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{{Acute disseminated encephalomyelitis }}
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==Overview==   
==Overview==   
Acute disseminated encephalomyelitis (ADEM) is an acute neurologic disease of the central nervous system characterized by scattered foci of demyelination and perivenular inflammation.  The disease may occur without precipitant, or may develop after infection or vaccination.
[[Acute disseminated encephalomyelitis]] ([[ADEM]]) is an [[acute]] [[neurologic]] [[disease]] of the [[central nervous system]] characterized by scattered [[foci]] of [[demyelination]] and [[perivascular]] [[inflammation]].  The [[disease]] may occur without[[precipitant]], or may develop after [[infection]] or [[vaccination]].


==Historical Perspective==
==Historical Perspective==
[[Encephalomyelitis]] was primarily an experimental finding discovered after injection of rabbits with rabbit [[spinal]] [[cord]] infused with solutions of sodium chloride and [[lecithinase]], adjuvants, like [[bayol F],] and killed [[tubercle]] bacilli, and human spinal cord treated with [[formaldehyde]] solution. Clinical signs were [[spasticity]], [[ataxia]], [[weakness]] and even death. The [[perivascular]] [[inflammatory]] [[lesions]] had a predilection for the [[white]] [[matter]] and [[demyelination]] was seen in all ages. Older [[lesions]] had [[glial]] [[scars]].


==Classification==
==Classification==
[[Acute]] [[disseminated]] [[encephalomyelitis]] can occur after an episode of [[infection]] (post-[[infectious]]), [[vaccination]] or even, spontaneously without an obvious trigger ([[idiopathic]]).


==Pathophysiology==
==Pathophysiology==
The exact mechanism of [[acute]] [[disseminated]] [[encephalomyelitis]] is not determined. However, it is usually preceded by an environmental trigger, e.g. an [[infection]] or [[vaccination]] and affects individuals with a [[genetic]] predisposition.


==Causes==
==Causes==
In the past, [[ADEM]] was a sequelae of common childhood [[infections]] like [[measles]], [[smallpox]] and [[chickenpox]]. With the improvements in [[infectious]] [[disease]] management practices, [[ADEM]] in developed countries frequently follow non-specific upper [[respiratory]] tract [[infections]]. Failure to identify a definite cause could suggest that the inciting agents are unusual and not recovered by standard laboratory tests. [[ADEM]] is much more common in the developing countries where [[measles]] and other [[viral]] [[infections]] still account for a major proportion of cases.
Another common variant is the [[postimmunisation]] [[encephalomyelitis]], which has a preference for the peripheral [[nervous]] system. Currently, the most common implicated [[vaccines]] are [[measles]], [[mumps]] and [[rubella]]. The risk of the condition developing after [[measles]] [[vaccination]] is considerably lower than the [[natural]] [[infection]].


==Differentiating Acute disseminated encephalomyelitis from Other Diseases==
==Differentiating Acute disseminated encephalomyelitis from Other Diseases==
No one test established the diagnosis of ADEM. Supporting features include an appropriate viral or vaccination history, an appropriate acute neurologic illness, and consistent features on CNS imaging.
The [[differential]] diagnoses of [[Acute disseminated encephalomyelitis]] include:
* [[Viral]] [[encephalitis]]
* [[HIV]] [[encephalopathy]]
* [[Multiple sclerosis]]
* [[Antiphospholipid antibody syndrome]]


==Epidemiology and Demographics==
==Epidemiology and Demographics==
The average annual [[incidence]] of [[ADEM]] is between 0.07 and 0.6 per 1,00,000 individuals per year. It is more common during childhood, with a median age on onset between 5-8 years and a male predominance (1.8:1).


==Risk Factors==
==Risk Factors==
The [[risk]] factors for [[ADEM]] include:
*[[Infections]] (most common)
*[[Vaccinations]]
*[[Genetic]] predisposition


==Screening==
==Screening==
There is no [[screening]] tool currently used for [[Acute disseminated encephalomyelitis]].


==Natural History, Complications, and Prognosis==
==Natural History, Complications, and Prognosis==
The classic form, accounting for 70-90% of cases, typically follows a [[monophasic]] pattern. Residual severe [[disability]] is quite rare in [[pediatric]] [[ADEM]] cases (7%). Adult patients frequently suffer from residual [[ataxia]], [[clumsiness]], [[hemiparesis]] or [[epilepsy]]. The poor [[prognosis]] and long-term outcomes of [[ADEM]] have changed dramatically owing to efficient [[vaccination]] coverage and widespread, early use of high-dose [[steroids]].


==Diagnosis==
==Diagnosis==
===Diagnostic Study of Choice===
===Diagnostic Study of Choice===
[[MRI]] is the best method for further evaluation after an initial suspicion of [[ADEM]]. [[MRI]] brain with [[gadolinium]] [[enhancement]] is indicated in stable [[patients]] whereas, [[MRI]] of the [[dorsal]] and [[cervical]] [[spinal cord]] can determine the [[extent]] of [[inflammation]] in [[symptoms]] and [[signs]] suggestive of [[myelopathy]].


===History and Symptoms===
===History and Symptoms===
Classic [[ADEM]] is [[monophasic]], with a history of usually a preceding [[illness]] or less commonly, a [[vaccination]]. It is characterised by an [[acute]] onset of [[focal]] [[neurologic]] [[symptoms]], often with rapid deterioration of [[consciouness]], after a variable [[latent]] period of several days to few months.


===Physical Examination===
===Physical Examination===
Physical [[examination]] of [[ADEM]] may reveal positive findings in different parts of the [[nervous system]] namely, the [[cerebral]] [[cortex]], [[brainstem]], [[cranial nerves]] and the [[sensory]] and [[motor]] [[tracts]]. [[Respiratory failure]] may prove fatal in some cases.


===Laboratory Findings===
===Laboratory Findings===
[[Antibodies]] like [[anti-MOG]] [[antibodies]] are found in the serum of [[patients]] suffering from [[ADEM]]. A [[lumbar]] [[puncture]] is also useful for evaluation of the changes in the [[Cerebrospinal fluid]] ([[CSF]]).


===Imaging Findings===
===Imaging Findings===
The appearance of [[ADEM]] on [[cranial]] [[CT]] has rarely been reported. There is a delay between the onset of the [[clinical signs]] and the appearance of [[lesions]] on [[CT scan]]. The correlation was limited between the [[clinical]] course and the [[anatomical]] distribution and type of abnormality seen on [[CT scan]].
[[MRI]] is the best method for further evaluation after an initial suspicion of [[ADEM]]. [[MRI]] brain with [[gadolinium]] [[enhancement]] is indicated in stable [[patients]] whereas, [[MRI]] of the [[dorsal]] and [[cervical]] [[spinal cord]] can determine the [[extent]] of [[inflammation]] in [[symptoms]] and [[signs]] suggestive of [[myelopathy]].


===Other Diagnostic Studies===
===Other Diagnostic Studies===
Many experts discourage [[diagnostic biopsies]] in the absence of structured [[histopathological]] guidelines. Nevertheless, typical [[lesions]] of [[ADEM]] may be identified by [[histopathology]] anywhere in the [[white matter]] of [[brain]] and [[spinal cord]].


==Treatment==
==Treatment==
===Medical Therapy===
===Medical Therapy===
The analogy between the [[pathogenesis]] of [[ADEM]] and [[MS]] forms the basis of the use of [[high-dose]] [[steroids]], [[plasma exchange]] and [[intravenous]] [[immunoglobulin]] for the [[treatment]] of [[ADEM]].


===Surgery===
===Surgery===
[[Surgical]] interventions can be helpful for managing [[complications]] like [[cerebral edema]], [[optic neuritis]] and [[elevated intracranial pressure]]. The options include:
*[[Decompressive hemi-craniectomy]]
*[[Bilteral]] [[optic nerve]] sheath decompression]]
*[[Lumboperitoneal]] [[shunting]]


===Prevention===
===Prevention===
The management protocol for [[ADEM]] does not routinely include [[strategies]] for [[primary prevention]].Case reports and [[literature reviews]] have highlighted the importance of early [[MRI]] scans of the [[brain]] as a guide for immediate intervention for [[ADEM]].[[Plasmapheresis]] should be considered early in the [[disease]] course for severe or life-threatening cases of [[ADEM]].


==References==
==References==
{{Reflist|2}}
{{Reflist|2}}


[[Category:Neurology]]
[[Category:Neurology]]

Latest revision as of 10:21, 8 December 2022

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]: Associate Editor(s)-in-Chief: Sujaya Chattopadhyay, M.D.[2] Shameera Shaik Masthan MBBS, DLO, DNB[3]

Overview

Acute disseminated encephalomyelitis (ADEM) is an acute neurologic disease of the central nervous system characterized by scattered foci of demyelination and perivascular inflammation. The disease may occur withoutprecipitant, or may develop after infection or vaccination.

Historical Perspective

Encephalomyelitis was primarily an experimental finding discovered after injection of rabbits with rabbit spinal cord infused with solutions of sodium chloride and lecithinase, adjuvants, like [[bayol F],] and killed tubercle bacilli, and human spinal cord treated with formaldehyde solution. Clinical signs were spasticity, ataxia, weakness and even death. The perivascular inflammatory lesions had a predilection for the white matter and demyelination was seen in all ages. Older lesions had glial scars.

Classification

Acute disseminated encephalomyelitis can occur after an episode of infection (post-infectious), vaccination or even, spontaneously without an obvious trigger (idiopathic).

Pathophysiology

The exact mechanism of acute disseminated encephalomyelitis is not determined. However, it is usually preceded by an environmental trigger, e.g. an infection or vaccination and affects individuals with a genetic predisposition.

Causes

In the past, ADEM was a sequelae of common childhood infections like measles, smallpox and chickenpox. With the improvements in infectious disease management practices, ADEM in developed countries frequently follow non-specific upper respiratory tract infections. Failure to identify a definite cause could suggest that the inciting agents are unusual and not recovered by standard laboratory tests. ADEM is much more common in the developing countries where measles and other viral infections still account for a major proportion of cases.

Another common variant is the postimmunisation encephalomyelitis, which has a preference for the peripheral nervous system. Currently, the most common implicated vaccines are measles, mumps and rubella. The risk of the condition developing after measles vaccination is considerably lower than the natural infection.

Differentiating Acute disseminated encephalomyelitis from Other Diseases

The differential diagnoses of Acute disseminated encephalomyelitis include:

Epidemiology and Demographics

The average annual incidence of ADEM is between 0.07 and 0.6 per 1,00,000 individuals per year. It is more common during childhood, with a median age on onset between 5-8 years and a male predominance (1.8:1).

Risk Factors

The risk factors for ADEM include:

Screening

There is no screening tool currently used for Acute disseminated encephalomyelitis.

Natural History, Complications, and Prognosis

The classic form, accounting for 70-90% of cases, typically follows a monophasic pattern. Residual severe disability is quite rare in pediatric ADEM cases (7%). Adult patients frequently suffer from residual ataxia, clumsiness, hemiparesis or epilepsy. The poor prognosis and long-term outcomes of ADEM have changed dramatically owing to efficient vaccination coverage and widespread, early use of high-dose steroids.

Diagnosis

Diagnostic Study of Choice

MRI is the best method for further evaluation after an initial suspicion of ADEM. MRI brain with gadolinium enhancement is indicated in stable patients whereas, MRI of the dorsal and cervical spinal cord can determine the extent of inflammation in symptoms and signs suggestive of myelopathy.

History and Symptoms

Classic ADEM is monophasic, with a history of usually a preceding illness or less commonly, a vaccination. It is characterised by an acute onset of focal neurologic symptoms, often with rapid deterioration of consciouness, after a variable latent period of several days to few months.

Physical Examination

Physical examination of ADEM may reveal positive findings in different parts of the nervous system namely, the cerebral cortex, brainstem, cranial nerves and the sensory and motor tracts. Respiratory failure may prove fatal in some cases.

Laboratory Findings

Antibodies like anti-MOG antibodies are found in the serum of patients suffering from ADEM. A lumbar puncture is also useful for evaluation of the changes in the Cerebrospinal fluid (CSF).

Imaging Findings

The appearance of ADEM on cranial CT has rarely been reported. There is a delay between the onset of the clinical signs and the appearance of lesions on CT scan. The correlation was limited between the clinical course and the anatomical distribution and type of abnormality seen on CT scan.

MRI is the best method for further evaluation after an initial suspicion of ADEM. MRI brain with gadolinium enhancement is indicated in stable patients whereas, MRI of the dorsal and cervical spinal cord can determine the extent of inflammation in symptoms and signs suggestive of myelopathy.

Other Diagnostic Studies

Many experts discourage diagnostic biopsies in the absence of structured histopathological guidelines. Nevertheless, typical lesions of ADEM may be identified by histopathology anywhere in the white matter of brain and spinal cord.

Treatment

Medical Therapy

The analogy between the pathogenesis of ADEM and MS forms the basis of the use of high-dose steroids, plasma exchange and intravenous immunoglobulin for the treatment of ADEM.

Surgery

Surgical interventions can be helpful for managing complications like cerebral edema, optic neuritis and elevated intracranial pressure. The options include:

Prevention

The management protocol for ADEM does not routinely include strategies for primary prevention.Case reports and literature reviews have highlighted the importance of early MRI scans of the brain as a guide for immediate intervention for ADEM.Plasmapheresis should be considered early in the disease course for severe or life-threatening cases of ADEM.

References

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