首页> 外文期刊>Journal of Endodontics: Official Journal of American Association of Endodontists >Development of an ex vivo coculture system to model pulpal infection by streptococcus anginosus group bacteria
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Development of an ex vivo coculture system to model pulpal infection by streptococcus anginosus group bacteria

机译:开发体外共培养系统以模拟链球菌性心绞痛组细菌的牙髓感染

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Introduction: Streptococcus anginosus group (SAG) bacteria are opportunistic pathogens and a major cause of pulpal infection and subsequent abscess formation. Understanding of the processes involved in SAG oral infections has been limited by the lack of an appropriate model system. Methods: Cocultures of SAG bacteria and mammalian tooth slices were maintained using a combination of Dulbecco modified eagle medium and brain-heart infusion broth at 60 rpm, 37??C, 5% CO2 for 4, 8, or 24 hours before histologic examination or staining with acridine orange/ethidium bromide. Tooth slices were also incubated as described with SAG bacteria stained with fluorescein diacetate. Pulps were extirpated from infected and sterile cultured tooth slices, messenger RNA was extracted and converted to complementary DNA, and polymerase chain reaction were performed for genes encoding tumor necrosis factor ??, interleukin 1??, and interleukin-6. Results: SAG bacteria were able to adhere directly to the central region of the pulpal matrix in small foci that were associated with a localized matrix breakdown. Acridine orange-ethidium bromide staining and cell counts indicated a decrease in mammalian cell viability with increasing incubation times in the presence of SAG bacteria. The increased expression of tumor necrosis factor ?? and interleukin 1?? was detected in infected tooth slices. Conclusions: A novel ex vivo model system has been developed that allows coculture of SAG bacteria with a 3-dimensional organotypic tooth slice. The model allows observation of bacterial growth patterns and subsequent responses from host tissues. Therefore, it may be of future use in testing the efficacy of both antimicrobial and anti-inflammatory treatments for use in endodontic therapy. ? 2013 American Association of Endodontists.
机译:简介:链球菌性心绞痛(SAG)细菌是机会病原体,是牙髓感染和随后形成脓肿的主要原因。由于缺乏合适的模型系统,对SAG口腔感染涉及的过程的了解受到限制。方法:在组织学检查或组织学检查之前,使用Dulbecco改良的Eagle培养基和脑心浸液在60 rpm,37°C,5%CO2的条件下维持SAG细菌和哺乳动物牙齿切片的共培养4小时,8小时或24小时。用a啶橙/溴化乙锭染色。如所述,将牙齿切片与用荧光素二乙酸酯染色的SAG细菌一起温育。从感染和无菌培养的牙齿切片中去除牙髓,提取信使RNA并转化为互补DNA,并对编码肿瘤坏死因子β1,白介素1β和白介素6的基因进行聚合酶链反应。结果:SAG细菌能够直接粘附在与局部基质分解相关的小病灶的牙髓基质的中央区域。 SA啶橙-溴化乙锭染色和细胞计数表明,在存在SAG细菌的情况下,随着孵育时间的增加,哺乳动物细胞的活力降低。肿瘤坏死因子??的表达增加和白介素1 ??在感染的牙齿切片中检测到。结论:已经开发了一种新型的离体模型系统,该系统允许SAG细菌与3维器官型牙齿切片共培养。该模型允许观察细菌的生长方式以及宿主组织的后续反应。因此,它可能在将来测试用于牙髓治疗的抗微生物和抗炎治疗的功效。 ? 2013美国牙医学院会员协会。

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