Neurologic Examination and Lesion Localization
World Small Animal Veterinary Association World Congress Proceedings, 2005
Luisa De Risio, DMV, DECVN
Animal Health Department, Faculty of Veterinary Medicine, University of Parma
Italy

The neurological examination is the basic and most important tool of clinical neurology.

The neurological examination allows:

 to determine if the nervous system is affected by a disease process

 to localize the lesion within the nervous system (neuroanatomic diagnosis)

 to assess the severity of dysfunction

 to construct a list of differential etiological diagnoses (along with the information provided by the signalment, the history and the general physical examination)

These information are necessary to establish which diagnostic procedures are required (CBC, chemistry profile, serology, urinalysis, CSF analysis, survey radiographs, myelography, CT, MRI, electrodiagnostics, muscle/nerve biopsy, etc).

I would like to emphasize that performing the neuroanatomic diagnosis should always precede consideration of the differential etiological diagnoses and therefore of the diagnostic work-up.

Taking a thorough medical history and performing a detailed general physical examination are prerequisites to the neurological examination. This should be performed in a systematic manner and each result has to be recorded in a standard form so that no part of the examination is omitted. In certain cases, it might be necessary to modify the examination according to the chief complaint, the condition and cooperative attitude of the patient. For instance, in an animal presented with acute spinal trauma any manipulation that might exacerbate a possible vertebral instability (such as performing hopping and wheel-barrowing) should be avoided until an unstable vertebral injury has been ruled out. In addition, in order to perform and interpret correctly each test, it is of paramount importance to achieve and maintain patient cooperation throughout the examination. Therefore any disagreeable or painful procedures, such as palpating a painful area, should be performed only at the end of the examination.

The neurologic examination includes assessment of mental status and behaviour, posture, gait, postural reactions, cranial nerve function, muscle tone and mass, spinal reflexes, and pain perception.

Mental status and behaviour

The level of consciousness is influenced by the functional relationship between the ascending reticular activating system within the brain stem and the cerebral cortex. An animal with normal mental status is bright, alert and appropriately responsive to the surrounding environment. Depression or obtundation occurs in animals that are awake but relatively unresponsive to normal environmental stimuli. Depression is not a specific sign of brain disease and may be seen in association with systemic illness. Stupor is present in an animal that sleeps except when aroused by strong stimuli. Coma is a state of unconsciousness from which an animal cannot be aroused even with noxious stimuli. Stupor and coma are commonly caused by a brain stem lesion that produces a partial or complete, respectively, disconnection of the reticular formation and the cerebral cortex. Stupor and coma Stupor and coma can also take place with severe diffuse forebrain disease. Delirium occurs when an animal is overactive and responds inappropriately to stimuli; it indicates forebrain dysfunction.

Behavioural changes such as loss of learned habits (for instance house training), aggression, head pressing, inability to recognize the owner suggest a forebrain disorder involving the limbic system.

Hemi-neglect syndrome, also known as hemi-inattention syndrome, refers to an abnormal phenomenon in which an animal with a structural forebrain disease ignores sensory input from one half of his/her environment (e.g., eats only from one side of the bowl, turns to the opposite direction when called from the ignored side). Since most sensory stimuli are interpreted primarily in the cerebral hemisphere contralateral to the side of the stimulus, the side that the patient ignores is contralateral to the side of the lesion.

Posture

Normal posture is maintained by coordinated motor responses to sensory inputs from receptors in the limbs and the body, the visual system, and the vestibular system to the CNS. Posture abnormalities include:

 Wide-based stance in animals with vestibular or cerebellar disease, or with a lesion involving proprioceptive pathways between the spinal cord and the cerebral cortex. This stance may also be seen with generalised peripheral nerve disease.

 Knuckling on one or more paws while standing indicates a conscious proprioceptive deficit.

 Head tilt (one ear lower than the other) indicates unilateral vestibular dysfunction. The head is usually tilted toward the side of the lesion. Cerebellar lesions involving the flocculonodular lobe, the fastigial nucleus, or the caudal cerebellar peduncle can also produce a head tilt.

 Head turn (the ears are level, the nose is turned to one side) and Pleurothotonus (the head, neck and trunk are twisted to one side) may occur with cerebral lesions and usually are toward the side of the lesion.

 Head and neck ventroflexion may be observed with certain myopathies (e.g., hypokalemic myopathy in cats) or junctionopathies (e.g., myasthenia gravis in cats).

 Kyphosis is often present in association with painful diseases of the thoracolumbar spine (e.g., intervertebral disc extrusion). Lordosis or scoliosis may occur in animals with vertebral column malformations (e.g., hemivertebrae).

 The head and neck may be held in a fixed position when cervical pain is present.

 Shiff-Sherrington posture is characterised by thoracic limb extension (best appreciated with the animal in lateral recumbency) and pelvic limb paralysis. It results from an acute severe lesion of the thoracolumbar spinal cord which interrupts the ascending inhibitory impulses from the border cells of the lumbar gray matter to the extensor muscle α-motor neurons in the cervical intumescence.

 Decerebrate rigidity is due to a rostral brain stem lesion and is characterised by extension of all four limbs and sometimes opisthotonus. Affected animals are recumbent and typically have decreased consciousness (often stupor or coma).

 Decerebellate rigidity is characterized by opisthotonus, thoracic limb extension, flexion of the hips (pelvic limbs flexed forward), and normal consciousness. It is due to an acute cerebellar lesion mostly involving the rostral lobe which is especially inhibitory to the stretch reflex mechanism of antigravity muscles. If the cerebellar rostral lobe lesion involves the ventral lobules, the pelvic limbs may be rigidly extended away from the body.

Gait

The ability to stand and move requires intact proprioceptive and motor systems. Gait assessment should be performed by observing the patient walking (straight, in circles, up and down stairs) on non-slippery surface. The observer should look at the animal from the side, front and rear. The examiner must be knowledgeable of gait differences among dog breeds. Patients that are recumbent and have no disease that could be exacerbated by movement (e.g., spinal fracture/luxation) should be encouraged/helped to get up and walk if they can, or at least to show any voluntary motor activity.

Gait abnormalities include ataxia, circling, paresis, and lameness. Ataxia is an inability to perform normal coordinated motor activity that is not caused by weakness, musculoskeletal problems, or abnormal movements. Ataxia can be classified as sensory, cerebellar and vestibular.

 Sensory or proprioceptive ataxia is caused by lesions of the general proprioceptive pathways in the peripheral nerve, dorsal root, spinal cord, brain stem and forebrain. It is characterized by a loss of the sense of limb and body position. The animal has a swinging motion of the affected limbs and scuffing of the toes while walking. It is important to remember that since proprioceptive and motor pathways are intimately associated, sensory ataxia is often compounded by weakness.

 Cerebellar ataxia is caused by cerebellar disease or selective dysfunction of the spinocerebellar tracts. It is characterized by inability to regulate the rate and range of movements with subsequent dysmetria, especially hypermetria.

 Vestibular ataxia is associated with unilateral vestibular dysfunction and is characterized by leaning, drifting, falling, rolling to one side. This type of ataxia is often accompanied by other vestibular signs such as head tilt, circling, strabismus and spontaneous nystagmus.

Circling may occur with unilateral vestibular diseases and with asymmetrical or focal forebrain disorders. The presence of other neurological deficits typical of each syndrome (vestibular versus forebrain) will help to localize the lesion.

Paresis is a partial loss of voluntary movement. Plegia or paralysis is a complete loss of voluntary movement. These two terms are combined with the following prefixes to designate the limb involved: mono (of one limb), para (of both pelvic limbs), hemi (of both limbs on one side of the body), tetra (of all four limbs). There are two types of paresis: upper motor neuron (UMN) and lower motor neuron (LMN), causing a spastic or flaccid paresis, respectively.

Lameness is usually caused by orthopaedic disorders, but it can occur also with neurological diseases affecting a nerve root (e.g., attenuation by a lateralised intervertebral disc extrusion causing the so called "root signature") or a spinal nerve (e.g., nerve sheath tumor).

Abnormal involuntary movements include

 Tremors are involuntary rhythmic movements of a body part (or of the entire body) produced by alternating contractions of antagonistic groups of muscles. Tremors may be associated with several conditions such as cerebellar disorders (intention tremors), hypomyelination of the CNS, "shaker dog disease", toxin exposure (e.g., hexachlorophene), hypocalcemia.

 Myoclonus is a repetitive rhythmic contraction of a particular group of muscles (e.g., limb flexors, masticatory muscles) and may persist during sleep. It can be associated with encephalomyelitis, especially canine distemper.

 Myotonia is a delayed relaxation of muscle following voluntary contraction. It occurs in certain congenital or acquired muscle disorders.

Postural reactions assess the same neurologic pathways that are involved in gait, that is, the proprioceptive and motor systems. The main value of postural reaction testing is to detect subtle deficits that may not be obvious during the analysis of locomotion (e.g., in animals with forebrain disease). Postural reactions are sensitive indicators of neurologic dysfunction, but, by themselves, do not provide a specific localization of the lesion within the nervous system. Postural reaction deficits typically occur ipsilateral to peripheral nerve, spinal cord, medulla oblongata and pontine lesions, and contralateral to forebrain and midbrain lesions. Postural reaction tests include the paw placement response (proprioceptive positioning), tactile and visual placing, hopping, hemiwalking, wheelbarrowing, and extensor postural thrust. The occurrence of deficits during two or more of these tests in any limb indicates a significant deficit.

Cranial nerve function

The cranial nerve examination should be performed when the patient is in the most cooperative attitude. Space precludes a detailed description of the functional neuroanatomy of each cranial nerve, consequently the procedure for cranial nerve examination will be briefly described indicating in parenthesis the specific cranial nerve/s being evaluated. The head is observed for any evidence of a head tilt (vestibular VIII), facial asymmetry related to weakness/ spasm of the muscles of facial expression (VII) or to atrophy of the masticatory muscles (motor V). To elicit the menace response (II-VII) one eye of the patient is covered and the opposite eye is menaced with a threatening gesture of the hand, being careful to avoid mechanical stimulation of the vibrissae; the normal response is a blink (VII) and some degree of head withdrawal. The menace response is a learned response and may not occur until 10 to 12 weeks of age in puppies and kittens. The palpebral and corneal reflexes are elicited by touching the medial/lateral canthus of the eye and the cornea (sensory V), respectively; the normal response is a blink (VII) and a retraction of the globe (VI). Facial sensation (sensory V) is assessed over the distribution of the three branches: ophthalmic, maxillary, and mandibular of the trigeminal nerve (V). If a sensory deficit is suspected, the most sensitive area to test with a blunt object is the mucosa of the nasal septum inside each nostril, the normal animal will immediately withdraw the head. The temporalis and masseter muscles are palpated to detect any swelling, atrophy, or asymmetry (motor V). The eyes are observed for evidence of strabismus or spontaneous nystagmus (III, IV, VI, vestibular VIII). By moving the head from side to side and up and down the vestibulo-ocular reflex (physiological nystagmus) can be elicited (III, IV, VI, vestibular VIII). The size and symmetry of the pupils (II, parasympathetic III, sympathetic innervation) and their response to light (II-parasympathetic III) are assessed. By opening the mouth we can evaluate jaw tone (motor V), position, movements and symmetry of the tongue (XII), and elicit the gag reflex (IX, X).

Muscle tone and mass

Muscle tone is maintained by the muscle stretch reflex (muscle stretch receptor- Ia afferent neurons--spinal cord--lower motor neuron--muscle). Decreased muscle tone can result from injury to this reflex arc or intrinsic disease of the muscle itself. Increased muscle tone can result from a lesion of the upper motor neurons that originate in the brain and have an inhibitory influence on the lower motor neurons. Muscle mass and tone are evaluated with the animal standing (try to have the patient bearing the same amount of weight on the two limbs that are being compared) and in lateral recumbency. Abnormalities include atrophy (early and severe with LMN diseases, chronic and mild with UMN disorders), hypo/atonia (LMN signs), and spasticity (UMN sign). Generalized or localized muscle hypertrophy may be associated with myotonic myopathies or with muscular dystrophies.

Spinal reflexes

Examination of the spinal reflexes tests the integrity of the sensory and motor components of the spinal reflex arch and the influence of descending UMN pathways on this reflex. Spinal reflexes include muscle stretch reflexes (such as extensor carpi radialis and patellar reflexes), thoracic and pelvic limb flexor reflexes, perineal and cutaneous trunci reflexes. Accurate evaluation of spinal cord reflexes, and particularly muscle stretch reflexes, requires a relaxed patient, a muscle placed in optimum position and the application of an adequate stimulus. Spinal reflexes are decreased to absent with LMN disorders and normal to increased with UMN disease. It is important to evaluate muscle tone and spinal reflexes along with the gait abnormality. For instance, in dogs with myasthenia gravis we might observe severe neuromuscular paresis with normal muscle tone and reflexes.

Pain perception (nociception)

Perception of a noxious stimulus should be assessed with the animal relaxed in a quiet environment. It is important to remember that pain is the subjective response of the patient to a noxious stimulus and varies between individuals.

Superficial pain sensation is assessed by grasping and lifting a small fold of skin at the test site with a blunt haemostat. The force of pinch is gradually increased until a response is elicited.

Deep pain sensation is tested by pinching the digits with the fingers or a haemostat. Always apply the minimum stimulus that allows eliciting a response. Normal responses to superficial or deep pain testing include:

 A reflex flexion of the limb or a skin twitch indicating that peripheral nerves, nerve roots (motor and sensory) and spinal cord segments are intact.

 A behavioural response, (such as turning the head towards the stimulus, crying or biting), which indicates that peripheral nerves, nerve roots, spinal cord segments and the ascending pain pathways in the spinal cord and brain stem to the forebrain are intact.

The pain pathways that carry superficial and deep pain sensation are different. The latter ones are more resistant to damage than other pathways including those responsible for proprioception, motor function, and superficial pain. Therefore testing deep pain perception is necessary only if superficial pain is absent. In patients with severe spinal cord injuries, the presence or absence of deep pain perception is important in assessing prognosis for recovery. It is very important NOT to confuse reflex flexion of the limb with conscious perception of the noxious stimulus (look for a behavioural response!). Altered states of consciousness (e.g., following trauma and shock) and certain drugs such as analgesics and sedatives may alter results of pain sensation testing.

Superficial pain assessment is particularly useful to map the distribution of a sensory loss in cases of peripheral nerve and brachial plexus injuries. Thorough knowledge of dermatomes and autonomous zones is required.

Finally the spine is palpated in order to detect any areas of hyperalgesia.

The abnormalities recorded during the neurological examination form the "building blocks" of the neurological syndromes. These include: cerebral, diencephalic, midbrain, cerebellar, vestibular, pontomedullary, cervical, cervicothoracic, thoracolumbar, lumbosacral, neuropathic and multifocal syndromes. The neurological syndrome approach helps performing correct lesion localization within the nervous system.

For further information on functional neuroanatomy, correct execution and interpretation of each test of the neurological examination and for a detailed description of the clinical signs that characterize each neurological syndrome I recommend reading the references listed below (n° 2 is available also in Spanish).

References

1.  Braund KG: Clinical Syndromes in Veterinary Neurology, 2nd ed, Mosby, St Louis, 1994

2.  Braund KG: Clinical Neurology in Small Animals. International Veterinary Information Service, IVIS (www.ivis.org), Ithaca, New York, 2003

3.  Braund KG, Sharp NJ: Neurological examination and localization. In: Slatter D: Textbook of Small Animal Surgery, WB Saunders, Philadelphia, 2003

4.  Chrisman CL, Mariani C, Platt S, Clemmons R: Neurology for the Small Animal Practitioner, Teton New Media, Jackson, WY, 2002

5.  De Lahunta A: Veterinary neuroanatomy and clinical neurology, 2nd ed, WB Saunders, Philadelphia, 1983

6.  Dewey CW: A practical guide to canine and feline neurology. Blackwell, Iowa State Press, 2003

7.  Lorenz MD, Kornegay JN: Handbook of Veterinary Neurology, 4th ed, WB Saunders, Philadelphia, 2004

8.  Platt SR, Olby NJ: BSAVA Manual of Canine and Feline Neurology, 3rd ed, BSAVA Publications, 2004

9.  Thomas WB: Initial assessment of patients with neurologic dysfunction. In: Thomas WB: Common neurologic problems. The Veterinary Clinics of North America, Small Animal Practice, WB Saunders, Philadelphia, 2000

10. Wheeler SJ: BSAVA Manual of Small Animal Neurology, 2nd ed, BSAVA Publications, 1995

Speaker Information
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Luisa De Risio, DMV, DECVN


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