考虑到是否存在1型糖尿病诊断的第5透析期慢性肾病患者的矿物质和骨骼紊乱的结构

IF 0.7 Q4 ENDOCRINOLOGY & METABOLISM
Diabetes Mellitus Pub Date : 2022-12-28 DOI:10.14341/dm12958
I. Maganeva, A. Eremkina, A. Miliutina, S. Martynov, A. Severina, R. Salimkhanov, M. I. Evloeva, M. Shamkhalova, M. Shestakova, N. Mokrysheva
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引用次数: 0

摘要

背景:在终末期CKD患者中,接受肾脏替代疗法(RRT)和程序性血液透析(HD),并发症的严重程度与代谢紊乱有关:尿毒症毒素积累、肾源性贫血、继发性甲状旁腺功能亢进(SHPT)、骨骼外钙化、清除和激素分泌节律受损。目的:在考虑是否存在糖尿病的情况下,评价接受RRT合并HD患者在血液透析前后的主要生化和激素指标以及矿物性骨病(MBD)的表现。材料和方法:我们将所有接受RRT的HD患者分为两组:#1 (n=24) - DM患者,#2 (n=16) -非DM患者。所有患者在HD之前和之后都进行了血液分析。使用Statistica 13 (StatSoft, USA)进行数据分析。p0.05认为模型具有预后显著性;1组的高磷血症完全消除,2组的高磷血症持续存在7% (p=0.417)。在HD治疗前,1组的RAGE、胰高血糖素、免疫反应性胰岛素(IRI)、皮质醇和葡萄糖水平显著高于HD治疗后(p<0.05)。2组HD后胰高血糖素、IRI、皮质醇水平显著降低(p<0.05), 3-硝基酪氨酸(3-HT)水平显著升高(p=0.026)。在1组中,ECHO显示的心脏瓣膜纤维钙化症和超声多普里图显示的下肢动脉钙化比2组更常见(分别为42%比25%,p<0.001和75%比37.5%,p=0.018)。(χ2))。两组的压缩性骨折发生率相同(60%)。骨密度(BMD)下降至骨质减少水平在1组中更为常见(50%对18.8%),骨质疏松症在2组中更为常见(68.8%对33.3%)(p<0.001, χ2)。结论:1组PTH水平低可能反映了糖尿病对钙磷代谢的影响。由于糖尿病固有的一些代谢因素,糖尿病患者患肾性骨营养不良的风险增加,且骨转化率低。同时,HD过程中磷和钙指标的动态相似。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The structure of mineral and bone disorders in patients with сhronic kidney disease of the 5th dialysis stage, taking into account the presence or absence of a diagnosis of type 1 diabetes mellitus
BACKGROUND: In patients with end-stage CKD, receiving renal replacement therapy (RRT) with programmed hemodialysis (HD), the severity of complications is associated with metabolic disturbances: accumulation of uremic toxins, nephrogenic anemia, secondary hyperparathyroidism (SHPT), extraskeletal calcification, impaired clearance and rhythm of hormone secretion.AIM: To evaluate the main biochemical and hormonal parameters, and manifestations of mineral bone disease (MBD) in patients receiving RRT with HD, before and after hemodialysis, taking into account the presence or absence of diabetes mellitus.MATERIALS AND METHODS: We divided all patients receiving RRT with HD in two groups: #1 (n=24) — patients with DM, #2 (n=16) — patients without DM. All of them had their blood analyzed before and immediately after the HD. Data analysis was performed with the Statistica 13 (StatSoft, USA). A prognostically significant model was considered at p<0.05.RESULTS: The level of iPTH, both at baseline and after HD, was lower in group #1 (p<0.001). The level of alkaline phosphatase (AP) was significantly higher in group #2 (p=0.012). In both groups before HD, a high incidence of hypocalcemia was detected (according to albumin-corrected calcium in group #1 in 58.3%, in group #2 in 43.7% of cases, p = 0.366) and hyperphosphatemia (in 66.7% and in 43 .7% of cases, respectively, p=0.151). Hypocalcemia after HD in group #1 persisted in 14%, in group #2 — in 20% of cases (p>0.05); hyperphosphatemia in group #1 was completely leveled, in group #2 it persisted in 7% of cases (p=0.417). Prior to the HD session, group #1 had significantly higher levels of RAGE, glucagon, immunoreactive insulin (IRI), cortisol, and glucose than after the HD session (p<0.05). In group #2, after HD, the levels of glucagon, IRI and cortisol significantly decreased (p<0.05), and the level of 3-nitrotyrosine (3-HT) increased significantly (p=0.026). In group #1, fibrocalcinosis of the heart valves according to ECHO and calcification of the arteries of the lower extremities according to ultrasonic doplerography were more common than in group #2 (42% vs 25%, p<0.001 and 75% vs 37.5%, p=0.018, respectively). (χ2)). Compression fractures occurred with the same frequency in both groups (60%). A decrease in bone mineral density (BMD) to the level of osteopenia was noted more often in group #1 (50% vs 18.8%), and osteoporosis was more common in group #2 (68.8% vs 33.3%) (p<0.001, χ2).CONCLUSION: The low level of PTH in group #1 may reflect the effect of diabetes on calcium-phosphorus metabolism. Patients with DM have an increased risk of renal osteodystrophy with a low bone turnover because of a number of metabolic factors inherent in diabetes. At the same time, the dynamics of phosphorus and calcium indicators during the HD procedure were similar.
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来源期刊
Diabetes Mellitus
Diabetes Mellitus ENDOCRINOLOGY & METABOLISM-
CiteScore
1.90
自引率
40.00%
发文量
61
审稿时长
7 weeks
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