What Syndrome’s That? - American Academy of Dermatology F081 - Siegel... · What Syndrome’s...

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What Syndrome’s That? Syndromes Associated with Vascular Anomalies Dawn Siegel, MD Medical College of Wisconsin American Academy of Dermatology Meeting San Diego, CA Sat. February 17 th , 2018

Transcript of What Syndrome’s That? - American Academy of Dermatology F081 - Siegel... · What Syndrome’s...

Page 1: What Syndrome’s That? - American Academy of Dermatology F081 - Siegel... · What Syndrome’s That? Syndromes Associated with Vascular Anomalies Dawn Siegel, MD Medical College

What Syndrome’s That?

Syndromes Associated with Vascular Anomalies Dawn Siegel, MD

Medical College of Wisconsin American Academy of Dermatology Meeting

San Diego, CA Sat. February 17th, 2018

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Learning objectives

• Recognize the syndromic features associated with vascular anomalies and infantile hemangiomas

• Learn about genotype-phenotype correlations for these disorders

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De novo germline and postzygotic mutations in AKT3, PIK3R2, PIK3CA cause a spectrum of related megalencephaly syndromes

Large head, prominent forehead

Diffuse capillary malformation

Digital anomalies and syndactyly

Riviere et al, Nature Genetics, 2012 and Mirzaa et al 2012

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PI3K pathway

– Signaling enzymes, regulate wide range of processes

– Cell growth, proliferation, survival, migration, angiogenesis, apoptosis, tumorigenesis, brain development

Nature Medicine 14, 1315 - 1316 (2008)

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Somatic Mosaic Activating Mutations in PIK3CA Cause CLOVES Syndrome

Kurek et al, Am J Hum Gen, 2012

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Somatic gain-of-function mutations in PIK3CA in patients with macrodactaly

Rios et al, Human Molecular Genetics 2013

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De Novo somatic mutations in

components of PI3K-AKT3-mTOR

pathway cause hemimegalencephaly

Lee et al, Nature Genetics, 2012

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PIK3CA Activating Mutations in Facial Infiltrating Lipomatosis

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Vascular Overgrowth Syndromes

• Mutations in the PIK3CA gene can cause many different phenotypes

– Likely based on the tissue distribution of the mosaic mutations

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n engl j med 368;21 nejm.org may 23, 2013

Sturge-Weber is caused by mutations in GNAQ

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GNAQ

• Uveal melanoma

• Capillary malformation

GNAQ p.Arg183Gln GNAQ p.Gln209Leu and p.Arg183Gln

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Sturge-Weber Syndrome

1 in 20,000 to 50,000 live births Venous-capillary abnormalities of the leptomeninges and choroid plexus

Neurological

– Seizures – Developmental delay – Calcification of the occipital and/or temporal cortex

Ocular findings:

– Congenital glaucoma – Increased choroidal vascularity

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Spectrum of phenotypes associated with G-proteins

• Capillary malformations

• Phakomatosis pigmentovascularis

• Sturge-Weber

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• Patient with multiple capillary malformations

• Family History: Stroke in Maternal Uncle in 30’s

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Capillary Malformation AVM- Cutaneous findings

• CMs are small, oval multifocal and randomly distributed

• Pink-to-red or brown

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CM-AVM Extracutaneous features

• AVM’s and AVF’s in 18.5%

– Brain 7.1%

– Limb 3.6%

– Face 7.8%

Revencu et al, Human Mutation 29(7),959-965, 2008

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CM-AVM Extracutaneous features: spinal AVM

• 5 index cases of AVM and AVF

– 3 AVM’s on the lower spine

– 2 AVF’s on the cervico-thoracic spine

– Age of presentation:16 months and 23 years

• Upper spine: headache

• Lower spine: Neurogenic bladder and hemiplegia

– Treatment: embolization, surgery

AJNR Am J Neuroradiol 31:775–79 Apr 2010 www.ajnr.org

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CM-AVM- Molecuar Genetics

• Autosomal dominant

• Loss of function mutations in RASA1 gene

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Segmental patterning

• S1: upper eyelid, temple

• S2: lower eyelid, cheek

• S3: jaw, beard

• S4: nose and glabella

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PHACES syndrome and ectopia cordis.

• Ectopia cordis

• Parotid Hemangioma

• Supraumbilical raphe

• Aberrant communication between the left common carotid and subclavian arteries

J.C. Lopez-Gutierrez / Interactive CardioVascular and Thoracic Surgery 12 (2011) 642–644

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Ventral midline blanching

• 9 infants with segmental IH and areas of midline ventral blanching

– 5 ventral wall defects

– 6 cardiac anomalies

– 6 intracranial anomalies

• 5 definite PHACE

• 3 possible PHACE Feigenbaum DF, Sybert VP, Vanderhooft SL, Siegel D, Drolet BA, Frieden IJ, Mathes EF. Pediatr Dermatol. 2015 Mar-Apr;32(2):180-7. doi: 10.1111/pde.12462.

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Supraumbilical raphe

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Variations of PHACE syndrome

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Consensus statement on PHACE syndrome diagnostic criteria

• Multidisciplinary group met in Houston, Texas at the PHACE research conference in 2008

• Definite PHACE:

– Segmental hemangioma or hemangioma > 5 cm on the face or scalp PLUS 1 major criterion OR 2 minor criteria

Metry D, Heyer G, Hess C, et al. Consensus Statement on Diagnostic Criteria for PHACE Syndrome. Pediatrics 2009;124:1447-56.

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“PHACE without face”

Cardiac

Right-sided aortic arch

Narrowing of distal transverse aortic arch

Tetralogy of Fallot

Arteriopathy

Aberrant left subclavian artery/ vascular ring

Tortuosity of right internal carotid and basilar arteries

Sternal scar Pediatric Dermatology Vol. 28 No. 3 235–241, 2011

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LUMBAR syndrome

• Lower body hemangioma/ cutaneous defects

• Urogenital anomalies/ Ulceration

• Myelopathy

• Bony deformities

• Anorectal /Arterial anomalies

• Renal anomalies

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PeDRA gives me a platform for collaborating with investigators on

pediatric dermatology research.

Helping Children with Skin Diseases through Collaborative Research

www.pedraresearch.org