1- Community (Screening)

Question 1

healthy child programme: newborn screening timeline

Answer 1

Question 2

types of screening in the healthy child programme

Answer 2

• newborn physical examination
• newborn Blood splot
• newborn hearing screen
• infant physical examination

Question 3

when is the newborn physical examination done

Answer 3

by 72 hours

Question 4

when is the newborn blood spot done

Answer 4

day 5

Question 5

when is the newborn blood spot done

Answer 5

day 5

Question 6

when is the newborn hearing screen done

Answer 6

from 0 to 5 weeks

Question 7

when is the infant examination done

Answer 7

6-8 weeks

Question 8

why do newborn infant screening

Answer 8

• To identify babies with rare, but serious conditions
• Aims to achieve early detection, treatment and referral of babies thought to be affected by these conditions

Question 9

who do the newborn examination

Answer 9

• Community team
• Or inpatient team

Question 10

aim of newborn and infant physical examination

Answer 10

• Screen for congenital abnormalities.
• Refer where appropriate.
• Reassure parents.

Question 11

what is examined in the newborn physical examination

Answer 11

• Eyes
• Heart
• Hips
• Testes

Question 12

examination of eyes: risk factors for problems

Answer 12

• Family history of congenital or hereditary cataracts (1st degree).
• Maternal exposure to viruses (rubella, CMV) in pregnancy.
• Prematurity.
• Trisomy 21.

Question 13

examination of eyes: newborn examination

Answer 13

• Ability to fully open eyelids.
• Both eyes same size.
• Roundness and symmetry of pupils.

Presence of red reflex.
* Absence - ? Cataracts
* White - ? Retinoblastoma

Question 14

examination of eyes: 6-8 week examination

Answer 14

• Smiles as visual response.
• Ability to fix steadily (without nystagmus)
• Ability to fix and follow. (large bright object)
• Alignment of eyes.
  (can be variable, consistent abnormal)

Question 15

examination of the heart: risk factors for problems

Answer 15

• Family history of congenital heart disease (1st degree).
• Cardiac anomaly suspected from antenatal scan.
• Trisomies.
• Maternal exposure to viruses e.g. rubella in first trimester.
• Maternal conditions e.g. Type 1 diabetes, epilepsy, SLE.
• Teratogenic drugs during pregnancy e.g. anti-epileptics.
• Maternal drug or alcohol abuse.

Question 16

examination of the heart: observation

Answer 16

• General tone.
• Central and peripheral colour.
• Chest inspection: size and shape; symmetry of movement.
• Use of diaphragm and abdominal muscles.
• Signs of respiratory distress: respiratory rate, recession/grunting.

Question 17

examination of the heart: palpation

Answer 17

• Assess perfusion through capillary refill time.
• Femoral and brachial pulses for strength, rhythm and volume.
• Position of cardiac apex (dextrocardia); any abnormalities (thrill).
• Abdomen to assess liver size (enlarged in congestive heart failure).

Question 18

examination of the heart: auscultation and murmurs

Answer 18

• Significant murmur
  o usually loud.
  o heard over a wide area.
  o harsh rather than soft quality.
  o associated with other abnormal findings.
• Benign murmur
  o Sensitive (changes with child’s position)
  o Short duration (not holosystolic)
  o Single (no associated clicks or gallops)
  o Small (murmur limited to a small area and non-radiating)
  o Soft (low amplitude)
  o Sweet (not harsh sounding)
  o Systolic (occurs during and is limited to systole)

Question 19

examination of the heart: signs which suggest major congenital heart anomaly

Answer 19

• Tachypnoea at rest (normal newborn RR 40-60 breaths/min).
• Apnoea lasting >20 seconds or associated colour change.
• Recession and nasal flaring.
• Central cyanosis.
• Visible pulsation over precordium, heaves, thrills.
• Absent or weak femoral pulses.
• Presence of cardiac murmur or extra heart sounds.

side note
* Many babies will have a murmur at birth without a heart defect.
* BUT, murmurs can be absent with a significant heart defect.

Question 20

examination of the hips: risk factors for problems

Answer 20

• Family history of hip problems (1st degree).
• Breech presentation at or after 36 weeks gestation.

Question 21

examination of the hips: examination

Answer 21

• Differences in leg length.
• Knees at different levels when hips and knees are bilaterally flexed.
• Buttock/posterior thigh skin folds asymmetry on ventral suspension.
• Difficulty in adducting the hip to 90 degrees.

Question 22

examination of the hips: manipulation

Answer 22

Palpable ‘clunk’ when undertaking Barlow and Ortolani manouvres.

Question 23

examiantion of the testes: risk factors for problems

Answer 23

• Family history of cryptorchidism (1st degree).
• Low birth weight.
• Small for gestational age or preterm delivery.

Question 24

examiantion of the testes: examination

Answer 24

• Observe scrotum for symmetry, size and colour.
• Palpate scrotal sac to locate testes; if none check inguinal canal.

Question 25

Associations of cryptorchidism:

Answer 25

• Significant increase in the risk of testicular cancer.
• Reduced fertility when compared to normally descended testes.
• Associated other urogenital problems: hypospadias, testicular torsion.

Question 26

why is heelprick testing done on days 5-8

Answer 26

before this too much of the mothers blood)

Question 27

heelprick screening background

Answer 27

10 illnesses

• Congenital hypothyroidism
• Cystic Fibrosis
• Phenylketonuria (PKU)
• Medium chain acyl XCoA Dehydrogenase deficiency
• Maple syrup urine disease
• Isovaleric acidaemia
• Sickle cell disease
• Glutaric aciduria Type 1
• Homocystinuria
• Severe combined immune deficiency (SCID)- newly added

Question 28

heelprick screening important principles

Answer 28

• Doesn’t mean child definitely has disease
• Emphasise early treatment is the goal

Question 29

inborn errors of emtabolism screened for in heelprick

Answer 29

• Start treatment for PKU and MCADD within 21 days

Question 30

heelprick procedure

Answer 30

• dont use vaseline
• take from lateral side

Question 31

congenital hypothyroidism: background

Answer 31

• One of most common preventable causes of intellectual impairment.
• Inverse relationship between age of treatment initiation and IQ.

Question 32

aetiology behind congenital hypothyroidism

Answer 32

Primary- defect in thyroid
- Thyroid dysgenesis (absent, hypoplastic or ectopic)
- Dyshormonogenesis

Secondary- hypothalamic-pituitary dysfunction

Question 33

congenital hypothyroidism presentation

Answer 33

Few or no clinical manifestations of hypothyroidism
* Due to maternal thyroxine which crosses the placenta
* Many infants have some, although inadequate functioning thyroid tissue

Manifestations at birth
* Birth length and weight within normal range
* Weight often at relatively higher centile due to myxoedema
* Delayed calcification in epiphyses

Question 34

CF background

Answer 34

• Most common life-shortening autosomal recessive condition.
• Occurs more commonly in Caucasians (1 in 2500) but increasingly recognised in South and East Asia, Africa and Latin America.
• Median predicted survival is 39 years.

Question 35

screening test for CF

Answer 35

Immunoreactive tryspin (IRT)

• Trypsinogen normally produced in pancreas and carried to small intestine where it changes from inactive ‘proenzyme’ to active ‘enzyme’ trypsin.
• Blocked pancreatic ducts in CF impede passage of trypsinogen into gut and result in build up in the blood. Can be detected and measured as IRT levels increase.
• Best screening test for CF, but several other causes for raised IRT.

Question 36

if IRT screen positive

Answer 36

Sweat test and genotyping

Sweat test
- Sweat chloride elevated in CF (60-125 mmol/L); normal value 20-60 mmol/L.
- Sweating stimulated by pilocarpine iontophoresis.
- Requires adequate volume of sweat (>100 mg)
Genotyping
- CF transmembrane conductance regulator (CFTR) gene

Question 37

presentation of CF

Answer 37

Question 38

newborn hearing screen

Answer 38

4-5 weeks
- automated otacoustic emissions testing
- if baby fails this then you repeat the test
- if they fail again -> auditory brainstem response

Question 39

automated otoacoustic emissions (AOAE)

Answer 39

A small soft-tipped earpiece is placed in your baby’s ear and gentle clicking sounds are played. It’s not always possible to get clear responses from the 1st test.
- detects normal sound vibrations from outer hair cells in the cochlea