Phantom Sensations

Phantom sensations are nonpainful perceptions that occur in the region of the missing body part after a traumatic or surgical amputation. Phantom sensations are common after limb amputation surgery, with an incidence of 90% during the first 6 months. One third of patients experience phantom sensations within 24 hours after their surgery. Excision of a body part, however, is not essential for phantom sensations. Phantom sensations of the arm have been reported after avulsion of the brachial plexus without amputation of the limb. Excision of other body parts—such as the tongue, bladder, rectum, breast, or genitalia—may also present with phantom sensations.

Phantom sensations may present with various manifestations including kinetic sensations and kinesthetic and exteroceptive perceptions. Kinetic sensations are exemplified by perception of movements in the amputated body region, such as flexion/extension of the toes. Kinesthetic perceptions are characterized by distorted representations in size or position of the missing body part (e.g., feeling that the hand or foot is twisted). Exteroceptive perceptions can include paresthesias, tingling, touch, pressure, itching, heat, cold, and wetness. Complete paraplegic and quadriplegic patients can also have phantom sensations. Phantom sensations are commonly experienced in the distal portion of the limbs—hands and feet—possibly due to the rich innervation of these regions and the disproportionately large cortical representation of these regions in the homunculus.

Telescoping

Phantom limbs are also associated with a phenomenon called “telescoping”: the perception of progressive shortening of the phantom body part resulting in the sensation that the distal part of the limb is becoming more proximal. At the start of the phenomenon, the phantom sensation can feel so real that the patient may actually reach for objects or attempt to ambulate with a phantom leg. However, over time, phantom sensations of the distal extremities may change and become less distinct so that the patient may feel a hand close to the end of the residual limb but not feel the proximal arm or forearm. This phenomenon is common, occurring in up to two thirds of limb amputees.

Phantom Pain

Phantom pain, often referred to as phantom limb pain (PLP), is the perception of dysesthesias, or unpleasant sensations, in the distribution of the missing or deafferentated body part. PLP has been reported to occur in up to 79% of postamputation patients 6 months after surgery, with about 60% of patients still reporting significant PLP 2 years after surgery. The pain can vary in character, duration, frequency, and intensity. It can present as sharp, dull, burning, squeezing, cramping, shooting, or as a shocklike electrical sensation. Patients may occasionally complain of intermittent tremors or painful muscle spasms in the stump associated with paroxysms of PLP.

In a prospective study by Jensen and colleagues of 58 patients undergoing limb amputation, the authors found that PLP often changed in presentation within the first 6 months after amputation. The characteristic of the phantom pain changed from a mainly exteroceptive-like pain (knifelike or sticking) localized in the entire limb or at least involving proximal parts of the lost limb to a mainly proprioceptive type of pain (squeezing or burning) localized in the distal parts of the amputated limb. Forty-seven percent of patients experienced phantom pain within 24 hours after the amputation and 83% within the first 4 days. The study also demonstrated that the frequency, duration, and severity of PLP decreased during the first 6 months, after which the characteristics did not change significantly. Sometimes PLP can resolve spontaneously without treatment. Similar to other neuropathic conditions, PLP persisting longer than 6 months is extremely difficult to treat.

The incidence of PLP seems to be independent of the patient’s age, sex, previous health status, and cause of amputation. One factor that appears to increase its incidence after amputation is the presence of pain in the limb before the amputation. In a prospective study of 56 patients who had amputation of a lower limb, Nikolajsen and colleagues noted that the presence of preamputation pain significantly increased the incidence of both residual limb pain (RLP) and PLP after 1 week and the incidence of PLP after 3 months. Approximately 42% of the patients reported that their PLP at 3 months resembled the pain they had experienced at the time of amputation. Associations of PLP with phantom sensations and between PLP and RLP have also been demonstrated for upper limb amputees.

Residual Limb Pain

RLP, classically referred to as “stump pain,” is pain localized to the residual body part following amputation. Longitudinal studies previously reported an incidence of RLP of about 20% 2 years after amputation. However, more recent studies with longer duration of follow-up report an incidence of 56%–74%. RLP is often secondary to local pathologic processes such as infection; lesions of the skin, soft tissue, or bone; heterotopic ossification (>50% in traumatic amputations); and local ischemia. These processes can generally be classified into the following categories: postsurgical nociceptive, neurogenic, prosthogenic, arthrogenic, ischemic, referred (usually from the spine or joints), sympathetically maintained, and abnormal residual limb tissue (e.g., adhesive scar tissue). RLP can be superficial (localized to the scar region of the incision), felt deep in the distal residual limb, or encompassing the whole residual limb. RLP can frequently be differentiated from PLP based on the fact that it is classically provoked or exacerbated by traction or pressure, which often occurs during the use of a prosthesis. This factor can greatly limit function in lower extremity amputees. The management of RLP entails a detailed history and physical examination that includes ensuring a properly fitting prosthesis. Arthrogenic RLP is usually secondary to abnormal gait and asymmetrically distributed weight bearing, resulting in excessive stress on adjacent joints and/or lumbosacral spine structures. This can lead to bursitis, accelerated arthritis, sacroiliac joint disease, discogenic and facetogenic pain, and lumbosacral radiculopathy.

Phantom Phenomena After Mastectomy

Well over 100,000 mastectomies are performed each year in the United States. Recent studies indicate that phantom sensations are felt by 14%–48% of patients who underwent mastectomy. Most of these phantom sensations are felt intermittently, occurring once every 2 or 4 weeks. The incidence of phantom pain after mastectomy appears to be lower than that after limb amputation, ranging from 0% to 23%. This lower incidence may be related to the smaller cortical representation of breasts and the fact that breasts do not mediate kinesthetic sensory impulses. The onset of phantom sensation often appears within 3–6 months of surgery and begins to dissipate after 1 year. The phantom pain usually localizes to the entire breast or around the nipple. The relationship between preamputation pain and phantom pain or phantom sensations appears to be less after mastectomy than after limb amputation. There is, however, a striking similarity in the location and character of the pain before and after mastectomy, a phenomenon seen after other amputations. The relationship between phantom pain and preamputation pain is more significant within the first month after mastectomy. In view of the high incidence of pain after breast surgery in general, the only way to distinguish between true “phantom” pain and other sources of postmastectomy pain (e.g., intercostal brachial neuralgia, neuroma) may be via a detailed history and physical examination.

Wounded Warriors

The US military conflicts since 9/11 have placed more emphasis on the management of traumatic amputation and its complications. As of June 2015, the Department of Defense reports that 1645 individuals have suffered major limb loss since September 2001, including approximately 17% with upper extremity amputations and 30% with multiple limb loss. A majority of these injuries are related to blast exposures; therefore many have concomitant comorbidities including traumatic brain injury, posttraumatic stress disorder, peripheral nerve injuries, fractures, and soft tissue injuries. Studies have shown a higher prevalence of chronic pain among individuals with posttraumatic stress and traumatic brain injury than in similar cohorts without these conditions.

The unique mechanisms of injury and related comorbidities associated with amputations in military service members present management challenges that may not be similar to those in other patient populations with PAP. In a study of traumatic amputations in sustained by 30 military personnel during combat or training, the prevalence of PLP was similar (77%), but RLP was higher (87%) than previously reported. In addition, the average (3.3) and worst (5.4) pain intensity as measured on a numerical rating scale was less than in other amputee populations.

Pharmacotherapy

Most medication options for PAP require extrapolation from the treatment of other conditions. For somatic pain, acetaminophen, nonsteroidal antiinflammatory drugs, and/or opioids may be indicated. Neuropathic pain is more likely to respond to adjuvant analgesics such as tricyclic antidepressants (e.g., nortriptyline), anticonvulsants (e.g., gabapentin), or selective norepinephrine reuptake inhibitors (e.g., duloxetine). The results of available randomized controlled trials specifically for the pharmacologic treatment of PAP are summarized in Table 29.1 , and some are discussed here.

TABLE 29.1

Randomized Controlled Trials Evaluating Pharmacologic Treatments for Postamputation Pain

Study	N	Treatment/Placebo	Chronicity a	Adverse Events	Follow-Up	Effect b
Antidepressants
Robinson et al.	39	1. Oral amitriptyline 10 mg/day titrated to max 125 mg/day 2. Oral benztropine 0.5 mg/day	>3 months	Dry mouth, dizziness	6 weeks	−
Wilder-Smith et al.	94	1. Oral amitriptyline (avg 55 mg/day) 2. Oral tramadol (avg 200 mg/day) 3. Placebo	10–16 years	Nausea, tiredness, dizziness, constipation, headache (all more common with tramadol)	1 month	+
Anticonvulsants
Bone et al.	19	1. Oral gabapentin titrated to 2400 mg/day 2. Placebo	>6 months	Somnolence, dizziness, headache, nausea	6 weeks	+
Smith et al.	24	1. Oral gabapentin titrated to 3600 mg/day 2. Placebo	>6 months	Not described	6 weeks	−
Nikolajsen et al.	46	1. Oral gabapentin 2400 mg/day 2. Placebo	POD #1 (prevention)	Nausea, stomachache, fatigue, confusion, nightmares, itching, ataxia	6 months	−
NMDA Antagonists
Nikolajsen et al.	11	1. IV ketamine 0.5 mg/kg infusion ×45 min 2. Placebo	Avg. 4 years	Insobriety, mood elevation, discomfort	45 min	+
Eichenberger et al.	20	1. IV ketamine 0.4 mg/kg infusion ×1 h 2. IV calcitonin 200 IU infusion ×1 h 3. Combo ketamine/calcitonin 4. Placebo	Avg. 12 years	Loss of consciousness, light visual hallucination, hearing impairment (all with ketamine); facial flushing (calcitonin)	48 h	+
Ben Abraham et al.	10	1. Oral dextromethorphan 120 mg/day ×10 days 2. Oral dextromethorphan 180 mg/day ×10 days 3. Placebo	Avg. 4.8 months	None reported	10 days	+
Maier et al.	36	1. Oral memantine 30 mg/day ×3 weeks 2. Placebo	>12 months	Vertigo, fatigue, headache, nausea, restlessness, excitation, cramps	3 weeks	−
Schwenkreis et al.	16	1. Oral memantine 30 mg/day 2. Placebo	>12 months	Not described	3 weeks	−
Wiech et al.	8	1. Oral memantine 30 mg/day ×4 weeks 2. Placebo	Chronic	Fatigue, agitation, dizziness, nausea, headache	30 days	−
Calcitonin
Jaeger and Maier	21	1. IV calcitonin 200 IU ×20 min infusion 2. Saline infusion	0–7 days postamputation	Headache, vertigo, nausea, vomiting, augmented phantom sensations, drowsiness, hot flashes	1 year	+
Eichenberger et al.	20	1. IV ketamine 0.4 mg/kg infusion ×1 h 2. IV calcitonin 200 IU infusion ×1 h 3. Combo ketamine/calcitonin 4. Placebo	Avg. 12 years	Loss of consciousness, light visual hallucination, hearing impairment (all with ketamine); facial flushing (calcitonin)	48 h	+
Opioids
Huse et al.	12	1. Oral morphine up to 300 mg/day 2. Placebo	Chronic	Constipation	4 weeks	+
Wu et al.	32	1. IV morphine 0.2 mg/kg infusion ×40 min 2. IV lidocaine 4 mg/kg infusion ×40 min 3. IV diphenhydramine 40 mg infusion (placebo)	>6 months	Sedation	30 min	+
Wilder-Smith et al.	94	1. Oral amitriptyline (avg. 55 mg/day) 2. Oral tramadol (avg 200 mg/day) 3. Placebo	10–16 years	Nausea, tiredness, dizziness, constipation, headache (all more common with tramadol)	1 month	+
Wu et al.	56	1. Oral morphine (180 mg/day) 2. Oral mexiletine (1200 mg/day) 3. Placebo	>6 months	Constipation, nausea, drowsiness, dizziness (all more common with morphine)	6 weeks	+ (morphine only)

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