Conflicting evidence has been reported about the association of TSH and kidney status in euthyroid DM subjects [14, 36, 37]. linear regression showed that UACR levels were negatively associated with FT3 and T3 ( 0.001). In addition, eGFR was positively associated with FT3 and T3 and was negatively associated Dicloxacillin Sodium hydrate with TSH and FT4 levels and TgAb positivity (all 0.05). By using binary logistic regression, higher TSH and FT4 and lower FT3 and T3 were associated with kidney disorders (all 0.05). Similar results were seen in sensitivity analyses, which were performed in 3035 euthyroid diabetic participants; however, TSH was no longer related to them. The area under the receiver operating characteristic curve (AUROC) of lower FT3 for existing kidney disorder was greater than that for any other thyroid hormones (all 0.001). The cutoff value of FT3 for reduced eGFR was 4.39?pmol/L. Regarding thyroid homeostasis parameters, SPINA-GD was negatively associated with three statuses of kidney disorders, and TSHI and TTSI were positively associated with reduced eGFR (all 0.05). Conclusions Among patients with type 2 diabetes, elevated TSH and FT4 (or T4), Dicloxacillin Sodium hydrate lower FT3 (or T3), TgAb positivity, lower SPINA-GD, and higher TSHI and TTSI were associated with kidney disorders. The lower FT3, even within the normal range ( 4.38?pmol/L), may be the factor most related to reduced eGFR compared with other thyroid hormones in diabetic patients. 1. Introduction Diabetes mellitus (DM) and its complications have become highly prevalent and have gained increasing attention [1], especially in developing countries. The estimated prevalence of diabetes among a representative sample of Chinese adults was 11.6%, which indicates the importance of diabetes as a public health problem in China [2]. Chronic kidney disease (CKD) is defined by the sustained presence of reduced kidney function or damage, often resulting from diabetes mellitus (DM) and hypertension [3]. Approximately 13% of individuals in the general US population have CKD, and the incidence is increasing globally [4C6]. Diabetic kidney disease (DKD) is one of the most common microvascular complications of diabetes mellitus and the leading cause of end-stage renal disease (ESRD) worldwide [7]. Approximately 20%C40% of patients with diabetes progress to DKD, and 40% also progress to ESRD [8]. Reduced estimated glomerular filtration rate (eGFR) and higher urinary albumin to creatinine ratio (UACR) levels are two main markers of diabetic kidney status, quantifying renal function and serving as a proxy of renal damage severity, respectively [3, 9]. The thyroid gland is one of the most important Dicloxacillin Sodium hydrate organs in the human body. It regulates the majority of the body’s physiological actions [10]. Thyroid hormone has an impact on renal tubular function and the renin-angiotensin system and is associated with hemodynamic and cardiovascular alterations that interfere with renal blood flow [11]. Conversely, the kidney is not only an organ for the metabolism and elimination Dicloxacillin Sodium hydrate of TH but also a target organ of some of the actions of the iodothyronines [12]. Acute kidney injury and chronic kidney disease are accompanied by notable effects on the hypothalamus-pituitary-thyroid axis. Hormonal derangements at the level of the hypothalamic-pituitary axis are often seen with the worsening of kidney function, and recent evidence points towards the implication of such hormonal disorders in the genesis of CKD [13]. Thyroid dysfunction Dicloxacillin Sodium hydrate causes remarkable changes in glomerular and tubular functions and in electrolyte and water homeostasis [12]. Although several studies have suggested the association of thyroid disorders CIT and CKD or DKD with conflicting results.
Conflicting evidence has been reported about the association of TSH and kidney status in euthyroid DM subjects [14, 36, 37]
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