Thyroxine Metabolism in the Low Thyroxine State of Critical Nonthyroidal Illnesses*

Abstract

This study reports in vitro and in vivo parameters of T₄ metabolism in patients with critical nonthyroidal (illnesses who were selected because of serum total T₄ values less than 3µg/dl and normal TSH levels. Despite the depressed total (T)4 concentrations, the normal serum free T₄ values (7 of 9 patients), T₄ production rates (8 of 9), and TSH responses to TRH (8 of 8) provided evidence for normal free T₄ availability to peripheral tissues. Elevated rT₃ values in 10 of 14 patients were consistent with this view. However, serum free T₄ index (determinations markedly underestimated free T₄ (20 of 20). This resulted from failure of the T₃ uptake measurement to reflect the defective state of serum T₄ binding. Defective serum T₄ binding to carrier proteins was evidenced by the 2- to 3-fold increase in both the free fraction and the MCR values for T₄. The normal early distribution phase, despite defective serum T₄ binding, suggested an additional abnormality of deficient extra-vascular T₄ binding. The blunted TSH response to TRH and (the low normal values for both T₄ (production rates and free T₄ levels measured by equilibrium dialysis indicated mild pituitary subpression, possibly related to elevated serum cortisol levels. (Since an overt deficiency of free T)4 availability does not appear t o exist in the low T₄ state of critical nonthyroidal (illness, T₄ therapy cannot currently be recommended.