Posterior reversible encephalopathy syndrome: Difference between revisions

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(Major expansion: MRI FLAIR/DWI interpretation, atypical patterns, causes (eclampsia/immunosuppressants), BP targets, prognostic factors, DWI restricted diffusion significance, references with PMIDs)
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==Background==
==Background==
*PRES, a rare syndrome characterized by acute neurological symptoms due to vasogenic edema in the posterior brain  
*Clinical-radiographic syndrome characterized by '''headache, seizures, visual disturbances, and altered mental status''' with '''vasogenic edema''' predominantly in posterior brain regions
**Somewhat of a misnomer as changes seen on MRI are not limited to the posterior fossa and symptoms are not always reversible
*Previously known as reversible posterior leukoencephalopathy syndrome (RPLS)
**Renamed reversible posterior leukoencephalopathy syndrome (RPLS) by the American Academy of Neurology
*'''Usually reversible''' with prompt treatment of underlying cause, but '''can be irreversible''' if untreated (cytotoxic edema, hemorrhage)
*Risk factors: [[malignant hypertension]], kidney disease, autoimmune disease, immunosuppression, [[eclampsia]]
*Pathophysiology (two proposed mechanisms):
*Poorly understood entity, but thought to be due to 2 theoretical mechanisms:<ref>Zelaya JE, Al-Khoury L. Posterior Reversible Encephalopathy Syndrome. [Updated 2022 May 1]. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2024 Jan-.</ref>
**'''Hypertensive theory''': severe hypertension exceeds cerebral autoregulation → hyperperfusion vasogenic edema (posterior brain more vulnerable due to less sympathetic innervation)
**Hypertension-hyperperfusion: Hypertensive emergency causes vascular extravasation of fluid and vasogenic edema
**'''Endothelial dysfunction theory''': direct endothelial injury from toxins, medications, or autoimmune activation → blood-brain barrier disruption → vasogenic edema
**Endothelial dysfunction: Autoimmune or cytotoxic etiologies lead to endothelial dysfunction, leading to increased  vascular permeability and edema
*Epidemiolgy: Most frequently in middle-aged females, which may be related to underlying disease<ref>Fischer M, Schmutzhard E. Posterior reversible encephalopathy syndrome. J Neurol. 2017 Aug;264(8):1608-1616. doi: 10.1007/s00415-016-8377-8. Epub 2017 Jan 4. PMID: 28054130; PMCID: PMC5533845.</ref>
*Prognosis: While many case reports suggest PRES is benign and fully reversible, the consequences of PRES, including intracerebral hemorrhage or extensive intracerebral edema, can result in residual neurologic deficits


[[File:Posterior reversible encephalopathy syndrome MRI.jpg|thumb|Magnetic resonance image showing multiple cortico-subcortical areas of hyperdense signal involving the occipital and parietal lobes bilaterally and pons in a patient with posterior reversible encephalopathy syndrome]]
===Common Causes===
*'''Hypertensive emergency''' (most common; including [[eclampsia]]/[[preeclampsia]])
*'''Immunosuppressive/cytotoxic medications''': cyclosporine, tacrolimus, cisplatin, bevacizumab, methotrexate
*'''Autoimmune conditions''': [[SLE]], [[thrombotic thrombocytopenic purpura]], [[hemolytic uremic syndrome]]
*'''Renal failure''' (especially with fluid overload)
*[[Eclampsia]]/[[preeclampsia]] ('''most common cause in young women''')
*[[Sepsis]], [[shock]], organ transplantation


==Clinical Features<ref>Staykov D. "Posterior reversible encephalopathy syndrome". PMID 21257628</ref>==
==Clinical Features==
*Onset may range from hours to days
*'''Headache''' (most common presenting symptom)
*[[Seizures]], including [[status epilepticus]]
*'''Seizures''' (60-75% of cases; may be the presenting feature)
*[[Encephalopathy]], ranging from mild [[altered mental status]] to [[coma]]
*'''Visual disturbances''': blurred vision, cortical blindness, visual neglect, homonymous hemianopia
*[[Acute Vision Loss (Noninflamed)|Visual disturbances]]
*'''Altered mental status''': confusion, obtundation, decreased alertness
*[[Hypertension]]
*'''Focal neurologic deficits''' (less common but can occur)
**Note that some proportion of patients may not exhibit significant hypertension; of note, a significant proportion of patients also had no known pre-existing hypertension<ref>Fugate JE, Claassen DO, Cloft HJ, Kallmes DF, Kozak OS, Rabinstein AA. Posterior reversible encephalopathy syndrome: associated clinical and radiologic findings. Mayo Clin Proc. 2010 May;85(5):427-32. doi: 10.4065/mcp.2009.0590. PMID: 20435835; PMCID: PMC2861971.</ref>
*'''Hypertension''' (present in 70-80% but '''PRES can occur with normal BP''' in 20-30% of cases)
*[[Headache]], [[vomiting]], or other focal neurological deficits
*Nausea, vomiting


==Differential Diagnosis<ref name="Garg">Garg RK (January 2001). "Posterior leukoencephalopathy syndrome". Postgrad Med J 77 (903): 24–8. doi:10.1136/pmj.77.903.24. PMC 1741870. PMID 11123390</ref>==
==Differential Diagnosis==
*[[Eclampsia]]
*[[Ischemic stroke]] (especially posterior circulation)
*Vascular
*[[Cerebral venous sinus thrombosis]]
**[[Hypertensive Emergency|Hypertensive Encephalopathy]]
*[[Encephalitis]]
**[[CVA]]
*CNS vasculitis
**[[Intracranial Hemorrhage]]
*Toxic leukoencephalopathy
**[[Cerebral Venous Thrombosis]]
*Demyelinating disease (ADEM)
*Infectious
*[[Subarachnoid hemorrhage]]
**[[Encephalitis]]
*[[Status epilepticus]]
**[[Meningitis]]
*'''CNS metastatic disease'''
*Metabolic
 
**[[Hepatic Encephalopathy]]
==Evaluation==
**[[Hyponatremia]]
===MRI (Diagnostic Study of Choice)===
**[[Porphyria]]
*'''MRI with FLAIR and DWI''' is the gold standard
*Demyelinating Disorders (e.g. [[MS]])
*'''Classic pattern''': bilateral, symmetric '''vasogenic edema''' in '''parieto-occipital''' white matter
**[[Systemic Lupus Erythematosus|SLE]]
*'''FLAIR/T2''': hyperintense signal in affected regions
*Psychiatric disorder
*'''DWI/ADC''': '''elevated ADC''' (vasogenic edema) vs restricted diffusion (cytotoxic edema → '''worse prognosis''')
*Atypical patterns (30-40%): frontal lobe, temporal lobe, cerebellum, brainstem, unilateral, hemorrhagic
*'''Hemorrhage occurs in 5-15%''' of cases (petechial or frank hemorrhage)


{{Seizure DDX}}
===CT Head===
*May show hypodensity in posterior regions but '''sensitivity is low'''
*Useful to '''rule out hemorrhage''' or '''ischemic stroke''' initially
*If MRI unavailable, CT findings may be suggestive but are often subtle


==Evaluation==
===Labs===
*[[CT head]] to rule out other etiologies
*BMP (renal function, electrolytes)
*[[brain MRI|MRI]] often shows symmetrical cerebral edema, showing as hyperintensities on T2-weighted image in the posterior circulation, most commonly in the parietal-occipital areas<ref name="Garg"/>
*CBC with smear (evaluate for TMA — schistocytes if TTP/HUS)
**However, any brain region can be involved, including the frontal and temporal lobes
*LFTs, LDH, haptoglobin (hemolysis workup)
*Focus on [[Altered Mental Status#Work-Up|altered mental status workup]], with PRES as diagnosis of exclusion
*Urinalysis (proteinuria if eclampsia)
*Consider [[lumbar puncture]] if there is a concern for [[meningitis]] or [[encephalitis]]
*Magnesium level
*May require EEG for detection of status epilepticus
*Drug levels (cyclosporine, tacrolimus)
*Pregnancy test in reproductive-age women


==Management==
==Management==
*Treat the underlying etiology
===Blood Pressure Control (If Hypertensive)===
*[[Hypertensive Emergency#Treatment|Control Blood Pressure]], considering gradual reduction to avoid sudden hypoperfusion
*'''Gradual reduction''' — target '''25% reduction in MAP in first few hours'''
*Discontinue immunosuppressants or cytotoxic medications
*'''Avoid precipitous drops''' (risk of posterior circulation ischemia)
*Standard seizure management, if seizures are present
*Preferred agents:
*In cases related to [[Preeclampsia]] or [[HELLP syndrome]], consider early OB/GYN consultation for delivery<ref>Parasher A, Jhamb R. Posterior reversible encephalopathy syndrome (PRES): presentation, diagnosis and treatment. Postgrad Med J. 2020 Oct;96(1140):623-628. doi: 10.1136/postgradmedj-2020-137706. Epub 2020 May 28. PMID: 32467104.</ref>
**'''Nicardipine infusion''' 5-15 mg/hr (easily titratable)
**'''Labetalol''' 10-20 mg IV q10-20min
*If '''eclampsia''': '''magnesium sulfate''' is first-line for seizure prevention (see [[eclampsia]])
 
===Seizure Management===
*'''Benzodiazepines''' for acute seizures (lorazepam 2-4 mg IV)
*AEDs for ongoing seizure prophylaxis (levetiracetam preferred)
*If eclampsia: '''magnesium sulfate''' (primary treatment)
*Most seizures resolve with BP control and treatment of underlying cause
 
===Treat Underlying Cause===
*'''Discontinue or reduce offending medication''' (cyclosporine, tacrolimus, chemotherapy)
*'''Delivery''' for eclampsia/preeclampsia with severe features
*Treat [[sepsis]], [[renal failure]], autoimmune flare as indicated
*Dialysis for uremic patients
 
===Monitoring===
*ICU admission for most patients
*Continuous BP monitoring (arterial line preferred)
*Serial neurologic exams
*'''Repeat MRI''' at 1-2 weeks to confirm resolution of edema
 
==Prognosis==
*'''Majority of cases are fully reversible''' within days to weeks with appropriate treatment
*'''Risk factors for poor outcome''':
**Restricted diffusion on DWI (cytotoxic edema → infarction)
**Hemorrhage
**Delayed diagnosis and treatment
**'''Untreated PRES can progress to permanent brain injury'''


==Disposition==
==Disposition==
*Admit
*'''Admit to ICU''' for BP monitoring, seizure management, and neurologic observation
**Consider ICU for blood pressure titration, obtunded state, status epilepticus, intracranial hemorrhage, or other serious sequelae
*Neurology consultation
*Nephrology if drug-related (immunosuppressant dose adjustment)
*OB consultation if eclampsia/preeclampsia


==See Also==
==See Also==
*[[Eclampsia]]
*[[Preeclampsia]]
*[[Hypertensive emergency]]
*[[Hypertensive emergency]]
*[[Eclampsia]]
*[[Status epilepticus]]
*[[Ischemic stroke]]
*[[Cerebral venous sinus thrombosis]]


==References==
==References==
<references/>
*Fugate JE, Rabinstein AA. Posterior reversible encephalopathy syndrome: clinical and radiological manifestations, pathophysiology, and outstanding questions. ''Lancet Neurol''. 2015;14(9):914-925. PMID 26184985
*Bartynski WS. Posterior reversible encephalopathy syndrome, part 2: controversies surrounding pathophysiology of vasogenic edema. ''AJNR Am J Neuroradiol''. 2008;29(6):1043-1049. PMID 18403560
*Hinchey J, et al. A reversible posterior leukoencephalopathy syndrome. ''N Engl J Med''. 1996;334(8):494-500. PMID 8559202
*Liman TG, et al. Clinical and radiological differences in posterior reversible encephalopathy syndrome between patients with preeclampsia-eclampsia and other predisposing diseases. ''Eur J Neurol''. 2012;19(7):935-943. PMID 22248339


[[Category:Neurology]]
[[Category:Neurology]]
[[Category:Critical Care]]

Revision as of 20:01, 21 March 2026

Background

  • Clinical-radiographic syndrome characterized by headache, seizures, visual disturbances, and altered mental status with vasogenic edema predominantly in posterior brain regions
  • Previously known as reversible posterior leukoencephalopathy syndrome (RPLS)
  • Usually reversible with prompt treatment of underlying cause, but can be irreversible if untreated (cytotoxic edema, hemorrhage)
  • Pathophysiology (two proposed mechanisms):
    • Hypertensive theory: severe hypertension exceeds cerebral autoregulation → hyperperfusion → vasogenic edema (posterior brain more vulnerable due to less sympathetic innervation)
    • Endothelial dysfunction theory: direct endothelial injury from toxins, medications, or autoimmune activation → blood-brain barrier disruption → vasogenic edema

Common Causes

Clinical Features

  • Headache (most common presenting symptom)
  • Seizures (60-75% of cases; may be the presenting feature)
  • Visual disturbances: blurred vision, cortical blindness, visual neglect, homonymous hemianopia
  • Altered mental status: confusion, obtundation, decreased alertness
  • Focal neurologic deficits (less common but can occur)
  • Hypertension (present in 70-80% but PRES can occur with normal BP in 20-30% of cases)
  • Nausea, vomiting

Differential Diagnosis

Evaluation

MRI (Diagnostic Study of Choice)

  • MRI with FLAIR and DWI is the gold standard
  • Classic pattern: bilateral, symmetric vasogenic edema in parieto-occipital white matter
  • FLAIR/T2: hyperintense signal in affected regions
  • DWI/ADC: elevated ADC (vasogenic edema) vs restricted diffusion (cytotoxic edema → worse prognosis)
  • Atypical patterns (30-40%): frontal lobe, temporal lobe, cerebellum, brainstem, unilateral, hemorrhagic
  • Hemorrhage occurs in 5-15% of cases (petechial or frank hemorrhage)

CT Head

  • May show hypodensity in posterior regions but sensitivity is low
  • Useful to rule out hemorrhage or ischemic stroke initially
  • If MRI unavailable, CT findings may be suggestive but are often subtle

Labs

  • BMP (renal function, electrolytes)
  • CBC with smear (evaluate for TMA — schistocytes if TTP/HUS)
  • LFTs, LDH, haptoglobin (hemolysis workup)
  • Urinalysis (proteinuria if eclampsia)
  • Magnesium level
  • Drug levels (cyclosporine, tacrolimus)
  • Pregnancy test in reproductive-age women

Management

Blood Pressure Control (If Hypertensive)

  • Gradual reduction — target 25% reduction in MAP in first few hours
  • Avoid precipitous drops (risk of posterior circulation ischemia)
  • Preferred agents:
    • Nicardipine infusion 5-15 mg/hr (easily titratable)
    • Labetalol 10-20 mg IV q10-20min
  • If eclampsia: magnesium sulfate is first-line for seizure prevention (see eclampsia)

Seizure Management

  • Benzodiazepines for acute seizures (lorazepam 2-4 mg IV)
  • AEDs for ongoing seizure prophylaxis (levetiracetam preferred)
  • If eclampsia: magnesium sulfate (primary treatment)
  • Most seizures resolve with BP control and treatment of underlying cause

Treat Underlying Cause

  • Discontinue or reduce offending medication (cyclosporine, tacrolimus, chemotherapy)
  • Delivery for eclampsia/preeclampsia with severe features
  • Treat sepsis, renal failure, autoimmune flare as indicated
  • Dialysis for uremic patients

Monitoring

  • ICU admission for most patients
  • Continuous BP monitoring (arterial line preferred)
  • Serial neurologic exams
  • Repeat MRI at 1-2 weeks to confirm resolution of edema

Prognosis

  • Majority of cases are fully reversible within days to weeks with appropriate treatment
  • Risk factors for poor outcome:
    • Restricted diffusion on DWI (cytotoxic edema → infarction)
    • Hemorrhage
    • Delayed diagnosis and treatment
    • Untreated PRES can progress to permanent brain injury

Disposition

  • Admit to ICU for BP monitoring, seizure management, and neurologic observation
  • Neurology consultation
  • Nephrology if drug-related (immunosuppressant dose adjustment)
  • OB consultation if eclampsia/preeclampsia

See Also

References

  • Fugate JE, Rabinstein AA. Posterior reversible encephalopathy syndrome: clinical and radiological manifestations, pathophysiology, and outstanding questions. Lancet Neurol. 2015;14(9):914-925. PMID 26184985
  • Bartynski WS. Posterior reversible encephalopathy syndrome, part 2: controversies surrounding pathophysiology of vasogenic edema. AJNR Am J Neuroradiol. 2008;29(6):1043-1049. PMID 18403560
  • Hinchey J, et al. A reversible posterior leukoencephalopathy syndrome. N Engl J Med. 1996;334(8):494-500. PMID 8559202
  • Liman TG, et al. Clinical and radiological differences in posterior reversible encephalopathy syndrome between patients with preeclampsia-eclampsia and other predisposing diseases. Eur J Neurol. 2012;19(7):935-943. PMID 22248339
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