Handbook of Genetic Counseling/Noonan Syndrome

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• We will be discussing if we think there is a diagnosis that can be made at this time
• If a diagnosis is made we will explain the inheritance and information we know about the cause

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• Common autosomal dominant, single gene
• Mistakenly called male Turner syndrome due to similar characteristics
• Occurs in both males and females equally

• Short stature
• Congenital heart defects
• Broad or webbed neck
• Unusual chest shape (low set nipples, superior pectus carinatum, inferior pectus excavatum)
• Developmental delay
• Cryptorchidism
• Characteristic physical appearance changes over time

• Low set posteriorly rotated ears with thick helix (90%)
• Vivid blue or blue-green eyes (lighter than expected for background)
• thickened or ptotic eyelids
• hypertelorism

(age features are most striking)

• tall forehead
• hypertelorism with downslant palpebral fissures (95%)
• prominent eyes
• Nose has depressed root, wide base, bulbous tip
• Deeply grooved philtrum
• High wide peaks to vermillion border of upper lip
• Excess nuchal skin and low posterior hairline

• Facial appearance lacks expression (resembles individual with myopathy)

• Facial shape inverted triangle, wide forehead tapered chin
• Pinched nasal root and thin bridge
• Neck lengthens accentuates skin webbing or trapezius muscle
• Eyes less prominent
• Curly or wooly hair in older child

• Nasolabial folds prominent
• Skin appears transparent and wrinkled
  • Genetics of Noonan syndrome
    • missense mutations in gene PTPN11 at 12q24.1 identified in 50% of patients
    • gene identified in 2001 (normal gene encodes protein-tyrosine phosphatase, non-receptor type 11 seems to be essential in several intracellular signal transduction pathways controlling diverse developmental processes
    • absence of this mutation in some families suggests heterogeneity
    • AD single gene
    • 50% chance to pass on if affected
    • if parents not affected chance is low <1% (gene clinics)
    • direct transmission reported 30-75% of time rest are de novo
    • predominantly mothers not fathers transmit gene (3:1 ratio) (likely due to cryptorchidism and reduced fertility in males)

• 1/1000-1/2,500

• Testing for PTPN11 mutations available on research basis
• Diagnosis based on clinical findings though
• High-resolution ultrasound only prenatal test available

• Turner syndrome in females should be ruled out through karyotype
• Trisomy 8p, trisomy 22 mosaicism, sex chromosome rearrangement, in utero exposure to alcohol or primidone
• Williams, Aarskog, Baraitser-Winter, Costello syndromes share some features
• Multiple lentigines/LEOPARD syndrome can also have pulmonary valve dysplasia, cardiomyopathy, short stature, hypertelorism, pectus deformity, hearing loss, developmental delay
• Watson syndrome shares pulmonary valve stenosis, short stature, mild intellectual handicap, café-au-lait patches
• Cardio-facio-cutaneous syndrome lot of overlap and debate about whether same condition, but MR more severe, skin findings hyperkeratosis, ichthyosis, absent eyebrows, sparse hair, gastrointestinal problems more severe, eyes rarely characteristically light blue/ blue-green

• Hypothesized to be consequences of lymphatic obstruction

• B.W. usually normal
• 15% have poor suck, 38% poor suck and vomiting, 24% require tube feeding 2 weeks or more
• length at birth normal usually then follows 3% ile
• final height lower end of normal in adults
• some endocrinologists choose to treat with growth hormone even if deficiency not seen

• Delayed milestones
• Mean age sitting 10 mth, walking 21 mth, two-word sentence 31 mth
• 10-15 % require special ed
• IQ usually within normal range, but mild MR seen in 1/3
• Verbal lower than nonverbal performance
• Usually good peer, social interactions and self-esteem, but one study suggests that less socially competent and more behavior problems than sibs (not clinically significant)

• May cause delayed speech
• Reported in >1/3 usually secondary to ottitis media
• Sensorineural loss in 3%

• Potential bias in frequency due to requirement for diagnosis by many (50-80%)
• Stenotic or dysplastic pulmonary valve most common (20-50%)
• 7% of all children with pulmonary stenosis have Noonan
• hypertrophic cardiomyopathy (20-30%) found at birth, infancy or childhood
• ASD (10-20%)
• VSD (5-15%)
• Coarctation of aorta (9%)
• Others
• ECG abnormality found in 87-90%

• Strabismus (48-63%)
• Refractive errors (60-70%)
• Amblyopia (33%)
• Nystagmus (9%)
• Other problems common

• 1/3 have coagulation problems
• 2/3 give history of abnormal bleeding or mild-severe bruising
• hepatosplenomegaly occurs reason unknown(clinically evident 25% ultrasound 51%)
• should avoid aspirin

• Renal abnormalities (generally mild 11%)
• Cryptorchidism in 60-80% of males may cause deficient spermatogenesis
• Fertility is rule in females

• Follicular keratosis
• Scalp hair curly, thick and wooly, or sparse with easy breakage
• Café-au-lait spots and lentigines more frequent than general population

• Physical and neuro exam
• Plot growth on NS charts
• Cardiology eval
• Ophthalmology
• Hearing
• Coagulation screen
• Renal ultrasound
• Clinical and x-ray of spine and rib cage
• Develop eval
• Genetics consult

• Diagnosis may not be certain
• Difficulty and stress of having child with health concerns or learning issues
• Guilt if passed on the gene

• The Noonan Syndrome Support Group

PO box 145

Upperco, MD 21155

Phone: 410-374-5345

Email: info@noonansyndrome.org

Website:www.noonansyndrome.org

• MAGIC Foundation for Children's Growth

1327 North Harlem Ave

Oak Park, IL 60302

Phone: 708-383-0899

Email: mary@magicfoundation.org

www.magicfoundation.org

• Management of Genetic Syndromes, Edited by Suzanne b. Cassidy and Judith e. Allanson. 2001. Wiley-Liss Inc. Chapter 15 written by Judith E. Allanson.
• Gene Clinics: Noonan Syndrome

The information in this outline was last updated in 2002.