Dermatophagoides farinae

粉尘螨
  • 文章类型: Journal Article
    变应原特异性免疫治疗(AIT)对链格孢菌的临床疗效(A.alt)和粉尘螨(Derf)提取物在中国仍然未知。我们试图回顾性评估中国制造的AIT药物对A.alt和Derf.
    5-27岁哮喘和常年性过敏性鼻炎(AR)患者的疗效,AIT与A.alt和Derf一起被招募,然后分为两组:A.alt-AIT(n=31)和A.altDerf-AIT组(n=39)。所有数据都是回顾性收集的,包括生物学参数,肺功能,以及症状和药物评分。
    纳入70例接受A.alt和DerfAIT的患者。在肺功能的FEV1%(P<0.0001)和MEF25(P=0.023)的值中观察到显著改善。AIT后哮喘的鼻炎症状和综合症状和药物评分均下降(分别为45.3%和80.3%,分别,各P<0.0001)。鼻结膜炎生活质量改善率近67%(P<0.0001),至少1年AIT后,哮喘控制测试(ACT)评分显著增加(P<0.0001),尽管两组间无显著变化.此外,在对不同过敏原的特异性IgE中没有显示出显著性。
    使用A.alt和Derf提取物的AIT对中国许多患者具有临床疗效,随着症状和药物评分的减少,肺活量测定功能有很大改善。
    UNASSIGNED: The clinical efficacy of allergen-specific immunotherapy (AIT) for Alternaria alternata (A. alt) and Dermatophagoides farinae (Der f) extracts remains largely unknown in China. We sought to retrospectively evaluate the efficacy caused by AIT agents manufactured in China of patients who are sensitized to A. alt and Der f.
    UNASSIGNED: Patients aged 5-27 years with asthma and perennial allergic rhinitis (AR), and AIT with A. alt and Der f were recruited, and then classified into two groups: A. alt-AIT (n = 31) and A. alt + Der f-AIT group (n = 39). All data were gathered retrospectively, including biological parameters, pulmonary function, and symptom and medication scores.
    UNASSIGNED: 70 patients who underwent A. alt and Der f AIT were enrolled. A significant improvement was observed in the values of FEV1% (P < 0.0001) and MEF 25 (P = 0.023) of lung function. Both the rhinitis symptoms and combined symptoms and medication scores for asthma decreased after AIT (by 45.3% and 80.3%, respectively, P < 0.0001 for each). Nearly 67% improvement rate (P < 0.0001) occurred in rhinoconjunctivitis quality of life, and a great increase existed in Asthma Control Test (ACT) score (P < 0.0001) after at least 1 year AIT, although there were no significant changes between these two groups. Besides, no significance was displayed in specific IgE to different allergens.
    UNASSIGNED: AIT with A. alt and Der f extracts had clinical efficacy for many patients in China, with a reduction of symptom and medication scores, and great improvement in spirometry function.
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  • 文章类型: Journal Article
    暴露于储存螨(SM)和屋尘螨(HDM)过敏原是致敏和哮喘发展的危险因素;然而,相关的免疫反应及其病理尚未得到充分研究。HDMs粉尘螨和翼状螨螨和SM热解螨是诱发哮喘的有效过敏原。大多数SM相关研究通过测量个体的免疫球蛋白(Ig)E表达来关注个体的过敏反应。考虑到对该主题的研究有限,本研究旨在研究HDM和SM诱导的免疫反应的差异,并对小鼠哮喘模型的肺组织进行组织学分析,以了解HDM和SM的差异效应.结果表明,所有螨物种都会引起气道炎症。用腐殖质T.腐殖质攻击的小鼠具有最高的气道阻力和总细胞,嗜酸性粒细胞,支气管肺泡灌洗液(BALF)中的中性粒细胞计数。SM致敏组比HDM致敏组表现出更严重的病变和粘液分泌过多。尽管HDM和SM的暴露程度相同,暴露于SM的小鼠对呼吸肺组织的损伤更为严重,导致粘蛋白分泌过多和纤维化增加。此外,这些研究结果表明,在哮喘模型中,SM致敏在粘膜免疫中诱导的超敏反应比HDM致敏更显著.
    Exposure to storage mite (SM) and house dust mite (HDM) allergens is a risk factor for sensitization and asthma development; however, the related immune responses and their pathology have not been fully investigated. The HDMs Dermatophagoides farinae and Dermatophagoides pteronyssinus and SM Tyrophagus putrescentiae are potent allergens that induce asthma. Most SM-related studies have focused on the allergic reactions of individuals by measuring their immunoglobulin (Ig)E expression. Considering the limited research on this topic, the present study aims to investigate the differences in the immune responses induced by HDMs and SMs and histologically analyze lung tissues in a mouse asthma model to understand the differential effects of HDM and SM. The results revealed that all mite species induced airway inflammation. Mice challenged with T. putrescentiae had the highest airway resistance and total cell, eosinophil, and neutrophil counts in the bronchoalveolar lavage fluid (BALF). The SM-sensitized groups showed more severe lesions and mucus hypersecretions than the HDM-sensitized groups. Although the degree of HDM and SM exposure was the same, the damage to the respiratory lung tissue was more severe in SM-exposed mice, which resulted in excessive mucin secretion and increased fibrosis. Furthermore, these findings suggest that SM sensitization induces a more significant hypersensitivity response in mucosal immunity than HDM sensitization in asthma models.
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  • 文章类型: Journal Article
    背景:粉尘螨蛋白(DFP)在D.farinae中大量表达;然而,它们的功能仍然未知。我们先前的转录组测序分析显示,DFP1和DFP2在D.farinae中的基础表达很高,并且,更重要的是,在温度胁迫下上调。因此,推测DFP发挥温度应激反应功能。
    结果:实时定量聚合酶链反应检测显示,在温度胁迫下,DFP1和DFP2均显着上调。特别是,DFP1在冷胁迫下上调。D.farinae总蛋白的电泳显示,在温度胁迫下,DFP1和DFP2(40-55kDa条带)的丰度增加,质谱结果证实了这一点。DFP1和DFP2进一步沉默后,温度胁迫导致基因表达和存活率降低。此外,DFP1被确定为DFP2的上游调节因子。
    结论:这项研究强调了DFP1和DFP2在mRNA和蛋白质水平上的温度应激反应功能。这些结果为将DFP1和DFP2作为潜在的靶基因用于预防变态反应性疾病的分子预防和控制提供了重要的见解。新建立的方法为螨虫功能未知基因的研究提供了方法学指导。
    BACKGROUND: Dermatophagoides farinae proteins (DFPs) are abundantly expressed in D. farinae; however, their functions remain unknown. Our previous transcriptome sequencing analyses revealed that the basal expression of DFP1 and DFP2 in D. farinae was high and, more importantly, upregulated under temperature stress. Therefore, DFPs were speculated to exert a temperature stress response function.
    RESULTS: Real-time quantitative polymerase chain reaction detection revealed that both DFP1 and DFP2 were significantly upregulated under temperature stress. Particularly, DFP1 was upregulated under cold stress. Electrophoresis of D. farinae total proteins revealed an increased abundance of DFP1 and DFP2 (40-55 kDa bands) under temperature stress, which was corroborated by the mass spectrometry results. After silencing DFP1 and DFP2 further, temperature stress led to decreases in gene expression and survival rates. Moreover, DFP1 was identified as the upstream regulator of DFP2.
    CONCLUSIONS: This study highlights the temperature stress response functions of DFP1 and DFP2 at the mRNA and protein levels. These results provide important insights for applying DFP1 and DFP2 as potential target genes for the molecular prevention and control of D. farinae to prevent allergic diseases. The newly established methods provide methodological guidance for the study of genes with unknown functions in mites.
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  • 文章类型: Journal Article
    背景:舌下免疫治疗(SLIT)的精确给药逐渐成为研究热点,但没有标准的剂量调整模式的屋尘螨(HDM)-SLIT。本研究旨在探讨动态维持剂量递增方案用于个体化SLIT的临床可行性。
    方法:本回顾性研究共纳入258例接受HDM-SLIT治疗的变应性鼻炎(AR)患者。根据SLIT维持剂量的不同,将患者分为常规剂量(RD)组(n=101)和高剂量(HD)组(n=157)。在RD组中,患者接受制造商推荐的固定剂量.在HD组中,患者接受动态剂量递增确定的最大耐受剂量.基线时采用症状和药物联合评分(CSMS)和视觉模拟评分法(VAS)评价临床疗效,0.5年,1年,和2年。通过不良事件(AE)评估安全性。
    结果:在0.5年时CSMS和VAS显着减少,1年,与基线相比,RD组和HD组均观察到2年(P<0.05)。此外,与RD组相比,HD组的这些临床参数在0.5~2年有更大的改善(P<0.05).对于HD组的亚组分析,<14岁和≥14岁患者的CSMS和VAS差异无统计学意义(P>0.05)。在递增阶段和维持阶段,两组均未发现严重的AE,RD组和HD组的AE发生率之间也没有显着差异。
    结论:动态维持剂量递增方案的2年HDM-SLIT为AR患者提供了“最佳”治疗,同时保持了安全性。这项研究引入了临床实践中个性化剂量调整的模式,为AR患者提供潜在的益处。
    BACKGROUND: Precision dosing in sublingual immunotherapy (SLIT) has become a hotspot gradually, yet no standardized dose adjustment pattern for house dust mite (HDM)-SLIT. This study aims to investigate the clinical feasibility of the dynamic maintenance dose ascending regimen for individualized SLIT.
    METHODS: A total of 258 allergic rhinitis (AR) patients treated with HDM-SLIT were included in this retrospective study. Patients were divided into the regular dose (RD) group (n = 101) and the high dose (HD) group (n = 157) according to different maintenance dosages of SLIT. In the RD group, patients received the fixed dose recommended by the manufacturer. In the HD group, patients received a maximum tolerance dose determined by dynamic dose ascending. The clinical efficacy was evaluated by combined symptom and medication score (CSMS) and visual analogue scale score (VAS) at the baseline, 0.5-year, 1-year, and 2-year. The safety was evaluated by adverse events (AEs).
    RESULTS: Significant reductions of CSMS and VAS at 0.5-year, 1-year, and 2-year were observed in both the RD group and the HD group compared to the baseline (P < 0.05). In addition, greater improvements in these clinical parameters from 0.5- to 2-year were found in the HD group compared to the RD group (P < 0.05). For subgroup analysis in the HD group, no significant differences in CSMS and VAS were observed among subgroups of patients <14 years old and patients ≥14 years old (P > 0.05). No serious AEs in the two groups and no significant differences were observed between the AE incidence rate of the RD group and HD group during the incremental and maintenance phases.
    CONCLUSIONS: The 2-year HDM-SLIT with dynamic maintenance dose ascending regimen offers an \"optimal\" treatment for AR patients while maintaining safety. This study introduced a pattern for individualized dose adjustment in clinical practice, offering potential benefits for AR patients.
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  • 文章类型: Journal Article
    粉尘螨(D.farinae)和翼状螨(D.翼楼)是常见的室内尘螨(HDMs)。HDMs是常见的吸入性过敏原,会导致一系列过敏性疾病,如鼻炎,特应性皮炎,和哮喘。这些疾病的流行病学与暴露于螨虫有关。因此,在本研究中,开发了一种称为多重环介导等温扩增(LAMP)的方法来检测环境尘螨。多重LAMP测定法允许在单个管中进行扩增,并且对于单个尘螨和混合尘螨,ITS质粒检测限均低至40fg/µL(D.翼楼和D.farinae),比经典的PCR技术灵敏十倍。此外,将多重LAMP方法应用于单个尘螨和临床粉尘样品,以确认其有效性。多重LAMP分析显示出更高的灵敏度,更简单的仪器,以及测试结果的可视化,表明该方法可以用作传统的HDM检测技术的替代方法。
    Dermatophagoides farina (D. farinae) and Dermatophagoides pteronyssinus (D. pteronyssinus) are the prevalent kinds of house dust mites (HDMs). HDMs are common inhalant allergens that cause a range of allergic diseases, such as rhinitis, atopic dermatitis, and asthma. The epidemiology of these diseases is associated with exposure to mites. Therefore, in the present study, a method named multiplex loop-mediated isothermal amplification (LAMP) was developed to detect environmental dust mites. The multiplex LAMP assay allows amplification within a single tube and has an ITS plasmid detection limit as low as 40 fg/µL for both single dust mites and mixed dust mites (D. pteronyssinus and D. farinae), which is up to ten times more sensitive than classical PCR techniques. Furthermore, the multiplex LAMP method was applied to samples of single dust mites and clinical dust to confirm its validity. The multiplex LAMP assay exhibited higher sensitivity, simpler instrumentation, and visualization of test results, indicating that this method could be used as an alternative to traditional techniques for the detection of HDMs.
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  • 文章类型: Journal Article
    背景:翼状螨和粉尘螨属于Pyroglyphidae家族(“Dermaticoidinae”亚家族),分别具有Derp1,Derp2和Derp23以及Derf1和Derf2的变应原蛋白。欧照梅尼,属于Pyroglyphidae家族(亚家族:“Pyroglyphinae”),其主要致敏蛋白是Eurm1,一种致敏来源。通过皮肤试验评估对D.pteronysinus和D.farinae的敏感性,而对E.maynei的敏感性评估较少。
    目的:这项实验工作旨在分析在巴里的M.Albanesi过敏和免疫学部门治疗的呼吸道过敏患者对E.maynei的致敏率,意大利,并分析了E.maynei与D.farinae和D.pteronysinus的主要致敏蛋白的序列同源性。
    方法:在这项现实生活中的研究中,65例患者入组。特别是,呼吸道过敏患者接受了常见呼吸道过敏原的皮肤点刺试验,包括欧彩玛尼.在E.maynei的主要过敏原蛋白与D.pteronysinus和D.farinae的主要过敏原蛋白之间进行序列同源性分析。
    结果:对E.maynei敏感的患者占41.5%。所有患有E.maynei致敏的患者均对D.farinae和D.pteronysinus致敏。Derp1和Derf1蛋白与Eurm1蛋白序列的序列同源性分析显示出84.4%和86%的同一性,分别。
    结论:近50%的屋尘螨致敏患者对E.maynei有伴随致敏作用。交叉敏化可能是由于Derf1、Derp1和Eurm1相似性。
    BACKGROUND: Dermatophagoides pteronyssinus and Dermatophagoides farinae belong to the family Pyroglyphidae (subfamily: \"Dermatophagoidinae\") and have the respective allergenic proteins of Der p1, Der p2, and Der p23 and Der f1 and Der f2. Euroglyphus maynei, belongs to the family Pyroglyphidae (subfamily: \"Pyroglyphinae\") and its main allergenic protein is Eur m1, a source of sensitization. Sensitization to D. pteronyssinus and D. farinae is assessed through skin tests, while sensitization to E. maynei is assessed less frequently.
    OBJECTIVE: This experimental work aims to analyze the prevalence of sensitization to E. maynei in patients with respiratory allergies treated at M. Albanesi Allergy and Immunology Unit in Bari, Italy, and the sequence homology of major allergenic proteins of E. maynei with D. farinae and D. pteronyssinus was analyzed.
    METHODS: In this real-life study, 65 patients were enrolled. In particular, patients with respiratory allergy were subjected to skin prick tests for common respiratory allergens, including Euroglyphus maynei. The sequence homology analysis was performed between the major allergenic proteins of E. maynei and those of D. pteronyssinus and D. farinae.
    RESULTS: Sensitization to E. maynei accounts for 41.5% of patients. All patients with E. maynei sensitization had concomitant sensitization to D. farinae and D. pteronyssinus. The analysis of sequence homology of Der p1 and Der f1 proteins with the sequence of Eur m1 protein demonstrated an identity of 84.4% and 86%, respectively.
    CONCLUSIONS: Nearly 50% of house dust mites-sensitized patients have a concomitant sensitization to E. maynei. The cross-sensitization could be due to Der f1, Der p1, and Eur m1 similarity.
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  • 文章类型: Journal Article
    粉尘螨中高表达基因DFP1和DFP2的功能仍然未知。在我们之前的RNA-seq研究中,DFP1和DFP2已被大量注释,并且在43°C和-10°C的温度胁迫下上调。表明DFP1和DFP2可能具有温度应激反应功能。这里,我们放大了,克隆,并测序获得DFP1和DFP2的完整编码序列,并利用生物信息学分析预测其蛋白特征。然后,构建了原核表达系统,发现DFP1在大肠杆菌Rosetta-gami2(DE3)中表达,而在BL21(DE3)中不表达;DFP2在BL21(DE3)和Rosetta-gami2(DE3)中表达,在BL21(DE3)中具有较高的表达。最后,绘制了细菌的生长曲线,表明在热和冷胁迫后,携带DFP1-和DFP2-pET32a的重组细菌比仅携带pET32a的对照细菌生长更好。这项研究首次证实了DFP1和DFP2在蛋白质水平上对温度应激的反应。构建的原核表达系统将为将来用于蛋白质印迹检测以证实DFP1和DFP2的温度-应激反应功能的抗体制备提供实验基础。
    The functions of highly expressed genes DFP1 and DFP2 in Dermatophagoides farinae remain unknown. DFP1 and DFP2 have been abundantly annotated and were up-regulated under temperature stress at 43 °C and -10 °C in our previous RNA-seq study, indicating that DFP1 and DFP2 may have temperature stress response function. Here, we amplified, cloned, and sequenced to obtain the complete coding sequences of DFP1 and DFP2 and predicted their protein characteristics using bioinformatics analysis. Then, prokaryotic expression systems were constructed and found that DFP1 was expressed in Escherichia coli Rosetta-gami 2 (DE3) but not BL21 (DE3); DFP2 was expressed in both BL21 (DE3) and Rosetta-gami 2 (DE3), with higher expression in BL21 (DE3). Finally, the growth curves of bacteria were drawn and indicated that the DFP1- and DFP2-pET32a carrying recombinant bacteria grew better than the respectiveonly pET32a carrying control bacteria after heat and cold stress. This study confirms for the first time that DFP1 and DFP2 respond to temperature stress at the protein level. The constructed prokaryotic expression systems will provide an experimental foundation for future antibody preparation for western blotting detection to confirm the temperature-stress response functions of DFP1 and DFP2.
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  • 文章类型: Journal Article
    特应性皮炎(AD)是一种全球范围内不断增加的慢性炎症性皮肤病,具有有限且潜在的副作用倾向的治疗选择。单曲霉素是巴林达中主要的环烯醚萜苷,先前已显示出缓解AD症状的希望。本研究旨在通过2,4-二硝基氯苯(DNCB)/粉尘螨提取物(DFE)诱导的AD小鼠和肿瘤坏死因子(TNF)-α/干扰素(IFN)-γ刺激的角质形成细胞,系统研究单曲霉素对AD的药理作用。口服单曲霉素显示AD表型显著减少,包括缩放,红斑,和增加AD诱导小鼠的皮肤厚度。组织学分析显示,皮肤病变中免疫细胞浸润明显减少。此外,单曲霉素有效下调炎症标志物,包括促炎细胞因子,T辅助(Th)1和Th2细胞因子,和皮肤组织中的促炎趋化因子。值得注意的是,单曲霉素还导致血清免疫球蛋白(Ig)E和IgG2a水平显着降低。在机械层面,单曲霉素通过抑制AD诱导小鼠皮肤组织和TNF-α/IFN-γ刺激的角质形成细胞中Janus激酶/信号转导子和转录蛋白激活子的磷酸化来发挥其抗炎作用。总之,在使用的实验模型中,单曲霉素表现出明显的AD症状缓解。这些发现强调了单曲霉素作为治疗药物在AD中的潜在应用。为进一步勘探开发提供科学依据。
    Atopic dermatitis (AD) is a globally increasing chronic inflammatory skin disease with limited and potentially side-effect-prone treatment options. Monotropein is the predominant iridoid glycoside in Morinda officinalis How roots, which has previously shown promise in alleviating AD symptoms. This study aimed to systematically investigate the pharmacological effects of monotropein on AD using a 2, 4-dinitrochlorobenzene (DNCB)/Dermatophagoides farinae extract (DFE)-induced AD mice and tumor necrosis factor (TNF)-α/interferon (IFN)-γ-stimulated keratinocytes. Oral administration of monotropein demonstrated a significant reduction in AD phenotypes, including scaling, erythema, and increased skin thickness in AD-induced mice. Histological analysis revealed a marked decrease in immune cell infiltration in skin lesions. Additionally, monotropein effectively downregulated inflammatory markers, encompassing pro-inflammatory cytokines, T helper (Th)1 and Th2 cytokines, and pro-inflammatory chemokines in skin tissues. Notably, monotropein also led to a considerable decrease in serum immunoglobulin (Ig)E and IgG2a levels. At a mechanistic level, monotropein exerted its anti-inflammatory effects by suppressing the phosphorylation of Janus kinase / signal transducer and activator of transcription proteins in both skin tissues of AD-induced mice and TNF-α/IFN-γ-stimulated keratinocytes. In conclusion, monotropein exhibited a pronounced alleviation of AD symptoms in the experimental models used. These findings underscore the potential application of monotropein as a therapeutic agent in the context of AD, providing a scientific basis for further exploration and development.
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  • 文章类型: Journal Article
    目的:本研究旨在探讨标准化粉尘螨滴剂舌下免疫疗法(SLIT)治疗尘螨致敏儿童变应性鼻炎(AR)的临床疗效和安全性。这些发现有助于为未来对AR治疗的深入研究奠定初步基础。
    方法:根据血清学检查结果,将152例接受SLIT的AR患儿分为两组:吸入组(尘螨合并吸入过敏)和摄入组(尘螨合并摄入过敏)。通过评估鼻部症状总评分(TNSS)评价临床疗效和安全性,药物总评分(TMS),视觉模拟量表评分(VAS评分),治疗前和治疗两年后的不良反应发生率。
    结果:经过两年的治疗,TNSS,TMS,与吸入组和摄入组的治疗前值相比,VAS评分显着改善(p<0.05)。然而,两组治疗2年后疗效差异无统计学意义(p>0.05)。在治疗期间,只有15例(10.9%,吸入组9例,摄入组6例)出现轻度不良反应。两组不良反应发生率差异无统计学意义(p>0.05)。
    结论:SLIT使用标准化粉尘螨滴剂对AR患儿具有长期疗效,无论它们属于吸入或摄入组,治疗结果无显著差异。
    OBJECTIVE: This study aimed to investigate the clinical efficacy and safety of sublingual immunotherapy (SLIT) using standardized dermatophagoides farina drops for the treatment of allergic rhinitis (AR) in children sensitized to dust mites combined with different allergens. The findings contribute to establishing a preliminary foundation for future in-depth studies on AR treatment.
    METHODS: A total of 152 AR children undergoing SLIT were categorized into two groups based on serological test results: the inhalation group (dust mite combined with inhalation allergy) and the ingestion group (dust mite combined with ingestion allergy). The clinical efficacy and safety were evaluated by assessing the total nasal symptoms score (TNSS), total medication scores (TMS), visual analog scale scores (VAS scores), and the incidence of adverse reactions before treatment and after two years of treatment.
    RESULTS: After two years of treatment, TNSS, TMS, and VAS scores significantly improved compared to pre-treatment values in both the inhalation and ingestion groups (p < 0.05). However, there were no significant differences in efficacy between the two groups after two years of treatment (p > 0.05). During the treatment period, only 15 cases (10.9 %, 9 cases in the inhalation group and 6 cases in the ingestion group) experienced mild adverse reactions. There was no significant difference in the incidence of adverse reactions between the two groups (p > 0.05).
    CONCLUSIONS: SLIT using standardized dermatophagoides farina drops demonstrates long-term efficacy in children with AR, regardless of whether they belong to the inhalation or ingestion group, without significant differences in treatment outcomes.
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  • 文章类型: Journal Article
    特应性皮炎(AD)是一种以皮肤屏障功能障碍和慢性炎症反应为特征的慢性炎症性皮肤病。日本雷诺菌,在中医中被称为虎掌,可以增强血液循环,消除风病原体和终止咳嗽。尽管有药理学证据支持金黄在抑制水肿引起的皮肤炎症或结缔组织疾病方面的功效,其治疗AD样皮肤炎症的药物潜力仍未被开发。本研究探讨了金花乙醇提取物(RJE)对粉尘螨提取物(DfE)诱导的NC/Nga小鼠AD样皮肤炎症的可能影响。为了阐明RJE抑制皮肤炎症的潜在机制,我们研究了RJE对人表皮角质形成细胞(HEKs)和人真皮成纤维细胞(HDFs)中IFN-γ/TNF-α诱导的信号转导和转录激活因子(STAT)信号传导的影响。我们的发现揭示RJE减轻了DfE诱导的AD样症状和小鼠皮肤损伤中的皮肤屏障破坏。此外,RJE减弱DfE诱导的肥大细胞浸润和血清炎性细胞因子水平(IL-1α,IL-1β,IL-6,IL-23,IFN-γ,TNF-α,和GM-CSF)。RJE还抑制HEK和HDF中IFN-γ/TNF-α诱导的趋化因子水平和STAT3磷酸化。RJE成分的虚拟结合分析表明大黄素-8-β-D-葡萄糖苷与Janus激酶(JAK)1/2结合,从而抑制STAT信号传导,通过蛋白质印迹分析证实。总之,我们的研究结果表明,RJE可能通过抑制JAK/STAT信号,缓解DfE诱导的皮肤屏障功能障碍,并通过抑制AD样皮肤病中的炎症介质,缓解促炎免疫反应.这些发现表明RJE具有作为AD管理的有效疗法的潜力。
    Atopic dermatitis (AD) is a chronic inflammatory skin disease characterized by skin barrier dysfunction and chronic inflammatory responses. Reynoutria japonica, known as Huzhang in traditional Chinese Medicine, can enhance blood circulation to eliminate wind pathogens and terminate coughing. Despite pharmacological evidence supporting the efficacy of R. japonica in suppressing edema-induced skin inflammation or connective tissue diseases, its pharmaceutical potential for treating AD-like skin inflammation remains unexplored. This study investigated the possible effects of R. japonica ethanol extract (RJE) on Dermatophagoides farinae extract (DfE)-induced AD-like skin inflammation in NC/Nga mice. To elucidate the underlying mechanisms by which RJE inhibits skin inflammation, we examined the effect of RJE on IFN-γ/TNF-α-induced signal transducer and activator of transcription (STAT) signaling in human epidermal keratinocytes (HEKs) and human dermal fibroblasts (HDFs). Our findings revealed that RJE mitigates DfE-induced AD-like symptoms and skin barrier disruptions in mouse skin lesions. Moreover, RJE attenuated DfE-induced mast cell infiltration and serum levels of inflammatory cytokines (IL-1α, IL-1β, IL-6, IL-23, IFN-γ, TNF-α, and GM-CSF). RJE also inhibited IFN-γ/TNF-α-induced chemokine levels and STAT3 phosphorylation in HEKs and HDFs. Virtual binding analysis of the RJE components suggested that emodin-8-β-D-glucoside binds to Janus kinase (JAK) 1/2, thereby suppressing STAT signaling, which was confirmed by Western blot analysis. In conclusion, our results suggest that RJE may alleviate DfE-induced skin barrier dysfunction by inhibiting JAK/STAT signaling and the proinflammatory immune response through the suppression of inflammatory mediators in AD-like skin disease. These findings suggest that RJE has potential as an effective therapy for AD management.
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