Neuromuscular I Flashcards
giant axonal neuropathy (GAN)
autosomal recessive disorder that manifests in early childhood. Predominantly axonal Sensorimotor neuropathy, corticospinal tract involvement with upper motor neuron signs, and optic atrophy leading to vision loss.
Neuropath large focal axonal swelling that contains tightly packed disorganized neurofilaments. GAN gene that encodes for gigaxonin
Refsum’s disease (RD)
autosomal dominant peroxisomal disorder. Fatty acid metabolism, leading to accumulation of an intermediate in this pathway, phytanic acid. retinitis pigmentosa (with night blindness and visual field constriction), cardiomyopathy, and skin change. Large-fiber sensorimotor neuropathy, hearing loss, anosmia, ataxia, and cerebellar signs
Rx reduce dietary intake of phytanic acid
F wave obtained by?
after supramaximal stimulation of a motor nerve.
Significant axon loss lesions?
produce reductions in action potential amplitudes and tend to have preserved or mildly reduced conduction velocities
NCS modalities?
sensory and motor conduction studies.
Sensory NCS
stimulating a sensory nerve while recording the transmitted potential at a different site along the same nerve. Three main measures can be obtained: SNAP amplitude, sensory latency (onset and peak), and conduction velocity.
SNAP
amplitude (in microvolts) represents a measure of the number of axons conducting between the stimulation site and the recording site.
Sensory latency
(in milliseconds) is the time that it takes for the action potential to travel between the stimulation site and the recording site of the nerve.
conduction velocity
is measured in meters per second and is obtained dividing the distance between stimulation site and the recording site by the latency: Conduction velocity = Distance/Latency.
Motor NCS
are obtained by stimulating a motor nerve and recording at the belly of a muscle innervated by that nerve
Motor CMAP
CMAP is the resulting response, and depends on the motor axons transmitting the action potential, status of the neuromuscular junction, and muscle fibers.
CMAP/SNAP interpretation
prolonged latencies and slow conduction velocities correlate with demyelination, decrease in the amplitudes correlates with axon loss lesions.Low amplitudes can result from demyelinating conduction block when the nerve stimulation is proximal to the block.
F-wave
F-wave is obtained after supramaximal stimulation of a motor nerve while recording from a muscle.travels antidromically (conduction along the axon opposite to the normal direction of impulses) along the motor axons toward the motor neuron, backfiring and then traveling orthodromically (conduction along the motor axon in the normal direction) down the nerve to be recorded at the muscle.
H-wave
H-reflex is the electrophysiologic equivalent of the ankle reflex (S1 reflex arc) and is obtained by stimulating the tibial nerve at the popliteal fossa while recording at the soleus. The electrical impulse travels orthodromically through a sensory afferent, enters the spinal cord, and synapses with the anterior horn cell, traveling down the motor nerve to be recorded at the muscle.
Large polyphasic motor unit potentials (MUPs)
seen in acute neuropathic lesions, but rather in chronic ones.
Insertional activity
is recorded as the needle is inserted into a relaxed muscle. It is increased in denervated muscles and myotonic disorders, and is decreased when the muscle is replaced by fat or connective tissue and during episodes of periodic paralysis
Spontaneous activity
is assessed with the muscle at rest, and examples include fibrillation potentials, fasciculation potentials, and myokymia and myotonic potentials. All spontaneous activity is abnormal.
Voluntary contraction
MUPs are obtained while the needle is inserted into the muscle during voluntary contraction. Characteristics include recruitment pattern and MUP morphologic features, such as duration, amplitude, and configuration.
Recruitment
is a measure of the number of MUPs firing during increased force of voluntary muscle contraction
Axon loss lesions
reduced recruitment is characterized by a less-than-expected number of MUPs firing more rapidly than expected.
Myopathic processes
Early or rapid recruitment occurs in myopathic processes with loss of muscle fibers, in which an excessive number of short-duration and small-amplitude MUPs fire during the muscle contraction.
Poor voluntary effort or with CNS disorders
causing weakness, recruitment is reduced with normal MUPs firing at slow or moderate rates, sometimes in a variable fashion
neuropathic disorders with denervation and reinnervation
MUPs disclose increased duration and amplitude, and may be polyphasic
myopathic disorders
MUPs are of reduced duration and amplitude, and may also be polyphasic.
Radiculopathy NCS?
normal SNAPs despite sensory symptoms, because SNAPs are recorded distal to the lesion, in the postganglionic projections from the dorsal root ganglion. Thus radiculopathies are usually diagnosed with the needle EMG component rather than the NCS component of the electrodiagnostic study.
Radiculopathy path?
occurs from an intraspinal canal lesion resulting in damage of the preganglionic fibers. The cell body in the dorsal root ganglia and the postganglionic fibers remain unaffected, and therefore, even though sensory symptoms are prominent, the SNAPs are normal.
axon loss radiculopathy
injure motor fibers in the intraspinal canal region affecting the respective myotome. This leads to denervation, with fibrillation potentials seen 3 weeks after the onset of motor axon loss, decreased recruitment, and 3 to 6 months later, large and polyphasic motor unit potentials (MUPs). The presence of these large and polyphasic MUPs is dependent on reinnervation and collateral innervation, typically occurring in a proximal to distal fashion, with proximal muscles more successfully reinnervated as compared to distal muscles.
SFEMG
highly sensitive but not specific for MG, being frequently abnormal in other neuromuscular junction
Type 1 muscle fibers
also called slow-oxidative, have slow ATPase activity and large oxidative capacity, with large numbers of mitochondria. They are red in color and small in diameter.
Type IIa fibers
fast oxidative glycolytic fibers, and have fast ATPase activity, with high glycolytic capacity and moderate oxidative capacity. These fibers are fast and resistant to fatigue.
Type IIb fibers
fast-oxidative-glycolytic fibers, and have fast ATPase activity, with high glycolytic capacity but low oxidative capacity. These fibers are fast and fatigable. Their color is pale and diameter is large.
Demyelination cardinal features
conduction velocity is reduced (normal >50 m/s), peak latency is prolonged (normal is <4 ms) and CMAP amplitude dispersion
CIDP dx
CIDP is the diagnosis when symptoms progress or relapse beyond 8 weeks.
Peripheral nerve injury severity
can range from focal demyelination to axonal injury and finally nerve transection with discontinuity of the nerve. Electrophysiologic studies can help determine the degree of injury.
Focal nerve injury
segmental demyelination, which is characterized by the presence of slowing at a specific site, or the presence of a conduction block, which is a decrease in the CMAP amplitude with proximal stimulation as compared to distal stimulation, without significant temporal dispersion.
Axon loss lesion
Wallerian degeneration, which is typically completed in 7 to 10 days from the injury. After 10 days, the distal axon degenerates and can no longer conduct.Once denervation occurs, spontaneous muscle activity appears on EMG, manifested by fibrillation potentials, which usually appear after the third week from the injury.
GBS resp vitals
negative inspiratory force of less than −30 cc H2O or vital capacity of less than 15 to 20 mL/kg support elective endotracheal intubation.
Brachial plexus
C5 to T1 nerve roots
Roots
Two nerves that innervate the upper extremity branch off the nerve roots themselves. The dorsal scapular nerve, which innervates the rhomboids and levator scapulae, arises from the C5 nerve root. The long thoracic nerve, which innervates the serratus anterior, arises from the C5 to C7 roots.
Trunks
The ventral rami of the C5 to T1 nerve roots join to form the trunks of the brachial plexus. The upper (or superior) trunk, formed from the C5 and C6 nerve roots, gives off two branches: the suprascapular nerve, which innervates the supraspinatus and infraspinatus, and the nerve to subclavius. The point where the C5 and C6 nerve roots meet is called Erb’s point. The middle trunk is formed from the C7 root. There are no branches from the middle trunk. The lower (inferior trunk) is formed from the C8 and T1 roots. There are no branches from the inferior trunk. The trunks then divide into anterior and posterior divisions.
Cords
lateral cord gives rise to the lateral pectoral nerve, which innervates the pectoralis major. The lateral cord ends as two nerves, the median nerve and the musculocutaneous nerve. posterior cord ends as two nerves, the axillary nerve and radial nerve. The medial cord gives fibers to the median nerve and then continues as the ulnar nerve
familial amyloid polyneuropathy (FAP) type 1
polyneuropathy, autonomic features, and a family history.
familial amyloid polyneuropathy (FAP) type 2
carpal tunnel, a family history of carpal tunnel, mild predominantly sensory polyneuropathy, and absence of prominent autonomic features.
FAP 4
corneal dystrophy being a prominent early feature. In later life, cranial neuropathies and skin changes occur; cranial nerves VII, VIII, and XII are commonly affected.
FAP 3
FAP3 is similar to FAP1 in clinical manifestations, but with earlier renal involvement and more gastrointestinal involvement, with a higher incidence of duodenal ulcers.
FAP pathology
mutations in transthyretin, a plasma protein that is synthesized predominantly in the liver and transports thyroxine and other proteins.
Autonomic dysfunction resulting from diabetic neuropathy
resting tachycardia or bradycardia, loss of the respiratory variability of the heart rate, loss of the normal tachycardic response, orthostatic hypotension, and increased risk of silent myocardial infarction. Gastrointestinal abnormalities, Neurogenic bladder, impotence
Charcot–Marie–Tooth disease
hereditary sensorimotor neuropathies or peroneal muscular atrophy. group of inherited peripheral neuropathies. The CMTs can be divided into demyelinating, axonal, and combined demyelinating and axonal forms.
(CMT) 1
MT1A is due to a duplication in the peripheral myelin protein 22 (PMP22) gene on chromosome 17 related to myelin synthesis. hammertoes, high-arched feet, palpably enlarged nerves, two decades of life and include slowly progressive weakness, muscle atrophy, kyphosis. CMT 3 presents in infancy.
