[免疫抑制治疗作为移植后新发糖尿病的一个危险因素]

[Immunosuppressive therapy as a risk factor for new-onset diabetes after transplantation].

作者信息

Allazova S S, Novikova M S, Kotenko O N, Shilov E M

机构信息

Sechenov First Moscow State Medical University (Sechenov University).

Endocrinology Dispensary.

出版信息

Ter Arkh. 2020 Dec 15;92(12):137-141. doi: 10.26442/00403660.2020.12.200454.

DOI:10.26442/00403660.2020.12.200454

PMID:33720585

Abstract

AIM

To analyze the modes of immunosuppressive therapy as a risk factor for new-onset diabetes after transplantation (NODAT) in kidney recipients.

MATERIALS AND METHODS

The retrospective analysis included data from 1367 recipients (755 men and 612 women) who lived more than one year after NODAT and were observed at the Moscow City Nephrology Center from January 1989 to December 2018. NODAT was established for 178 (13%) patients based on criteria from the World Health Organization and the American Diabetes Association. The modes of immunosuppressive therapy using cyclosporin A (CSA), tacrolimus (Tac), mTOR inhibitors, glucocorticoids in patients with NODAT and without NODAT were evaluated. To assess the impact of risk factors, descriptive statistics methods were used, the odds ratio (OR) and the 95% confidence interval (CI) were calculated.

RESULTS

NODAT was diagnosed in 105 men and 73 women. The OR for men was 1.19 (95% CI 0.871.64), the OR for women was 0.84 (95% CI 0.611.15). At the time of transplantation, the average age of the kidney recipients in the NODAT group was higher than in the group without NODAT: 51 [43; 57] and 43 [32; 52] years, respectively (p=0.0001). Most patients with NODAT (82%) were older than 50 years, while in the group without NODAT, the proportion of patients of the same age was 48.5% (p=0.0001). Among patients without NODAT, transplantation of a kidney from a living donor was significantly more often compared with the group with NODAT+ (7.1% vs 1.1%;p=0.001). Among the recipients who received the regimen with CSA, diabetes developed in 75 (42.1%), those who received Tac in 102 (57.3%;p0.05). The chance (risk of development) of NODAT in patients receiving i-mTOR + Tac was 3.2 (95% CI 1.476.78;p=0.032), and for patients receiving i-mTOR + cyclosporin A, the chance of development NODAT was 1.95 (95% CI 0.884.35;p=0.044).

CONCLUSION

13% of recipients developed de novo kidney diabetes after allograft. Age at the time of allotransplantation, gender, as well as the use of tacrolimus in combination with i-mTOR are the most significant risk factors for the development of NODAT.

摘要

目的

分析免疫抑制治疗模式作为肾移植受者移植后新发糖尿病（NODAT）的危险因素。

材料与方法

回顾性分析纳入了1989年1月至2018年12月在莫斯科市肾脏病中心观察的1367例受者（755例男性和612例女性）的数据，这些受者在发生NODAT后存活超过1年。根据世界卫生组织和美国糖尿病协会的标准，178例（13%）患者被诊断为NODAT。评估了NODAT患者和非NODAT患者使用环孢素A（CSA）、他克莫司（Tac）、mTOR抑制剂、糖皮质激素的免疫抑制治疗模式。为评估危险因素的影响，采用描述性统计方法，计算比值比（OR）和95%置信区间（CI）。

结果

105例男性和73例女性被诊断为NODAT。男性的OR为1.19（95%CI 0.87-1.64），女性的OR为0.84（95%CI 0.61-1.15）。移植时，NODAT组肾移植受者的平均年龄高于非NODAT组：分别为51[43；57]岁和43[32；52]岁（p=0.0001）。大多数NODAT患者（82%）年龄超过50岁，而非NODAT组中同年龄患者的比例为48.5%（p=0.0001）。在非NODAT患者中，活体供肾移植的比例显著高于NODAT组（7.1%对1.1%；p=0.001）。在接受CSA方案的受者中，75例（42.1%）发生糖尿病，接受Tac的受者中有102例（57.3%；p<0.05）。接受i-mTOR+Tac的患者发生NODAT的几率（发生风险）为3.2（95%CI 1.47-6.78；p=0.032），接受i-mTOR+环孢素A的患者发生NODAT的几率为1.95（95%CI 0.88-4.35；p=0.044）。