Hepatic Failure/GI/Endocrine Emergencies
iv.
In patients who are allergic to iodine, lithium carbonate may be used as an alternative. Initial
dose should be 300 mg every 6 hours, with subsequent adjustment to maintain serum lithium
concentration of 0.8β1.2 mEq/L.
| d. | Reduce levels of circulating thyroid hormone. |
|---|
Cholestyramine can be given to bind circulating T3 and T4.
ii.
Salicylates should be avoided because use can decrease binding of thyroid hormones to proteins
and therefore increase concentrations of free thyroid hormones.
iii.
In severe cases that do not respond to standard therapy, plasmapheresis and therapeutic plasma
exchange may be considered to decrease T4 and T3 levels.
Reduce heart rate.
Because cardiovascular collapse leads to systemic decompensation, Ξ²-blockers should be
initiated as quickly as possible.
ii.
Ξ²-Blocker dose should be titrated to achieve heart rate control (typically below 90 beats/minute).
iii.
Traditionally, propranolol is the preferred therapy because it may block T4 to T3 conversion at
high doses. Propranolol is also the agent of choice in women who are pregnant or breastfeeding.
Dosing for this indication is aggressive, starting at 60 mg orally every 4 hours with an optional
initial loading dose of 80 mg.
iv.
Alternative agents include carvedilol, esmolol, and diltiazem. Diltiazem should be reserved for
patients with active bronchospasm or for those who do not tolerate Ξ²-blockers.
Myxedema Coma
Clinical presentation
Myxedema coma is defined as decompensated hypothyroidism that leads to multiorgan failure.
Despite its name, the primary manifestation of the disease is decline in mental status rather than
edema or coma.
Diagnosis is made on the basis of clinical presentation, not laboratory evidence of hypothyroidism.
Altered mental status and hypothermia are the most common presenting symptoms. Other
clinical features include hypotension, bradycardia, hypoglycemia, constipation, urinary
retention, puffiness of the hands and face, and pleural, pericardial, or peritoneal effusions.
ii.
Patients may present with shock or arrhythmias, including prolongation of the QT interval that
can lead to torsades de pointes.
iii.
If a patient presents with signs of infection without the systemic inflammatory response
syndrome, myxedema coma should be suspected.
iv.
Patients typically have elevated TSH and low or undetectable T3 and T4, but TSH may be
inappropriately low or normal in cases of central hypothyroidism. The level of change in
thyroid hormones does not correlate well with disease severity.
Myxedema coma is more common in older women and occurs more often during winter months
because of altered temperature regulation.
| d. | Discussion of nonthyroidal illness syndrome (βeuthyroid sick syndromeβ or βSICU thyroidβ) is |
|---|
beyond the scope of this chapter.
Myxedema coma may be the consequence of longstanding hypothyroidism but can also be
precipitated by an acute event such as infection, myocardial infarction, surgery, or cold exposure.
Drugs associated with the development of myxedema coma include sedatives, anesthetics, narcotics,
lithium, immune checkpoint inhibitors, and amiodarone, as well as abrupt discontinuation of
levothyroxine.
Management
Because myxedema coma is an endocrine emergency, treatment should be initiated without waiting
for laboratory data.