endotoxin

内毒素
  • 文章类型: Journal Article
    目前用于测试粪便污染的水的方法依赖于粪便指示细菌(FIB;大肠杆菌和肠球菌)的培养,需要24-48小时,这导致采取积极措施的延误,并对公众健康构成风险。因此需要更快速的方法。这里,我们测试了一种快速的,便携式测定(细菌),在30分钟内检测细菌生物标志物内毒素,以量化存在的细菌生物量,评估159个沿海水样,并将结果与FIB的传统培养进行比较。以内毒素风险(ER)单位给出的细菌数据与FIB培养物之间存在显着相关性,可以使用EU沐浴指令值准确区分差,充足或优质的沐浴水。接收器工作特性分析用于确定沿海水样的最佳ER阈值,曲线下面积为0.9176,p值<0.0001。最佳阈值为7,300个ER单位,灵敏度为95.45%,特异性为83.48%。总之,我们已经证明,细菌测定提供了一种快速且易于使用的原位方法来评估沐浴水质。
    Current methods for testing water for faecal contamination rely on the culture of faecal indicator bacteria (FIB; Escherichia coli and Enterococci) that take 24-48 h, which leads to delays in taking proactive measures and poses a risk to public health. More rapid methods are therefore required. Here, we have tested a rapid, portable assay (Bacterisk) that detects the bacterial biomarker endotoxin in 30 min to quantify the bacterial biomass present, to evaluate 159 coastal water samples and to compare the results with the traditional culture of FIB. There was a significant correlation between the Bacterisk data given in endotoxin risk (ER) units and FIB culture that could accurately distinguish between poor and sufficient or good quality bathing water using the EU bathing directive values. Receiver operating characteristic analysis was used to determine the optimal ER threshold for coastal water samples, and the area under the curve was 0.9176 with a p-value of <0.0001. The optimal threshold was 7,300 ER units with a sensitivity of 95.45% and a specificity of 83.48%. In conclusion, we have shown that the Bacterisk assay provides a rapid and easy-to-use in situ method to assess bathing water quality.
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  • 文章类型: Journal Article
    当前对空气质量或控制有效性的评估仅基于颗粒物(PM)质量水平,不考虑它们在健康益处方面的毒性差异。这里,我们收集了来自中国31个主要城市的465个汽车空调过滤器,以在全国范围内研究PM的成分和毒性。二硫苏糖醇测定表明,中国不同城市的归一化PM毒性(NIOG)差异很大,从长沙的最高4.99×10-3到银川的最低7.72×10-4。观察到NIOG值与年PM10浓度(r=-0.416,p=0.020)和一些PM成分(总真菌,SO42-和钙元素)。中国31个城市的PM中不同元素和水溶性离子的浓度也有几个数量级的变化。在中国31个城市中,使用limulus动物细胞裂解物测定法分析的PM中的内毒素浓度范围为2.88EU/mgPM(杭州)至62.82EU/mgPM(石家庄)。此外,实时qPCR显示,中国31个城市的总细菌和真菌水平差异为10~100倍。化学物质(水溶性离子和微量元素)和生物(真菌,发现PM中的细菌和内毒素)成分与某些气象因素和SO2等气态污染物显着相关。我们的结果表明,来自31个主要城市的PM毒性差异很大,差异高达6.5倍;PM中的真菌和SO42-等成分可能在观察到的PM毒性中起重要作用。应制定结合毒性因素的针对城市的空气污染控制策略,以最大程度地提高健康和经济上的共同利益。这项工作还提供了对中国整体PM污染状况的全面看法。
    Current assessment of air quality or control effectiveness is solely based on particulate matter (PM) mass levels, without considering their toxicity differences in terms of health benefits. Here, we collected a total of 465 automobile air conditioning filters from 31 major Chinese cities to study the composition and toxicity of PM at a national scale. Dithiothreitol assay showed that normalized PM toxicity (NIOG) in different Chinese cities varied greatly from the highest 4.99 × 10-3 for Changsha to the lowest 7.72 × 10-4 for Yinchuan. NIOG values were observed to have significant correlations with annual PM10 concentration (r = -0.416, p = 0.020) and some PM components (total fungi, SO4 2- and calcium element). The concentrations of different elements and water-soluble ions in PM also varied by several orders of magnitude for 31 cities in China. Endotoxin concentrations in PM analyzed using limulus amebocyte lysate assay ranged from 2.88 EU/mg PM (Hangzhou) to 62.82 EU/mg PM (Shijiazhuang) among 31 Chinese cities. Besides, real-time qPCR revealed 10∼100-fold differences in total bacterial and fungal levels among 31 Chinese cities. The concentrations of chemical (water soluble ions and trace elements) and biological (fungi, bacteria and endotoxin) components in PM were found to be significantly correlated with some meteorological factors and gaseous pollutants such as SO2. Our results have demonstrated that PM toxicity from 31 major cities varied greatly up to 6.5 times difference; and components such as fungi and SO4 2- in PM could play important roles in the observed PM toxicity. The city-specific air pollution control strategy that integrates toxicity factors should be enacted in order to maximize health and economic co-benefits. This work also provides a comprehensive view on the overall PM pollution situation in China.
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  • 文章类型: Journal Article
    这项研究比较了源自过表达hsa-let-7i-5p的RAW264.7细胞的工程化外泌体(工程化外泌体)与来自人胎盘来源的间充质干细胞(hpMSC外泌体)的外泌体对脓毒症诱导的急性肺损伤的治疗效果。成年雄性C57BL/6小鼠分为脂多糖(LPS),LPS加工程外泌体(LEExo),或LPS加hpMSC外泌体(LMExo)组,与对照组并驾齐驱。结果显示,肺损伤评分(基于病理组织学特征)和肺功能改变的水平,组织水肿,LEExo和LMExo组的白细胞浸润具有可比性,并明显低于LPS组(均p<0.05)。此外,炎症水平(核因子-κB激活,细胞因子上调),巨噬细胞活化(缺氧诱导因子-1α活化,M1相位极化),氧化,与LPS组相比,LEExo和LMExo组的细胞凋亡减少(均p<0.05)。hsa-let-7i-5p的抑制减弱了工程和hpMSC外泌体的治疗效果。这些发现强调了富含hsa-let-7i-5p的工程外泌体的有效治疗能力,以及它们作为hpMSC外泌体替代脓毒症治疗的潜力。对工程化外泌体的作用机制和优化的持续研究可以为其未来的临床应用铺平道路。
    This study compared the therapeutic effects of engineered exosomes derived from RAW264.7 cells overexpressing hsa-let-7i-5p (engineered exosomes) to exosomes from human placenta-derived mesenchymal stem cells (hpMSC exosomes) against sepsis-induced acute lung injury. Adult male C57BL/6 mice were divided into lipopolysaccharide (LPS), LPS plus engineered exosome (LEExo), or LPS plus hpMSC exosome (LMExo) groups, alongside control groups. The results showed that lung injury scores (based on pathohistological characteristics) and the levels of lung function alterations, tissue edema, and leukocyte infiltration in LEExo and LMExo groups were comparable and significantly lower than in the LPS group (all p < 0.05). Furthermore, the levels of inflammation (nuclear factor-κB activation, cytokine upregulation), macrophage activation (hypoxia-inducible factor-1α activation, M1 phase polarization), oxidation, and apoptosis were diminished in LEExo and LMExo groups compared to the LPS group (all p < 0.05). Inhibition of hsa-let-7i-5p attenuated the therapeutic effects of both engineered and hpMSC exosomes. These findings underscore the potent therapeutic capacity of engineered exosomes enriched with hsa-let-7i-5p and their potential as an alternative to hpMSC exosomes for sepsis treatment. Continued research into the mechanisms of action and optimization of engineered exosomes could pave the way for their future clinical application.
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  • 文章类型: Journal Article
    用于低内毒素恢复(LER)研究的自然发生内毒素(NOE)的评估一直是行业中的一个主题,并且监管机构一直不愿认可NOE在LER研究中的使用,而不是纯化的脂多糖(LPS)标准,例如对照标准内毒素(CSE)或参考标准内毒素(RSE)。在最近的一项研究中,涉及13个站点的11个BioPhorum成员公司,在两种常见的单克隆抗体缓冲液制剂中评估了在高和低营养条件下制备的NOE:10mM柠檬酸钠,0.05%聚山梨酯80,pH6.0和20mM组氨酸,0.05%聚山梨酯80,pH6.0。12g阴性细菌分离物用于制备NOE分析物,将其掺入制剂缓冲液中。此外,将NOE掺加到LibrusAmebocyte裂解物(LAL)试剂水中作为对照,并将纯化的LPS掺入柠檬酸盐/聚山梨酯缓冲液中作为LER对照。结果显示,每个生物体三次运行的平均回收率>50%,在7天期限结束时,无论营养培养物制备条件如何。此外,纯化的LPS对照在柠檬酸盐/聚山梨酯缓冲液中变得不可检测(<50%回收率),突出LER的存在。这些发现强调了当纯化的LPS回收不足时,使用相关生产设施的NOE评估总体风险的潜在价值。
    The evaluation of Naturally Occurring Endotoxins (NOEs) for Low Endotoxin Recovery (LER) studies has been a topic in the industry and regulatory agencies have been hesitant to endorse NOE use in LER studies over purified Lipopolysaccharide (LPS) standards such as Control Standard Endotoxin (CSE) or Reference Standard Endotoxin (RSE). In a recent study involving 11 BioPhorum member companies across 13 sites, NOEs prepared in high and low nutrient conditions were evaluated in two common monoclonal antibody buffer formulations: 10 mM Sodium Citrate, 0.05 % Polysorbate 80, pH 6.0 and 20 mM Histidine, 0.05 % Polysorbate 80, pH 6.0. 12 g-negative bacterial isolates were used to prepare NOE analytes, which were spiked into the formulation buffers. Additionally, the NOEs were spiked into Limulus Amebocyte Lysate (LAL) reagent water as controls and purified LPS into the citrate/polysorbate buffer as the LER control. Results showed the average of three runs per organism was >50 % recovery, at the conclusion of the 7-day period, regardless of nutrient culture preparation conditions. Furthermore, purified LPS controls became undetectable (<50 % recovery) in the citrate/polysorbate buffer, highlighting the presence of LER. These findings highlight the potential value of using NOEs from relevant manufacturing facilities to assess overall risk when purified LPS recovery is insufficient.
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  • 文章类型: Journal Article
    目的:主要目的是探索劳累热应激(EHS)促进运动相关菌血症的影响。次要目的是检查氨基酸饮料(AAB)干预是否可以减轻运动相关的菌血症。
    方法:平衡随机对照试验。
    方法:20名接受耐力训练的男性参与者完成了两项随机EHS试验。有一次,参与者每天两次服用237毫升AAB,持续7天,在EHS之前和期间每20分钟(在35°C下以60%V²O2max运行2小时)。在另一个场合,消耗水体积控制(CON)当量。在EHS之前和之后立即收集全血样本,并在微生物提取后通过荧光计定量分析血浆DNA浓度,和细菌相对丰度通过下一代16srRNA基因测序。
    结果:在CON上观察到EHS前后血浆中微生物DNA的浓度增加(EHS前0.014ng/μL,EHS后0.039ng/μL)(p<0.001)和AAB(EHS前0.015ng/μL,EHS后0.031ng/μL)(p<0.001)。AAB从运动前到运动后的变化幅度降低了40%,但与CON相比没有观察到显著差异(p=0.455)。确定的主要细菌组包括:门-变形杆菌(88.0%),伯克氏菌科(59.1%),和属弯曲杆菌属(58.6%)。门的α-多样性和相对丰度的绝对和相对变化没有显着变化,家庭,在AAB和CON中观察到属细菌群。
    结论:全身循环中微生物细菌DNA的增加对EHS的反应在所有参与者中都呈阳性。在EHS之前和期间食用的氨基酸饮料补充期并未显着减轻EHS相关的菌血症。
    OBJECTIVE: The primary aim was to explore the impact of exertional-heat stress (EHS) promoted exercise-associated bacteraemia. A secondary aim was to examine if an amino acid beverage (AAB) intervention may mitigate exercise-associated bacteraemia.
    METHODS: Counterbalanced randomised control trial.
    METHODS: Twenty endurance trained male participants completed two randomised EHS trials. On one occasion, participants consumed a 237 mL AAB twice daily for 7 days prior, immediately before and every 20 min during EHS (2 h running at 60 % V̇O2max in 35 °C). On the other occasion, a water volume control (CON) equivalent was consumed. Whole blood samples were collected pre- and immediately post-EHS, and were analysed for plasma DNA concentration by fluorometer quantification after microbial extraction, and bacterial relative abundance by next generation 16s rRNA gene sequencing.
    RESULTS: Increased concentration of microbial DNA in plasma pre- to post-EHS was observed on CON (pre-EHS 0.014 ng/μL, post-EHS 0.039 ng/μL) (p < 0.001) and AAB (pre-EHS 0.015 ng/μL, post-EHS 0.031 ng/μL) (p < 0.001). The magnitude of change from pre- to post-exercise on AAB was 40 % lower, but no significant difference was observed versus CON (p = 0.455). Predominant bacterial groups identified included: phyla-Proteobacteria (88.0 %), family-Burkholderiaceae (59.1 %), and genus-Curvibacter (58.6 %). No significant variation in absolute and relative change in α-diversity and relative abundance for phyla, family, and genus bacterial groups was observed in AAB versus CON.
    CONCLUSIONS: The increased presence of microbial-bacterial DNA in systemic circulation in response to EHS appears positive in all participants. An amino acid beverage supplementation period prior to and consumption during EHS did not provide significant attenuation of EHS-associated bacteraemia.
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  • 文章类型: Journal Article
    三氯蔗糖,广泛使用的甜味剂,长期食用可能导致代谢紊乱,但三氯半乳蔗糖是否对女性生殖健康有任何影响仍不确定。我们将三氯半乳蔗糖加入饮用水中,并观察食物摄入量,体重,发情周期,卵泡发育,血清激素,和小鼠的胰岛素敏感性。在食用三氯蔗糖后,小鼠的食物摄取或体重没有经历任何变化。然而,他们在发情周期中表现出不规则性,以原始数量减少为标志,小学,和次级卵泡,再加上窦卵泡数量的显著增加。卵泡刺激素(FSH)下降,雌二醇(E2),和孕酮(P4)水平,而睾酮(T)和黄体生成素(LH)水平飙升,导致LH/FSH比值显著升高。三氯蔗糖还诱导胰岛素抵抗,胰岛素水平升高和胰岛素耐受性受损证明,这对细菌来源的血清内毒素的增加有反应。通过罗格列酮(RSG)消除胰岛素抵抗,用新霉素(NEO)根除肠道菌群来源的内毒素,或增强肠屏障功能与吲哚-3-甲醇(I3C),发情周期的异常,卵泡发育中断,三氯半乳蔗糖诱导的激素失衡和血清内毒素升高被成功逆转。本研究表明三氯蔗糖诱导的小鼠卵泡发育不良可能与肠通透性受损有关。内毒素的浸润,全身炎症的开始,和胰岛素抵抗。
    Sucralose, the extensively utilized sweetener, might lead to metabolic disorders with prolonged consumption, but it remains uncertain if sucralose has any impact on female reproductive health. We incorporated sucralose into drinking water and observed food intake, body weight, estrous cycle, follicular development, serum hormones, and insulin sensitivity of mice. The mice did not experience any changes in their food intake or body weight after consuming sucralose. However, they displayed irregularities in the estrous cycle, marked by a reduced count of primordial, primary, and secondary follicles, coupled with a significant increase in the number of antral follicles. There was a decline in follicle-stimulating hormone (FSH), estradiol (E2), and progesterone (P4) levels, while testosterone (T) and luteinizing hormone (LH) levels surged, leading to a notable elevation in the LH / FSH ratio. Sucralose also induced insulin resistance, as evidenced by elevated insulin levels and impaired insulin tolerance, which responded to an increase in bacterial-derived serum endotoxin. By eliminating insulin resistance with rosiglitazone (RSG), eradicating intestinal flora-derived endotoxins with neomycin (NEO), or enhancing intestinal barrier function with indole-3-carbinol (I3C), the abnormalities in estrous cycle, disruptions in follicular development, hormonal imbalances and elevation in serum endotoxins induced by sucralose were successfully reversed. The present study indicates that sucralose-induced follicular dysplasia in mice is probably related to impaired intestinal permeability, infiltration of endotoxins, initiation of systemic inflammation, and insulin resistance.
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  • 文章类型: Journal Article
    神经免疫相互作用的调节因鸟类而异。目前对鹦鹉的外周和中枢神经系统(CNS)之间的相互作用知之甚少,对神经炎症敏感的鸟类。在这里,我们研究了鹦鹉对葡聚糖硫酸钠(DSS)和脂多糖(LPS)诱导的亚临床急性外周炎症的全身和中枢神经系统反应。将DSS和LPS刺激不同的三个实验处理组与对照进行比较。用DSS治疗的个体显示出显著的组织学肠损伤。通过定量蛋白质组学,我们描述了血浆(PL)和脑脊液(CSF)组成的变化。总的来说,我们在PL中鉴定出180种蛋白质,在CSF中鉴定出978种蛋白质,蛋白质组之间具有中等的共结构。在治疗之间,我们检测到免疫差异,凝血和代谢途径。蛋白质组变异与肠和脑中促炎细胞因子mRNA表达水平相关。我们的发现揭示了鸟类周围低度炎症的全身影响。
    Regulation of neuroimmune interactions varies across avian species. Little is presently known about the interplay between periphery and central nervous system (CNS) in parrots, birds sensitive to neuroinflammation. Here we investigated the systemic and CNS responses to dextran sulphate sodium (DSS)- and lipopolysaccharide (LPS)-induced subclinical acute peripheral inflammation in budgerigar (Melopsittacus undulatus). Three experimental treatment groups differing in DSS and LPS stimulation were compared to controls. Individuals treated with DSS showed significant histological intestinal damage. Through quantitative proteomics we described changes in plasma (PL) and cerebrospinal fluid (CSF) composition. In total, we identified 180 proteins in PL and 978 proteins in CSF, with moderate co-structure between the proteomes. Between treatments we detected differences in immune, coagulation and metabolic pathways. Proteomic variation was associated with the levels of pro-inflammatory cytokine mRNA expression in intestine and brain. Our findings shed light on systemic impacts of peripheral low-grade inflammation in birds.
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  • 文章类型: Journal Article
    高铁酸盐(Fe(VI))是一种环保消毒剂,广泛用于根除再生水中的微生物。然而,吸入经Fe(VI)处理的含细菌再生水的潜在健康风险仍不确定.我们旨在探讨K2FeO4处理的大肠杆菌(E.大肠杆菌ATCC25922)。我们的发现表明,Fe(VI)消毒诱导了剂量和时间依赖性的大肠杆菌灭活,伴随着细菌内毒素的快速释放,脂多糖(LPS)。扫描电子显微镜(SEM)观察表明,Fe(VI)诱导的内毒素产生至少包括两个阶段:内毒素与细菌的初始结合以及随后的解离以释放游离内毒素。此外,Fe(VI)消毒不能有效地消除纯的或大肠杆菌衍生的内毒素。本研究中使用的大肠杆菌菌株缺乏肺部感染能力,因此,单独吸入细菌不会引起严重的肺损伤。然而,小鼠吸入暴露于Fe(VI)处理的大肠杆菌显示肺结构和功能的严重损害。此外,我们观察到中性粒细胞/巨噬细胞募集的积累,细胞凋亡,和在经受Fe(VI)处理的大肠杆菌的小鼠的肺组织中的ROS产生。RNA测序(RNA-seq)和PCR结果显示,与内毒素刺激有关的基因,细胞凋亡,抗氧化防御,炎症反应,趋化因子及其受体响应于Fe(VI)处理的大肠杆菌而上调。总之,Fe(VI)在消除内毒素方面是无效的,并且由于从灭活的细菌释放内毒素而可引发继发性危害。气溶胶暴露于Fe(VI)处理的大肠杆菌通过诱导氧化应激和炎症反应对肺组织造成相当大的损害。
    Ferrate (Fe(VI)) is an environmentally friendly disinfectant that is widely used to eradicate microbes in reclaimed water. However, the potential health risks associated with inhalation of Fe(VI)-treated bacteria-laden reclaimed water remains uncertain. We aimed to explore the inhalation hazards and potential mechanisms of K2FeO4-treated Escherichia coli (E. coli, ATCC 25922). Our findings indicated that Fe(VI) disinfection induced a dose- and time-dependent E. coli inactivation, accompanied by a rapid release of the bacterial endotoxin, lipopolysaccharide (LPS). Scanning electron microscopy (SEM) observations indicate that Fe(VI)-induced endotoxin production consists of at least two stages: initial binding of endotoxin to bacteria and subsequent dissociation to release free endotoxin. Furthermore, Fe(VI) disinfection was not able to effectively eliminate pure or E. coli-derived endotoxins. The E. coli strain used in this study lacks lung infection capability, thus the inhalation of bacteria alone failed to induce severe lung injury. However, mice inhaled exposure to Fe(VI)-treated E. coli showed severe impairment of lung structure and function. Moreover, we observed an accumulation of neutrophil/macrophage recruitment, cell apoptosis, and ROS generation in the lung tissue of mice subjected to Fe(VI)-treated E. coli. RNA sequencing (RNA-seq) and PCR results revealed that genes involved with endotoxin stimuli, cell apoptosis, antioxidant defence, inflammation response, chemokines and their receptors were upregulated in response to Fe(VI)-treated E. coli. In conclusion, Fe(VI) is ineffective in eliminating endotoxins and can trigger secondary hazards owing to endotoxin release from inactivated bacteria. Aerosol exposure to Fe(VI)-treated E. coli causes considerable damage to lung tissue by inducing oxidative stress and inflammatory responses.
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  • 文章类型: Journal Article
    这项研究首先研究了携带氯己定和银(nMS-nAg-Chx)的介孔二氧化硅纳米颗粒(nMS)对牙周炎相关生物膜的影响。本研究旨在研究(1)对牙龈卟啉单胞菌(P。牙龈)生物膜;(2)对牙龈卟啉单胞菌生物膜毒力的抑制作用;(3)对牙周炎相关多种生物膜的调节作用。
    将银纳米颗粒(nAg)和氯己定(Chx)共同负载到nMS中以形成nMS-nAg-Chx。测试了抑制区测试和针对牙龈卟啉单胞菌的最小抑制浓度(MIC)。生长曲线,结晶紫(CV)染色,进行活/死染色和扫描电子显微镜(SEM)观察。评估生物膜毒力。进行了3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四唑溴化物(MTT)测定和定量实时PCR(qPCR),以验证多种生物膜的活性和组成变化(P。牙龈,格氏链球菌和血链球菌)。
    nMS-nAg-Chx剂量依赖性地抑制牙龈卟啉单胞菌生物膜(p<0.05),MIC为18.75µg/mL。活细菌较少,nMS-nAg-Chx组生物量较少,毒力较小(p<0.05)。nMS-nAg-Chx抑制和修饰牙周炎相关生物膜。在25μg/mLnMS-nAg-Chx组中,病原菌的比例从16.08%下降到1.07%,有益细菌的比例从82.65%上升到94.31%。
    nMS-nAg-Chx抑制牙龈卟啉单胞菌生长,降低生物膜毒力和调节牙周炎相关的多物种生物膜向健康趋势。pH敏感的nMS-nAg-Chx抑制病原体并调节口腔微生态,在牙周炎辅助治疗中显示出巨大的潜力。
    UNASSIGNED: This research first investigated the effect of mesoporous silica nanoparticles (nMS) carrying chlorhexidine and silver (nMS-nAg-Chx) on periodontitis-related biofilms. This study aimed to investigate (1) the antibacterial activity on Porphyromonas gingivalis (P. gingivalis) biofilm; (2) the suppressing effect on virulence of P. gingivalis biofilm; (3) the regulating effect on periodontitis-related multispecies biofilm.
    UNASSIGNED: Silver nanoparticles (nAg) and chlorhexidine (Chx) were co-loaded into nMS to form nMS-nAg-Chx. Inhibitory zone test and minimum inhibitory concentration (MIC) against P. gingivalis were tested. Growth curves, crystal violet (CV) staining, live/dead staining and scanning electron microscopy (SEM) observation were performed. Biofilm virulence was assessed. The 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide (MTT) assay and Quantitative Real Time-PCR (qPCR) were performed to validate the activity and composition changes of multispecies biofilm (P. gingivalis, Streptococcus gordonii and Streptococcus sanguinis).
    UNASSIGNED: nMS-nAg-Chx inhibited P. gingivalis biofilm dose-dependently (p<0.05), with MIC of 18.75 µg/mL. There were fewer live bacteria, less biomass and less virulence in nMS-nAg-Chx groups (p<0.05). nMS-nAg-Chx inhibited and modified periodontitis-related biofilms. The proportion of pathogenic bacteria decreased from 16.08 to 1.07% and that of helpful bacteria increased from 82.65 to 94.31% in 25 μg/mL nMS-nAg-Chx group for 72 h.
    UNASSIGNED: nMS-nAg-Chx inhibited P. gingivalis growth, decreased biofilm virulence and modulated periodontitis-related multispecies biofilms toward healthy tendency. pH-sensitive nMS-nAg-Chx inhibit the pathogens and regulate oral microecology, showing great potential in periodontitis adjunctive therapy.
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  • 文章类型: Journal Article
    背景:非酒精性脂肪性肝炎(NASH)的管理是一个未满足的临床需求。米索前列醇,前列腺素E1是天然存在的前列腺素E1的结构类似物,据报道可以减少促炎细胞因子的产生,并且可能在治疗NASH中具有潜在作用。我们旨在评估米索前列醇治疗NASH患者的疗效和安全性。
    方法:在此阶段2,双盲,随机化,安慰剂对照试验,NASH患者以1∶1的比例随机分组,接受200µg米索前列醇或安慰剂,每日3次,共2个月.主要终点是肝功能测试(LFTs)的改善,白细胞介素-6(IL-6)和内毒素水平。次要终点是胰岛素抵抗的改善,血脂异常,肝纤维化和肝脂肪变性。
    结果:共有50名患者接受了随机分组,其中44人(88%)为男性。年龄范围为25-64岁(平均值±SE(SEM)38.1±1.4)。19例(38%)患者合并2型糖尿病。32例(64%)患者超重或肥胖。在2个月的治疗结束时,总白细胞计数(TLC)减少(p=0.005),丙氨酸氨基转移酶(ALT)(p<0.001),谷草转氨酶(AST)(p=0.002)和受控衰减参数(CAP)(p=0.003)在米索前列醇组中观察到,而安慰剂随后ALT下降(p<0.001),AST(p=0.018),γ-谷氨酰转移酶(GGT)(p=0.003),CAP(p=0.010)和甘油三酯(p=0.048)。胰岛素抵抗没有减少,两组的肝纤维化(弹性成像)和血脂异常。然而,与安慰剂组相比,米索前列醇导致CAP显著降低(p=0.039)。此外,在米索前列醇组中,治疗前和治疗后IL-6和内毒素水平保持稳定,而在安慰剂组,IL-6水平升高(p=0.049).米索前列醇组有6例(12%)患者出现至少1例不良事件,安慰剂组中有5例(10%)。米索前列醇组最常见的不良事件是腹泻。各组均未发生危及生命事件或治疗相关死亡。
    结论:米索前列醇和安慰剂组的生化特征均有改善,无统计学意义。然而,脂肪变性有了更多的改善,正如CAP所描绘的,米索前列醇组和安慰剂组IL-6水平恶化。
    背景:NCT05804305。
    BACKGROUND: The management of non-alcoholic steatohepatitis (NASH) is an unmet clinical need. Misoprostol, a structural analogue of naturally occurring prostaglandin E1, has been reported to decrease proinflammatory cytokine production and may have a potential role in treating NASH. We aimed to evaluate the efficacy and safety of misoprostol in treating patients with NASH.
    METHODS: In this phase 2, double-blind, randomised, placebo-controlled trial, patients with NASH were randomly assigned in a 1:1 ratio to receive 200 µg of misoprostol or placebo thrice daily for 2 months. The primary endpoint was an improvement in liver function tests (LFTs), interleukin-6 (IL-6) and endotoxin levels. The secondary endpoint was improvement in insulin resistance, dyslipidaemia, hepatic fibrosis and hepatic steatosis.
    RESULTS: A total of 50 patients underwent randomisation, of whom 44 (88%) were males. The age range was 25-64 years (mean±SE of mean (SEM) 38.1±1.4). 19 (38%) patients had concomitant type 2 diabetes mellitus. 32 (64%) patients were either overweight or obese. At the end of 2 months\' treatment, a reduction in total leucocyte count (TLC) (p=0.005), alanine aminotransferase (ALT) (p<0.001), aspartate aminotransferase (AST) (p=0.002) and controlled attenuation parameter (CAP) (p=0.003) was observed in the misoprostol group, whereas placebo ensued a decline in ALT (p<0.001), AST (p=0.018), gamma-glutamyl transferase (GGT) (p=0.003), CAP (p=0.010) and triglycerides (p=0.048). There was no diminution in insulin resistance, hepatic fibrosis (elastography) and dyslipidaemia in both groups. However, misoprostol resulted in a significant reduction in CAP as compared with the placebo group (p=0.039). Moreover, in the misoprostol group, pretreatment and post-treatment IL-6 and endotoxin levels remained stable, while in the placebo group, an increase in the IL-6 levels was noted (p=0.049). Six (12%) patients had at least one adverse event in the misoprostol group, as did five (10%) in the placebo group. The most common adverse event in the misoprostol group was diarrhoea. No life-threatening events or treatment-related deaths occurred in each group.
    CONCLUSIONS: Improvement in the biochemical profile was seen in both misoprostol and placebo groups without any statistically significant difference. However, there was more improvement in steatosis, as depicted by CAP, in the misoprostol group and worsening of IL-6 levels in the placebo group.
    BACKGROUND: NCT05804305.
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