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BB1 > Injury and Repair of the Nervous System > Flashcards

Injury and Repair of the Nervous System Flashcards

1
Q

Who was Clint Hallam and why is he important?

A

Cut off arm in 1984

Received first ever forearm transplant in 1998 in Lyon, France

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2
Q

How does a limb transplant work (in terms of revascularisation and nerve regrowth)?

A
  • After revascularization, a composite tissue allograft is viable… but not functional!
  • The axons of the recipient have to regrow and replace the axons of the donor to reinnervate the muscles and the sensory end organs within the graft
  • The donor nerves only serve as temporary scaffold for the axons to grow into
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3
Q

What happens to nerve axons after nerve damage?

A
  • Comparison between nerve axon and train track

- In a train track damage is localised, whereas in axons damage is not simply localised to the site of injury

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4
Q

What are the main challenges of nerve repair?

A
  • Nerve damage may spread:
    o Through anterograde degeneration (=Wallerian degeneration)
    o Through retrograde degeneration (axonal “die-back”)
    o To the cell body (spinal cord, ganglia)
    o Through transneuronal degeneration
  • Nerve repair is not always successful: repairs may happen but the attempts may not always be successful!
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5
Q

What does the success of nerve repair depend on?

A
  • The success of nerve repair will depend on:
    o The severity of the initial injury (primary damage)
     What has been damaged; how much has been damaged
    o The extent of the secondary damage
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6
Q

What is neurapraxia?

A
  • Temporary loss of motor and sensory function due to blockage of nerve conduction (see diagram/table in lecture notes)
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7
Q

What is axonotmesis?

A
  • A disruption of axons, resulting from severe crush or contusion (see diagram/table in lecture notes)
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8
Q

What is neurotmesis?

A
  • Both the axons and the nerve sheath are disrupted (see diagram/table in lecture notes)
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9
Q

Summarise the challenges of nerve repair.

A
  • Nerve damage may spread
  • Nerve repair may happen but is NOT always successful
  • The success of repair depends on the severity of the injury (primary and secondary)
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10
Q

What must the nerve cell body do after damage has been done?

A

Know an injury has happened

Respond to the injury

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11
Q

What happens in cells in the dorsal root ganglion after damage occurs?

A
  • After damage there is a burst of action potentials that let the dorsal root ganglion know that there is a problem
  • Disruption of retrograde flow
  • Altered Phenotype (cells change their function)
    o NEURONS SWITCH FROM A TRANSMISSION STATE TO A GROWTH STATE
    o  ion channels and proteins involved in neurotransmission
    o proteins involved in axonal growth
  • Neurotrophic factors
    o released by innervated cells
    o taken up by the nerve terminals
    o transported retrogradely to the neuronal cell body to promote neuronal growth and survival
  • Examples of neurotrophic factors:
    o NGF: Nerve Growth Factor
    o BDNF: Brain-Derived Neurotrophic Factor
    o GDNF: Glial cell-Derived Neurotrophic Factor
    (see diagrams in the lecture notes)
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12
Q

How are Schwann cells involved in the process of nerve regeneration?

A
  • Schwann cells divide, secrete trophic factors to attract axon, then remyelinate new axon
  • Growth rate: 1mm / day (can vary from 0.5 - 9mm / day)
  • After complete nerve transection, only a low percentage of adult patients will regain normal function

See diagram in lecture notes

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13
Q

Why is early repair associated with a better outcome?

A
  1. Prolonged axotomy significantly reduces the number of motoneurons and their axons that can regenerate
  2. After 1 month, Schwann cells down-regulate regeneration-associated factors
  3. Prolonged muscle denervation:
    o Muscle atrophy and fibrosis
    o Profound decrease in numbers of regenerating axons through the deteriorating intra-muscular sheath

See diagram in lecture notes

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14
Q

Can nerves regenerate in the PNS?

A
  • In the PNS, nerve can regenerate, but this is always imperfect
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15
Q

How quickly did the nerves regenerate in Clint Hallam’s new arm?

A
  • What happened to Clint Hallam?
    o Growth rate: 2 mm / day
    o Sensory recovery:
     By 100 days: at the wrist (= 200 mm for the ulnar nerve)
     By 1 year: at all fingertips (= 360 mm)
     By 2 years: discriminates pain, hot/cold, sharp blunt in hand & fingers
    o Motor recovery:
     At 3 months: grip & pinch movement
     At 12 months: intrinsic hand muscle activity appeared into the abductor digiti minimi muscle
     At 16 months: very weak muscle activity in the other intrinsic hand muscles
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16
Q

How does CNS nerve regeneration occur after a spinal cord injury?

A
  • Spinal cord trauma produces a site of primary cell death (the “epicentre”), which rapidly spreads into a zone of secondary cell death
  • Macrophages and microglia engulf debris and the injury site becomes walled off by a glial scar
    o A physical and chemical barrier for neuroregeneration!
     ENGULFS DEBRIS
     SEALS THE LESION SITE
     REPAIRS THE Blood-Spinal Cord Barrier
     EXPRESSES CHEMICALS THAT INHIBIT AXON GROWTH (CHONDROITIN SULPHATE PROTEOGLYCANS –CSPGs)
  • At the glial scar, axons show an abortive sprouting response; distal tracts undergo Wallerian degeneration

See diagrams in lecture notes

17
Q

What are the two main barriers to CNS repair?

A
  • Two main barriers to CNS repair:
    1. Hostile Environment
    o Scar tissue (physical; chemical barrier –CSPGs)
     Myelin-associated inhibitory proteins:
     Nogo proteins;
     Omgp (Oligodendrocyte myelin glycoprotein)
    2. Poor regenerative response
18
Q

Are there many possibilities for CNS repair?

A
  • In the CNS, the possibilities for regeneration are limited –but research is ongoing…
19
Q

What are the steps in assisting CNS regeneration?

A
  1. Neuroprotection
    o To contain the effects of early trauma, inflammation, and scar formation
    o Injected with Omega-3 polyunsaturated fatty acids – docosahexaenoic acid (DHA) (with Prof. Adina Michael-Titus) in these pictures
  2. Promotion of axonal regeneration
    o Positive trophic support (e.g. adding growth factors)
    o Counteracting inhibitory influences
    1. Guiding axonal regrowth
      o to re-establish appropriate connectivities
  4. Activity based rehabilitation
    - 5 hours of physiotherapy, 5 days a week (in Derek Fidyka’s case)
    - Stabilises new synapses and reverses muscle atrophy

A combinatorial approach offers the greatest hope for treatment in the CNS

See diagrams in lecture notes

20
Q

What is chromatolysis?

A
  • Chromatolysis = precursor to apoptosis - nucleus moves towards cell edge

BB1 (28 decks)

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