Xenobiotics Triggering Acute Intermittent Porphyria and Their Effect on Mouse Brain Respiratory Complexes.

IF 6.8 Q1 TOXICOLOGY
Johanna Romina Zuccoli, María Del Carmen Martínez, Pablo Vallecorsa, Ana María Buzaleh
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Abstract

Heme enzyme dysfunction causes a group of diseases called porphyrias. Particularly, a decrease in porphobilinogen deaminase, involved in the third step of heme biosynthesis, leads to acute intermittent porphyria (AIP). Considering our previous works demonstrating the multiplicity of brain metabolisms affected by porphyrinogenic agents, this study aimed to elucidate whether they cause any alteration on the mitochondrial respiratory chain. The activities of respiratory chain complexes (I to IV) were measured in encephalon mitochondria of CF1 male mice receiving volatile anesthetics: isoflurane (2 mL/kg) and sevoflurane (1.5 mL/kg), ethanol (30%), allylisopropylacetamide (AIA) (350 mg/kg), and barbital (167 mg/kg). Moreover, they were compared versus animals with pathological levels of 5-aminolevulinic acid (ALA, 40 mg/kg). Complex I-III activity was induced by isoflurane and decreased by AIA, ethanol, and ALA. Complex II-III activity was increased by sevoflurane and decreased by isoflurane and AIA. Complex II activity was increased by sevoflurane and barbital and decreased by AIA, ethanol, and ALA. Complex IV activity was increased by barbital and ALA and decreased by sevoflurane. The damage to the respiratory chain by ALA could be reflecting the pathophysiological condition of patients with AIP. Better understanding the broad effect of porphyrinogenic drugs and the mechanisms acting on the onset of AIP is vital in translational medicine.

诱发急性间歇性卟啉症的外来物质及其对小鼠脑呼吸复合体的影响
血红素酶功能障碍会导致一组名为卟啉症的疾病。特别是,参与第三步血红素生物合成的卟啉原脱氨酶的减少会导致急性间歇性卟啉症(AIP)。考虑到我们之前的研究表明卟啉生成剂对大脑代谢的影响是多方面的,本研究旨在阐明卟啉生成剂是否会对线粒体呼吸链造成任何改变。研究人员测量了接受异氟醚(2 mL/kg)和七氟醚(1.5 mL/kg)、乙醇(30%)、烯丙基异丙基乙酰胺(AIA)(350 mg/kg)和巴比妥(167 mg/kg)等挥发性麻醉剂的 CF1 雄性小鼠脑线粒体中呼吸链复合物(I 至 IV)的活性。此外,它们还与5-氨基乙酰丙酸(ALA,40毫克/千克)达到病理水平的动物进行了比较。异氟醚诱导了复合体 I-III 的活性,而 AIA、乙醇和 ALA 则降低了复合体 I-III 的活性。七氟醚可增加复合体 II-III 的活性,异氟醚和 AIA 可降低其活性。七氟醚和巴比妥会增加复合体 II 的活性,而 AIA、乙醇和 ALA 会降低复合体 II 的活性。巴比妥和 ALA 可提高复合物 IV 的活性,而七氟烷则会降低其活性。ALA 对呼吸链的破坏可能反映了 AIP 患者的病理生理状况。更好地了解致卟啉药物的广泛作用以及AIP的发病机制对转化医学至关重要。
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来源期刊
CiteScore
5.30
自引率
1.70%
发文量
21
审稿时长
10 weeks
期刊介绍: The Journal of Xenobiotics publishes original studies concerning the beneficial (pharmacology) and detrimental effects (toxicology) of xenobiotics in all organisms. A xenobiotic (“stranger to life”) is defined as a chemical that is not usually found at significant concentrations or expected to reside for long periods in organisms. In addition to man-made chemicals, natural products could also be of interest if they have potent biological properties, special medicinal properties or that a given organism is at risk of exposure in the environment. Topics dealing with abiotic- and biotic-based transformations in various media (xenobiochemistry) and environmental toxicology are also of interest. Areas of interests include the identification of key physical and chemical properties of molecules that predict biological effects and persistence in the environment; the molecular mode of action of xenobiotics; biochemical and physiological interactions leading to change in organism health; pathophysiological interactions of natural and synthetic chemicals; development of biochemical indicators including new “-omics” approaches to identify biomarkers of exposure or effects for xenobiotics.
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