LIM和SH3蛋白2（Lasp2）是小鼠肝脏中一种新型孕烷X受体靶基因。

IF 3.2 3区医学 Q2 PHARMACOLOGY & PHARMACY

Molecular Pharmacology Pub Date : 2025-02-07 DOI:10.1016/j.molpha.2025.100019

Anja Konzack, Mikko Karpale, Tomas Smutny, Mohamed Hassanen, Piia Lassila, Maria H Ahonen, Mahmoud-Sobhy Elkhwanky, Outi Kummu, Petr Pavek, Jukka Hakkola

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引用次数: 0

摘要

LIM和Src同源3（SH3）蛋白2（LASP2）是一种小型局灶粘附蛋白，最早被鉴定为nebulette基因（Nebbl）的剪接变体。作为 nebulin 蛋白家族的最新成员，LASP2 的调控和功能在很大程度上仍然未知。我们之前的 RNA 测序结果发现，Nebl 是小鼠肝脏中对孕烷 X 受体（PXR）激活反应诱导程度最高的基因之一。在本研究中，我们进一步研究了这一现象，结果表明 PXR 诱导的是 Lasp2，而不是 Nebl，两者部分使用相同的外显子。研究发现，PXR配体孕烯诺龙16α-甲腈（PCN）处理小鼠肝脏4天后，以及长期处理28天后，Lasp2在雄性和雌性小鼠体内都会被诱导。有趣的是，与正常饲料喂养的小鼠（4 天 PCN 处理后为 32 倍）相比，高脂饮食喂养的小鼠（4 天 PCN 处理后为 103 倍）对 Lasp2 的诱导更为有效。在 PXR 基因敲除的小鼠中，Lasp2 的诱导作用被取消，但可以通过重新表达 PXR 得到挽救，这表明 Lasp2 的诱导作用是由 PXR 介导的。在小鼠原代肝细胞中，环己亚胺不能抑制 PCN 对 Lasp2 的诱导，而且在小鼠 Lasp2 基因的上游可以识别出一个 PXR 结合位点，这表明 Lasp2 是由 PXR 直接调控的。在人三维肝细胞中，利福平仅诱导 LASP2 表达的适度增加。本研究首次表明，PXR 激活可强烈诱导小鼠肝脏中 Lasp2 的表达，并将 Lasp2 确立为新型 PXR 靶基因。意义声明：之前的 RNA 测序结果发现，孕烷 X 受体激活化合物可有效诱导 Nebulette（Nebl）。本研究表明，在小鼠肝脏中，LIM 和 Src 同源物 3（SH3）蛋白 2（Lasp2）代替 Nebl 成为孕烷 X 受体的新靶基因，Lasp2 编码一种小型局灶粘附蛋白，与 Nebl 基因共享部分外显子。

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LIM and SH3 protein 2 (Lasp2) is a novel pregnane X receptor target gene in mouse liver.

LIM and Src homology 3 (SH3) protein 2 (LASP2) is a small focal adhesion protein first identified as a splice variant of the nebulette gene (Nebl). As the newest member of the nebulin protein family, the regulation and function of LASP2 remain largely unknown. Our previous RNA-sequencing results identified Nebl as one of the most highly induced genes in the mouse liver in response to the activation of pregnane X receptor (PXR). In this study, we investigated this phenomenon further and show that PXR induces Lasp2 instead of Nebl, which partially use the same exons. Lasp2 was found to be induced in response to PXR ligand pregnenolone 16α-carbonitrile (PCN) treatment in mouse liver in vivo both after 4-day treatment and after long-term, 28-day treatment and in both male and female mice. Interestingly, the Lasp2 induction was more efficient in high-fat diet-fed mice (103-fold after 4-day PCN treatment) than in the normal chow-fed mice (32-fold after 4-day PCN treatment). Lasp2 induction was abolished in PXR knockout mice but could be rescued by re-expression of PXR, indicating that Lasp2 induction is PXR mediated. In mouse primary hepatocytes cycloheximide did not inhibit Lasp2 induction by PCN and a PXR binding site could be recognized upstream of the mouse Lasp2 gene suggesting direct regulation of Lasp2 by PXR. In human 3D hepatocytes, rifampicin induced only a modest increase in LASP2 expression. This study shows for the first time that PXR activation strongly induces Lasp2 expression in mouse liver and establishes Lasp2 as a novel PXR target gene. SIGNIFICANCE STATEMENT: RNA-sequencing results have previously identified nebulette (Nebl) to be efficiently induced by pregnane X receptor activating compounds. This study shows that instead of Nebl, LIM and Src homology 3 (SH3) protein 2 (Lasp2) coding for a small focal adhesion protein and partly sharing exons with the Nebl gene is a novel target of pregnane X receptor in mouse liver.

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来源期刊

Molecular Pharmacology 医学-药学

CiteScore

7.20

自引率

2.80%

发文量

审稿时长

3-6 weeks

期刊介绍： Molecular Pharmacology publishes findings derived from the application of innovative structural biology, biochemistry, biophysics, physiology, genetics, and molecular biology to basic pharmacological problems that provide mechanistic insights that are broadly important for the fields of pharmacology and toxicology. Relevant topics include: Molecular Signaling / Mechanism of Drug Action Chemical Biology / Drug Discovery Structure of Drug-Receptor Complex Systems Analysis of Drug Action Drug Transport / Metabolism