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ame-miR-34 调节工蜂幼虫体重和对入侵的免疫反应。

ame-miR-34 Modulates the Larval Body Weight and Immune Response of Workers to Invasion.

机构信息

College of Animal Sciences (College of Bee Science), Fujian Agriculture and Forestry University, Fuzhou 350002, China.

Apitherapy Research Institute of Fujian Province, Fuzhou 350002, China.

出版信息

Int J Mol Sci. 2023 Jan 7;24(2):1214. doi: 10.3390/ijms24021214.

Abstract

MiRNAs are critical regulators of numerous physiological and pathological processes. Ascosphaera apis exclusively infects bee larvae and causes chalkbrood disease. However, the function and mechanism of miRNAs in the bee larval response to A. apis infection is poorly understood. Here, ame-miR-34, a previously predicted miRNA involved in the response of Apis mellifera larvae to A. apis invasion, was subjected to molecular validation, and overexpression and knockdown were then conducted to explore the regulatory functions of ame-miR-34 in larval body weight and immune response. Stem-loop RT-PCR and Sanger sequencing confirmed the authenticity of ame-miR-34 in the larval gut of A. mellifera. RT-qPCR results demonstrated that compared with that in the uninfected larval guts, the expression level of ame-miR-34 was significantly downregulated (p < 0.001) in the guts of A. apis-infected 4-, 5-, and 6-day-old larvae, indicative of the remarkable suppression of host ame-miR-34 due to A. apis infection. In comparison with the corresponding negative control (NC) groups, the expression level of ame-miR-34 in the larval guts in the mimic-miR-34 group was significantly upregulated (p < 0.001), while that in the inhibitor-miR-34 group was significantly downregulated (p < 0.01). Similarly, effective overexpression and knockdown of ame-miR-34 were achieved. In addition, the body weights of 5- and 6-day-old larvae were significantly increased compared with those in the mimic-NC group; the weights of 5-day-old larvae in the inhibitor-miR-34 group were significantly decreased in comparison with those in the inhibitor-NC group, while the weights of 4- and 6-day-old larvae in the inhibitor-miR-34 group were significantly increased, indicating the involvement of ame-miR-34 in modulating larval body weight. Furthermore, the expression levels of both hsp and abct in the guts of A. apis-infected 4-, 5-, and 6-day-old larvae were significantly upregulated after ame-miR-34 overexpression. In contrast, after ame-miR-34 knockdown, the expression levels of the aforementioned two key genes in the A. apis-infected 4-, 5-, and 6-day-old larval guts were significantly downregulated. Together, the results demonstrated that effective overexpression and knockdown of ame-miR-34 in both noninfected and A. apis-infected A. mellifera larval guts could be achieved by the feeding method, and ame-miR-34 exerted a regulatory function in the host immune response to A. apis invasion through positive regulation of the expression of hsp and abct. Our findings not only provide a valuable reference for the functional investigation of bee larval miRNAs but also reveal the regulatory role of ame-miR-34 in A. mellifera larval weight and immune response. Additionally, the results of this study may provide a promising molecular target for the treatment of chalkbrood disease.

摘要

miRNAs 是许多生理和病理过程的关键调节因子。粉孢子虫(Ascosphaera apis)专门感染蜜蜂幼虫并引起白垩病。然而,miRNAs 在蜜蜂幼虫对白垩病的反应中的功能和机制尚不清楚。在这里,ame-miR-34 是一种先前预测的与 Apis mellifera 幼虫对白垩病入侵反应有关的 miRNA,进行了分子验证,并进行了过表达和敲低实验,以探索 ame-miR-34 在幼虫体重和免疫反应中的调节功能。茎环 RT-PCR 和 Sanger 测序证实了 ame-miR-34 在 Apis mellifera 幼虫肠道中的真实性。RT-qPCR 结果表明,与未感染的幼虫肠道相比,ame-miR-34 在感染 4、5 和 6 日龄粉孢子虫的幼虫肠道中的表达水平显著下调(p<0.001),表明宿主 ame-miR-34 由于粉孢子虫感染而受到显著抑制。与相应的阴性对照(NC)组相比, mimic-miR-34 组幼虫肠道中 ame-miR-34 的表达水平显著上调(p<0.001),而 inhibitor-miR-34 组的表达水平显著下调(p<0.01)。同样,有效地实现了 ame-miR-34 的过表达和敲低。此外,与 mimic-NC 组相比,5 日龄和 6 日龄幼虫的体重显著增加;与 inhibitor-NC 组相比,5 日龄幼虫的体重显著降低,而 4 日龄和 6 日龄幼虫的体重显著增加,表明 ame-miR-34 参与调节幼虫体重。此外,ame-miR-34 过表达后,感染粉孢子虫的 4、5 和 6 日龄幼虫肠道中 hsp 和 abct 的表达水平显著上调。相反,ame-miR-34 敲低后,感染粉孢子虫的 4、5 和 6 日龄幼虫肠道中上述两个关键基因的表达水平显著下调。综上所述,通过喂食方法可以有效地实现非感染和感染粉孢子虫的 Apis mellifera 幼虫肠道中 ame-miR-34 的过表达和敲低,ame-miR-34 通过正调控 hsp 和 abct 的表达在宿主对白垩病的免疫反应中发挥调节作用。我们的研究结果不仅为蜜蜂幼虫 miRNA 的功能研究提供了有价值的参考,还揭示了 ame-miR-34 在 Apis mellifera 幼虫体重和免疫反应中的调节作用。此外,本研究结果可能为白垩病的治疗提供有前景的分子靶标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b12/9863880/f2e5ede959d9/ijms-24-01214-g001.jpg

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