Sharov Victor S, Dremina Elena S, Galeva Nadezhda A, Gerstenecker Gary S, Li Xiaobao, Dobrowsky Rick T, Stobaugh John F, Schöneich Christian
Department of Pharmaceutical Chemistry, University of Kansas, 2095 Constant Avenue, Lawrence, KS 66047, USA.
Chromatographia. 2010 Jan 1;71(1-2):37-53. doi: 10.1365/s10337-009-1409-0.
Protein 3-nitrotyrosine (3-NT) has been recognized as an important biomarker of nitroxidative stress associated with inflammatory and degenerative diseases, and biological aging. Analysis of protein-bound 3-NT continues to represent a challenge since in vivo it frequently does not accumulate on proteins in amounts detectable by quantitative analytical methods. Here, we describe a novel approach of fluorescent tagging and quantitation of peptide-bound 3-NT residues based on the selective reduction to 3-AT followed by reaction with 4-(amino-methyl)benzenesulfonic acid (ABS) in the presence of K(3)Fe(CN)(6) to form a highly fluorescent 2-phenylbenzoxazole product. Synthetic 3-NT peptide (0.005-1 μM) upon reduction with 10 mM sodium dithionite and tagging with 2 mM ABS and 5 μM K(3)Fe(CN)(6) in 0.1 M Na(2)HPO(4) buffer (pH 9.0) was converted with yields >95% to a single fluorescent product incorporating two ABS molecules per 3-NT residue, with fluorescence excitation and emission maxima at 360 ± 2 and 490 ± 2 nm, respectively, and a quantum yield of 0.77 ± 0.08, based on reverse-phase LC with UV and fluorescence detection, fluorescence spectroscopy and LC-MS-MS analysis. This protocol was successfully tested for quantitative analysis of in vitro Tyr nitration in a model protein, rabbit muscle phosphorylase b, and in a complex mixture of proteins from C2C12 cultured cells exposed to peroxynitrite, with a detection limit of ca. 1 pmol 3-NT by fluorescence spectrometry, and an apparent LOD of 12 and 40 pmol for nitropeptides alone or in the presence of 100 μg digested cell proteins, respectively. LC-MS-MS analysis of ABS tagged peptides revealed that the fluorescent derivatives undergo efficient backbone fragmentations, allowing for sequence-specific characterization of protein Tyr nitration in proteomic studies. Fluorogenic tagging with ABS also can be instrumental for detection and visualization of protein 3-NT in LC and gel-based protein separations.
蛋白质3-硝基酪氨酸(3-NT)已被公认为是与炎症性疾病、退行性疾病及生物衰老相关的氮氧化应激的重要生物标志物。蛋白质结合型3-NT的分析仍然是一项挑战,因为在体内它通常不会以定量分析方法可检测的量积累在蛋白质上。在此,我们描述了一种基于将肽结合的3-NT残基选择性还原为3-氨基酪氨酸(3-AT),然后在铁氰化钾(K(3)Fe(CN)(6))存在下与4-(氨基甲基)苯磺酸(ABS)反应形成高荧光2-苯基苯并恶唑产物的荧光标记和定量肽结合3-NT残基的新方法。在0.1 M磷酸氢二钠缓冲液(pH 9.0)中,用10 mM连二亚硫酸钠还原并与2 mM ABS和5 μM K(3)Fe(CN)(6)标记的合成3-NT肽(0.005 - 1 μM)以>95%的产率转化为每个3-NT残基结合两个ABS分子的单一荧光产物,基于反相液相色谱(LC)结合紫外和荧光检测、荧光光谱以及LC-MS-MS分析,其荧光激发和发射最大值分别在360 ± 2和490 ± 2 nm,量子产率为0.77 ± 0.08。该方法已成功用于对模型蛋白兔肌肉磷酸化酶b以及暴露于过氧亚硝酸盐的C2C12培养细胞的蛋白质复杂混合物中的体外酪氨酸硝化进行定量分析,通过荧光光谱法检测限约为1 pmol 3-NT,单独的硝基肽或在存在100 μg消化细胞蛋白时的表观检测限分别为12和40 pmol。对ABS标记肽的LC-MS-MS分析表明,荧光衍生物经历有效的主链断裂,从而在蛋白质组学研究中实现对蛋白质酪氨酸硝化的序列特异性表征。用ABS进行荧光标记在基于LC和凝胶的蛋白质分离中也有助于蛋白质3-NT的检测和可视化。