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  • 文章类型: Case Reports
    一名71岁的男子因肺癌右上叶切除术后间质性肺炎急性加重而入院。入院后呼吸衰竭加重,他需要机械通气.他正在接受强化免疫抑制治疗,包括大剂量皮质类固醇和环孢素,每天有六次水样腹泻。在粪便中发现了白细胞,怀疑是肠道感染。粪便培养物显示无致病菌。胃肠道感染的多重聚合酶链反应产生阴性结果。基于CMV抗原血症测定中巨细胞病毒(CMV)抗原阳性细胞的数量增加,我们怀疑CMV结肠炎.然而,患者仍在接受机械通气,结肠镜检查很难进行。在向患者解释程序并获得其同意后,BioFire®FilmArray®脑膜炎/脑炎(ME)小组使用粪便标本进行。检测到CMV。立即开始静脉输注5mg/kg更昔洛韦,每12小时给药3周。此后每24小时继续静脉输注5mg/kg,再持续三周。当怀疑CMV结肠炎,但患者的病情阻止通过结肠镜检查收集组织和通过组织病理学的标准诊断,使用粪便样本添加CMVPCR可能有助于CMV结肠炎的临床诊断.多重聚合酶链反应的使用有望有助于及时和适当的治疗。
    A 71-year-old man was admitted because of acute exacerbation of interstitial pneumonia following a right upper lobectomy for lung cancer. His respiratory failure worsened after admission, and he required mechanical ventilation. He was undergoing intensive immunosuppressive treatment, including high-dose corticosteroids and cyclosporine, and had watery diarrhea six times a day. White blood cells were found in the stool, and an intestinal infection was suspected. Fecal cultures showed no pathogenic bacteria. Multiplex polymerase chain reaction for gastrointestinal infection yielded negative results. Based on the increasing number of cytomegalovirus (CMV) antigen-positive cells in the CMV antigenemia assay, we suspected CMV colitis. However, the patient was still undergoing mechanical ventilation, and colonoscopy was difficult to perform. After explaining the procedure to the patient and obtaining his consent, the BioFire® FilmArray® Meningitis/Encephalitis (ME) Panel was performed using a fecal specimen. CMV was detected. Intravenous infusion of ganciclovir at 5 mg/kg was immediately commenced and administered every 12 hours for three weeks. Intravenous infusion at 5 mg/kg was continued every 24 hours thereafter for a further three weeks. When CMV colitis is suspected but the patient\'s condition prevents tissue collection through colonoscopy and standard diagnosis by histopathology, the addition of CMV PCR using a stool sample may assist in the clinical diagnosis of CMV colitis. The use of multiplex polymerase chain reaction is expected to contribute to prompt and appropriate treatment.
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  • 文章类型: Journal Article
    儿童炎症性肠病(IBD)的诊断和区分亚型(克罗恩病(CD)和溃疡性结肠炎(UC))的需要需要长期的调查和侵入性程序。非侵入性,快速,并且需要具有成本效益的测试来支持这些诊断。粪便挥发性有机化合物(VOCs)在IBD中是独特的。可以使用气相色谱传感器装置(OdoReader®)快速确定VOC分布。在出现疑似IBD的儿童的初始队列中,我们直接比较了粪便钙卫蛋白(FCP,肠道炎症的非特异性蛋白质标志物)与OdoReader©随后诊断为IBD的儿童与诊断为其他胃肠道疾病的匹配对照的VOC谱。OdoReader©在来自同一队列的单独样本中验证时,在其他胃肠道疾病中诊断IBD的敏感性为82%(95%置信区间75-89%),特异性为71%(61-80%),但未优于FCP(敏感性为93%(77-99%)和特异性为86%(67-96%);250µg/gFCP截止)。然而,与FCP不同,也比其他类似技术更好,OdoReader©可以区分儿科CD和UC(在验证集中高达88%(82-93%)的敏感性和80%(71-89%)的特异性),并证明在大型研究中进一步验证是合理的.基于VOC的非侵入性测试可以帮助简化和限制儿童的侵入性调查。
    The diagnosis of inflammatory bowel disease (IBD) in children and the need to distinguish between subtypes (Crohn\'s disease (CD) and ulcerative colitis (UC)) requires lengthy investigative and invasive procedures. Non-invasive, rapid, and cost-effective tests to support these diagnoses are needed. Faecal volatile organic compounds (VOCs) are distinctive in IBD. VOC profiles can be rapidly determined using a gas chromatography-sensor device (OdoReader©). In an inception-cohort of children presenting with suspected IBD, we directly compared the diagnostic fidelity of faecal calprotectin (FCP, a non-specific protein marker of intestinal inflammation) with OdoReader© VOC profiles of children subsequently diagnosed with IBD with matched controls diagnosed with other gastrointestinal conditions. The OdoReader© was 82% (95% confidence interval 75-89%) sensitive and 71% (61-80%) specific but did not outperform FCP (sensitivity 93% (77-99%) and specificity 86% (67-96%); 250 µg/g FCP cut off) in the diagnosis of IBD from other gastrointestinal conditions when validated in a separate sample from the same cohort. However, unlike FCP and better than other similar technologies, the OdoReader© could distinguish paediatric CD from UC (up to 88% (82-93%) sensitivity and 80% (71-89%) specificity in the validation set) and justifies further validation in larger studies. A non-invasive test based on VOCs could help streamline and limit invasive investigations in children.
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  • 文章类型: Journal Article
    烫伤发生在皮肤遇到热液体或蒸汽时。虽然大多数烫伤都是偶然的,医疗提供者必须评估可能的滥用。我们报告了一例2岁女性,她因臀部烧伤而与父母一起去医院,有大便从肛门排出并被困在皮肤上的病史。医疗提供者需要考虑偶然和造成的差异,因为意外伤害确实发生在儿童身上,错误的诊断可能会产生严重的法医学后果。
    Scald burns occur when the skin encounters hot liquid or steam. Although most scald burns are accidental, the medical provider must assess for possible abuse. We report a case of a 2-year-old female who presented to the hospital with her parents due to a burn to the buttocks with a history of stool expelling from the anus and becoming trapped against the skin. Medical providers need to consider accidental and inflicted differentials, as accidental injuries do occur in children, and an incorrect diagnosis may have severe medicolegal consequences.
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  • 文章类型: Journal Article
    螺旋体病包括一组通过性或直接接触传播并归因于梅毒螺旋体的慢性和使人衰弱的细菌性疾病。尽管早在1963年就被记录在案,但由于与进行检查和从野生动物获得侵入性生物样本相关的固有挑战,野生灵长类动物中的密螺旋体病的流行病学仍然是一个未经调查的领域。这项研究的主要目的是调查塞内加尔极度濒危的西方黑猩猩中螺旋体感染的存在,利用创新的非侵入性粪便血清学方法。我们提供了令人信服的证据,证明29只黑猩猩中有13只存在抗螺旋体特异性抗体。我们的研究还强调了粪便血清学作为一种有价值的非侵入性工具的巨大潜力,用于监测和监测野生动物中关键的新兴疾病。我们认识到两个主要含义:(1)迫切需要评估西方黑猩猩群体的密螺旋体病风险;(2)必须采用整体的“一种健康”方法来监测和管理这种疾病。
    Treponematoses encompass a group of chronic and debilitating bacterial diseases transmitted sexually or by direct contact and attributed to Treponema pallidum. Despite being documented since as far back as 1963, the epidemiology of treponematoses in wild primates has remained an uninvestigated territory due to the inherent challenges associated with conducting examinations and obtaining invasive biological samples from wild animals. The primary aim of this study was to investigate the presence of treponemal infections in the critically endangered Western chimpanzees in Senegal, utilizing an innovative non-invasive stool serology method. We provide compelling evidence of the existence of anti-Treponema-specific antibodies in 13 out of 29 individual chimpanzees. Our study also underscores the significant potential of stool serology as a valuable non-invasive tool for monitoring and surveilling crucial emerging diseases in wild animals. We recognize two major implications: (1) the imperative need to assess the risks of treponematosis in Western chimpanzee populations and (2) the necessity to monitor and manage this disease following a holistic One Health approach.
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  • 文章类型: Journal Article
    粪便元蛋白质组学是测量微生物和宿主蛋白质丰度变化并推断肠道微生物群的哪些成员参与特定功能和途径的有用方法。本章描述了一个方案,能够分析和表征粪便元蛋白质组,成功应用于人类,鼠标,和大鼠粪便样本。该协议结合了蛋白质提取的机械和热处理,基于离心过滤器的清理和消化程序,用于肽分离的长梯度液相色谱,和用于肽检测的高分辨率质谱。
    Fecal metaproteomics is a useful approach to measure changes in microbial and host protein abundance and to infer which members of the gut microbiota are involved in specific functions and pathways. This chapter describes a protocol enabling analysis and characterization of fecal metaproteomes, successfully applied to human, mouse, and rat stool samples. The protocol combines mechanical and thermal treatments for protein extraction, a centrifugal filter-based procedure for cleanup and digestion, long-gradient liquid chromatography for peptide separation, and high-resolution mass spectrometry for peptide detection.
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  • 文章类型: Journal Article
    霍乱弧菌O1引起腹泻病霍乱,小肠是活跃感染的部位。霍乱期间,霍乱毒素由霍乱弧菌分泌,并诱导大量液体流入小肠,导致呕吐和腹泻。通常,霍乱弧菌基因组从粪便中通过的细菌测序,但很少因为呕吐物,一种可能更接近地代表活动性感染部位的液体。我们假设与呕吐物相比,沿着胃肠道的霍乱弧菌O1种群瓶颈会导致粪便遗传变异减少。为了测试这个,我们对10例霍乱患者的霍乱弧菌基因组进行了测序,这些患者有配对的呕吐物和粪便样本。呕吐物和粪便的遗传多样性都很低,与单一感染人群一致,而不是与不同的霍乱弧菌O1谱系合并感染。4名患者从呕吐物到粪便的单核苷酸变异量减少,增加了两个,四个保持不变。8例患者的呕吐物和粪便之间的基因存在/缺失变异减少,2例增加。组装的短阅读测序的Pangenome分析表明,与粪便相比,毒素共同调节的菌毛操纵子更频繁地包含来自呕吐物的基因组缺失。然而,这些缺失没有通过PCR或长读测序检测到,这表明仅从短读数据解释基因存在或缺失模式可能是不完整的。总的来说,我们发现从粪便中分离的霍乱弧菌O1与从上肠道回收的霍乱弧菌在遗传上相似。
    目的:霍乱弧菌O1,引起霍乱的细菌,摄入受污染的食物或水中,然后在小肠上部定植,并在粪便中排泄。通常研究粪便中的霍乱弧菌基因组,但从呕吐物中分离出的霍乱弧菌可能更能代表霍乱弧菌在上肠上皮定植的地方。五、霍乱可能会遇到瓶颈,或者细菌种群规模和遗传多样性的大幅减少,当它穿过肠道时。通过肠道的传代可以选择适应于存活和肠道定植的不同霍乱弧菌突变体。我们没有找到这种适应性突变的有力证据,相反,观察到通过肠道导致霍乱弧菌遗传多样性的适度减少,只有一些病人。这些结果填补了我们对霍乱弧菌生命周期理解的空白,传输,和进化。
    Vibrio cholerae O1 causes the diarrheal disease cholera, and the small intestine is the site of active infection. During cholera, cholera toxin is secreted from V. cholerae and induces a massive fluid influx into the small intestine, which causes vomiting and diarrhea. Typically, V. cholerae genomes are sequenced from bacteria passed in stool, but rarely from vomit, a fluid that may more closely represents the site of active infection. We hypothesized that V. cholerae O1 population bottlenecks along the gastrointestinal tract would result in reduced genetic variation in stool compared to vomit. To test this, we sequenced V. cholerae genomes from 10 cholera patients with paired vomit and stool samples. Genetic diversity was low in both vomit and stool, consistent with a single infecting population rather than coinfection with divergent V. cholerae O1 lineages. The amount of single-nucleotide variation decreased from vomit to stool in four patients, increased in two, and remained unchanged in four. The variation in gene presence/absence decreased between vomit and stool in eight patients and increased in two. Pangenome analysis of assembled short-read sequencing demonstrated that the toxin-coregulated pilus operon more frequently contained deletions in genomes from vomit compared to stool. However, these deletions were not detected by PCR or long-read sequencing, indicating that interpreting gene presence or absence patterns from short-read data alone may be incomplete. Overall, we found that V. cholerae O1 isolated from stool is genetically similar to V. cholerae recovered from the upper intestinal tract.
    OBJECTIVE: Vibrio cholerae O1, the bacterium that causes cholera, is ingested in contaminated food or water and then colonizes the upper small intestine and is excreted in stool. Shed V. cholerae genomes from stool are usually studied, but V. cholerae isolated from vomit may be more representative of where V. cholerae colonizes in the upper intestinal epithelium. V. cholerae may experience bottlenecks, or large reductions in bacterial population sizes and genetic diversity, as it passes through the gut. Passage through the gut may select for distinct V. cholerae mutants that are adapted for survival and gut colonization. We did not find strong evidence for such adaptive mutations, and instead observed that passage through the gut results in modest reductions in V. cholerae genetic diversity, and only in some patients. These results fill a gap in our understanding of the V. cholerae life cycle, transmission, and evolution.
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  • 文章类型: Journal Article
    目的描述17周龄以下健康婴儿的排便规律。我们纳入了来自前瞻性HELMi队列(NCT03996304)的1052名健康足月婴儿。父母填写了关于喂养的经常性在线问卷,胃肠功能,在生命的前17周,每周哭一次。3周龄时排便频率最高(中位数为4次/天,四分位数间距(IQR)2.9-5)。在每个时间点,母乳喂养婴儿的中位排便频率高于接受配方奶粉的婴儿(例如,在第17周,平均每天2次,IQR0.9-3.6,中位数分别为1.1,IQR0.6-1.4)。粪便的主要颜色通常是黄色或浅棕色。在生命的第一周,几乎有黑色的粪便占3.4%。近一半(47.4%)的婴儿有绿色大便颜色占主导地位至少1周,母乳喂养(47.7%)和配方喂养(45.2%)婴儿的频率相当。绿色粪便与更高的排便频率相关(线性混合效应模型p<0.0001)。据报道,在9.3%的婴儿中偶尔出现粪便中的血液,在5.2%的婴儿中出现复发性血液,粪便稠度没有差异。硬便罕见(≤1%)。结论:这项研究启发了健康足月婴儿在生命的前17周内的排便模式。更好地了解肠道功能有助于医疗保健专业人员在解决排便时区分正常和异常,大便的颜色,和喂养的类型。已知:•母乳喂养的婴儿比配方喂养的婴儿具有更频繁和更多的黄色粪便。•绿色粪便通常由父母或甚至由医疗专业人员建议,以表明早期生活中的疾病或不适。新增内容:•在前17周期间,将近一半的健康足月婴儿具有至少一周的绿色粪便主导,并且在此期间,几乎10%的婴儿报告偶尔有血液。•肠道功能和粪便正常变化的数据可以为初级卫生保健专业人员提供教育婴儿的家庭和照顾者。
    The purpose of this study is to describe the defecation pattern of healthy infants up to 17 weeks of age. We included 1052 healthy term infants from the prospective HELMi cohort (NCT03996304). Parents filled in recurring online questionnaires on feeding, gastrointestinal function, and crying weekly for the first 17 weeks of life. Defecation frequency was highest at the age of 3 weeks (a median of 4 times/day, interquartile range (IQR) 2.9-5). At each time point, the median defecation frequency of breastfed infants was higher than that of infants receiving formula (e.g., at week 17 a median of 2 times/day, IQR 0.9-3.6, and a median of 1.1, IQR 0.6-1.4, respectively). The dominant color of the stool was most often yellow or light brown. Nearly black stools were reported in the first week of life in 3.4%. Nearly half (47.4%) of the infants had green stool color dominating for at least 1 week, with comparable frequency among breastfed (47.7%) and formula-fed (45.2%) infants. Green stools were associated with a higher defecation frequency (linear mixed-effect model p < 0.0001). Occasional blood in stool was reported in 9.3% and recurrent blood in 5.2% of the infants with no difference in stool consistency. Hard stools were rare (≤ 1%).     Conclusion: This study enlightens the spectrum of defecation patterns in healthy term infants during the first 17 weeks of life. A better understanding of bowel function helps healthcare professionals distinguish normal from abnormal when addressing defecation, the color of stools, and the type of feeding. What is Known: • Breastfed infants have more frequent and more yellow-colored stools than formula-fed infants. • Stools with green color are often suggested by the parents or even by medical professionals to indicate disease or discomfort in early life. What is New: • Nearly half of the healthy term infants had green stool dominating for at least one week during the first 17 weeks and occasional blood was reported in almost 10% of the infants during this period. • Data on normal variation in bowel function and stool may serve primary health care professionals when educating the families and caretakers of infants.
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  • 文章类型: Journal Article
    每年有一半以上的儿童结核病病例仍未确诊。世界卫生组织建议将Xpert-Ultra检测作为第一个儿科诊断测试,但微生物确认仍然很低。我们旨在确定Xpert-Ultra在2种高结核病负担环境中的粪便和尿液样本的诊断性能。
    这项无国界医生横断面多中心研究在西芒门德斯医院进行,几内亚比绍(2019年7月至2020年4月)和马拉卡勒医院,南苏丹(2021年4月至2023年6月)。6个月至15岁的儿童患有结核病,接受了临床和实验室评估,1个呼吸和/或肺外样本(参考标准[RS]),1个凳子,用Xpert-Ultra分析1份尿液样本。
    共有563名儿童参加了这项研究,有133人来自几内亚比绍,400人来自马拉卡勒;30人被排除在外。在75例(14.1%)中确认了结核病,而248(46.5%)患有未确诊的结核病。有RS样本的553,总诊断率为12.4%(533例中的66例).总共493个粪便和524个尿液样品用于评估Xpert-Ultra与这些样品的性能。与RS相比,Xpert-Ultra的敏感性和特异性为62.5%(95%置信区间,49.4%-74%)和98.3%(96.7%-99.2%),分别,粪便样本,和13.9%(7.5%-24.3%)和99.4%(98.1%-99.8%)的尿液样本。9名患者的粪便和/或尿液样本呈阳性,但RS呈阴性。
    与RS相比,粪便样本中的Xpert-Ultra显示出中等至高的灵敏度和高特异性,并且在RS结果为阴性时增加了诊断结果。粪便样本中的Xpert-Ultra在肺外病例中有用。尿液样品中的Xpert-Ultra显示低测试性能。
    NCT06239337。
    UNASSIGNED: More than half of childhood tuberculosis cases remain undiagnosed yearly. The World Health Organization recommends the Xpert-Ultra assay as a first pediatric diagnosis test, but microbiological confirmation remains low. We aimed to determine the diagnostic performance of Xpert-Ultra with stool and urine samples in presumptive pediatric tuberculosis cases in 2 high-tuberculosis-burden settings.
    UNASSIGNED: This Médecins Sans Frontières cross-sectional multicentric study took place at Simão Mendes Hospital, Guinea-Bissau (July 2019 to April 2020) and in Malakal Hospital, South Sudan (April 2021 to June 2023). Children aged 6 months to 15 years with presumptive tuberculosis underwent clinical and laboratory assessment, with 1 respiratory and/or extrapulmonary sample (reference standard [RS]), 1 stool, and 1 urine specimen analyzed with Xpert-Ultra.
    UNASSIGNED: A total of 563 children were enrolled in the study, 133 from Bissau and 400 from Malakal; 30 were excluded. Confirmation of tuberculosis was achieved in 75 (14.1%), while 248 (46.5%) had unconfirmed tuberculosis. Of 553 with an RS specimen, the overall diagnostic yield was 12.4% (66 of 533). A total of 493 stool and 524 urine samples were used to evaluate the performance of Xpert-Ultra with these samples. Compared with the RS, the sensitivity and specificity of Xpert-Ultra were 62.5% (95% confidence interval, 49.4%-74%) and 98.3% (96.7%-99.2%), respectively, with stool samples, and 13.9% (7.5%-24.3%) and 99.4% (98.1%-99.8%) with urine samples. Nine patients were positive with stool and/or urine samples but negative with the RS.
    UNASSIGNED: Xpert-Ultra in stool samples showed moderate to high sensitivity and high specificity compared with the RS and an added diagnostic yield when RS results were negative. Xpert-Ultra in stool samples was useful in extrapulmonary cases. Xpert-Ultra in urine samples showed low test performance.
    UNASSIGNED: NCT06239337.
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  • 文章类型: Journal Article
    隐孢子虫。微孢子虫是机会性微生物,由于它们感染人类和动物的能力,具有显着的人畜共患传播潜力。这项研究的目的是评估这些微生物在动物和人类粪便样本中的患病率。总的来说,研究中包括369个粪便样品(205个来自患有腹泻的人类患者和164个动物来源)。隐孢子虫。使用多重巢式PCR确定微孢子虫的存在。通过使用扩增子的Sanger测序分析阳性结果,利用BLASTN和ClustalX软件确认身份。隐孢子虫。在0.97%和4.26%的人类和动物样本中发现,分别。在6.82%和3.05%的样本中,在人和动物粪便中检测到肠孢子虫。分别。分析隐孢子虫的存在时未发现关联。和E.bieneusi以及患者和动物的人口统计学和临床变量。这项研究表明,这些微生物存在于来自不同物种的人类和动物样品中,最有趣的发现是隐孢子虫的检测。在宠物中(例如,啮齿动物)通常不包括在这种类型的研究中,以及无基础疾病的腹泻患者中E.bieneusi的鉴定。
    Cryptosporidium spp. and Microsporidia are opportunistic microorganisms with remarkable zoonotic transmission potential due to their capacity to infect humans and animals. The aim of this study was to evaluate the prevalence of these microorganisms in stool samples of animal and human origin. In total, 369 stool samples (205 from human patients with diarrhea and 164 of animal origin) were included in the study. Cryptosporidium spp. and Microsporidia presence were determined by using multiplex nested PCR. Positive results were analyzed by using Sanger sequencing of the amplicon, utilizing BLASTN and ClustalX software to confirm identification. Cryptosporidium spp. were found in 0.97% and 4.26% of human and animal samples, respectively. Enterocytozoon bieneusi was detected in human and animal stools in 6.82% and 3.05% of the samples, respectively. No associations were found when analyzing the presence of Cryptosporidium spp. and E. bieneusi and the demographic and clinical variables of patients and animals. This study demonstrates the presence of these microorganisms in human and animal samples from different species, and the most interesting findings are the detection of Cryptosporidium spp. in pets (e.g., rodents) that are not usually included in this type of study, and the identification of E. bieneusi in patients with diarrhea without underlying disease.
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  • 文章类型: Journal Article
    背景:最近的研究表明酒渣鼻与患者肠道菌群之间可能存在联系。
    目的:研究酒渣鼻患者和健康对照者粪便微生物谱的差异。
    方法:使用MiSeq16SrRNA测序分析了54例酒渣鼻患者(RP)的肠道菌群。肠型,厚壁菌/拟杆菌(F/B)比,α和β多样性的重要性,和差异丰度分析(DAA)进行计算,并与年龄和性别匹配的对照(CP,n=50)。
    结果:在RP和CP之间观察到肠型和F/B比率的显着变化(分别为p=0.017和p=0.002)。与CP相比,RP显示出微生物的丰富度和多样性降低(Shannonp=0.012,Simpson倒数p=0.034)。两组之间的β多样性也不同(PERMANOVA,p=0.006)。根据DAA检测到14个显着不同的分类单元。普劳斯尼齐粪杆菌(coef。-0.0800,p=0.008),天螺科ND3007组sp。(coef。-0.073,p<0.001),和反刍动物科(coef。-0.072,p=0.015)显着降低。(coef。0.023,p=0.031),Flavonifractorplautii(coef。0.011,p=0.037),和反刍动物科UBA1819(coef。与CP相比,RP中的0.010,p=0.031)显着增加。
    结论:RP中存在肠道菌群的显著改变。与CP相比,观察到分类学上的变化以及减少的丰富度和多样性。需要更大的前瞻性研究来研究与临床特征的相关性,并将这些发现转化为未来的治疗方法。
    BACKGROUND: Recent studies have suggested a possible connection between rosacea and patients\' gut microbiota.
    OBJECTIVE: To investigate the differences in fecal microbial profiles between patients with rosacea and healthy controls.
    METHODS: Gut microbiota of 54 rosacea patients (RP) were analyzed using MiSeq 16S rRNA sequencing. Enterotypes, the Firmicutes/Bacteroides (F/B) ratio, the significance of alpha and beta diversity, and differential abundance analysis (DAA) were calculated and compared with age- and gender-matched controls (CP, n = 50).
    RESULTS: Significant changes in the enterotypes and F/B ratio were observed between the RP and CP (p = 0.017 and p = 0.002, respectively). The RP showed a decreased microbial richness and diversity compared to the CP (Shannon p = 0.012, inverse Simpson p = 0.034). Beta diversity also differed between both groups (PERMANOVA, p = 0.006). Fourteen significantly different taxa were detected according to DAA. Faecalibacterium prausnitzii (coef. -0.0800, p = 0.008), Lachnoospiraceae ND 3007 group sp. (coef. -0.073, p < 0.001), and Ruminococcaceae (coef. -0.072, p = 0.015) were significantly decreased; Oscillobacter sp. (coef. 0.023, p = 0.031), Flavonifractor plautii (coef. 0.011, p = 0.037), and Ruminococccaceae UBA 1819 (coef. 0.010, p = 0.031) were significantly increased in the RP compared to the CP.
    CONCLUSIONS: Significant alterations in gut microbiota were present in the RP. Taxonomic shifts and reduced richness and diversity were observed when compared to the CP. Larger prospective studies are needed to investigate correlations with clinical features and to translate these findings into future therapeutic approaches.
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