Endo & Growth

Question 1

what is the MOST common cause of precocious puberty in girls?

Answer 1

Idiopathic

presents just like normal puberty

Question 2

what is the staging for puberty?

Answer 2

Tanner staging

Question 3

What are the outcomes of premature therlache?

Answer 3

Persists

Regresses

Does NOT progress to precocious puberty (eg secondary sexual characteristics)

Question 4

what is the best immediate diagnostic measure to test for CAH?

Answer 4

17aOH progesterone levels (though this condition itself is a defficiency of 21 alpha hydroxylase)

random level AND 72hour levels

Question 5

Why is CAH called CAH?

Answer 5

deficiency of end hormones leads to overstimulation of adrenal gland by ACTH = hyperplasia of the adrenal glands! (+ excess androgens)

Question 6

what is CAH?

Answer 6

Congenital adrenal hyperplasia (CAH) is a group of autosomal recessive disorders characterized by impaired cortisol synthesis.

It results from the deficiency of one of the five enzymes required for the synthesis of cortisol in the adrenal cortex.

Most of these disorders involve excessive or deficient production of such hormones as glucocorticoids, mineralocorticoids, or sex steroids, and can alter development of primary or secondary sex characteristics in some affected infants, children or adults.

It is one of the most common autosomal recessive disorders in humans

Question 7

what is the most common cause of a disorder of sexual development?

Answer 7

CAH

Question 8

which are the most deficient hormones in CAH?

Answer 8

More than 90% show a deficiency of 21-hydroxylase – needed for cortisol

• 80% are unable to produce aldosterone – leading to decreased Na and increased K (hyperkalaemia)
• Cortisol deficiency stimulates pituitary to increase ACTH → overproduction of adrenal ANDROGENS

Question 9

How does CAH present?

Answer 9

Classic forms:

1. Simple-virilising 25%: Virilization (masculinisation) of external genitalia in female infants → clitoromegaly and variable fusion of labia ( +ambiguous gentialia)
   • In males → enlarged penis, pigmented scrotum

-> if not identified and treated they will grow rapidly and have more virilisation:
present tall, muscular, pubic hair, acne, precocious puberty
• Boys - enlarged penis, small testes
• Girls - abnormal or absent periods, facial hair

2• Salt-wasting: in 75% of cases of severe enzyme deficiency, insufficient aldosterone production can lead to salt wasting, failure to thrive, and potentially fatal hypovolemia and shock.
The missed diagnosis of salt-loss CAH is related to the increased risk of early neonatal morbidity and death.

Non-classic:
1. The non-classic form is characterized by mild subclinical impairment of cortisol synthesis; serum cortisol concentration is usually normal.

presentation : late in childhood, accelerated growth, premature sexual maturation

Question 10

what causes the hypoglycaemia in CAH?

Answer 10

cortisol deficiency

Question 11

what ivx do we conduct for CAH and what are the findings?

Answer 11

In classic 21-hydroxylase deficiency, laboratory studies will show:

Increased 17α-hydroxyprogesterone in blood (precursor for deoxycortisol so cortisol)
- random and 72 hour levels

• ↑ testosterone, progesterone, adrenal androgen precursors

U&Es -> • In salt losers → low Na, high K, metabolic acidosis, (as aldosterone is low),

Blood glucose - > hypoglycaemia

If virilisation:
Karyotype with fluorescent in situ hybridization (FISH) for sex-determining region of the Y chromosome

Question 12

how does a Salt losing adrenal crisis present?

Answer 12

→ aged 1-3w MALE
-> salt losers

→ vomiting, weight loss, floppiness, circulatory collapse ± arrhythmias, dehydration and hypoglycemia

Question 13

what is the mx AND follow up of CAH?

Answer 13

Mx:
• MDT involving endocrinologists, urologists and paeds
• Female
o Corrective surgery to external genitalia if required
- there is a debate surrounding gender assignment

• Lifelong glucocorticoids (hydrocortisone) to suppress ACTH and testosterone
• Mineralocorticoids (fludrocortisone) if there is salt loss

Regular blood tests → monitoring of growth, skeletal maturity, plasma androgens, 17α-hydroxyprogesterone to allow adjustment of steroid replacement doses

• Additional hydrocortisone to cover periods of illness or surgery
• Child may have short stature so may benefit from GH replacement
• Males usually have normal fertility but females may have problems conceiving so may need additional help

Question 14

what is the mx of a salt losing crisis?

Answer 14

• Male

o Salt losing adrenal crisis → saline, dextrose, IV hydrocortisone

Question 15

what is the 2nd most common enzyme deficiency in CAH?

what would ivx show?

Answer 15

11β-Hydroxylase CAH (5%)

ivx would show increased 11-Deoxycortisol as it catalyses the conversion of 11-Deoxycortisol→DOC

Question 16

define delayed puberty?

Answer 16

the lack of any pubertal signs by 14 years in boys (m = no testicular development)

and 13 years (f = no breast development) or 15 (no periods).

Question 17

what are the CAUSES OF DELAYED PUBERTY?

Answer 17

1. Constitutional delay – commonest
   short stauture because of a delay in the onset
   of puberty
2. LOW Gonadotrophin secretion = Hypogonadotrophic hypogonadism
   a. Systemic disease – CF, severe asthma, Crohn’s, organ failure, anorexia nervosa, starvation, XS exercise

b. Hypothalamo-pituitary disorders – panhypopituitarism, intercranial tumours, Kallmann syndrome (LHRH deficiency and anosmia), isolated gonadotrophin or GH deficiency
c. Acquired hypothyroidism

3. Failure of end organ with HIGH Gonadotrophin secretion = Hypergonadotrophic hypogonadism

a. Chromosomal abnormalities – Klinefelter’s 47XXY, Turner’s 45 XO
b. Steroid hormone enzyme deficiencies
c. Acquired gonadal damage – post-surgery, chemo, radio, trauma, torsion of testes, AI disease

Question 18

what is the aetiology of Constitutional delay?

Answer 18

Majority simple constitutional delay - late bloomers - not requiring detailed investigation

• More common in males
• Often familial – usually FHx of same in parent of same sex

• Also associated with dieting and XS exercise
• Children are short during childhood, delay in sexual maturation and delayed skeletal maturity
delayed bone age

• Legs are long in comparison to back

Question 19

how do we ivx constitutional delay or delayed puberty?

Answer 19

1. Height and weight of child - plot on growth curve
   
   • Compare to mid-parental heights
2. Assess for features of malnutrition
3. Assess for features of disproportion eg webbed neck, longer legs (kleinfelter)
4. Cranial nerve and neuro exams - identify brain tumours, anosmia - kallmans

Boys → pubertal staging - Tanners (testicular volume), Karyotype (Kleinfelters)
• Girls → Karyotype (Turner’s), thyroid and sex steroid hormone levels

Also:
- Non dominant wrist xray: delayed bone age
- Blood - basal FSH,LH (low in HypoHypo, High in gonad disease)
- LHRH stimulation test
• Use LHRH to stimulate gonadotrophins then measure LH and FSH

TFTs → if hypo
• Also ask for prolactin

Consider MRI brain for structural causes eg tumours

• Look for signs of chronic disease, dysmorphia, plot height and weight, calculate mid-parental height
• Can only diagnose once other causes have been eliminated

Question 20

how do we mx constitutional delay?

Answer 20

• Reassurance as treatment not usually required
• They will eventually reach their target height

Boys:
• Oral oxandrolone can be used (3-6 months) for catch up growth - but not secondary sexual characteristics.
- ONLY give if psychosocial distress present
- Can give testosterone - get 2ndary characteristics

• Females can be treated with oestradiol for same reason
• Consider need for psych input regarding bullying, body image, social etc

Question 21

Pubertal development and progress are best assessed by ______ ?

Answer 21

Tanner staging

Question 22

what are the signs of puberty in BOYS in order?

Answer 22

1. The first sign of puberty in boys is an increase in the size of the testes. enlargement to over 4-mL volume
   measured
2. This is followed by penile and scrotal changes.
3. Growth of axillary + pubic hair and other changes, such as changes of the voice

Rapid height growth is next, occur in mid- to late puberty - (12 mL to 15 mL testicular volume) - 18 months post first sign of puberty

4. Facial hair does not appear until late puberty.

Testicular size is documented as a measurement of the longest axis or by the testicular volume using the Prader orchidometer.

Question 23

what are the signs of puberty in GIRLS in order?

Answer 23

The first demonstrable sign of puberty in girls is breast development (palpable breast disc).

Pubic and axillary hair, acne, and body odour develop as a result of androgens secreted from the adrenal gland. occur almost immediately after breast development

The peak growth spurt occurs in Tanner stage 3 breast development,

and menarche occurs in Tanner stage 4 breast development . Menarche occurs 2.5 years after the
start of puberty and signals that growth is coming
to an end, with only around 5-cm height gain
remaining

Caution must be exercised in examination of breast tissue in obese girls, as simple fat may be mistaken for breast tissue.

Question 24

define puberty

Answer 24

Puberty = interval characterized by the acquisition of secondary sexual characteristics, accelerated linear growth, increase in secretion of sex hormones, maturation of gonads (testes in boys and ovaries in girls), potential for reproduction.

Question 25

how do we treat delayed puberty of organic/permanent cause?

Answer 25

• Girls - Organic cause:

▪ Pubertal induction with oestrogen –
weekly transdermal patch of gradually increasing dose over 6 months to adult dose
- note : do NOT give COCPs instead!

▪ Cyclical progesterone after breakthrough bleeding or adequate oestrogenisation

o If Turners → give GH subcut daily ± oxandrolone
(until 12-14 y/o)
- If the diagnosis is made late, oxandrolone added to promote linear growth.

• Boys – organic cause
o Pubertal induction with testosterone – IM every 6 weeks for 6 months then increase dose and increase frequency until adult dose reached

-> side effects: hyper aggression and hyper sexuality for a few days post dose.

Question 26

define precocious puberty

Answer 26

Premature sexual development is the development of secondary sexual characteristics before 8y in females and 9y in males

• Precocious puberty is when its accompanied by a growth spurt

Question 27

what are the forms of precocious puberty?

Answer 27

Gonadotrophin dependent – central – from premature activation of HPA
o Gonadotrophin independent – pseudo – from autonomous excess sex steroid secretion

Question 28

what is the aetiology of precocious puberty?

red flags?

Answer 28

FEMALES
• Most commonly due to premature onset of normal puberty - Idiopathic

• Abnormal or organic cause when there is dissonance (sequence of pubertal changes is abnormal - if the sequence is normal then should be normal)
• Red flags: Rapid onset, neuro symptoms or signs

MALES
• Most commonly has an organic cause eg abnormal

Question 29

how do we ivx precocious puberty?

Answer 29

Females:
• IX → US of ovaries and uterus
o In premature onset of NORMAL puberty, multicystic ovaries and enlarging uterus will be identified (most common)
• Rule out gonadal tumour, cysts

Male:
• Examination of testes
o Bilateral enlargement → gonadotrophin release – usually intercranial lesion
o Small testes → adrenal cause → tumour or CAH
o Unilateral → gonadal tumour

• MRI for suspected intercranial tumour

• Non-dominant wrist x-ray to assess skeletal age
• Check basal LH/FSH, serum testosterone and oestrogen
• LHRH stimulation test – (suppressed LH/FSH if G-independent)

Gonadotrophin-dependent (↑LH > ↑FSH) Gonadotrophin-independent (↓FSH, ↓LH, Rare)

Question 30

how do we mx precocious puberty?

Answer 30

1. Gonadotrophin dependent disease
   o Give GNRH analogues
   o Only pulsatile exposure triggers pubertal progression, continuous exposure suppresses

o ± growth hormone if required

2. Gonadotrophin independent
   o Identify source of excess sex steroids and give androgen or oestrogen inhibitors

• Increased testosterone or McCune Albright → ketoconazole as inhibitor of steroid synthesis
• CAH → hydrocortisone + GNRH analogue
• Tumours → surgery

Question 31

what is premature Adrenarche/Pubarche?

aetiology?

Ivx?
mx?

main differential?

Answer 31

• Pubic OR Axillary hair before 8y in females and 9y in males
• Along with NO other signs of sexual development
• May be slight increase in growth rate

An adult-type axillary body odor is the other major clinical finding.

Aetiology: weak androgens secreted by adrenals (this is NOT the usual steroids)

• Most commonly due to accentuation of normal maturation of androgen production by adrenal gland
• More common in Asian or Afro-C

• Usually self-limiting

Ivx:
Obtaining a urinary steroid profile,
Blood androgens levels
Bone age

• If more aggressive virilization – consider non-classical congenital adrenal hyperplasia or adrenal tumour (virilising tumour)

main differential - non-classical CAH, virilising tumour

Question 32

what are the recognized patterns of premature

sexual development ?

Answer 32

• precocious puberty
• premature breast development (thelarche)
• premature pubic hair development (pubarche or
adrenarche)
• isolated premature menarche.

Question 33

what are the complications of premature Adrenarche/Pubarche?

Answer 33

Girls who develop premature pubarche are
at an increased risk of developing polycystic ovarian
syndrome in later life.

Question 34

how does premature thelarche present?

ivx and mx?

Answer 34

This usually affects females between 6 months
and 2 years of age.

The breast enlargement may be asymmetrical and fluctuate in size, rarely progressing beyond stage 3 of puberty.

It is differentiated from gonadotrophin-dependent precocious puberty by the absence of axillary and pubic hair and of a significant growth spurt.

It is nonprogressive and self-limiting. Investigations are not usually requiredq

Question 35

what is the aetiology and clinical presentation of Achondroplasia?

Answer 35

• Most common type of skeletal dysplasia
• Auto dom but 80% sporadic mutations
• Caused by mutation in fibroblast growth factor receptor 3 – FGFR3

Clinically:
• Short stature, shortening of limbs
• Large head, frontal bossing, depression of nasal bridge
• Short, broad hands
• Marked lumbar lordosis
• ± hydrocephalus

Question 36

what is the ivx and mx of Achondroplasia?

Answer 36

Not apparent until more than 22w GA so may be missed

• Diagnosis made by clinical features and XR findings;

o Metaphyseal irregularity, flaring in long bones, late-appearing irregular epiphyses

• Full skeletal survey ± confirmatory molecular analysis

identifying disproportionate short stature
• sitting height – base of spine to top of head
• subischial leg length – subtraction of sitting height
from total height

Management:

• Regular follow up to detect complictions;
• Gross motor skill delay, kyphosis, early osteoarthritis, risks from hydrocephalus, obesity, ENT issues
• No evidence of benefit from growth hormones
• Final height varies from 80cm to 150cm

• use Condition specific centile charts

Question 37

what is Prepubertal vaginal bleeding / “premature menarche”?

Aetiology?

Ivx and mx?

Answer 37

When a girl with little or no breast development has vaginal bleeding, this causes great concern for parents and providers.

This condition, sometimes referred to as “premature menarche,” has been well-described in the literature, although its cause is unknown.

Studies show that hormonal levels are prepubertal, and pelvic ultrasonography shows a prepubertal uterus and ovaries.

The bleeding can occur monthly but resolves in a few months, so reassurance and watchful waiting are often the best course. In persistent cases, a foreign body such as toilet paper may be found on pelvic exam.

Question 38

when bone age < constitutional age but
growth velocity is normal
what is the cause?

Answer 38

constitutional delay aka late bloomers

Question 39

when bone age < constitutional age but
growth velocity is ABnormal
what is the cause?

Answer 39

chronic illness
malnutrition
endocrine

Question 40

when bone age = constitutional age but
growth velocity is ABnormal
what is the cause?

Answer 40

genetic

Question 41

person is short
when bone age = constitutional age but
growth velocity is normal
what is the cause?

Answer 41

familial short stature - ALL family members are short

=

be sure to rule out skeletal dysplasia

Question 42

define short stature

Answer 42

Short stature is usually defined as a height below the
second centile (i.e. 2 SDs below the mean).

they usually start below the centiles and remain there.
if they are falling down centiles (reducing height velocity), this is growth failure

Question 43

what is the aetiology of short stature?

Answer 43

1 in 50 children have short stature

- most will be normal, with short parents

Question 44

how do we calculate Height velocity?

Answer 44

Two accurate measurements at least 6
months but preferably a year apart allow calculation
of height velocity in cm/year

• highly dependent on the accuracy of
  the height measurements and so tend not to be used
  outside specialist growth clinics

Question 45

how do we calculate an estimate of a childs adult height?

Answer 45

(mum height + dad height)/2 + 7cm - boy

(mum height + dad height)/2 - 7cm - girl

Question 46

list the causes of short stature

Answer 46

Constitutional delay - most common

Familial short stature:
- growth course follows predicted midparental height

SGA - Small for gestational age and extreme prematurity:
-GH treatment may be indicated if there is insufficient catch-up growth by 4 years of age.

Chromosomal:
Turners & Russell-silver - may present with short stature and minimal symptoms.

Nutritional/long-term illness:
usually short and underweight, i.e. their weight is on a lower centile than their height.
- Iron deficiency
- Coeliac - can present with short stature without GI sx
- Chrons, CKD (due to increased metabolic demand)
- CF (malabsorption), CHD

Psychosocial deprivation: Environmental understimulation / neglect or abuse (may fail to grow despite adequate calories due to emotional neglect)

Endocrine
Hypothyroidism, GH deficiency, IGF-1 deficiency, and
steroid excess -> Cushings

Extreme short stature
abnormalities in a gene called short stature homeobox (SHOX) located on the X chromosome lead to severe short stature with skeletal abnormalities

Question 47

what would show the following on growth curves :
Falling off height centiles.
Weight centile >height centile.
i.e. short and overweight
Markedly delayed bone age.

Answer 47

endocrine causes of SS

Question 48

which thyroid condition is the most common cause of short stature in childhood?

Answer 48

autoimmune thyroiditis
- growth failure, usually with excess weight gain

NOT congenital hypothyroid as that is discovered and treated early.

Question 49

how might short stature due to GH deficiency present?

Answer 49

Visual defects if there is a pituitary tumour, that has resulted in GH deficiency - bitemporal hemianopia

Question 50

how might short stature due to Cushings present?

Answer 50

history of long term health condition eg asthma that they are taking STEROIDS for

cushings in kids is usually caused by steroid excess rather than adrenal/pituitary issue:

alternate the days on steroid therapy
but even low doses may still not stop growth failure

+ excess weight gain

Question 51

How can we treat short stature?

Answer 51

GH deficiency is treated with biosynthetic GH, which
is given by subcutaneous injection, usually daily.

It is expensive and the management of GH deficiency is
undertaken at specialist centres. The best response
is seen in children with the most severe hormone
deficiency.

Other indications include Turner syndrome, Prader–Willi syndrome, CKD, SHOX deficiency, and intrauterine
growth restriction or SGA with failure of catch-up growth

Question 52

define growth restriction?

Answer 52

• Small for gestational age or small for dates – if birthweight <10th centile for GA

Question 53

what are the forms of growth restriction?

aetiology and prognosis?

Answer 53

• Majority are normal, some may be due to IUGR – failure to reach fully genetically determined potential

1. Asymmetrical growth restriction
   • More common, weight or abdo circumference is on lower centile than head

• Occurs when placenta fails to provide adequate nutrition late in pregnancy – brain growth is spared at expense of liver glycogen and skin fat. Head is disproportionally bigger than weight& length eg head is in 50th centile but weight/ length are in 8th and 7th centiles.
• Associated with uteroplacental dysfunction secondary to maternal PET, multiple pregnancy, maternal smoking, idiopathic
• These babies rapidly put on weight after birth

2. Symmetrical growth restriction
   • Head circumference is equally reduced as weight and length so baby has normal proportions.
   • Suggests prolonged period of poor intrauterine growth starting in early pregnancy
   • Usually due to small but normal foetus
   • Could be due to chromosomal disorder or syndrome, congenital infection, maternal drug or alcohol abuse, malnutrition or chronic medical condition
   • These babies more likely to stay small permanently

Question 54

what are the causes of developmental delay?

Answer 54

Prentatal period:
• Chromosomal disorders – Down’s syndrome,
 fragile X (has trinucleotide repeats)
• Cerebral dysgenesis, e.g. microcephaly, hydrocephalus
• TORCH infections
• Metabolic causes – hypothyroidism
• Teratogens - alcohol and drugs
• Cerebral palsy

Perinatal period:

• Metabolic; neonatal hypoglycaemia, kernicterus
• Birth asphyxia; hypoxic brain injury

Postnatal period:
•Anoxic episodes: Epilepsy/seizures, drowning
• Infectious causes - Meningitis, encephalitis
• Malabsorption disorders – coeliac, IBD
• Cerebrovascular - stoke (SCD)
• Autism, ADHD, learning disabilities, eating disorders
• Physical abuse, emotional neglect

Question 55

how would developmental delay present clinically?

Answer 55

• Isolated developmental delay in one domain
• Global delay - numerous causes
• FHx of developmental delay or syndromes
• Dysmorphic disorders IX

Question 56

how do we ivx developmental delay?

Answer 56

• Screening tests for autism or ADHD
• IQ testing
• Infection screen
• Genetic screen
• Metabolic screen

Question 57

how do we manage developmental delay?

Answer 57

• MDT – SALT, OT, PhysioT, family counselling, behavioural intervention, educational assistance
• Manage associated conditions
• Prognosis – usually good if isolated but global delay has high association with syndromes – poor

also see tutorial (one-note)

Question 58

what do the following terms mean:

• delay
• learning difficulty
• disorder

Answer 58

• delay – implies slow acquisition of all skills (global
delay) or of one particular field or area of skill
(specific delay), particularly in relation to
developmental problems in the 0–5-year age
group

• learning difficulty – used in relation to children of
school age and may be cognitive, physical, both,
or relate to specific functional skills

• disorder – maldevelopment of a skill.

Question 59

how can the pattern of abnormal development (global or

specific) can be categorised?

Answer 59

• slow but steady
• plateau effect

• showing regression
– acute regression following acute brain injury
with subsequent slow recovery but not to
normal levels (partial recovery) or slow
regression as with neurodegenerative disorders

Question 60

define global delay

Answer 60

Global developmental delay (also called early developmental impairment) implies delay in acquisition of all
skill fields (gross motor, vision and fine motor, hearing
and speech, language and cognition, social/emotional
and behaviour).

It usually becomes apparent in the first 2 years of life

the older, the more obvious abnormalities become to see

Question 61

what are potential causes of abnormal motor development?

Answer 61

Causes of abnormal motor development include:

• central motor deficit, e.g. cerebral palsy (CP)
CP is the MOST COMMON cause of motor impairment
in children, affecting about 2 per 1000 live births.

• congenital myopathy/primary muscle disease
• spinal cord lesions, e.g. spina bifida
• global developmental delay, as in many
syndromes, or of unidentified cause.

Note:

• children with joint hypermobility may also achieve walking later than average (>18mnths).
• asymmetry of motor skills during the first year of life is always abnormal (as hand dominance is not acquired until 1–2 years of age or later).

Question 62

who should be involved in the ivx and mx of kids with abnormal motor development?

Answer 62

assessment by a neurodevelopmental paediatrician
and physiotherapist.

Ongoing physiotherapy input and
subsequent involvement of an occupational therapist
are also likely to be needed.

Question 63

define cerebral palsy

Answer 63

A permanent disorder of movement
and/or posture and of motor function due to a
non-progressive abnormality in the developing brain.

Question 64

how does Cerebral palsy present?

Answer 64

disturbances of cognition, communication, vision,
perception, sensation, behaviour, seizure disorder
and secondary musculoskeletal problem

symptoms may present at different times

•abnormal limb and/or trunk posture and tone in
infancy with delayed motor milestones ;
this may be accompanied by slowing of head
growth
• feeding difficulties, with oromotor incoordination,
slow feeding, gagging and vomiting
• abnormal gait once walking is achieved
• asymmetric hand function before 12 months
of age.

Primitive reflexes may persist and become obligatory

Question 65

what is the aetiology of CP?

Answer 65

80% Antenatal group of causes - cerebrovascular haemorrhage or ischaemia , or maldevelopment

Some of these problems are linked to gene deletions

10% - Intrapartum causes:
hypoxic-ischaemic injury before or during delivery
- high-risk factors for brain damage = significant prematurity or those with difficulties around the time of birth
Birth asphyxia

10% are postnatal:
meningitis/encephalitis/encephalopathy, head trauma from accidental or
non-accidental injury, symptomatic hypoglycaemia,
hydrocephalus and hyperbilirubinemia

Question 66

what are the types of cerebral palsy?

Answer 66

spastic: bilateral, unilateral, not otherwise specified
(90%)
- upper motor neurone damage (corticospinal tract) pathway
- Increased tone : PREDOMINANT sign!
- dynamic catch, which is the hallmark of spasticity.
-> worse with exercise/movement

• dyskinetic (6%)
- movements are involuntary, uncontrolled, occasionally stereotyped and often more evident with active movement or stress.

• ataxic (4%)
• other.

Bilateral (quadriplegia) – all four limbs are affected,
often severely.
Bilateral (diplegia) – all four limbs, but the legs are
affected to a much greater degree than the arms,
so that hand function may appear to be relatively
normal

Question 67

which condition may present like this on examination:

unilateral involvement of the arm and leg.
The arm is usually affected more
than the leg, with the face spared.

Affected children often present at 4–12 months of age with fisting of the affected hand, a flexed arm, a
pronated forearm, asymmetric reaching, hand
function or toe pointing when lifting the child.

Subsequently, a tiptoe walk (toe–heel gait) on the
affected side may become evident

Answer 67

Spastic cerebral palsy

Affected limbs may initially be flaccid and hypotonic, but tonicity increases eventually

page 63 LISSAUER is good

Question 68

how may diskinetic cerebral palsy present?

Answer 68

May be described as:
• chorea – irregular, sudden and brief non-repetitive
movements
• athetosis – slow writhing movements occurring
more distally such as fanning of the fingers
• dystonia –twsiting appearance

Intellect may be relatively unimpaired.

due to hypoxic-ischaemic encephalopathy at term (the 10%)

Question 69

Bilateral spastic cerebral palsy (diplegia) may present how?

Answer 69

so legs more affected than arms.

Young child – pattern with walking on their toes with
scissoring of the legs.

Older child – crouch gait pattern is typical when the child gets heavier and can’t remain on their toes

Usually no feeding or communication difficulties and good cognition

Question 70

Dyskinetic cerebral palsy may present how?

Answer 70

Typical dystonic pattern with open mouth posture and
internal rotation and extension of the arms.

Mixture of motor patterns including dystonia, athetosis and chorea

Cognition may be preserved but feeding difficulties are common.
Risk of hip deformity and scoliosis.

Many are dependent on others for activities of daily living due to their severe movement difficulties.

Usually GMFCS level 4–5 ie in a wheelchair

Question 71

Unilateral cerebral palsy (hemiplegia) may present how?

Answer 71

Spastic or dystonic tone, one side of body affected (opposite to the side of the brain lesion)
Arm often more affected than leg

May have visual field defect on side of hemiplegia
Risk of learning difficulties and seizures

Question 72

Bilateral spastic cerebral palsy (quadriplegia, 4 limb pattern) may present how?

Answer 72

Both arm and leg involvement – predominantly spastic but dystonia often also present.

Associated with learning difficulty, feeding difficulties,
problems with speech, vision and hearing.

Seizures common. At increased risk of hip subluxation and dislocation and scoliosis.
Usually dependent on others for activities of daily living

Powered mobility a common requirement
Usually GMFCS level 4–5 ie in a wheelchair

Question 73

list causes of speech and language delays and disorders

Answer 73

Delays:
• hearing loss
• global developmental delay
• difficulty in speech production from an
anatomical deficit, e.g. cleft palate, or oromotor
incoordination, e.g. CP
• environmental deprivation/lack of opportunity for
social interaction
• normal variant/familial pattern.

Speech and language disorders include disorders of:
• language comprehension
• language expression – inability or difficulty in
producing speech whilst knowing what is needing
to be said
• stammering (dysfluency), dysarthria or verbal
dyspraxia
• social/communication skills (autistic spectrum
disorder).

Question 74

what are tests of language development?

Answer 74

• the Symbolic Toy test, which assesses very early
language development
• the Reynell test for eexpressive and receptive language

refer to speech and language therapist SALT

Question 75

See psych learning difficulty notes

Answer 75

dyslexia, dyscalculia

Question 76

List the causes of congenital hypothyroidism?

Answer 76

Maldescent of the thyroid and athyrosis (75%)–
the most common cause of sporadic congenital
hypothyroidism. supposed to migrate from a position at the base of the tongue to below the larynx but doesn’t.
partial or complete failure to develop.

• Disorder of thyroid hormone metabolism (10%) – TSH unresponsiveness or defects in thyroglobulin structure, inherited
• Hypothalamic or pituitary dysfunction (5%)– can include tumours, ischemic damage, congenital defects
• Transient hypothyroidism (10%) – can be due to maternal meds (carbimaozole) or maternal antibodies (maternal thyroid disease with IgG antibodies)

Hypothyroidism due to TSH deficiency – Rare (<1% of cases) due to pituitary dysfunction.

• dyshormonogenesis – an inborn error of thyroid
hormone synthesis. 5% to 10%. more common with consanguinity

• iodine deficiency – the most common cause of
congenital hypothyroidism worldwide - rare in developed nations.

Question 77

what are the clinical features of congenital hypothyroidism?

Answer 77

Usually asymptomatic and picked up on screening.

Clinical features:
• faltering growth !
• feeding problems !
• prolonged jaundice !
• constipation !
• pale, cold, mottled dry skin
• coarse facies
• large tongue
• hoarse cry
• goitre (occasionally)
• umbilical hernia
• delayed development !

later on in life/sx of acquired hypothyroid: 
Slow-relaxing reflexes
Delayed puberty/ amenorrhoea
Obesity
Slipped upper femoral epiphysis SUFE
Poor concentration
Deterioration in school work
Learning difficulties

Question 78

how do we ivx congenital hypothyroidism?

rx?

Answer 78

(Guthrie test) performed on all newborn infants, by
identifying a raised TSH in the blood.

However, thyroid dysfunction secondary to pituitary abnormalities will not be picked up at neonatal screening as they have a low TSH.

measure thyroid autoantibodies ± US or radionucleotide scan

Rx: lifelong thyroxine PO - must alter dose as TFTs adapt.
Monitor growth and developmental milestones.
good outcome, no intellectual inhibition

Question 79

what is the most comon cause of Acquired hypothyroidism ?

ivx findings?

Answer 79

This is usually caused by Hashimoto’s autoimmune thyroiditis.

Female > Male
Down syndrome or Turner syndrome have high risk of developing autoimmune disorders, e.g. vitiligo, rheumatoid arthritis, diabetes mellitus. In some families, Addison disease may also occur.

There is growth failure accompanied
by delayed bone age. Goitre is often present
but this may also be physiological in pubertal girls.

ivx:
Thyroid peroxidase antibodies (TPOAb) and thyroglobulin antibodies (TgAb)

Treatment is with thyroxine.

Question 80

what is the most comon cause of hyperthyroidism in paeds? epidemiology?

other causes?

Answer 80

(Graves disease)
thyroid-stimulating antibodies (TSIs), TSH receptor antibodies (TSH-rAb)

The clinical features are similar to those in adults, although eye signs are less common.

It is most often seen in teenage girls.

Neonatal hyperthyroidism:
can be caused by plavental transfer of TSIs -> from a mother with hyperthyroid to fetus. Needs urgent treatment.

Question 81

what is the aetiology of rickets?

Answer 81

1• Calcium deficiency – due to diet or malabsorption

2• Vitamin D
o Deficiency – diet, malabsorption, lack of sunlight, iatrogenic (drug induced – phenytoin therapy)
o Metabolic defect – due to 1α hydroxylase deficiency, liver disease, renal disease
o Defect in action – mutations in vitamin D receptor gene = end-organ resistance to vitamin D

• Rickets – low maternal vitamin D may adversely affect developing fetal brain – shown to affect postnatal head and linear growth

3• Phosphate deficiency
A o Renal tubular phosphate loss – isolated → hypophosphatemic rickets
▪ X-linked, Auto Rec or Auto Dom

B o Acquired hypophosphatemic rickets
▪ Fanconi syndrome, renal tubular acidosis, nephrotoxic drugs
C o Reduced phosphate intake

Question 82

How may rickets present clinically?

how do we ivx?

Answer 82

• Growth delay or arrest
• Bone pain, fracture
• Skeletal deformities – swelling of wrists, swelling of costochondral junctions (rickets rosary), bowing of long bones, frontal cranial bossing
• Delayed closure of anterior fontanelle
• Delayed dentition
• Misery
• Hypotonia
• Seizures - remember Ca is low

O/E:

• Harrisons sulcus - indentation of the lower rib cage where the diaphragm attaches
• Widened wrists and ankles

Ivx:
Xray - poorly mineralised bones, cupping and
fraying of the metaphyses and a widened
epiphyseal plate.

Question 83

How do we mx rickets?

Answer 83

1 • Prevention
o All infants should receive vitamin D daily (part of fortified formula or multivitamin); pregnant or lactating mothers should receive 400IU daily

2 • Dietary sources
o Fatty fish, egg yolk, fortified foods, shop bought milk, cereals

3 • Correct low Vit D levels with increased intake
o Ca supplements
o Oral Vit D2 (ergocalciferol) or oral vit D3 (cholecalciferol)
o Measure serum Ca, phosphate, Alk Phos, urine Ca:Creatinine ratio periodically

Question 84

Causes of tall stature

Answer 84

Familial tall stature

Chronosomal:
Kleinfelters 47 XXY
Soto’s syndrome

Precocious puberty - tall early, short overall

Endocrine disorders

• GH excess
• thyrotoxicosis

Question 85

If a childs bone age is less than chronological age, what does this mean?

Answer 85

Child has growth potential

Question 86

what are the types of diabetes mellitus?

most common in kids?

Answer 86

• Type 1. Most childhood diabetes
– Destruction of pancreatic β-cells by an
autoimmune process

• Type 2. Insulin resistance followed later by
β-cell failure
– Usually older children, obesity-related,
positive family history, not as prone to
ketosis, more common in some ethnic
groups (e.g. Black and Asian children)

• Other types
– Maturity onset diabetes of the young
– various types caused by genetic defects in
β-cell function. Strong family history.
– Drugs, e.g. corticosteroids
– Pancreatic insufficiency, e.g. cystic fibrosis,
iron overload in thalassaemia

– Endocrine disorders, e.g. Cushing syndrome
– Genetic/chromosomal syndromes, e.g. Down
and Turner
– Neonatal diabetes: transient and permanent
secondary to defective B cell function.
– Gestational diabetes

Question 87

what is the aetiology of type 1 diabetes?

Answer 87

An environmental trigger exhibits Molecular mimicry for an antigen on the surface of β-cells of the pancreas.

Triggers :
enteroviral infections (most common)
diet - cow’s milk proteins

In genetically predisposed individuals, this results in an
autoimmune process which damages the pancreatic β-
cells and leads to increasing insulin deficiency

Markers of β-cell destruction include:
antibodies to glutamic acid decarboxylase (GAD), the islet cells and insulin.

Question 88

how does ketoacidosis present?

Answer 88

Late sign in diabetes

• Smell of acetone on breath
• Vomiting
• Dehydration
• Abdominal pain
• Hyperventilation due to acidosis (Kussmaul
breathing)
• Hypovolaemic shock
• Drowsiness
• Coma and death

Question 89

what is the diagnostic criteria for T1DM?

Answer 89

The diagnosis is usually confirmed in a symptomatic
child by finding;

1. a markedly raised random blood
   glucose (>11.1 mmol/L),
2. glycosuria
3. Cap Blood ketones >3.0mmol/L

A blood glucose, capillary gas and ketone level will confrim DKA - tutorial

U&Es – demonstrate dehydration
Blood gas – shows severe metabolic acidosis
Urine glucose and ketones – both present
ECG – shows T wave changes of hypokalaemia – can be fatal

if doubt:

1. fasting blood glucose (>7 mmol/L)
2. raised (HbA1c)

An OGTT is rarely required to diagnose type 1 diabetes in children.

Question 90

Acanthosis nigricans in axilla is a sign of which type of diabetes?

Answer 90

Type 2 - its a sign of insulin resistance.

Question 91

How do we manage DKA?

Answer 91

1. ABCDE approach and don’t ever forget glucose

1b. Rehydration (0.9% NaCl with K added in) – treat dehydration over 48 hours
- If child shocked – give intial fluid bolus

2. FIXED RATE IV Insulin therapy – usually 0.1 units/kg/hour
3. Potassium correction
   - add from start if hypokalaemic

ORAL rehydration with subcutaneous insulin :
Patients with <5% dehydration who are not clinically unwell, ie mild acidosis and no nausea or
vomiting, can be given this

IV fluids and potassium replacement should occur for 1-2 hours before starting insulin, by which point the blood glucose should have started falling.

Check that blood glucose and ketones are falling

Question 92

what are the different severities of DKA?

Answer 92

→ Mild - pH <7.3 or bicarbonate <15 mmol/L
→ Moderate - pH <7.2 or bicarbonate <10 mmol/L
→ Severe - pH <7.1 or bicarbonate <5 mmol/L

Question 93

what is the admission criteria in DKA?

Answer 93

The following are recommended criteria for admission to PICU/HDU:

o Severe acidosis (pH <7.1) with marked hyperventilation

o Severe dehydration or shock

o Depressed consciousness with risk of aspiration from vomiting

o Very young (ie aged <2 years)

o Insufficient staffing on wards

Question 94

what are the principles of fluid replacement in DKA?

Answer 94

Aim to replace deficit over 48 hours – slowly due to increased risk of cerebral oedema, use reduced volume maintaining fluid doses

All fluids must contain 40mmol/L potassium chloride

We do NOT add glucose to initial therapy until:
→ When the BG falls to 12-15 mmol/L, change fluids to 0.45% saline with 5% glucose

Question 95

What are the complications of/ in the treatment of DKA? and their rx?

Answer 95

1. Cerebral Oedema: unpredictable, occurs more in younger children and newly diagnosed diabetes. 25% mortality.

Presentation:
Altered consciousness, headache, agitation, high blood pressure, unequal pupils, abnormal posturing
Unknown mechanism for development
Should treat with 3% saline or 20% mannitol and early referral to intensive care

2. Hypokalaemia: secondary to insulin therapy, this can cause cardiac arrthymias -> cardiac arrest
3. VTE

Question 96

what kind of monitoring is needed in DKA management?

Answer 96

Hourly paws,
accurate fluid input and output,
ECG due to potassium,
capillary blood GLUCOSE AND KETONES.

Weigh child twice daily,
U&Es, FBC, VBG,
look for signs of cerebral oedema

Question 97

target blood glucose in DM?

Answer 97

Explain target HbA1c of 48mmol/mol (6.5%) to minimize long term risk and plasma glucose <7 waking/premeal or <5 if driving

Question 98

what additional management measures must be taken in an individual with T1DM?

Answer 98

• If suspected T1 – refer to MDT paeds diabetes team to confirm diagnosis and provide immediate care

o Offer continuing education program covering insulin therapy, blood glucose monitoring, diet, intercurrent illness and managing hypos

• Advise more than 5 capillary blood glucose tests per day

Management of hypos → also have an immediate source of fast acting glucose and blood glucose monitoring equipment

Question 99

see chempath diabetes cards for hypos + its mx

Answer 99

k

Question 100

what are the different insulin regimes and indications ?

Answer 100

1. Multiple daily insulin basal-bolus regimens
   a. Short acting before meals
   b. 1 or more intermediate/long acting
2. Continuous sub-cut insulin infusion – insulin pump therapy. 1, 2 or 3 insulin injections per day, short mixed with intermediate-acting
   - if reccurent hypos that are affecting life eg school

Question 101

how does mx for T1DM and T2DM differ?

Answer 101

T2DM:
Diet, exercise, education, growth monitoring + Metformin
occasional Hba1c measurement - 3 monthly?

T1DM - more complex:
Diet advice,
daily monitoring blood sugars,
using insulin injections / pumps
avoiding, detecting and managing hypos
growth and other monitoring

Question 102

what are the common and less common causes of developmental delay – isolated / global?

Answer 102

Common causes

• Environmental understimulation / neglect
• Iron deficiency
• Cerebral palsy (including hypoxic ischaemic encephalopathy

Less common causes
- Congenital/inherited conditions
- chromosomal rearrangements
single gene defects (Duchenne muscular dystrophy, storage disorders, inborn errors of metabolism)
- Brain dysplasia, Vitamin D deficiency (delayed motor milestones)

Question 103

An 10 yo girl comes in to GP for tiredness, abdominal pain, and 4kg weight loss, polyuria and recurrent cold sores.
Urine dip shows glycosuria. Subsequent tests shows ketones 4, glucose > 11.1, no metabolic acidosis.
How would you manage?

Answer 103

T1DM likely triggered by infection.

Rx:
SC insulin (basal bonus regime), oral fluid rehydration - encourage her to drink. No drips

Not in DKA (as no metabolic acidosis) so does not need IV insulin.

MDT:
Diabetes nurses - for patient education about condition, and diet and lifestyle changes. inform about injections.
DAPHNE - structured teaching for carb counting and correcting nova rapid to this. - diabetes team calculate requirements.
Refer to paediatric diabetes team

Question 104

what is the pattern of inheritance of Turners?

Answer 104

Autosommal RECESSIVE

but since there is a deletion of the other X chromosome, it is expressed!