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黄粉虫 HMGB1 样背侧开关蛋白 1 作为损伤相关分子模式起作用。

HMGB1-like dorsal switch protein 1 of the mealworm, Tenebrio molitor, acts as a damage-associated molecular pattern.

机构信息

Department of Plant Medicals, College of Life Sciences, Andong National University, Andong, Korea.

出版信息

Arch Insect Biochem Physiol. 2021 Jul;107(3):e21795. doi: 10.1002/arch.21795. Epub 2021 May 11.

Abstract

High-mobility group box 1 (HMGB1) is a nuclear protein highly conserved in eukaryotes and ubiquitously expressed to regulate transcription and chromatin remodeling. Dorsal switch protein 1 (DSP1) is its insect homolog. A lepidopteran DSP1 acts as a damage-associated molecular pattern (DAMP) in response to immune challenge. The objective of this study was to determine the role of DAMP in the mealworm beetle, Tenebrio molitor, a coleopteran insect. DSP1 of T. molitor (Tm-DSP1) encodes 536 amino acids and shares sequence similarities with Homo sapiens HMGB1 (56.3%) and Spodoptera exigua DSP1 (59.2%). An antisera raised against S. exigua DSP1 was cross-reactive to Tm-DSP1. Like other insect DSPs, Tm-DSP1 has a relatively long N-terminal extension in addition to two conserved HMG box domains. It was expressed in all developmental stages of T. molitor and different larval tissues. Upon immune challenge, its expression level was upregulated. Its RNA interference (RNAi) treatment resulted in a significant reduction in immune responses measured by hemocyte nodule formation against bacterial infection. In addition, the induction of some antimicrobial peptide genes to the immune challenge was suppressed by its RNAi treatment. Interestingly, phospholipase A associated with eicosanoid biosynthesis was significantly suppressed in its catalytic activity by the RNAi treatment specific to Tm-DSP1 expression. Without any pathogen infection, injection of a lepidopteran DSP1 induced both cellular and humoral immune responses. These results suggest that Tm-DSP1 in T. molitor can act as a DAMP molecule and mediate immune responses upon immune challenge.

摘要

高迁移率族蛋白 B1(HMGB1)是真核生物中高度保守的核蛋白,广泛表达以调节转录和染色质重塑。脊椎动物开关蛋白 1(DSP1)是其昆虫同源物。鳞翅目昆虫的 DSP1 作为一种损伤相关分子模式(DAMP),对免疫挑战作出反应。本研究的目的是确定 DAMPs 在鞘翅目昆虫黄粉虫(Tenebrio molitor)中的作用。黄粉虫的 DSP1(Tm-DSP1)编码 536 个氨基酸,与人类 HMGB1(56.3%)和斜纹夜蛾 DSP1(59.2%)具有序列相似性。针对斜纹夜蛾 DSP1 制备的抗血清与 Tm-DSP1 发生交叉反应。与其他昆虫的 DSP 一样,Tm-DSP1 除了两个保守的 HMG 盒结构域外,还有一个相对较长的 N 端延伸。它在黄粉虫的所有发育阶段和不同的幼虫组织中都有表达。在免疫挑战下,其表达水平上调。其 RNA 干扰(RNAi)处理导致针对细菌感染的血细胞结节形成的免疫反应显著降低。此外,其 RNAi 处理抑制了一些抗菌肽基因对免疫挑战的诱导。有趣的是,其 RNAi 处理特异性地抑制了与类二十烷酸生物合成相关的磷脂酶 A 的催化活性。在没有任何病原体感染的情况下,注射鳞翅目动物的 DSP1 会诱导细胞和体液免疫反应。这些结果表明,黄粉虫的 Tm-DSP1 可以作为 DAMPs 分子,在免疫挑战时介导免疫反应。

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