脂质磷酸酶抑制剂局部放大溶血磷脂酸LPA1受体信号，而不影响整体LPA降解。

IF 2.9 3区医学 Q2 Medicine

BMC Pharmacology & Toxicology Pub Date : 2012-06-11 DOI:10.1186/1471-2210-12-7

Niina Aaltonen, Marko Lehtonen, Katri Varonen, Gemma Arrufat Goterris, Jarmo T Laitinen

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引用次数: 19

摘要

背景:溶血磷脂酸(Lysophosphatidic acid, LPA)是一种具有多种生物学功能的信号磷脂，主要通过特异性G蛋白偶联受体介导。异常LPA信号越来越多地与常见人类疾病的病理有关，如动脉硬化和癌症。LPA信号池的寿命由合成酶和降解酶活性之间的平衡控制。在目前的研究中，我们通过药理学操纵LPA降解所需的酶机制来表征大鼠脑中的这些酶途径。结果:在大鼠脑冷冻切片中，发现生物活性LPA的寿命受Mg2+不依赖、n -乙基丙烯酰亚胺不敏感的磷酸酶活性控制，该活性归因于脂质磷酸盐磷酸酶(LPPs)。功能放射自显像显示，LPP活性的药理抑制放大了LPA1受体信号。虽然两种LPP抑制剂，正钒酸钠和心得安，局部放大受体反应，但它们不影响整体脑LPA磷酸酶活性(也归因于Mg2+不依赖，n -乙基马来酰亚胺不敏感的磷酸酶)，经Pi测定和LC/MS/MS证实。有趣的是，磷酸类似物氟化铝(AlFx-)不仅不可逆地抑制LPP活性，从而增强LPA1受体的反应，而且完全阻止LPA降解，但是后一种作用对于观察AlFx依赖性受体信号传导的增强并不是必需的。结论:我们得出结论，对钒酸盐和心得安敏感的LPP活性局部保护LPA的信号池，而大部分脑LPA磷酸酶活性归因于LPP样酶活性，与LPP活性一样，对AlFx-敏感，但对LPP抑制剂，钒酸盐和心得安有抗性。

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Lipid phosphate phosphatase inhibitors locally amplify lysophosphatidic acid LPA1 receptor signalling in rat brain cryosections without affecting global LPA degradation.

Background: Lysophosphatidic acid (LPA) is a signalling phospholipid with multiple biological functions, mainly mediated through specific G protein-coupled receptors. Aberrant LPA signalling is being increasingly implicated in the pathology of common human diseases, such as arteriosclerosis and cancer. The lifetime of the signalling pool of LPA is controlled by the equilibrium between synthesizing and degradative enzymatic activity. In the current study, we have characterized these enzymatic pathways in rat brain by pharmacologically manipulating the enzymatic machinery required for LPA degradation.

Results: In rat brain cryosections, the lifetime of bioactive LPA was found to be controlled by Mg2+-independent, N-ethylmaleimide-insensitive phosphatase activity, attributed to lipid phosphate phosphatases (LPPs). Pharmacological inhibition of this LPP activity amplified LPA1 receptor signalling, as revealed using functional autoradiography. Although two LPP inhibitors, sodium orthovanadate and propranolol, locally amplified receptor responses, they did not affect global brain LPA phosphatase activity (also attributed to Mg2+-independent, N-ethylmaleimide-insensitive phosphatases), as confirmed by Pi determination and by LC/MS/MS. Interestingly, the phosphate analog, aluminium fluoride (AlFx-) not only irreversibly inhibited LPP activity thereby potentiating LPA1 receptor responses, but also totally prevented LPA degradation, however this latter effect was not essential in order to observe AlFx--dependent potentiation of receptor signalling.

Conclusions: We conclude that vanadate- and propranolol-sensitive LPP activity locally guards the signalling pool of LPA whereas the majority of brain LPA phosphatase activity is attributed to LPP-like enzymatic activity which, like LPP activity, is sensitive to AlFx- but resistant to the LPP inhibitors, vanadate and propranolol.

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来源期刊

BMC Pharmacology & Toxicology PHARMACOLOGY & PHARMACY-TOXICOLOGY

CiteScore

4.40

自引率

0.00%

发文量

审稿时长

12 weeks

期刊介绍： BMC Pharmacology and Toxicology is an open access, peer-reviewed journal that considers articles on all aspects of chemically defined therapeutic and toxic agents. The journal welcomes submissions from all fields of experimental and clinical pharmacology including clinical trials and toxicology.