Cerebral palsy differential diagnosis: Difference between revisions

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Revision as of 15:49, 3 October 2017

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief:

Overview

[Disease name] must be differentiated from other diseases that cause [clinical feature 1], [clinical feature 2], and [clinical feature 3], such as [differential dx1], [differential dx2], and [differential dx3].

OR

[Disease name] must be differentiated from [[differential dx1], [differential dx2], and [differential dx3].

Differentiating Cerebral Palsy from other Diseases

Cerebral Palsy must be differentiated from other slowly progressive diseases such as neurodegenerative disease or metabolic disorders.
Presence of any of the following factors may suggest an alternative diagnosis:^[1]
- Family history of any CNS disease
- Progressive worsening of neurological symptoms
- Symptoms worsened during stress such as illness or fasting
- Absence of any specific risk factor causing cerebral palsy
- Hypotonia with weakness
- Failure to develop milestones normally
- Clinical findings such as muscle atrophy, ataxia, sensory disturbances and involuntary movements
Cerebral Palsy must be differentiated from
- Inherited Metabolic Disorders Overview
- Intellectual Disability
- Metabolic Myopathies
- Metabolic Neuropathy
- Traumatic Peripheral Nerve Lesions
- Tumors of the Conus and Cauda Equina
- Vascular Malformations of the Spinal Cord

As [disease name] manifests in a variety of clinical forms, differentiation must be established in accordance with the particular subtype. [Subtype name 1] must be differentiated from other diseases that cause [clinical feature 1], such as [differential dx1] and [differential dx2]. In contrast, [subtype name 2] must be differentiated from other diseases that cause [clinical feature 2], such as [differential dx3] and [differential dx4].

Preferred Table

Diseases	Type of motor abnormality				Clinical findings	Laboratory findings and dianostic tests	Radiographic findings
Diseases	Spasticity	Hypotonia	Ataxia	Dystonia	Clinical findings	Laboratory findings and dianostic tests	Radiographic findings
Leigh syndrome	-	-	+	+	Progressive psychomotor regression Seizures External ophthalmoplegia Lactic acidosis Vomiting	Increased lactate levels in blood and CSF Genetic testing	MRI: abnormal white matter signal in the putamen, basal ganglia, and brainstem on T2 images
Niemann-Pick disease type C	-	-	+	+	Progressive neurodegeneration Hepatosplenomegaly Systemic involvement of liver, spleen, or lung precedes neurologic symptoms	Abnormal liver function tests Fibroblast cell culture with filipin staining	MRI: cerebral and cerebellar atrophy thinning of the corpus callosum
Infantile Refsum disease	-	+	+	-	Abnormalities of the optic nerve and disc Retinitis pigmentosa Sensorineural hearing loss Hepatomegaly and cirrhosis Neurologic deterioration is slower than in Zellweger syndrome or ALD	Elevated plasma VLCFA levels
Adrenoleukodystrophy	+	-	-	-	Cognitive and behavioral abnormalities Adrenal insufficiency Hyperpigmented skin Gonadal dysfunction Neurologic deterioration progresses at a variable rate
Differential Diagnosis 5

References

↑ Gupta R, Appleton RE (2001). "Cerebral palsy: not always what it seems". Arch. Dis. Child. 85 (5): 356–60. PMC 1718969. PMID 11668092.

Template:WH Template:WS

[pmid11668092-1] Gupta R, Appleton RE (2001). "Cerebral palsy: not always what it seems". Arch. Dis. Child. 85 (5): 356–60. PMC 1718969. PMID 11668092.

[1]

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 | style="background: #DCDCDC; padding: 5px; text-align: center;" |Leigh syndrome
-| style="background: #F5F5F5; padding: 5px;" |-
+| style="background: #F5F5F5; padding: 5px;" | -
-| style="background: #F5F5F5; padding: 5px;" |-
+| style="background: #F5F5F5; padding: 5px;" | -
 | style="background: #F5F5F5; padding: 5px;" |<nowiki>+</nowiki>
-| style="background: #F5F5F5; padding: 5px;" |+
+| style="background: #F5F5F5; padding: 5px;" | +
 |
 * Progressive psychomotor regression
@@ Line 58: / Line 58: @@
 |
 * Increased lactate levels in blood and CSF
-* Genetic testing for specific mutations
+* Genetic testing
 |
+* <blockquote>MRI: abnormal white matter signal in the putamen, basal ganglia, and brainstem on T2 images</blockquote>
 |-
-| style="background: #DCDCDC; padding: 5px; text-align: center;" |Differential Diagnosis 2
+| style="background: #DCDCDC; padding: 5px; text-align: center;" |Niemann-Pick disease type C
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |-
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |-
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |+
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" | +
 |
+* Progressive neurodegeneration
+* Hepatosplenomegaly
+* Systemic involvement of liver, spleen, or lung precedes neurologic symptoms
 |
+* Abnormal liver function tests
+* Fibroblast cell culture with filipin staining
 |
+* <blockquote>MRI: </blockquote>
+** <blockquote>cerebral and cerebellar atrophy </blockquote>
+** <blockquote>thinning of the corpus callosum</blockquote>
 |-
-| style="background: #DCDCDC; padding: 5px; text-align: center;" |Differential Diagnosis 3
+| style="background: #DCDCDC; padding: 5px; text-align: center;" |Infantile Refsum disease
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |-
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |+
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |+
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |-
-|
 |
+* Abnormalities of the optic nerve and disc
+* Retinitis pigmentosa
+* Sensorineural hearing loss
+* Hepatomegaly and cirrhosis
+* Neurologic deterioration is slower than in Zellweger syndrome or ALD
+|Elevated plasma VLCFA levels
 |
 |-
-| style="background: #DCDCDC; padding: 5px; text-align: center;" |Differential Diagnosis 4
+| style="background: #DCDCDC; padding: 5px; text-align: center;" |Adrenoleukodystrophy
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |+
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |-
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |-
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |-
 |
+* Cognitive and behavioral abnormalities
+* Adrenal insufficiency
+* Hyperpigmented skin
+* Gonadal dysfunction
+* Neurologic deterioration progresses at a variable rate
 |
 |