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Revision as of 15:18, 15 June 2020

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Zehra Malik, M.B.B.S [2]

Synonyms and keywords: Dandy-Walker Malformation, Dandy-Walker Deformity

Overview

Historical Perspective

The term Dandy-Walker Syndrome was introduced in 1954 by a German psychiatrist Clemens Benda in the light of the following discoveries,
- In 1914, American neurosurgeon Walter Dandy and American pediatrician Kenneth Blackfan recognized the association between the partial or complete absence of cerebellar vermis, hydrocephalus, and fourth ventricular enlargement.
- In 1942, Canadian-American neurosurgeon Arthur Earl Walker and American physician John Taggart contributed by highlighting the possible cause to be the maldevelopment of the foramen of Lushka and Magendie.
An English surgeon named John Bland Sutton was the first to describe the association of underdeveloped cerebellar vermis, hydrocephalus, and an enlarged posterior fossa in 1887.

Classification

There is no established system for the classification of Dandy-Walker Syndrome. However, Barkovich classified posterior fossa CSF collection into the following:


Dandy-Walker Complex	Posterior fossa arachnoid cyst	Prominent Cisterna Magna
Includes posterior fossa CSF collection communicating with the fourth ventricle.	Includes posterior fossa CSF
Further divided into Type A or B depending on the visibility of cerebellar vermis. In Type A cerebellar vermis is not visible and in Type B cerebellar vermis is visible

Pathophysiology

It is thought that Dandy-Walker Syndrome is the result of disruptions that occur during the development of cerebellar vermis leading to a fourth ventricle that is in continuation with the posterior fossa subarachnoid space.
Embryonic development of cerebellum starts at week 5, it forms from the top part of metencephalon. The cerebellar hemisphere is formed from the forward surface of fourth ventricle. The lack of midline fusion of the cerebellar hemisphere by the 15th week of embryonic development results into underdeveloped cerebellar vermis. ^[1]
The exact pathogenesis of hydrocephalus in Dandy-Walker Syndrome is not fully understood. Several factors could play a role in development of hydrocephalus.
- The initial hypothesis of atresia of foramen of Luschka and Magendie as a possible cause is not well supported. It was found later that these foramens are patent in a large number of patients with DWM and hydrocephalus is not present at birth in more than 80% of patients diagnosed with DWM. Moreover, the closure of one or two foramen can be compensated by presence of other foramens preventing collection of fluid.
- Another hypothesis was proposed suggesting the outflow impairment to be distal to fourth ventricle outlets, possibly caused by inflammation of arachnoid mater causing outflow obstruction. Excisions of these obstructions have not been able to show whether impaired arachnoid absorption is involved, since the subarachnoid space always takes days to weeks to fill up following excision. ^[1]
- Stenosis of aqueduct of Sylvius once suggested, does not seem to be the causing factor in pathogenesis of hydrocephalus. Shunts placed in the posterior fossa cyst almost always drain all above ventricles. Occasionally when it is present, it is functional stenosis caused by herniation of posterior fossa content. ^[1]
- Increased pressure in venous sinuses due to compression from the posterior fossa cyst could also contribute to the pathogenesis or worsening of hydrocephalus, no evidence has been found so far.^[1]
- The importance of understanding the pathogenesis of hydrocephalus in Dandy-Walker Syndrome forms the basis of choosing most appropriate treatment.

Causes

Several etiologic factors can lead to Dandy-Walker Syndrome, it is the time (4th to 7th embryonic week) and duration of insult that has more influence on the occurrence of disease rather than the type of causative factor.
Mendelian conditions like Walker-Warburg Syndrome, Mohr Syndrome, Meckel-Gruber Syndrome are associated with Dandy-Walker Malformation.
Genetic factors that are associated with DWM phenotype include:
- Trisomy 18, triploidy and trisomy 13 most commonly.
- First molecularly defined cause is the Z1C1 and Z1C4 heterozygous deletion on chromosome 3q24.
- Second DWM-linked locus is the deletion or duplication of FOXC1 gene on 6p25.3.
- Deletions on the long arm of chromosome 13.
Environmental factors include prenatal exposure to rubella, cytomegalovirus, toxoplasmosis, coumadin, alcohol and maternal diabetes.^[2]

Differentiating Dandy-Walker Syndrome from other Diseases

Dandy-Walker Syndrome must be differentiated from Blake's pouch cyst, mega cisterna magna, and posterior fossa arachnoid cyst.

Blake's pouch cyst occurs if invagination of the fourth ventricle fails to rupture by the fourth month of gestation. The disease differs from Dandy-Walker Syndrome due to the following features:
- The cerebellum is not hypoplastic, though it may be compressed by the enlarged posterior fossa (mass effect).
- The cerebellar tentorium/confluence of sinuses is not raised.
- Hydrocephalus, if present involves all four ventricles.

Mega cisterna magna occurs due to delay in rupture of the fourth ventricle invagination. The disease differs from Dandy-Walker Syndrome due to the following features:
- The cerebellum is not usually hypoplastic.
- The fourth ventricle is of relatively normal shape.
- Hydrocephalus is uncommon.

Posterior fossa arachnoid cyst is a collection of cerebrospinal fluid in the arachnoid mater. The disease differs from Dandy-Walker Syndrome due to the following features:
- The cyst is clearly localized in a specific location separate from the fourth ventricle outlets.
- The cerebellum is not hypoplastic, though it may be compressed by the cyst (mass effect).
- The CSF flow in the cyst is not continuous with that of the fourth ventricle.
- Hydrocephalus, if it occurs, is due to the cyst pressing on the cerebellum and compressing the cerebral aqueduct or fourth ventricle outlets.

Epidemiology and Demographics

The prevalence of Dandy-Walker Syndrome is approximately 1 in 25,000 to 1 in 30,000 live births.
Slight female predominance is observed.^[1]
Dandy-Walker Syndrome is the underlying cause of 1% to 4% of cases of hydrocephalus.
There is no established racial predilection to Dandy-Walker Syndrome.

Risk Factors

There are no established risk factors for Dandy-Walker Syndrome. However, non-Hispanic black ethnicity and history of infertility were seen to increase the risk of DWM, further research is required. ^[3]

Screening

There is insufficient evidence to recommend routine screening for DWM.

Natural History, Complications, and Prognosis

If left untreated, patients with Dandy-Walker Syndrome may progress to develop severe neurologic deficits. Fifty percent of patients affected die before reaching the third year of life. The 20-23% of patients that reach adult life will have auditory, visual, and motor deficits.
Other possible complications include malformations of gastrointestinal, face, limb, heart, and genitourinary system.
Prognosis is generally poor if hydrocephalus is left untreated.

Diagnosis

Diagnostic Study of Choice

History and Symptoms

The majority of the patients (up to 85%) present in the first year of life with signs and symptoms of increased intracranial pressure such as irritability, increased head circumference, vomiting, convulsions.^[1]

Physical Examination

Signs of hydrocephalus in infants include increasing head size, vomiting, excessive sleepiness, irritability, downward deviation of the eyes (known as "sunsetting eyes"), and seizures.

Laboratory Findings

There are no diagnostic laboratory findings associated with Dandy-Walker Syndrome.

Electrocardiogram

There are no ECG findings associated with Dandy-Walker Syndrome.

X-ray

There are no x-ray findings associated with Dandy-Walker Syndrome.

Echocardiography or Ultrasound

There are no echocardiography findings associated with Dandy-Walker Syndrome.
Fetal 3D ultrasound can suspect posterior fossa malformation as early as 14 weeks of gestation. However, it should be confirmed by a fetal MRI.

CT scan

If MRI is unavailable then CT may be used, but it is less detailed.^[1]
It is suggested that a suspected diagnosis based on CT should be confirmed by performing an MRI.

MRI

An MRI is the most important imaging modality in diagnosing Dandy-Walker Syndrome due to its superior anatomic resolution and multiplanar imaging.

Other Imaging Findings

There are no other imaging findings associated with Dandy-Walker Syndrome.

Other Diagnostic Studies

There are no other diagnostic studies associated with Dandy-Walker Syndrome.

Treatment

Medical Therapy

Surgery

Primary Prevention

There are no established measures for the primary prevention of Dandy-Walker Syndrome.

Secondary Prevention

References

↑ ^1.0 ^1.1 ^1.2 ^1.3 ^1.4 ^1.5 ^1.6 Spennato, Pietro; Mirone, Giuseppe; Nastro, Anna; Buonocore; Ruggiero, Claudio; Trischitta, Vincenzo; Aliberti, Ferdinando; Cinalli, Giuseppe (2011). "Hydrocephalus in Dandy–Walker malformation". Child's Nervous System. 27 (10): 1665–1681. doi:10.1007/s00381-011-1544-4. ISSN 0256-7040. Unknown parameter |sufirst4= ignored (help)
↑ Murray, Jeffrey C.; Johnson, Jennifer A.; Bird, Thomas D. (2008). "Dandy-Walker malformation: etiologic heterogeneity and empiric recurrence risks". Clinical Genetics. 28 (4): 272–283. doi:10.1111/j.1399-0004.1985.tb00401.x. ISSN 0009-9163.
↑ Reeder, Matthew R.; Botto, Lorenzo D.; Keppler-Noreuil, Kim M.; Carey, John C.; Byrne, Janice L. B.; Feldkamp, Marcia L. (2015). "Risk factors for Dandy-Walker malformation: A population-based assessment". American Journal of Medical Genetics Part A. 167 (9): 2009–2016. doi:10.1002/ajmg.a.37124. ISSN 1552-4825.

[SpennatoMirone2011-1] 1.0 ^1.1 ^1.2 ^1.3 ^1.4 ^1.5 ^1.6 Spennato, Pietro; Mirone, Giuseppe; Nastro, Anna; Buonocore; Ruggiero, Claudio; Trischitta, Vincenzo; Aliberti, Ferdinando; Cinalli, Giuseppe (2011). "Hydrocephalus in Dandy–Walker malformation". Child's Nervous System. 27 (10): 1665–1681. doi:10.1007/s00381-011-1544-4. ISSN 0256-7040. Unknown parameter |sufirst4= ignored (help)

[MurrayJohnson2008-2] Murray, Jeffrey C.; Johnson, Jennifer A.; Bird, Thomas D. (2008). "Dandy-Walker malformation: etiologic heterogeneity and empiric recurrence risks". Clinical Genetics. 28 (4): 272–283. doi:10.1111/j.1399-0004.1985.tb00401.x. ISSN 0009-9163.

[ReederBotto2015-3] Reeder, Matthew R.; Botto, Lorenzo D.; Keppler-Noreuil, Kim M.; Carey, John C.; Byrne, Janice L. B.; Feldkamp, Marcia L. (2015). "Risk factors for Dandy-Walker malformation: A population-based assessment". American Journal of Medical Genetics Part A. 167 (9): 2009–2016. doi:10.1002/ajmg.a.37124. ISSN 1552-4825.

[1]

[2]

[3]

@@ Line 11: / Line 11: @@
 ==Historical Perspective==
-*The term Dandy-Walker Syndrome was introduced in 1954 by a German psychiatrist Clemens Benda in the light of the following discoveries,<ref name="Benda1954">{{cite journal|last1=Benda|first1=Clemens E.|title=The Dandy-Walker Syndrome or The So-Called Atresia of the Foramen Magendie*|journal=Journal of Neuropathology & Experimental Neurology|volume=13|issue=1|year=1954|pages=14–29|issn=1554-6578|doi=10.1093/jnen/13.1.14}}</ref>
+*The term Dandy-Walker Syndrome was introduced in 1954 by a German psychiatrist Clemens Benda in the light of the following discoveries,
-**In 1914, American neurosurgeon Walter Dandy and American pediatrician Kenneth Blackfan recognized the association between the partial or complete absence of [[cerebellar vermis]], [[hydrocephalus]], and fourth ventricular enlargement.<ref name="Dandy1914">{{cite journal|last1=Dandy|first1=Walter E.|title=AN EXPERIMENTAL, CLINICAL AND PATHOLOGICAL STUDY|journal=American Journal of Diseases of Children|volume=VIII|issue=6|year=1914|pages=406|issn=0096-8994|doi=10.1001/archpedi.1914.02180010416002}}</ref>
+**In 1914, American neurosurgeon Walter Dandy and American pediatrician Kenneth Blackfan recognized the association between the partial or complete absence of [[cerebellar vermis]], [[hydrocephalus]], and fourth ventricular enlargement.
-**In 1942, Canadian-American neurosurgeon Arthur Earl Walker and American physician John Taggart contributed by highlighting the possible cause to be the maldevelopment of the foramen of Lushka and Magendie.<ref name="Taggart1942">{{cite journal|last1=Taggart|first1=John K.|title=CONGENITAL ATRESIA OF THE FORAMENS OF LUSCHKA AND MAGENDIE|journal=Archives of Neurology And Psychiatry|volume=48|issue=4|year=1942|pages=583|issn=0096-6754|doi=10.1001/archneurpsyc.1942.02290100083008}}</ref>
+**In 1942, Canadian-American neurosurgeon Arthur Earl Walker and American physician John Taggart contributed by highlighting the possible cause to be the maldevelopment of the foramen of Lushka and Magendie.
-*An English surgeon named John Bland Sutton was the first to describe the association of underdeveloped [[cerebellar vermis]], [[hydrocephalus]], and an enlarged [[posterior fossa]] in 1887.<ref name="Sutton1886">{{cite journal|last1=Sutton|first1=J. Bland|title=THE LATERAL RECESSES OF THE FOURTH VENTRICLE; THEIR RELATION TO CERTAIN CYSTS AND TUMOURS OF THE CEREBELLUM, AND TO OCCIPITAL MENINGOCELE|journal=Brain|volume=9|issue=3|year=1886|pages=352–361|issn=0006-8950|doi=10.1093/brain/9.3.352}}</ref>
+*An English surgeon named John Bland Sutton was the first to describe the association of underdeveloped [[cerebellar vermis]], [[hydrocephalus]], and an enlarged [[posterior fossa]] in 1887.
 ==Classification==
 *There is no established system for the [[classification]] of Dandy-Walker Syndrome. However, Barkovich classified posterior fossa CSF collection into the following:
+<br />
+{| class="wikitable"
+|+
+!Dandy-Walker Complex
+!Posterior fossa arachnoid cyst
+!Prominent Cisterna Magna
+|-
+|Includes posterior fossa
+CSF collection communicating
+with the fourth ventricle.
+|Includes posterior fossa CSF
+|
+|-
+|Further divided into Type A or B
+depending on the visibility of cerebellar vermis. In Type A cerebellar vermis is not visible and in Type B cerebellar vermis is visible
+|
+|
+|-
+|
+|
+|
+|}
 ==Pathophysiology==
-*It is thought that Dandy-Walker Syndrome is the result of disruptions that occur during the development of [[cerebellar vermis]] leading to a [[fourth ventricle]] that is in continuation with the [[posterior fossa]] [[subarachnoid space]].<ref name="SpennatoMirone2011">{{cite journal|last1=Spennato|first1=Pietro|last2=Mirone|first2=Giuseppe|last3=Nastro|first3=Anna|last4=Buonocore| sufirst4=Maria Consiglio|last5=Ruggiero|first5=Claudio|last6=Trischitta|first6=Vincenzo|last7=Aliberti|first7=Ferdinando|last8=Cinalli|first8=Giuseppe|title=Hydrocephalus in Dandy–Walker malformation|journal=Child's Nervous System|volume=27|issue=10|year=2011|pages=1665–1681|issn=0256-7040|doi=10.1007/s00381-011-1544-4}}</ref>
+*It is thought that Dandy-Walker Syndrome is the result of disruptions that occur during the development of [[cerebellar vermis]] leading to a [[fourth ventricle]] that is in continuation with the [[posterior fossa]] [[subarachnoid space]].
 *Embryonic development of [[cerebellum]] starts at week 5, it forms from the top part of [[metencephalon]]. The [[cerebellar hemisphere]] is formed from the forward surface of [[fourth ventricle]]. The lack of midline fusion of the [[cerebellar hemisphere]] by the 15th week of embryonic development results into underdeveloped [[cerebellar vermis]]. <ref name="SpennatoMirone2011">{{cite journal|last1=Spennato|first1=Pietro|last2=Mirone|first2=Giuseppe|last3=Nastro|first3=Anna|last4=Buonocore| sufirst4=Maria Consiglio|last5=Ruggiero|first5=Claudio|last6=Trischitta|first6=Vincenzo|last7=Aliberti|first7=Ferdinando|last8=Cinalli|first8=Giuseppe|title=Hydrocephalus in Dandy–Walker malformation|journal=Child's Nervous System|volume=27|issue=10|year=2011|pages=1665–1681|issn=0256-7040|doi=10.1007/s00381-011-1544-4}}</ref>
 *The exact [[pathogenesis]] of [[hydrocephalus]] in Dandy-Walker Syndrome is not fully understood. Several factors could play a role in development of [[hydrocephalus]].
-**The initial hypothesis of atresia of foramen of Luschka and Magendie as a possible cause is not well supported. It was found later that these foramens are patent in a large number of patients with [[DWM]] and [[hydrocephalus]] is not present at birth in more than 80% of patients diagnosed with DWM.  Moreover, the closure of one or two foramen can be compensated by presence of other foramens preventing collection of fluid.<ref name="TakamiShin2010">{{cite journal|last1=Takami|first1=Hirokazu|last2=Shin|first2=Masahiro|last3=Kuroiwa|first3=Masafumi|last4=Isoo|first4=Ayako|last5=Takahashi|first5=Kan|last6=Saito|first6=Nobuhito|title=Hydrocephalus associated with cystic dilation of the foramina of Magendie and Luschka|journal=Journal of Neurosurgery: Pediatrics|volume=5|issue=4|year=2010|pages=415–418|issn=1933-0707|doi=10.3171/2009.10.PEDS09179}}</ref>
+**The initial hypothesis of atresia of foramen of Luschka and Magendie as a possible cause is not well supported. It was found later that these foramens are patent in a large number of patients with [[DWM]] and [[hydrocephalus]] is not present at birth in more than 80% of patients diagnosed with DWM.  Moreover, the closure of one or two foramen can be compensated by presence of other foramens preventing collection of fluid.
 **Another hypothesis was proposed suggesting the outflow impairment to be distal to [[fourth ventricle]] outlets, possibly caused by [[inflammation]] of [[arachnoid mater]] causing outflow obstruction. Excisions of these obstructions have not been able to show whether impaired arachnoid absorption is involved, since the subarachnoid space always takes days to weeks to fill up following excision. <ref name="SpennatoMirone2011">{{cite journal|last1=Spennato|first1=Pietro|last2=Mirone|first2=Giuseppe|last3=Nastro|first3=Anna|last4=Buonocore| sufirst4=Maria Consiglio|last5=Ruggiero|first5=Claudio|last6=Trischitta|first6=Vincenzo|last7=Aliberti|first7=Ferdinando|last8=Cinalli|first8=Giuseppe|title=Hydrocephalus in Dandy–Walker malformation|journal=Child's Nervous System|volume=27|issue=10|year=2011|pages=1665–1681|issn=0256-7040|doi=10.1007/s00381-011-1544-4}}</ref>
 **[[Stenosis]] of [[aqueduct of Sylvius]] once suggested, does not seem to be the causing factor in [[pathogenesis]] of [[hydrocephalus]]. [[Shunts]] placed in the [[posterior fossa]] [[cyst]] almost always drain all above [[ventricles]]. Occasionally when it is present, it is functional [[stenosis]] caused by herniation of posterior fossa content. <ref name="SpennatoMirone2011">{{cite journal|last1=Spennato|first1=Pietro|last2=Mirone|first2=Giuseppe|last3=Nastro|first3=Anna|last4=Buonocore| sufirst4=Maria Consiglio|last5=Ruggiero|first5=Claudio|last6=Trischitta|first6=Vincenzo|last7=Aliberti|first7=Ferdinando|last8=Cinalli|first8=Giuseppe|title=Hydrocephalus in Dandy–Walker malformation|journal=Child's Nervous System|volume=27|issue=10|year=2011|pages=1665–1681|issn=0256-7040|doi=10.1007/s00381-011-1544-4}}</ref>
 **Increased pressure in venous sinuses due to compression from the posterior fossa cyst could also contribute to the pathogenesis or worsening of [[hydrocephalus]], no evidence has been found so far.<ref name="SpennatoMirone2011">{{cite journal|last1=Spennato|first1=Pietro|last2=Mirone|first2=Giuseppe|last3=Nastro|first3=Anna|last4=Buonocore| sufirst4=Maria Consiglio|last5=Ruggiero|first5=Claudio|last6=Trischitta|first6=Vincenzo|last7=Aliberti|first7=Ferdinando|last8=Cinalli|first8=Giuseppe|title=Hydrocephalus in Dandy–Walker malformation|journal=Child's Nervous System|volume=27|issue=10|year=2011|pages=1665–1681|issn=0256-7040|doi=10.1007/s00381-011-1544-4}}</ref>
 **The importance of understanding the [[pathogenesis]] of [[hydrocephalus]] in Dandy-Walker Syndrome forms the basis of choosing most appropriate [[treatment]].
 ==Causes==
-*Several etiologic factors can lead to Dandy-Walker Syndrome, it is the time (4th to 7th embryonic week) and duration of insult that has more influence on the occurrence of disease rather than the type of causative factor. <ref name="Jaspan2008">{{cite journal|last1=Jaspan|first1=Tim|title=New concepts on posterior fossa malformations|journal=Pediatric Radiology|volume=38|issue=S3|year=2008|pages=409–414|issn=0301-0449|doi=10.1007/s00247-008-0848-3}}</ref>
+*Several etiologic factors can lead to Dandy-Walker Syndrome, it is the time (4th to 7th embryonic week) and duration of insult that has more influence on the occurrence of disease rather than the type of causative factor.
-*Mendelian conditions like [[Walker-Warburg Syndrome]], [[Mohr Syndrome]], [[Meckel-Gruber Syndrome]] are associated with Dandy-Walker Malformation. <ref name="MurrayJohnson2008">{{cite journal|last1=Murray|first1=Jeffrey C.|last2=Johnson|first2=Jennifer A.|last3=Bird|first3=Thomas D.|title=Dandy-Walker malformation: etiologic heterogeneity and empiric recurrence risks|journal=Clinical Genetics|volume=28|issue=4|year=2008|pages=272–283|issn=00099163|doi=10.1111/j.1399-0004.1985.tb00401.x}}</ref>
+*Mendelian conditions like [[Walker-Warburg Syndrome]], [[Mohr Syndrome]], [[Meckel-Gruber Syndrome]] are associated with Dandy-Walker Malformation.
 *Genetic factors that are associated with DWM [[phenotype]] include:
 **[[Trisomy 18]], [[triploidy]] and [[trisomy 13]] most commonly.
@@ Line 61: / Line 85: @@
 ==Epidemiology and Demographics==
-*The [[prevalence]] of Dandy-Walker Syndrome is approximately 1 in 25,000 to 1 in 30,000 live births.<ref name="StambolliuIoakeim-Ioannidou2017">{{cite journal|last1=Stambolliu|first1=Emelina|last2=Ioakeim-Ioannidou|first2=Myrsini|last3=Kontokostas|first3=Kimonas|last4=Dakoutrou|first4=Maria|last5=Kousoulis|first5=Antonis A.|title=The Most Common Comorbidities in Dandy-Walker Syndrome Patients: A Systematic Review of Case Reports|journal=Journal of Child Neurology|volume=32|issue=10|year=2017|pages=886–902|issn=0883-0738|doi=10.1177/0883073817712589}}</ref>
+*The [[prevalence]] of Dandy-Walker Syndrome is approximately 1 in 25,000 to 1 in 30,000 live births.
 *Slight female predominance is observed.<ref name="SpennatoMirone2011">{{cite journal|last1=Spennato|first1=Pietro|last2=Mirone|first2=Giuseppe|last3=Nastro|first3=Anna|last4=Buonocore|first4=Maria Consiglio|last5=Ruggiero|first5=Claudio|last6=Trischitta|first6=Vincenzo|last7=Aliberti|first7=Ferdinando|last8=Cinalli|first8=Giuseppe|title=Hydrocephalus in Dandy–Walker malformation|journal=Child's Nervous System|volume=27|issue=10|year=2011|pages=1665–1681|issn=0256-7040|doi=10.1007/s00381-011-1544-4}}</ref>
-*Dandy-Walker Syndrome is the underlying cause of 1% to 4% of cases of [[hydrocephalus]].<ref name="HirschPierre-Kahn1984">{{cite journal|last1=Hirsch|first1=Jean-François|last2=Pierre-Kahn|first2=Alain|last3=Renier|first3=Dominique|last4=Sainte-Rose|first4=Christian|last5=Hoppe-Hirsch|first5=Elizabeth|title=The Dandy-Walker malformation|journal=Journal of Neurosurgery|volume=61|issue=3|year=1984|pages=515–522|issn=0022-3085|doi=10.3171/jns.1984.61.3.0515}}</ref>
+*Dandy-Walker Syndrome is the underlying cause of 1% to 4% of cases of [[hydrocephalus]].
-*There is no established [[racial]] predilection to Dandy-Walker Syndrome.<ref name="ReederBotto2015">{{cite journal|last1=Reeder|first1=Matthew R.|last2=Botto|first2=Lorenzo D.|last3=Keppler-Noreuil|first3=Kim M.|last4=Carey|first4=John C.|last5=Byrne|first5=Janice L. B.|last6=Feldkamp|first6=Marcia L.|title=Risk factors for Dandy-Walker malformation: A population-based assessment|journal=American Journal of Medical Genetics Part A|volume=167|issue=9|year=2015|pages=2009–2016|issn=15524825|doi=10.1002/ajmg.a.37124}}</ref>
+*There is no established [[racial]] predilection to Dandy-Walker Syndrome.
 ==Risk Factors==
@@ Line 76: / Line 100: @@
 ==Natural History, Complications, and Prognosis==
-*If left untreated, [[patients]] with Dandy-Walker Syndrome may progress to develop severe neurologic deficits. Fifty percent of patients affected die before reaching the third year of life. The 20-23% of patients that reach adult life will have auditory, visual, and motor deficits. <ref name="ChumasTyagi2001">{{cite journal|last1=Chumas|first1=P|last2=Tyagi|first2=A|last3=Livingston|first3=J|title=Hydrocephalus---what's new?|journal=Archives of Disease in Childhood - Fetal and Neonatal Edition|volume=85|issue=3|year=2001|pages=149F–154|issn=1359-2998|doi=10.1136/fn.85.3.F149}}</ref>
+*If left untreated, [[patients]] with Dandy-Walker Syndrome may progress to develop severe neurologic deficits. Fifty percent of patients affected die before reaching the third year of life. The 20-23% of patients that reach adult life will have auditory, visual, and motor deficits.
 *Other possible [[complications]] include [[malformations]] of gastrointestinal, face, limb, heart, and genitourinary system.
 *[[Prognosis]] is generally poor if [[hydrocephalus]] is left untreated.
@@ Line 101: / Line 125: @@
 '''Echocardiography or Ultrasound'''
 *There are no echocardiography findings associated with Dandy-Walker Syndrome.
-*Fetal 3D ultrasound can suspect posterior fossa malformation as early as 14 weeks of gestation. However, it should be confirmed by a fetal MRI.<ref name="StamatianKovacs2015">{{cite journal|last1=Stamatian|first1=Florin|last2=Kovacs|first2=Tunde|last3=Boitor-Borza|first3=Dan|title=Transvaginal Three-dimensional Sonographic Assessment of the Embryonic Brain: A Pilot Study|journal=Medicine and Pharmacy Reports|volume=88|issue=2|year=2015|pages=152–158|issn=2668-0572|doi=10.15386/cjmed-437}}</ref>
+*Fetal 3D ultrasound can suspect posterior fossa malformation as early as 14 weeks of gestation. However, it should be confirmed by a fetal MRI.
 '''CT scan'''
 *If MRI is unavailable then CT may be used, but it is less detailed.<ref name="SpennatoMirone2011">{{cite journal|last1=Spennato|first1=Pietro|last2=Mirone|first2=Giuseppe|last3=Nastro|first3=Anna|last4=Buonocore|first4=Maria Consiglio|last5=Ruggiero|first5=Claudio|last6=Trischitta|first6=Vincenzo|last7=Aliberti|first7=Ferdinando|last8=Cinalli|first8=Giuseppe|title=Hydrocephalus in Dandy–Walker malformation|journal=Child's Nervous System|volume=27|issue=10|year=2011|pages=1665–1681|issn=0256-7040|doi=10.1007/s00381-011-1544-4}}</ref>
-*It is suggested that a suspected diagnosis based on CT should be confirmed by performing an MRI.<ref name="KleinPierre-Kahn2003">{{cite journal|last1=Klein|first1=O.|last2=Pierre-Kahn|first2=A.|last3=Boddaert|first3=N.|last4=Parisot|first4=D.|last5=Brunelle|first5=F.|title=Dandy-Walker malformation: prenatal diagnosis and prognosis|journal=Child's Nervous System|volume=19|issue=7-8|year=2003|pages=484–489|issn=0256-7040|doi=10.1007/s00381-003-0782-5}}</ref>
+*It is suggested that a suspected diagnosis based on CT should be confirmed by performing an MRI.
 '''MRI'''
@@ Line 130: / Line 154: @@
 ==References==
+<references />