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体外培养的血吸虫未能产卵:寄生虫如何满足其对宿主来源的细胞因子(如 TGF-β)的需求?

Failure of in vitro-cultured schistosomes to produce eggs: how does the parasite meet its needs for host-derived cytokines such as TGF-β?

机构信息

School of Life Sciences, University of Nottingham, University Park, Nottingham NG7 2RD, UK.

Modha Biomedical Ltd, 9B St Cuthberts Avenue, Great Glen, Leicester LE8 9EJ, UK.

出版信息

Int J Parasitol. 2019 Sep;49(10):747-757. doi: 10.1016/j.ijpara.2019.05.004. Epub 2019 Jul 23.

Abstract

When adult schistosome worm pairs are transferred from experimental hosts to in vitro culture they cease producing viable eggs within a few days. Female worms in unisexual infections fail to mature, and when mature adult females are separated from male partners they regress sexually. Worms cultured from the larval stage are also permanently reproductively defective. The cytokine transforming growth factor beta derived from the mammalian host is considered important in stimulating schistosome female worm maturation and maintenance of fecundity. The means by which schistosomes acquire TGF-β have not been elucidated, but direct uptake in vivo seems unlikely as the concentration of free, biologically active cytokine in host blood is very low. Here we review the complexities of schistosome development and male-female interactions, and we speculate about two possibilities on how worms obtain the TGF-β they are assumed to need: (i) worms may have mechanisms to free active cytokine from the latency-inducing complex of proteins in which it is associated, and/or (ii) they may obtain the cytokine from alpha 2-macroglobulin, a blood-borne protease inhibitor to which TGF-β can bind. These ideas are experimentally testable.

摘要

当成年血吸虫虫对从实验宿主转移到体外培养,它们在几天内停止产生有活力的卵。在单性感染中,雌性虫无法成熟,而当成熟的雌性虫与雄性伴侣分离时,它们会在性方面退化。从幼虫期培养的虫也是永久性的生殖缺陷。来源于哺乳动物宿主的细胞因子转化生长因子β被认为在刺激血吸虫雌性虫成熟和保持生育能力方面很重要。血吸虫获得 TGF-β 的途径尚未阐明,但体内直接摄取似乎不太可能,因为宿主血液中游离的、具有生物活性的细胞因子浓度非常低。在这里,我们回顾了血吸虫发育和雌雄相互作用的复杂性,并推测了虫可能获得它们所需的 TGF-β 的两种可能性:(i)虫可能有机制将活性细胞因子从与其相关的潜伏期诱导蛋白复合物中释放出来,和/或(ii)它们可能从α 2-巨球蛋白中获得细胞因子,α 2-巨球蛋白是一种血液来源的蛋白酶抑制剂,TGF-β可以与之结合。这些想法是可以通过实验验证的。

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