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ACUTE DISSEMINATED ENCEPHALOMYELITIS

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Physiotherapy can also be helpful. DIFFERENTIAL DIAGNOSIS At first presentation, it is difficult to differentiate between ADEM and MS. New lesions and relapses, ... – PowerPoint PPT presentation

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Title: ACUTE DISSEMINATED ENCEPHALOMYELITIS


1
ACUTE DISSEMINATED ENCEPHALOMYELITIS
2
PATIENT DETAILS
  • 9 month old male visiting Jhb with his parents
    and brother, living in Durban
  • Three day history of mild gastroenteritis with a
    low grade fever and a cough.
  • One day history of not moving his left arm.
  • Birth history- NVD at a hospital in Natal, no
    birth complications and well after birth.

3
DETAILS CONTINUED
  • PMH- nil
  • PSH- nil
  • Allergies- nil known
  • Medications- Augmentin and Panado from a private
    GP.
  • Feeding- Nan, cereal, purity and some vegetables

4
DETAILS CONTINUED
  • Development- appropriate for his age i.e. pulling
    to stand, sitting on his own and saying a few
    words.
  • Social- lives in Durban with his parents and an
    older brother, all of whom are well.
  • Immunizations up to date according to mother.

5
ON EXAMINATION
  • Growth parameters all on 50th centiles
  • Vitals essentially normal with a mild pyrexia
  • No lymphadenopathy
  • Not pale/jaundiced, not dehydrated
  • Chest harsh breath sounds bilaterally
  • CVS normal heart sounds no murmurs or
    gallop

6
EXAMINATION CONTINUED
  • Abdomen soft, non tender, no organomegaly
  • CNS lethargic and irritable but consolable,
    tone, power and reflexes decreased in
    left upper limb other limbs NAD
    mild terminal neck stiffness
  • ENT mild pharyngitis

7
INVESTIGATIONS
  • Blood results FBC- 9,2/13,4/301
    DIFF-27/10/62 UE- 136/5/103/22/4,2/30 Glucos
    e- 5 CRP- 2,3
  • CXR- features suggestive of mild pneumonia
  • In view of the apparent localising signs, we
    requested a CT brain prior to doing the LP-
    essentially normal.

8
INVESTIGATIONS CONTINUED
  • LP results CSF-clear and colourless prot
    ein- 0,33 glucose- 4,1 chloride-123
    polys- 0 lymphs- 40 erythrocytes-
    0 no bacteria grown

9
ASSESSMENT AND MANAGEMENT
  • 9/12 old male infant with acute mild
    bronchopneumonia and viral meningoencephalitis.
  • Treatment cefotaxime physiotherapy neur
    ological consult

10
NEUROLOGICAL REVIEW
  • On review it was noted that there was mild
    weakness in the left upper limb and that the
    condition seemed to be progressing to involve the
    left lower limb.
  • A suggestion was made to order an MRI scan which
    was done a few days later at Donald Gordon Centre
    with a finding of Acute Disseminated
    Encephalomyelitis (ADEM).

11
ADEM
  • This is an inflammatory demyelinating disorder of
    the subcortical white matter.
  • Most frequently seen in children, mf often
    evolving from antecedent infection or
    immunization.
  • Typical presentation encephalitic signs with non
    specific CSF changes and minimal or no changes on
    CT brain.

12
ADEM CONTINUED
  • Thought to be an autoimmune disease via cross
    reactivity of the antiviral antibodies with the
    myelin autoantigens.
  • Viruses associated include HSV,HIV, HSV6,
    measles, hepatitis, influenza, EBV etc.
  • There has also been an association post
    immunisation for MMR,Influenza, BCG.

13
APPROPRIATE INVESTIGATIONS
  • Lymphocytosis, raised CRP and ESR
  • CSF- can have a raised protein but can
    be normal.
  • CT Brain - may be normal
  • MRI- gold standard for diagnosis T2 weighted
    images show areas of prolonged T2 in
    subcortical white matter, usually assymetrical.

14
TREATMENT
  • Empirically treated as a meningitis with
    cefotaxime /- acyclovir.
  • Once diagnosis is made then steroids become the
    mainstay of management.
  • Physiotherapy can also be helpful.

15
DIFFERENTIAL DIAGNOSIS
  • At first presentation, it is difficult to
    differentiate between ADEM and MS.
  • New lesions and relapses, esp after 6/12 should
    alert to the possibility of MS.
  • MS - no prodromal viral illness and no fever or
    meninigism at presentation. It presents as a
    monosymptomatic syndrome eg optic neuritis or
    myelopathy and develops a relapsing remitting
    course.

16
PROGNOSIS OF ADEM
  • Most make excellent progress over the following
    days, weeks and months with no subsequent
    neurological impairment.
  • A minority have neurological impairment eg motor
    disability, visual/ cognitive or behavioural
    impairment.

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