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1 型糖尿病与早期糖尿病肾病中凋亡、临床和实验室参数分析:聚类及潜在分组评估以寻求更多治疗干预。

Analysis of Apoptotic, Clinical, and Laboratory Parameters in Type 1 Diabetes and Early Diabetic Nephropathy: Clustering and Potential Groups Evaluation for Additional Therapeutic Interventions.

机构信息

Bogomolets National Medical University, Department of Pediatrics, Kyiv, Ukraine

出版信息

J Clin Res Pediatr Endocrinol. 2022 Aug 25;14(3):313-323. doi: 10.4274/jcrpe.galenos.2022.2022-1-21. Epub 2022 May 31.

Abstract

OBJECTIVE

Type 1 diabetes (T1D) is one of the most prevalent chronic illnesses diagnosed in childhood. Diabetic nephropathy (DN) is one of the commonest complication of T1D. Therefore the development of specific treatment that arrests progression of DN based on an individual approach would be beneficial. Analysis of criteria of apoptosis, and clinical, and laboratory characteristics in T1D and early DN in the framework of clustering may be helpful in the identification of potential groups for additional therapeutic interventions.

METHODS

A survey of 104 children (62 males, 42 females) with T1D and DN aged 2 to 17 years in the Endocrinology unit of Clinical Pediatric Hospital No 6 (Kyiv, Ukraine) was performed. Clinical data (age, gender, disease duration, blood pressure), conventional laboratory markers including complete blood count, serum cholesterol, hemoglobin A1c (Hb1Ac), glomerular filtration rate (GFR), and microalbuminurea (MAU), and markers of apoptosis (BcL-xL, caspase-3) and transcriptional factor HIF-1alfa were analyzed.

RESULTS

A cluster group in T1D children was characterized by somewhat higher number of platelets (PLT) - 344.9±7.88·10/L, increased GFR up to hyperfiltration level 124.5±8.86 mL/min/1.73 m and decreased anti-apoptotic defense - BcL-xL 144.9±2.35 a.u. was identified. Children with DN may be divided into three groups based on age, body mass index, systolic blood pressure, PLT count, erthyrocyte sedimentation rate, albumin/globulin ratio, serum cholesterol, Hb1Ac, number of diabetic ketoacidosis (DKA) episodes, GFR, MAU, HIF-1alfa, Bcl-xL, caspase-3 levels. Among children with early DN a cluster characterized by the following parameters was found: PLT count - 311.±12.05·10/L, frequency of DKA episodes - 4.82±0.26 episodes/year, MAU - 112.0±10.12 mm/24 h, HIF - 200.5±3.49 a.u., BcL-xL - 128.8±3.1 a.u., and caspase-3 - 159.6±5.5 a.u.

CONCLUSION

Thus, we hypothesize that T1D pediatric patients with increased PLT count, hyperfiltration and reduced anti-apoptotic defense may represent a group for additional therapeutic interventions, such as antioxidants along with stndard therapies to achieve optimal glycemic control. Within the DN group there was a sub-group with somewhat increased PLT count, high frequency of DKA episodes/year, high MAU, prominent increase in HIF level, prominent disturbances in apoptosis controlling factors BcL-xL and caspase-3 tht may require additional therapeutic interventions, again including antioxidants, but may additionally benefit from anti-apoptotic effectors along with optimal glycemic control, and management of hypertension and albuminuria.

摘要

目的

1 型糖尿病(T1D)是儿童期最常见的慢性病之一。糖尿病肾病(DN)是 T1D 最常见的并发症之一。因此,开发基于个体化治疗的特异性治疗方法来阻止 DN 的进展将是有益的。在聚类的框架内分析细胞凋亡的标准以及 T1D 和早期 DN 的临床和实验室特征,可能有助于识别潜在的治疗干预群体。

方法

对基辅 6 号临床儿科医院内分泌科 104 名年龄在 2 至 17 岁的 T1D 和 DN 儿童(男 62 名,女 42 名)进行了调查。临床数据(年龄、性别、疾病持续时间、血压)、常规实验室标志物包括全血细胞计数、血清胆固醇、糖化血红蛋白(Hb1Ac)、肾小球滤过率(GFR)和微量白蛋白尿(MAU)以及凋亡标志物(BcL-xL、caspase-3)和转录因子 HIF-1alfa 进行了分析。

结果

在 T1D 儿童中,聚类组的血小板(PLT)计数略高,为 344.9±7.88·10/L,GFR 升高至高滤过水平 124.5±8.86 mL/min/1.73 m,抗凋亡防御降低,BcL-xL 为 144.9±2.35 a.u.。DN 患儿可根据年龄、体重指数、收缩压、PLT 计数、红细胞沉降率、白蛋白/球蛋白比值、血清胆固醇、Hb1Ac、糖尿病酮症酸中毒(DKA)发作次数、GFR、MAU、HIF-1alfa、Bcl-xL、caspase-3 水平分为三组。在早期 DN 患儿中,发现了一个具有以下参数的聚类:PLT 计数为 311.±12.05·10/L,DKA 发作频率为 4.82±0.26 次/年,MAU 为 112.0±10.12 mm/24 h,HIF 为 200.5±3.49 a.u.,BcL-xL 为 128.8±3.1 a.u.,caspase-3 为 159.6±5.5 a.u.。

结论

因此,我们假设 T1D 患儿血小板计数升高、高滤过和抗凋亡防御降低可能代表需要额外治疗干预的群体,例如抗氧化剂与标准治疗相结合,以实现最佳血糖控制。在 DN 组中,存在一个亚组,其血小板计数略有升高,DKA 发作次数/年较高,MAU 较高,HIF 水平显著升高,凋亡调控因子 BcL-xL 和 caspase-3 明显紊乱,可能需要额外的治疗干预,再次包括抗氧化剂,但可能额外受益于抗凋亡效应物以及最佳血糖控制和高血压和白蛋白尿的管理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/520d/9422907/f69bdf1acd0e/JCRPE-14-313-g1.jpg

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