首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >ADP-ribosylation of human defensin HNP-1 results in the replacement of the modified arginine with the noncoded amino acid ornithine
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ADP-ribosylation of human defensin HNP-1 results in the replacement of the modified arginine with the noncoded amino acid ornithine

机译:人防御素HNP-1的ADP-核糖基化导致修饰的精氨酸被非编码氨基酸鸟氨酸替代

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摘要

Defensins (e.g., human neutrophil peptides, or HNPs) contribute to innate immunity through diverse actions, including microbial killing; high concentrations are present in the lung in response to inflammation. Arginines are critical for HNP activity, which is decreased by their replacement with ornithine. ADP-ribosyltransferases (ARTs) catalyze transfer of ADP-ribose from NAD to an acceptor arginine in a protein substrate, whereas ADP-ribosylarginine hydrolases release ADP-ribose. ART1 on the surface of airway epithelial cells ADP-ribosylated HNP-1 specifically on arginines 14 and 24, with ADP-ribosylation altering biological activity. Di- and mono-ADP-ribosylated HNP-1 were isolated from bronchoalveolar lavage fluid (BALF) of patients with asthma and idiopathic pulmonary fibrosis (IPF), suggesting a role for ADP-ribosylation in disease. In the present study, we observed that ART1-catalyzed ADP-ribosylation of HNP-1 in vitro generated a product with ADP-ribose on arginine 24, and ornithine replacing arginine at position 14. We hypothesized that ADP-ribosylarginine is susceptible to a nonenzymatic hydrolytic reaction yielding ornithine. On incubation of di- or mono-ADP-ribosyl-HNP-1 at 37 ℃, ADP-ribosylarginine was partially replaced by ornithine, whereas ornithine was not detected by amino acid analysis and mass spec-trometry of unmodified HNP-1 incubated under the same conditions. Further, ornithine was produced from the model compound, ADP-ribosylarginine. BALF from an IPF patient contained ADP-ribosyl-HNP-ornithine as well as mono- and di-ADP-ribosylated HNP-1, consistent with in vivo conversion of arginine to ornithine. Targeted ADP-ribosylation of specific arginines by transferases, resulting in their replacement with ornithine, is an alternative pathway for regulation of protein function through posttranslational modification.
机译:防御素(例如人嗜中性粒细胞肽或HNP)通过多种作用(包括杀死微生物)来促进先天免疫。响应炎症,肺中存在高浓度。精氨酸对于HNP活性至关重要,而HNP活性因被鸟氨酸替代而降低。 ADP核糖基转移酶(ARTs)催化ADP核糖从NAD转移到蛋白质底物中的受体精氨酸,而ADP核糖基精氨酸水解酶释放ADP核糖。气道上皮细胞ADP-核糖基化的HNP-1在精氨酸14和24的表面上具有ART1,ADP-核糖基化改变了生物活性。从患有哮喘和特发性肺纤维化(IPF)的患者的支气管肺泡灌洗液(BALF)中分离出双和单ADP核糖基化的HNP-1,表明ADP核糖基化在疾病中的作用。在本研究中,我们观察到体外HART-1的ART1催化的ADP-核糖基化在精氨酸24上生成了带有ADP-核糖的产物,在位置14上用鸟氨酸取代了精氨酸。我们假设ADP-核糖基精氨酸对非酶敏感水解反应生成鸟氨酸。在37℃下孵育二或单ADP-核糖基-HNP-1时,ADP-核糖基精氨酸被鸟氨酸部分取代,而氨基酸分析和质谱未检出未修饰的HNP-1的鸟氨酸含量。相同的条件。此外,从模型化合物ADP-核糖基精氨酸生产鸟氨酸。 IPF患者的BALF含有ADP-核糖基-HNP-鸟氨酸以及单-和二-ADP-核糖基化的HNP-1,与精氨酸在体内的转化为鸟氨酸一致。特异性精氨酸被转移酶靶向ADP-核糖基化,导致其被鸟氨酸替代,是通过翻译后修饰调节蛋白功能的另一种途径。

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