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抑制丝状化可用于治疗播散性念珠菌病。

Inhibition of filamentation can be used to treat disseminated candidiasis.

作者信息

Saville Stephen P, Lazzell Anna L, Bryant Alexander P, Fretzen Angelika, Monreal Alex, Solberg Erik O, Monteagudo Carlos, Lopez-Ribot Jose L, Milne G Todd

机构信息

Department of Biology and South Texas Center for Emerging Infectious Diseases, University of Texas at San Antonio, San Antonio, TX 78249, USA.

出版信息

Antimicrob Agents Chemother. 2006 Oct;50(10):3312-6. doi: 10.1128/AAC.00628-06.

Abstract

Candida albicans remains the leading causative agent of invasive fungal infection. Although the importance of filamentation in C. albicans pathogenesis has been extensively investigated, in vivo studies to date have been unable to dissect the role of this developmental process in the establishment of infection versus the development of active disease as characterized by damage to the host leading to mortality. To address this issue, we genetically engineered a C. albicans tet-NRG1 strain in which filamentation and virulence can be modulated both in vitro and in vivo simply by the presence or absence of doxycycline (DOX): this strain enabled us, in a prior study, to demonstrate that yeast-form cells were able to infect the deep organs but caused no disease unless filamentation (induced by the addition of DOX) was allowed to occur. In the present study, we examined whether inhibiting filamentation (by withdrawing the DOX) at 24 or 48 h postinfection could serve as an effective therapeutic intervention against candidiasis. The results obtained indicate that DOX removal led to an alteration in the morphology of the infecting fungal cells and a dramatic increase in survival, but as with conventional antifungal drug therapy regimens, mortality rates increased markedly the longer this intervention was delayed. These observations reinforce the importance of invasive filamentous growth in causing the damage to the host and the lethality associated with active disease and suggest this process could be fruitfully targeted for the development of new antifungal agents.

摘要

白色念珠菌仍然是侵袭性真菌感染的主要病原体。尽管已经广泛研究了白色念珠菌致病过程中菌丝形成的重要性,但迄今为止的体内研究仍无法剖析这一发育过程在感染建立过程中的作用,以及与以宿主损伤导致死亡为特征的活动性疾病发展之间的关系。为了解决这个问题,我们构建了一种白色念珠菌tet-NRG1菌株,在该菌株中,仅通过添加或不添加强力霉素(DOX),就可以在体外和体内调节菌丝形成和毒力:在之前的一项研究中,该菌株使我们能够证明酵母形态的细胞能够感染深部器官,但除非发生菌丝形成(通过添加DOX诱导),否则不会引发疾病。在本研究中,我们研究了在感染后24小时或48小时抑制菌丝形成(通过撤除DOX)是否可以作为治疗念珠菌病的有效干预措施。获得的结果表明,撤除DOX会导致感染真菌细胞的形态发生改变,并使存活率显著提高,但与传统抗真菌药物治疗方案一样,这种干预延迟的时间越长,死亡率就会显著增加。这些观察结果强化了侵袭性丝状生长在导致宿主损伤和与活动性疾病相关的致死率方面的重要性,并表明这一过程有望成为开发新型抗真菌药物的靶点。

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