRPS.66 Identifying patients who might benefit from bisphosphonate therapy may require the use of bone scan.67,68 Additionally, MRI can reveal periarticular bone-marrow edema, soft-tissue swelling, joint effusions, and atrophy of periarticular structures in later stages.69 In a subgroup of CRPS patients, sympathetically maintained pain can be identifying by applying a diagnostic block of sympathetic nerves using local anesthetic.70 A more-permanent sympathetic block can then be achieved percutaneously using phenol or radiofrequency ablation if sympathetic blockade significantly reduces pain.71,72

DIFFERENTIAL DIAGNOSIS

Various disorders including as inflammatory disorders, nervous system disorders, and vascular diseases are included in the differential diagnosis of CRPS (Table 6).73,74

Differential diagnosis

CONCLUSION

CRPS is a complex disorder that is notoriously difficult to treat and frequently manifests with permanent debilitating sequelae. There is no single standard diagnostic test to confirm the diagnosis, but these patients can be identified using well-established clinical criteria. Although there have been considerable advances since the early definitions, the current knowledge of CRPS remains insufficient. A better understanding of the mechanisms underlying this disorder requires larger clinical investigations of higher quality. This will lead to faster diagnoses and the development of more precisely targeted treatments.

Notes

Conflicts of Interest

The author has no potential conflicts of interest to disclose.

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Article information Continued

Fig. 1.

Hypothetical model of mechanisms interacting in the development of complex regional pain syndrome. PTSD, post-traumatic stress disorder; CGRP, calcitonin-gene-related peptide; IL, interleukin; TNF, tumor necrosis factor.

Table 1.

Synonyms for CRPS

Synonyms for CRPS
Reflex sympathetic dystrophy
Sudeck’s atrophy
Causalgia
Minor causalgia
Mimocausalgia
Algodystrophy
Algoneurodystrophy
Posttraumatic pain syndrome
Painful posttraumatic dystrophy
Painful posttraumatic osteoporosis
Transient migratory osteoporosis

CRPS, complex regional pain syndrome.

Table 2.

The various pathophysiologies of CRPS

The various pathophysiologies of CRPS
Psychological factors
Depression
PTSD
Immobilization
Hyperactivity of the sympathetic nervous system and vasomotor disturbance
Neurogenic inflammation
Deep-tissue microvascular pathology
Autonomic dysregulation and small-fiber neuropathy
Central processes
Cortical reorganization
Central changes in pain processing
Genetic predisposition
Genetic factors
Epigenetic factors
Autoimmunity

CRPS, complex regional pain syndrome; PTSD, post-traumatic stress disorder.

Table 3.

Signs and symptoms of CRPS

Pain not proportionate to the inciting injury Symptoms spread to another limb
Movement disorder, such as weakness, spasms, dystonia, myoclonus, atrophy, or decreased range of motion Visceral pain
Insomnia or other sleep disorder Hyperhidrosis
Neurogenic edema/swelling Tremor
Changes in skin color Nail changes
Hyperemia Hair changes
Hyperesthesia Body-temperature asymmetry

CRPS, complex regional pain syndrome.

Table 4.

Criteria for diagnosing CRPS

A. Veldman criteria
1. Presence of four of the five following signs/symptoms:
a. Unexplained diffuse pain
b. Different skin color from the other limb
c. Diffuse edema
d. Different skin temperature from the other limb
e. Limited range of motion
2. Occurrence or increase in the above signs and symptoms after use
3. The above signs and symptoms are present in an area larger than the area of the primary injury or operation and include the area distal to the primary injury.
B. Original 1994 IASP criteria (Orlando criteria)
1. Presence of an initiating noxious event, or a cause of immobilization
2. Continuing pain, allodynia, or hyperalgesia in which the pain is disproportionate to any known inciting event
3. Evidence at some time of edema, changes in skin blood flow, or abnormal sudomotor activity in the region of pain (can be a sign or symptom)
4. This diagnosis is excluded by the existence of other conditions that would otherwise account for the degree of pain and dysfunction.
C. Harden-Bruehl criteria/Budapest criteria
- General definition of the syndrome: CRPS describes an array of painful conditions that are characterized by continuing (spontaneous and/or evoked) regional pain that is seemingly disproportionate in time or degree to the usual course of any known trauma or other lesion. The pain is regional (not in a specific nerve territory or dermatome) and usually has a distal predominance of abnormal sensory, motor, sudomotor, vasomotor, and/or trophic findings. The syndrome shows variable progression over time.
- Establishing the clinical diagnosis requires the following criteria to be met:
1. Continuing pain, which is disproportionate to any inciting event
2. Presence of at least one symptom in three of the four following categories:
a. Sensory: hyperesthesia and/or allodynia
b. Vasomotor: temperature asymmetry, skin-color changes, and/or skin-color asymmetry
c. Sudomotor/edema: edema, sweating changes, and/or sweating asymmetry
d. Motor/trophic: decreased range of motion, motor dysfunction (weakness, tremor, or dystonia), and/or trophic changes (in hair, nail, or skin)
3. Presence of at least one sign at the time of evaluation in two of the following four categories:
a. Sensory: hyperalgesia (to pinprick) and/or allodynia (to light touch) and/or temperature sensation and/or deep somatic pressure and/or joint movement
b. Vasomotor: temperature asymmetry (> 1°C), skin-color changes, and/or symmetry
c. Sudomotor/edema: edema, sweating changes, and/or sweating asymmetry
d. Motor/trophic: decreased range of motion, motor dysfunction (weakness, tremor, or dystonia), and/or trophic changes (in hair, nail, or skin)
4. No other diagnosis that better explains the signs and symptoms
- For research purposes the diagnostic decision rule is that there should be at least one symptom in all four symptom categories and at least one sign (observed at evaluation) in two or more of the sign categories.

CRPS, complex regional pain syndrome; IASP, International Association for the Study of Pain.

Table 5.

Diagnostic tests for CRPS

Diagnostic tests
Plain radiography (only in the chronic stage)
Bone scintigraphy (only in the acute stage)
Quantitative sensory testing
Bone mineral density
MRI (e.g., of skin or joints), computed tomography
Skin biopsy
Three-phase bone scintigraphy
QSART
Thermography
Laser Doppler flowmetry
Nerve conduction study
Electromyography

CRPS, complex regional pain syndrome; QSART, quantitative sudomotor axon reflex test; MRI, magnetic resonance imaging.

Table 6.

Differential diagnosis

Bone or soft-tissue injury Stress fractures
Ligament damage
Neuropathies Due to peripheral nerve damage, entrapment, or compression
Due to central nervous system or spinal lesions
Diabetic neuropathy
Infection (e.g., Lyme disease) or postherpetic neuralgia
Guillain-Barre syndrome (chronic inflammatory demyelinating polyneuropathy)
Erythromelalgia
Thoracic outlet syndrome
Vascular disorders Raynaud’s disease
Arterial insufficiency due to atherosclerosis, trauma, or Burger’s disease
Phlebothrombosis
Deep-vein thrombosis
Angiomatosis
Lymphedema
Compartment syndrome
Inflammatory/autoimmune disorders Arthritis, including reactive arthritis and rheumatoid arthritis
Multiple sclerosis
Cellulitis
Infections Viral, fungal, or bacterial infections of bone, joints, soft tissue, or skin
Toxic exposure Vinca alkaloids (antitumor agents) or heavy metals
Psychological Somatoform disorders, including conversion disorder
Malingering, factitious disorder