nn 6 hof Hf*

onset.

Methods: Matched case-contiolstudyol SS patients

at 21 emergency departments between 2000 and

2011,and diagnoses were verified by LP.

Results: The clinical pied ci on rule fotdiagnosis

of SAH was 97.1% sen sitire.22.7% specific, and

tad a negative likelr

-wod ratio of 0.13. Using the

nagmg prediction rule resulted in a false negalne

rate of 20%.

Conclusions: Performing tte clinical and imag -g

rules together hasthe potential for maximizing

sensitivity of prediction and reducing rates of IP. but

using imaging alone can resell in missed cases.

Blood in

Sylvian fissures

Blood on

surface of tentorium

Figure 19. Diagnosis of SAH

Positive (NCCT}

s

03— (Positive)

rtf No CT or MRA

positive f

T

( Diagnostic PSA )

Gold Standard

( MRI/MRA ) ( LP ) C 1 J I

, l l

LP positive

Diagnostic DSA i

( OR

! .1 .1

The Vasograde:A Simple Grading Scale for

Prediction of Delayed Cerebral Ischemia after

Subarachnoid Hemorrhage

Stroke 2015;46|7):1826TJ31

Purpose: Patients are classically at risk of delayed

ceietual ischemia (OCI)aftei aneurysmal SAH.Ihis

study validated a grading scale-the VASOGRADE -

for prediction of DCI.

Methods: Oata from three Phase II RCTs and a s ogle

hospitalseries were used to assess the lelationshp

between the VASOGRADE and DCI.

Results: in a cohort of 746 patients, the VASOGRADE

significantly predicted Ml (P<0.001). lire

YASOGRADE-Yellow had a tendency lor increased risk

for DCI (OR 1.31:95% Cl 0.77-2.23) when compared

With VASOGRADE- Green:those with VASOGRAOE-Red

had a 3 fold higher tisk of DCI (OR 3.19;95% Cl 2.07-

4.50|.VASOGRADE had an adequate diswmuut c - foi

prediction of OCI {area under the receiver operating

characteristics cune-0.63) and good calibration.

Conclusions:Ire VASOGRADE results validated

previously published risk chartsin a large and

d versesample of SAH patients,which allows DCI risk

stiatdication on piesentalon after SAH.It coJd help

to select patients at fugh-nsk of OCI and standardize

treatment protocols and research studies.

to

x—> 6

— — r-

(Coiling) (Clipping)

'

r

( Stop ] ( Stop ] ( Slop )

Gold Standard

Figure 20. Approach to SAH

Adapted from:de Oliveira Manoel et al. (2014)Subarachnoid haemorrhage Irom a neuroimaging perspective.Critical Care

Treatment

•admit to K!U or NICU

oxygen/ventilation PRN

NPO, bed rest, elevate head of bed 30“, minimal external stimulation, neurological vitals ql h

• aim to maintain sBP=120-150 mmHg (balance of vasospasm prophylaxis, risk of rebleed, risk of

hypotension since CBF autoregulation impaired by SAH)

• cardiac rhythm monitor, Foley PRN,strict monitoring of ins and outs

•medications

IV NS with 20 mmol KC1/L at 125-150 cc/h

nimodipine 60 mg PO/NG q4 h x 21 d for delayed cerebral ischemia neuroprotection; may

discontinue earlier if patient is clinically well

seizure prophylaxis:levetiracetam (Keppra*) 500 mg PO/IV q12 h x 1 wk

• mild sedation PRN

• neuroprotection

the only validated neuroprotective agent is nimodipine

studies on the use of IV magnesium and endothelin-A receptor antagonist (clazosentan)showed

reduction in DCI and vasospasm, respectively, without any effect on functional outcome

a trial on the use of statins did not show any neuroprotective benefit

r -x

L J

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Complications

• vasospasm:vasoconstriction and permanent pathological vascular changes in response to vessel

irritation by blood can lead to delayed cerebral ischemia and death

onset: 4-14 d post-SAH, peak at 6-8 d; most commonly due to SAH, rarely due to ICH/IVH

• clinical features(new onset ischemic deficit):confusion, decreased LOC,focal deficit (speech or

motor, e.g. pronator drift)

risk factors:large amount of blood on CT (high fisher grade),smoking,increased age, HT'

N

“symptomatic"vasospasm in 20-30% of SAH patients

“angiographic” vasospasm in 30-70% of arteriograms performed 7 d following SAH

diagnosed clinically, and/or with transcranial Doppler (increased velocity of blood flow)

risk of cerebral infarct and death

treatment

hyperdynamic (“triple H”) therapy using fluids and pressors, usually after ruptured

aneurysm has been clipped/coiled

direct vasodilation via angioplasty or intra-arterial verapamil for refractory cases

• delayed cerebral ischemia: neurological deterioration persisting >1 h in the absence of any obvious

contributing physiological,radiological, or laboratory abnormalities

peaks 4-10 d post-ictus

can progressto cerebral infarction and is associated with significant morbidity and mortality

• mechanism behind DG is unclear, hut includes vasospasm, vascular dysautoregulation,

neurotoxic effects from the blood breakdown products, inflammation, micro-thrombi, and

corticalspreading depolarizations

» it is an essential target for SAH management

• hydrocephalus(15-20%):due to blood obstructing arachnoid granulations

can be acute or chronic, requires extraventricular drain orshunt, respectively

• neurogenic pulmonary edema

• hyponatremia:due to cerebral salt wasting (increased renal sodium loss and EG;

volume loss), not

S1ADH

• Dl

• cardiac:arrhythmia (>50% have ECG changes), Ml,CHF

VASOGRADE

VASOGRAOi WFNS Modified

Fisher scale

Green M 1-2

Yellow 1-3 34

Red 45 Any

The Durability of Endovascular Coiling vs.

Neurosurgical Clipping of Ruptured Cerebral

A ncurysms:18 Yr Follow-Up of The U K Cohort

of the International Subarachnoid Aneurysm

Trial(ISM)

lancet 2015:385(9969):691-697

Methods: RCT comparing endovascular coiling

treatment with craniotomyand dipping for luptured

intracranial aneurysms in 2143 patients who were

considered eligible for either modality or therapy

between 1994-2002.1644 patients were Mowed lor

deaths and outcomesfor10-18.5 yr.

Results:At10 yr.83% of endovascular coiling group

and 79% of neurosurgical clipping groupwere alive.

82% of patientstreated with endovascular coiling and

78% of patients treated with neurosurgical dipping

were independent.Fatients m the endovascular

group were more likely to be alive and independent

at10 yr vs.neu rosurgery group (081.34,95% Cl

1.07-1.67). Rebleeding risks from target aneurysm for

endovascular group and neurosurgery groupwere

0.0216 (95% Cl 0.0121 0.0383) and 0.0064|95% CI

0.0024-0.0173),respectively..

Conclusions:

IThe probability of death or dependency was

significantly greater in the neurosurgical group (vs.

endovascular group) at10 yr follow-up.

2.Rebleeding was more likely in endovascular group

(vs. neurosurgical group), but risk wassaall at 10

yr follow-up.

3. Probability of disability-free survival was

significantly greater in the endovascular group (vs.

neurosurgical group) at 10 yt follow-up.

Prognosis

• 10-15% mortality before reaching hospital, overall 50% mortality (majority within first 2-3 wk)

• 30% ofsurvivors have moderate to severe disability'

• a major cause of mortality is rebleeding, for untreated aneurysms:

• risk of reblecd: 4% on 1st day, 15-20% within 2 wk, 50% by 6 mo

• if no rebleed by 6 mo, risk decreases to same incidence as unruptured aneurysm (2%)

• only prevention is early clipping or coiling of “cold" aneurysm

rebleed risk for “perimesencephalic SAH” is approximately same asfor general population

Intracranial Aneurysms

Epidemiology

• prevalence 1-4% (20-30% have multiple)

• 1

;

>M; 35-65 yr (mean age of presentation is 50 yr)

Types

• saccular (berry)

most common type

located at branch points of major cerebral arteries (circle of Willis)

85-95% in carotid (anterior) system, 5-15% in vertebrobasilar (posterior) circulation

• fusiform

atherosclerotic

more common in vertebrobasilarsystem, rarely rupture

• infectious(mycotic)

secondary to any infection of vessel wall, 20% multiple

60% Streptococcus and Staphylococcus

• 3-15% of patients with bacterial endocarditis

Most Common Locations of Saccular

Aneurysms

• Anterior communicating artery

(ACom):30%

• Posterior communicating artery

(PCom):25%

- MCA:20%

• Basilar tip:7%

Risk Factors for Saccular Aneurysms

Smok ing

HTN

Adult Polycystic kidney disease

Ehlers-Danlos syndrome

Family history:>2 first-degree relatives

Risk Factors

• autosomal dominant polycystic kidney disease (15%)

• fibromuscular dysplasia (7-21%)

. AVMs

• connective tissue diseases (Ehlers-Danlos syndrome, Marfan syndrome)

• family history

• bacterial endocarditis

• Osier-Weber-Kendu syndrome (hereditary hemorrhagic telangiectasia)

• atherosclerosis, HT N, and smoking

• trauma

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Table 16. Five Year Cumulative Rupture Risk in Unruptured Aneurysms Based on Size and

Location

Long-Term.Serial Screening for Intracranial

Aneurysms in Individuals wilti a Family History

d Aneurysmal Subarachnoid Hemorrhage:A

Cohort Study

lance!Neurol 2014:13:385-392

Purpose: Toei amine the y.eld of long-term serial

screening lor Intracranial aneurysms loi Individuals

with a positive famdy history ol aneurysmal

subarachnoid hemorrhage (aSAH) (hroor more first

degree relatives who have had aSAH or unruptured

Intracranial aneurysms).

Study:Screening results Iron April 11993 toApril 1

2013wece reviewed in a cohortstudy.MSAor CIA was

done from ages16-18 to ages 65 )0.Alter a negative

screen, individuals were advised to contact IheOnme

hsSyrfoi follow-up.

Results:Aneurysmswere identified in11% of

indivvduals al (listscreening|n-458),8% at second

screening (n*

261).5% atlhird screening (n-128|.

and &% atfourth screening (n*63|.Smoking (OR 2.

)

.

95% Cl1.2-5 j), history of previous aneurysms(3.9.

1.2-12.

)).and fami al history olaneurysms(3.5.

1.68.1) were significant risk factorsfor aneurysm at

first screening. History ol previous aneurysms vrastte

only significant risk factor for aneurysms at follow -up

screening (HR 4.5.95% Cl1.1-18.)).

Conclusions: Ihe benefit ol long- term screening in

individuals with a family history of aSAH issubstantial

up to and after 10 yr of follow-up and twn initial

negative screens.

Cavernous Carotid ACAorACom/MCA/ICA Vertebrobasilar/PCAtPCom

*7mm 0% 0% 2.5%

7-12 mm 0% 2.6% 14.5%

13-24 mm 3%

v

24 mm

14.5% 18.4%

6.4% 40% 50%

ACA = anterior cerebral artery:ACom = anterior communicating artery:ICA -internal carotid artery:MCA - middle cerebral artery: RCA- posterior

cerebral artery: PCom = posterior commuiicating artery.

Table adopted Irorn the ISUIA Trial: lancet 2003:362:W3-!10

Clinical Features

• rupture (90%), most often SAH, but 30% ICH, 20% IVH, 3% subdural bleed

• sentinel hemorrhage (“thunderclap H /A") > requires urgent clipping/coiling to prevent catastrophic

bleed

• mass effect (giant aneurysms)

• ICA or ACom aneurysm may compress:

the pituitary stalk or hypothalamus causing hypopituitarism

the optic nerve or chiasm producing a visual field defect

basilar artery aneurysm may compress midbrain, pons (limb weakness),or CN III

PCom aneurysm may produce CN III palsy

intracavernous aneurysms (CN 111, IV, VI, V2, VI)

• distal embolization (e.g. amaurosisfugax)

• seizures

• H/A (without hemorrhage)

• incidental CT or angiography finding (asymptomatic)

Investigations

• CTA, MRA, cerebral angiogram

Treatment

• ruptured aneurysms

overall trend towards better outcome with early surgery or coiling (48-96 h after SAH)

treatment options: surgical placement of dip across aneurysm neck, trapping (clipping of

proximal and distal vessels), coiling using (iuglielmi detachable coils, (low diversion stents,

wrapping (last resort)

choice of surgery vs. coiling: consider location,size,shape, and tortuosity of the aneurysm,

patient comorbidities, age, and neurological condition; in general:

endovascular coiling > clipping for ruptured intracranial aneurysmssuitable for both

treatments -> greater survival benefit at 1 yr with sustained effect for up to 7 yr post-treatment

coiling: posterior > anterior circulation, deep/eloquent location, basilar artery bifurcation/

apex, older age, presence of comorbidities, presence of vasospasm

clipping:difficult endovascular access, broad aneurysmal base, branching arteries at the

aneurysm base, tortuosity/atherosclerosis of afferent vessels, dissection, hematoma, acute

brainstem compression

• unruptured aneurysms

average 1.4% annual risk of rupture; predictors include: age, HTN, history of SAH, aneurysm size

and location, and geographical region (Finnish people = 3.6 times increased risk;Japanese people

= 2.8 times increased risk)

no clear evidence on when to operate; need to weigh life expectancy

• risk of niorbidity/mortality of SAH (20-50%) vs. risk of coiling (

-2%)

generally treat unruptureu aneurysms >10 mm

• treatment guided by balance of risks of SAH per ISUIA and PHASES and of intervention per

centre experience and outcomes

follow smaller aneurysms with serial angiography

The Unruptureil Intracranial Aneurysm Treatment

Score

Ffc.rc ogy 2015:85(101:881 839

Purpose: To develop an unruptured intracranial

aneurysm (UIA) treatmentscore|UIA!$|model lira!

includes and quantifies key lectorsinvolved in clinical

decision- making m the management of UlAs and lo

assess agreement for this model airo'g specialists in

UIA management and research.

Methods: An international mullidisup inary

(neurosurgery, neuroradiology. neurology, clinical

eptdeminlogyl group of 69 specaiists was convened

to develop and validate the UIAIS model using a

Delphi consensus method .

Results: Hie UIAIS accountslor 29 key factors m UIA

management.

Conclusions: T'

is novel UIA decs on guidance

study captures an encellent consensus among

highly informed individuals on UIA management,

irrespective of their underlying specialty.

See landmark Neurosurgery Trials ta£>le for more

information on the natural history ol unrupluied

intracranial aneurysms and the risk associated with

the repair.

Intracerebral Hemorrhage

Definition

• hemorrhage svithin brain parenchyma, accountsfor ~10% of strokes

• can dissect into ventricular system (IVH) or through cortical surface (SAH )

Etiology

• HT N (usually causes bleeds at putamen, thalamus, pons, and cerebellum)

• hemorrhagic transformation (reperfusion post-stroke,surgery,strenuous exercise, etc.)

• vascular anomalies

aneurysm, AVMs, and other vascular malformations (see Vascular Malformations, NS27)

venoussinus thrombosis

arteriopathies (cerebral amyloid angiopathy, lipohvalinosis, vasculitis)

location of ICH

• Basal ganglia/internal capsule (50%)

• Thalamus (15%)

• Cerebral white matter (15%)

• Cerebellum/brainstem - usually

pons (15%)

• Other (5%)

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NS26 Neurosurgery Toronto Notes 2023

• tumours(1%):often malignant (e.g. GBM, lymphoma, metastases)

• drugs(amphetamines,cocaine, alcohol, anticoagulants, etc.)

• coagulopathy (iatrogenic,leukemia, thrombotic thrombocytopenic purpura, aplastic anemia)

• CNS infections(fungal,granulomas, herpessimplex encephalitis)

• post-trauma (immediate or delayed,frontal and temporal lobes most commonly injured via coupcontrecoup mechanism)

• eclampsia

• postoperative ( post-carotid endarterectomy cerebral reperfusion, craniotomy)

• idiopathic

ICH Score Components

• GCS score (3-4-2 pts;5-12-1pt,

13-15-

0pt)

. ICH volume(>30 cm~

1pt,<30 cm-Q

pi)

. Presence of IVH (yes-1pt no-0 pt)

. Infratentorial origin (yes-1pt,no'

0

• Age (i80-1pt <80 *

0 pt)

Epidemiology

• 12-31 cases in 100000 population per yr

Surgical Dedsrca Makiag inBrain Hemorrhage:

Hew Analysis of theSIKH.STICK IIand STITCH

(Tranra) Bandocaed Trials

Stroke 2015:50:1108-1115

Summary:IheSICH(Snrgical Trial in Lobar

IntracerebralBesonhage)I(“1033 patients)and

II(n401patents)trials randomized patients with

spontaneoss ateceehralhemorrhage (ICH)to

early sargeryorrmtaltyaiasenatrire treatment.The

STITCH (Tranma)triadimestgatedthese options in

the entailof tead-apredpatents(n-170 patients).

Ilea-analyse of spontaneous ICH patients suggests

that thosepresentrgnoa 6CS0110-13 anda large

KHare more Skety to benefit from early surgery

than'

Josepresentegndh a CCS ontside this range.

S»gical treatseaof fsroatic ICH with CCS10-13

-ares - a- . oe-eSca ariOMS

Refer athe landmark lenrosnrgery trialsable for

details of STICH.

Risk Factors

• increasing age (mainly >55 yr)

• male

• HTN

. Black/Asian > White

• previous cerebrovascular accident of any type (23 times risk)

• both acute and chronic heavy EtOH use; cocaine, amphetamines

• liver disease

• anticoagulants

Clinical Features

• TIA-like symptoms often precede ICH, can localize to site of impending hemorrhage

• gradual onset of symptoms over minutes-hours, usually during activity

• H/A, N/Y,and decreased LOG are common

• specific symptoms/deficits depend on location of ICH

Investigations

• baseline severity score such asthe ICH Score should be performed as part of the initial

workup

• hvperdense blood on non-contrast CT

• CTA routine,ifspot sign (contrast in the hematoma) demonstrated there is high likelihood of clot

growth

Spetder-Martin AVM Grading Scale

Rea Store

Size

Treatment

• patientsshould be transferred to and managed in a neuro-ICC orstroke unit

• medical

• decrease MAP to pre-morbid level or by -20% (target BP 140/90) in emergency department

• check partial thromboplastin time/international normalized ratio (PTT/1NR), and correct

coagulopathy (immediate reversal of anticoagulation)

• control raised ICP (see Intracranial Pressure Dynamics, SS4 )

• corticosteroidsshould NOT be used for elevated ICP in ICH

0-3 re

Wire 2

4c- 3

location

hfrdow*

0

Oogocct

OtepVzoonsOrainagt

Httpceswt

Presetf

I

levetiracetam/phenytoin for seizure prophylaxis

• follow electrolytes (S1ADH common)

• angiogram to rule out vascular lesion unless >45 yr,known HTN,and putamen/thalamic/

posterior fossa ICH (yield -0%)

0

ZVU varies w? ukdntod by nddntg trio 3 individual

Sperite-HortiSafe scare horn the above table.

-9- a 2 cn hnctx e rcr

-etoquetit locaticci without

bawtage = Grade I

• surgical

* craniotomy with evacuation of clot, treatment ofsource of ICH (i.e.AVM, tumour, cavernoma),

ventriculostomy to treat hydrocephalus

• indications

symptoms of raised ICP or mass effect

rapid deterioration (especially ifsigns of brainstem compression)

favourable location (e.g. cerebellar, non-dominant hemisphere)

young patient (<50 yr)

suspected tumour, AVM, aneurysm, or cavernoma (resection or clip to decrease risk of

rebleed)

• contraindications

small bleed:minimal symptoms, GCS >10

poor prognosis: massive hemorrhage (especially dominant lobe), low GCS/coma, lost

brainstem function

medical reasons (e.g.advanced age,severe coagulopathy,difficult location (e.g. basal ganglia,

thalamus)) n

u

Prognosis

• 30 d mortality rate 44%,mostly due to cerebral herniation

• rebleed rate 2-6%,higher if HTN poorly controlled +

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XS27 Neurosurgery Toronto Notes 2023

Vascular Malformations

Types

• AVMs

• cavernous malformations (cavernomas, cavernous hemangiomas/angiomas)

• venous angioma

• capillary telangiectasias

• AY1 (carotid-cavernous fistula, dural AYF,vein of Galen aneurysm)

•

“angiographically occult vascular malformations” (any type, 10% of malformations)

Arteriovenous Malformations, Cavernous Malformations,

and Dural Arteriovenous Fistulas

Table 17. Comparison of Pathoetiology,Clinical Features, and Treatment of Arteriovenous

Malformations, Cavernous Malformations, and Dural Fistulas

Arteriovenous Malformations Cavernous Malformations Dural Fistulas

Definition Tangle of abnormal vessels/arteriovenous Benign vascular hamartoma

shunts,with no intervening capillary beds consisting ol irregular sinusoidal

or brain parenchyma;usually congenital vascular channels located within

Frstu'as connecting dural arteries to

dural veinsor the dural sinus

frequently occur at the transverse and

the brain without intervening neural cavernous sinuses,but can be found at

tissue or associated large arteries/ every cranial dural sinus

Hypothesised to be related to venous

Several genes now described:CCM1. sinus thrombosis formation,and

subsequent microvascular shunt

lor.mat on within the dura between

arteries and veins

Unknown trueincidence

Constitute 10-15% of all intracranial

vascular abnormalities

veins

CCM2.CCM3

Epidemiology Prevalence -0.14%.M:F"2:1.average age Prevalence ol0.10.2%,both

sporadic andhereditary forms

described

Figure 21. MRI of cavernous

malformation

A. T2-weighted imaging MRI

B.Gradient echo sequencing MRI

at diagnosis-33 yr

15-20% ol patients with hereditary

hemorrhagic telangiectasia (Osier-WeberRendu syndrome)will havecerebral AVUs

Clinical Features Hemorrhage (40-60%);small AVMs are

more likely to bleed due to directhigh

pressure AV connections

Seizures (50%);more commonwith

larger AVMs

Mass effect

Focal neurologicalsigns secondary

to ischemia (high (low "steal

phenomena")

localized H/A,increased ICP

Bruit (especially with dural AVMs)

May be asymptomatic (“silent")

Investigations MRI (flow void),MRA

Angiography (7% will also have one or

more associatedaneurysms)

Seizures (60%),progressive

neurological deficit (50%),

hemorrhage (20%),H/A

Often an incidental finding

Hemorrhage risk less than AVM.

usually minor bleeds

Asymptomatic,pulsatile tinnitus if

involving sigmoid or transverse sinuses,

bruits.H/A

Carotid cavernousinvolvement

classically produces proptosis,

chemosis.and bruits

Symptoms of SAH,S0H.or ICH

Clinical Course ofUntreated Cerebral Cavernous

Nalforwations (CCM)

laxe:leant2015 pi.

^

1474-4422(15)00303-8

Purpose. loohCam precise estimates and predictors

of tteris< of rtratrana semorrhage (ICH) in patients

urth.

^

treated cerebral cavernous malformations

(CCMs).

Methods Colected individual patient data from

iwestigMhtsof pubkstedstudies on MEDLINE aid

Eriasesnce mteoSon cut April 201517 cohorts

from 6 sides.-16211) on clmcalcourse from CCM

dagnpss 5rsiCCM treatment or last armlaile

Hnp

Results:2Mof tte1520patients experienced ICH

darng 5187persoc-yr -nllouv-up (Kaplan-Meier

estoaSd5 yr risk 15.8%.95% Cl13.7-17.9).ICH

irtnSyr of CCM degnoss was associated with

clinical presernateo with ICH or focal neurological

deScitw-thoatbra n imaging evidenceof recent

renrrtage(is.Oder presentations;HR 5,6.95% Cl

32-9.7)asd»8b-amstem CCM location|vs.other

locahoos;Hi44.95% 02.3-8.6).

Conclusions :liMode of deucal presentation and

(2) CCM scatoc a-e rdeoendentlyassocratedwith

ICH w“

- 5 yr of CCM diagnosis. The risk of recurrent

hemortage‘

-or a CCM is greater than the risk of the

hrst ere:rddec!res over 5 yr.

T2-weighted image MRI|nonenhancing)

Gradient echo sequencing (best for

diagnosis)

Surgical excision:

Only appropriate for symptomatic

lesions that are surgically

accessible (supratentorial lesions

are less likely to bleed than

infratentorial lesions)

Ang ogr aphy remains the gold standard

Non-enhanced CT to rule out hemorrhage

MRI:however,this does not demonstrate

the arterial supply to the fistula

Approach is dependent on size,location

and symptoms,and includes:

Conservative treatment

Neuroradiotogical endovascular

interventions

Radiation therapy

Surgery

Combination olthe above

Decreases risk of future hemorrhage

and seizure

Surgical excisionis treatment of choice

even in Spetzler-Martin gradesI-IIwith

general good health

SRS is preferred tor small (<3 cm) or very

deep lesions

Endovascular embolization (glue,balloon)

can be curative (5%) or used as adjuvant

to surgery or SRS in larger lesions

Conservative (e.g. palliative

embolization,seizure control if

necessary)

12-66% mortality.23-40% morbidity

(serious neurologicaldeficit) per bleed

Risk olmajor bleed in untreatedAYMs;

2-4%/yr

Outcomes dependon Speltzer-Martm

grade

Treatment

Annual bleeding rates:0.25-1.1% for 8.1% anrnalrisk of hemorrhage

supratentorial,2-3% for brainstem 6.9% annual risk for non-hemorrhagic

Symptomatic lesions have a higher neurological deficit

hemorrhage risk than asymptomatic 10.4%mortality rate

Outcomes influencedby dural fistula

type (presence olcortical venous

drainage -•poorer outcomes)

Prognosis

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Cerebrospinal Fluid Fistulas

Suspect CSF fistula in patients with

otorrhea or rhinorrhea after head trauma

or recurrent meningitis

Etiology

• cranial orspinal

• traumatic:after head trauma,iatrogenic (post-transsphenoidal surgery, post skull base surgery)

• nontraumatic:high pressure (hydrocephalus, tumour), normal pressure (bone erosion secondary to

infection, congenital defect)

Clinical Features

• otorrhea or rhinorrhea (clear fluid)

• low pressure H/A (worse when sitting up)

• confirmatory testing for CSF:(5-transferrin test, quantitative glucose analysis of fluid, “ring sign",

“reservoir sign'

Investigations

• CT (detect pneumocephalus,fractures,skull base defects), water contrast CT cisternography

Ring Sign:If CSF is mixed with blood.

Allow CSF to drain onto the surrounding

sheets;positive if dear in centre with

surrounding blood coloured ring (double

ring sign)

Reservoir Sign:Gush of CSF leaks out in

certain head positions (i.e.teapot sign):

not specific or sensitive

Treatment

• lower ICP (avoid straining, acetazolamidc to reduce CSF production, modest fluid restriction)

• persistent leak: may require continuous lumbar drainage via percutaneous catheter

• surgical indications: traumatic leak lasting >2 wk,spontaneous leaks,delayed onset of leak after

trauma orsurgery, leaks complicated by meningitis

Red Flags for Back fein

BACK PAIN

Bowel/Bladder (retention or

incontinence)

Anesthesia (saddle)

Constitutional symptoms

“K"hronic disease

Parasthesia

Age >50 or <20

IV drug use

Neuromotor deficits

EXTRACRANIAL PATHOLOGY

Approach to Limb/Back Pain Cauda Equina

Urinary retention or incontinence,fecal

incontinence or loss of anal sphincter

tone,saddle anesthesia,uni/bilateral leg

weakness/pain

Malignancy

Age >50,previous Hx of cancer,pain

unrelieved by bed rest constitutional

symptoms

Infection

Increased ESR.IV drug use.

immunosuppressed.fever

Compression Fracture

Age >50,trauma,prolonged steroid use

• see Orthopaedic Surgery

Extradural Lesions

Post circulation

Ant circulation

AXIAL SECTION OF

THORACIC SPINE

-

[

Dorsal

funiculus

asciculus gracilis

.Fasciculus cuneatus Posterior spinal

artery

Dorsal horn

(sensory!

.lateral

corticospinal

Lateral hon tract (efferent)

(autonomic! j 'jL

*onlv present

T1-LZS2 SS \

-

lateral

funiculus

,O J

n .f

-Spinothalamic

tract (afforcntl Ventral horn

(motor)

Anterior

spinal artery

Ventral

funiculus Anterior

corticospinal

tract (efferent)

Posterior spinal aa.

Anterior

segmental

medullary a.

Arachnoid mater /.Dura mater

Post & ant. interior spinal a.

reticular aa.

Branch to vertebral

body & dura mater

Dorsal branch - of intercostal a

Spinal a.

Thoracic aorta

r1

L J

Intercostal a. © Natalie Cormier 2D1S.after Takami lijima +

Figure 22. Vascular supply of spinal cord

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Root Compression

Sensory Fibres

• Fasciculus gracilis/cuneatus:

proprioception,fine touch,vibration

• Spinothalamic tract: pain and

temperature

Motor Fibres

• Corticospinal tract:skilled

movements

•radiculopathy is a pain and/or sensorimotor deficitsyndrome that involves compression of a nerve

root.Nerve compression generally occurs as a result of disc herniation, degenerative disc diseases

(spondylosis),instability, and masses (rare)

•patients generally present with referred pain,sensory changes (numbness and/or tingling) or

weakness. Whereas patients might sometimes describe sensory changes in a dermatomal distribution,

the referred pain will not be in a dermatomal distribution.The areas of pain and altered sensorium

may be incongruent

•muscle innervation hasless overlap than sensory innervation and hence is a better predictor of level of

pathology

Differential Diagnosis

•herniated disc

•neoplasm (neurofibroma,schwannoma)

•synovial cyst,abscess

•hypertrophic bone/spur

Cervical Disc Syndrome

Etiology

• nucleus pulposus herniates through annulus fibrosus and impinges upon nerve root, most commonly

Disc herniations impinge the nerve root

at the level below the interspace fie.

Clinical C5-6disc affectsthe C6 nerve root)

Features

• pain in arm follows nerve root distribution,worse with neck extension,ipsilateral rotation, and lateral

flexion (all compressthe ipsilateral neural foramen)

• LMN signs and symptoms (diminished reflexes,non-spastic motor weakness)

• central cervical disc protrusion may cause myelopathy as well as nerve root deficits

Investigations

• if red flags: cervical spine (C-spine) x-ray,Cl'

, MR1 (imaging of choice)

• only consider HMG/nerve conduction studies if diagnosis uncertain and presenting more as peripheral

nerve issue

Treatment

• nonsurgical

• no bed rest unlesssevere radicular symptoms

• activity modification, patient education (reduce sitting,lifting)

physiotherapy, exercise programsfocus on strengthening core muscles

• analgesics;NSAlDs are more efficacious

• avoid cervical manipulation like traction

• surgical indications

anterior cervical discectomy is the usual approach (posterior foraminotomy with discectomy is

the other option)

• intractable pain despite adequate conservative treatment for >3 mo

progressive neurological deficit

Prognosis

• 95% improve spontaneously in 4-8 wk

Table 18.Lateral Cervical Disc Syndromes

C4-5 C5-6 C6-7 C7-T1

Root Involved C5 C6 C7 C8

Incidence

Sensory

Motor

2% m. 69% 10%

Shoulder

Deltoid,biceps,

supraspinatus

No change

Middle finger

Biceps,wrist extensors Triceps

Thumb Ring finger.Sth finger

Digital flexors,intrinsics

Reflex Biceps,brachioradialis triceps Finger jerk (Hoffmann's

r n

i.J

+

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Degenerative Cervical Myelopathy

Definition

• progressive degenerative process of cervical spine leading to canal stenosis; congenital spinal

stenosis;degeneration of intervertebral discs;hypertrophy of dura or ligaments;subluxation; altered

mobility; telescoping of the spine due to loss of height of vertebral bodies; alteration of normal lordotic

curvature

• resultantsyndromes:mechanical neck pain,radiculopathy (root compression),myelopathy (spinal

cord compression)

Epidemiology

• typically begins at age 40-50,M>F,most commonly at the C5-C6 > C6-C7 levels

Pathogenesis

• any of:disc degeneration/herniation,osteophyte formation, ossification, and hypertrophy of

ligaments

• pathophysiology includesstatic compression,dynamic compression, and vascular compromise

Clinical Features

• insidious onset of mechanical neck pain exacerbated by excess vertebral motion (particularly rotation

and lateral bending with a vertical compressive force Spurling'

stest)

• the earliest symptoms are gait disturbance and lower extremity weakness or stiffness

• occipital H/A is common

• radiculopathy may involve 1 or more roots,and symptomsinclude neck,shoulder, and arm pain;

paresthesias;and numbness

• cervical spondylotic myelopathy may present with:

weakness (upper > lower extremity),lower extremity weakness (corticospinal tracts) is most

worrisome complaint

decreased dexterity,lossof fine motor control

sensor)'changes

UMN findings such as hyperreflexia,clonus, and Babinski reflex

funicular pain,characterized by burning and stinging ± Lhermitte’

ssign (lightning-like

sensation down the back with neck flexion)

Investigations

• x-ray of cervicalspine ± flexion/extension (alignment,fractures)

• MR1 most usefulfor determination of compression of the neural element

• CT is only used for better determination of bony anatomy (i.e.OPLL)

• HMG/nerve conduction studiesreserved for peripheral nerve investigation

Cervical spondylotic myelopathy isthe

most common cause of spinal cord

impairment

'

Clinical Grading Scoresto Assess CSM

• Modified Japanese Orthopaedic

Association (mJOA)

• Nunck Grade

• Neck Disability Index

A ClinicalPractice Gnidetine for dtMaaagcntn:

ofPrintsnritk DagncratinCtmul

Mjelopatbj(OCM):iKoaandrionsta

Patients with Mild. Moderate,aadSeme Disease

and NonaayelcpatAic Patients witkEvidence of

CordCoapressioo

(<obil Spue Josraa!20W:7|3S)2«S43S

Sente ndaoderateDCM Moderateendeete

soggestnag stoegrecosneodatoo of sorgcal

initriwtioa.

Mild DCM:legIontoIonerdetce saggssti-g

offeringsorgcalicteneitiOfl or a sinefared

retrain!trio:aaddeoo-ogerriienasageaeot

naitiaMy persaed.coasder operatneEotenertoo if

endeset of oenrologcai deteriocatoa_

oo-nyelopatkk patientsnitkoitradialopatky

In sadpriestsnidisagagendeace af cemcai

popAjIacticsBrgerj:coaaeledacate.and felon

cfaolp.

an-nyelopatkic patientsvitk radiolopatky:

Sock prietSsnttcsgcgerdetceof terrcal

cord canpressioo are at a tgter risk of deielopng

•rjekipadjaadskatid becaarseled.OMersurgical

or nosoperetiae treatamt nrfl appraprratsfo5ow-«p

and stiict_red reatiitatioe.

Figure 23.CT (left) and MRI (right)representations of cervical spondylosis

Images courtesy of Or.Eric Masskotte r n

L J

Treatment

•nonsurgical: physiotherapy, anti-inflammatory medications

•surgical:anterior approach (anterior cervical discectomy or corpectomy), posterior approach

(decompressive cervical laminectomy)

•in multilevel degenerative cervical myelopathy (DCM), both anterior and posterior options are

acceptable approaches with generally comparable outcomes

• with kyphosis -> anterior approach generally preferred

+

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• with preserved cervical lordosis -> posterior approach generally preferred

• surgical indications: myelopathy with motor impairment, progressive neurologic impairment,

intractable pain

• complete remission almost never occurs;surgical decompression stops progression of disease in

almost all cases; 80'V, of patients experience neurological improvement

Table 19.2017 Summary AO Spine-CSRS Guideline for the Management of Degenerative Cervical

Myelopathy

Patient Population Level of Recommendation Guideline/Recommendation

Severe DCM (raJOA 0-H)

Moderate 0CM|mJ0A 1244)

Mild DCM {mJ0A1S.1T)

Strong

Strong

Surgical intervention isrecommended

Surgical intervention is recommended

Surgical intervention or structured rehabilitationis recommended:

consider surgery if withneurologic deterioration or failure to

improve

Prophylactic surgery isnot recommended

Weak

Non-myelopathic patients with Weak

cord compression and without

radiculopathy

Non-myElopathic patients with cord Weak

compression and withrad.allopathy

Either surgical intervention or nonoperative treatment(dose

follow-up or structured rehabilitation)

Lumbar Disc Syndrome

Definition

• compression of nerve roots caused by herniation of the nucleus pulposus through the annulus fibrosus

of an intervertebral disc in the lumbar spine

Etiology

• posterolaterally herniated disc compressed nerve root exiting BELOW the level of the disc or the

traversing nerve root

• far lateral disc herniation compressed nerve root AT the level of the disc or the exiting nerve root

• central herniation may cause cauda equina compression or lumbar stenosis (neurogenic claudication)

Clinical Features

• initially back pain,then leg pain > back pain

• limited back movement (especially forward flexion) due to pain

• motor weakness, dermatomal sensory changes, decreased reflexes

• exacerbation with Valsalva; relief with flexing the knee or thigh

• nerve root tension signs

• straight leg raise (SLR) (Lasegue’s test) or crossed SLR (pain should occur at less than 60°)

suggests L5, SI root involvement

• femoral stretch test suggests L2, L3, or L4 root involvement

Figure 24.T2-weighted MRI of

lumbar disc herniation

Investigations

• MRI is modality of choice

• x-ray spine (only to rule out other lesions), CT (bony anatomy)

myelogram and post-myelogram CT (only if MRI is contraindicated)

See landmark Heu-osa-gery Inals table for mote

i-brmat^

"e SPOBI trial fir outcomes of surgery

*

.rorooeraive care foe lumbar diseberniabun.

Treatment

• nonsurgical (same as cervical disc disease)

• surgical indications:same as cervical disc and cauda equina syndrome

Magnetic BesoiaiceImaging inFollow-Up

Assessaeniof Sciatica

IBM 2013:3S85$9-M)0?

Backgroud: Fo cn .:MB) is a coistroveisia!

etkod for nKSrrgsciatica c patients wifi known

liBSar-dsckertateo.

Metlods: Paridpants(n-283|weierecruited

froa a s

=ul2:eoas. parallel,raodomraed study

coaparmg surgery aid conservative care loi sciatica

(aeSciatica trial).MBI and clinical assessment weie

usderulei prMreatmett and 1 yi post-tieatment

’ri:~ to nsualiae disc herniation and

evaluate outome.

Besitts 1p.4sc tar- ation was visible in 35%

wis a fanuraieoutcome (complete,or nearly

carpea sy-jtom resolntjos) acid m 33% wifi

ai uifavou-cSie aut:ire (NI.70).A favourable

outcome was-eocried v:85%. of patients with disc

henetoa erd13% wiiewt isc heiniatioo (H)J0|.

Conclusions:Aretoniccl abnormalities visible on

itbeSrd1011 perne-treatmentforsciabca due to

taber-dsc temaSoo cou d not distinguish patients

witt resobtoa of theirsymptomsfrom patientsstill

eipe-ercog symptoms.

Prognosis

• 95% improve spontaneously within 4-8 wTk

• those who do not improve writh conservative treatment achieve symptom relief quicker with surgery

than continuation of conservative management; however, the long-term outcome after surgery is

comparable to conservative therapy

• do not follow patients with serial MRIs; clinicalstatusis more important at guiding management

Table 20. Lateral Lumbar Disc Syndromes

13-4 L4-5 L5-S1

Root Involved L4 L5 S1

r -\

Incidence <10%

Femoral pattern

Medial leg

45% 45% i

_ j

Pain Sciatic pattern

Dorsal foot to hallux

Lateralleg

Extensor halloas longus (hallux

extension)

Medial hamstrings

Sciatic pattern

Sensory Lateral loot

tibialis anterior (dorsiflexion) Gastrocnemius,soleus (plantar +

flexion)

Achilles

Motor

Reflex Patellar

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Table 21.Differentiating Conus Medullaris Syndrome from Cauda Equina Syndrome

Conus Medullaris Syndrome Cauda Equina Syndrome

Onset

Spontaneous Pain

Gradual, unilateral

Rare,if present usually bilateral,symmetric in Severe, radicular type:in perineum, thighs,

perineum or thighs

Saddle:bilateral and symmetric:sensory

dissociation

Sudden,bilateral

legs. back,or bladder

Sensory Deficit Saddle:no sensory dissociation:may be

unilateral and asymmetric

Symmetric:paresisless marked:fascicutabons Asymmetric:paresis more marked: atrophy

may be present:fasciculations rare

Motor Deficit

may be present

Reflexes Only ankle jerkabsent (preserved knee jerk) Knee and ankle jerk may be absent

Sphincter dysfunction presents late; impotence

lessfrequent

Autonomic Symptoms (bladder dysfunction. Urinary retention and atonic anal sphincter

impotence.etc.) prominent early:impotence frequent

Cauda Equina Syndrome

Etiology

• compression or irritation of lumbosacral nerve roots below conus medullaris(below L2 level)

• decreased space in the vertebral canal below L2

• common causes:herniated disc ± spinal stenosis,vertebral fracture, and tumour

Causes of Cauda Equina Syndrome

• Lumbar disc herniation

• Spinal stenosis

. Spinal tumour

• Epidural abscess

• Hematoma

• Trauma

Clinical Features

• usually acute (develops in less than 24 h ); rarely subacute or chronic

• motor (LMN signs)

weakness in multiple root distribution

reduced deep tendon reflexes(knee or ankle)

• autonomic

» urinary retention (or overflow incontinence) and/or fecal incontinence due to loss of anal

sphincter tone

• sensory'

low back pain radiating to legs (sciatica) aggravated by Valsalva maneuver and by sitting;relieved

by lying down

bilateral sensory loss or pain:depends on the level affected

saddle area (S2-S5) anesthesia

• sexual dysfunction (late finding)

Investigations

• urgent MRI to confirm compression of S2-S3-S4 nerve root by a large disc herniation

• post-void residual very helpful to determine if true retention is present; volumes controversial but

anything over 250 cc in a healthy individual is cause for concern

Treatment

• surgical decompression (<48 h) to preserve bowel,Madder, and sexual function, and/or to prevent

progression to paraplegia

• consult radiation oncology for urgentsymptomatic management if palliative oncology patient

Prognosis

• markedly improves with surgical decompression

• recovery correlates with function at initial presentation:if patient is ambulatory, likely to continue to

be ambulatory;if unable to walk, unlikely to walk aftersurgery

Lumbar Spinal Stenosis

Etiology

• congenital narrowing ofspinal canal combined with degenerative changes(herniated disc,

hypertrophied facet joints, and ligamentum flavum)

Clinical Features

• gradually progressive back and leg pain with standing and walking that is relieved by sitting or lying

down or movementsinvolving lumbar flexion (e.g.riding a bicycle,leaning over a shopping cart);

neurogenic claudication 60% sensitive

• neurologic exam may be normal,including straight leg raise test

See landmark Neurosurgery trials(able lor more

information on the SPORI trial lor outcomes ol

s urgery n. nonoperative care forsymptomatic lumbar

spinalstenosis.

Investigations

• MRI is best to confirm and localize the level ofstenosis(unlike nerve root compression which can be

localized with clinical exam)

L J

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Treatment

• nonsurgical: NSAlDs, analgesia, physical therapy

• surgical:laminectomy with root decompression

• fusion typically advised if evidence of segmental instability prior to surgery (e.g. in flexion/

extension x-rays)

Neurogenic Claudication

Etiology

• ischemia of lumbosacral nerve rootssecondary to vascular compromise and increased demand from

exertion,often associated with lumbar stenosis

Key Features of Neurogenic vs.

Vascular Claudication

• Neurogenic Claudication:

dermatomal distribution with

positional relief occurring over

minutes

• Vascular Claudication:sclcrotomal

distribution with relief occurring with

rest over seconds

Clinical Features

• dermatomal pain/paresthesia/weakness of buttock, hip, thigh, or leg initiated by standing or walking

• slow relief with postural changes (sitting >30 min), NOT simply exertion cessation

• induced by variable degrees of exercise or standing

• may be elicited with lumbar extension, but may not have any other neurological findings, no signs of

vascular compromise (e.g. ulcers, poor capillary refill)

Investigations

• bicycle test may help distinguish NC from vascular claudication (the waist-flexed individuals on the

bicycle with NC can last longer)

Treatment

• same asfor lumbarspinal stenosis

Intradural Intramedullary Lesions

Syringomyelia (Syrinx)

Definition

• cystic cavitation of the spinal cord

• presentation is highly variable, usually progresses over mo to yr

• initially pain, weakness;later atrophy and loss of pain and temperature sensation

Etiology

• 70% are associated with Chiari 1 malformation, 10% with basilar invagination

• post-traumatic

• post-infectious

• post-inflammatory

• tumour

• tethered cord

Clinical Features

• nonspecific features for any intramedullary spinal cord pathology:

initially pain, weakness, atrophy, then loss of pain and temperature (spinothalamic tract) in

upper extremities (central syrinx) with progressive myelopathy over years

sensory loss with preserved touch and proprioception (dorsal column-medial lemniscus

pathway) in a band-like distribution at the level of cervicalsyrinx

dysesthetic pain often occurs in the distribution of the sensory loss

LMN arm/hand weakness or wasting

painless neuropathic arthropathies (Charcot’s joints),especially in the shoulder and neck due to

loss of pain and temperature sensation

Figure 25. T1weighted MRI of

syringomyelia

Investigations

• MRI is best method, myelogram with delayed CT

Treatment

• treat underlying cause (e.g. posterior fossa decompression for Chiari l,surgical removal of tumour if

causing a syrinx)

• rarely doesthe syrinx need to be shunted,

r T

only when progressive and size allows for insertion of tube LJ

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Spinal Cord Syndromes

Complete Spinal Cord Lesion

• bilateral loss of motor/sensory and autonomic function at >4 segments below lesion/injury, with UMN

signs

• about 3% of patients with complete injuries will develop some recovery within 24 h; beyond 24 h, no

distal function will recover

American SpinalInjury Association

Impairment Scale

Grade Descriptiot

A Corpete.oo moton'

sensory below

:e:T3 ogee : level including MS

loarajlete.sensory dot not motor

fcuebe- presented below nearoiogica:

ere ackdmgStS

locoaplete.motor function preserved

seem tesrologiul level,and more

Sax badof Sie key muscles below

nnro'

ogcai level have a muscle

grade <3

laciapfcfe.motor function preserved

oe ow resroiogical level,and more

tor ~af of toe key muscles below

neoroog.Q level bare a muscle

grade >3

Iona!motor aed sensory function

B

Incomplete Spinal Cord Lesion

• any residual function at >4 segments below lesion

• signs include sensory/motor function in lower limbs and “sacral sparing"

(perianal sensation,

voluntary rectal sphincter contraction)

C

Table 22. Comparison Between Incomplete Spinal Cord Lesion Syndromes

Syndrome Etiology Motor Sensory

D

Brown-Sequard Herrisection of cord Ipsilateral LMN weakness at the

lesion

Ipsilateral loss of vibration and

proprioception

Ipsilateral UMN weakness below Contralateral loss of painand

the lesion temperature

Preserved light touch E

Anterior Cord Anterior spinal artery compression Bilateral LMN weakness at the

or occasion

Preserved vibration and

proprioception

Bilateral loss of pain and

temperature

Preserved light touch

lesion

Bilateral UMN weakness below T

2 r

the lesion =

Urinary retention •

1

5

•2 1

Central Cord (most common) Syringomyelia,tumours,spinal 5

I

1 £

tiyperextension injury

Bilateral motor weakness:Upper Variable bilateral suspended

limb weakness (LMN lesion) > sensory loss

Lower limb weakness (UMN lesion) Loss of pain and temperature

Urinary retention

m - N

E

C-

»

proprioception

Bilateral

loss of vibration

loss of vibraboo

and

.

C

proprioception,light touch at and

below the lesion

Preserved pain and temperature

Posterior Cord Posterior spinal artery infarction. Preserved

trauma I

Ifttt Peripheral Nerves

• see Nuurnlogy. N38

Classification

Table 23. Seddon’s Classification of Peripheral Nerve Injury

© Jenna Rebelo 2010y

Nerve Injury Description Recovery

Figure 26.Spinal cord lesion

syndromes Neurapraxia (classI)

Aionotmesis (class It)

Axon structurally intact but fails to function

Axon and myelin sheath disrupted butendoneurium and Spontaneous axonal recovery at1mm/d.max at12 yr

supporting structures intact-» Val erian degeneration

of axon segment distal to injury

Nerve completely transected

Within h to mo (average 6 -8 wkj

Neurotmesis (class III) Need surgicalrepair tor possibility of recovery

Etiology

• ischemia

• nerve entrapment (compression) by nearby anatomic structures, often secondary to localized,

repetitive mechanical trauma with additional vascular injury to nerve

• direct trauma (e.g. transection)

• iatrogenic

Investigations

• clinical exam: muscle bulk and tone, power,sensation, reflexes, localization via Tinel’

ssign

(paresthesias elicited by tapping along the course of a nerve)

• electrophysiological studies: EMG/nerve conduction study (assess nerve integrity and monitoring

recovery after 2-3 wk post-injury)

• labs: blood work (e.g.CBC,TSH , vitamin Bit),CST

• imaging: C-spine, chest/bone x-rays, myelogram, CT, magnetic resonance neurography, angiogram if

vascular damage issuspected

ri

iJ

Treatment

• early neurosurgical consultation if injury issuspected +

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XS35 Neurosurgery Toronto Notes 2023

Table 24. Treatment by Injury Type

Injury Treatment

Nonsurgical: Prevent repeated stress/injur/

,physiotherapy.NSAIDs. local anesthesia/steroid injection

Surgical:Nerve decompression t transposition for progressive deficits, muscle weakness/atrophy, failure of medical

management

Follow up clinically for recovery;exploration if no recovery in 3 mo

If no evidence of recovery, resect damaged segment

Prompt physical therapy and rehabilitation to increase muscle function, maintain joint ROM.maximire return of useful

function

Recovery usually incomplete

Surgicalrepair of nerve sheath unless known to be intact {suture nerve sheaths directly if ends approximate or nerve

graft {usually sural nerve))

Clean laceration:early exploration and repair

Contamination or associated injuries: tag initially with nonabsorbable suture, reapproach within 10 d

Entrapment

Stretch/Contusion

Blood vesselsAxonotmesis

• •

«®rt>

I Neurotmesis 1

I r

Complications

• loss of function (temporarily or permanently)

• neuropathic pain: with neuroma formation

• complex regional pain syndrome: with sympathetic nervous system involvement

Perineurium

Epineurium

/

mmM

Emloneurium SPECIALTY TOPICS

0

•

-

'

Tty Ay

Fascicle

Myelin

Neurotrauma sheath

Trauma Management

• see Emergency Medicine, EU7

Indications for Intubation in Trauma

1 . depressed or decreasing loss of consciousness ( patient cannot protect airway): usually GCS £8

2. need for hyperventilation

3.severe maxillofacial trauma: patency of airway is doubtful

•I. need for pharmacologic paralysis for evaluation or management

• if basal skull fracture suspected, avoid nasotracheal intubation as may inadvertently enter brain

note: intubation prevents patient'

s ability to verbalize for determining GCS

/

Axon -

2

Schwann cell

S1

r,

5

r

I

G

Schwann cell

nucleus

Trauma Assessment

Figure 27. Peripheral nerve structure Initial Management

ABCs of Trauma Management

• see Emergency Medicine, ER2

NEUROLOGICAL ASSESSMENT Glasgow Coma Scale

Eye Verbal

Response Response

Motor

Mini-History

• period of loss of consciousness, post-traumatic amnesia, loss of bowel/bladder control, loss of

sensation, weakness, type of injury/accident

• in urgent situations, remember "SAMPLE-1

'”: signs/symptoms, allergies, medications, past medical

history, last meal, events leading up to the trauma, and baseline functioning

Neurological Exam

• ABCs

• vital signs

- GCS

• brainstem reflexes (if appropriate)

• cranial nerve exam

• motor and sensory exam,including peripheral reflexes

• spine (pain/tenderness, palpable deformity)

• sphincter tone and saddle sensation

• record and repeat neurological exam at regular intervals, as appropriate

Response

4 spontaneous 5 oriented 6 obeys

commands

3 opens eyes 4 contused Slocalizes to

toMice

2 opens eyes 3 inappropriate

to pain wards

Inoeye

opening sounds

pain

4 withdraws

from pan

2 incomprehensible 3 flexion

to pain

(decorticate

postnnng)

1no response 2 extension

to pain

(decerebrate

postering)

Iintubated 1no r-i

response L J

Best response for each component recorded

individually (e

_ g_ E3V3M5)

e13b mild injury:9-T2 is moderate injury;sSis

severe injury

+