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Inhibition by yeast killer toxin-like antibodies of oral Streptococci adhesion to tooth surfaces in an ex vivo model.

机译:在离体模型中酵母杀伤毒素样抗体抑制口腔链球菌粘附于牙齿表面。

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摘要

BACKGROUND: Monoclonal (KTmAb) and recombinant (KTscFv) anti-idiotypic antibodies, representing the internal image of a yeast killer toxin, proved to be microbicidal in vitro against important eukaryotic and prokaryotic pathogens such as Candida albicans, Pneumocystis carinii, Mycobacterium tuberculosis, Staphylococcus aureus, S. haemolyticus, Enterococcus faecalis, E. faecium, and Streptococcus pneumoniae, including multidrug-resistant strains. KTmAb and KTscFv exerted a strong therapeutic effect in well-established animal models of candidiasis and pneumocystosis. Streptococcus mutans is the most important etiologic agent of dental caries that might result from the metabolic end products of dental plaque. Effective strategies to reduce the disease potential of dental plaque have considered the possibility of using antibiotics or antibodies against oral streptococci in general and S. mutans in particular. In this study, the activity of KTmAb and KTscFv against S. mutans and the inhibition and reduction by KTmAb of dental colonization by S. mutans and other oral streptococci in an ex vivo model of human teeth were investigated. MATERIALS AND METHODS: KTscFv and KTmAb were used in a conventional colony forming unit (CFU) assay against a serotype C strain of S. mutans, and other oral streptococci (S. intermedius, S. mitis, S. oralis, S. salivarius). An ex vivo model of human teeth submerged in saliva was used to establish KTmAb potential of inhibiting or reducing the adhesion to dental surfaces by S. mutans and other oral streptococci. RESULTS: KTmAb and KTscFv kill in vitro S. mutans and other oral streptococci. KTmAb inhibit colonization of dental surfaces by S. mutans and oral streptococci in the ex vivo model. CONCLUSIONS: Killer antibodies with antibiotic activity or their engineered derivatives may have a potential in the prevention of dental caries in vivo.
机译:背景:代表酵母杀手毒素内部图像的单克隆(KTmAb)和重组(KTscFv)抗独特型抗体在体外对重要的真核和原核病原体(如白色念珠菌,卡氏肺孢子虫,结核分枝杆菌,葡萄球菌)具有杀菌作用金黄色葡萄球菌,溶血链球菌,粪肠球菌,粪肠球菌和肺炎链球菌,包括耐多药菌株。 KTmAb和KTscFv在完善的念珠菌病和肺囊虫病动物模型中发挥了强大的治疗作用。变形链球菌是龋齿最重要的病因,可能是由于牙菌斑的代谢终产物所致。减少牙菌斑潜在疾病的有效策略已考虑了使用一般针对口腔链球菌的抗生素或抗体,尤其是针对变形链球菌的抗体。在这项研究中,在人牙齿的离体模型中,研究了KTmAb和KTscFv对变形链球菌的活性以及KTmAb对变形链球菌和其他口腔链球菌的牙齿定植的抑制和减少。材料与方法:KTscFv和KTmAb用于常规的菌落形成单位(CFU)检测,以抵抗变形链球菌和其他口腔链球菌(间质链球菌,链球菌,口腔链球菌,唾液链球菌)的血清型C株。 。使用浸没在唾液中的人牙齿的离体模型来建立抑制或降低变形链球菌和其他口腔链球菌粘附于牙齿表面的KTmAb潜力。结果:KTmAb和KTscFv杀死体外变形链球菌和其他口服链球菌。在离体模型中,KTmAb抑制变形链球菌和口腔链球菌在牙齿表面的定殖。结论:具有抗生素活性的杀伤性抗体或其工程衍生物可能具有体内预防龋齿的潜力。

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