首页> 外文期刊>Pfluegers Archiv: European Journal of Physiology >Physiological regulation of phosphate by vitamin D, parathyroid hormone (PTH) and phosphate (Pi)
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Physiological regulation of phosphate by vitamin D, parathyroid hormone (PTH) and phosphate (Pi)

机译:维生素D,甲状旁腺激素(PTH)和磷酸盐(PI)的生理调节

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Inorganic phosphate (Pi) is an abundant element in the body and is essential for a wide variety of key biological processes. It plays an essential role in cellular energy metabolism and cell signalling, e.g. adenosine and guanosine triphosphates (ATP, GTP), and in the composition of phospholipid membranes and bone, and is an integral part of DNA and RNA. It is an important buffer in blood and urine and contributes to normal acid-base balance. Given its widespread role in almost every molecular and cellular function, changes in serum Pi levels and balance can have important and untoward effects. Pi homoeostasis is maintained by a counterbalance between dietary Pi absorption by the gut, mobilisation from bone and renal excretion. Approximately 85% of total body Pi is present in bone and only 1% is present as free Pi in extracellular fluids. In humans, extracellular concentrations of inorganic Pi vary between 0.8 and 1.2mM, and in plasma or serum Pi exists in both its monovalent and divalent forms (H2PO4- and HPO42-). In the intestine, approximately 30% of Pi absorption is vitamin D regulated and dependent. To help maintain Pi balance, reabsorption of filtered Pi along the renal proximal tubule (PT) is via the NaPi-IIa and NaPi-IIc Na+-coupled Pi cotransporters, with a smaller contribution from the PiT-2 transporters. Endocrine factors, including, vitamin D and parathyroid hormone (PTH), as well as newer factors such as fibroblast growth factor (FGF)-23 and its coreceptor -klotho, are intimately involved in the control of Pi homeostasis. A tight regulation of Pi is critical, since hyperphosphataemia is associated with increased cardiovascular morbidity in chronic kidney disease (CKD) and hypophosphataemia with rickets and growth retardation. This short review considers the control of Pi balance by vitamin D, PTH and Pi itself, with an emphasis on the insights gained from human genetic disorders and genetically modified mouse models.
机译:无机磷酸盐(PI)是体内丰富的元素,对于各种关键生物过程至关重要。它在细胞能量代谢和细胞信号中起着重要作用,例如,腺苷和鸟苷三磷酸(ATP,GTP),以及磷脂膜和骨的组成,是DNA和RNA的一部分。它是血液和尿液中的一个重要缓冲液,有助于正常的酸碱平衡。鉴于其几乎每种分子和细胞功能的广泛作用,血清PI水平和平衡的变化可能具有重要且不提供的效果。 PI同性化通过肠道膳食PI之间的抵抗,从骨骼和肾脏排泄中培养。大约85%的总体Pi存在于骨中,只有1%作为细胞外液中的游离PI存在。在人类中,无机PI的细胞外浓度在0.8和1.2mm之间变化,并且在其单价和二价形式(H2PO4-和HPO 42-)中存在血浆或血清PI。在肠道中,大约30%的PI吸收是维生素D调节和依赖性。为了帮助维持PI平衡,沿着肾近端小管(PT)的过滤PI的重吸收通过NaPi-Iia和Napi-IIC Na + -coupled Pi Cot转发器,具有较小的坑2转运蛋白的贡献。内分泌因子,包括维生素D和甲状旁腺激素(PTH)以及诸如成纤维细胞生长因子(FGF)-23及其Coreceptor -colepor -klotho等较新因素,依赖于PISoosoTasis的控制。 Pi的紧张调节至关重要,因为高渗血症与慢性肾脏疾病(CKD)和具有佝偻病和生长迟缓的咳咳病毒的心血管发病率增加有关。本次审查考虑了维生素D,PTH和PI本身对PI平衡的控制,重点是人类遗传障碍和转基因小鼠模型中获得的见解。

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