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Neuroglobin, cytoglobin, and myoglobin contribute to hypoxia adaptation of the subterranean mole rat Spalax

机译:神经血红蛋白,细胞血红蛋白和肌红蛋白有助于黑痣大鼠Spalax的低氧适应

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摘要

The subterranean mole rat Spalax is an excellent model for studying adaptation of a mammal toward chronic environmental hypoxia. Neuroglobin (Ngb) and cytoglobin (Cygb) are O2-binding respiratory proteins and thus candidates for being involved in molecular hypoxia adaptations of Spalax. Ngb is expressed primarily in vertebrate nerves, whereas Cygb is found in extracellular matrix-producing cells and in some neurons. The physiological functions of both proteins are not fully understood but discussed with regard to O2 supply, the detoxification of reactive oxygen or nitrogen species, and apoptosis protection. Spalax Ngb and Cygb coding sequences are strongly conserved. However, mRNA and protein levels of Ngb in Spalax brain are 3-fold higher than in Rattus norvegicus under normoxia. Importantly, Spalax expresses Ngb in neurons and additionally in glia, whereas in hypoxia-sensitive rodents Ngb expression is limited to neurons. Hypoxia causes an approximately 2-fold down-regulation of Ngb mRNA in brain of rat and mole rat. A parallel regulatory response was found for myoglobin (Mb) in Spalax and rat muscle, suggesting similar functions of Mb and Ngb. Cygb also revealed an augmented normoxic expression in Spalax vs. rat brain, but not in heart or liver, indicating distinct tissue-specific functions. Hypoxia induced Cygb transcription in heart and liver of both mammals, with the most prominent mRNA up-regulation (12-fold) in Spalax heart. Our data suggest that tissue globins contribute to the remarkable tolerance of Spalax toward environmental hypoxia. This is consistent with the proposed cytoprotective effect of Ngb and Cygb under pathological hypoxic/ischemic conditions in mammals.
机译:地下mole鼠Spalax是研究哺乳动物对慢性环境低氧适应的极好模型。神经血红蛋白(Ngb)和细胞血红蛋白(Cygb)是与O2结合的呼吸蛋白,因此可能参与Spalax的分子低氧适应。 Ngb主要在脊椎动物神经中表达,而Cygb在细胞外基质产生细胞和某些神经元中发现。尚不完全了解这两种蛋白质的生理功能,但在氧气供应,活性氧或氮物质的解毒以及细胞凋亡保护方面进行了讨论。 Spalax Ngb和Cygb编码序列非常保守。然而,在常氧下,Spalax脑中Ngb的mRNA和蛋白水平比褐家鼠高3倍。重要的是,Spalax在神经元以及神经胶质细胞中表达Ngb,而在对缺氧敏感的啮齿动物中Ngb的表达仅限于神经元。缺氧导致大鼠和mole鼠的脑中Ngb mRNA约下调2倍。在Spalax和大鼠肌肉中发现了对肌红蛋白(Mb)的平行调节反应,表明Mb和Ngb的功能相似。 Cygb还揭示了Spalax与大鼠大脑中正常氧含量的表达增加,但在心脏或肝脏中却没有,这表明它们具有明显的组织特异性功能。低氧诱导两种哺乳动物的心脏和肝脏中的Cygb转录,在Spalax心脏中最显着的mRNA上调(12倍)。我们的数据表明,组织球蛋白有助于Spalax对环境低氧的显着耐受性。这与拟议的Ngb和Cygb在哺乳动物病理性缺氧/缺血条件下的细胞保护作用一致。

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