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首页> 外文期刊>Toxins >Toxic Dimethylarginines: Asymmetric Dimethylarginine (ADMA) and Symmetric Dimethylarginine (SDMA)
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Toxic Dimethylarginines: Asymmetric Dimethylarginine (ADMA) and Symmetric Dimethylarginine (SDMA)

机译:有毒的二甲基精氨酸:不对称的二甲基精氨酸(ADMA)和对称的二甲基精氨酸(SDMA)

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Asymmetric and symmetric dimethylarginine (ADMA and SDMA, respectively) are toxic, non‐proteinogenic amino acids formed by post‐translational modification and are uremic toxins that inhibit nitric oxide (NO) production and play multifunctional roles in many human diseases. Both ADMA and SDMA have emerged as strong predictors of cardiovascular events and death in a range of illnesses. Major progress has been made in research on ADMA‐lowering therapies in animal studies; however, further studies are required to fill the translational gap between animal models and clinical trials in order to treat human diseases related to elevated ADMA/SDMA levels. Here, we review the reported impacts of ADMA and SDMA on human health and disease, focusing on the synthesis and metabolism of ADMA and SDMA; the pathophysiological roles of these dimethylarginines; clinical conditions and animal models associated with elevated ADMA and SDMA levels; and potential therapies against ADMA and SDMA. There is currently no specific pharmacological therapy for lowering the levels and counteracting the deleterious effects of ADMA and SDMA. A better understanding of the mechanisms underlying the impact of ADMA and SDMA on a wide range of human diseases is essential to the development of specific therapies against diseases related to ADMA and SDMA.
机译:不对称和对称二甲基精氨酸(分别为ADMA和SDMA)是有毒的,非蛋白原性氨基酸,是通过翻译后修饰形成的,并且是尿毒症毒素,可抑制一氧化氮(NO)的产生并在许多人类疾病中发挥多种作用。 ADMA和SDMA都已成为各种疾病中心血管事件和死亡的有力预测指标。动物研究中降低ADMA疗法的研究已取得重大进展。然而,为了治疗与ADMA / SDMA水平升高有关的人类疾病,需要进一步的研究来填补动物模型与临床试验之间的翻译空白。在这里,我们回顾了ADMA和SDMA对人类健康和疾病的报道影响,重点是ADMA和SDMA的合成和代谢。这些二甲基精氨酸的病理生理作用;与ADMA和SDMA水平升高有关的临床状况和动物模型;以及针对ADMA和SDMA的潜在疗法。目前,尚无用于降低ADMA和SDMA的水平并抵消其有害作用的药物治疗方法。更好地了解ADMA和SDMA对广泛人类疾病的潜在影响机制对于开发针对ADMA和SDMA相关疾病的特定疗法至关重要。

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