Brachial Plexus injuries, or brachial plexopathies, are considered among the most devastating of neurological injuries. Numerous mechanisms of injury leading to these afflictions exist, including traction injuries (falls, sports injuries, obstetric), compression injuries (crutches, pack straps, surgical malpositioning), lacerations from penetrating trauma, ischemia, and neoplastic disease. Since most nerves of the brachial plexus are mixed nerves containing both motor and sensory components, patients usually present with some combination of weakness and sensory deficit in the upper extremity, within the distribution of the injured root, trunk, cord, or branch of the brachial plexus. Thorough history and physical examination are the first steps in evaluation of brachial plexopathies and provide valuable clues as to the anatomical location of the injury, as well as the extent of the injury. Based on a provisional diagnosis derived from the physical exam, radiographic imaging and electrodiagnostic studies are then used to further pinpoint the location and severity of injury. Here, we focus on the use of electromyography and nerve conduction studies in the diagnosis and prognostication of brachial plexopathies.

The brachial plexus is an interwoven “netting” of nerves, which are bundles of axons belonging to nerve cells or neurons. These specific neuronal cells originate in in the dorsal horn (sensory) and ventral horn (motor) of the spinal cord from the C5-T1 levels. Nerve roots are mixed nerves containing both sensory and motor axons and are the first bundles of axons which leave the spinal cord and exit the spinal canal. Weaving of these fibers first forms trunks, then divisions, cords, and finally, the terminal nerve branches. The five terminal nerve branches are, the axillary, musculocutaneous, median, radial, and ulnar nerves.

Roots emerge from the spinal canal and travel laterally between the anterior and middle scalene muscles, and deep to the trapezius muscle. After a short distance the 5 roots (C5-T1) merge to form three trunks (superior, middle, inferior). These trunks travel laterally superficial to the first rib and beneath or deep to the clavicle. As these trunks pass under the clavicle to enter the axilla, each trunk divides into two divisions to form six total divisions (three anterior and three posterior). These six divisions then shortly merge to form three cords, which are named for their position relative to the axillary artery (medial, lateral, posterior). Finally, as the cords travel to exit the axilla and enter the arm medial to the humerus, they divide into the five terminal branches or nerves supplying the upper extremity: the axillary, musculocutaneous, median, radial, and ulnar nerves. Lesions along any region of the brachial plexus will produce characteristic presentations of sensory deficit and weakness that can be elicited in the history and physical exam and must be ascertained prior to electrodiagnostic evaluation.

There are many different mechanisms of injury to the brachial plexus. The most common of which is avulsion injury. Iatrogenic surgical trauma, penetrating trauma, compression injuries, ischemia, and neoplastic invasion are less common but possible mechanisms as well.[1]

The area of the brachial plexus most commonly injured is the supraclavicular zone. This is due to the fact that this zone is the most anatomically exposed portion and is most susceptible to avulsion injury due to excessive cervical or upper extremity motion during traumatic mechanisms of injury. Upper roots (C5-C7) and upper trunk are most commonly affected, usually secondary to violent lateral flexion of the head away from the ipsilateral shoulder, or violent head rotation away from the ipsilateral shoulder. A common example of this is Erb’s palsy secondary to birth trauma. Lower root avulsion is far less common and is due to violent abduction of the ipsilateral arm above the head, such as when hanging from the arm from an elevated height. Supraclavicular injuries typically present with “Erb’s Palsy”, or an internally rotated and adducted shoulder, with a pronated forearm. Infraclavicular injuries present with “Klumpke’s Palsy”, or “claw hand deformity” with unopposed forearm supination, extension at the wrist and metacarpophalangeal joints, with flexion at the interphalangeal joints.[1][2][3][4]

Penetrating and compressive trauma can affect any exposed portion of the brachial plexus. Examples of this include penetrating trauma in the arm affecting terminal nerve branches, compressive injuries in the infraclavicular region secondary to crutch use, or in the supraclavicular region secondary to strap compression from packs.[5][6]

Clinical presentation will depend on the nerve(s) affected, therefore, in depth knowledge of the function of each terminal nerve, as well as the anatomical contribution of the brachial plexus to that particular distribution, is vital to understanding the origin of the pathology along the plexus[1]:

• Axillary: C5-C6 root and posterior cord origin. Innervates deltoid and teres minor muscles. Sensory innervation to superior lateral cutaneous nerve. Deficits after injury include paralysis of these muscles, resulting in loss of abduction of the arm at the shoulder from 15-90 degrees, and sensory deficit over the upper lateral arm superficial to the deltoid muscle.
• Musculocutaneous:C5-C7 root and lateral cord origin. Innervates the coracobrachialis, biceps brachii, and brachialis muscles. Sensory innervation to lateral cutaneous nerve of the forearm. Deficits after injury include loss of flexion of the arm at the elbow, loss of supination of the forearm, and sensory deficit over the lateral aspect of the forearm.
• Median: C5-T1, lateral cord, and medial cord origin. Innervation to all forearm flexor muscles except flexor carpi ulnaris, and the part of flexor digitorum profundus which supplies digits 4 and 5. The median nerve also supplies the first and second lumbrical muscles, and as well as the muscles of the thenar eminence, via the recurrent thenar branch. Sensory innervation is to the palmar aspect of the first three and half of the fourth digit. A proximal median nerve injury results in loss of forearm pronation, weakness in wrist flexion, loss of flexion in the first three digits, loss of opposition and abduction of the thumb, and sensory loss over the palmar aspect of the first three and a half digits. There is an “ape hand” deformity at rest, and “benediction sign” when attempting to form a fist.
• Ulnar: C8-T1 and medial cord origin. Innervation to flexor carpi ulnaris, flexor digitorum profundus (medial half), hypothenar muscles, and the third and fourth digital lumbricals. Sensory innervation is to palmar and dorsal cutaneous branches of the hand, which supply sensory innervation to entire medial 1.5 digits. Deficits after proximal injury include weakness of flexion of the wrist, loss of flexion in the 4 and 5 digits and sensory loss over entire medial 1.5 digits. “Claw hand” deformity is typically seen at rest.
• Radial: C5-T1 and posterior cord origin. Innervation to triceps brachii, brachioradialis, and extensor muscles of the forearm. Sensory innervation is to posterior cutaneous, inferior lateral cutaneous, and posterior lateral cutaneous nerves. Deficits after proximal injury include loss of extension of the forearm, weakness of supination, and loss of extension of the hand and fingers. Sensory deficit is over the lateral arm, much of the posterior aspect of the forearm, radial half of the dorsum of the hand, and dorsal aspect of the radial 3 ½ digits.

Knowing these anatomical contributions and deficits allows the examiner to use the presenting history and physical as a starting point. Electrodiagnosis can then be used to trace backwards along the affected distribution in order to pinpoint the exact location. For more detail on this technique see the “technique” section below.

Electrodiagnostic studies may be used to confirm, localize, prognosticate, age, and grade severity of neurological injuries and/or diseases. They can also be used to differentiate axonal vs demyelinating lesions, motor vs sensory vs autonomic lesions, and diffuse vs focal vs multifocal lesions. It may also be used to differentiate myopathies from neuromuscular junction disorders and traumatic injuries. The specifics of how each of these is accomplished is beyond the scope of this discussion. Of note, lesions which are limited to A-delta and C fibers will most commonly produce completely normal electrodiagnostic studies. [7][8]

There are no absolute contraindications to electrodiagnostic studies. Electrodiagnosis has even been deemed safe in pregnant patients to date. These are generally well tolerated by the patient, however, a certain subset of patients will be “electrically sensitive” and will not tolerate the procedure well. The following are relative contraindications to the procedure:

• Infection at the site of needle insertion for EMG. Sites of superficial infection should be avoided.
• Electrical sensitivity. Delivery of electrical impulses during electrodiagnostic studies are safe and generally well tolerated. In patients with indwelling pacemaker wires or central lines, leak currents have the potential to reach the heart directly resulting in arrhythmia. Electrical stimulation near these devices should be avoided.[9]
• Areas where edema/lymphedema is present have been postulated to have a higher rate of infection and are generally avoided, although no cases reports of lymphoedema-related complications of EMG have been reported.
• The most common reported complication of EMG is pain at the site of needle insertion. Some patients simply will not tolerate the pain of electrode needle insertion. [10]
• Patients who are on chronic anticoagulation or those who have a coagulation disorder are predisposed to excessive bleeding. In these patients, needle insertion should be limited to superficial muscles.[11]

Commercially available EMG and NCS machines are available and typically contain the following components:

• Computer- for processing and graphing of electrical signals.
• Speakers- produce audible feedback directly related to levels of electrical activity.
• Printer- for graphical red-outs
• Amplifier- amplifies minute electrical activity to a level which can be recorded and interpreted.
• Stimulator- produces the applied electrical stimulus.
• Surface electrodes- for stimulation and recording electrical impulses along skin during NCS.
• Disposable needle electrodes- for recording electrical impulses during EMG.