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生物化学计量学鉴定紫檀心材中促炎基因表达的抑制剂。

Biochemometry identifies suppressors of pro-inflammatory gene expression in Pterocarpus santalinus heartwood.

机构信息

Department of Pharmaceutical Sciences, Division of Pharmacognosy, University of Vienna, Josef-Holaubek-Platz 2, 1090, Vienna, Austria.

Department of Pharmaceutical Sciences, Division of Pharmacognosy, University of Vienna, Josef-Holaubek-Platz 2, 1090, Vienna, Austria.

出版信息

Phytochemistry. 2023 Aug;212:113709. doi: 10.1016/j.phytochem.2023.113709. Epub 2023 May 5.

DOI:10.1016/j.phytochem.2023.113709
PMID:37150433
Abstract

The heartwood extract of the Ayurvedic medicinal plant Pterocarpus santalinus L. f. has previously been shown to significantly suppress the expression of CX3CL1 and other pro-inflammatory molecules in IL-1-stimulated human endothelial cells. Here, we identify the pigment-depleted extract PSD as the most promising yet still complex source of metabolites acting as an inhibitor of CX3CL1 gene expression. For the target-oriented identification of the constituents contributing to the observed in vitro anti-inflammatory effect of PSD, the biochemometric approach ELINA (Eliciting Nature's Activities) was applied. ELINA relies on the deconvolution of complex mixtures by generating microfractions with quantitative variances of constituents over several consecutive fractions. Therefore, PSD was separated into 35 microfractions by means of flash chromatography. Their H NMR data and bioactivity data were correlated by heterocovariance analysis. Complemented by LC-MS-ELSD data, ELINA differentiated between constituents with positive and detrimental effects towards activity and allowed for the prioritization of compounds to be isolated in the early steps of phytochemical investigation. A hyphenated high-performance counter-current chromatographic device (HPCCC+) was employed for efficient and targeted isolation of bioactive constituents. A total of 15 metabolites were isolated, including four previously unreported constituents and nine that have never been described before from red sandalwood. Nine isolates were probed for their inhibitory effects on CX3CL1 gene expression, of which four isoflavonoids, namely pterosonin A (1), santal (6), 7,3'-dimethylorobol (12) and the previously unreported compound pterosantalin A (2), were identified as pronounced inhibitors of CX3CL1 gene expression in vitro.

摘要

药用植物紫檀的心材提取物先前已被证明可显著抑制白细胞介素-1 刺激的人内皮细胞中 CX3CL1 和其他促炎分子的表达。在这里,我们确定色素耗尽提取物 PSD 是最有前途但仍然复杂的代谢物来源,可作为 CX3CL1 基因表达抑制剂。为了针对目标鉴定 PSD 观察到的体外抗炎作用的成分,应用了生化计量学方法 ELINA(引出自然活性)。ELINA 依赖于通过生成具有几种连续馏分中成分定量方差的微馏分来对复杂混合物进行去卷积。因此,通过闪蒸色谱将 PSD 分离成 35 个微馏分。它们的 H NMR 数据和生物活性数据通过异方差分析相关联。通过 LC-MS-ELSD 数据进行补充,ELINA 区分了对活性具有正向和不利影响的成分,并允许在植物化学研究的早期步骤中优先分离化合物。使用高效和靶向分离生物活性成分的高效逆流色谱设备(HPCCC+)。共分离出 15 种代谢产物,包括 4 种以前未报道的成分和 9 种从未在红檀香中描述过的成分。对 15 种分离物进行了抑制 CX3CL1 基因表达的实验,其中 4 种异黄酮,即紫檀素 A(1)、紫檀素(6)、7,3'-二甲基奥罗醇(12)和以前未报道的化合物紫檀素 A(2),被鉴定为体外 CX3CL1 基因表达的强抑制剂。

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