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Endocrine Abstracts (2023) 90 P143 | DOI: 10.1530/endoabs.90.P143

ECE2023 Poster Presentations Pituitary and Neuroendocrinology (123 abstracts)

Role of fT4 and TSH-index fluctuations as early diagnostic tools in milder forms of central hypothyroidism: data from 221 patients with pituitary lesions from a single tertiary center

Silvia Carrara 1 , Elena Galazzi 2 , Federico Nicoli 1 , Mirella Moro 2 , Letizia Fatti 2 , Biagio Cangiano 1,2 & Luca Persani 1,2


1University of Milan, Department of Medical Biotechnology and Translational Medicine, Italy; 2Italian Auxological Institute San Luca Hospital, Department of Endocrine and Metabolic Diseases, Milano, Italy


Diagnosis of Central Hypothyroidism (CeH) is commonly given when FT4 concentrations are below the lower limit of normal range. A reduction in FT4 concentrations greater than 20% was proposed in ETA 2018 Guidelines as an unphysiological fluctuation indicating the onset of milder forms of CeH with FT4 still within the normal range. Similarly, TSH-index was proposed to quantify thyrotrope reserve, hence as a tool to detect patients at risk of CeH. Here we verified the performance of these parameters for the diagnosis of CeH in 221 patients with pituitary lesions – 127 adenomas and 94 empty sellas – and at least three evaluations of Thyroid Function Tests (TFTs, i.e. paired detection of TSH and FT4) during a median follow-up of 4 years. We also studied TFTs of 42 matched controls, selected from a cohort of euthyroid patients (TSH 0.5-4.5 mU/l) with multinodular goiter and negative thyroid autoimmunity followed up during the same period. We evaluated FT4 concentrations, TSH, TSH-index and defined two derived parameters, FT4var and ΔTSH-index, which were respectively the greatest reduction of FT4 and TSH-index compared to their median value for each patient (FT4var=FT4 nadir – median FT4; ΔTSH-index = TSH-index nadir – median TSH-index). The diagnosis of CeH+ was made according to ETA 2018 Guidelines. In CeH- patients, FT4var did not differ statistically in patients with adenomas, empty sellas and controls (varying from 15 to 25%; P=n.s.). Consistently, in patients diagnosed with CeH+, FT4var (and its percentage value FT4var%) was able to distinguish patients harbouring adenomas or empty sellas with and without CeH [CeH+ vs CeH-: FT4var -3.1±1.9 vs -1.4 pmol/l (IQR-2.1; -0.7), P=0.03; FT4var% -28%±15 vs -8% (IQR -14; -5), P<0.001]. Moreover, in our cohort, TSH-index allowed in distinguishing patients harbouring a pituitary lesion CeH+ vs CeH-, at baseline [CeH+ vs CeH– 1.8 (IQR 0.8; 2.2) vs 2.5 (IQR 2; 2.9); P<0.001]) and during follow-up [CeH+ vs CeH–: 1.3±1.3 vs 2.5±0.7, P<0.001]. In conclusion, both patients with pituitary lesions and controls show fluctuations of TFTs around an individual set-point. In patients with pituitary lesions such as adenomas and empty sellas, FT4var, FT4var% and TSH-index are useful tools able to highlight milder forms of CeH. We found that a fluctuation of FT4 value (FT4var) or FT4var% respectively greater than 3.1 pmol/l or 28% indicated the onset of mild CeH. The coexistence of a TSH-index lower than 1.3 may be useful to support this challenging diagnosis.

Volume 90

25th European Congress of Endocrinology

Istanbul, Turkey
13 May 2023 - 16 May 2023

European Society of Endocrinology 

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