Location via proxy:   [ UP ]  
[Report a bug]   [Manage cookies]                

Graves' Hyperthyroidism in Pregnancy: A Clinical Review

Download as pptx, pdf, or txt
Download as pptx, pdf, or txt
You are on page 1of 22

REVIEW ARTICLE

Graves’ hyperthyroidism in
pregnancy: a clinical review
Caroline T. Nguyen, Elizabeth B. Sasso, Lorayne Barton and
Jorge H. Mestman

AULIYA SYISMA AGHNESI (G4A017087)


SMF ILMU PENYAKIT DALAM
RSUD PROF. DR. MARGONO SOEKARJO PURWOKERTO
FAKULTAS KEDOKTERAN UNIVERSITAS JENDERAL SOEDIRMAN
Background
Graves’ Hyperthyroidism (GH) is an autoimmune condition
caused by antibodies stimulating the thyroid stimulating
hormone receptor (TSHR)

• GH affects 0.2% of pregnant women


• Pregnancy alters thyroid physiology and laboratory testing, antithyroid drugs
(ATDs) are associated with teratogenicity
• Fetal and neonatal hyperthyroidism occurs in 1% to 5% of women with active or a
past history of GH
• All women of reproductive age with GH or past history of GH should receive
preconception counseling.
Preconception counseling
Counseling should take into consideration the woman’s desired
timeline to conception and include a discussion of the risks and
benefits of all treatment options (medical therapy, 131-I
radioactive iodine ablation (RAIA), and surgery)
Women with GH should be advised to postpone conception and
use contraception until GH is controlled
Etiologies of hyperthyroidism

Gestational Transient Thyrotoxicosis


GTT affects 1–5% of pregnant women early in pregnancy

Dx :
• Hyperthyroidsm syndrome
• Hyperemesis gravidarum hCG levels
rise at weeks 7,
• Negative TRAb decrease between
• Absence of Graves weeks 14 and 20
ophthalmopathy, goiter,
and prior history of GH
Etiologies of hyperthyroidism

Graves’ hyperthyroidism (GH)


The diagnosis of GH should be suspected in a hyperthyroid pregnant
woman who :
1) was having symptoms prior to pregnancy
2) had a prior diagnosis of hyperthyroidism
3) had a previous birth to an infant with thyroid
dysfunction.
Thyroid function tests
TSH concentrations may be below the non-pregnant
reference range
FT4 concentration also continuously declines throughout
pregnancy
Total thyroxine (TT4) assay is more consistent between
assays. After week 16, the non-pregnancy reference range
may be adjusted by a factor of 1.5 and used to assess
thyroid status (i.e., 4.5–12.5µg/dL becomes 6.75–
18.75µg/dL)
FT4 index (FT4I) is a reliable marker of free thyroxine status
during pregnancy
TSH Receptor Antibodies (TRAb)
TSH-binding inhibiting Ig
(TBI)/thyrotropin binding
Thyroid-stimulating Ig (TSI) inhibitory immunoglobulin (TBII)
• Bioassay that detects cyclic • Detect all TRAb (stimulating, blocking,
adenosine monophosphate and neutral)
(cAMP) production in cells • Assays by compete for binding of the
incubated with patients’ sera TSHR
and measures stimulating TRAb • 97% sensitivity and 99% specificity for
• Have the ability to differentiate GH
between stimulating and • unable to differentiate between
blocking antibodies stimulating or blocking antibodies
Maternal Management
First trimester, PTU can be dosed at 50–150 mg every 8 h
When switching from MMI to PTU, a ratio of 1:20 is used (i.e., MMI 15
mg = 300 mg of PTU per day dosed as 100 mg PO every 8 h)

After the first trimester, MMI 5-20 mg can be given as a


single dose.

Propranolol 10-20 mg every 6–8 h can be used to control hyperadrenergic


symptoms
The role of thyroidectomy
Thyroidectomy in the second trimester is an effective option
if a woman is unable to tolerate ATDs, nonconsistent with drug
therapy, requiring very high doses of ATDs, has a large goiter, or
allergic to ATD

Nb : A few days of SSKI or saturated solution of potassium iodide (50-100 mg/day) to


help decrease the vascularity of the thyroid gland and control hyperthyroidism
Anti-thyroid drugs: Complications for
mother and fetus
ATD associated defects are most common and severe in
those exposed during weeks 6–10
PTU has traditionally been
preferred over MMI in the first
trimester because the birth
defects associated with PTU are
considered less severe and
surgically correctable 👉 👉
Monitoring the fetus
Fetal risks in mothers with GH include hyperthyroidism due to
inappropriate transplacental passage of maternal TRAb and
hypothyroidism due to excessive maternal administration of
ATD.
Do You Know?
Maternal TRAb levels
greater than 3 times
the ULN in the latter
half of pregnancy
predicted neonatal
hyperthyroidism
Indications for fetal ultrasound (FUS)
• Women with a prior fetus
or neonate with a thyroid
disorder
• TRAb greater than 3 performed at
times the ULN 18–22 weeks
and then every 4 weeks
• Fetal tachycardia
• Poorly controlled
hyperthyroidism
US findings of hyperthyroidism
The earliest sonographic sign of fetal thyroid dysfunction is fetal
goiter.
• HR > 160 bpm for over 10 min Further complications..
• Intrauterine growth restriction • Polyhydramnios secondary
• Presence of fetal goiter • Cervical dystocia
• Advanced bone age • Mechanical obstruction of the
• Oligo/polyhydramnios fetal airway
Fetal hypothyroidism secondary to ATD
drugs
Fetuses of mothers with GH on ATD can develop
hypothyroidism and/or goiter due to overtreatment
with ATDs
Diagnosis 👉 cordocentesis involves US guided
Therapy 👉 intra-amniotic levothyroxine injections
(the change in size of fetal goiter and extent of
polyhydramnios help determine the response to
treatment)
Fetal thyrotoxicosis
Isolated fetal hyperthyroidism in a euthyroid mother is treated
with MMI 10-20 mg daily after the first trimester
Fetal assessment should then be performed every 1–2 weeks or
as necessary with evaluation of fetal heart tones with hand-held
doppler and US to assess growth, size of fetal thyroid gland, and
amniotic fluid index
Neonatal management

TRAb can remain in the • FT4 measurement at birth should be


infant’s circulation for up repeated between days 3 and 5 of life and
to four months after continuously followed if elevated.
delivery leading to • TRAb positive neonates without biochemical
postnatal thyrotoxicosis in
or clinical evidence of thyroid dysfunction
1–5% of infants of mothers
with GH should have weekly clinical and laboratory
follow up until the TRAb test becomes
negative
Signs of neonatal thyrotoxicosis
Tachycardia
Tachypnea
Pulmonary arterial hypertension
Systemic hypertension and heart failure Treatment
Small for gestational age MMI 0.5–1 mg/day
Accelerated bone maturation with addition of
propranolol (2 mg/
and craniosynostosis
kg/d) if severe
In cases of non-transient hypothyroidism, the
recommended starting dose of levothyroxine is 10–15
mcg/kg/ day in term neonates. Therapy should be initiated
within two weeks of life for optimal outcomes and the
infant should be followed for the first three years of life
Breastfeeding
Breastfeeding has been shown to be safe in mothers
taking ATDs in appropriate doses. MMI and PTU both
appear in breast milk in very small concentrations
Conclusions
GH from GTT, the most common Limited course of ß-adrenergic
cause of hyperthyroidism in blockers may be used to control
pregnancy. symptoms of GH.
ATDs remain the cornerstone of Surgery in the second trimester may
treatment of GH in pregnancy, with be indicated for women unable to
the lowest doses needed to maintain take ATD, uncontrolled on high doses
TT4 at 1.5× the upper limit of the non- of ATD, or with large goiters
pregnant reference range or FT4I in Persistently elevated levels of TRAb >
the upper limit of the reference 3× upper limit of normal is prognostic
range. of fetal thyroid dysfunction
PTU is preferred in the first trimester

You might also like