Ginseng

人参
  • 文章类型: English Abstract
    Trihelix转录因子的功能是在许多非生物胁迫中发挥重要作用,特别是在低温的信号通路中,干旱,洪水,盐水,脱落酸,茉莉酸甲酯,和其他非生物胁迫。然而,关于人参Trihelix基因家族的研究很少。在这项研究中,从人参基因组数据库中鉴定并筛选出41个Trihelix基因家族成员,以及它们的物理化学性质,顺式作用元素,亚细胞定位,染色体分配,通过生物信息学方法分析了非生物胁迫诱导的表达模式。结果表明,人参中85%的Trihelix家族成员位于细胞核,Trihelix蛋白的二级结构主要为无规卷曲和α螺旋。在Trihelix的启动子区域,与低温等各种非生物胁迫相关的顺式调控元件,激素反应,并确定了生长和发育。通过对模型植物拟南芥和人参种间Trihelix转录因子的共线性分析,在拟南芥和人参之间发现了19个共线基因对,并且仅在3号、6号和12号染色体上不存在共线基因对。qRT-PCR分析表明,GWHGBEIJ010320.1在低温胁迫下表达显著上调,对低温胁迫的显著响应。本研究为进一步研究人参Trihelix转录因子在非生物胁迫中的作用奠定了基础,以及人参的生长发育。
    The function of the Trihelix transcription factor is that it plays an important role in many abiotic stresses, especially in the signaling pathway of low temperature, drought, flood, saline, abscisic acid, methyl jasmonate, and other abiotic stresses. However, there are few studies on the Trihelix gene family of ginseng. In this study, 41 Trihelix gene family members were identified and screened from the ginseng genome database, and their physicochemical properties, cis-acting elements, subcellular localization, chromosomal assignment, and abiotic stress-induced expression patterns were analyzed by bioinformatics methods. The results showed that 85% of Trihelix family members of ginseng were located in the nucleus, and the main secondary structure of Trihelix protein was random coil and α helix. In the promoter region of Trihelix, cis-acting regulatory elements related to various abiotic stresses such as low temperature, hormone response, and growth and development were identified. Through the collinearity analysis of interspecific Trihelix transcription factors of model plants Arabidopsis thaliana and ginseng, 19 collinear gene pairs were found between A. thaliana and ginseng, and no collinear gene pairs existed on chromosomes 3, 6, and 12 only. qRT-PCR analysis showed that the expression of GWHGBEIJ010320.1 was significantly up-regulated under low temperature stress, a significant response to low temperature stress. This study lays a foundation for further research on the role of the Trihelix transcription factor of ginseng in abiotic stress, as well as the growth and development of ginseng.
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  • 文章类型: Journal Article
    人参,一种重要的药用植物,以其主要活性成分为特征,人参皂苷。在40多种人参皂苷中,Rg1是用于测定人参质量的人参皂苷之一。因此,Rg1生物合成基因的鉴定和表征对于阐明Rg1生物合成的分子基础很重要。在这项研究中,我们利用了吉林省344个核心人参品种的39,327个SNP和相应的Rg1含量。我们进行了全基因组关联研究(GWAS)结合加权基因共表达网络分析(WGCNA),SNP-Rg1含量关联分析,和基因共表达网络分析;鉴定了三个候选Rg1基因(PgRg1-1,PgRg1-2和PgRg1-3)和一个关键候选基因(PgRg1-3)。使用茉莉酸甲酯(MeJA)调节和RNAi进行PgRg1-3的功能验证,证实该基因调节Rg1生物合成。PgRg1-3基因和已知参与人参皂苷生物合成的关键酶基因的时空表达模式不同。此外,它们的网络变化对Rg1的生物合成有显著影响。本研究建立了一种准确、高效的候选基因鉴定方法,克隆了一个控制Rg1生物合成的新基因,并鉴定出73个与Rg1含量显著相关的SNP。这为进一步探索Rg1生物合成的分子机制和分子育种提供了遗传资源和有效工具。
    Ginseng, an important medicinal plant, is characterized by its main active component, ginsenosides. Among more than 40 ginsenosides, Rg1 is one of the ginsenosides used for measuring the quality of ginseng. Therefore, the identification and characterization of genes for Rg1 biosynthesis are important to elucidate the molecular basis of Rg1 biosynthesis. In this study, we utilized 39,327 SNPs and the corresponding Rg1 content from 344 core ginseng cultivars from Jilin Province. We conducted a genome-wide association study (GWAS) combining weighted gene co-expression network analysis (WGCNA), SNP-Rg1 content association analysis, and gene co-expression network analysis; three candidate Rg1 genes (PgRg1-1, PgRg1-2, and PgRg1-3) and one crucial candidate gene (PgRg1-3) were identified. Functional validation of PgRg1-3 was performed using methyl jasmonate (MeJA) regulation and RNAi, confirming that this gene regulates Rg1 biosynthesis. The spatial-temporal expression patterns of the PgRg1-3 gene and known key enzyme genes involved in ginsenoside biosynthesis differ. Furthermore, variations in their networks have a significant impact on Rg1 biosynthesis. This study established an accurate and efficient method for identifying candidate genes, cloned a novel gene controlling Rg1 biosynthesis, and identified 73 SNPs significantly associated with Rg1 content. This provides genetic resources and effective tools for further exploring the molecular mechanisms of Rg1 biosynthesis and molecular breeding.
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  • 文章类型: Journal Article
    简介:与老年人相关的脑损伤和肠道微生物组破坏很常见。研究证实,调节微生物群-肠-脑轴可以帮助减少与年龄相关的脑损伤。方法:人参,受人尊敬的中医,以其抗衰老能力而闻名。然而,以前的人参抗衰老研究主要集中在患病的动物模型上。为此,因此,我们努力探索补充人参的老年小鼠粪便微生物群移植(FMT)对抗生素预处理的小鼠的潜在神经保护作用。结果:结果,在自然衰老小鼠中进行特定修饰的FMT改善了动物体重增加,延长端粒长度,脑组织抗氧化应激,调节细胞因子的血清水平,平衡Treg细胞的比例.此外,FMT增加了虎尾草科有益菌的丰度,Dubosiella,拟杆菌,等。并降低了自然衰老小鼠粪便样本中潜在致病菌螺杆菌和幼虫的水平。这表明FMT显著地重塑了肠道微生物组。此外,FMT处理的老年小鼠显示熊果酸代谢物水平升高,β-胡萝卜素,S-腺苷甲硫氨酸,亚精胺,鸟苷,塞来昔布,亚油酸,等。,与上述关键有益菌呈显著正相关。此外,这些确定的关键微生物群和代谢产物主要富集在氨基酸代谢途径中,脂质代谢,核苷酸代谢,等。此外,FMT下调p53/p21/Rb信号并上调p16/p14、ATM/突触素I/突触素/PSD95、CREB/ERK/AKT信号在自然衰老后脑损伤中的作用。讨论:总的来说,这项研究表明,FMT对肠道微生物群的重编程阻碍了自然衰老过程中的脑损伤,可能是通过调节微生物群-肠-脑轴。
    Introduction: Aged-related brain damage and gut microbiome disruption are common. Research affirms that modulating the microbiota-gut-brain axis can help reduce age-related brain damage. Methods: Ginseng, esteemed in traditional Chinese medicine, is recognized for its anti-aging capabilities. However, previous Ginseng anti-aging studies have largely focused on diseased animal models. To this end, efforts were hereby made to explore the potential neuroprotective effects of fecal microbiota transplantation (FMT) from Ginseng-supplemented aged mice to those pre-treated with antibiotics. Results: As a result, FMT with specific modifications in natural aging mice improved animal weight gain, extended the telomere length, anti-oxidative stress in brain tissue, regulated the serum levels of cytokine, and balanced the proportion of Treg cells. Besides, FMT increased the abundance of beneficial bacteria of Lachnospiraceae, Dubosiella, Bacteroides, etc. and decreased the levels of potential pathogenic bacteria of Helicobacter and Lachnoclostridium in the fecal samples of natural aged mice. This revealed that FMT remarkably reshaped gut microbiome. Additionally, FMT-treated aged mice showed increased levels of metabolites of Ursolic acid, β-carotene, S-Adenosylmethionine, Spermidine, Guanosine, Celecoxib, Linoleic acid, etc., which were significantly positively correlated with critical beneficial bacteria above. Additionally, these identified critical microbiota and metabolites were mainly enriched in the pathways of Amino acid metabolism, Lipid metabolism, Nucleotide metabolism, etc. Furthermore, FMT downregulated p53/p21/Rb signaling and upregulated p16/p14, ATM/synapsin I/synaptophysin/PSD95, CREB/ERK/AKT signaling in brain damage following natural aging. Discussion: Overall, the study demonstrates that reprogramming of gut microbiota by FMT impedes brain damage in the natural aging process, possibly through the regulation of microbiota-gut-brain axis.
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  • 文章类型: Journal Article
    人参在东方文化中被认为是一种具有神奇功效的珍贵药草。人参的主要化学成分是皂苷,人参皂苷的生理活性决定了其食用和药用价值。本研究的目的是全面系统地研究20(S)-原人参二醇(PPD)在大鼠和犬体内的动力学过程,以促进人参作为药物和膳食成分的合理结合。
    给予PPD,采用液相色谱串联质谱(LC/MS/MS)和放射性示踪法检测不同生物样品中的药物浓度。药代动力学参数,如吸收,生物利用度,组织分布,血浆蛋白结合率,排泄率,并计算了累积排泄量,以及主要代谢物的推断。
    这项研究系统地研究了吸收,分布,新陈代谢,PPD在大鼠和犬中的排泄(ADME)为首次。PPD的生物利用度相对较低,口服吸收几乎完全,大多数人经历了首过代谢。PPD具有高的血浆蛋白结合率并且在体内相对均匀地分布。口服后,PPD经历了广泛的代谢,可能涉及一个结构转变和三个羟基化反应。代谢产物主要通过粪便和尿液排出,表明存在肝肠循环。静脉内给药后PPD的药代动力学过程与三室模型吻合良好。相比之下,经胃给药后,它更适合两个隔间的模型,符合线性药代动力学和比例消除。在PPD方面,大鼠和狗之间存在明显的种间差异,但是这种药物在同一物种中的个体差异很小。
    本研究系统研究了大鼠PPD的动力学过程,并首次研究了犬PPD的动力学特征。这些发现为进一步研究PPD的膳食营养和药理作用奠定了基础。
    UNASSIGNED: Ginseng has been regarded as a precious medicinal herb with miraculous effects in Eastern culture. The primary chemical constituents of ginseng are saponins, and the physiological activities of ginsenosides determine their edible and medicinal value. The aim of this study is to comprehensively and systematically investigate the kinetic processes of 20(S)-protopanaxadiol (PPD) in rats and dogs, in order to promote the rational combination of ginseng as a drug and dietary ingredient.
    UNASSIGNED: PPD was administered, and drug concentration in different biological samples were detected by liquid chromatography tandem mass spectrometry (LC/MS/MS) and radioactive tracer methods. Pharmacokinetic parameters such as absorption, bioavailability, tissue distribution, plasma protein binding rate, excretion rate, and cumulative excretion were calculated, along with inference of major metabolites.
    UNASSIGNED: This study systematically investigated the absorption, distribution, metabolism, excretion (ADME) of PPD in rats and dogs for the first time. The bioavailabilities of PPD were relatively low, with oral absorption nearly complete, and the majority underwent first-pass metabolism. PPD had a high plasma protein binding rate and was relatively evenly distributed in the body. Following oral administration, PPD underwent extensive metabolism, potentially involving one structural transformation and three hydroxylation reactions. The metabolites were primarily excreted through feces and urine, indicating the presence of enterohepatic circulation. The pharmacokinetic processes of PPD following intravenous administration aligned well with a three-compartment model. In contrast, after gastric administration, it fitted better with a two-compartment model, conforming to linear pharmacokinetics and proportional elimination. There were evident interspecies differences between rats and dogs regarding PPD, but individual variations of this drug were minimal within the same species.
    UNASSIGNED: This study systematically studied the kinetic process of PPD in rats and also investigated the kinetic characteristics of PPD in dogs for the first time. These findings lay the foundation for further research on the dietary nutrition and pharmacological effects of PPD.
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  • 文章类型: Journal Article
    本研究使用Caco-2细胞模型和超高效液相色谱-电喷雾电离-串联质谱法(UPLC-ESI-MS),研究了raphani对人参C.A.Meyer(人参)中人参皂苷吸收的影响。六种主要人参皂苷(Rg1,Re,Rb1,Rb2,Rc,Rd)进行了量化。结果表明,莱佛尼提高了人参皂苷的外排率,特别是在较高的浓度下,表明它抑制了它们的吸收。该研究阐明了人参皂苷的肠道吸收过程以及莱佛子对人参的拮抗机制。
    This study examined the impact of Semen raphani on the absorption of ginsenosides from Panax ginseng C.A. Meyer (ginseng) using a Caco-2 cell model and Ultra-High-Performance Liquid Chromatography-Electrospray Ionization-Tandem Mass Spectrometry (UPLC-ESI-MS). Six primary ginsenosides (Rg1, Re, Rb1, Rb2, Rc, Rd) were quantified. Results showed that Semen Raphani increased the efflux rate of ginsenosides, particularly at higher concentrations, suggesting it inhibits their absorption. The research elucidates the intestinal absorption process of ginsenosides and the antagonistic mechanism of Semen Raphani against ginseng.
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  • 文章类型: Journal Article
    人参在生长发育过程中经常遇到环境压力。晚期胚胎发生丰富(LEA)蛋白在对抗逆境胁迫中起着至关重要的作用,特别是针对非生物挑战,在这项研究中,107个来自人参的LEA基因,跨越八个亚科,被确认,证明了重要的进化保守性,LEA2亚家族最为突出。基因复制事件,主要是分段重复,在LEA基因家族的扩展中发挥了重要作用,经过强大的净化选择。PgLEAs在22条染色体上分布不均,每个亚家族都具有独特的结构域和保守的基序。PgLEAs在各种组织中表达,在丰度和组织特异性方面表现出明显的变化。众多的监管顺式因素,与非生物胁迫和激素有关,在启动子区域鉴定。此外,PgLEAs受多种非生物胁迫相关转录因子调控。用ABA处理后,共有35个PgLEA差异表达,GA,还有IAA.23个PgLEA对干旱表现出显著但不同的反应,极端温度,和盐度压力。用关键基因PgLEA2-50转化烟草增强了转基因株系的渗透调节和抗氧化水平,提高对非生物胁迫的抵抗力。这项研究提供了对功能基因分析的见解,专注于LEA蛋白,建立了人参抗逆性研究的基础框架。
    Ginseng frequently encounters environmental stress during its growth and development. Late Embryogenesis Abundant (LEA) proteins play a crucial role in combating adversity stress, particularly against abiotic challenges In this study, 107 LEA genes from ginseng, spanning eight subfamilies, were identified, demonstrating significant evolutionary conservation, with the LEA2 subfamily being most prominent. Gene duplication events, primarily segmental duplications, have played a major role in the expansion of the LEA gene family, which has undergone strong purifying selection. PgLEAs were unevenly distributed across 22 chromosomes, with each subfamily featuring unique structural domains and conserved motifs. PgLEAs were expressed in various tissues, exhibiting distinct variations in abundance and tissue specificity. Numerous regulatory cis-elements, related to abiotic stress and hormones, were identified in the promoter region. Additionally, PgLEAs were regulated by a diverse array of abiotic stress-related transcription factors. A total of 35 PgLEAs were differentially expressed following treatments with ABA, GA, and IAA. Twenty-three PgLEAs showed significant but varied responses to drought, extreme temperatures, and salinity stress. The transformation of tobacco with the key gene PgLEA2-50 enhanced osmoregulation and antioxidant levels in transgenic lines, improving their resistance to abiotic stress. This study offers insights into functional gene analysis, focusing on LEA proteins, and establishes a foundational framework for research on ginseng\'s resilience to abiotic stress.
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  • 文章类型: Journal Article
    本研究评估了热处理对人参皂苷转化的影响以及新鲜人参中热处理的人参总皂苷(HG)对环磷酰胺(CTX)诱导的肝损伤的改善作用。LC-MS分析表明,热处理后稀有人参皂苷的含量显着增加。HG可显着减轻CTX诱导的小鼠肝组织病理学损伤。Western印迹分析表明,未经处理的人参总皂苷(UG)和HG调节Nrf2/HO-1和TLR4/MAPK通路。重要的是,这些结果可能与肠道菌群的调节有关。UG和HG显着增加了产生短链脂肪酸(SCFA)的细菌乳杆菌,并减少了产生LPS的细菌拟杆菌属和副杆菌属。肠道菌群的这些变化影响了TNF-α的水平,LPS和SCFA。总之,UG和HG通过调节肠道菌群和LPS-TLR4-MAPK通路减轻CTX诱导的肝损伤,HG更有效。HG有可能成为一种功能性食品,可以减轻化学性肝损伤。
    This study evaluated the effect of heat treatment on the conversion of ginsenoside and the ameliorative effect of heat-treated total ginsenoside (HG) from fresh ginseng on cyclophosphamide (CTX)-induced liver injury. LC-MS analysis revealed that the content of rare ginsenosides increased markedly after heat treatment. HG significantly attenuated CTX-induced hepatic histopathological injury in mice. Western blotting analysis showed that untreated total ginsenoside (UG) and HG regulated the Nrf2/HO-1 and TLR4/MAPK pathways. Importantly, these results may be relevant to the modulation of the intestinal flora. UG and HG significantly increased the short-chain fatty acids (SCFAs)-producing bacteria Lactobacillus and reduced the LPS-producing bacteria Bacteroides and Parabacteroides. These changes in intestinal flora affected the levels of TNF-α, LPS and SCFAs. In short, UG and HG alleviated CTX-induced liver injury by regulating the intestinal flora and the LPS-TLR4-MAPK pathway, and HG was more effective. HG has the potential to be a functional food that can alleviate chemical liver injury.
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  • 文章类型: Journal Article
    肠道炎症失衡和免疫功能障碍可能导致一系列肠道疾病,如炎症性肠病(IBD)和胃肠道肿瘤。作为草药之王,人参在各种疾病中发挥了广泛的药理作用。尤其是,研究表明,人参和人参皂苷在肠道系统具有很强的免疫调节和抗炎能力。在这次审查中,我们总结了人参和各种提取物如何影响肠道炎症和免疫功能,包括调节免疫平衡,调节炎症介质和细胞因子的表达,促进肠粘膜伤口愈合,预防结肠炎相关的结直肠癌,恢复肠道菌群和代谢失衡,缓解抗生素引起的腹泻,缓解肠易激综合征的症状.此外,并简要介绍了具体的实验方法和关键控制机制。
    Intestinal inflammatory imbalance and immune dysfunction may lead to a spectrum of intestinal diseases, such as inflammatory bowel disease (IBD) and gastrointestinal tumors. As the king of herbs, ginseng has exerted a wide range of pharmacological effects in various diseases. Especially, it has been shown that ginseng and ginsenosides have strong immunomodulatory and anti-inflammatory abilities in intestinal system. In this review, we summarized how ginseng and various extracts influence intestinal inflammation and immune function, including regulating the immune balance, modulating the expression of inflammatory mediators and cytokines, promoting intestinal mucosal wound healing, preventing colitis-associated colorectal cancer, recovering gut microbiota and metabolism imbalance, alleviating antibiotic-induced diarrhea, and relieving the symptoms of irritable bowel syndrome. In addition, the specific experimental methods and key control mechanisms are also briefly described.
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  • 文章类型: Journal Article
    OBJECTIVE: To explore the mechanism of ginseng in the treatment of periodontitis based on network pharmacology and molecular docking technology.
    METHODS: Potential targets of ginseng and periodontitis were obtained through various databases. The intersection targets of ginseng and periodontitis were obtained by using VENNY, the protein-protein interaction network relationship diagram was formed on the STRING platform, the core target diagram was formed by Cytoscape software, and the ginseng-active ingredient-target network diagram was constructed. The selected targets were screened for gene ontology (GO) and Kyoto encyclopedia of genes and genomes (KEGG) pathway enrichment analysis. The core targets of ginseng\'s active ingredients in treating periodontitis were analyzed by molecular docking technique.
    RESULTS: The 22 ginseng\'s active ingredients, 591 potential targets of ginseng\'s active ingredients, 2 249 periodontitis gene targets, and 145 ginseng-periodontitis intersection targets were analyzed. Ginseng had strong binding activity on core targets such as vascular endothelial growth factor A and epidermal growth factor receptor, as well as hypoxia induced-factor 1 (HIF-1) signaling pathway and phosphatidylinositol 3-kinase-protein kinase B (PI3K-Akt) signaling pathway.
    CONCLUSIONS: Ginseng and its active components can regulate several signaling pathways such as HIF-1 and PI3K-Akt, thereby indicating that ginseng may play a role in treating periodontitis through multiple pathways.
    目的: 采用网络药理学和分子对接技术探讨人参治疗牙周炎的潜在作用机制。方法: 通过多种数据库获得人参、牙周炎的潜在靶点,利用VENNY获得人参-牙周炎交集靶点,在STRING平台形成蛋白质互作网络关系图,采用Cytoscape软件形成核心靶点图并构建人参-活性成分-靶点网络图,将核心靶点进行基因本体论(GO)和京都基因与基因组百科全书(KEGG)通路富集分析,通过分子对接技术分析人参活性成分治疗牙周炎的核心靶点。结果: 分析获得22个人参活性成分、591个人参活性成分潜在作用靶点、2 249个牙周炎基因靶点和145个人参-牙周炎交集靶点。人参对血管内皮生长因子A、表皮生长因子受体等核心靶点以及低氧诱导因子-1(HIF-1)信号通路、磷脂酰肌醇3-激酶-蛋白激酶B(PI3K-Akt)信号通路分子具有较强的结合活性。结论: 人参及其活性成分可通过调节HIF-1、PI3K-Akt等多条信号通路发挥治疗牙周炎的作用。.
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  • 文章类型: Journal Article
    人参是以人参皂苷为主要生物活性成分的最受欢迎的健康促进食品。非法硫磺熏蒸导致人参皂苷转化为有毒的含硫衍生物,并降低了人参的功效/安全性。24-磺基-25-烯人参皂苷Rg1(25-烯SRg1),含硫衍生物之一,是熏蒸人参的潜在质量控制标志,但由于其未知的生成机制,可及性低。在这项研究中,金属/亚硫酸氢盐系统涉及的生成机理进行了研究和验证。硫磺熏蒸人参中25-烯SRg1的产生是硫磺熏蒸过程中形成的SO2,与水反应并电离成HSO3-。一方面,在金属/亚硫酸氢盐系统下,HSO3-产生HSO5-和自由基,将人参皂苷Rg1转化为24,25-环氧化物Rg1;另一方面,作为亲核基团,HSO3-与24,25-环氧化物Rg1反应并进一步脱水为25-烯SRg1。本研究为推广25-烯SRg1作为硫磺熏蒸人参的特征性质量控制标记提供了技术支持。
    Ginseng is a most popular health-promoting food with ginsenosides as its main bioactive ingredients. Illegal sulfur-fumigation causes ginsenosides convert to toxic sulfur-containing derivatives, and reduced the efficacy/safety of ginseng. 24-sulfo-25-ene ginsenoside Rg1 (25-ene SRg1), one of the sulfur-containing derivatives, is a potential quality control marker of fumigated ginseng, but with low accessibility owing to its unknown generation mechanism. In this study, metals/bisulfite system involved generation mechanism was investigated and verified. The generation of 25-ene SRg1 in sulfur-fumigated ginseng is that SO2, formed during sulfur-fumigation, reacted with water and ionized into HSO3-. On the one hand, under the metals/bisulfite system, HSO3- generates HSO5- and free radicals which converted ginsenoside Rg1 to 24,25-epoxide Rg1; on the other hand, as a nucleophilic group, HSO3- reacted with 24,25-epoxide Rg1 and further dehydrated to 25-ene SRg1. This study provided a technical support for the promotion of 25-ene SRg1 as the characteristic quality control marker of sulfur-fumigated ginseng.
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