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将空腹血糖与餐后血糖作为降低升高的糖化血红蛋白的治疗靶点

FASTING VERSUS POSTPRANDIAL HYPERGLYCEMIA AS A TREATMENT TARGET TO LOWER ELEVATED HEMOGLOBIN A1C.

作者信息

Shaefer Charles, Reid Timothy, Vlajnic Aleksandra, Zhou Rong, DiGenio Andres

出版信息

Endocr Pract. 2015 Dec;21(12):1323-32. doi: 10.4158/EP14498.OR. Epub 2015 Aug 26.

DOI:10.4158/EP14498.OR
PMID:26307902
Abstract

OBJECTIVE

Postprandial hyperglycemia (PPHG) may need addressing when glycemic control cannot be maintained in patients with type 2 diabetes mellitus. We investigated whether glycated hemoglobin A1c (A1c) levels ≥7.0% can indicate postprandial defects warranting prandial therapy after optimized basal insulin therapy.

METHODS

From 6 clinical trials of insulin glargine treatment, data were pooled from 496 patients with A1c ≥7.0% after 24 weeks. Patient characteristics and clinical outcomes were summarized according to fasting plasma glucose (FPG) target achievement (<130 mg/dL), postprandial blood glucose (PPBG) levels, and PPBG increments (ΔPPBG). Basal and postprandial contributions to hyperglycemia were determined.

RESULTS

After 24 weeks of insulin glargine titration, A1c change from baseline was greater in patients with FPG <130 mg/dL versus ≥130 mg/dL (-1.35% versus -1.11%, respectively; P = .0275), but with increased confirmed hypoglycemia rates (blood glucose <70 mg/dL; 4.06 events/patient-year versus 3.31 events/patient-year; P = .0170). However, increased severe hypoglycemia rates were observed in patients with FPG ≥130 mg/dL. At week 24, postprandial contributions to hyperglycemia increased (>60% regardless of PPBG). Patients with high FPG had lower, but substantial, relative postprandial contributions versus patients achieving FPG target. A similar pattern was observed according to whether patients had a ΔPPBG ≥50 mg/dL after any meal.

CONCLUSION

After optimized basal insulin therapy, elevated A1c is the most effective indicator of residual PPHG, regardless of existent FPG or PPBG. When confronted with an uncontrolled A1c after reasonable titration of basal insulin, clinicians should be aware of probable postprandial contributions to hyperglycemia and consider prandial therapy.

摘要

目的

对于2型糖尿病患者,若血糖控制不佳,餐后高血糖(PPHG)可能需要加以处理。我们研究了糖化血红蛋白A1c(A1c)水平≥7.0%是否能表明在基础胰岛素治疗优化后存在需要进行餐时治疗的餐后缺陷。

方法

从6项甘精胰岛素治疗的临床试验中,汇总了24周后A1c≥7.0%的496例患者的数据。根据空腹血糖(FPG)目标达成情况(<130 mg/dL)、餐后血糖(PPBG)水平以及PPBG增加值(ΔPPBG)对患者特征和临床结局进行总结。确定基础和餐时因素对高血糖的影响。

结果

甘精胰岛素滴定24周后,FPG<130 mg/dL的患者A1c较基线的变化大于FPG≥130 mg/dL的患者(分别为-1.35%对-1.11%;P = 0.0275),但确诊低血糖发生率增加(血糖<70 mg/dL;4.06次事件/患者年对3.31次事件/患者年;P = 0.0170)。然而,FPG≥130 mg/dL的患者严重低血糖发生率增加。在第24周时,餐时因素对高血糖的影响增加(无论PPBG如何均>60%)。FPG高的患者相对餐时因素的影响较低但仍很显著,与达到FPG目标的患者相比。根据患者在任何一餐后ΔPPBG≥50 mg/dL与否,观察到类似模式。

结论

在基础胰岛素治疗优化后,无论现有FPG或PPBG如何,A1c升高是残余PPHG的最有效指标。当在合理滴定基础胰岛素后面对未控制的A1c时,临床医生应意识到餐时因素对高血糖的可能影响并考虑进行餐时治疗。

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