Skeletal & PNS Pathology - Lawlor

Question 1

What are the two varieties of drug-induced myopathies?

Answer 1

Steroid myopathy

Statin-induced myopathy

Question 2

What fibers are affected in steroid myopathy?

What muscle groups does it affect?

Answer 2

Type 2b fibers

It affects muscles in the proximal limb

Question 3

What tissue makes up the peripheral nervous system?

What is the biggest difference between the PNS and the CNS?

Answer 3

Anything that is not the brain or the spinal cord

The CNS can not regenerate, while the PNS can

Question 4

Define the following terms

Motor Unit

Axon

Schwann cell

Answer 4

Motor Unit-one neuron and all the muscle fibers it innervates

Axon- the long connector between the neuron cell body and the dendrites

Schwann cell- the cell that myelinates the axon in PNS

Question 5

What patterns of myelination should you see as nerve fibers increase in size?

What can clusters of small, poorly myelinated axons indicate?

Answer 5

As the axon increases in size, the myelin sheath should be thicker

Axonal regrowth

Question 6

Explain the difference between Wallerian degeneration, Neuronopathy, and axonopathy.

Which of these syndromes have digestion chambers on histology?

Answer 6

Wallerian degeneration- degeneration of a distal neuron after an injury cuts it off from the cell body

Neuronopathy- a generalized disorder that affects the cell body

Axonopathy- a generalized disorder that attacks the axon, resulting in “dying back”

Wallerian degeneration and axonopathy have digestion chambers (they are the only disorders where the axon is dying and being digested)

Question 7

What are the three inflammatory neuropathies?

What are the differences seen between them?

Answer 7

Guillain Barre- rapidly ascending weakness, that clears quickly; immune system target the muscle fibers

Chronic Inflammatory Demyelinating Polyradiculopathy- slowly progressing weakness moving from proximal to distal; immune system targets the muscle fibers

Vasculitis- death of perivesicular muscle fibers; immune system targets the vessels, but muscle gets caught in the fray. Typically affects ONE nerve as opposed to many

Question 8

What is seen on histology in Chronic Inflammatory Demyelinating Polyradiculopathy?

Answer 8

On cross-section, axons of similar size may have drastically reduced levels of myelin

Also, inflammatory infiltrate

Question 9

What two infectious diseases might cause neuropathy?

What might help distinguish these two?

Answer 9

Leprosy

Shingles

Leprosy will typically have travel outside of the US, can affect any age, and tends to attack cooler area of the body. On histology, there will be granulomas (pathognomonic)

Shingles typically affects only the immunocompromised and the elderly. It tends to follow a single dermatome, usually on the trunk.

Question 10

What is Charcot Marie Tooth type 1?

What is the genetic defect and how is it inherited?

Answer 10

A demyelinating disorder that affects long nerves, causing atrophy of distal limbs.

It is caused by a duplication or deletion (so any frame shift I guess?) in PMP22. This is autosomal dominant inheritance.

Question 11

What is seen on histology in Charcot Marie Tooth?

What symptoms are seen?

Answer 11

Onion skin formation around nerves from failed myelination attempts

Gait disorders, stork legs, foot drop, hammer toes, pes cavus

Question 12

What type of neuropathy is diabetic neuropathy?

What distribution of nerve problems is seen?

Answer 12

It is an axonal degeneration

loss of motor and sensation are seen in the hands and feet

Question 13

What is carpal tunnel syndrome?

How is it treated?

Answer 13

Impingement of the median nerve at the wrist causing pain/tingling in the thumb and first three digits.

Brhavior modification, wrist splinting, surgical fascia release

Question 14

What are neuromas?

What “harmless” procedure can they result from?

Answer 14

intraneural scarring/overgrowth of peripheral nerves, causing intense pain, tingling

A nerve biopsy, so be judicious

Can also be cause by compression, fracture, or surgical lesion

Question 15

Abnormal grouping of muscle fiber types is indicative of what process?

Answer 15

Denervation with reinnervation

Question 16

Describe each of the following pathologic reactions of muscle:

• hypertrophy
• degeneration/necrosis
• regeneration

Answer 16

• Hypertrophy: reaction to increased load due to exercise or pathologic condition
• Degeneration/necrosis: destruction of all or part of a myofiber; stimulates infiltration by macrophages
• Regeneration: satellite cells around degenerated fibers proliferation. Regenerating fibers have a bluish (basophilic) color

Question 17

Describe the fiber type grouping reaction in the context of reinnervation

Answer 17

After denervation, neighboring axons sprout and reinnervate denervated myocytes. The reinnervated fiber assumes the same fiber type as those innervated by the new axon

Question 18

Describe the histologic appearance of neurogenic degradation. Is there necrosis?

Describe the histologic appearance of myopathic degradation. Is there necrosis?

Answer 18

• Neurogenic -> no necrosis, fibrosis, or inflammation
  
  • Bimodal size distribution
  • Angulated fibers
  • Apparent increase in nuclei (nuclear clumps)
• Myopathic -> necrosis with regeneration, fibrosis (+/-), and inflammation
  
  • centralization of nuclei
  • round fibers
  • random size variation

Question 20

What is the main distinction between ALS and SMA?

Answer 20

ALS: UMNs and LMNs

SMA: LMNs

Question 21

What age group is most affected by ALS?

What age group is most affected by SMA?

Answer 21

50-60 years old

children >>> adults

Question 22

What is the genetic inheritance pattern of spinal muscular atrophy?

What is the genetic defect?

Are patients with SMA intellectually normal?

Compare the deep tendon reflex findings of SMA to ALS

Answer 22

autosomal recessive

SMN1 (survival motor neuron gene 1)

normal intellect

SMA: areflexia; ALS: hyperreflexia

Question 23

Describe the histologic pattern seen in Werdnig Hoffmann disease

Answer 23

Large groups of atrophic fibers (panfascicular) with scattered hypertrophic fibers

Question 24

What is the function of dystrophin?

Defects of dystrophin are associated with which two diseases?

What is the genetic inheritance pattern of these two diseases?

Answer 24

Plays a major role in connecting the myoblast cytoskeleton to the extracellular collagen matrix in muscle tissue

Duchenne MD and Becker MD

X-linked

Question 25

Dystrophin: which is more important: quality or quantity?

How is this related to the severity/presentation of DMD and BMD?

Answer 25

Quantity

DMD patients do not produce any dystropin (or nearly none), so the disease is more severe. BMD patients produce less (or lower quality) dystrophin, leading to less severe disease and (possibly) later presentation.

Question 26

Gower’s maneuver is characteristically seen with what disease?

Give one major serum lab finding that is associated with this disease.

Answer 26

DMD

CK greatly increased (>10,000)

Question 27

Describe the physical findings in DMD

Answer 27

• proximal muscle weakness
• slower movement -> wheelchair-bound by age 11-12y
• Large calves (squishy, filled with fibro-fatty tissue rather than muscle)
• Waddling
• Gower’s maneuver
• Scapular winging
• Contractures
• Sparing of the eyes and face
• Dilated cardiomyopathy
• Mild intellectual impairment and developmental delay (IQ ~85)

Question 28

Describe (3) major immunohistologic stain findings in DMD

Answer 28

Dystrophin(-): some dystrophin may appear in isolated islands where (for some reason) there was spontaneous ‘read-through’ of the defective gene.

Spectrin(+): marked increase over normal tissue

Utrophin(+): normally found in capillaries/vessels only. Seen throughout muscle tissue in DMD.

Question 29

Modern genetic testing makes western blots unnecessary for diagnosis of DMD and BMD (but still useful for treating doctor-wallet dystrophy). Descibe the findings for:

• BMD
• DMD

Answer 29

BMD: reduced size and amount (lighter bands than control, bands further down the gel = smaller)

DMD: essentially no dystrophin present (blank gel)

Question 30

What is the most common muscular dystrophy in adults?

What is the genetic inheritance pattern? What is the defective gene? How many repeats must be present for disease?

Answer 30

Myotonic dystrophy

Autosomal dominant. CTG repeats in DMPK gene on chromosome 19 (DM1)

Disease requires at least 80 repeats. Shows genetic anticipation.

Question 31

Describe the major physical exam finding of myotonic dystrophy. Why does this happen?

Describe other clinical findings

Answer 31

Difficulty releasing grip

Due to impaired Cl- conduction -> slower repolarization -> impaired relaxation

Other clinical findings:

• elongated face (myopathic facies)
• temporal wasting
• weakness in distal hands and feet (grip and foot drop)
• premature cataracts
• cardiac arrhythmias
• decreased intellect (more severe with increasing repeats)
• ptosis, receding hairline, testicular atrophy

Question 32

What accounts for the dramatic variation in severity/presentation of mitochondrial myopathies?

Answer 32

Mitochondia segregate independently, so different proportions of ‘good’ and ‘bad’ mitochondria can end up in different tissues. More severe disease depends on (1) greater proportion of defective mitochondria and (2) segregation of more defective mitochondria into especially-sensitive tissues (CNS, liver, nerves -> i.e. metabolically demanding tissues). Skin is relatively unaffected.

Question 33

What is the defect in MELAS?

Describe the clinical features

What’s ‘weird’ about the distribution of affected muscles?

Answer 33

MtDNA mutation (tRNA_Leu)

Clinical features:

• Stroke-like episodes before age 40 (metabolic, not vascular)
• Encephalopathy
• Lactic acidosis with ragged red fibers

Muscle distribution:

• Opthalmoparesis: myopathy of the motor muscles of the eyes with relative sparing of the face and head
• ‘cape-like’ proximal upper weakness
• Thigh

Question 34

Which glycogen storage disease features generalized (multi-organ) glycogen storage dysfunction with particular prominence in the heart?

Which enzyme is deficient?

Answer 34

Pompe’s disease

Acid maltase (glucosidase)

Question 35

Which enzyme is deficient in McArdle’s disease?

Which tissue does this primarily affect?

Answer 35

Phosphorylase a

Muscle (myopathic disease)

Question 36

Does polymyositis feature a rash? What about dermatomyositis?

Which sex is more affected by polymyositis? Inflammation is mediated primarily by what cell type? Where are the immune cells found?

Which is more affiliated with malignancy?

Answer 36

Poly: no rash; Dermato: rash

F > M; CD8+ T-cell mediated, endomysial (intermingled among muscle fibers)

Dematomyositis (poly has no malignancy association)

Question 37

Describe the skin findings of dermatomyositis

Answer 37

Rash

Shawl sign (skin redness over upper/lateral face - like a shawl)

Heliotropic rash (violaceous)

Nail bed thrombi with hemorrhages

painful subQ calcifications (more common in juvenile variant)

Gottron’s papules (erythematous lesions over knuckles)

Question 38

Which immune cell is predominant in the pathogenesis of dermatomyositis?

How does this contibute to the histological appearance of dermatomyositis?

Answer 38

B cells predominate

The humoral reaction attacks the microvasculature, leading to perifascular atrophy and necrosis (not endofascicular like polymyositis)

Question 39

Describe the clinical exam findings of Inclusion Body Myositis (IBM)

Which age group is primarily affected?

Describe the histologic findings

Describe another histologic finding (hint: amyloid)

Describe the EM findings

Answer 39

Medial forearm atrophy (deep finger flexors), Severe quadriceps atrophy (early effect)

Older adults >50 y.o.

Large basophilic vacuoles in regenerating cells

Amyloid deposits noted with Congo Red Stain (apple-green birefringence)

Cytoplasmic inclusions of tuberofilaments (tangle of yarn)

Question 40

Which of the following diseases responds to immunosuppressive therapy?

• Dermatomyositis
• Polymyositis
• Inclusion Body Myositis

Answer 40

• Yes
• Yes
• No