Glucuronoxylomannan

  • 文章类型: Journal Article
    新生隐球菌是世界卫生组织(WHO)发布的真菌优先病原体清单(FPPL)中排名最高的真菌病原体。在这项研究中,通过计算机模拟,利用甘露糖蛋白抗原(MP88)作为候选疫苗,开发了一种针对新生隐球菌的多表位疫苗.在检索MP88蛋白序列后,这些被用来预测抗原性B细胞和T细胞表位通过bepipred工具和人工神经网络,分别。保守的B细胞表位AYSTPA,AYSTPAS,PASSNCK,和DSAYPP被鉴定为最有前途的B细胞表位。而YMAADQFCL,VSYEEWMNY,和FQQRYTGTF被鉴定为CD8+T细胞表位的最佳候选;和YARLLSLNA,ISYGTAMAV,和INQTSYARL被鉴定为最有前途的CD4+T细胞表位。将疫苗构建体与佐剂和肽接头一起建模,并使用expasyprotparam工具来预测理化性质。据此,预测构建疫苗是抗原性的,无毒,非过敏性,可溶性,稳定,亲水性,和热稳定。此外,三维结构也用于与Toll样受体(TLR4)的对接分析.最后,将疫苗的cDNA成功克隆到大肠杆菌pET-28a(+)表达载体中。本文提出的结果可能有助于设计针对新生隐球菌的有效疫苗。
    Cryptococcus neoformans is the highest-ranked fungal pathogen in the Fungal Priority Pathogens List (FPPL) released by the World Health Organization (WHO). In this study, through in silico simulations, a multi-epitope vaccine against Cryptococcus neoformans was developed using the mannoprotein antigen (MP88) as a vaccine candidate. Following the retrieval of the MP88 protein sequences, these were used to predict antigenic B-cell and T-cell epitopes via the bepipred tool and the artificial neural network, respectively. Conserved B-cell epitopes AYSTPA, AYSTPAS, PASSNCK, and DSAYPP were identified as the most promising B-cell epitopes. While YMAADQFCL, VSYEEWMNY, and FQQRYTGTF were identified as the best candidates for CD8+ T-cell epitopes; and YARLLSLNA, ISYGTAMAV, and INQTSYARL were identified as the most promising CD4+ T-cell epitopes. The vaccine construct was modeled along with adjuvant and peptide linkers and the expasy protparam tool was used to predict the physiochemical properties. According to this, the construct vaccine was predicted to be antigenic, nontoxic, nonallergenic, soluble, stable, hydrophilic, and thermostable. Furthermore, the three-dimensional structure was also used in docking analyses with Toll-like receptor (TLR4). Finally, the cDNA of vaccine was successfully cloned into the E. coli pET-28a (+) expression vector. The results presented here could contribute towards the design of an effective vaccine against Cryptococcus neoformans.
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  • 文章类型: Journal Article
    葡糖醛酸木甘露聚糖(GXM)是隐球菌属的主要荚膜成分。这种复合多糖参与了许多与隐球菌的生理和发病机制有关的事件。这突出了建立分离和分析方法的重要性。文献中广泛讨论了GXM分离的常规方法。在这一章中,我们描述了两种快速获得富含隐球菌GXM的细胞外级分的方法。
    Glucuronoxylomannan (GXM) is the principal capsular component in the Cryptococcus genus. This complex polysaccharide participates in numerous events related to the physiology and pathogenesis of Cryptococcus, which highlights the importance of establishing methods for its isolation and analysis. Conventional methods for GXM isolation have been extensively discussed in the literature. In this chapter, we describe two fast methods for obtaining extracellular fractions enriched with cryptococcal GXM.
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  • 文章类型: Journal Article
    真菌病原体新生隐球菌的标准测定之一是葡糖醛酸木甘露聚糖(GXM)ELISA。该测定法利用靶向关键毒力因子的单克隆抗体,多糖(PS)胶囊。GXMELISA是用于诊断隐球菌感染的领域中最常用的检测方法之一。PS含量的量化,和确定抗体的结合特异性。在这里,我们提出了我们小组使用的GXMELISA的三个变体-间接,捕获,和竞争ELISA。我们还提供了一些历史,透视,以及关于这些方法的注释,我们希望能帮助读者选择,并实施,他们研究的最佳检测方法.虽然它长期以来被称为GXMELISA,我们还建议进行名称更新,以更好地反映我们对该测定靶向多糖抗原的最新理解。隐球菌PSELISA是对这组方法及其测量的抗原的更准确描述。最后,我们讨论了该方法的局限性,并提出了扩展ELISA检测抗原的未来计划。
    One of the standard assays for the fungal pathogen Cryptococcus neoformans is the glucuronoxylomannan (GXM) ELISA. This assay utilizes monoclonal antibodies targeted against the critical virulence factor, the polysaccharide (PS) capsule. GXM ELISA is one of the most used assays in the field used for diagnosis of cryptococcal infection, quantification of PS content, and determination of binding specificity for antibodies. Here we present three variations of the GXM ELISA used by our group-indirect, capture, and competition ELISAs. We have also provided some history, perspective, and notes on these methods, which we hope will help the reader choose, and implement, the best assay for their research.While it has long been referred to as the GXM ELISA, we also suggest a name update to better reflect our updated understanding of the polysaccharide antigens targeted by this assay. The Cryptococcal PS ELISA is a more accurate description of this set of methodologies and the antigens they measure. Finally, we discuss the limitations of this assay and put forth future plans for expanding the antigens assayed by ELISA.
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  • 文章类型: Preprint
    新生隐球菌是一种真菌病原体,可在免疫功能低下的个体中引起危及生命的脑部感染。与其他真菌病原体不同,它具有保护性多糖胶囊对其毒力至关重要。在感染期间,隐球菌细胞释放大量的细胞外多糖(exo-PS),其干扰宿主免疫应答。exo-PS和capsular-PS在隐球菌感染中至关重要,代表疾病诊断和疫苗开发策略的关键目标。然而,理解它们的结构因它们的多分散性而变得复杂,复杂性,对样品分离和处理的敏感性以及缺乏能够分离和分析它们同时保留其天然结构的方法。在这项研究中,我们首次使用小角度中子散射(SANS)和超小角度中子散射(USANS)来研究溶液中的真菌细胞悬浮液和细胞外多糖。我们的数据表明,溶液中的exo-PS表现出塌陷的链状行为和质量分形特性,这意味着在不同放大倍数下重复出现的重复模式或结构。多糖的局部结构表征为对应于3至4个重复单元的标度长度上的刚性杆。这项研究不仅揭示了对exo-PS和capsular-PS结构的见解,而且还证明了USANS在研究细胞尺寸变化以及未来中子散射研究中对比度变化的潜力。
    Cryptococcus neoformans is a fungal pathogen that can cause life-threatening brain infections in immunocompromised individuals. Unlike other fungal pathogens, it possesses a protective polysaccharide capsule that is crucial for its virulence. During infections, Cryptococcus cells release copious amounts of extracellular polysaccharides (exo-PS) that interfere with host immune responses. Both exo-PS and capsular-PS play pivotal roles in Cryptococcus infections and serve as essential targets for disease diagnosis and vaccine development strategies. However, understanding their structure is complicated by their polydispersity, complexity, sensitivity to sample isolation and processing, and scarcity of methods capable of isolating and analyzing them while preserving their native structure. In this study, we employ small-angle neutron scattering (SANS) and ultra-small angle neutron scattering (USANS) for the first time to investigate both fungal cell suspensions and extracellular polysaccharides in solution. Our data suggests that exo-PS in solution exhibits collapsed chain-like behavior and demonstrates mass fractal properties that indicate a relatively condensed pore structure in aqueous environments. This observation is also supported by scanning electron microscopy (SEM). The local structure of the polysaccharide is characterized as a rigid rod, with a length-scale corresponding to 3 to 4 repeating units. This research not only unveils insights into exo-PS and capsular-PS structures but also demonstrates the potential of USANS for studying changes in cell dimensions and the promise of contrast variation in future neutron scattering studies.
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  • 文章类型: Journal Article
    尚未鉴定出有助于诊断隐球菌性脑膜脑炎(CM)的宿主非T细胞标志物。在这项病例对照研究中,我们对最近诊断为CM的Kinh族HIV阴性和HIV阳性越南个体和对照者的抗体和B细胞谱进行了表征。该研究包括60名HIV阴性,没有已知的免疫受损状况和60名HIV阳性个体,每组30例,对照组30例。参与者按年龄匹配,性别,艾滋病毒血清状态,HIV阳性组的CD4计数。血浆免疫球蛋白(Ig)水平,包括IgG1、IgG2、IgM、还有IgA,隐球菌属。葡糖醛酸木甘露聚糖(GXM)-和海带多糖(支链${\\\rm{\\beta}}$-[1-3]-葡聚糖)-结合IgG,IgM,IgA水平,测定外周血B细胞亚群。Logistic回归,主成分,和调解分析进行评估抗体之间的关联,B细胞水平,和CM。结果显示,CM患者的GXM-IgG水平高于对照组,IgG1和IgG2水平低于对照组,无论艾滋病毒状况如何。在艾滋病毒阴性的个体中,IgG2介导CD19+CD27+CD43+CD5-(B-1b样)细胞与CM之间的反向关联。在艾滋病毒阳性者中,IgA水平较低,laminarin-IgA,CD19+CD27+IgM+IgA-(IgM+记忆B)细胞均与CM相关。在HIV阴性和HIV阳性CM病例中鉴定出的共有和不同的抗体和B细胞谱可能有助于鉴定CM风险或未怀疑的疾病的非T细胞标志物。特别是在HIV阴性个体中。
    与HIV阳性个体的隐球菌性脑膜炎(CM)不同,在HIV阴性个体中没有已知的风险生物标志物,诊断通常不会被怀疑和延迟.这项研究确定了非T细胞,包括抗体和B细胞CM相关谱,可以指导HIV阴性个体的隐球菌抗原检测。
    Host non-T cell markers to aid in the diagnosis of cryptococcal meningoencephalitis (CM) have not been identified. In this case-control study, we characterized antibody and B cell profiles in HIV-negative and HIV-positive Vietnamese individuals of the Kinh ethnicity recently diagnosed with CM and controls. The study included 60 HIV-negative with no known immunocompromising condition and 60 HIV-positive individuals, with 30 CM cases and 30 controls in each group. Participants were matched by age, sex, HIV serostatus, and CD4 count in the HIV-positive group. Plasma immunoglobulin (Ig) levels, including IgG1, IgG2, IgM, and IgA, Cryptococcus spp. glucuronoxylomannan (GXM)- and laminarin (branched ${\\rm{\\beta }}$-[1-3]-glucan)-binding IgG, IgM, IgA levels, and peripheral blood B cell subsets were measured. Logistic regression, principal component, and mediation analyses were conducted to assess associations between antibody, B cell levels, and CM. The results showed that GXM-IgG levels were higher and IgG1 and IgG2 were lower in CM cases than controls, regardless of HIV status. In HIV-negative individuals, IgG2 mediated an inverse association between CD19+CD27+CD43+CD5- (B-1b-like) cells and CM. In HIV-positive individuals, lower levels of IgA, laminarin-IgA, and CD19+CD27+IgM+IgD- (IgM+ memory B) cells were each associated with CM. The shared and distinct antibody and B cell profiles identified in HIV-negative and HIV-positive CM cases may inform the identification of non-T-cell markers of CM risk or unsuspected disease, particularly in HIV-negative individuals.
    Unlike cryptococcal meningitis (CM) in HIV-positive individuals, there are no known biomarkers of risk in HIV-negative individuals and the diagnosis is often not suspected and delayed. This study identified non-T cells, including antibody and B cell CM-associated profiles that may guide cryptococcal antigen testing in HIV-negative individuals.
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  • 文章类型: Journal Article
    尚未在患有隐球菌病的器官移植受体(OTR)中研究抗体免疫。我们确定了OTR中的血清抗体水平:23例隐球菌病病例和21例对照。葡糖醛酸木甘露聚糖免疫球蛋白M(IgM)和海带多糖IgM均低于对照组,与隐球菌病状态呈负相关,并可能作为隐球菌病的标志。
    Antibody immunity has not been studied in organ transplant recipients (OTRs) with cryptococcosis. We determined serum antibody levels in OTRs: 23 cryptococcosis cases and 21 controls. Glucuronoxylomannan immunoglobulin M (IgM) and laminarin IgM were lower in cases than controls, were inversely associated with cryptococcosis status, and may hold promise as markers of cryptococcosis.
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  • 文章类型: Journal Article
    Cryptococcosis, a systemic mycosis that affects both the immunocompromised and immunocompetent, is caused by the inhalation of dehydrated yeasts or fungal spores of Cryptococcus gattii or Cryptococcus neoformans. The Cryptococcus spp. polysaccharide capsule is composed mainly of glucuronoxylomannan-GXM, its major virulence factor. The capsule thickness increases to more than 15 μm during titanization, favoring the pathogenesis of cryptococcosis. Previous studies demonstrated that cytotoxic T cells that had been bioengineered with GXM-targeting chimeric antigen receptor (GXMR-CAR) were able to recognize C. neoformans by promoting the control of titanization. GXMR-CAR, a second-generation CAR, contains a single-chain variable fragment that originates from a 18B7 clone: a human IgG4 hinge, followed by a human CD28 (transmembrane/cytoplasmic domains) and a CD3ς chain. In the current study, we redirected T cells to target distinct C. neoformans and C. gattii cell types by GXMR-CAR. Lentiviral particles carrying the GXMR-CAR sequence were used to transduce Jurkat cells, and these modified cells interacted with the GXM of the C. gattii R265 strain. Moreover, GXMR-CAR mediated the recognition of C. gattii and C. neoformans yeasts with both thin and thick polysaccharide capsules, and GXMR-CAR Jurkat cells interacted with titan cells sourced from both Cryptococcus spp. Thus, bioengineered cells using CAR can improve the treatment of cryptococcosis.
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    文章类型: Journal Article
    隐球菌是一种担子菌酵母,与HIV相关的发病率和死亡率相当高。一名26岁的恶病质HIV阳性男子,CD4计数为103个细胞/μl,伴有发烧,呼吸困难,和双侧下肢无力。脑部计算机断层扫描无法阐明神经功能缺损。他的血液被送去培养和血清隐球菌抗原检测,后者的测试为阴性。在入学的第四天,病人的病情急剧恶化。进行了腰椎穿刺,就像他的血清样本一样,脑脊液的隐球菌抗原也呈阴性。到这个时候,从入院血培养物中分离出新生隐球菌。实验室稀释血清和脑脊液标本以重新检测隐球菌抗原,最后,记录的抗原滴度≥1:2560.
    Cryptococcus is a basidiomycetous yeast responsible for considerable HIV-related morbidity and mortality. A cachectic 26-year-old HIV-positive man with a CD4 count of 103 cells/μl presented with fever, breathlessness, and bilateral lower limb weakness. A brain computed tomography scan could not elucidate the neurological deficit. His blood was sent for culture and serum cryptococcal antigen detection, with the latter testing as negative. By the fourth day of admission, the patient\'s condition had deteriorated drastically. A lumbar puncture was performed, and like his serum sample, the cerebrospinal fluid also tested negative for cryptococcal antigens. By this time, Cryptococcus neoformans was isolated from the admission blood culture. The laboratory diluted both the serum and cerebrospinal fluid specimens to retest for cryptococcal antigens, and finally, an antigen titer of ≥1:2560 was recorded.
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  • 文章类型: Journal Article
    Glucuronoxylomannan (GXM) participates in several immunoregulatory mechanisms, which makes it an important Cryptococcus virulence factor that is essential for the disease. Trichosporon asahii and Trichosporon mucoides share with Cryptococcus species the ability to produce GXM. To check whether other opportunistic species in the Trichosporonaceae family produce GXM-like polysaccharides, extracts from 28 strains were produced from solid cultures and their carbohydrate content evaluated by the sulfuric acid / phenol method. Moreover, extracts were assessed for cryptococcal GXM cross-reactivity through latex agglutination and lateral flow assay methods. Cryptococcus neoformans and Saccharomyces cerevisiae were used as positive and negative controls, respectively. In addition to T. asahii, the species Trichosporon inkin, Apiotrichum montevideense, Trichosporon japonicum, Trichosporon faecale, Trichosporon ovoides, Cutaneotrichosporon debeurmannianum, and Cutaneotrichosporon arboriformis are also producers of a polysaccharide immunologically similar to the GXM produced by human pathogenic Cryptococcus species. The carbohydrate concentration of the extracts presented a positive correlation with the GXM contents determined by titration of both methodologies. These results add several species to the list of fungal pathogens that produce glycans of the GXM type and bring information about the origin of potential false-positive results on immunological tests for diagnosis of cryptococcosis based on GXM detection.
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  • 文章类型: Journal Article
    The aim of this study was to develop a novel lateral flow immunochromatoghaphic strip test (ICT) for detecting cryptococcal polysaccharide capsular antigens using only a single specific monoclonal antibody, mAb 18B7. The mAb 18B7 is a well characterized antibody that specifically binds repeating epitopes displayed on the cryptococcal polysaccharide glucuronoxylomannan (GXM). We validated the immunoreactivities of mAb 18B7 against capsular antigens of different cryptococcal serotypes. The mAb 18B7 ICT was constructed as a sandwich ICT strip and the antibody serving in the mobile phase (colloidal gold conjugated mAb 18B7) to bind one of the GXM epitopes while the stationary phase antibody (immobilized mAb18B7 on test line) binding to other remaining unoccupied epitopes to generate a positive visual readout. The lower limit of detection of capsular antigens for each of the Cryptococcus serotypes tested was 0.63 ng/mL. No cross-reaction was found against a panel of antigens isolated from cultures of other pathogenic fungal, except the crude antigen of Trichosporon sp. with the lower limit of detection of 500 ng/mL (~800 times higher than that for cryptococcal GXM). The performance of the mAb 18B7 ICT strip was studied using cerebrospinal fluid (CSF) and serum and compared to commercial diagnostic kits (latex agglutination CALAS and CrAg IMMY). The sensitivity, specificity and accuracy of the mAb18B7 ICT with CSF from patients with confirmed cryptococcal meningitis were 92.86%, 100% and 96.23%, respectively. No false positives were observed with samples from non-cryptococcosis patients. With serum samples, the mAb 18B7 ICT gave a sensitivity, specificity and accuracy of 96.15%, 97.78% and 96.91%, respectively. Our results show that the mAb 18B7 based ICT was reliable, reproducible, and cost-effective as a point-of-care immunodiagnostic test for cryptococcosis. The mAb 18B7 ICT may be particularly useful in countries where commercial kits are not available or affordable.
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