SLC35G1 is a highly chloride-sensitive transporter responsible for the basolateral membrane transport in intestinal citrate absorption.

IF 6.4 1区 生物学 Q1 BIOLOGY eLife Pub Date : 2024-11-07 DOI:10.7554/eLife.98853
Yoshihisa Mimura, Tomoya Yasujima, Katsuhisa Inoue, Shogo Akino, Chitaka Namba, Hiroyuki Kusuhara, Yutaro Sekiguchi, Kinya Ohta, Takahiro Yamashiro, Hiroaki Yuasa
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Abstract

The intestinal absorption of essential nutrients, especially those not readily biosynthesized, is a critical physiological process for maintaining homeostasis. Numerous studies have indicated that intestinal absorption is mediated by various membrane transporters. Citrate, a crucial bioactive compound produced as an intermediate in the Krebs cycle, is absorbed in the small intestine through carrier-mediated systems because of its high hydrophilicity. While the luminal absorption of citrate is mediated by Na+-dicarboxylate cotransporter 1 (NaDC1/SLC13A2), the mechanism governing the release of the transported citrate into the bloodstream remains unknown. Here, we explored the transporters responsible for intestinal citrate absorption at the basolateral membrane, focusing on highly expressed orphan transporters in the small intestine as candidates. Consequently, SLC35G1, originally identified as a partner of stromal interaction molecule 1, a cell surface transmembrane glycoprotein, was found to play a role in the intestinal absorption of citrate at the basolateral membrane. Furthermore, our results revealed that SLC35G1-mediated citrate transport was diminished by chloride ions at physiologically relevant extracellular concentrations. This suggests that SLC35G1, to our best knowledge, is the first transporter identified to be extremely sensitive to chloride ions among those functioning on the basolateral membrane of intestinal epithelial cells. This study provides valuable insights into the intestinal absorption of citrate and significantly contributes to elucidating the poorly understood molecular basis of the intestinal absorption system.

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SLC35G1 是一种对氯化物高度敏感的转运体,负责肠道柠檬酸盐吸收过程中的基底膜转运。
肠道吸收必需营养素,尤其是不易生物合成的营养素,是维持体内平衡的关键生理过程。大量研究表明,肠道吸收是由各种膜转运体介导的。柠檬酸盐是一种重要的生物活性化合物,在克雷布斯循环中作为中间体产生,由于其亲水性强,在小肠中通过载体系统吸收。虽然柠檬酸盐的管腔吸收是由 Na+-二羧酸共转运体 1(NaDC1/SLC13A2)介导的,但将转运的柠檬酸盐释放到血液中的机制仍然未知。在这里,我们以小肠中高表达的孤儿转运体为候选对象,探索了在基底侧膜上负责肠道柠檬酸盐吸收的转运体。结果发现,SLC35G1最初被鉴定为基质相互作用分子1(一种细胞表面跨膜糖蛋白)的伙伴,在肠道基底侧膜吸收柠檬酸盐的过程中发挥作用。此外,我们的研究结果表明,在生理相关的细胞外浓度下,氯离子会减少 SLC35G1 介导的柠檬酸盐转运。这表明,据我们所知,SLC35G1 是肠上皮细胞基底侧膜上第一个对氯离子极为敏感的转运体。这项研究为柠檬酸盐的肠道吸收提供了有价值的见解,并为阐明肠道吸收系统的分子基础做出了重要贡献。
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来源期刊
eLife
eLife BIOLOGY-
CiteScore
12.90
自引率
3.90%
发文量
3122
审稿时长
17 weeks
期刊介绍: eLife is a distinguished, not-for-profit, peer-reviewed open access scientific journal that specializes in the fields of biomedical and life sciences. eLife is known for its selective publication process, which includes a variety of article types such as: Research Articles: Detailed reports of original research findings. Short Reports: Concise presentations of significant findings that do not warrant a full-length research article. Tools and Resources: Descriptions of new tools, technologies, or resources that facilitate scientific research. Research Advances: Brief reports on significant scientific advancements that have immediate implications for the field. Scientific Correspondence: Short communications that comment on or provide additional information related to published articles. Review Articles: Comprehensive overviews of a specific topic or field within the life sciences.
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