neuro

Question 1

What is Multiple Sclerosis

Answer 1

• An immune-mediated disease of the central nervous system
• A disease of myelin and axons
• primarily diagnosed clinically

Question 2

For MS, where are Immune cells are made throughout the body?

Answer 2

•	Tonsils
•	Thymus
•	Bone Marrow
•	Spleen
•	Lymphoid tissue of the gut
******EXCEPT the brain and spinal cord******

Question 3

Tell me about the Nerve Damage and Myelin Loss pathway

Answer 3

A. Normally, axons have a protective myelin coating that is necessary for normal conduction of electrical impulses
B. In MS, the immune system destroys myelin, resulting in slowed (not absence) conduction and exposure of axons
C. Exposed axons may then be severed…
D. …leading to permanent loss of the axon
E. The result is permanent loss of nerve function

Question 4

What are common MS presenting s/s?

Answer 4

• Spasticity
• Gait, balance, and coordination problems
• Speech/swallowing problems
• Tremor
• *****s/s unpredictable

Question 5

between ages is MS usually dx?

Answer 5

20-50

Question 6

risk factors with MS

Answer 6

risk is higher in any family in which there are several family members with the disease (multiplex families)

Question 7

What happens with Myelin in Chronic Multiple Sclerosis Lesion?

Answer 7

In Early MS lesions as “shadow plaques,” which are areas of thinly remyelinated axons.

Question 8

What will You Do in the Diagnosing MS?

Answer 8

• The core requirement for the diagnosis →dissemination in time and space: evidence that damage has occurred in at least two separate areas of the CNS at different points in time
• There must be no other explanation
• Diagnosis of MS require evidence of plaques that occurred in different places in the CNS at different points in time
• Clinical findings alone or a combination of clinical and MRI findings
• Can sometimes take months or even years to confirm the diagnosis

Question 9

WHAT IS Dissemination in space

Answer 9

demonstrated with MRI by one or more T2 lesions in at least two of four MS-typical regions of the central nervous system (periventricular, juxtacortical, infratentorial, or spinal cord) OR by the development of a further clinical attack implicating a different central nervous system site. For patients with brainstem or spinal cord syndromes, symptomatic MRI lesions are excluded from the criteria and do not contribute to lesion count.

Question 10

WHAT IS Dissemination in time

Answer 10

demonstrated with MRI by the simultaneous presence of asymptomatic gadolinium-enhancing and nonenhancing lesions at any time, OR a new T2 and/or gadolinium-enhancing lesion(s) on follow-up MRI, irrespective of its timing with reference to a baseline scan, or by the development of a second clinical attack

Question 11

What is the test of choice to support the clinical diagnosis of MS

Answer 11

MRI

Question 12

T/F: Most patients with MS have relapsing-

remitting disease

Answer 12

TRUE

Question 13

role of lumbar puncture with MS:

Answer 13

not a requirement for the diagnosis of MS in patients with classic MS symptoms and brain MRI appearance- but - it can be used to help rule out the diagnosis in equivocal cases

Question 14

What is Evoked potential testing

Answer 14

• • electrical events generated in the central nervous system by peripheral stimulation of a sensory organ
• *Used to detect subclinical, abnormal central nervous system function
• *Detection of a subclinical lesion in a site remote from the region of clinical dysfunction supports a diagnosis of multifocal MS
• *Evoked potentials also may help define the anatomical site of the lesion in tracts not easily visualized by imaging (eg, optic nerves, dorsal columns).

Question 15

what is a Clinically Isolated Syndrome (CIS)

Answer 15

**A first neurologic event suggestive of demyelination
• pt with CIS are at high risk for developing MS if the neurologic event was accompanied by multiple, clinically silent (asymptomatic) lesions on MRI typical of MS

Question 16

Name the four stages of MS and describe

Answer 16

• Primary Progessice MS [ppms]- gradual progession of disease since onset without remission/relapse
• Relapsing/Remitting MS [rrms]- unpredicatable attacks which may or may not leave permanent deficits followed by periods of remission
• Secondary Progressive MS [spms]- initial rrms that progressed to progessive ms/ sudden steady decline without remission/relapse
• Progressive relapsing MS [prms]- steady decline since onset with SUPER-imposed attacks

Question 17

define relapse with ms

Answer 17

new symptom or sudden worsening of old symptom lasting at least 24 hours, and usually accompanied by an objective change in neurologic findings

Question 18

in a pt with rrms, how would the np manage a relapse?

Answer 18

• Treatment with corticosteroids recommended if relapse significantly interferes with everyday functioning
• 3-5 day course of high-dose intravenous methylprednisolone with or without oral taper
• High-dose oral steroids may also be used
• Rehabilitation can help restore function following a relapse

Question 19

How would the NP medically treat MS?

Answer 19

• Baclofen (Lioresal) – oral; intrathecal or procedure with • Baclofen pump

Question 20

T/F: Temperature Sensitivity is common with pts with MS

Answer 20

TRUE: Heat sensitivity is common AND cold sensitivity may occur too

Question 21

What is pseudoexacerbation

Answer 21

When even a slight elevation in core body temperature in MS pt can cause temporary worsening of symptoms

Question 22

What is Parkinson’s Disease?

Answer 22

a chronic, progressive neurodegenerative disorder characterized by any combination of four cardinal signs: rest tremor, rigidity, bradykinesia, and gait disturbance.

Question 23

what are the 4 cardinal signs of parkinsons diease?

Answer 23

rest tremor, rigidity, bradykinesia, and gait disturbance.

Question 24

what is the patho of parkinson disease?

Answer 24

Loss of dopamine in the corpus stratia is the primary defect in Parkinson’s disease. [Destruction of neural cells in the substantia nigra pars compacta (midbrain) that secrete dopamine]

Nerve cells in the substantia nigra send out fibers to the corpus stratia, gray and white bands of tissue located in both sides of the brain.

There the cells release dopamine, an essential neurotransmitter (a chemical messenger in the brain)

Question 25

what is the pathological hallmark of parkinsons?

Answer 25

lewy bodies (on autopsy)

Question 26

risk factors for parkinsons

Answer 26

increased with older age

decreased risk with smoking cigarettes

Question 27

Motor parkinsonism required traits:

Answer 27

Bradykinesia

Rest tremor or rigidity

Question 28

clinical presentation of pt with Parkinson disease

Answer 28

• Bradykinesia
• Plus Tremor (most common presenting sign)
• or Rigidity
• Postural instability (occurs late in disease)
• Resting tremor
• Asymmetry (one side more affected than the other)
• Good response to Levodopa

Question 29

What are the red flags that mean dx is NOT parkinsons

Answer 29

• Falls at presentation or early in the course of the disease
• Poor response to Levodopa
• Symmetrical motor signs
• Lack of tremor
• Rapid progression
• Dysautonomia early in the disease (urinary urgency/incontinence, orthostatic hypotension, erectile failure)
• History of repeated head injury, or encephalitis
• History of recurrent strokes

Question 30

T/F: There are no tests to diagnose parkinson disease

Answer 30

TRUE

Question 31

Pharmacological management for parkinsons

Answer 31

• Levodopa**INITIAL TX
• Dopamine agonists*****INITIAL TX
• Monoamine oxidase (MAO) B inhibitors- Rasagiline 5mg once a day (in AM)
• Anticholinergic agents
• Amantadine (Symmetrel, Symadine)- Antiviral agent 200-300 mg/day in divided doses [weak antiparkinsonian drug with low toxicity that is most useful in treating patients with early or mild PD]
• Catechol-O-methyl transferase (COMT) inhibitors

Question 32

Bradykinesia in parkinsons

Answer 32

Generalized slowness of movement
• May be described as “weak”, “incoordination”, “tired”, “stiffness”
- Typically starts distally in arms, w/ dec. manual dexterity of fingers

Question 33

Resting tremor

Answer 33

• occurs @ rest
• seen as a “pill-rolling” action of the hands that may also affect the chin, lips, legs, and trunk, can be markedly increased by stress or emotions.
• Onset of parkinsonian tremor is generally after age 60. -Movement starts in one limb or on one side of the body and usually progresses to include the other side.

Question 34

caution with pts with tremors

Answer 34

the majority of people with tremor do not have PD:

• essential tremor (Usually B/L and intention),
• MS (intention),
• cerebellar dysfunction (Usually intention & w/ other cerebellar signs)

Question 35

rigidity with parkinsons

Answer 35

• Often begins unilaterally, typically same side as tremor
• “Cogwheel rigidity”- ratchet pattern of resistance and relaxation
• “Leadpipe rigidity”- present throughout movement

Question 36

Name Craniofacial features with parkinsons:

Answer 36

• Hypomimia (masked facial expression)
• Decreased spontaneous eye blink (dysarthria)
• Speech impairment (hypophonia)
• Sialorrhea (excessive salivation)

Question 37

initial Parkinson tx

Answer 37

Levodopa or Dopamine agonists

Question 38

what is is the most effective symptomatic therapy for parkinson s/s

Answer 38

Levodopa (combined with a peripheral decarboxylase inhibitor, ie, Sinemet, Madopar, or Prolopa)
-initiate with immediate release

Question 39

anticholinergic use with parkinson disease

Answer 39

should be reserved for younger patients in whom tremor is the predominant problem.
-Their use in older or demented individuals and those without tremor is strongly discouraged.

Question 40

T/F: Patients with Parkinson disease (PD) who take levodopa chronically are increasingly likely to develop motor fluctuations and dyskinesia as the disease progresses.

Answer 40

TRUE

Question 41

T/F: Younger patients on levodopa can develop motor fluctuations and dyskinesia SOON after starting treatment.

Answer 41

TRUE

Question 42

Describe wearing off phenomenon in parkinsons disease pts on Levodopa

Answer 42

• As the disease advances, effect of levodopa begins to wear off approx. 4 hrs. after each dose (1/2 life = 90 min.)
• Pt’s will begin to be aware of a wearing “off” effect less than 4 hrs after levodopa dose

Question 43

whats is Dyskinesia

Answer 43

abnormal involuntary movements

Question 44

how should the np manage wearing off phenomenon with levodopa?

Answer 44

• DO Shorten the dose interval while administering lower doses
  • Add COMT inhibitor
• DONT Increase dosE = not usually effective = increase SE w/o increasing dose duration
• DONT take levodopa w/ high protein meals

Question 45

what are Motor fluctuations ?

Answer 45

alterations between periods of being “on”= responding to medication, and being “off”= experiencing symptoms of underlying PD

Question 46

What is Myasthenia gravis?

Answer 46

• most common disorder of neuromuscular transmission. -well understood autoimmune disorder
• HALLMARK: fluctuating /combo of weakness in ocular (eye/eyelid movement- ptosis), bulbar (facial expression, chewing, talking, and swallowing), limb, and respiratory muscles.
• ***skeletal muscle weakness INCREASES during periods of activity and IMPROVES after periods of rest

Question 47

what is the patho of myasthenia gravis?

Answer 47

Weakness is the result of an antibody-mediated, T-cell dependent immunologic attack directed at proteins in the postsynaptic membrane of the neuromuscular junction (acetylcholine receptors or receptor-associated proteins).
****antibodies BLOCK, alter or destroy the receptors for acetylcholine at the neuromuscular junction = PREVENTION of muscle contraction occurring

Question 48

myasthenia gravis s/s

Answer 48

• increase in females in 20s-30s
• fluctuating skeletal muscle weakness, often with true muscle fatigue.
• HALLMARK: fluctuating /combo of weakness in ocular (eye/eyelid movement- ptosis), bulbar (facial expression, chewing, talking, and swallowing), limb, and respiratory muscles.
• ***skeletal muscle weakness INCREASES during periods of activity and IMPROVES after periods of rest

Question 49

What are the bedside tests for myasthenia gravis?

Answer 49

• the edrophonium test and the ice pack test

- sensitive, but many false-positive results

Question 50

how will the np preform the edrophonium test?

Answer 50

• uses the drug Tensilon (edrophonium) to diagnose myasthenia gravis. Tensilon prevents the breaking down of the chemical acetylcholine, which then helps stimulate the muscles.
• inject iv and then sub q
• Pt tests positive for myasthenia gravis if their muscles get stronger after being injected with Tensilon.

Question 51

how will the np preform the ice pack test?

Answer 51

• preform in pt with ptosis
• NOT helpful for those with extraocular muscle weakness.
• ice pack placed on pt’s closed lid for two minutes.
• The ice is then removed and the extent of ptosis is immediately assessed.

Question 52

what SEROLOGIC TESTINGshould be preform to confirm dx?

Answer 52

Patients with positive AChR-Ab or MuSK-Ab assays (positive antibodies) have seropositive myasthenia gravis (SPMG)= confirmation of myasthenia gravis
-but DONT rely

Question 53

neuro exam should include

Answer 53

• getting up and down from chair
• crossing and uncrossing legs
• holding arms overhead until they get tired
• counting backward from 100 until their voice starts to weaken

Question 54

t/f : Once the diagnosis of myasthenia gravis has been established, a chest CT or MRI scan should be performed to look for a possible associated thymoma

Answer 54

TRUE

Question 55

Where is the birthplace of myasthenia gravis

Answer 55

thymus

Question 56

Describe the two clinical forms of myasthenia gravis

Answer 56

• ocular myasthenia = weakness limited to the eyelids and extraocular muscles.
• generalized disease = the weakness commonly affects ocular muscles & combo of bulbar, limb, and respiratory muscles.

Question 57

what antibiotic is contraindicated with MG?

Answer 57

Ketolides (telithromycin)

Question 58

what drugs may mask/worsen MG?

Answer 58

abx:
-Aminoglycosides* - eg, gentamicin, neomycin, tobramycin
-Clindamycin
-Fluoroquinolones - eg, ciprofloxacin, levofloxacin, 
-Vancomycin
Cardiovascular drugs:
-Beta blockers 
-magnesium 
Anesthetic agents:
-Neuromuscular blocking agents*

Question 59

what drugs are well tolerated with MG:

Answer 59

CArdio:
-calcium channel blockers
Abx:
-Antiretroviral agents - eg, ritonavir
-Tetracyclines - eg, doxycycline, tetracycline
-Macrolides - eg, azithromycin, clarithromycin, erythromycin
-Metronidazole
Anesthetic agents:
-Inhalation anesthetics - eg, isoflurane, halothane
-Local anesthetics- bupivacaine, lidocaine, procaine