Download SPASTICITY - wikimotorio

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

page
1
page
2
page
3
page
4
page
5
page
6
page
7
page
8
page
9
page
10
page
11
page
12
page
13
page
14
page
15
page
16
page
17
page
18
page
19
page
20
page
21
page
22
page
23
page
24
page
25
page
26
page
27
page
28
page
29
page
30
page
31
page
32
page
33
page
34
page
35
page
36
page
37
page
38
page
39
Document related concepts
no text concepts found
Transcript 
S PA S T I C I T Y
• Motor disorder
characterized by
velocity dependent
increase in tonic
stretch reflexes and
exaggerated tendon
jerks
D.S.N.V. - UniGE
UPPER MOTONEURONE
SYNDROME
• Negative phenomena
- Weakness
- Fatigability
- Reduced MUs
recruitment
- Reduced dexterity
• Positive phenomena
- Tone increase
- Stretch hyperreflexia
- Clonus
- Flexor-extensor spasms
- Abnormal cutaneous r.
- Babinski sign
- Cocontraction/Dystonia
D.S.N.V. - UniGE
Higher
Centres
Descending
+
Peripheral
Afferents
+
-
Spinal Cord
Circuitry
Pathways
Skeletal
Muscle
-
D.S.N.V. - UniGE
SPASTICITY and UMN Syndrome
Pathophysiological Mechanisms
• Defective Inhibition
 MNs
Postsynaptic  MNs inhibition
Presynaptic Ia inhibition
Excitatory group II INs
• Defective Excitation
Inhibitory Ia-INs ‘ Reciprocal’
Inhibitory Ib- INs ‘Autogenetic’
Renshaw cells ‘Recurrent’
D.S.N.V. - UniGE
SPASTICITY
Ia Pre-synaptic Inhibition
D.S.N.V. - UniGE
SPASTICITY
Ia Reciprocal Inhibition
D.S.N.V. - UniGE
SPASTICITY
Interneuronal Excitability
D.S.N.V. - UniGE
SPASTICITY and UMN Syndrome
Pathophysiological Mechanisms
• Motor Units changes
–
–
–
–
–
collateral sprouting
transynaptic degeneration
dendrite shortening
silent synapses activation
denervation supersensitivity
• Changes of Stiffnes and
muscle properties
D.S.N.V. - UniGE
Muscle & Nerve suppl 6 - 1997
D.S.N.V. - UniGE
TREATMENT of SPASTICITY
Therapeutic Objectives
• TECHNICAL:
- Promote: TONE REDUCTION
- Improve: RANGE of MOTION, JOINT POSITION
- Facilitate: REHABILITATION
• FUNCTIONAL:
- Improve: GAIT, HYGIENE, ADL, EASE of CARE
- Reduce: SPASMS, PAIN
D.S.N.V.- UniGE
PHARMACOLOGIC TREATMENT
OF SPASTICITY
• Recommended when spasticity produces a clinical disability
by interfering with posture, motor capacity, nursing, ADL
• Indicated when muscle overactivity is diffusely distributed
(spinal > cerebral)
• Timed in the early stages to prevent permanent
musculoskeletal deformities or contractures
• The goal is to decrease spinal reflex excitability by:
- reducing the release of excitatory neurotransmitters
- potentiating the activity of inhibitory circuits
D.S.N.V.- UniGE
NEUROTRANSMITTERS AND
PHYSIOLOGICAL MECHANISMS
INVOLVED IN SPASTICITY
GABA
Glycine
Glutamate
EAAs
Noradrenaline
Serotonine
D.S.N.V. - UniGE
DIAZEPAM
• Aumenta l’affinità del
GABA per il suo
recettore ionoforico
(GABA a)
-
-
Livello postsinaptico: aumento
conduttanza Cl,
iperpolarizzazione, inibizione
postsinaptica
Livello presinaptico: aumento
conduttanza Cl,
depolarizzazione, inibizione
rilascio aminoacidi eccitatori
D.S.N.V. - UniGE
BACLOFEN
• Stimolazione recettori
GABA b (metabotropici)
- Livello postsinaptico: aumento
conduttanza K,
iperpolarizzazione cellulare,
inibizione
- Livello presinaptico: blocco dei
canali del Ca, alterazione
liberazione aminoacidi eccitatori
D.S.N.V. - UniGE
D.S.N.V. - UniGE
DIAZEPAM (2)
• CLINICAL EFFECTS:
- Reduction of resistance to stretch (increased range of motion)
- Reduction of deep tendon reflexes and of painful spasms
• SIDE EFFECTS:
- Sedation & drowsiness, Attention & memory impairment
- Weakness amd motor incoordination
- Tolerance, dependency (withdrawal phenoemena)
• INDICATIONS: SCI - MS (possible: TBI - CP - CVA)
• EFFICACY SHOWN BY DOUBLE-BLIND PROTOCOLS IN SC
LESIONS (POSSIBLE STRENGTH-GAIT DETERIORATION)
D.S.N.V. - UniGE
BACLOFEN (2)
• CLINICAL EFFECTS:
- Reduction of flexor-extensor spasms
- Reduction of mono- polysynaptic reflexes
- Reduction of sphincter hyperreflexia
• SIDE EFFECTS:
- Sedation, Drowsiness, Fatigue, Confusion, Dizziness
- Hypotonia, Ataxia
• INDICATIONS: Spinal spasticity
• EFFICACY SUFFICIENTLY DOCUMENTED IN PATIENTS
WITH SC LESIONS (LESS IN CEREBRAL)
D.S.N.V. - UniGE
INTRATHECAL BACLOFEN
• Consists of direct long-term delivery of baclofen to the
intrathecal space via an implanted programmable pump
• Indicated in patients with severe spasticity, not managed by
oral baclofen (inadequate BBB penetration, side effects) or
other oral medications
• Same clinical effects at much lower doses (1 %)
• -
Selection
Screening
Implantation
Dose adjustment & maintenance
D.S.N.V. - UniGE
INTRATHECAL BACLOFEN (2)
• Benefits have been documented by placebo-controlled
studies in severely disabled nonambulatory patients with
overactivity mainly in ther lower limbs and with flexor
spasms
• Reduction of spasticity, spasms and pain
Sleep improvement and better bladder management
• IMPROVEMENT IN QUALITY OF LIFE
• COMPLICATIONS: infection, pump dysfunction, high cost
and invasiveness
D.S.N.V. - UniGE
TIZANIDINA
• Attività 2-agonista
(spinale e sopra-spinale)
- riduce la liberazione di
aminoacidi eccitatori nel
midollo spinale
- inibisce la via coerulo-spinale
(questa via normalmente
facilita i circuiti spinali)
D.S.N.V. - UniGE
TIZANIDINE (2)
• CLINICAL EFFECTS:
- reduction of tonic stretch polysynaptic reflexes
- reduction of co- contraction
• SIDE EFFECTS:
sedation, dizziness, dry mouth, but not weakness
• INDICATIONS: MS - SCI (possible: cerebral spasticity)
• EFFICACY PROVEN BY PLACEBO-CONTROLLED
STUDIES (> DIAZEPAM IN CEREBRAL). NO DEFINITE
FUNCTIONAL CHANGES
D.S.N.V. - UniGE
DANTROLENE
• Peripheral inhibition of calcium release from sarcoplasmic
reticulum. Decreased excitation-coupling reaction.
• CLINICAL EFFECTS:
Reduction of muscle tone, phasic reflexes and spasms
Increased range of passive motion
• INDICATIONS: CVA - CP (possible: TBI - SCI -MS)
• SIDE EFFECTS:
hepatotoxicity, GE symptoms, weakness, but less sedation
D.S.N.V. - UniGE
ANTISPASTIC DRUGS
• Clonazepam, Ketazolam, Tetrazepam
Progabide, Gabapentin
Piracetam
Clonidine
L-threonine
Thymoxamine
Cyproheptadine, Orphenadrine
• ONLY FEW CONTROLLED STUDIES
MOSTLY OPEN OR ANECDOTICAL OBSERVATIONS
D.S.N.V. - UniGE
Cochrane Database Syst. Rev. (2000)
- To assess the effectiveness and safety of antispastic drugs in
patients with SCI
- 9 out of 53 parallel and crossover studies (up to 1998) included
•
2 studies (placebo controlled) showed a significant effect of
intrathecal baclofen in reducing spasticity (Ashworth - ADL)
• 1 study (placebo controlled) showed a significant effect of
tizanidine in improving Ashworth scale but not ADL
• No significant evidence for the other drugs (Gabapentin,
Clonidine, Diazepam, oral Baclofen)
D.S.N.V. - UniGE
Neurolytic Agents
• Phenol and alcohol injections may be used to induce a
focal chemodenervation by:
- protein denaturation
- non-selective tissue destruction
(nerve coagulation - muscle necrosis)
- Wallerian degeneration
• Motor nerve block
Motor point block
D.S.N.V. - UniGE
Phenol and Alcohol (1)
• INDICATIONS:
focal spasticity - proximal muscles (lower limb)
• CLINICAL EFFECTS
Reduction of muscle tone (and clonus) without impairment
of strength and voluntary contraction. Long duration.
• SIDE EFFECTS
sensory damage (dysesthesia, causalgia, neuralgic pain)
tissue damage (edema, venous thrombosis)
• NO CONTROLLED FUNCTIONAL DATA
D.S.N.V. - UniGE
BOTULINUM TOXIN
Potent neurotoxin
7 serotypes (A-G) with different antigenic properties
reversible block of Acetylcholine release
D.S.N.V. - UniGE
BOTULINUM TOXIN
Mechanism of action
D.S.N.V. - UniGE
D.S.N.V. - UniGE
BTX e SPASTICITA’
Indicazioni
• Trattamento della spasticità focale, cioè di limitati
gruppi muscolari la cui iperattività o ipertonia
interferisce con lo svolgimento di specifiche attività
‘funzionali’ statiche o dinamiche
• Lo scopo è ottenere un effetto locale, in assenza di
effetti sistemici
• Controindicazioni:
- mancanza di un’adeguata attività dinamica
- presenza di contratture fisse o deformità
D.S.N.V. - UniGE
BTX e SPASTICITA’
Possibili obiettivi
E’ fondamentale la selezione dei pazienti e dei muscoli
bersaglio e l’identificazione degli obiettivi terapeutici
• Prevenzione complicazioni (evitare chirurgia)
• Controllo del dolore
• Facilitazione dell’igiene e/o assistenza
• Miglioramenti funzionali
- adattabilità ortesi, ampliamento ROM
- incremento autonomia (controllo motorio, appoggio, autonomia)
D.S.N.V. - UniGE
BTX e SPASTICITA’
Effetti principali
• Riduzione dell’iperattività muscolare:
-
riflesso tonico da stiramento (Ashworth Scale)
dolore
-
‘range’ di movimento passivo
• Evidenze neurofisiologiche:
- modificazioni attività riflesse spinali
- effetti di tipo centrale ?
D.S.N.V. - UniGE
BTX e SPASTICITA’
Effetti principali
• Modificazioni funzionali:
- scale di autovalutazione (patient/caregiver)
- scale di valutazione funzionale
(ADL, FIM, Rivermead)
- test motori
(Frenchay Arm test, reaching, tapping)
- analisi EMG/Video del cammino
INCERTEZZA SULLE MISURE DI OUTCOME
D.S.N.V. - UniGE
BTX e SPASTICITA’
Problemi metodologici
• Sede d’iniezione: Quali criteri ??
valutazione clinica e/o infiltrazione EMG-guidata
- pattern MUPs
- localizzazione punto motore
- ‘turns amplitude analysis’
- stimolazione elettrica
Childers et al., 1996 - Finsterer et al., 1997
• Numero iniezioni e volume diluizione ??
D.S.N.V. - UniGE
BTX e SPASTICITA’
Problemi metodologici
• Dosaggio ??
- l’entità (ma non la durata) del miglioramento
funzionale può essere dose-dipendente
Wissel et al., 1999; Hyman et al., 2000; Smith et al., 2000;
Bakheit et al., 2000
- problema della ‘immunoresistenza’
- ‘basse dosi’ in associazione a procedure
riabilitative
D.S.N.V. - UniGE
BTX e SPASTICITA’
Trattamenti concomitanti
• La stimolazione elettrica o l’attività muscolare potenzia l’attività
della tossina
Hesse et al., 1995 e 1998, Eleopra et al. 1997
D.S.N.V. - UniGE
BTX e SPASTICITA’
Follow-up
• Efficacia nel tempo del trattamento ??
- analogia con altre indicazioni
 Lagalla et al. 2000
- efficacia invariata a 3 anni in pz. con ‘stroke’
dose invariata, > intervallo
D.S.N.V. - UniGE
SURGICAL TECHNIQUES
in Spasticity
• Objective: to treat permanently static or dynamic
consequernces opf UMN sundrome in stable patients
• Timing: early and before severe and fixed deformities
• Methods: specific interventions for individual
muscle/joints
- TENDON LENGTHENING
- INTRAMUSCULAR LENGTHENING
- TENDON TRANSFER
- NEURECTOMY
D.S.N.V. - UniGE
Management of Spasticity
Prevent:
- provocative factors or
noxious stimuli
(medication if necessary)
- delayed consequences
(surgery if necessary)
Treat muscle overactivity
with different strategies
MEDICAL
THERAPY
PHYSICAL
THERAPY
GENERAL
REGIONAL
FOCAL
ORAL
DRUGS
IT/BACLOFEN
NERVE BLOCKS
BTX
INJECTIONS
D.S.N.V. - UniGE
Related documents
E. coli - Sezione di Microbiologia
E. coli - Sezione di Microbiologia
gen 13 pol - Sezione di Microbiologia
gen 13 pol - Sezione di Microbiologia
Diapositiva 1 - Sezione di Microbiologia
Diapositiva 1 - Sezione di Microbiologia
BIBLIOGRAFIA (vnd.ms-powerpoint, it, 3961 KB, 1/20/15)
BIBLIOGRAFIA (vnd.ms-powerpoint, it, 3961 KB, 1/20/15)
Neuromuscular Localization
Neuromuscular Localization
MOLECULAR CELL BIOLOGY VOLUME 3 | MAY 2002 | 349
MOLECULAR CELL BIOLOGY VOLUME 3 | MAY 2002 | 349
Dr Emiliano Cè Current position: Assistant Professor in the
Dr Emiliano Cè Current position: Assistant Professor in the
2. Functional anatomy of the pelvic floor and lower
2. Functional anatomy of the pelvic floor and lower
The Muscular System
The Muscular System
Poster
Poster
TREATMENT OF HIRSUTISM
TREATMENT OF HIRSUTISM
Global Regents Review
Global Regents Review
FUNKCIONALNO ISPITIVANJE MUSKULATURE TRUPA …
FUNKCIONALNO ISPITIVANJE MUSKULATURE TRUPA …