Center for Theoretical and Evolutionary Immunology (CETI), Department of Biology, MSC03 2020, 1 University of New Mexico, Albuquerque, NM 87131, USA.
Int J Parasitol. 2010 Jun;40(7):819-31. doi: 10.1016/j.ijpara.2009.12.005. Epub 2010 Jan 18.
Successful colonization of a compatible snail host by a digenetic trematode miracidium initiates a complex, proliferative development program requiring weeks to reach culmination in the form of production of cercariae which, once started, may persist for the remainder of the life span of the infected snail. How are such proliferative and invasive parasites able to circumvent host defenses and establish chronic infections? Using a microarray designed to monitor the internal defense and stress-related responses of the freshwater snail Biomphalaria glabrata, we have undertaken a time course study to monitor snail responses following exposure to two different trematode species to which the snail is susceptible: the medically important Schistosoma mansoni, exemplifying sporocyst production in its larval development, or Echinostoma paraensei, representing an emphasis on rediae production in its larval development. We sampled eight time points (0.5, 1, 2, 4, 8, 16 and 32 days p.i.) that cover the period required for cercariae to be produced. Following exposure to S. mansoni, there was a preponderance of up-regulated over down-regulated array features through 2 days p.i. but by 4 days p.i. and thereafter, this pattern was strongly reversed. For E. paraensei, there was a preponderance of down-regulated array features over up-regulated features at even 0.5 days p.i., a pattern that persists throughout the course of infection except for 1 day p.i., when up-regulated array features slightly outnumbered down-regulated features. Examination of particular array features revealed several that were up-regulated by both parasites early in the course of infection and one, fibrinogen related protein 4 (FREP 4), that remained significantly elevated throughout the course of infection with either parasite, effectively serving as a marker of infection. Many defense-related transcripts were persistently down-regulated, including several fibrinogen-containing lectins and homologs of molecules best known from vertebrate phagocytic cells. Our results are consistent with earlier studies suggesting that both parasites are able to interfere with host defense responses, including a tendency for E. paraensei to do so more rapidly and strongly than S. mansoni. They further suggest mechanisms for how trematodes are able to establish the chronic infections necessary for their continued success.
成功地将一个合适的蜗牛宿主被双殖吸虫的尾蚴定植,启动了一个复杂的增殖发育程序,需要数周时间才能达到产生尾蚴的高潮,而一旦开始,这种尾蚴可能会在受感染蜗牛的剩余寿命内持续存在。这些增殖性和侵袭性寄生虫是如何规避宿主防御并建立慢性感染的?我们使用一种微阵列来监测淡水蜗牛 B. glabrata 的内部防御和应激相关反应,开展了一项时间进程研究,以监测蜗牛在暴露于两种易感染蜗牛的不同吸虫后的反应:具有代表性的医学重要性曼氏血吸虫,其幼虫发育过程中会产生孢囊;或者代表其幼虫发育过程中更强调雷蚴的 E. paraensei。我们在 8 个时间点(感染后 0.5、1、2、4、8、16 和 32 天)取样,这些时间点涵盖了产生尾蚴所需的时间。暴露于 S. mansoni 后,在感染后 2 天内,上调的微阵列特征明显多于下调的微阵列特征,但在感染后 4 天及以后,这种模式被强烈逆转。对于 E. paraensei,即使在感染后 0.5 天,下调的微阵列特征也明显多于上调的微阵列特征,这种模式在整个感染过程中持续存在,除了感染后 1 天,当时上调的微阵列特征略多于下调的微阵列特征。对特定微阵列特征的检查显示,有几个特征在感染早期被两种寄生虫上调,而一个纤维蛋白原相关蛋白 4(FREP 4)在感染过程中一直显著升高,有效地成为感染的标志物。许多防御相关的转录物持续下调,包括几种含有纤维蛋白原的凝集素和来自脊椎动物吞噬细胞的分子的同源物。我们的结果与早期研究一致,表明两种寄生虫都能够干扰宿主防御反应,E. paraensei 比 S. mansoni 更快、更强地干扰宿主防御反应。它们进一步提出了吸虫如何建立慢性感染的机制,这是它们持续成功所必需的。
