Dongdong Luo, Chenxi Zhang, Bingrui Gao, Deping Wang, Zhaoying Chen, Kan Chen, Bojuan Li, Song Leng, Jing Li
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引用次数: 0
摘要
目的:甲状腺自身免疫(TAI)患者中普遍存在维生素D(VitD)缺乏症。本研究旨在探讨低VitD2或VitD3是否可能导致甲状腺功能正常的男性患者患上甲状腺自身免疫病(TAI):从2021年大连医科大学附属第二医院医疗保健项目的参与者中招募了2882名甲状腺功能正常的男性石油工人,同时检测了他们的血清VitD水平、甲状腺功能和自身抗体滴度。其中,2587 人(89.8%)在 2022 年接受了第二次健康随访。血清维生素D包括25(OH)D2(VitD2)和25(OH)D3(VitD3)水平通过液相色谱-串联质谱法进行检测。采用化学发光免疫测定法对甲状腺功能和自身抗体滴度进行量化:结果:患有 TAI 的男性甲状腺功能正常者(n = 195)的血清中 VitD 和 VitD3 水平明显低于非 TAI 男性(n = 2687,P基于横断面和前瞻性调查,我们的研究结果进一步表明,VDD可能是TAI发生的一个独立风险因素。此外,在甲状腺功能正常的男性人群中,后者可能与缺乏 VitD3 而非 VitD2 有关,但相关机制有待深入探讨。研究注册:大连健康管理队列(DHMC)ChiCTR2300073363。
The development of thyroid autoimmunity is potentially associated with the deficiency of vitamin D3 rather than vitamin D2 in euthyroid men.
Objective: Vitamin D(VitD) deficiency has been found prevalent among patients with thyroid autoimmunity (TAI). This study aimed to investigate whether low VitD2 or VitD3 potentially contributed to the development of TAI in euthyroid male patients, which had not been reported before.
Methods: A total of 2882 euthyroid male petroleum workers were recruited from those participants in the healthcare program at the second affiliated hospital of Dalian Medical University in 2021, whose serum VitD levels, thyroid functions, and autoantibody titers were all examined at the same time. Among them, 2587 (89.8%) individuals received the second health follow-up in 2022. Serum VitD including 25(OH)D2 (VitD2) and 25(OH)D3 (VitD3) levels were detected by liquid chromatography-tandem mass spectrometry. Thyroid functions and autoantibody titers were quantified using chemiluminescent immunoassays.
Results: The serum levels of VitD and VitD3 were pronouncedly lower in the male euthyroid subjects with TAI (n = 195) than those non-TAI men (n = 2687, P < 0.05), whereas serum VitD2 was not significantly different based on the data from the initial investigation in 2021. The prevalence of subjects with TAI among the total male euthyroid subjects with TAI population was markedly increased with the decreasing levels of serum VitD and VitD3, respectively (P for trend < 0.05), but not significantly changed with that of serum VitD2. The binary logistic regression analysis revealed that either the deficiency of VitD (serum VitD < 20 ng/mL, VDD) or low VitD3 level was an independent risk factor for the development of TAI, which had been further demonstrated by the follow-up observation in 2022. Among the non-TAI men in 2021, 6.52% (n = 157) individuals became TAI patients after a one-year follow-up, and their serum VitD and VitD3 levels both exhibited significantly more reduction as compared with those of the remained non-TAI ones in 2022. More of those with VDD developed TAI than the non-VDD ones did in 2022 (8.5% vs. 5.6%, P<0.05). Additionally, the change in serum VitD over the two years was more strongly correlated with serum VitD3 (rs = 0.971, P < 0.001) when compared with that of VitD2 (rs = 0.085, P < 0.001) in the whole euthyroid male population.
Conclusion: Based on the cross-sectional and prospective investigations, our findings further indicate that VDD may be an independent risk factor for TAI development. Moreover, the latter is potentially associated with the deficiency of VitD3 rather than VitD2 in the euthyroid male population although the related mechanisms await in-depth exploration. Our findings also suggest that VitD3 supplementation might provide more potential benefits than VitD2 among VDD men in terms of preventing TAI development.
Study registration: the Dalian Health Management Cohort (DHMC) ChiCTR2300073363.