5. Cerebral Venous Thrombosis:
⢠Thrombosis of the dural sinus and/or cerebral
veins (CVT).
⢠CVT represents 0.5% to 1% of all strokes.
â Roughly 5 people per million.
⢠More commonly seen in young individuals.
⢠78% of 624 cases in International Study on
Cerebral Venous and Dural Sinuses(ISCVT)
Thrombosis occurred in patients < 50 years of
age.
7. Cause and Pathogenesis
⢠The risk factors for venous thrombosis in
general are linked classically to the Virchow
triad.
â stasis of the blood, changes in the vessel wall, and
changes in the composition of the blood.
⢠Acquired - surgery, trauma, pregnancy,
puerperium, antiphospholipid syndrome,
cancer, exogenous hormones
⢠Genetic causes- inherited thrombophilias.
8. Prothrombotic Conditions:
⢠Antithrombin III, Protein C, and Protein S
Deficiency.
⢠Antiphospholipid and Anticardiolipin
Antibodies.
⢠Factor V Leiden Gene Mutation and Resistance
to Activated Protein C.
⢠Prothrombin G20210A Mutation.
⢠Hyperhomocysteinemia.
9. Pregnancy and Puerperium:
⢠2% of pregnancy-associated strokes are
attributable to CVT.
⢠Approximate frequency - 12 cases per 100 000
deliveries.
⢠During pregnancy (last trimester) and for 6 to
8 weeks after birth, women are at increased
risk of venous thromboembolic events.
⢠Increased prothrombotic factors, infection,
instrumentation, dehydration, cesarian, htn
10. Oral Contraceptives:
⢠22 times more chance of having CVT than
those not using OCPâs.
⢠Presence of other thrombophilias increases
the risk further.
Cancer:
⢠Hematologic malignancies.
⢠Direct tumour compression.
⢠Hypercoagulable state associated with cancer
chemotherapeutic and hormonal agents
11. Para meningeal Infections:
⢠Infections of ear, sinus, mouth, face, and neck.
⢠8.2% of all cases (ISCVT series).
⢠CVT caused by infection is more common in
children.
Other identified causes:
⢠paroxysmal nocturnal hemoglobinuria, iron
deficiency anemia, thrombocythemia, heparin-induced
thrombocytopenia, thrombotic
thrombocytopenic purpura, nephrotic syndrome,
inflammatory bowel disease, systemic lupus
erythematosus, Behçcet disease, mechanical
precipitants, epidural blood patch, spontaneous
intracranial hypotension, lumbar puncture.
12. Clinical Diagnosis of CVT:
⢠Clinical findings fall in to 2 categories.
â Those due to increased ICT
â Those due to focal brain infarction/ hemorrhage.
⢠Headache is the MC symptom â 90%.
â Diffuse and often progresses in severity over days
to weeks.
â minority of patients may present with thunderclap
headache.
â 25% with CVT can present with head and
papilledema alone.
13. ⢠Venous infarction/ hemorrhage:
â Hemiparesis and aphasia MC
â Psychosis and other cortical dysfunction can occur.
⢠Superior sagittal sinus is most commonly
involved.
â Headache, increased intracranial pressure, and
papilledema.
â Motor deficit, seizure.
â Scalp edema and dilated scalp veins.
â Cortical involvement of frontal, parietal, occipital
areas.
14. ⢠Lateral sinus thromboses:
â Features of middle ear infections.
â Increased intracranial pressure and distension of
the scalp veins.
â Hemianopia, contralateral weakness, and aphasia.
â Temporal cortical involvement seen.
⢠16% of patients with CVT have thrombosis of
the deep cerebral venous system.
â thalamic or basal ganglia infarction.
â Decreased mentation, encephalopathy.
15. Features specific to CVT:
⢠Roughly 40% presents with partial/generalized
seizure.
⢠Relative bilateralism of symptoms/ signs/
imaging.
⢠Slowly progressive symptoms.
â In ISCVT: acute (<48 hours) in 37% of
patients,subacute (>48 hours to 30 days) in 56% of
patients, and chronic (>30 days) in 7% of patients.
16. Work Up:
⢠A complete blood count.
⢠Chemistry panel.
⢠Sedimentation rate.
⢠Measures of the prothrombin time and
activated partial thromboplastin time.
⢠Screening for potential prothrombotic
conditions that may predispose a person to
CVT.
17. ⢠Lumbar Puncture:
â Elevated opening pressure in > 80%
â Unless there is clinical suspicion of meningitis,
examination of the cerebrospinal fluid (CSF) is
typically not helpful.
â Elevated cell counts (50%) and protein (35%) can
be seen.
18. D-Dimer:
⢠A product of fibrin degradation.
⢠Diagnostic role in exclusion of DVT.
⢠Sensitivity of 97.1%, a specificity of 91.2%, a negative
predictive value of 99.6%.
⢠A normal D-dimer level according to a sensitive
immunoassay or rapid enzyme-linked immunosorbent
assay (ELISA) may be considered to help identify
patients with low probability of CVT (Class IIb; Level
of Evidence B). If there is a strong clinical suspicion of
CVT, a normal D-dimer level should not preclude
further evaluation.
19. Common Pitfalls in the Diagnosis of
CVT:
⢠Intracranial Hemorrhage:
â 30% to 40% of patients with CVT present with ICH.
â Prodromal headache, bilateral parenchymal
abnormalities, and clinical evidence of a
hypercoagulable state.
â In patients with lobar ICH of otherwise unclear
origin or with cerebral infarction that crosses
typical arterial boundaries, imaging of the
cerebral venous system should be performed
(Class I; Level of Evidence C).
20. ⢠Isolated Headache/Idiopathic Intracranial
Hypertension:
â Headache alone or headache and papilledema and/or
6th nerve palsy (25%).
â A new, atypical headache; headache that progresses
steadily over days to weeks despite conservative
treatment; and thunderclap headache can help
identify CVT.
â In patients with the clinical features of idiopathic
intracranial hypertension, imaging of the cerebral
venous system is recommended to exclude CVT (Class
I; Level of Evidence C).
â In patients with headache associated with atypical
features, imaging of the cerebral venous system is
reasonable to exclude CVT (Class IIa; Level of
Evidence C).
21. Imaging in the Diagnosis of CVT:
⢠Non Invasive Imaging:
â CT, MRI, Ultrasonography.
⢠Invasive Imaging:
â Cerebral Angiography and Direct Cerebral
Venography.
22. CT:
⢠Plain CT being abnormal only in <30% of CVT
cases.
⢠Hyperdensity of a cortical vein or dural sinus
seen.
⢠Acutely thromboses : Hyperdensity.
⢠Thrombosis of the posterior portion of the
superior sagittal sinus may appear as a dense
triangle â Dense delta sign.
⢠Ischemic infarction/hemorrhage may be seen.
â Not obeying any vascular territory.
23.
24. ⢠Contrast-enhanced CT:
â filling defect within the vein or sinus.
â may show the classic âempty deltaâ sign, in which
a central hypointensity due to very slow or absent
flow within the sinus is surrounded by contrast
enhancement in the surrounding triangular shape
in the posterior aspect of the superior sagittal
sinus.
⢠CT Venogram.
25. Magnetic Resonance Imaging:
⢠MRI signal intensity vary according to duration of
the thrombus.
â 1st week : isointense to brain tissue on T1-weighted
images and hypointense on T2- weighted images.
â 2nd week - hyperintensity on T1- and T2-weighted
images.
⢠A thrombosed dural sinus or vein may then
demonstrate low signal on gradient-echo and
susceptibility-weighted images of magnetic
resonance images.
26. ⢠Routine TOF MRV : absence of a flow void
with alteration of signal intensity in the dural
sinus indicate CVT.
⢠Contrast MRI â if TOF sequence inconclusive.
⢠Secondary changes: cerebral swelling, edema,
and/or hemorrhage.
⢠Focal edema without hemorrhage is visualized
on CT in about 8% of cases and on MRI in 25%.
⢠Focal parenchymal changes with edema and
hemorrhage may be identified in up to 40% of
patients.
27.
28. ⢠Types of parenchymal hemorrhage in CVT:
â Brain parenchymal changes in frontal, parietal,
and occipital lobes usually correspond to superior
sagittal sinus thrombosis.
â Temporal lobe parenchymal changes correspond
to lateral (transverse) and sigmoid sinus
thrombosis.
â Thalamic hemorrhage, edema, or intraventricular
hemorrhage, correspond to thrombosis of the
vein of Galen or straight sinus.
29.
30.
31.
32. CT Venogram:
⢠More useful in sub acute
or chronic situations.
⢠Bone artefact may
interfere.
⢠CTV is at least equivalent
to MRV.
⢠Risk of radiation
exposure and iodine
contrast allergy.
33. Invasive Diagnostic Angiographic
Procedures:
⢠Cerebral Angiography and Direct Cerebral
Venography:
â Reserved for situations in which the MRV or CTV
results are inconclusive.
â If an endovascular procedure is being considered.
⢠Delayed phase of angiography shows sinus.
â CVT seen as filling defects or delay in visualization
of sinus.
â Normally 7 to 8 second after arterial phase.
34. ⢠Direct Cerebral Venography Direct cerebral
venography is performed by direct injection of
contrast material into a dural sinus.
⢠Usually performed during endovascular
therapeutic procedures.
⢠Direct cerebral venography can identify
venous hypertension.
⢠Normal venous sinus pressure is 10 mm H2O.
⢠USS â more useful in neonates.
35.
36. Potential Pitfalls in the Radiological
Diagnosis of
CVT:
⢠Anatomic variants of normal venous anatomy
may mimic sinus thrombosis.
â Sinus atresia/hypoplasia, asymmetrical sinus
drainage, and normal sinus filling defects related
to prominent arachnoid granulations or intrasinus
septa.
⢠Studies show high prevalence of asymmetrical
lateral (transverse) sinuses (49%) and partial
or complete absence of 1 lateral sinus (20%).
37. ⢠Hypoplastic dural sinus may have a more
tapering appearance than an abrupt defect in
contrast-enhanced images of the sinus.
38.
39. Imaging Recommendations:
⢠1. Although a plain CT or MRI is useful in the initial evaluation of patients with
suspected CVT, a negative plain CT or MRI does not rule out CVT. A venographic
study (either CTV or MRV) should be performed in suspected CVT if the plain CT or
MRI is negative or to define the extent of CVT if the plain CT or MRI suggests CVT
(Class I; Level of Evidence C).
⢠2. An early follow-up CTV or MRV is recommended in CVT patients with persistent
or evolving symptoms despite medical treatment or with symptoms suggestive of
propagation of thrombus (Class I; Level of Evidence C).
⢠3. In patients with previous CVT who present with recurrent symptoms suggestive
of CVT, repeat CTV or MRV is recommended (Class I; Level of Evidence C).
⢠4. Gradient echo T2 susceptibility-weighted images combined with magnetic
resonance can be useful to improve the accuracy of CVT diagnosis (Class IIa; Level of
Evidence B).
⢠5. Catheter cerebral angiography can be useful in patients with inconclusive CTV or
MRV in whom a clinical suspicion for CVT remains high (Class IIa; Level of Evidence
C).
⢠6. A follow-up CTV or MRV at 3 to 6 months after diagnosis is reasonable to assess
for recanalization of the occluded cortical vein/sinuses in stable patients (Class IIa;
Level of Evidence C).
40. Management and Treatment:
⢠Organized care is one of the most effective
interventions to reduce mortality and
morbidity after acute stroke.
⢠Management of CVT in a stroke unit is
reasonable for the initial management of CVT
to optimize care and minimize complications.
41. Initial Anticoagulation:
⢠Acute anticoagulation: Heparin is indicated.
⢠Presence of pre treatment ICH is not a
contraindication.
⢠No definite recommendation regarding
dosage.
⢠LMW heparin is preferred over UFH.
⢠Anticoagulation appears safe and effective.
42. Other Treatments:
⢠Fibrinolytic Therapy:
â 9% to 13% have poor outcomes despite
anticoagulation.
â Anticoagulation alone may not dissolve a large
and extensive thrombus.
â Partial or complete recanalization rates for CVT
ranged from 47% to 100% with anticoagulation
alone.
43. ⢠Thrombolytic therapy is used if clinical
deterioration continues despite
anticoagulation or if a patient has elevated
intracranial pressure that evolves despite
other management approaches.
⢠Direct Catheter Thrombolysis.
⢠Mechanical Thrombectomy/Thrombolysis
â Balloon-Assisted Thrombectomy and
Thrombolysis.
â Catheter Thrombectomy.
⢠Surgical thrombectomy is rarely done.
44. ⢠Aspirin has no role in the management of CVT.
⢠Steroids are contraindicated.
â Associated with high mortality and morbidity.
⢠Antibiotics â indicated if there is associated
infections.
45. Management and Prevention of Early
Complications:
⢠Seizures:
â Seizures are present in 37% of adults, 48% of
children, and 71% of newborns who present with
CVT.
â Seizures increase anoxic damage.
â Anticonvulsant treatment after even a single
seizure is reasonable.
â Prophylactic use of antiepileptic drugs may be
harmful.
46. ⢠Early seizures indicate brain parenchymal
involvement.
â Supra tentorial lesions.
⢠Hydrocephalus
â Arachnoid granulation function may be impaired
and result in communicating hydrocephalus
(6.6%).
â obstructive hydrocephalus is less common â due
to ventricular hemorrhage.
â Raised ICT should be managed urgently as venous
pressure is already high.
47. ⢠Intracranial Hypertension:
â 40% of patients with CVT present with isolated
intracranial hypertension.
â progressive headache, papilledema, and third or sixth
nerve palsies.
â Primarily caused by venous outflow obstruction and
tissue congestion compounded by CSF malabsorption.
â Acute setting: decompressive craniotomy.
â Proper anticoagulation
â Reasonable to initiate treatment with acetazolamide.
â Repeated LP or in C/c cases LP shunt.
â Steroids contraindicated.
â Evaluation of vision.
48. Long-Term Management and
Recurrence of CVT:
⢠The overall risk of recurrence of any thrombotic
event (CVT or systemic) after a CVT is around
6.5%.
⢠The risk of other manifestations of VTE after CVT
ranges from 3.4% to 4.3%.
⢠Male sex and polycythemia/thrombocythemia
being the only independent predictors in ISCVT
study.
⢠Systemic VTE after CVT is more common than
recurrent CVT.
49. ⢠Thrombophilias have been stratified as mild or
severe on the basis of the risk of recurrence.
â Deficiencies of antithrombin, protein C, and
protein S, with a 19% recurrence at 2 years, 40%
at 5 years, and 55% at 10 years.
â Homozygous prothrombin G20210A; homozygous
factor V Leiden; deficiencies of protein C, protein
S, or antithrombin; combined thrombophilia
defects; and antiphospholipid syndrome are
categorized as severe.
⢠Testing to be done 2 to 4 weeks after
completion of anticoagulation.
50. Recommendations:
⢠In patients with provoked CVT (associated with a transient risk factor),
vitamin K antagonists may be continued for 3 to 6 months, with a
target INR of 2.0 to 3.0 (Table 3) (Class IIb; Level of Evidence C).
⢠In patients with unprovoked CVT, vitamin K antagonists may be
continued for 6 to 12 months, with a target INR of 2.0 to 3.0 (Class IIb;
Level of Evidence C).
⢠For patients with recurrent CVT, VTE after CVT, or first CVT with severe
thrombophilia (ie, homozygous prothrombin G20210A; homozygous
factor V Leiden; deficiencies of protein C, protein S, or antithrombin;
combined thrombophilia defects; or antiphospholipid syndrome),
indefinite anticoagulation may be considered, with a target INR of 2.0
to 3.0 (Class IIb; Level of Evidence C).
⢠Consultation with a physician with expertise in thrombosis may be
considered to assist in the prothrombotic testing and care of patients
with CVT (Class IIb; Level of Evidence C).
51. Management of Late Complications:
⢠Headache:
â 50%
â In Lille study 29% fulfilled criteria for migraine,
and 27% had headache of the tension type.
â In patients with persistent or severe headaches,
appropriate investigations should be completed to
rule out recurrent CVT.
â Lumbar puncture may be needed to exclude
elevated intracranial pressure.
52. ⢠Seizures:
â Remote seizures affect 5% to 32% of patients.
â Most occur in the 1st yr of follow up.
â Risk factors for remote seizures- hemorrhagic
lesion on admission in MRI/CT, early seizure,
paresis.
⢠Visual Loss:
â More common in Pt with papilledema.
â Severe visual loss due to CVT rarely occurs (2 to
4%).
â Visual acuity and formal visual field testing should
be done.
53. ⢠Dural Arteriovenous Fistula:
â Dural fistulas can be a late complication of
persistent dural sinus occlusion with increased
venous pressure.
â The fistula can close and cure if the sinus
recanalizes.
â A preexisting fistula can be the underlying cause
of CVT.
â A cerebral angiogram may help identify the
presence of a dural arteriovenous fistula.
54. CVT in Special Populations:
⢠CVT During Pregnancy:
â Incidence 1 in 2500 deliveries to 1 in 10 000
deliveries.
â Greatest risk - third trimester and the first 4
postpartum weeks.
â Up to 73% of CVT in women occurs during the
puerperium.
â Cesarean delivery appears to be associated with a
higher risk of CVT.
55. ⢠Vitamin K antagonists are associated with fetal
embryopathy and HDN in neonates.
⢠UHF also causes teratogenicity and HDN.
⢠LMW Heparin is the drug of choice.
⢠No contra indication for future pregnancies.
⢠LMW Heparin during future pregnancies and
post partum period can be beneficial.
56. Recommendations:
⢠For women with CVT during pregnancy, LMWH in full
anticoagulant doses should be continued throughout
pregnancy, and LMWH or vitamin K antagonist with a target
INR of 2.0 to 3.0 should be continued for at least 6 weeks
postpartum (for a total minimum duration of therapy of 6
months) (Class I;Level of Evidence C).
⢠It is reasonable to advise women with a history of CVT that
future pregnancy is not contraindicated. Further investigations
regarding the underlying cause and a formal consultation with
a hematologist and/or maternal fetal medicine specialist are
reasonable.(Class IIa; Level of Evidence B).
⢠It is reasonable to treat acute CVT during pregnancy with full-dose
LMWH rather than UFH (Class IIa; Level of Evidence C).
⢠For women with a history of CVT, prophylaxis with LMWH
during future pregnancies and the postpartum period is
probably recommended (Class IIa; Level of Evidence C).
57. CVT in the Pediatric Population:
⢠Incidence - 0.67 per 100 000 children per year.
⢠Neonates present with seizures or lethargy.
⢠Older infants and children
â Present with seizures, altered levels of
consciousness, increasing headache with
papilledema, isolated intracranial hypertension, or
focal neurological deficits.
58. ⢠Risk factors:
â Mechanical forces are exerted on the infantâs head
during birth.
â Increased thrombotic tendency of infants.
â Older children: systemic lupus erythematosus,
nephrotic syndrome, leukemia or lymphoma with
LL-asparaginase treatment, and trauma.
⢠Supportive measures for children with CVT
should include appropriate hydration, control
of epileptic Sz, and treatment of elevated
intracranial pressure.
59. ⢠Periodic assesment of vision should be done.
⢠In children with acute CVT diagnosed beyond the
first 28 days of life, it is reasonable to treat with
full-dose LMWH even in the presence of
intracranial hemorrhage (Class IIa; Level of
Evidence C).
⢠In children with acute CVT diagnosed beyond the
first 28 days of life, it is reasonable to continue
LMWH or oral vitamin K antagonists for 3 to 6
months (Class IIa; Level of Evidence C).
60. ⢠In neonates with acute CVT, treatment with
LMWH or UFH may be considered (Class IIb;
Level of Evidence B).
⢠Continuous electroencephalography
monitoring may be considered for individuals
who are unconscious or mechanically
ventilated.
⢠In neonates with acute CVT, continuation of
LMWH for 6 weeks to 3 months may be
considered (Class IIb; Level of Evidence C).