Lulu Wang, Yan Sun, Ruihao Zhang, Kehou Pan, Yuhang Li, Ruibing Wang, Lin Zhang, Chengxu Zhou, Jian Li, Yun Li, Baohua Zhu, Jichang Han
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Thus, it was overexpressed and knocked down, respectively. The frustule of the overexpress lines showed no obvious alteration in morphology compared to the wild type (WT), while the size, specific surface area (BET), pore volume, and pore diameter of the knockdown strains changed greatly. Particularly, the knockdown frustules achieved a more pronounced coagulation effect and in vivo hemostatic performance than the WT strains. Such observations suggested that silicalemma proteins are ideal genetic encoding targets for manipulating frustule morphology associated hemostatic properties. Furthermore, the Mantel test was adopted to identify the key morphologies associated with <i>C. cryptica</i> bleeding control. 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引用次数: 0
摘要
硅藻硅化细胞壁,又称硅藻胞壁,由于其止血效率高、生物相容性好、可利用性好等优点,作为一种杰出的生物纳米止血材料显示出巨大的潜力。由于截骨的结构特征决定了其止血性能,因此开发一种有效的方法来修饰截骨形态以进一步提高止血效率是非常有意义的。结果发现隐环菌(Cyclotella cryptica)的硅膜相关蛋白2 (Silicalemma Associated Protein 2,一种跨越硅膜的蛋白)编码基因CcSAP2是晶体形态发生的关键基因。因此,它分别被过度表达和敲低。与野生型(WT)相比,过表达菌株在形态上无明显变化,而过表达菌株的大小、比表面积(BET)、孔容和孔径变化较大。其中,敲低小体比WT菌株具有更明显的凝血效果和体内止血性能。这些观察结果表明,硅膜蛋白是理想的基因编码靶标,用于操纵与止血特性相关的血管形态。此外,采用Mantel试验鉴定与隐隐梭菌出血控制相关的关键形态学。最后,根据本文的研究结果和最新进展,讨论了折叶形态发生的机制。结论本研究探索了一种基于遗传形态学改变的提高截尾止血效率的新策略,为进一步了解截尾形态发生机制提供了新的思路。
Enhancement of hemostatic properties of Cyclotella cryptica frustule through genetic manipulation
Background
The silicified cell wall of diatoms, also known as frustule, shows huge potential as an outstanding bio-nanomaterial for hemostatic applications due to its high hemostatic efficiency, good biocompatibility, and ready availability. As the architectural features of the frustule determine its hemostatic performance, it is of great interest to develop an effective method to modify the frustule morphology into desired patterns to further improve hemostatic efficiency.
Results
In this study, the gene encoding Silicalemma Associated Protein 2 (a silicalemma-spanning protein) of Cyclotella cryptica (CcSAP2) was identified as a key gene in frustule morphogenesis. Thus, it was overexpressed and knocked down, respectively. The frustule of the overexpress lines showed no obvious alteration in morphology compared to the wild type (WT), while the size, specific surface area (BET), pore volume, and pore diameter of the knockdown strains changed greatly. Particularly, the knockdown frustules achieved a more pronounced coagulation effect and in vivo hemostatic performance than the WT strains. Such observations suggested that silicalemma proteins are ideal genetic encoding targets for manipulating frustule morphology associated hemostatic properties. Furthermore, the Mantel test was adopted to identify the key morphologies associated with C. cryptica bleeding control. Finally, based on our results and recent advances, the mechanism of frustule morphogenesis was discussed.
Conclusion
This study explores a new strategy for enhancing the hemostatic efficiency of the frustule based on genetic morphology modification and may provide insights into a better understanding of the frustule morphogenesis mechanism.
期刊介绍:
Biotechnology for Biofuels is an open access peer-reviewed journal featuring high-quality studies describing technological and operational advances in the production of biofuels, chemicals and other bioproducts. The journal emphasizes understanding and advancing the application of biotechnology and synergistic operations to improve plants and biological conversion systems for the biological production of these products from biomass, intermediates derived from biomass, or CO2, as well as upstream or downstream operations that are integral to biological conversion of biomass.
Biotechnology for Biofuels focuses on the following areas:
• Development of terrestrial plant feedstocks
• Development of algal feedstocks
• Biomass pretreatment, fractionation and extraction for biological conversion
• Enzyme engineering, production and analysis
• Bacterial genetics, physiology and metabolic engineering
• Fungal/yeast genetics, physiology and metabolic engineering
• Fermentation, biocatalytic conversion and reaction dynamics
• Biological production of chemicals and bioproducts from biomass
• Anaerobic digestion, biohydrogen and bioelectricity
• Bioprocess integration, techno-economic analysis, modelling and policy
• Life cycle assessment and environmental impact analysis