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来源于血凝素-2 的血红素结合肽对牙龈卟啉单胞菌感染的免疫保护作用。

Immunoprotective effects of a hemin-binding peptide derived from hemagglutinin-2 against infection with Porphyromonas gingivalis.

机构信息

Beijing Institute for Dental Research, Beijing Stomatological Hospital and School of Stomatology, Capital Medical University, Beijing, China.

出版信息

Mol Oral Microbiol. 2018 Feb;33(1):81-88. doi: 10.1111/omi.12202. Epub 2017 Nov 9.

Abstract

The principal etiologic agent in periodontal disease, Porphyromonas gingivalis, generates cysteine proteases that bind heme with domains such as hemagglutinin-2 (HA2). High-affinity HA2-hemin binding supplies the porphyrin and ferric iron needed for growth and virulence. The DHYAVMISK peptide, recently identified at the hemin-binding site of HA2, inhibits hemin binding. We now evaluate the protective effect of vaccination with DGFPGDHYAVMISK (termed DK) against P. gingivalis using a rat infection model. Rats immunized with DK generated anti-peptide serum IgGs and salivary sIgAs (as measured by ELISA). In a subcutaneous abscess model, the protective effect of immunization was then investigated by measuring abscess size following subcutaneous injection with P. gingivalis. In an oral infection model, a ligature inoculated with P. gingivalis was used to induce periodontitis. The degree of bone erosion, ordinarily provoked by infection, was then evaluated by micro-computed tomography. We found that anti-peptide antibody titers of serum IgGs and salivary sIgAs for rats immunized with DK and adjuvant were significantly higher than for sham-immunized rats (injected with adjuvant/PBS alone; P < .05). In the subcutaneous abscess model, the DK + adjuvant-vaccinated rats recovered faster than sham-vaccinated animals, with their abscess sizes significantly smaller (P < .05). Further, in the experimental periodontitis model, bone loss at the molar palatal side for DK + adjuvant-vaccinated rats was significantly lower than for sham-vaccinated animals (P < .05). Collectively, these data demonstrate the potential of (DK) peptide immunization in terms of eliciting an immunoprotective effect against infection with P. gingivalis.

摘要

牙周病的主要病原体牙龈卟啉单胞菌产生半胱氨酸蛋白酶,这些蛋白酶与血凝素-2(HA2)等结构域结合血红素。高亲和力的 HA2-血红素结合提供了卟啉和铁,这是生长和毒力所必需的。最近在 HA2 的血红素结合位点鉴定出的 DHYAVMISK 肽抑制血红素结合。我们现在使用大鼠感染模型评估用 DGFPGDHYAVMISK(称为 DK)接种疫苗对牙龈卟啉单胞菌的保护作用。用 DK 免疫的大鼠产生抗肽血清 IgG 和唾液 sIgA(通过 ELISA 测量)。在皮下脓肿模型中,通过测量皮下注射牙龈卟啉单胞菌后脓肿的大小来研究免疫的保护作用。在口腔感染模型中,用结扎线接种牙龈卟啉单胞菌来诱导牙周炎。然后通过微计算机断层扫描评估由感染引起的通常的骨侵蚀程度。我们发现,用 DK 和佐剂免疫的大鼠的血清 IgG 和唾液 sIgA 的抗肽抗体滴度明显高于假免疫大鼠(单独用佐剂/ PBS 注射;P<.05)。在皮下脓肿模型中,DK+佐剂接种的大鼠比假疫苗接种的动物恢复得更快,其脓肿尺寸明显更小(P<.05)。此外,在实验性牙周炎模型中,DK+佐剂接种的大鼠的磨牙腭侧骨丢失明显低于假疫苗接种的动物(P<.05)。总的来说,这些数据表明(DK)肽免疫在引发针对牙龈卟啉单胞菌感染的免疫保护作用方面具有潜力。

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