Effect of the administration of different forms of vitamin D on central blood pressure and aortic stiffness, and its implication in the reduction of albuminuria in chronic kidney disease

Almudena Martin-Romero , Jary Perelló-Martínez , Juan Carlos Hidalgo-Santiago , Alfredo Michan-Doña , Juan Bosco López Sáez , Pablo Gómez-Fernández
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The administration of nutritional vitD and the activator of the vitD receptor<span>, paricalcitol, may promote beneficial effects on vascular and renal function. The objective of this work was to study in subjects with </span></span>chronic kidney disease<span> (CKD) the effect that the administration of different forms of vitD has on arterial function and albuminuria, and the possible relationship between the modifications of these variables.</span></span></p></div><div><h3>Patients and methods</h3><p><span>We studied in 97 patients with CKD stages 3–4 the effect of the administration of cholecalciferol (group 2; n: 35) and paricalcitol (n: 31; group 3) on parameters derived from brachial blood pressure, aortic blood pressure<span> and on aortic stiffness studied using carotid-femoral pulse velocity (Vp</span></span><sub>c-f</sub>), and on albuminuria. A group of patients with stages 3–4 CKD who did not receive vitD therapy served as a control group (n: 31; group 1). 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A decrease in albuminuria ≥30% was observed more frequently in the groups treated with some form of vitD (group 2: 23%; group 3: 45%) than in the control group (13%) (p:0.03). The decrease in albuminuria observed in the groups treated with any of the forms of vitD did not vary when the baseline values ​​of the biochemical parameters of phosphorus-calcium metabolism, those of arterial function (PPb, PPc, Vp<strong><sub>c-f</sub></strong>) or its modifications were introduced as covariates. There was no significant correlation between changes in Vp<strong><sub>c-f</sub></strong><span> and albuminuria. In logistic regression, changes in arterial function parameters were also not explanatory for the ≥30% decrease in albuminuria.</span></p></div><div><h3>Conclusions</h3><p>In patients<span> with CKD stages 3–4, treated with RAS blockers and with residual albuminuria, the administration of or paricalcitol reduces brachial and aortic pulse pressures, and albuminuria. 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引用次数: 0

Abstract

Background and objectives

Vitamin D (vitD) participates in phospho-calcium metabolism and exerts multiple pleiotropic effects. There is tissue 1-α (OH)ase that converts 25-OH cholecalciferol (25 (OH) D) in calcitriol that exerts autocrine and paracrine effects. 25 (OH)D deficiency could limit these tissue effects of vitD. The administration of nutritional vitD and the activator of the vitD receptor, paricalcitol, may promote beneficial effects on vascular and renal function. The objective of this work was to study in subjects with chronic kidney disease (CKD) the effect that the administration of different forms of vitD has on arterial function and albuminuria, and the possible relationship between the modifications of these variables.

Patients and methods

We studied in 97 patients with CKD stages 3–4 the effect of the administration of cholecalciferol (group 2; n: 35) and paricalcitol (n: 31; group 3) on parameters derived from brachial blood pressure, aortic blood pressure and on aortic stiffness studied using carotid-femoral pulse velocity (Vpc-f), and on albuminuria. A group of patients with stages 3–4 CKD who did not receive vitD therapy served as a control group (n: 31; group 1). All parameters were studied at baseline and after the follow-up period which was 7 ± 2 months.

Results

In the baseline phase, no differences were observed between the groups in brachial systolic blood pressure (bSBP), central systolic blood pressure (SBP), brachial pulse pressure (bPP), and central pulse pressure (pCP) or in aortic stiffness that was increased in all groups with a baseline Vpc-f value of 10.5 (9.2–12.1) m/sec. The baseline albuminuria value in the grouped patients was 229 (43–876) mg/g (median (interquartile range)), with no differences between the groups.

Serum calcium and phosphorus increased significantly in those treated with cholecal-ciferol (native vitD) and paricalcitol (active vitD). Parathormone (PTH) values ​​decreased in those treated with paricalcitol. bPP and cPP decreased in all groups treated with native and active vitD. No significant changes in bPP and cPP were observed in the control group.

Vpc-f did not change significantly in any of the groups, although the variation was quantitatively greater in group 3 (11.2 ± 2 vs. 10.7 ± 1.6 (p:0.06)). No differences were observed in the changes in Vpc-f between the groups when adjusted to the baseline values ​​of estimated glomerular filtration rate (eGFR), albuminuria, PTH, vitD, brachial and central blood pressure parameters, and their changes with treatment.

Those who received treatment with native and active vitD presented a significant decrease in albuminuria of 17% (group 2) and 21% (group 3) compared to a 16% increase in the untreated group (group 1) (p:0 .01). A decrease in albuminuria ≥30% was observed more frequently in the groups treated with some form of vitD (group 2: 23%; group 3: 45%) than in the control group (13%) (p:0.03). The decrease in albuminuria observed in the groups treated with any of the forms of vitD did not vary when the baseline values ​​of the biochemical parameters of phosphorus-calcium metabolism, those of arterial function (PPb, PPc, Vpc-f) or its modifications were introduced as covariates. There was no significant correlation between changes in Vpc-f and albuminuria. In logistic regression, changes in arterial function parameters were also not explanatory for the ≥30% decrease in albuminuria.

Conclusions

In patients with CKD stages 3–4, treated with RAS blockers and with residual albuminuria, the administration of or paricalcitol reduces brachial and aortic pulse pressures, and albuminuria. The decrease in albuminuria does not seem to be mediated, at least not decisively, by changes in central hemodynamics or aortic stiffness.

不同形式维生素D对中心血压和主动脉硬度的影响及其对慢性肾病患者蛋白尿减少的影响
背景与目的维生素D (vitD)参与磷钙代谢,发挥多种多效作用。骨化三醇中有组织1-α (OH)酶转化25-OH胆骨化醇(25 (OH) D),发挥自分泌和旁分泌作用。缺乏25 (OH)D可以限制维生素D的这些组织作用。营养维生素d和维生素d受体的激活剂,特别是糖醇,可以促进血管和肾脏功能的有益作用。本研究的目的是研究慢性肾脏疾病(CKD)患者服用不同形式的维生素d对动脉功能和蛋白尿的影响,以及这些变量的改变之间可能的关系。患者和方法我们研究了97例CKD 3-4期患者给予胆钙化醇的效果(2组;N: 35)和paricalcitol (N: 31;第3组)肱血压、主动脉血压、颈-股动脉脉速(vc -f)研究的主动脉硬度参数和蛋白尿。一组未接受vitD治疗的3-4期CKD患者作为对照组(n: 31;1组)。在基线及随访(7±2个月)后进行各项指标的研究。结果基线期各组间肱收缩压(bSBP)、中心收缩压(SBP)、肱脉压(bPP)、中心脉压(pCP)均无差异,各组间主动脉硬度均升高,基线Vpc-f值为10.5 (9.2-12.1)m/sec。分组患者的基线蛋白尿值为229 (43-876)mg/g(中位数(四分位数范围)),组间无差异。血清钙和磷在使用胆-枸橼醇(天然维生素d)和部分枸橼醇(活性维生素d)治疗组显著升高。paricalcitol治疗组甲状旁腺激素(PTH)值降低。所有天然和活性维生素d治疗组的bPP和cPP均下降。对照组bPP、cPP无明显变化。Vpc-f在任何组中都没有显著变化,尽管在数量上变化在第3组更大(11.2±2比10.7±1.6 (p:0.06))。当调整到肾小球滤过率(eGFR)、蛋白尿、甲状旁腺素(PTH)、vitD、肱和中枢血压参数的基线值时,两组间Vpc-f的变化及其随治疗的变化无差异。与未治疗组(1组)增加16%相比,接受天然和活性维生素d治疗的患者蛋白尿显著减少17%(2组)和21%(3组)(p: 0.01)。在接受某种形式维生素d治疗的组中,蛋白尿下降≥30%的情况更为常见(组2:23%;第3组:45%)高于对照组(13%)(p:0.03)。当引入磷钙代谢的生化参数基线值、动脉功能(PPb、PPc、Vpc-f)或其修改值作为协变量时,任何形式的vitD治疗组观察到的蛋白尿减少都没有变化。Vpc-f变化与蛋白尿无显著相关性。在逻辑回归中,动脉功能参数的改变也不能解释蛋白尿减少≥30%的原因。结论在3-4期CKD患者中,接受RAS受体阻滞剂治疗并伴有残余蛋白尿,给予或特定的糖醇可降低肱动脉脉压和主动脉脉压以及蛋白尿。蛋白尿的减少似乎不是由中央血流动力学或主动脉僵硬的改变介导的,至少不是决定性的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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