Down-regulation of magnesium transporting molecule, claudin-16, as a possible cause of hypermagnesiuria with the development of tubulo-interstitial nephropathy.

IF 1.5 4区 医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY
Taisuke Shimizu, Kaori Takayanagi, Takatsugu Iwashita, Akira Ikari, Naohiko Anzai, Shimpei Okazaki, Hiroaki Hara, Minoru Hatano, Tatsuro Sano, Tomonari Ogawa, Koichi Kanozawa, Hajime Hasegawa
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引用次数: 4

Abstract

Tubulo-interstitial nephropathy (TIN) is a critical pathological setting for the renal prognosis, and an increase in the urine magnesium excretion is a well-known characteristic feature as one of clinical parametets for the assessment of TIN. We examined the correlation between the development of TIN and the changes in the mRNA expression of renal magnesium-transporting molecules in rats with unilateral ureter obstruction (UUO). Ureter-ligated kidney was sampled at day-0 (control), day-1 (early phase) and day-7 (late phase). The development of TIN was assessed by immunohistochemistry and the real-time PCR of fibrosis-related genes (MCP-1: 105.1 ± 14.8% on day-0, 132.9 ± 25.7% on day-1, 302.7 ± 32.7% on day-7, TGF-β: 101.1 ± 7.6% on day-0, 93.6 ± 4.1% on day-1, 338.9 ± 20.7% on day-7) . The respective expressions of claudin-10, 14, 16, 19, and transient receptor potential (TRP) M6 as magnesium-transporting molecules were also studied. The expression of calcium sensing receptor (CaSR) as an inhibitory regulator of claudin-14 was additionally studied. The gene expression of claudin-16 was decreased in the late phase of UUO (100.2 ± 2.9% at day-0, 90.3 ± 6.3% at day-1, 36.4 ± 1.6% at day-7) which was consistent with the increased urine magnesium excretion. Immunohistochemistry showed an apparent reduction of the immunoreactivity of claudin-16 in the late phase. The expression of TRPM6 was reduced even in the early phase. The immunohistochemistry and gene expression of MCP-1 and TGF-ß showed that TIN was not apparent in the early phase but was significant in the late phase of UUO. The density of peritubular capillaries was diminished in the late phase but not in the early phase. Expression of claudin-14 and CaSR was up- and down-regulated, respectively. Our findings may indicate that the characteristic hypermagnesiuria in TIN is principally caused by the dysfunction of magnesium reabsorption in the thick ascending limb of Henle resulting from a significant decrease in the claudin-16 expression. The down-regulation might be closely related to the development of TIN.
镁转运分子claudin-16的下调可能导致高镁尿伴小管间质肾病的发生。
肾小管间质肾病(TIN)是肾脏预后的重要病理环境,而尿镁排泄量的增加是评估TIN的临床参数之一。探讨单侧输尿管梗阻(UUO)大鼠肾镁转运分子mRNA表达变化与TIN发育的关系。在第0天(对照)、第1天(早期)和第7天(晚期)采集输尿管结扎肾。采用免疫组织化学和实时荧光定量PCR检测纤维化相关基因(MCP-1: 105.1±14.8%,第1天132.9±25.7%,第7天302.7±32.7%,TGF-β: 101.1±7.6%,第1天93.6±4.1%,第7天338.9±20.7%)。研究了claudin-10、14、16、19和瞬时受体电位(TRP) M6作为镁转运分子的表达。此外,还研究了钙敏感受体(CaSR)作为claudin-14的抑制调节因子的表达。claudin-16基因表达在UUO晚期下降(第0天为100.2±2.9%,第1天为90.3±6.3%,第7天为36.4±1.6%),与尿镁排泄量增加一致。免疫组化显示晚期claudin-16的免疫反应性明显降低。即使在早期,TRPM6的表达也有所降低。免疫组化及MCP-1、TGF-ß基因表达结果显示,TIN在UUO早期不明显,但在UUO晚期显著。小管周围毛细血管密度在晚期减少,而在早期没有。claudin-14和CaSR的表达分别上调和下调。我们的研究结果可能表明,TIN特征性高镁尿主要是由于claudin-16表达显著降低导致Henle厚升肢镁重吸收功能障碍所致。这种下调可能与TIN的发育密切相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Magnesium research
Magnesium research 医学-内分泌学与代谢
CiteScore
3.50
自引率
9.40%
发文量
6
审稿时长
>12 weeks
期刊介绍: Magnesium Research, the official journal of the international Society for the Development of Research on Magnesium (SDRM), has been the benchmark journal on the use of magnesium in biomedicine for more than 30 years. This quarterly publication provides regular updates on multinational and multidisciplinary research into magnesium, bringing together original experimental and clinical articles, correspondence, Letters to the Editor, comments on latest news, general features, summaries of relevant articles from other journals, and reports and statements from national and international conferences and symposiums. Indexed in the leading medical databases, Magnesium Research is an essential journal for specialists and general practitioners, for basic and clinical researchers, for practising doctors and academics.
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