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The Correlation between Thyroid Hormone Levels and the Kidney Disease Progression Risk in Patients with Type 2 Diabetes

Authors Yang Z, Duan P, Li W, Nie R, Lou X, Wang L, Wu K, Liu J, Tu P, Lai X 

Received 12 November 2021

Accepted for publication 15 December 2021

Published 5 January 2022 Volume 2022:15 Pages 59—67

DOI https://doi.org/10.2147/DMSO.S347862

Checked for plagiarism Yes

Review by Single anonymous peer review

Peer reviewer comments 2

Editor who approved publication: Professor Ming-Hui Zou



Zhi Yang,1– 3 Peng Duan,2 Weihong Li,2 Ronghui Nie,2,3 Xiaoyang Lou,2,4 Lina Wang,2 Kexia Wu,2 Jiang Liu,2 Ping Tu,2 Xiaoyang Lai1

1Department of Endocrinology and Metabolism, The Second Affiliated Hospital of Nanchang University, Nanchang, 330008, Jiangxi, People’s Republic of China; 2Department of Endocrinology and Metabolism, The Third Hospital of Nanchang, Nanchang, 330000, Jiangxi, People’s Republic of China; 3Jiangxi Medical College of Nanchang University, Nanchang, 330036, Jiangxi, People’s Republic of China; 4Jiangxi University of Traditional Chinese Medicine, Nanchang, 330004, Jiangxi, People’s Republic of China

Correspondence: Xiaoyang Lai Tel +86 13607916298
Email [email protected]

Objective: We investigated the relationship between thyroid hormones and the risk of diabetic kidney disease (DKD) progression.
Methods: A total of 452 patients with type 2 diabetes were included, and a cross-sectional analysis was performed. Urine albumin/creatinine ratio (ACR) and estimated glomerular filtration rate (eGFR) were used to diagnose persistent albuminuria and stage chronic kidney disease, respectively. The Kidney Disease: Improving Global Outcomes (KDIGO) clinical practice guideline was used to describe the risk of DKD progression (low, moderate, and high or very high risks).
Results: The DKD group had higher levels of thyroid-stimulating hormone (TSH) and lower levels of free triiodothyronine (FT3) and free thyroxine (FT4) than the non-DKD group. The prevalence of thyroid dysfunction in the DKD group was significantly higher than in the non-DKD group, especially the prevalence of subclinical hypothyroidism. FT3 levels decreased gradually with the deterioration of DKD. TSH levels increased with an increasing KDIGO category. FT3 and FT4 levels were negatively correlated with serum creatinine levels and ACR, and positively correlated with eGFR. Contrastingly, TSH was positively correlated with ACR, and negatively correlated with eGFR. After adjustment, an increase in FT3 levels significantly reduced the risk of DKD [odds ratio, OR (95% confidence interval, CI)=0.58 (0.42– 0.79)] and DKD progression [ORs (95% CIs)=0.65 (0.45– 0.93) for the moderate risk group and 0.50 (0.33– 0.74) for the high or very high-risk group, using the low-risk group as a reference]. FT3 levels below 4.30 pmol/L in men and 3.99 pmol/L in women were the cut-off points for an increased risk of DKD progression.
Conclusion: Low FT3 level is an independent risk factor for DKD and DKD progression. FT3 ≤ 4.30 pmol/L in men and ≤ 3.99 pmol/L in women will greatly increase the risk of kidney disease progression in patients with type 2 diabetes.

Keywords: thyroid hormone, prognosis of chronic kidney disease, type 2 diabetes mellitus

Introduction

Diabetes leads to the damage of several organs and tissues, resulting in chronic complications; kidney disease is one of the common microvascular complications. Approximately 40% of the patients with diabetes develop chronic kidney disease (CKD).1 This increases the risk of end-stage kidney disease and cardiovascular disease, leading to a high mortality.2 In patients with type 2 diabetes mellitus (T2DM), the risk of cardiovascular diseases increases by 2–3 times when patients have higher levels of albuminuria, compared with those without significant albuminuria.3 Therefore, early detection and management of diabetic nephropathy is very important in delaying its progression. Furthermore, it is important to protect the kidneys, in order to significantly reduce the risk of comorbidities.

Thyroid hormones are involved in cell metabolism, blood sugar regulation, and insulin resistance. The prevalence of an abnormal thyroid function is higher in patients with diabetes (approximately 2.2–17% increase) than in healthy individuals.4 Hypothyroidism is the commonest abnormal thyroid function in these patients.5 In addition, thyroid hormones interact with the kidneys.6 Thyroid hormones contribute to the growth and development of the kidneys, maintain water and electrolyte balance, and participate in the renal transport system. Thyroid dysfunction affects the function of the glomerulus and renal tubules, and indirectly affects the renin–angiotensin system and renal blood flow. Changes in hemodynamics and the cardiovascular system have an effect on renal function.7,8 Besides, the kidneys are the target organs for thyroid hormones. They are involved in the metabolism and elimination of thyroid hormones. Chronic kidney disease affects the synthesis of thyroid hormones by regulating the hypothalamus-pituitary-thyroid axis.9,10 Previous studies have shown that thyroid hormones can interfere with the accumulation of collagen in the cortical interstitium and glomeruli;11 thyroid-stimulating hormone (TSH) influences kidney disease progression;12 and low triiodothyronine (T3) levels may play a role in worsening renal function.13 Therefore, the purpose of this study was to explore the correlation between thyroid hormones and the progression risk of type 2 diabetic kidney disease (DKD).

Methods

The present cross-sectional study analyzed the hospitalization data of 452 subjects with type 2 diabetes Table S1. The risk of DKD progression was evaluated by a combination of urine albumin/creatinine ratio (ACR) and estimated glomerular filtration rate (eGFR).

Study Population

All subjects of this study were patients with type 2 diabetes aged 18 years or above. They were routinely hospitalized in the Department of Endocrinology and Metabolism of the Third Hospital of Nanchang between February 2018 and November 2020. We tried our best to obtain sufficient informed consent from the subjects and avoid selection bias as much as possible. All subjects participated in the study voluntarily and signed written the informed consent form at admission. The exclusion criteria were as follows: 1) other types of diabetes; 2) taking drugs that affect thyroid hormone levels; 3) urinary tract infections or receiving drugs that affect urine protein; 4) an active urinary sediment (containing red or white blood cells or cellular casts), rapidly increasing albuminuria or nephrotic syndrome, rapidly decreasing eGFR;14 5) multiple hospitalizations. A total of 486 patients were enrolled, and 34 patients with incomplete data were excluded. Finally, 452 patients were included in the study.

Laboratory Assays

An ultrasonic instrument (Omron HNH–318, Japan) was used to measure the height and weight of each patient to the nearest 0.1 cm and 0.1 kg, respectively. These values were used to calculate the body mass index (BMI) by the formula, BMI=weight (kg)/height2 (m2).

Venous blood was collected from patients in the morning in an empty stomach (fasting for at least 8 h). Fasting blood glucose (FBG), serum creatinine (SCr), blood urea nitrogen (BUN), uric acid (UA), serum total cholesterol (TC), triglycerides (TG), high-density lipoprotein cholesterol (HDL-C), and low-density lipoprotein cholesterol (LDL-C) levels were measured on the same autoanalyzer (Roche, Basel, Switzerland). Glycated hemoglobin (HbA1c) was detected using high-performance liquid chromatography (Bio Rad D-10, Berkeley, USA). Chemiluminescence immunoassay was used to measure serum TSH, FT3, and FT4 levels (Siemens ADVIA Centaur XP, Germany). The reference ranges of TSH, FT3, and FT4 levels were 0.38–4.34 mIU/L, 2.77–6.31 pmol/L and 10.45–24.38 pmol/L, respectively. Urine albumin levels were measured using the immunological turbidimetry assay, and urine creatinine levels were measured using the picric acid method (Siemens ADVRI 2400, Germany). The urine albumin/creatinine ratio (ACR) was calculated. The eGFR was calculated using the Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI) equation.

DKD was defined as eGFR <60 mL/min/1.73 m2 and/or ACR ≥30 mg/g.14 Patients with or without DKD were grouped. Three different renal function classifications were used for the grouping analysis: 1) ACR <30, 30–300 and >300 mg/g were defined as normal albuminuria, microalbuminuria and massive albuminuria, respectively; 2) eGFR ≥90, 60–89, 45–59, 30–44, 15–19 and <15 mL/min/1.73m2 were defined as stages 1, 2, 3a, 3b, 4 and 5 CKD, respectively; and 3) the Kidney Disease: Improving Global Outcomes (KDIGO) classification,15 which combined eGFR with ACR, was used to assess the risk of DKD progression (low, moderate, high or very high risks) (Figure 1).

Figure 1 The KDIGO risk categories.

Abbreviations: ACR, albumin/creatinine ratio; eGFR, estimated glomerular filtration rate; KDIGO, Kidney Disease: Improving Global Outcomes.

Notes: Green, low risk; yellow, moderate risk; orange, high risk; red, very high risk.

Statistical Analyses

All analyses were performed using SPSS 25.0. Count data are expressed as rates (%), and the χ2 test was used for comparison between groups. Normally distributed measurement data are expressed as means ± standard deviations; the differences between the groups were calculated using one-way analysis of variance. Non-normally distributed data are expressed as medians (interquartile ranges: 25th and 75th percentile); the Mann–Whitney and Kruskal–Wallis tests were used to compare between the groups. The correlation between thyroid hormones and various variables were assessed using Spearman correlation analysis method. A multivariable logistic regression model was used to analyze the association between thyroid function and diabetic nephropathy. The confounding factors included sex, age, FBG, HbA1c, TC, TG, HDL-C and LDL-C. To identify the cut-off points for thyroid hormones in assessing the risk of DKD progression, further subgroup analyses by sex were performed. P values <0.05 were considered statistically significant.

Results

The Clinical Characteristics of Study Subjects

Among the 452 subjects, 188 (41.6%) had diabetic nephropathy, 264 (58.4%) did not have diabetic nephropathy, and there was no significant difference between female and male (P>0.05). Compared with the patients without DKD, patients with DKD were a little younger, had lower eGFR, FT3 and FT4 levels; and higher BUN, SCr, UA, LDL-C, ACR, and TSH levels (P<0.05) (Table 1).

Table 1 The Clinical Characteristics of Study Subjects with or without DKD

The Prevalence of Thyroid Dysfunction in Subjects with or without DKD

In subjects with DKD, the overall prevalence of thyroid dysfunction (any of hyperthyroidism or subclinical hyperthyroidism or hypothyroidism or subclinical hypothyroidism) was 22.9%, compared with 17.5% in patients without DKD (P=0.009). The proportion of subclinical hypothyroidism in DKD group was observed as high as 19.7%, which was significantly different from that in the non-DKD group (9.5%). (Figure 2)

Figure 2 The prevalence of thyroid dysfunction in subjects with or without DKD.

Notes: A, B, C and D represent the prevalence of hyperthyroidism, subclinical hyperthyroidism, hypothyroidism, and subclinical hypothyroidism respectively.

Comparison of Thyroid Hormone Levels in Different DKD Categories

Due to the small numbers of people in stages 4 and 5 CKD, we combined the two groups into eGFR<30 mL/min/1.73m2. The results showed that FT3 levels varied with degrees of albuminuria, kidney damage, and KDIGO risk (P<0.05), and decreased with increasing severity. FT4 levels decreased with worsening CKD stages, and TSH levels increased with a higher risk of KDIGO categories (P<0.05) (Table 2).

Table 2 Thyroid Hormone Levels in Different ACR, eGFR and KDIGO Risk Categories

Correlation Analysis Between Thyroid Hormones and Indexes of Renal Function

There was a negative correlation between FT3 and FT4 levels with both SCr and ACR (r=−0.168, P<0.001 and r=−0.107, P=0.023; r=−0.267, P<0.001 and r=−0.109, P=0.021, respectively). Meanwhile, FT3 and FT4 levels were positively correlated with eGFR (r=0.325, P<0.001 and r=0.165, P<0.001, respectively). In contrast, there was a negative correlation between TSH levels and eGFR (r=−0.128, P=0.006), and a positive correlation between TSH levels and ACR (r=0.104, P=0.027) (Table 3).

Table 3 Correlation Between Thyroid Hormones and Parameters of Renal Function

Regression Analysis of Thyroid Hormones and the Risk of Diabetic Nephropathy Progression

A logistic regression analysis was performed, using with or without diabetic nephropathy as the dependent variable and using thyroid hormone levels as the independent variable. After adjusting for sex, age, FBG, HbA1c, TC, TG, HDL-C and LDL-C, an increase in FT3 levels significantly reduced the risk of having diabetic nephropathy [odds ratio, OR (95% confidence interval, CI)=0.58 (0.42–0.79), P=0.001]. However, FT4 and TSH levels did not influence the risk of disease [OR (95% CI) of FT4=0.97 (0.92–1.02), P=0.281; OR (95% CI) of TSH=1.02 (0.99–1.05), P=0.147] (Table 4).

Table 4 Logistic Regression Analysis of Thyroid Hormones and the Risk of Having Diabetic Nephropathy

The risk of diabetic nephropathy progression (KDIGO risk categories) was further used as the dependent variable. When using the low KDIGO risk group as the reference group, an increase in FT3 level significantly reduced the risk of DKD progression [moderate risk, OR (95% CI)=0.65 (0.45–0.93), P=0.020; high or very high risk, OR (95% CI)=0.50 (0.33–0.74), P=0.001] (Table 5).

Table 5 Logistic Regression Analysis of Thyroid Hormones and the Risk of Diabetic Nephropathy Progression

Subgroup Analysis of FT3 and the Risk of Diabetic Nephropathy Progression

Further, the KDIGO risk categories were the dependent variables in the subgroup analysis (reference: the low-risk group), and the tri-sectional quantiles of FT3 were the independent variables (reference: the highest tertile). The results showed that the lowest tertile of FT3 not only increased the high or very high risk of DKD progression in men [OR (95% CI)=3.66 (1.54–8.71), P=0.003] but also increased all risks of DKD progression in women [moderate risk, OR (95% CI)=2.37 (1.02–5.51), P=0.044; high or very high risk, OR (95% CI)=7.23 (1.72–30.34), P=0.007]. Therefore, we obtained two cut-off points for FT3 to assess the increased risk of DKD progression, which were less than 4.30 pmol/L for men and less than 3.99 pmol/L for women, respectively (Table 6).

Table 6 Subgroup Analysis of FT3 and Risk of DKD Progression Stratified by Male and Female

Discussion

Our results showed that FT3 and FT4 were negatively correlated with SCr and ACR and positively correlated with eGFR. In contrast, TSH was negatively correlated with eGFR and positively correlated with ACR. These findings were consistent with previous studies16–18 and suggested that thyroid hormones were related to renal function in patients with diabetes. Firstly, thyroid hormones were involved in glucose metabolism, and the prevalence of thyroid dysfunction in patients with diabetes was higher than that in healthy individuals.19 Secondly, our further findings showed that FT3 levels decreased gradually with increased severity of kidney damage and albuminuria. Even with normal thyroid function, FT3 was positively correlated with eGFR and negatively correlated with ACR in previous study.18 Thirdly, TSH levels increased and FT3 levels decreased in higher risk groups of DKD progression, using the KDIGO classification. Previous studies suggested that patients with diabetes who had higher TSH levels and lower FT3 levels were more likely to develop DKD.12,20 In addition, a higher prevalence of subclinical hypothyroidism was found in the DKD group. Subclinical hypothyroidism was regarded as an independent risk factor for DKD,21,22 and thyroid replacement therapy can play a role in renal protection.23,24

An insufficiency of the thyroid gland may be related to intrarenal vasoconstriction, a decrease in cardiac output, and a decrease in effective renal blood flow, which cause the final results of renal damage and an appearance of microalbuminuria.25,26 In addition, Reinhardt et al27 showed that the severity of albuminuria in patients with CKD had the greatest impact on the concentration of reverse triiodothyronine (rT3), and the serum rT3 concentration was significantly negatively correlated with the degree of albuminuria. Furthermore, because most thyroid hormones bind to proteins, protein loss caused by albuminuria will lead the depletion of thyroid hormones, which in turn stimulates the hypothalamus-pituitary-thyroid axis through negative feedback and inhibits the conversion of T4 to T3 in peripheral tissues, resulting in an increase in the TSH level and a decrease in the T3 level.28

In order to confirm the strong association between thyroid hormones and DKD, a logistic regression analysis was performed. Our study suggested that the increase in FT3 level significantly reduced the risks of DKD and DKD progression by about 35–50%. Consistently with other studies,29–32 low T3 level was disclosed as a common feature in patients with kidney disease, and FT3 could be an effective marker for predicting DKD and evaluating prognosis.

The role of FT3 in diabetic nephropathy progression is unclear. However, there are some hypotheses. Firstly, endothelial dysfunction and podocyte disease play a key role in the pathogenesis and development of DKD.33 Microalbuminuria is a sign of systemic endothelial dysfunction and vascular damage,34 and thyroid hormones can affect vasodilation, regulate endothelial function and homeostatic signal transduction processes.35 Experimental models have confirmed that T3 can directly or indirectly relax vascular smooth muscle cells, thereby affecting endothelial function.36 In patients with stage 3–4 CKD without diabetes, it was also proven that low serum FT3 level was related to endothelial dysfunction assessed by the blood flow-mediated expansion method.37 On the contrary, sufficient T3 can promote podocyte redifferentiation, reduce hypertrophy, and improve the kidney structure.38 Secondly, hyperglycemia can lead to an increase of renal cell cytoplasmic glucose concentration, which leads to the activation of various signaling pathways and oxidative stress.39 However, T3 can reduce renal cortex collagen accumulation and glomerular matrix expansion in db/db mice, improve kidney damage in diabetic mice, increase renal PI3K activity, and reduce hyperglycemia. Besides, T3 can reduce renal transforming growth factor-β1 expression, promote insulin synthesis and release, enhance insulin signal transduction, and improve insulin resistance.11 Therefore, low T3 levels may indirectly aggravate DKD progression by concomitant hyperglycemia. Thirdly, it was confirmed in an animal study40 that overexpressed sirtuin 1 (SIRT1) in podocytes and renal tubular cells can reduce albuminuria and kidney damage. 3,5-diiodothyronine, the natural metabolite of T3 in the deiodination pathway, can prevent a significant decrease in the activity of SIRT1 in the kidneys of diabetic rats, and can inhibit renal tubular epithelium cell nuclear factor-κB acetylation and c-Jun N-terminal kinase phosphorylation, which ultimately play a role in protecting the kidneys. Fourthly, inflammation seriously interferes with the thyroid function in subjects with CKD. In these patients, an independent negative correlation between inflammatory cytokines (tumor necrosis factor-α, interleukin-6, and C-reactive protein) and FT3 was observed.41,42

Beyond doubt, similar results were obtained in both men and women in the subgroup analyses. More seriously, women with a low FT3 level had a maximum risk of DKD progression by 7.23 times. The clinical significance of the results was to set the low FT3 threshold to predict the prognosis of chronic kidney disease, which was less than 4.30 pmol/L for men and less than 3.99 pmol/L for women, respectively.

This study provides new evidence for the use of low FT3 in evaluating the prognosis of diabetic nephropathy. However, this study has some limitations. First, this was a cross-sectional study, and causality could not be established. Further prospective and longitudinal studies should be conducted. Second, the thyroid autoantibodies of the patients were not evaluated. Studies have shown that anti-thyroid peroxidase antibodies may be related to endothelial dysfunction and subsequent microalbuminuria.43 Third, the study population consisted of hospitalized patients with type 2 diabetes; hence, the results could not represent the overall population.

Conclusions

The results of this study indicated that low FT3 level was an independent risk factor for having DKD and DKD progression. Low FT3 levels, which are less than 4.30 pmol/L in men and less than 3.99 pmol/L in women will greatly increase the risk of kidney disease progression in patients with type 2 diabetes.

Data Sharing Statement

All data included in this study are available upon request by contact with the corresponding author.

Ethics Approval and Consent to Participate

The study protocol was approved by the ethics committee of the Third Hospital of Nanchang. The written informed consent was obtained from each subject. The study was carried out in conformity to the Declaration of Helsinki (as revised in 2013).

Author Contributions

ZY, PD, WL, JL, PT contributed to the conception and design of the study. ZY, WL, RN, XL (X. Lou), LW and KW participated in data collection. ZY and WL were responsible for data analysis and drafting manuscript. PD and XL (X. Lai) critically revised the manuscript. All authors contributed to data analysis, drafting or revising the article, have agreed on the journal to which the article was submitted, gave final approval of the version to be published, and agree to be accountable for all aspects of the work.

Funding

This work was supported by the National Natural Science Foundation of China [grant number 81760153, Recipient: Peng Duan], the Key Research and Development Programs by Science and Technology Department of Jiangxi Province [grant numbers 20171BBG70058, 20171ACH80002 and 20181BBG70014, Recipient: Zhi Yang, Ping Tu and Jiang Liu], the Science and Technology Support Project by Science and Technology Department of Nanchang City [grant number [2020]133, Recipient: Peng Duan].

Disclosure

The authors declare that they have no conflicts of interest for this work.

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