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轻度再喂养综合征模型中无机磷酸盐浓度与葡萄糖代谢之间的相互作用。

Interaction between inorganic phosphate concentration and glucose metabolism in mild refeeding syndrome model.

作者信息

Tanaka Sarasa, Kawamura Hiromi, Imoto Yumeno, Urata Yuri, Hontama Sayuka, Oda Momoko, Sakaue Motoyoshi, Ito Mikiko

机构信息

Graduate School of Human Science and Environment, University of Hyogo, 1-1-12 Shinzaike-Honcho, Himeji, Hyogo 670-0092, Japan.

School of Human Science and Environment, University of Hyogo, 1-1-12 Shinzaike-Honcho, Himeji, Hyogo 670-0092, Japan.

出版信息

J Clin Biochem Nutr. 2023 Mar;72(2):126-131. doi: 10.3164/jcbn.22-99. Epub 2023 Feb 8.

Abstract

Refeeding syndrome is a major clinical problem that leads to fatal complications in patients suffering from malnutrition. Hypophosphatemia inevitably is observed at the onset of refeeding syndrome and therefore is monitored during refeeding; however, the causes of metabolic changes in phosphate concentration during refeeding remain poorly understood. In a previous study, we established a refeeding syndrome model employing total parenteral nutrition with insulin-induced hypophosphatemia, but the symptoms were severe and the metabolic mechanisms in this model may not have been representative of clinical conditions. Therefore, we established a new animal model of mild refeeding syndrome by using a shorter fasting period followed by a single refeeding. These mild refeeding syndrome-model rats exhibited hypophosphatemia without increases in urinary phosphate excretion. Interestingly, administration of the combination of phosphate and insulin during refeeding promoted insulin secretion during refeeding. This model implies that Pi may directly promote insulin secretion in pancreatic cells. These results clarify the interaction between phosphate and glucose metabolism pancreatic cells during refeeding syndrome in a mild refeeding syndrome model.

摘要

再喂养综合征是一个主要的临床问题,会导致营养不良患者出现致命并发症。再喂养综合征开始时不可避免地会出现低磷血症,因此在再喂养期间会对其进行监测;然而,再喂养期间磷酸盐浓度代谢变化的原因仍知之甚少。在之前的一项研究中,我们建立了一种采用全胃肠外营养并伴有胰岛素诱导的低磷血症的再喂养综合征模型,但症状严重,且该模型中的代谢机制可能并不代表临床情况。因此,我们通过缩短禁食期然后进行单次再喂养,建立了一种轻度再喂养综合征的新动物模型。这些轻度再喂养综合征模型大鼠表现出低磷血症,而尿磷排泄并未增加。有趣的是,再喂养期间给予磷酸盐和胰岛素的组合可促进再喂养期间的胰岛素分泌。该模型表明,无机磷可能直接促进胰腺细胞中的胰岛素分泌。这些结果阐明了轻度再喂养综合征模型中再喂养综合征期间磷酸盐与胰腺细胞葡萄糖代谢之间的相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8868/10017325/c130c2dd6ddf/jcbn22-99f01.jpg

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