Neonatal hyperthyroidism on rat heart: interrelation with nitric oxide and sex.

J Endocrinol Invest

Department of Physiology, School of Pharmacy and Biochemistry, University of Buenos Aires, IQUIMEFA-CONICET, Junin 956, C1113AAD, Buenos Aires, Argentina.

Published: June 2015

AI Article Synopsis

  • The study aimed to understand how hyperthyroidism affects heart function in rats, specifically looking at differences between male and female rats during their second month of life.
  • Male rats treated with triiodothyronine (T3) showed a decrease in left ventricle volume, while female euthyroid rats exhibited higher levels of atrial nitric oxide synthase (NOS); T3 treatment reduced NOS activity in both sexes.
  • The findings highlight significant sex-related differences in heart response to hyperthyroidism, suggesting that factors like nitric oxide may play a role in how each sex experiences cardiovascular dysfunction.

Article Abstract

Purpose: To clarify the mechanism mediating the effect of hyperthyroidism on cardiac function during the second month of life in rats.

Methods: Male and female Sprague-Dawley rats were assigned to a control or to a triiodothyronine (T3)-treated group. Treatment of each group was started on the third day after birth. Control rats (Eut) received 0.9 NaCl [0.1 ml/100 g body weight (BW)] every second day during 60 days and T3-treated rats (Hyper) received subcutaneous (SC) T3 injections every second day during 60 days.

Results: Hyperthyroidism decreased left ventricle volume only in male rats. Female euthyroid rats presented higher atrial nitric oxide synthase (NOS) activity than male rats and hormonal treatment decreased this enzyme's activity in both sexes. Euthyroid male and female rats had similar atrial NOS protein levels, but females had higher caveolin (cav) 3 protein levels. T3 treatment increased this protein only in males. Female rats had lower ventricular NOS activity than male rats; hyperthyroidism increased NOS activity in both sexes but this effect was associated with lower cav 3 protein levels. Hyperthyroidism did not change cav 1 protein levels in both male and female rats.

Conclusions: The results of this study demonstrating clinically relevant sex-related differences in the pathophysiology of the hyperthyroid heart have raised new questions regarding the mechanisms responsible for the observed differences. This study suggests that sex-related intrinsic factors such as nitric oxide may modulate the response to hyperthyroidism that leads to cardiovascular dysfunction.

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Source
http://dx.doi.org/10.1007/s40618-015-0244-4DOI Listing

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