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磷脂酶 D (Ymt) 在蚤生物膜形成初始聚集步骤中的作用。

Role of the phospholipase D (Ymt) in the initial aggregation step of biofilm formation in the flea.

机构信息

Laboratory of Bacteriology, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Hamilton, Montana, USA.

Electron Microscopy Unit, Research Technologies Branch, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Hamilton, Montana, USA.

出版信息

mBio. 2024 Jun 12;15(6):e0012424. doi: 10.1128/mbio.00124-24. Epub 2024 May 9.

Abstract

UNLABELLED

Transmission of by fleas depends on the formation of condensed bacterial aggregates embedded within a gel-like matrix that localizes to the proventricular valve in the flea foregut and interferes with normal blood feeding. This is essentially a bacterial biofilm phenomenon, which at its end stage requires the production of a exopolysaccharide that bridges the bacteria together in a cohesive, dense biofilm that completely blocks the proventriculus. However, bacterial aggregates are evident within an hour after a flea ingests , and the bacterial exopolysaccharide is not required for this process. In this study, we characterized the biochemical composition of the initial aggregates and demonstrated that the yersinia murine toxin (Ymt), a phospholipase D, greatly enhances rapid aggregation following infected mouse blood meals. The matrix of the bacterial aggregates is complex, containing large amounts of protein and lipid (particularly cholesterol) derived from the flea's blood meal. A similar incidence of proventricular aggregation occurred after fleas ingested whole blood or serum containing , and intact, viable bacteria were not required. The initial aggregation of in the flea gut is likely due to a spontaneous physical process termed depletion aggregation that occurs commonly in environments with high concentrations of polymers or other macromolecules and particles such as bacteria. The initial aggregation sets up subsequent binding aggregation mediated by the bacterially produced exopolysaccharide and mature biofilm that results in proventricular blockage and efficient flea-borne transmission.

IMPORTANCE

, the bacterial agent of plague, is maintained in nature in mammal-flea-mammal transmission cycles. After a flea feeds on a mammal with septicemic plague, the bacteria rapidly coalesce in the flea's digestive tract to form dense aggregates enveloped in a viscous matrix that often localizes to the foregut. This represents the initial stage of biofilm development that potentiates transmission of when the flea later bites a new host. The rapid aggregation likely occurs via a depletion-aggregation mechanism, a non-canonical first step of bacterial biofilm development. We found that the biofilm matrix is largely composed of host blood proteins and lipids, particularly cholesterol, and that the enzymatic activity of a phospholipase D (Ymt) enhances the initial aggregation. transmitted by flea bite is likely associated with this host-derived matrix, which may initially shield the bacteria from recognition by the host's intradermal innate immune response.

摘要

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通过跳蚤传播取决于凝结细菌聚集体的形成,这些聚集体嵌入凝胶状基质中,定位于跳蚤前肠的前胃瓣,并干扰正常的血液摄取。这本质上是一种细菌生物膜现象,在其终末阶段需要产生一种 外多糖,将细菌桥接在一起形成一个有凝聚力的、密集的生物膜,完全阻塞前胃。然而,在跳蚤摄取 后一个小时内就可以看到细菌聚集体,而这个过程并不需要细菌外多糖。在这项研究中,我们描述了初始聚集体的生化组成,并证明了鼠疫耶尔森氏菌鼠毒素 (Ymt),一种 磷脂酶 D,大大增强了感染小鼠血液餐后的快速聚集。细菌聚集体的基质很复杂,包含大量来自跳蚤血液餐的蛋白质和脂质(特别是胆固醇)。当跳蚤摄取含有 的全血或血清时,也会发生类似的前胃聚集,而且不需要完整的、有活力的细菌。跳蚤肠道中 的初始聚集可能是由于一种自发的物理过程引起的,称为耗尽聚集,这种过程在聚合物或其他大分子和颗粒(如细菌)浓度高的环境中很常见。最初的聚集为随后由细菌产生的外多糖介导的结合聚集奠定了基础,并形成成熟的生物膜,导致前胃阻塞和有效的跳蚤传播。

重要性

鼠疫的细菌病原体在哺乳动物-跳蚤-哺乳动物传播循环中维持在自然界中。当跳蚤吸食患有败血性鼠疫的哺乳动物时,细菌会迅速在跳蚤的消化道中聚合并形成密集的聚集体,被粘性基质包裹,通常定位于前肠。这代表了生物膜发展的初始阶段,当跳蚤随后叮咬新宿主时,促进了 的传播。快速聚集可能通过耗尽聚集机制发生,这是细菌生物膜发展的非典型第一步。我们发现生物膜基质主要由宿主血液中的蛋白质和脂质组成,特别是胆固醇,而 磷脂酶 D (Ymt) 的酶活性增强了初始聚集。通过跳蚤叮咬传播的 可能与这种宿主衍生的基质有关,它可能最初使细菌免受宿主真皮固有免疫反应的识别。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a56/11237439/c9896f4b0f38/mbio.00124-24.f001.jpg

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