Oral mycobiome

口腔分枝杆菌
  • 文章类型: Journal Article
    口腔念珠菌病(OC),口腔粘膜普遍的机会性感染,带来了相当大的健康挑战,特别是在免疫反应受损的个体中,高龄,和当地的易感条件。相当一部分人群在口腔中携带念珠菌,但很少有人开发OC。因此,OC的发病机理可能取决于真菌属性以外的因素,如宿主因素和其他诱发因素。粘膜创伤和炎症损害上皮完整性,培养有利于真菌入侵的环境。对免疫受损状态的分子洞察揭示了先天和适应性免疫的失调,为念珠菌增殖创造一个宽松的环境。念珠菌物种的详细检查(spp。)和他们的毒力因子揭示了超越传统白色念珠菌重点的细微差别的理解,涵盖多样化的念珠菌属。和他们的策略,影响附着力,入侵,免疫逃避,和生物膜的形成。了解OC中的病理生理微环境对于开发有针对性的治疗干预措施至关重要。这篇综述旨在揭示影响OC发育的各种病理生理微环境,重点是微生物,host,和诱发因素,并考虑了念珠菌对抗真菌治疗的耐药性。全面的方法为OC提供了一个精致的视角,简要寻求确定未来有效管理的潜在治疗目标。
    Oral candidiasis (OC), a prevalent opportunistic infection of the oral mucosa, presents a considerable health challenge, particularly in individuals with compromised immune responses, advanced age, and local predisposing conditions. A considerable part of the population carries Candida in the oral cavity, but only few develop OC. Therefore, the pathogenesis of OC may depend on factors other than the attributes of the fungus, such as host factors and other predisposing factors. Mucosal trauma and inflammation compromise epithelial integrity, fostering a conducive environment for fungal invasion. Molecular insights into the immunocompromised state reveal dysregulation in innate and adaptive immunity, creating a permissive environment for Candida proliferation. Detailed examination of Candida species (spp.) and their virulence factors uncovers a nuanced understanding beyond traditional C. albicans focus, which embrace diverse Candida spp. and their strategies, influencing adhesion, invasion, immune evasion, and biofilm formation. Understanding the pathophysiological microenvironments in OC is crucial for the development of targeted therapeutic interventions. This review aims to unravel the diverse pathophysiological microenvironments influencing OC development focusing on microbial, host, and predisposing factors, and considers Candida resistance to antifungal therapy. The comprehensive approach offers a refined perspective on OC, seeking briefly to identify potential therapeutic targets for future effective management.
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  • 文章类型: Journal Article
    这项研究的目的是表征家犬口腔分枝杆菌的多样性和多样性,并鉴定存在的共生和潜在致病真菌。从家犬中获得二百五十一个颊拭子,并将其照射到生色真菌生长培养基上,该培养基根据菌落颜色和形态区分真菌物种。在分离和收获单个菌落后,从纯培养物中提取基因组DNA。PCR用于扩增基因组的真菌特异性可变rDNA区域,然后送去测序。将测序结果输入到NCBIBLAST数据库中以鉴定测试的狗的口腔真菌生物群组的单个组分。在251只被擦拭的狗中,73只存在可培养的真菌,10只狗分离出多种真菌。尽管当时这些狗没有出现口腔感染的迹象,我们确实发现了在动物和人类中引起致病性的真菌物种。在真菌分离物中,马拉色菌和念珠菌属的种类占主导地位。经过真菌分离鉴定,对每个分离物进行抗真菌药物敏感性试验,对医学上重要的抗真菌药物,包括氟康唑,酮康唑,还有特比萘芬.药敏试验结果表明,大量分离株对3种药物均有较高的MIC值。探索狗的口腔分枝杆菌,以及相应的药物敏感性概况,会对犬科牙齿卫生产生重要影响,健康,和医疗。识别犬嘴内的微生物可以说明一个健康问题的真菌病原体从我们的犬类同伴传播到人类的常见途径。
    The purpose of this study was to characterize the variety and diversity of the oral mycobiome of domestic dogs and to identify the commensal and potentially pathogenic fungi present. Two hundred fifty-one buccal swabs from domestic dogs were obtained and struck onto a chromogenic fungal growth medium that distinguishes between fungal species based on colony color and morphology. After isolating and harvesting single colonies, genomic DNA was extracted from pure cultures. PCR was used to amplify a fungal-specific variable rDNA region of the genome, which was then sent for sequencing. Sequencing results were input into the NCBI BLAST database to identify individual components of the oral mycobiome of tested dogs. Of the 251 dogs swabbed, 73 had cultivable fungi present and 10 dogs had multiple fungal species isolated. Although the dogs did not show signs of oral infections at the time, we did find fungal species that cause pathogenicity in animals and humans. Among fungal isolates, Malassezia pachydermatis and species from the genus Candida were predominant. Following fungal isolate identification, antifungal drug susceptibility tests were performed on each isolate toward the medically important antifungal drugs including fluconazole, ketoconazole, and terbinafine. Drug susceptibility test results indicated that a large number of isolates had high MIC values for all three drugs. Exploring the oral mycobiome of dogs, as well as the corresponding drug susceptibility profiles, can have important implications for canine dental hygiene, health, and medical treatment. Identifying the microorganisms within the canine mouth can illustrate a common pathway for fungal pathogens of One Health concern to spread from our canine companions to humans.
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  • 文章类型: Journal Article
    高活性抗逆转录病毒治疗(HAART)已大大减少了HIV感染者的机会性感染。然而,即使使用HAART,艾滋病毒感染者患口腔疾病的风险仍然增加,包括龋齿。龋齿的发展与导致群落生态失调的微生物群落变化有关。HIV感染可以显著改变口腔中的细菌群和分枝杆菌群组成;然而,这些影响尚未评估龋齿的发生和进展.这项研究的目的是表征来自HIV感染(HI)的牙龈上菌斑样本的分枝杆菌组,艾滋病毒暴露但未感染(HEU),以及未接触艾滋病毒和未感染(HUU)的有龋齿和无龋齿的儿童。要做到这一点,对127个样品的ITS1扩增子进行测序。我们发现,HIV感染和暴露会导致健康和龋齿的牙龈上菌斑的变化。总的来说,观察到随着龋齿的发展,群落多样性减少,HI儿童的多样性最低,HEU儿童的多样性最高。白色念珠菌是确定的最丰富的物种,具有177个不同的扩增子序列变体(ASV)。两个白色念珠菌ASV主导了数据(所有分类分配的53.0%和38.5%)。更频繁的ASV主导了HI和HUU社区,而第二个占主导地位的HEU社区。HEU儿童的白色念珠菌丰度也最低,与健康相关的分类单元(分类单元与无龋齿统计相关)数量最高。重要的全球,龋齿是最常见的慢性儿童疾病之一,尽管有证据表明真菌会导致酸产生增加,加剧牙釉质脱矿,但对负责的微生物群落的真菌成分的研究却很少。艾滋病毒感染是另一个全球健康危机。围产期HIV感染是龋齿的危险因素;然而,在没有感染的情况下,围产期HIV暴露的龋齿经验不太清楚。使用高通量扩增子测序,我们发现分类差异在晚期龋齿中变得明显。值得注意的是,我们显示,与未暴露和未感染的儿童相比,HIV暴露但未感染的儿童与健康相关分类群的相关性更强.对于暴露但未感染的儿童,这与6岁或6岁以下的乳牙中龋齿的发生率较低相符。最终,这些发现有助于改进风险评估,干预,和预防策略,如生物膜破坏和知情的设计,pre,和合生元口服疗法。
    OBJECTIVE: Globally, caries is among the most frequent chronic childhood disease, and the fungal component of the microbial community responsible is poorly studied despite evidence that fungi contribute to increased acid production exacerbating enamel demineralization. HIV infection is another global health crisis. Perinatal HIV exposure with infection are caries risk factors; however, the caries experience in the context of perinatal HIV exposure without infection is less clear. Using high-throughput amplicon sequencing, we find taxonomic differences that become pronounced during late-stage caries. Notably, we show a stronger correlation with health-associated taxa for HIV-exposed-but-uninfected children when compared to unexposed and uninfected children. This aligns with a lower incidence of caries in primary teeth at age 6 or less for exposed yet uninfected children. Ultimately, these findings could contribute to improved risk assessment, intervention, and prevention strategies such as biofilm disruption and the informed design of pro-, pre-, and synbiotic oral therapies.
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  • 文章类型: Journal Article
    背景:口腔真菌群的菌群失调与一些疾病有关,包括癌症。然而,口腔真菌群落在鼻咽癌(NPC)癌变中的作用以前尚未得到研究.
    方法:我们使用真菌内部转录间隔区(ITS)-2测序,在476名未经治疗的NPC患者和537名基于人群的对照中,对口腔唾液真菌真菌基因组进行了表征。通过生物信息学和生物统计学分析评估口腔真菌基因组与NPC风险之间的关系。
    结果:我们发现较低的真菌α多样性与NPC的几率增加有关[较低与较高:观察到的特征(调整后的比值比[OR]=5.81,95%置信区间[CI]=3.60-9.38);辛普森多样性(1.53,1.03-2.29);香农多样性(2.03,1.35-3.04)]。我们还观察到,基于Bray-Curtis差异,病例和对照组之间的全球真菌群落模式存在显着差异(P<0.001)。口腔真菌物种的运输,具体来说,酿酒酵母,热带念珠菌,长孢子菌,白色念珠菌,和镰刀菌,与显著较高的NPC几率相关,OR范围从1.56到4.66。真菌和细菌α多样性低的个体患NPC的风险显著升高。
    结论:我们的结果表明口腔真菌群的菌群失调,以真菌群落多样性的丧失和几种真菌有机体的过度生长为特征,与NPC的风险大幅增加有关。
    背景:这项工作由美国国立卫生研究院资助,瑞典研究委员会,福建医科大学高层次人才研究启动项目,和中国奖学金委员会。
    BACKGROUND: Dysbiosis of the oral mycobiome has been linked to some diseases, including cancers. However, the role of oral fungal communities in nasopharyngeal carcinoma (NPC) carcinogenesis has not previously been investigated.
    METHODS: We characterized the oral salivary fungal mycobiome in 476 untreated incident NPC patients and 537 population-based controls using fungal internal transcribed spacer (ITS)-2 sequencing. The relationship between oral fungal mycobiome and the risk of NPC was assessed through bioinformatic and biostatistical analyses.
    RESULTS: We found that lower fungal alpha diversity was associated with an increased odds of NPC [lower vs. higher: observed features (adjusted odds ratio [OR] = 5.81, 95% confidence interval [CI] = 3.60-9.38); Simpson diversity (1.53, 1.03-2.29); Shannon diversity (2.03, 1.35-3.04)]. We also observed a significant difference in global fungal community patterns between cases and controls based on Bray-Curtis dissimilarity (P < 0.001). Carriage of oral fungal species, specifically, Saccharomyces cerevisiae, Candida tropicalis, Lodderomyces elongisporus, Candida albicans, and Fusarium poae, was associated with significantly higher odds of NPC, with ORs ranging from 1.56 to 4.66. Individuals with both low fungal and low bacterial alpha diversity had a profoundly elevated risk of NPC.
    CONCLUSIONS: Our results suggest that dysbiosis in the oral mycobiome, characterized by a loss of fungal community diversity and overgrowth of several fungal organisms, is associated with a substantially increased risk of NPC.
    BACKGROUND: This work was funded by the US National Institutes of Health, the Swedish Research Council, the High-level Talents Research Start-up Project of Fujian Medical University, and the China Scholarship Council.
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  • 文章类型: Journal Article
    代谢功能障碍相关脂肪性肝病(MAFLD)是与代谢综合征相关的肝脏疾病的表型。MAFLD的发病机制尚不清楚。肝脏位于肠道附近,通过代谢交换和微生物传播与肠道在生理上相互依赖,支持最近提出的“口-肠-肝轴”概念。然而,对共生真菌在疾病发展中的作用知之甚少。本研究旨在描述口腔和肠道真菌的变化及其在MAFLD中的作用。纳入21名MAFLD参与者和20名健康对照。唾液的宏基因组学分析,牙龈上斑块,粪便显示MAFLD患者的肠道真菌成分发生了显着变化。尽管MAFLD和健康组的口腔分枝杆菌多样性没有统计学差异,在MAFLD患者的粪便样本中观察到多样性显著降低.一种唾液物种的相对丰度,五种牙龈上物种,MAFLD患者的7种粪便发生了显着变化。22个唾液,23牙龈上,22种粪便与临床参数相关。关于真菌物种的不同功能,涉及代谢途径的途径,次级代谢产物的生物合成,不同环境中的微生物代谢,在口腔和肠道分枝杆菌中,碳代谢都很丰富。此外,在MAFLD患者和健康对照组之间观察到不同的真菌对核心功能的贡献,尤其是牙龈上斑块和粪便样本。最后,口腔/肠道真菌群和临床参数之间的相关性分析确定了口腔和肠道生态位中某些真菌种类的相关性。特别是,Mucorambiguus,唾液和粪便中都很丰富,与体重指数呈正相关,总胆固醇,低密度脂蛋白,丙氨酸氨基转移酶,和天冬氨酸氨基转移酶,提供可能的“口腔-肠道-肝脏”轴的证据。这些发现说明了核心分枝杆菌群与MAFLD发展之间的潜在相关性,并可能提出潜在的治疗策略。
    Metabolic dysfunction-associated fatty liver disease (MAFLD) is a phenotype of liver diseases associated with metabolic syndrome. The pathogenesis MAFLD remains unclear. The liver maintains is located near the intestine and is physiologically interdependent with the intestine via metabolic exchange and microbial transmission, underpinning the recently proposed \"oral-gut-liver axis\" concept. However, little is known about the roles of commensal fungi in the disease development. This study aimed to characterize the alterations of oral and gut mycobiota and their roles in MAFLD. Twenty-one MAFLD participants and 20 healthy controls were enrolled. Metagenomics analyses of saliva, supragingival plaques, and feces revealed significant alterations in the gut fungal composition of MAFLD patients. Although no statistical difference was evident in the oral mycobiome diversity within MAFLD and healthy group, significantly decreased diversities were observed in fecal samples of MAFLD patients. The relative abundance of one salivary species, five supragingival species, and seven fecal species was significantly altered in MAFLD patients. Twenty-two salivary, 23 supragingival, and 22 fecal species were associated with clinical parameters. Concerning the different functions of fungal species, pathways involved in metabolic pathways, biosynthesis of secondary metabolites, microbial metabolism in diverse environments, and carbon metabolism were abundant both in the oral and gut mycobiomes. Moreover, different fungal contributions in core functions were observed between MAFLD patients and the healthy controls, especially in the supragingival plaque and fecal samples. Finally, correlation analysis between oral/gut mycobiome and clinical parameters identified correlations of certain fungal species in both oral and gut niches. Particularly, Mucor ambiguus, which was abundant both in saliva and feces, was positively correlated with body mass index, total cholesterol, low-density lipoprotein, alanine aminotransferase, and aspartate aminotransferase, providing evidence of a possible \"oral-gut-liver\" axis. The findings illustrate the potential correlation between core mycobiome and the development of MAFLD and could propose potential therapeutic strategies.
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  • 文章类型: Journal Article
    真菌是人类微生物生态系统的真菌成分,仅占该环境的一小部分,但在维持稳态中起着至关重要的作用。真菌在出生后立即开始定殖。最初的分枝杆菌群受到新生儿胎龄的影响,出生体重,交货方法和喂养方法。在人类的生活中,真菌群的组成进一步受到大量内源性和外源性因素的影响。最重要的因素是饮食,体重,年龄,性和抗生素和抗真菌治疗。人类的真菌群栖息在口腔中,胃肠道,呼吸道,泌尿生殖道和皮肤。其组成可以通过免疫和非免疫介导的串扰系统影响肠-脑轴。它还通过协同和拮抗关系与生态系统的其他共生相互作用。此外,机会性真菌病原体在免疫受损个体中的肠道定植可导致临床相关的疾病状态。因此,真菌生物组是与各种生理和病理过程相关的微生物组的重要组成部分。这篇综述总结了关于人体特定部位的分枝杆菌组成及其在健康和疾病中的作用的最新知识。
    The mycobiome is the fungal component of the human microbial ecosystem that represents only a small part of this environment but plays an essential role in maintaining homeostasis. Colonization by fungi begins immediately after birth. The initial mycobiome is influenced by the gestational age of a newborn, birth weight, delivery method and feeding method. During a human\'s life, the composition of the mycobiome is further influenced by a large number of endogenous and exogenous factors. The most important factors are diet, body weight, age, sex and antibiotic and antifungal therapy. The human mycobiome inhabits the oral cavity, gastrointestinal tract, respiratory tract, urogenital tract and skin. Its composition can influence the gut-brain axis through immune and non-immune mediated crosstalk systems. It also interacts with other commensals of the ecosystem through synergistic and antagonistic relationships. Moreover, colonization of the gut by opportunistic fungal pathogens in immunocompromised individuals can lead to clinically relevant disease states. Thus, the mycobiome represents an essential part of the microbiome associated with a variety of physiological and pathological processes. This review summarizes the current knowledge on the composition of the mycobiome in specific sites of the human body and its role in health and disease.
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  • 文章类型: Journal Article
    无烟烟草(SLT)改变无烟烟草使用者的口腔微生物组。口腔菌群失调已经确定;然而,SLT用户的分枝杆菌组尚未被表征。通过扩增和测序来自非SLT使用者的口腔拭子样品的真菌内部转录间隔区(ITS1)区域来测定口腔真菌生物群组,SLT使用者(有或没有口腔损伤),和SLT与酒精使用者。我们观察到,有口腔病变的SLT使用者的口腔分枝杆菌组的丰富度和多样性明显低于非使用者。β多样性分析显示,非使用者和SLT与口腔病变使用者之间的口腔分枝杆菌组明显不同。口腔分枝杆菌的线性判别分析效应大小和随机森林分析证实,毕赤酵母属是典型的SLT口腔病变使用者。毕赤酵母属真菌的患病率与Starmerella呈正相关,被孢霉,镰刀菌,Calonectria,还有Madurella,但与Pynochaeta负相关,葡萄孢菌,还有Alternaria.Further,口腔分枝杆菌功能的测定显示,在营养水平和行会水平上,高丰度的病菌-腐生-共生体和动物病原体-内生菌-附生植物-未定义的腐生,分别,表明真菌类型的正常生长抑制可能发生重大变化。首次确定并全面分析了SLT使用者的口腔分枝杆菌。SLT摄入与口腔真菌群菌群失调有关,口腔真菌群的这种改变可能有助于SLT使用者的口腔癌变。这项研究将为进一步大规模研究分枝杆菌在SLT诱导的口腔癌中的潜在作用提供基础。关键点:•SLT诱导口腔微生物组的菌群失调,其可导致口腔癌。•在具有口腔病变的SLT使用者中,口腔分枝杆菌多样性显著降低。•毕赤酵母的发生可以用作具有口腔病变的SLT使用者的生物标志物。
    Smokeless tobacco (SLT) alters the oral microbiome of smokeless tobacco users. Dysbiosis of oral bacteriome has been determined; however, the mycobiome of SLT users has not been characterized. The oral mycobiome was assayed by amplification and sequencing of the fungal internal transcribed spacer (ITS1) region from oral swab samples of non-SLT users, SLT users (with or without oral lesions), and SLT with alcohol users. We observed that the richness and diversity of oral mycobiome were significantly decreased in SLT with oral lesions users than in non-users. The β-diversity analysis showed significant dissimilarity of oral mycobiome between non-users and SLT with oral lesions users. Linear discriminant analysis effect size and random forest analysis of oral mycobiome affirm that the genus Pichia was typical for SLT with oral lesions users. Prevalence of the fungal genus Pichia correlates positively with Starmerella, Mortierella, Fusarium, Calonectria, and Madurella, but is negatively correlated with Pyrenochaeta, Botryosporium, and Alternaria. Further, the determination of oral mycobiome functionality showed a high abundance of pathotroph-saprotroph-symbiotroph and animal pathogen-endophyte-epiphyte-undefined saprotroph at trophic and guild levels, respectively, indicating possibly major changes in normal growth repression of types of fungi. The oral mycobiome in SLT users was identified and comprehensively analyzed for the first time. SLT intake is associated with oral mycobiome dysbiosis and such alterations of the oral mycobiome may contribute to oral carcinogenesis in SLT users. This study will provide a basis for further large-scale investigations on the potential role of the mycobiome in SLT-induced oral cancer. KEY POINTS: • SLT induces dysbiosis of the oral microbiome that can contribute to oral cancer. • Oral mycobiome diversity is noticeably reduced in SLT users having oral lesions. • Occurrence of Pichia can be used as a biomarker for SLT users having oral lesions.
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  • 文章类型: Journal Article
    萎缩性舌炎是口腔粘膜疾病中的常见疾病。目前的研究已经发现人类口腔中含有许多不同的微生物,各种口腔疾病可以改变它们的组成和多样性。了解萎缩性舌炎口腔微生物组的组成和多样性,更好地探讨萎缩性舌炎的病因和机制。唾液微生物组由每个人特有的土著口腔微生物组成,具有长期稳定性。我们使用基于细菌16SrRNA基因的V3-V4区域和来自萎缩性舌炎患者和健康个体唾液的真菌rRNA基因的内部转录间隔区(ITS)的lluminaMiSeq高通量测序来探索口腔微生物组的组成和多样性。在我们的报告中,与健康个体相比,萎缩性舌炎患者的细菌和真菌多样性较低。数据进一步表明,乳酸杆菌和酵母菌是萎缩性舌炎发生和发展的潜在指标。此外,我们还讨论了口腔微生物生态学与萎缩性舌炎之间的关系。
    Atrophic glossitis is a common disease in oral mucosal diseases. The Current studies have found the human oral cavity contains numerous and diverse microorganisms, their composition and diversity can be changed by various oral diseases. To understand the composition and diversity of oral microbiome in atrophic glossitis is better to explore the cause and mechanism of atrophic glossitis. The salivary microbiome is comprised of indigenous oral microorganisms that are specific to each person, exhibits long-term stability. We used llumina MiSeq high-throughput sequencing based on the V3-V4 region of the bacterial 16S rRNA gene and the internal transcribed spacer (ITS) region of fungal rRNA genes from saliva in atrophic glossitis patients and healthy individuals to explore the composition and diversity of oral microbiome. In our reports, it showed a lower diversity of bacteria and fungi in atrophic glossitis patients than in healthy individuals. The data further suggests that Lactobacillus and Saccharomycetales were potential indicators for the initiation and development of atrophic glossitis. Moreover, we also discuss the relationship between the oral microbial ecology and atrophic glossitis.
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  • 文章类型: Journal Article
    简介:囊性纤维化(CF)是一种常染色体遗传病,与粘膜过厚和危及生命的慢性肺部感染有关。口腔的微生物群可以充当可在肺定居的感染性微生物的储库或屏障。然而,CF中口腔微生物组的具体组成知之甚少。方法:与西班牙的CF协会合作,我们从31个CF人(年龄范围7-47岁)和匹配的对照中收集了口腔冲洗样本,然后进行16SrRNA元编码和高通量测序,结合培养和基于蛋白质组学的真菌鉴定来调查细菌和真菌口腔微生物组。结果:我们发现CF与较少多样性的口腔微生物有关,其特征是白色念珠菌的患病率较高,并且许多细菌分类群的丰度不同,这对CF中与肺部感染的联系都有影响,以及潜在的口腔健康问题,特别是牙周炎和龋齿。结论:总体而言,我们的研究提供了CF口腔微生物组的第一个全局快照.需要进一步的研究来建立CF中口腔和肺微生物组组成之间的关系。
    Introduction: Cystic fibrosis (CF) is an autosomal genetic disease, associated with the production of excessively thick mucosa and with life-threatening chronic lung infections. The microbiota of the oral cavity can act as a reservoir or as a barrier for infectious microorganisms that can colonize the lungs. However, the specific composition of the oral microbiome in CF is poorly understood.Methods: In collaboration with CF associations in Spain, we collected oral rinse samples from 31 CF persons (age range 7-47) and matched controls, and then performed 16S rRNA metabarcoding and high-throughput sequencing, combined with culture and proteomics-based identification of fungi to survey the bacterial and fungal oral microbiome.Results: We found that CF is associated with less diverse oral microbiomes, which were characterized by higher prevalence of Candida albicans and differential abundances of a number of bacterial taxa that have implications in both the connection to lung infections in CF, as well as potential oral health concerns, particularly periodontitis and dental caries.Conclusion: Overall, our study provides a first global snapshot of the oral microbiome in CF. Future studies are required to establish the relationships between the composition of the oral and lung microbiomes in CF.
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  • 文章类型: Journal Article
    简介:口腔拥有丰富多样的微生物群落(即微生物组),其组成和在健康和疾病中的作用一直是激烈研究的焦点。唐氏综合症(DS)与口腔中的特定特征有关,与对照组相比,龋齿的发生率较低,牙周炎和牙龈炎的发生率较高。然而,对DS中口腔微生物组的总体组成以及其如何随宿主年龄或口腔内pH等多种因素而变化的了解仍然很少。方法:与西班牙的DS协会合作,使用公民科学方法,我们进行了16SrRNA元编码和高通量测序,结合培养和基于蛋白质组学的真菌鉴定,以调查27个DS人(年龄范围7-55)和对照样品中的细菌和真菌口腔微生物组,并与地理分布相匹配,年龄范围,和性别。结果:我们发现DS与低唾液pH值和较少的口腔微生物有关,其特征是低水平的Alloprevotella,Atobobium,CandidatusSacchiimonas,更多的金埃拉,葡萄球菌,Gemella,心脏杆菌,Rothia,放线杆菌,念珠菌的患病率更高。结论:总之,我们的研究首次提供了DS口腔微生物组的全局快照.需要进一步的研究来确定观察到的差异是否与DS口腔中的差异病理有关。
    Introduction: The oral cavity harbors an abundant and diverse microbial community (i.e. the microbiome), whose composition and roles in health and disease have been the focus of intense research. Down syndrome (DS) is associated with particular characteristics in the oral cavity, and with a lower incidence of caries and higher incidence of periodontitis and gingivitis compared to control populations. However, the overall composition of the oral microbiome in DS and how it varies with diverse factors like host age or the pH within the mouth are still poorly understood. Methods: Using a Citizen-Science approach in collaboration with DS associations in Spain, we performed 16S rRNA metabarcoding and high-throughput sequencing, combined with culture and proteomics-based identification of fungi to survey the bacterial and fungal oral microbiome in 27 DS persons (age range 7-55) and control samples matched by geographical distribution, age range, and gender. Results: We found that DS is associated with low salivary pH and less diverse oral microbiomes, which were characterized by lower levels of Alloprevotella, Atopobium, Candidatus Saccharimonas, and higher amounts of Kingella, Staphylococcus, Gemella, Cardiobacterium, Rothia, Actinobacillus, and greater prevalence of Candida. Conclusion: Altogether, our study provides a first global snapshot of the oral microbiome in DS. Future studies are required to establish whether the observed differences are related to differential pathology in the oral cavity in DS.
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