HDL-associated vitamin D binding protein levels are inversely associated with necrotic plaque burden in psoriasis

IF 1.4 Q3 PERIPHERAL VASCULAR DISEASE Atherosclerosis plus Pub Date : 2024-12-13 DOI:10.1016/j.athplu.2024.12.002

M.P. Playford , H. Li , A.K. Dey , E.M. Florida , H.L. Teague , S.M. Gordon , N.N. Mehta

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Abstract

Background and aims

Vitamin D binding protein (DBP) serves a dual function as a vitamin D carrier and actin scavenger. Free DBP is present in high concentrations in serum, while a smaller pool is bound to lipoproteins like HDL and VLDL. The role of DBP's interaction with lipoproteins remains unclear. Given that HDL has been proposed to have both atheroprotective and anti-inflammatory properties, we sought to compare whether HDL-associated DBP and/or total serum DBP could serve as useful biomarkers for assessing disease severity in psoriasis and cardiovascular disease.

Methods

Psoriasis (PSO) patients (N = 83), which were part of a prospective, observational cohort and non-psoriasis (non-PSO) subjects (n = 35) underwent blood collection for HDL purification by liquid chromatography and CCTA scans to assess coronary plaque burden. Serum and HDL-bound DBP levels were measured by ELISA.

Results

The psoriasis cohort was middle-aged (mean ± IQR: 50 (38–59), predominantly male (n = 55, 66 %) and had moderate-to-severe skin disease [psoriasis area severity index score, PASI score, med (IQR): 9.6 (6–18.3)]. Consistent with our previous reports, PSO patients had significantly higher Framingham Risk Score (FRS), high sensitivity C-reactive protein (hs-CRP), Body Mass Index (BMI), insulin resistance (HOMA-IR) and total coronary plaque burden, driven by the rupture-prone non-calcified necrotic core. However, while the concentration of serum DBP (S-DBP) between PSO and non-PSO was unchanged (PSO: 177.80 (125.77–250.99) vs non-PSO: 177.74 (104.32–254.04), the concentration of DBP associated with HDL (HDL-DBP) was decreased in psoriatics (PSO μg/ml: 1.38 (0.64–2.75) vs non-PSO: 1.72 (1.18–3.90). Although both S-DBP and HDL-DBP levels showed inverse correlations with a measure of skin disease severity (PASI) (S-DBP, Rho = −0.022 vs HDL-DBP, Rho = −113), only HDL-DBP exhibited an inverse relationship with necrotic plaque burden [Rho −0.226, p = 0.085 vs S-DBP (0.041, p = 0.76)]. This relationship was strengthened after adjusting for traditional cardiovascular risk factors such as age and sex (β = −0.237, p = 0.045), FRS (β = −0.295, p = 0.033) and including biological treatment and HDL-cholesterol (β = −0.213, p = 0.048).

Conclusions

In conclusion, we found HDL-DBP levels may better capture the severity of psoriatic disease and association with cardiovascular risk factors than S-DBP.

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高密度脂蛋白相关的维生素D结合蛋白水平与牛皮癣坏死斑块负荷呈负相关。

背景与目的：维生素D结合蛋白（DBP）具有维生素D载体和肌动蛋白清除剂的双重功能。游离DBP在血清中以高浓度存在，而较小的池与HDL和VLDL等脂蛋白结合。DBP与脂蛋白相互作用的作用尚不清楚。鉴于HDL已被提出具有动脉粥样硬化保护和抗炎特性，我们试图比较HDL相关舒张压和/或总血清舒张压是否可以作为评估牛皮癣和心血管疾病严重程度的有用生物标志物。方法：作为前瞻性观察队列的一部分，银屑病（PSO）患者（N = 83）和非银屑病（non-PSO）受试者（N = 35）采集血液，通过液相色谱和CCTA扫描进行HDL纯化，以评估冠状动脉斑块负担。ELISA法测定血清及高密度脂蛋白结合DBP水平。结果：银屑病队列为中年人（平均±IQR: 50(38-59)），以男性为主（n = 55,66 %），患有中重度皮肤病[银屑病区域严重程度指数评分，PASI评分，med (IQR): 9.6(6-18.3)]。与我们之前的报道一致，PSO患者有明显更高的弗雷明汉风险评分（FRS）、高敏c反应蛋白（hs-CRP）、体重指数（BMI）、胰岛素抵抗（HOMA-IR）和总冠状动脉斑块负担，这是由易破裂的非钙化坏死核心驱动的。然而，银屑病患者血清DBP （S-DBP）与非PSO之间的差异无显著性(PSO: 177.80 (125.77-250.99) vs非PSO: 177.74(104.32-254.04)，而与HDL相关的DBP （HDL-DBP）浓度在银屑病患者中有所降低(PSO μg/ml: 1.38 （0.64-2.75) vs非PSO: 1.72(1.18-3.90)）。尽管S-DBP和HDL-DBP水平均与皮肤病严重程度（PASI）呈负相关（S-DBP, Rho = -0.022 vs HDL-DBP, Rho = -113），但只有HDL-DBP与坏死斑块负担呈负相关[Rho -0.226, p = 0.085 vs S-DBP (0.041, p = 0.76)]。在校正了传统的心血管危险因素如年龄和性别（β = -0.237, p = 0.045）、FRS （β = -0.295, p = 0.033）以及生物治疗和高密度脂蛋白胆固醇（β = -0.213, p = 0.048）后，这种关系得到加强。结论：总之，我们发现HDL-DBP水平比S-DBP水平更能反映银屑病的严重程度及其与心血管危险因素的关系。

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