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N-连接表面糖基生物合成、组成、抑制及刺胞动物-甲藻共生关系中的功能。

N-Linked Surface Glycan Biosynthesis, Composition, Inhibition, and Function in Cnidarian-Dinoflagellate Symbiosis.

机构信息

Department of Integrative Biology, Oregon State University, Corvallis, OR, USA.

Department of Entomology, Cornell University, Ithaca, NY, USA.

出版信息

Microb Ecol. 2020 Jul;80(1):223-236. doi: 10.1007/s00248-020-01487-9. Epub 2020 Jan 25.

Abstract

The success of symbioses between cnidarian hosts (e.g., corals and sea anemones) and micro-algal symbionts hinges on the molecular interactions that govern the establishment and maintenance of intracellular mutualisms. As a fundamental component of innate immunity, glycan-lectin interactions impact the onset of marine endosymbioses, but our understanding of the effects of cell surface glycome composition on symbiosis establishment remains limited. In this study, we examined the canonical N-glycan biosynthesis pathway in the genome of the dinoflagellate symbiont Breviolum minutum (family Symbiodiniaceae) and found it to be conserved with the exception of the transferase GlcNAc-TII (MGAT2). Using coupled liquid chromatography-mass spectrometry (LC-MS/MS), we characterized the cell surface N-glycan content of B. minutum, providing the first insight into the molecular composition of surface glycans in dinoflagellates. We then used the biosynthesis inhibitors kifunensine and swainsonine to alter the glycan composition of B. minutum. Successful high-mannose enrichment via kifunensine treatment resulted in a significant decrease in colonization of the model sea anemone Aiptasia (Exaiptasia pallida) by B. minutum. Hybrid glycan enrichment via swainsonine treatment, however, could not be confirmed and did not impact colonization. We conclude that functional Golgi processing of N-glycans is critical for maintaining appropriate cell surface glycan composition and for ensuring colonization success by B. minutum.

摘要

共生体(例如珊瑚和海葵)与微藻共生体之间共生的成功取决于控制细胞内共生建立和维持的分子相互作用。作为先天免疫的基本组成部分,糖 - 凝集素相互作用影响海洋共生体的发生,但我们对细胞表面聚糖组成对共生体建立的影响的理解仍然有限。在这项研究中,我们检查了甲藻共生体 Breviolum minutum(Symbiodiniaceae 科)基因组中的典型 N-聚糖生物合成途径,发现除了转移酶 GlcNAc-TII(MGAT2)外,该途径是保守的。使用耦合液相色谱 - 质谱(LC-MS/MS),我们表征了 B. minutum 的细胞表面 N-聚糖含量,首次深入了解甲藻表面糖的分子组成。然后,我们使用生物合成抑制剂 Kifunensine 和 Swainsonine 来改变 B. minutum 的聚糖组成。通过 Kifunensine 处理成功进行高甘露糖富集导致模型海葵 Aiptasia(Exaiptasia pallida)被 B. minutum 定植的显著减少。然而,通过 Swainsonine 处理进行杂交聚糖富集不能得到证实,也不会影响定植。我们得出的结论是,N-聚糖的功能性高尔基体加工对于维持适当的细胞表面聚糖组成以及确保 B. minutum 的定植成功至关重要。

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