Last update 01 Nov 2024

SLC26A3

Last update 01 Nov 2024

Basic Info

Synonyms

Chloride anion exchanger, CLD, congenital chloride diarrhea

+ [7]

Introduction

Mediates chloride-bicarbonate exchange with a chloride bicarbonate stoichiometry of 2:1 in the intestinal epithelia (PubMed:16606687, PubMed:19321737, PubMed:22159084, PubMed:22627094). Plays a role in the chloride and bicarbonate homeostasis during sperm epididymal maturation and capacitation (By similarity).

Drugs associated with SLC26A3

A-270

Target

SLC26A3

Mechanism

SLC26A3 inhibitors

Active Org.

The University of California, San Francisco

Originator Org.

The University of California, San Francisco

Active Indication

Hyperoxaluria [+1]

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

3a(UCSF)

Target

SLC26A3

Mechanism

SLC26A3 inhibitors

Active Org.

The University of California, San Francisco

Originator Org.

The University of California, San Francisco

Active Indication

Constipation

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

100 Clinical Results associated with SLC26A3

100 Translational Medicine associated with SLC26A3

0 Patents (Medical) associated with SLC26A3

944

Literatures (Medical) associated with SLC26A3

01 Dec 2024·Journal of Ethnopharmacology

Isoastragaloside I attenuates cholestatic liver diseases by ameliorating liver injury, regulating bile acid metabolism and restoring intestinal barrier

Article

Author: Shi, Jiewen ; Zhang, Jianwei ; Jiang, Xiaoyu ; Zhang, Hua ; Mu, Yongping ; Zhang, Linzhang ; Liu, Ping ; Chen, Jiamei ; Chen, Gaofeng ; Liu, Wei ; Xie, Zhishen ; Shi, Xiaoli ; Qi, Shenglan

ETHNOPHARMACOLOGICAL RELEVANCECholestatic liver diseases (CLD) are liver disorders resulting from abnormal bile formation, secretion, and excretion from various causes. Due to the lack of suitable and safe medications, liver transplantation is the ultimate treatment for CLD patients. Isoastragaloside I (IAS I) is one of the main saponin found in Astragalus membranaceus (Fisch.) Bge. var. mongholicus (Bge.) Hsiao or Astragalus membranaceus (Fisch.) Bge, which has been demonstrated to obviously alleviate CLD. Nevertheless, the IAS I's specific anti-CLD mechanism remains undecipherable.AIM OF THE STUDYThis study's purpose was to elucidate the protective consequence of IAS I on 0.1% 3, 5-diethoxycarbonyl-1,4-dihydroxychollidine (DDC) diet-induced CLD mice, and to reveal its potential mechanism.MATERIALS AND METHODSIn this study, mice with CLD that had been fed a 0.1% DDC diet were distributed two doses of IAS I (20 mg/kg, 50 mg/kg). The effects of IAS I on CLD models were investigated by assessing blood biochemistry, liver histology, and Hyp concentrations. We investigated markers of liver fibrosis and ductular reaction using immunohistochemistry, Western blot, and qRT-PCR. Liver inflammation indicators, arachidonic acid (ARA), and ω-3 fatty acid (FA) metabolites were also analyzed. Quantitative determination of 39 bile acids (BAs) in different organs employing UHPLC-Q-Exactive Orbitrap HRMS technology. Additionally, the H&E and Western blot analysis were used to evaluate differences in intestinal barrier function in DDC-induced mice before and after administering IAS I.RESULTSAfter treatment with IAS I, serum biochemical indicators and liver hydroxyproline (Hyp) increased in a dose-dependent manner in CLD mice. The IAS I group showed significant improvement in indicators of liver fibrosis and ductular response, including as α-smooth muscle actin (α-SMA) and cytokeratin 19 (CK19), and transforming growth factor-β (TGF-β)/Smads signaling pathway. And inflammatory factors: F4/80, tumor necrosis factor-α (TNF-α), Interleukin-1β (IL-1β), ARA and ω-3 FA metabolites showed significant improvement following IAS I treatment. Moreover, IAS I significantly ameliorated liver tau-BAs levels, particularly TCA, THCA, THDCA, TCDCA, and TDCA contents, which were associated with enhanced expression of hepatic farnesoid X receptor (FXR), small heterodimer partner (SHP), cholesterol 7α-hydroxylase (Cyp7a1), and bile-salt export pump (BSEP). Furthermore, IAS I significantly improved pathological changes and protein expression related to intestinal barrier function, including zonula occludens protein 1 (ZO-1), Muc2, and Occludin.CONCLUSIONSIAS I alleviated cholestatic liver injury, relieved inflammation, improved the altered tau-BAs metabolism and restored intestinal barrier function to protect against DDC-induced cholestatic liver diseases.

01 Nov 2024·International Journal of Biological Macromolecules

Deficiency of SLC26A3 promotes jejunal barrier damage in metabolic disease-susceptible transgenic pigs

Article

Author: Wu, Tianwen ; Wang, Yanfang ; Xu, Shuang ; Fang, Meiying ; Zhang, Kaiyi ; Yang, Shulin ; Yang, Yu ; Du, Juan ; Miao, Jiakun ; Tao, Cong

Intestinal disorders are common in metabolic syndrome. However, their pathogenesis is still not fully understood. Pig and human intestines are highly similar in terms of associated metabolic processes. Here, we successfully constructed a metabolic disease-susceptible transgenic (TG) Bama pig model by knocking in three humanized disease risk genes with the CRISPR/Cas9 technique to assess its potential as a model for human intestinal diseases and explore the possible pathological mechanisms involved. We found that jejunal barrier integrity was disrupted and that the infiltration of inflammatory cells increased in TG pigs after high-fat and high-sucrose diet (HFHSD) treatment. We revealed significant differences in the transcriptome, associated microbiome profiles and microbial metabolite short-chain fatty acid (SCFA) content of the jejunum of TG pigs. Notably, we found that SLC26A3 was significantly downregulated in TG pigs. Knockdown or overexpression of the SLC26A3 gene in IPEC-J2 cells significantly affected the expression of MUC2, MUC13 and occludin. Furthermore, in vitro experiments further verified that CDX2 directly regulated the expression of SLC26A3. Mechanistically, CDX2 mediated intestinal barrier function by enhancing the expression of SLC26A3 by binding to its promoter region between -1120 and - 1070 bp. TG pigs represent a promising model that provides new insights into preclinical research on human intestinal metabolic diseases associated with metabolic disorders and revealed that SLC26A3 may be a potential therapeutic target for intestinal metabolic diseases.

01 Nov 2024·American Journal of Physiology-Gastrointestinal and Liver Physiology

Decreased expression of DRA (SLC26A3) by a p38-driven IL-1α response contributes to diarrheal disease following in vivo challenge with Brachyspira spp.

Article

Author: Loewen, Matthew E. ; Enns, Cole B. ; Keith, Brandon A. ; Harding, John C. S. ; Challa, Nitin

The diarrheal disease caused by the two infectious spirochete spp. B. hyodysenteriae and B. hampsonii reduced the expression of DRA ( SLC26A3), a major Cl−/HCO–3 exchanger involved in Cl− absorption. This is attributed to the upregulation of IL-1α driven by p38 MAPK. This work also describes a potential new mechanism in inflammatory diseases while showing the importance of IL-1α in maintaining DRA levels.

News (Medical) associated with SLC26A3

09 Aug 2022

·www.sciencedaily.com

Uncovering the secret of insulin growth factor ternary complex

Scientists determined the cryo-EM structure of IGF Ternary complex and its assembly and activation mechanism. Insulin-like growth factor (IGF) is a hormone that greatly influences growth in fetuses and children, but also body maintenance and metabolism in adults. IGF regulates cell proliferation, differentiation, and survival by activating IGF receptors distributed in cell membranes of various tissues. However, IGF is so unstable that its half-life is less than 10 minutes in its free state. For, this reason more than 70% of IGF circulating in the body is bound to IGFBP (IGF Binding Protein) and ALS (Acid Labile Subunit). This IGF/IGFBP/ALS ternary complex is stable for a much longer duration of 12 hours and therefore serves as a carrier for IGF. In addition, the ternary complex also plays a role in regulating IGF so that it can act only when needed. However, the structure of the IGF/IGFBP/ALS ternary complex has not been well studied, making it difficult to understand how the complex is assembled and how IGF is activated. Now, a team led by Professor KIM Ho Min at the Center for Biomolecular and Cellular Structure within the Institute for Basic Science (IBS) in Daejeon, South Korea, determined the structure of IGF1/IGFBP3/ALS ternary complex for the first time. It is believed that this structural information could broaden the understanding of growth-related diseases such as growth hormone deficiency and ALS deficiency. The stable ternary complex was successfully expressed and purified through an animal cell expression system and a series of purification processes. The cryogenic transmission electron microscope (cryo-EM), data hub, and supercomputing resources of IBS were used to obtain its high-resolution three-dimensional molecular structure. It was discovered that IGF1 was surrounded by IGFBP3 to first form a binary complex. Then, ALS once more wraps this binary complex like a parachute, which protects IGF1 from being easily degraded within the body. Armed with the new knowledge of the protein structure, the researchers were now able to understand the structural basis for many diseases associated with the mutations in these proteins. In particular, many known point mutations in ALS were found to cause disease by inducing misfolding of ALS and hindering the formation of the ternary complex. On the other hand, known point mutations in IGF did not appear to have any negative effects on their ability to form complexes, but rather cause disease by decreasing IGF's affinity to IGF receptors. The researchers did not stop there, as they further explored how this ternary complex is assembled. First, the researchers ran SDS-PAGE of ALS, IGFBP3, and IGF1 proteins to verify if the complex is or isn't formed. They also fused GFP (green fluorescent protein) onto the IGF1 protein and used fluorescence detection chromatography to trace the GFP labeled protein as they succeed or fail to form complexes with the other two proteins. From this, they learned that IGFBP3 or IGF1 alone cannot form a binary complex with ALS. Moreover, it was discovered that IGF must first form a binary complex with IGFBP, and only after that, both proteins can bind to ALS to properly assemble a ternary complex. Furthermore, the researchers modified IGFBP to better determine the role of specific domains of the protein. When the N terminal domain (NBP) was removed, the protein was shown to be incapable of binding to IGF, hinting that the domain is required for the initial binary complex formation. The researchers also substituted the central-linker domain (CLD3) of the IGFBP with different variants. Contrary to NBP, all variants of CLD domains allowed the formation of the binary complex with IGF1. However, it was shown that some CLD variants allowed the modified IGFBP to bind to ALS even without IGF. This means that it is likely that the formation of the initial IGF1/IGFBP3 binary complex allows for some conformational change to the CLD3 domain to facilitate ternary complex formation with ALS. In addition, the researchers monitored how the complex can be disassembled to make IGF bioavailable. In order to do so, they treated both IGF/IGFBP binary complex and the final ternary complex using a protease called thrombin. After the proteolysis, it was observed that the C-terminus domain (CBP) of IGFBP is released, and an unstable intermediate ternary complex is formed. This process was believed to be an important step in activating the IGF, which is otherwise inactive when it is bound within a complex. The first author KIM Hyojin states, "The first and foremost step before investigating further processes is to understand the structure. This structure-based approach and proper biochemical assays allowed us to unveil the mechanism of IGF complex formation and activation." "This new knowledge of molecular structure and activation mechanism of the IGF ternary complex is expected to greatly contribute to the development of therapeutic agents and research related to adolescent growth or IGF-related diseases," explains Professor KIM Ho Min, the corresponding author of the study.

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SLC26A3

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