Adverse metabolic correlations relate to free T3 levels in subclinical hypothyroidism; common FOXE1 polymorphisms associate with blood pressure

Lloyd Anna de; Ilaria Muller; Alan Dodd; Ameen Bakhsh; Hilary Durrant; Lei Zhang; Carol Evans; Aled Rees; Marian Ludgate

doi:10.1530/endoabs.37.GP.26.03

GP.26.03

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Endocrine Abstracts (2015) 37 GP26.03 | DOI: 10.1530/endoabs.37.GP.26.03

ECE2015 Guided Posters Thyroid – hypothyroidism (10 abstracts)

Adverse metabolic correlations relate to free T₃ levels in subclinical hypothyroidism; common FOXE1 polymorphisms associate with blood pressure

Anna de Lloyd ¹ , Ilaria Muller ¹ , Alan Dodd ² , Ameen Bakhsh ¹ , Hilary Durrant ² , Lei Zhang ¹ , Carol Evans ² , Aled Rees ¹ & Marian Ludgate ¹

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¹Thyroid Research Group, IMEM, Cardiff University, Cardiff, UK; ²Department of Medical Biochemistry and Immunology, University Hospital of Wales, Wales, UK.

Introduction: The effects of mild subclinical hypothyroidism (SH; TSH <10 mU/l) on metabolic outcomes are unclear. This may relate to differences in aetiology, including thyroid autoimmunity or genetic factors such as TSH-receptor mutations (TSHR-M) and FOXE1 polyalanine tract length (FOXE1–PTL) polymorphisms, which are associated with altered thyroid function. We hypothesised that the metabolic manifestations of SH may depend upon its aetiology.

Aims: i) To establish whether free T₄, free T₃, or TSH associate with metabolic parameters and blood pressure (BP) in SH. ii) To investigate whether SH aetiology has a differential effect on metabolic parameters and BP.

Methods: A total of 208 adults with primary untreated SH (TSH ≥5 mU/l) were recruited and underwent a medical/lifestyle history, resting BP and BMI measurement, genetic evaluation (for TSHR-M and FOXE1–PTL status), thyroid function, anti-TPO antibody measurement, and metabolic assessments (HOMA-IR, full lipid profile). Associations were examined using stepwise multivariate regression analyses.

Results: TSH showed a small positive association with free T₃ (R +0.6, P=0.01) and a negative association with free T₄ (R −1.1, P<0.001) but no association with metabolic factors or BP. Free T₃ showed a positive association with BP (systolic R +10, P<0.001 and diastolic R +3, P=0.02) and HOMA-IR (R +1.3, P=0.009). No significant metabolic associations were found for TSHR-M or TPO antibody positivity. The 14/14 FOXE1–PTL (60% of cohort) was positively associated with free T₃ compared to other genotypes (R +0.2, P=0.007) and negatively associated with BP (systolic R −6, P=0.006 and diastolic R −4, P=0.01).

Conclusions: Free T₃ correlated positively with BP and HOMA-IR in this cohort, irrespective of SH aetiology. An unexpected association between FOXE1–PTL polymorphisms and BP was revealed.

Disclosure: Society for Endocrinology grant.

Volume 37

17th European Congress of Endocrinology

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