Blockade of sodium-glucose co-transporters improves peritoneal ultrafiltration in uraemic rodent models.

IF 2.7 3区 医学 Q2 UROLOGY & NEPHROLOGY Peritoneal Dialysis International Pub Date : 2024-01-01 Epub Date: 2023-05-02 DOI:10.1177/08968608231165865
Marina Vorobiov, Boris Rogachev, Reut Riff, Cidio Chaimowitz, Endre Z Neulander, Anna Basok, Alla Shnaider, Amos Douvdevani, Yosef-Shmuel Haviv
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Abstract

Background: The most used PD fluids contain glucose as a primary osmotic agent. Glucose peritoneal absorption during dwell decreases the osmotic gradient of peritoneal fluids and causes undesirable metabolic consequences. Inhibitors of sodium-glucose co-transporter (SGLT) type 2 are wildly used for the treatment of diabetes, heart and kidney failure. Previous attempts to use SGLT2 blockers in experimental peritoneal dialysis yielded contrasting results. We studied whether peritoneal SGLTs blockade may improve ultrafiltration (UF) via partial inhibition of glucose uptake from dialysis fluids.

Methods: Kidney failure was induced in mice and rats by bilateral ureteral ligation, and dwell was performed by injection of glucose-containing dialysis fluids. The effect of SGLT inhibitors on glucose absorption during fluid dwell and UF was measured in vivo.

Results: Diffusion of glucose from dialysis fluid into the blood appeared to be sodium-dependent, and blockade of SGLTs by phlorizin and sotagliflozin attenuated blood glucose increment thereby decreasing fluid absorption. Specific SGLT2 inhibitors failed to reduce glucose and fluid absorption from the peritoneal cavity in a rodent kidney failure model.

Conclusions: Our study suggests that peritoneal non-type 2 SGLTs facilitate glucose diffusion from dialysis solutions, and we propose that limiting glucose reabsorption by specific SGLT inhibitors may emerge as a novel strategy in PD treatment to enhance UF and mitigate the deleterious effects of hyperglycaemia.

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阻断钠-葡萄糖协同转运体可改善尿毒症啮齿动物模型的腹膜超滤。
背景:最常用的腹膜透析液含有作为主要渗透剂的葡萄糖。腹腔在停留期间吸收葡萄糖会降低腹腔液的渗透梯度,并导致不良的代谢后果。钠-葡萄糖协同转运体(SGLT)2 型抑制剂被广泛用于治疗糖尿病、心脏和肾衰竭。以前曾尝试在实验性腹膜透析中使用 SGLT2 阻断剂,结果却截然不同。我们研究了腹膜 SGLTs 阻断剂是否可以通过部分抑制透析液中葡萄糖的吸收来改善超滤(UF):方法:通过双侧输尿管结扎诱导小鼠和大鼠肾衰竭,并通过注射含葡萄糖的透析液进行透析。在体内测量 SGLT 抑制剂对透析液停留和超滤过程中葡萄糖吸收的影响:结果:葡萄糖从透析液中扩散到血液中似乎是钠依赖性的,而通过氯利嗪和索他利氟嗪阻断 SGLTs 可降低血糖升高,从而减少透析液的吸收。在啮齿动物肾衰竭模型中,特异性 SGLT2 抑制剂未能减少腹腔对葡萄糖和液体的吸收:我们的研究表明,腹膜非 2 型 SGLTs 可促进透析液中葡萄糖的扩散。我们建议,通过特异性 SGLT 抑制剂限制葡萄糖重吸收可能会成为治疗 PD 的一种新策略,以提高 UF 值并减轻高血糖的有害影响。
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来源期刊
Peritoneal Dialysis International
Peritoneal Dialysis International 医学-泌尿学与肾脏学
CiteScore
6.00
自引率
17.90%
发文量
69
审稿时长
6-12 weeks
期刊介绍: Peritoneal Dialysis International (PDI) is an international publication dedicated to peritoneal dialysis. PDI welcomes original contributions dealing with all aspects of peritoneal dialysis from scientists working in the peritoneal dialysis field around the world. Peritoneal Dialysis International is included in Index Medicus and indexed in Current Contents/Clinical Practice, the Science Citation Index, and Excerpta Medica (Nephrology/Urology Core Journal). It is also abstracted and indexed in Chemical Abstracts (CA), as well as being indexed in Embase as a priority journal.
期刊最新文献
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