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LongDistance Retrograde Effects of Botulinum Neurotoxin A

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Retrograde propogation? SNAP-25 cleavage has ... Retrograde transport, ... No passive spread, only retrograde axonal transport and transcytosis ... – PowerPoint PPT presentation

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Title: LongDistance Retrograde Effects of Botulinum Neurotoxin A


1
Long-Distance Retrograde Effects of Botulinum
Neurotoxin A
  • Flavia Antonucci, Chiara Rossi, Laura
    Gianfranceschi, Ornella Rossetto, and Matteo
    Caleo
  • J Neuro, April 2, 2008, 28 (14)3689-3696

2
Introduction
3
Introduction
  • BoNT/A-G, cleave SNARE, prevent vesicle fusion
  • BoNT/A and E cleave SNAP-25
  • BoNT/A treats
  • hyperfunction of cholinergic terminals
  • remove wrinkles
  • pain management

4
Introduction
  • BoNT/A enters neurons by binding to synaptic
    vesicle protein SV2
  • Internalized by
  • vesicle endocytosis,
  • translocated to cytosol
  • Thought to remain
  • at injection area
  • Retrograde axonal
  • transport?
  • Trancytosis to afferent?

Dong et al. 2006
5
Results
6
Results
  • Grew antibodies against A and E cleave SNAP-25
  • Inj. dorsal Hipp., found dose-response curve,
    comparing BoNT/A concentration to amount of
    cleaved SNAP-25 (3 days after injection)

7
Results
  • Inject dorsal hippocampus, analyze over a time
    course for levels of cleaved SNAP-25
  • BoNT/E maximal 1-10 days after
  • BoNT/A high through day 120
  • confirms

8
Results
  • Analyzed contralateral SNAP-25 cleavage
  • BoNT/E cleavage remained on ipsilateral side
  • BoNT/A treated animals had contralateral cleaved
    SNAP-25 after 3 days

9
Results
  • Immonohistochemistry confirms spread
  • Schaffer collateral connects CA3 and CA1
  • Redcleaved SNAP-25, Greenneuronal
  • Not passive spread
  • Layer II-III of entorhinal cortex, layers that
    project to hippocampus
  • Retrograde propogation?

10
Results
  • SNAP-25 cleavage has functional repercussions
  • Recorded spontaneous spike activity of CA1
    pyramidal cells
  • Reduced contralateral activity 3 d after A inj.
  • E blocks only ips.
  • Be skeptical

11
Results
  • Superior Colliculus receives 1-way projections
    from cont. retina and ips. primary visual cortex
  • Inject BoNT/A into SC, measure cleavage
  • Cleavage after 1 day only in SC, in retina and
    cortex after 3 days
  • Colchicine MT depolymerizing agent blocks
    spread of cleavage MT-based axonal tranport?

12
Results
  • Immunostaining showed cleavage in layer V of
    visual cortex (cells that project to SC)
  • Retrograde transport, not passive spread
  • In retina, cleavage in ON/OFF sublamina of inner
    plexiform layer (project to SC)

13
Results
  • Analyzed IPL to see type of synapse 3 d after
    inj.
  • Cleavage colocalized with choline
    acetyltransferase
  • Also colocalized with SV2C
  • Cleavage appears in cholinergic, SV2C synapses
    of retina

14
Results
  • Could it be that just the cleaved SNAP-25 is
    transported, not the toxin?
  • Inj. into SC, found expected cleavage 3 d after
  • Cut optic nerve, nothing more transported from SC
  • Inj BoNT/E into eye
  • BoNT/E cleaves off terminal where antibody binds

15
Results
  • BoNT/E cleaves off terminal where antibody binds
  • BoNT/E loses its effectiveness after about 3
    weeks
  • Expect initial disappearance of A-cleaved SNAP-25
  • If only A-cleaved SNAP-25 had been transported
    from SC to the eye, there would be no increase of
    A-cleaved SNAP-25 after BoNT/E loses its effect
  • If BoNT/A had been transported from SC, there
    WOULD be a recovery of A-cleaved SNAP-25

16
Results
  • Initially a lot of A-cleaved SNAP-25
  • With BoNT/E injection, large decrease in amount
    of A-cleaved SNAP-25
  • After 25 d, recovery of A-cleaved SNAP-25
  • It was BoNT/A that was retrogradely transported
    from SC to retina

17
Results
  • Natural target of BoNT/A is neuromuscular
    junction so examined transport in motoneurons
  • Injected into whisker muscles (no proprioceptive
    or sensory innervation)
  • After 3 days, cleavage in facial nucleus in pons

18
Conclusions
19
Conclusions
  • BoNT/A cleaves SNAP-25 at injection site and to
    far regions that project to the infusion site
  • No passive spread, only retrograde axonal
    transport and transcytosis
  • Functional changes?
  • Active BoNT/A is transported, rather than its
    cleaved substrate
  • Rather than left in cytosol, some loaded into
    vesicles, released at synapse, and taken up by
    afferent neurons

20
Further exploration
  • Functional effects?
  • Beyond second-order neuron transport?
  • Is BoNT/A like tentanus, in that it trancytosis
    is limited to specific synaptic inputs?
    Chonlinergic?
  • What is the mechanism for transcytosis
  • Implications of BoNT/A used medically?
  • Dystonic patients treated with BoNT/A have show
    changes in cortical excitability
  • BoNT/A administered in the periphery may directly
    affect central circuits via retrograde transport
    and transcytosis
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