Alberdi Pilar, Mansfield Karen L, Manzano-Román Raúl, Cook Charlotte, Ayllón Nieves, Villar Margarita, Johnson Nicholas, Fooks Anthony R, de la Fuente José
SaBio, Instituto de Investigación en Recursos Cinegéticos IREC-Consejo Superior de Investigaciones Científicas- Universidad de Castilla-La Mancha-Junta de Comunidades de Castilla-La Mancha Ciudad Real, Spain.
Animal and Plant Health Agency New Haw, Surrey, UK.
Front Cell Infect Microbiol. 2016 Feb 10;6:20. doi: 10.3389/fcimb.2016.00020. eCollection 2016.
Anaplasma phagocytophilum are transmitted by Ixodes spp. ticks and have become one of the most common and relevant tick-borne pathogens due to their impact on human and animal health. Recent results have increased our understanding of the molecular interactions between Ixodes scapularis and A. phagocytophilum through the demonstration of tissue-specific molecular pathways that ensure pathogen infection, development and transmission by ticks. However, little is known about the Ixodes ricinus genes and proteins involved in the response to A. phagocytophilum infection. The tick species I. scapularis and I. ricinus are evolutionarily closely related and therefore similar responses are expected in A. phagocytophilum-infected cells. However, differences may exist between I. scapularis ISE6 and I. ricinus IRE/CTVM20 tick cells associated with tissue-specific signatures of these cell lines. To address this hypothesis, the transcriptional response to A. phagocytophilum infection was characterized by RNA sequencing and compared between I. scapularis ISE6 and I. ricinus IRE/CTVM20 tick cell lines. The transcriptional response to infection of I. scapularis ISE6 cells resembled that of tick hemocytes while the response in I. ricinus IRE/CTVM20 cells was more closely related to that reported previously in infected tick midguts. The inhibition of cell apoptosis by A. phagocytophilum appears to be a key adaptation mechanism to facilitate infection of both vertebrate and tick cells and was used to investigate further the tissue-specific response of tick cell lines to pathogen infection. The results supported a role for the intrinsic pathway in the inhibition of cell apoptosis by A. phagocytophilum infection of I. scapularis ISE6 cells. In contrast, the results in I. ricinus IRE/CTVM20 cells were similar to those obtained in tick midguts and suggested a role for the JAK/STAT pathway in the inhibition of apoptosis in tick cells infected with A. phagocytophilum. Nevertheless, tick cell lines were derived from embryonated eggs and may contain various cell populations with different morphology and behavior that could affect transcriptional response to infection. These results suggested tissue-specific signatures in I. scapularis ISE6 and I. ricinus IRE/CTVM20 tick cell line response to A. phagocytophilum infection that support their use as models for the study of tick-pathogen interactions.
嗜吞噬细胞无形体通过硬蜱属蜱虫传播,由于其对人类和动物健康的影响,已成为最常见且重要的蜱传病原体之一。最近的研究结果通过展示确保病原体感染、发育和由蜱虫传播的组织特异性分子途径,增进了我们对肩突硬蜱与嗜吞噬细胞无形体之间分子相互作用的理解。然而,对于蓖麻硬蜱中参与对嗜吞噬细胞无形体感染反应的基因和蛋白质知之甚少。肩突硬蜱和蓖麻硬蜱在进化上密切相关,因此预计在感染嗜吞噬细胞无形体的细胞中会有相似的反应。然而,肩突硬蜱ISE6细胞系和蓖麻硬蜱IRE/CTVM20细胞系之间可能存在差异,这与这些细胞系的组织特异性特征有关。为了验证这一假设,通过RNA测序对嗜吞噬细胞无形体感染的转录反应进行了表征,并在肩突硬蜱ISE6细胞系和蓖麻硬蜱IRE/CTVM20细胞系之间进行了比较。肩突硬蜱ISE6细胞对感染的转录反应类似于蜱血细胞,而蓖麻硬蜱IRE/CTVM20细胞中的反应与先前报道的感染蜱中肠的反应更为密切相关。嗜吞噬细胞无形体对细胞凋亡的抑制似乎是促进其感染脊椎动物细胞和蜱细胞的关键适应机制,并被用于进一步研究蜱细胞系对病原体感染的组织特异性反应。结果支持了内源性途径在嗜吞噬细胞无形体感染肩突硬蜱ISE6细胞时抑制细胞凋亡中的作用。相比之下,蓖麻硬蜱IRE/CTVM20细胞中的结果与在蜱中肠中获得的结果相似,表明JAK/STAT途径在抑制感染嗜吞噬细胞无形体的蜱细胞凋亡中起作用。尽管如此,蜱细胞系来源于胚胎卵,可能包含具有不同形态和行为的各种细胞群体,这可能会影响对感染的转录反应。这些结果表明,肩突硬蜱ISE6细胞系和蓖麻硬蜱IRE/CTVM20细胞系对嗜吞噬细胞无形体感染的反应具有组织特异性特征,支持它们作为蜱-病原体相互作用研究模型的应用。
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