Genetic Diseases & Syndromes

Question 1

Down syndrome

Answer 1

• Most common chromosomal abnormality in live births
• Increased incidence w/ advancing maternal age
• Age 35 1:400
• Age 45 1:35

Question 2

Down syndrome prenatal testing

Answer 2

• Quad screen

- Nuchal translucency

Question 3

Cause of Down syndrome

Answer 3

• Gamete has 2 copies of chromosome 21
• Trisomy 21 is cause of 95%
• Roberstonian translocation = 4%

Question 4

Down syndrome prevalance

Answer 4

1:500 pregnancies

Question 5

Down syndrome characteristics

Answer 5

• Intellectual disability
• Characteristic facial appearance
• 40% cardiac defects
• 75% hearing loss
• > 50% visual problems
• 7% have GI defects
• Increased social skills
• 1/2 develop Alzheimer disease

Question 6

Edwards Syndrome

Answer 6

• Trisomy 18
• 2nd most common autosomal trisomy
• IUGR
• Many die before birth or in first month
• Increased risk w/ advanced maternal age

Question 7

Edwards syndrome characteristics

Answer 7

• Kidney, heart, GI defects
• Developmental delay
• Club foot (Rocker bottom feet)
• Low set ears, small jaw

Question 8

Edwards syndrome prevalence

Answer 8

1: 5000 live born infants
- Highly lethal in-utero (85% lost btwn 10 wks gestation & term)
- 50% die in 1st week of life
- 2% have 1 year survival

Question 9

Patau syndrome

Answer 9

• Trisomy 13

- Increased risk w/ advanced maternal age

Question 10

Patau syndrome prevalence

Answer 10

1: 16000 live births

- Many die within 1st days or weeks of life

Question 11

Patau syndrome characteristics

Answer 11

• Severe intellectual disability
• Cleft lip or palate
• Seizures
• Small jaw
• Polydactyly
• Heart, brain/spinal defects

Question 12

Patau syndrome etiology

Answer 12

• Most cases = 3 copies of chromosome 13

- Some due to Robertsonian translocation involving chromosome 13 & 14

Question 13

Cri-du-chat syndrome

Answer 13

• Deletion of part of short arm of chromosome 5

- Partial monosomy (only a portion of a chromosome has 1 copy instead of 2)

Question 14

Cri-du-chat etiology

Answer 14

• Most cases = spontaneously

Question 15

Cri-du-chat characteristics

Answer 15

• Cat like cry due to abnormal larynx
• Intellectual disability
• Wide set eyes, low ears

Question 16

Cri-du-chat prevalence & how is it detected?

Answer 16

1: 50,000 births

- Detected in utero w/ CVS

Question 17

Klinefelter’s syndrome

Answer 17

• Extra X chromosome, 47XXY
• Occurs during gametogenesis
• Accounts for 1st trimester losses
• Most common sex chromosome aneuploidy in males

Question 18

Klinefelter’s characteristics

Answer 18

• Affects male physical & cognitive development
• Physical traits become more apparent after puberty
• Hypogonadism, infertility
• Gynecomastia, reduced hair

Question 19

Turner syndrome

Answer 19

• 45X
• Affects development in females
• Monosomy

Question 20

Turner syndrome characteristics

Answer 20

• Gonadal dysgenesis (non-functional ovaries)
• Short stature
• Broad chest
• Webbed neck
• Amenorrhea
• Infertility
• Cardiovascular defects

Question 21

Huntington’s disease

Answer 21

• Neurodegenerative disease (progressive brain disorder)

- Adult onset: latent for 3-5 decades, then manifests as progressive neuronal dysfunction

Question 22

Huntington’s disease characteristics

Answer 22

• Uncontrolled movements
• Emotional problems
• Loss of thinking ability
• Changes in personality
• Involuntary jerking movements: chorea

Question 23

Early signs of Huntington’s

Answer 23

• Depression
• Irritability
• Poor coordination
• Trouble learning

Question 24

Huntington’s etiology

Answer 24

• HD gene on chromosome 4 that encodes for huntington
• Autosomal dominant
• Average time from sx onset to death = 15 yrs

Question 25

Alzheimers syndrome

Answer 25

• Neurodegenerative disease
• Most common form of dementia in elderly
• Death usually occurs within 10 yrs of dx

Question 26

Causes of dementia

Answer 26

• 65% Alzheimers

- 35% vascular

Question 27

Alzheimers population

Answer 27

Begins after age 60 (risk increases w/ age)

Question 28

Alzheimers pathophysiology

Answer 28

• Loss of cholinergic neurons in brain
• Formation of plaques/tangles
• Atrophy of brain
• Resultant effect - blocked communication

Question 29

Alzheimers mode of inheritance

Answer 29

Several gene mutations cause predisposition

- 2 forms of genes have been identified: familial (early onset); sporadic (late onset)

Question 30

Alzheimers clinical manifestations

Answer 30

• Progressive mental deterioration (memory loss, confusion, disorientation)

Question 31

Familial Alzheimers

Answer 31

• Many members of multiple generations affected
• Sx start before age 65
• Mutations on chromosomes 1, 14, or 21 (forms “sticky” protein that forms clumps in brain)
• Rare, <5%
• Autosomal dominant

Question 32

Sporadic Alzheimers

Answer 32

• Develops after 65
• Accounts for most cases of AD
• One gene increases risk: Chromosome 19 apolipoprotein E (APOE)

Question 33

Definitive dx of sporadic Alzheimers

Answer 33

Autopsy- plaques, tangles

Question 34

Risk factors of breast/ovarian cancer

Answer 34

• Gender
• Age
• Family hx

Question 35

Mode of inheritance of breast/ovarian cancer

Answer 35

Up to 10% are caused by predisposing genetic factors

Question 36

Clinical manifestations of breast/ovarian cancer

Answer 36

• Early age of breast cancer onset (<50)
• Family hx of both breast and ovarian cancer
• Increased bilateral cancers
• Increased development of both cancers in the same person
• Increased incidence of prostate cancer in family
• Male breast cancer

Question 37

2 major cancer susceptibility genes

Answer 37

BRCA1, BRCA2

- Tumor suppressor genes

Question 38

BRCA1

Answer 38

• On chromosome 17

- Autosomal dominant

Question 39

BRCA2

Answer 39

• On chromosome 13

- Autosomal dominant

Question 40

Genetic testing

Answer 40

• Test individual who is affected first

Question 41

Colorectal cancer

Answer 41

• May occur sporadically (most) or familial

- Results from interaction of both genetic and environmental factors (diet, lack of exercise, smoking, obesity)

Question 42

What is considered a positive family hx?

Answer 42

1 of more people in family w/ colorectal cancer or premalignant polyps
- May be due to: chance, shared exposure to a carcinogen or diet/lifestyle factors, combination of gene mutations and environmental risk factors)

Question 43

Familial adenomatous polyposis (FAP)

Answer 43

• < 1% of colorectal cancers

- Autosomal dominant (50% chance of passing to offspring)

Question 44

FAP genetic mutation

Answer 44

Mutation in APC gene

• Tumor suppressor on chromosome 5
• 100s/1000s of polyps developing in adolescents
• Cancer develops in 20s
• Risk of cancer = 100% (before 50yo)
• Polyp –> cancer = 10+ years

Question 45

Once FAP is dx, what is recommended?

Answer 45

Total colectomy before age 20

Question 46

Hereditary Nonpolyposis Colorectal Cancer (HNPCC)

Answer 46

• aka. Lynch Syndrome
• 2-3% of colorectal cancers
• Autosomal dominant
• More rapid transition from adenoma to cancer than FAP
• Cancer occurs in 30s & 40s

Question 47

HNPCC genetic mutation

Answer 47

In one of many genes that code for DNA repair

Question 48

Nonpolyposis refers to what?

Answer 48

Colorectal cancer that can occur when a small # or no polyps are present

• 50% chance of cancer in women
• 70% in men
• Associated w/ other cancers

Question 49

If genetic testing reveals HNPCC

Answer 49

• Regular colonoscopy starting at age 25 in relatives (or 5 yrs younger than age of dx of family member)
• Upper endoscopy every 2 yrs to screen for gastric cancer
• Screening for endometrial & ovarian cancer in women 25-35

Question 50

Chronic myelogenous leukemia

Answer 50

• Myloproliferative disorder
• Translocation btwn chromosome 9 & 22
• Philadelphia chromosome (22)

Question 51

Chronic myelogeneous leukemia population

Answer 51

• More common in men

- Median age = 55

Question 52

Philadelphia chromosome (22)

Answer 52

Produces a protein that codes for an enzyme that causes too many stem cells to develop into WBCs

Question 53

Pathophysiology of CML

Answer 53

• Increased production of abnormal/nonfunctional WBCs

- WBCs take up bone marrow space

Question 54

Clinical presentation of CML

Answer 54

• Insidious onset
• Slow progression over months to years
• Anemia, bleeding
• Fever, night sweats, fatigue

Question 55

CML Dx

Answer 55

Bone marrow aspiration for karyotype

Question 56

Hemophilia

Answer 56

• Bleeding disorder caused by mutations in genes that code for coagulation
• Mutation on F8 & F9 genes on X chromosome
• X-linked recessive
• Males are most affected

Question 57

Mutation on F8

Answer 57

• Causes factor VIII deficiency
• Results in hemophilia A (classic form)
• More common

Question 58

Mutation on F9

Answer 58

• Causes factor IX deficiency

- Results in hemophilia B (Christmas Disease)

Question 59

Clinical manifestations of hemophilia

Answer 59

• *Hemarthrosis
• Bleeding into muscles/tissues
• Prolonged bleeding/oozing after injury or surgery

Question 60

Sickle cell disease

Answer 60

• Atypical hemoglobin molecules (hemoglobin S)
• Distorts RBC into crescent shape
• Abnormally shaped RBCs break down prematurely
• Mutation on HBB gene

Question 61

Sickle cell clinical manifestations

Answer 61

• Anemia
• Infections
• Episodic pain
• SOB
• Fatigue
• Delayed growth

Question 62

Sickle cell inheritance

Answer 62

Autosomal recessive

Question 63

Sickle cell population

Answer 63

Greece, Africa, Turkey, Italy, Arabian Peninsula, India, South America, Central America, Caribbean

Question 64

Cystic fibrosis pattern of inheritance

Answer 64

Autosomal recessive

- 2 copies of mutated gene are needed for disease to be expressed

Question 65

Cystic fibrosis genetic mutation

Answer 65

Mutation in the CFTR gene

• CFTR codes for a protein that regulates chloride channels
• When mutated, a defective protein is made –> disruption of chloride & H2O transport

Question 66

Clinical manifestations of cystic fibrosis

Answer 66

• Thick, sticky mucous obstructing airways in lungs & ducts in pancreas
• Can affect pancreas, intestines, exocrine glands, hepatobiliary system

Question 67

Cystic fibrosis sx

Answer 67

• Difficulty breathing, infections in lungs
• Problems w/ nutrient digestion
• Buildup of mucous prevents pancreatic enzymes from reaching intestine
• Failure to thrive, poor growth rate
• *Meconium ileus: newborn intestinal obstruction due to thick fecal waste products

Question 68

What is the most common cause of morbidity associated with CF?

Answer 68

Pulmonary disease

• Pulmonary system can’t defend against pathogens –> sinusitis & bronchitis
• S. aureus, P. aeruginosa, Aspergillus
• Nasal polyps, nosebleeds, chronic sinus infections

Question 69

Population & incidence of CF

Answer 69

• White population in US
• 1 in 3500 white newborns
• Carrier incidence: 1 in 25

Question 70

CF Dx

Answer 70

• Most dx by age 1
• Sweat chloride test:
  Chloride channel doesn’t allow chloride to be reabsorbed
• [chloride] in sweat is elevated

Question 71

Marfan syndrome mode of inheritance

Answer 71

• Autosomal dominant
• An inherited mutation or a new mutation of fibrillin-1 gene (FBN1)
• Causes defects in CT affecting:
  Bones
  Ligaments
  Muscles
  Blood vessels
  Heart valves

Question 72

Marfan clinical manifestations

Answer 72

Tall stature
Long, thin arms & legs
Arm span wider than body height
Long, narrow face
High arched palate
Overcrowded teeth
Scoliosis
Hyperflexible joints
Chest deformities

Question 73

Marfan primary features

Answer 73

• Dislocated lens of the eye – vision problems

* Aortic aneurysm/dissection

Question 74

Major cause of morbidity/mortality in Marfan syndrome?

Answer 74

Heart defects

• Mitral valve prolapse, aortic valve regurg
• SOB, fatigue, palpitations

Question 75

Marfan syndrome recommendations

Answer 75

Avoid contact sports, caffeine, & decongestants due to increased stress placed on CV system

Question 76

Neurofibromatosis Type 1

Answer 76

• aka. von Recklinghausen
• Most common type
• Subcutaneous tumors

Question 77

Neruofibromatosis Type 1 pattern of inheritance

Answer 77

• Autosomal dominant
• Mutation on NF1 gene on chromosome 17
  (tumor suppressor gene)
• Results in:
  Growth of neurofibromas
  Changes in skin pigmentation

Question 78

NF - Type 1 manifestations

Answer 78

• Hyperpigmented skin lesions (café-au-lait spots)
• Lisch nodules in iris
• Freckles in axillae & groin

Question 79

NF Type 1 dx features

Answer 79

• 1.5 cm or larger café-au-lait spot post puberty OR 6 or more café-au-lait spots 0.5 cm or larger before puberty
• 2 or more neurofibromas
• Axillary or inguinal freckling (Crowe sign*)
• Optic glioma
• 2 or more Lisch nodules
• 1st degree relative w/ NF1

Question 80

Pathophysiology of PKD

Answer 80

• Clusters of fluid filled sacs develop in kidneys
• Affects ability to filter blood
• Kidneys become enlarged & can fail

Question 81

PKD clinical manifestations

Answer 81

• HTN
• Back pain
• Hematuria
• UTIs, kidney stones

Question 82

PKD other associations

Answer 82

• Liver cysts
• Heart valve abnormalities
• Increased risk of aortic & brain aneurysms

Question 83

What are the 2 forms of PKD?

Answer 83

Autosomal dominant: sx start in adulthood

• 1 in 1000
• PKD1 & PKD2 genes
• Usually inherited (90%)

Autosomal recessive: rare, lethal early in life

• 1 in 30,000
• PKHD1 gene

Question 84

What % of newborns have a congenital defect?

Answer 84

10%

- Unknown etiology*

Question 85

Teratology

Answer 85

Study of abnormal development

• Teratogens: anything capable of disrupting embryonic or fetal development & producing malformations
• Critical period for teratogenic effects is 3-16 weeks gestation
• Timing of exposure determines which systems are affected

Question 86

Newborn screening

Answer 86

• Biochemical analysis
• Determines whether certain proteins are present or absent
• Typically autosomal recessive conditions
• “Inborn errors of metabolism”: Inherited defect in 1 or more enzymes

Question 87

When is the 1st & 2nd test performed in newborn screening?

Answer 87

1st test: 24-36 hrs (heal stick)

2nd test: @ 1st office visit, 5-10 days