High concentrations of human β-defensin 2 in gastric juice of patients with Helicobacter pylori infection

MIA： Human β-defensin （HBD）-1 and HBD-2 are endogenous antimicrobial peptides. Unlike HBD-1, the HBD-2 expression is augmented by Helicobacter pylori （H pylon）. We sought to determine HBD-1 and HBD-2 concentrations in gastric juice during Hpylori infection. METHODS： HBD-1 and HBD-2 concentrations were measured by radioimmunoassay in plasma and gastric juice of 49 Hpylori-infected and 33 uninfected subjects and before and after anti-H pyloritreatment in,13 patients with Hpylori-associated gastritis. Interleukin （IL）-1β and IL-8 concentrations in gastric juice were measured by enzyme-linked immunosorbent assay （ELISA）. Histological grades of gastritis were determined using two biopsy specimens taken from the antrum and corpus. Reverse phase high performance liquid chromatography （RP-HPLC） was used to identify HBD-2. RESULTS： HBD-2 concentrations in gastric juice, but not in plasma, were significantly higher in Hpylori-positive than -negative subjects, albeit the post-treatment levels were unchanged. Immunoreactivity for HBD-2 was exclusively identified in Hpylori-infected mucosa by RPHPLC. HBD-2 concentrations in gastric juice correlated with histological degree of neutrophil and mononuclear cell infiltration in the corpus. IL-1β levels correlated with those of IL-8, but not HBD-2. Plasma and gastric juice HBD-1 concentrations were similar in H pylori-infected and uninfected subjects. CONCLUSION： Our results place the β-defensins, especiallyHBD-2, in the front line of innate immune defence. Moreover, HBD-2 may be involved in the pathogenesis of Hpylori-associated gastritis, possibly through its function as immune and inflammatory mediator.

糖尿病大鼠肝脏β-defensins表达及血清炎症因子的变化

目的:观察糖尿病大鼠病程中肝脏β-defensins的表达和血清炎症因子的变化,探讨在糖尿病状态时两者之间可能存在的影响.方法:实验大鼠分为普通饲料组、高糖饲料组、糖尿病4wk组和12wk组,采集血液检测血清炎症因子TNF-α,IL-1β及IL-10和血糖、胰岛素、三酰甘油等相关生化指标;收集肝脏标本,RT-PCR及Western Blot方法检测β-defensins的表达.结果:与对照组相比,糖尿病大鼠整个病程中都存在致炎因子TNF-α,IL-1β激活及抗炎因子IL-10的削弱.肝脏中表达β-defensins1(rBD-1)和β-defensins2(rBD-2).rBD-1呈少量表达,糖尿病病程中rBD-2表达呈减少趋势.高血糖或糖基化反应可能干扰rBD-2的组成性表达及炎症因子产生的诱导性表达.结论:糖尿病大鼠病程中存在慢性炎症,高血糖或糖基化反应干扰了炎症刺激重要的小分子抗菌肽β-defensins在肝脏表达的信号通路,使其表达下调.

中国南方汉族人β-defensin-1基因多态性与慢性阻塞性肺疾病易感性的关系

目的 探讨中国南方汉族人 β- defensin- 1基因多态性与慢性阻塞性肺疾病 (COPD)易感性的关系。方法 采用限制性片段长度多态性 (RFLP)技术检测 β defensin -1外显子 2基因型在 12 0例COPD吸烟患者和10 8例非COPD吸烟者中的频率。结果 COPD组同源野生型 (G/G)、杂合型 (G/A)和同源突变型 (A/A)频率分别为 82 .5 0 %、10 .83%和 6 .6 7% ,非COPD组的频率分别为 95 .37%、3.70 %和 0 .93% ,两组基因频率分布的差异有显著性 (P <0 .0 1)。两组等位基因的分布差异也有显著性 (等位基因G频率分别为 87.92 %∶97.2 2 % ;等位基因A频率分别为 12 .0 8%∶2 .78% ;P <0 .0 1) ;G→A的突变率随COPD病情的严重度增加而上升。结论 β defensin 1基因外显子 2的 16 5 4位多态性与中国南方汉族人群COPD易感性可能有关 ,而且可能还影响COPD的进展。

Concentrations of α-and β-defensins in gastric juice of patients with various gastroduodenal diseases

AIM: To determine the concentration of α-and β-defensins in gastric juice of patients with various gastroduodenal diseases. METHODS: Concentrations of human neutrophil peptides (HNPs) 1-3, the major forms of α-defensins, and human β-defensin (HBD)-1and HBD-2were measured by radioimmunoassay in plasma and gastric juice of 84 subjects, consisting of 54 Helicobacter pylori-infected and 30 uninfected subjects. They included 33 patients with chronic gastritis (CG), 12 with gastric ulcer (GU), 11 with duodenal ulcer (DU), 11 with benign gastric polyp (BGP) and 16 with normal mucosa (N group) on upper endoscopy. Plasma pepsinogen Ⅰ and Ⅱ levels, biomarkers for gastric mucosal inflammation and atrophy, were also measured. RESULTS: Gastric juice HNPs 1-3 levels in patients with CG, GU and BGP were significantly higher than those in patients with DU and N. Gastric juice HBD-2 concentrations in patients with CG and GU were significantly higher than those in the N group, but were significantly lower in DU patients than in GU patients. Gastric juice HBD-1 levels and plasma levels of these peptides were similar in the patient groups. Concentrations of gastric juice HNPs 1-3 and HBD-2 of in H pylori-infected patients were significantly different from those in uninfected subjects. HNPs 1-3 concentrations in gastric juice correlated negatively with plasma pepsinogen I levels and Ⅰ/Ⅱ ratios. HBD-2 levels in gastric juice correlated positively and negatively with plasma pepsinogen Ⅱ concentrations and Ⅰ/Ⅱratios, respectively. CONCLUSION: HNPs 1-3 and HBD-2 levels in gastric juice are diverse among various gastrointestinal diseases, reflecting the inflammatory and atrophic events of the background gastric mucosa affected by H pylori.

Human β-defensin 2 enhances IL-1β production and pyroptosis through P2X7-mediated NLRP3 expression in macrophages

Periodontal disease is the leading cause of tooth loss,which is also a high-risk factor for other diseases including oral cancer and cardiovascular disease.Periodontitis is one of the most common type of periodontal diseases.Interleukin-1β(IL-1β)plays a key role in the pathogenesis of periodontitis.However,the mechanism how IL-1βis produced during periodontitis is still unclear.In the present study,we found that humanβ-defensin 2(hBD2)enhances IL-1βproduction through an LPS-primed human acute monocytic leukemia(THP-1)macrophage model.Inhibition of P2X purinoceptor 7(P2X7)reduced hBD2-enhanced IL-1βproduction.Incubation of LPS-primed THP-1 macrophages with potassium chloride also suppressed hBD2-enhanced IL-1βproduction.Silence of inflammasome adaptor Nod-like receptor family pyrin domain containing 3(NLRP3)led to reduced hBD2-enhanced IL-1βproduction.Likewise,inhibition of caspase-1 also resulted in the decrease of IL-1β.Moreover,an ethidium bromide uptake test indicated that hBD2-activated caspase-1 mediated pyroptotic pore formation.Subsequent lactate dehydrogenase detection and flow cytometric analysis indicated that hBD2 also induced pyroptosis.In brief,these findings illustrated not only the mechanism of hBD2 in enhancing the inflammatory response,but also provided novel therapeutic targets for periodontitis.

Human β-defensin2(hBD-2)在幽门螺杆菌相关性胃炎中的表达

目的检测humanβdefensin2(hBD2)在幽门螺杆菌(Hp)相关性胃炎胃黏膜上皮中的表达,评价其在Hp感染的胃黏膜表面的抗菌作用。方法随机选择患者18例,取胃窦黏膜组织,以快速尿素酶及改良Giemsa染色两种方法判断Hp的存在与否。两者同时阳性诊断为Hp阳性,同时阴性为Hp阴性。18例患者中,Hp阳性10例,阴性8例。另以RTPCR法检测标本中hBD2的表达。结果10例Hp阳性标本中8例呈现hBD2mRNA的高表达,1例呈现低表达,总表达率90%;8例Hp阴性标本中6例未检测出hBD2mRNA,2例呈现hBD2mRNA的表达,表达率25%。结论Hp感染可诱导hBD2在胃黏膜上皮中的表达。体外试验表明hBD2抑制Hp的生长,推测hBD2在Hp相关性胃炎中起到一定的抗菌作用。

黄芪甲甙对吸烟大鼠气道-defensin 2表达的影响

目的了解熏烟对大鼠肺组织β-防御素2(β-defensin2)表达的影响,黄芪甲甙对β-defensin2表达的调控作用及其可能的机制。方法大鼠接受染毒柜被动吸烟三周,建立熏烟模型。分别给于黄芪甲甙1.2mg/kg·d,2.4mg/kg·d,3.6mg/kg·d灌胃。提取肺组织和支气管肺泡灌洗液,采用免疫组化、RT-PCR等方法检测β-defensin 2的表达水平。结果吸烟可以使气道上皮β-defensin 2表达升高,使BALF中炎细胞总数,中性粒细胞,巨噬细胞,淋巴细胞数增高。黄芪甲甙可以降低吸烟诱导的β-defensin 2的高表达,减少支气管肺泡灌洗液白细胞及中性粒细胞,淋巴细胞的数量。结论黄芪甲甙下调吸烟诱导的气道上皮β-defensin 2的高表达,减轻气道炎症。

Relevance of α-defensins(HNP1-3) and defensin β-1 in diabetes

AIM: To investigate the genetic background of human defensin expression in type 1 and 2 diabetes.

β-defensins and the epididymis： contrasting influences of prenatal, postnatal, and adult scenarios

β-defensins are components of host defense, with antimicrobial and pleiotropic immuno-modulatory properties. Research over the last 15 years has demonstrated abundant expression of a variety of β-defensins in the postnatal epididymis of different species. A gradient of region- and cell-specific expression of these proteins is observed in the epithelium of the postnatal epididymis. Their secretion into the luminal fluid and binding to spermatozoa as they travel along the epididymis has suggested their involvement in reproduction-specific tasks. Therefore, continuous attention has been given to various β-defensins for their role in sperm function and fertility. Although β-defensins are largely dependent on androgens, the underlying mechanisms regulating their expression and function in the epididymis are not well understood. Recent investigation has pointed out to a new and interesting scenario where β-defensins emerge with a different expression pattern in the Wolffian duct, the embryonic precursor of the epididymis, as opposed to the adult epididymis, thereby redefining the concept concerning the multifunctional roles of β-defensins in the developing epididymis. In this review, we summarize some current views of β-defensins in the epididymis highlighting our most recent data and speculations on their role in the developing epididymis during the prenatal-to-postnatal transition, bringing attention to the many unanswered questions in this research area that may contribute to a better understanding of epididymal biology and male fertility.

Novel phenotype of mouse spermatozoa following deletion of nine β-defensin genes

β-defensin peptides are a large family of antimicrobial peptides. Although they kill microbes in vitroand interact with immune cells, the precise role of these genes in vivo remains uncertain. Despite their inducible presence at mucosal surfaces, their main site of expression is the epididymis. Recent evidence suggests that a major function of these peptides is in sperm maturation. In addition to previous work suggesting this, work at the MRC Human Genetics Unit, Edinburgh, has shown that homozygous deletion of a cluster of nine β-defensin genes in the mouse results in profound male sterility. The spermatozoa derived from the mutants had reduced motility and increased fragility. Epididymal spermatozoa isolated from the cauda region of the homozygous mutants demonstrated precocious capacitation and increased spontaneous acrosome reactions compared with those from wild-types. Despite this, these mutant spermatozoa had reduced ability to bind to the zona pellucida of oocytes. Ultrastructural examination revealed a disintegration of the microtubule structure of mutant-derived spermatozoa isolated from the epididymal cauda region, but not from the caput. Consistent with premature acrosome reaction and hyperactivation, spermatozoa from mutant animals had significantly increased intracellular calcium content. This work demonstrates that in vivo β-defensins are essential for successful sperm maturation, and that their disruption alters intracellular calcium levels, which most likely leads to premature activation and spontaneous acrosome reactions that result in hyperactivation and loss of microtubule structure of the axoneme. Determining which of the nine genes are responsible for the phenotype and the relevance to human sperm function is important for future work on male infertility.

Human β-defensin-2 Enhances Anti-tumor Efficacy of Survivin-based Broad-spectrum DNA Vaccine in Mouse Tumor Model

Objective:Malignant tumors greatly endanger and affect the quality of human life.Among antitumor biotherapy strategies,DNA vaccines hold promise in part because of their unique advantages.In this study,an effective broad-spectrum antitumor DNA vaccine expressing human survivin T34A dominant-negative mutant fused with humanβ-defensin-2(HBD2)was investigated.Methods:The expression profiles of genes of interest were examined using western blotting,reverse transcription-polymerase chain reaction(RT-PCR),and enzyme-linked immunosorbent assay(ELISA)in vitro.The immune function of the fusion gene vaccine(FGV)was assessed in BALB/c mice,which included detection of serum antibody,spleen lymphocyte proliferation,interferon-gamma(IFN-γ)secretion,and lactate dehydrogenase(LDH)release.In vivo antitumor effects of FGV were examined in a mouse breast cancer(4T1)model,whereas in vitro effects were assessed using tumor cells derived from different origins.Caspase-3activity in tumor cells was also assessed after vaccine transfection.Results:The FGV triggered humoral as well as cellular immune responses against survivin.It exhibited more potent inhibition of tumor growth as well as prolonged the survival of immunized mice compared to mice immunized with only either survivin T34A or HBD2 vaccines.In addition,FGV displayed stronger cytotoxicity against tumor cells derived from different origins compared to the other vaccines and facilitated increased caspase-3 activity in transfected tumor cells.Conclusion:The novel DNA vaccine consisting of a fusion of the universal tumor antigen survivin T34A mutant with molecular adjuvant HBD2generates enhanced broad-spectrum antitumor efficacy against cancers derived from various origins.

血清HBD-3、DCR3对复杂性肾结石患者经皮肾镜碎石术后尿路感染的预测价值

目的分析血清β-防御素-3(HBD-3)、诱骗受体3(DCR3)对复杂性肾结石患者经皮肾镜碎石术后尿路感染的预测价值。方法选取2020年1月—2022年12月河北省沧州中西医结合医院收治的112例复杂性肾结石患者为研究对象进行回顾性研究,所有患者均行经皮肾镜碎石术(PCNL),根据术后感染情况将患者分为非尿路感染组52例、尿路感染组60例。比较两组一般资料及HBD-3、DCR3水平。受试者工作特征(ROC)曲线分析C反应蛋白(CRP)、降钙素原(PCT)、HBD-3、DCR3水平对术后尿路感染的预测价值。结果与非尿路感染组比较,尿路感染组的HBD-3[(0.77±0.08)ng/mL vs.(1.36±0.25)ng/mL,P=0.001]、DCR3[(4.68±0.53)ng/mL vs.(13.21±0.28)ng/mL,P=0.001]水平较高。多因素logistics回归分析显示,泌尿道手术史、术前尿路感染、手术时间、导尿管留置时间、结石负荷、抗菌药物种类、合并肾功能障碍、术中通道类型CRP、PCT、HBD-3、DCR3为患者术后尿路感染的影响因素(P<0.05)。ROC曲线显示,CRP、PCT、CRP联合PCT准确度分别为70.54%、72.32%、78.57%;HBD-3、DCR3、HBD-3联合DCR3准确度分别为69.64%、75.89%、86.61%。结论复杂性肾结石患者术后尿路感染与多种因素相关,且术后尿路感染患者HBD-3、DCR3表达水平较高,联合检测对术后尿路感染具有较高的预测价值。

鱼源β-防御素的生物信息学分析

鱼源β-防御素是抗菌肽家族的重要成员,具有广谱抗菌、不损伤真核细胞、不易产生耐药性等特点,可应用于渔业养殖和临床医学等方面,但目前面临着提取工艺复杂、含量较低、提取所用蛋白酶需求量大及以生产成本高等问题。因此分析其理化性质、结构和杀菌功能,对构造便捷和低廉的衍生肽具有重要的意义。本研究结合生物信息学软件和工具预测分析其理化性质、二级结构、磷酸化和糖基化位点、疏水性、细胞内定位和信号肽。结果提示鱼源β-防御素均为疏水性阳离子型抗菌肽。β-防御素抗菌肽通过C端亲水作用与细菌膜结合,引导N端氨基酸的疏水作用插入膜磷酸二酯键中改变细胞膜的通透性使细菌生物膜破裂而死亡,其中AJA33388.1(红牙鳞鲀)破膜杀菌能力最强。经检测发现β-防御素耐热性,稳定性相对较好,尤其是ACO88907.1(鳜鱼)和QNV47918.1(条石鲷)具有极高耐热性,可将其应用于杀菌以外的多方面领域。其二级结构以α螺旋为主,具有一定的刚性结构,且均具有3~4个磷酸化位点,分布于细胞外,具有19~20个氨基酸的信号肽序列,指导其在胞外蛋白产物的分泌等。通过预测分析结构,可为β-防御素的深入研究和应用以及多领域的抗菌肽衍生物设计提供思路。

β-防御素在子宫内膜癌及孕激素调控下癌细胞中的表达及意义

目的 探究β-防御素(DEFB)1、DEFB4A差异表达在子宫内膜癌(EC)发展预测中的价值,以及是否参与孕激素对EC的抑制。方法 利用TIMER、GEPIA2平台172例EC患者转录组测序数据进行DEFB1、DEFB4A差异表达及生存分析。EC Ishikawa细胞采用不同浓度孕酮进行处理,比较分析各浓度组DEFB1、DEFB4A表达情况。结果 EC组织DEFB1、DEFB4A表达水平均显著高于正常组织,约40个月后,DEFB1、DEFB4A高、低表达组患者的生存率差异均加大。孕酮处理后,10~(-6) mol/L组DEFB1 mRNA和蛋白水平在24、48 h后均较对照组显著升高,差异均有统计学意义(P<0.05),10~(-6) mol/L组DEFB1表达在48 h后较24 h无显著变化,差异无统计学意义(P>0.05)。各浓度组DEFB4A变化不显著,差异均无统计学意义(P>0.05)。孕酮作用下EC Ishikawa细胞活性与DEFB1表达呈显著负相关(P<0.05)。结论 DEFB1可能是预测EC发展的关键因子,可提示孕激素治疗的复发风险或将成为EC的抑制靶点。

血清高迁移率族蛋白B1、人β防御素2与腺病毒肺炎患儿闭塞性细支气管炎发生的关系

目的探讨血清高迁移率族蛋白B1(HMGB1)、人β防御素2(hBD-2)与腺病毒肺炎(AP)患儿闭塞性细支气管炎(BO)发生的关系。方法选取193例AP患儿,根据出院3个月后是否发生BO将AP患儿分为BO组58例和非BO组135例。收集两组临床资料并用酶联免疫吸附试验检测血清HMGB1、hBD-2,用单因素及多因素Logistic回归分析AP患儿发生BO的影响因素,以受试者工作特征(ROC)曲线分析血清HMGB1、hBD-2对AP患儿发生BO的预测价值。结果BO组月龄小于非BO组,热程长于非BO组,低氧血症、机械通气发生比例及血液白细胞计数、血小板计数、C反应蛋白、降钙素原、HMGB1、hBD-2高于非BO组(P均<0.05)。多因素Logistic回归分析显示,低氧血症、机械通气和HMGB1、hBD-2升高为AP患儿发生BO的独立危险因素(P均<0.05)。ROC曲线分析显示,血清HMGB1、hBD-2联合应用预测AP患儿发生BO的曲线下面积为0.818,与血清HMGB1、hBD-2单独预测的曲线下面积(0.739、0.726)比较差异有统计学意义(P均<0.05)。结论血清HMGB1、hBD-2水平升高是AP患儿发生BO的危险因素,二者联合检测对AP患儿发生BO的预测价值较高。

血清hBD-2、NT-proBNP、sICAM-1在急性下呼吸道感染患儿中的表达水平及对其病情预测的研究

目的 观察急性下呼吸道感染患儿血清β-防御素-2(hBD-2)、N末端脑钠肽前体(NT-proBNP)、可溶性细胞间黏附分子1(sICAM-1)表达水平,并分析3项指标对其病情检测的意义。方法 纳入2020年10月至2022年10月该院80例急性下呼吸道感染患儿为急性期组,另选取该院同期60例缓解期下呼吸道感染患儿为缓解期组,所有患儿入院时均接受血清hBD-2、NT-proBNP、sICAM-1检测,对比急性期组与缓解期组患儿血清hBD-2、NT-proBNP、sICAM-1表达水平。依据临床肺部感染评分(CPIS)将急性期组患儿分为轻症组和重症组,对比轻症组和重症组临床资料及实验室指标,分析血清hBD-2、NT-proBNP、sICAM-1表达水平与急性下呼吸道感染患儿病情的相关性,并绘制受试者工作特征(ROC)曲线分析3项指标对患儿病情的预测价值。结果 急性期组血清hBD-2、NT-proBNP、sICAM-1表达水平高于缓解期组,差异有统计学意义(P<0.05);经CPIS评分结果显示,80例急性下呼吸道感染患儿CPIS评分为(5.83±1.92)分,其中重症32例(40.00%),轻症48例(60.00%);经Pearson相关性分析,结果显示,CPIS评分与血清hBD-2、NT-proBNP、sICAM-1表达水平呈正相关(r=0.337、0.325、0.386,P=0.002、0.003、<0.001);重症组血清hBD-2、NT-proBNP、sICAM-1表达水平高于轻症组,差异有统计学意义(P<0.05);经Logistic回归分析发现,血清hBD-2、NT-proBNP、sICAM-1表达水平是急性下呼吸道感染患儿病情加重的危险因素(OR>1,P<0.05);绘制ROC曲线,血清hBD-2、NT-proBNP、sICAM-1表达水平对重症急性下呼吸道感染具有一定预测价值,曲线下面积(AUC)分别为0.728、0.769、0.786,联合检测预测价值更高(AUC=0.830)。结论 急性下呼吸道感染患儿血清hBD-2、NT-proBNP、sICAM-1表达水平升高,3项指标水平与患儿病情严重程度密切相关,可用于预测重症急性下呼吸道感染。

血清信号转导抑制因子3、β防御素2对胸部创伤并发细菌感染诊断价值研究

目的探讨血清细胞因子信号转导抑制因子3(SOCS3)、β防御素2(HBD2)对胸部创伤并发细菌感染的诊断价值。方法选取自2021年7月至2023年12月收治的胸部创伤(包括以胸部创伤为主的多发伤)患者152例为创伤组,并根据其是否并发细菌感染分为感染组(n=53)和无感染组(n=99),另选取同期在本院进行健康体检的志愿者152例为健康组。采用酶联免疫吸附法检测血清SOCS3、HBD2水平;采用Pearson相关分析感染组血清SOCS3与HBD2水平的相关性;采用多因素Logistic回归分析(逐步向前法)影响胸部创伤患者并发细菌感染的因素;采用受试者工作特征曲线分析血清SOCS3、HBD2对胸部创伤患者并发细菌感染的诊断价值,并采用Z检验比较其曲线下面积(AUC)。结果创伤组血清SOCS3、HBD2水平明显高于健康组,差异有统计学意义(P<0.05)。感染组创伤严重程度评分(ISS)、机械通气时间明显高于无感染组,差异有统计学意义(P<0.05)。感染组血清SOCS3、HBD2水平明显高于无感染组,差异有统计学意义(P<0.05)。感染组血清SOCS3与HBD2水平呈正相关(r=0.579,P<0.05)。SOCS3、HBD2、ISS评分是影响胸部创伤患者并发细菌感染的因素(P<0.05)。血清SOCS3、HBD2联合诊断胸部创伤患者并发细菌感染的AUC为0.920(95%可信区间:0.878~0.961),SOCS3、HBD2单独诊断胸部创伤患者并发细菌感染的AUC分别为0.830(95%可信区间:0.763~0.897)、0.811(95%可信区间:0.741~0.881),二者联合诊断效能较SOCS3(Z=2.252,P=0.024)、HBD2(Z=2.615,P=0.009)单独诊断效能更高。结论胸部创伤并发细菌感染患者血清SOCS3、HBD2水平异常升高,二者联合诊断胸部创伤患者并发细菌感染的价值较高。

Protective eff ect and mechanism of nanoantimicrobial peptide ND-C14 against Streptococcus pneumoniae infection

BACKGROUND:Streptococcus pneumoniae(S.pneumoniae)is a common pathogen that causes bacterial pneumonia.However,with increasing bacterial resistance,there is an urgent need to develop new drugs to treat S.pneumoniae infections.Nanodefensin with a 14-carbon saturated fatty acid(ND-C14)is a novel nanoantimicrobial peptide designed by modifying myristic acid at the C-terminus of humanα-defensin 5(HD5)via an amide bond.However,it is unclear whether ND-C14 is effective against lung infections caused by S.pneumoniae.METHODS:In vitro,three groups were established,including the control group,and the HD5 and ND-C14 treatment groups.A virtual colony-count assay was used to evaluate the antibacterial activity of HD5 and ND-C14 against S.pneumoniae.The morphological changes of S.pneumoniae treated with HD5 or ND-C14 were observed by scanning electron microscopy.In vivo,mice were divided into sham,vehicle,and ND-C14 treatment groups.Mice in the sham group were treated with 25μL of phosphate-buffered saline(PBS).Mice in the vehicle and ND-C14 treatment groups were treated with intratracheal instillation of 25μL of bacterial suspension with 2×108 CFU/mL(total bacterial count:5×10^(6) CFU),and then the mice were given 25μL PBS or intratracheally injected with 25μL of ND-C14(including 20μg or 50μg),respectively.Survival rates were evaluated in the vehicle and ND-C14 treatment groups.Bacterial burden in the blood and bronchoalveolar lavage fluid were counted.The lung histology of the mice was assessed.A propidium iodide uptake assay was used to clarify the destructive eff ect of ND-C14 against S.pneumoniae.RESULTS:Compared with HD5,ND-C14 had a better bactericidal eff ect against S.pneumoniae because of its stronger ability to destroy the membrane structure of S.pneumoniae in vitro.In vivo,ND-C14 significantly delayed the death time and improved the survival rate of mice infected with S.pneumoniae.ND-C14 reduced bacterial burden and lung tissue injury.Moreover,ND-C14 had a membrane permeation eff ect on S.pneumoniae,and its destructive ability increased with increasing ND-C14 concentration.CONCLUSION:The ND-C14 may improve bactericidal eff ects on S.pneumoniae both in vitro and in vivo.

酿酒酵母菌对绵羊瘤胃上皮细胞β-防御素-1(SBD-1)基因表达的影响

【目的】探索益生性酿酒酵母菌对绵羊瘤胃上皮细胞β-防御素-1(sheep beta-defensin-1,SBD-1)表达的调节作用,为在分子水平上揭示益生菌对防御素的调控机理提供一定的理论基础及依据。【方法】首先将新鲜的绵羊瘤胃组织用PBS和抗生素处理后进行瘤胃上皮细胞原代培养,当原代细胞数量长到细胞培养瓶的85%以上时,将细胞传于12孔板用于细胞刺激试验。同时将活化并纯化后的酿酒酵母菌25℃、180 r/min有氧培养48 h后,进行5次平行平板计数试验,根据平板计数的数据处理方法,得到浓度为5.2×108CFU·m L-1的酿酒酵母菌液,再通过倍比稀释把所得菌液依次稀释成浓度为5.2×107、5.2×106、5.2×105、5.2×104CFU·m L-1的菌液,用以上不同浓度(5.2×104—5.2×108CFU·m L-1)的酿酒酵母菌对体外培养的绵羊瘤胃上皮细胞分别进行不同时间(2、4、8、12、24 h)的刺激,并设置对照组用DMEM/F12培养基代替酿酒酵母菌。然后提取总RNA,逆转录为c DNA后,利用实时荧光定量PCR技术和酶联免疫吸附测定(ELISA)法检测瘤胃上皮细胞中SBD-1表达差异。最后用SAS 9.2软件对数据进行相关差异性分析。【结果】荧光定量PCR结果表明,在各时间组内SBD-1 m RNA的表达量随着菌液浓度的增加均呈先升高后降低的趋势,当菌液浓度为5.2×107CFU·m L-1时表达量达到最大,并与对照组和其他浓度组相比差异极显著(P<0.01)。当菌液浓度一定时,SBD-1 m RNA的表达量先是随着刺激时间的延长而呈上升趋势,刺激时间为12 h时SBD-1 m RNA表达量达到峰值,之后呈下降趋势。因此,当浓度为5.2×107CFU·m L-1的菌液刺激瘤胃上皮细胞12 h后,SBD-1基因的表达量达到最高,且与此浓度下其他时间组的表达量相比差异极显著(P<0.01)。ELISA检测结果显示,SBD-1蛋白表达趋势与SBD-1 m RNA检测结果基本一致。不同浓度的菌液分别刺激绵羊瘤胃上皮细胞2、4、8、12、24 h后均能提高共培养上清中SBD-1蛋白的表达,且与对照组相比存在极显著差异(P<0.01)。在菌液浓度为5.2×107CFU·m L-1刺激瘤胃上皮细胞12 h后SBD-1蛋白分泌水平达到最高,与此浓度下各时间组相比差异极显著(P<0.01)。【结论】酿酒酵母菌能够提高绵羊瘤胃上皮细胞SBD-1的表达,且菌液浓度为5.2×107CFU·m L-1刺激瘤胃上皮细胞12 h后,SBD-1的表达量达到最高。