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Cytoplasmic FKBPs are involved in molting and metamorphosis through regulating the nuclear localization of EcR

生物 蜕皮激素受体 蜕皮激素 细胞生物学 变形 内质网 细胞质 20-羟基蜕皮激素 信号转导 蜕皮 核受体 FKBP公司 基因 遗传学 转录因子 幼虫 植物
作者
Xian Zhang,Q. Wang,Qian Wu,Jun Gu,Li‐Hua Huang
出处
期刊:Insect Science [Wiley]
卷期号:31 (3): 759-772
标识
DOI:10.1111/1744-7917.13278
摘要

Abstract Molting and metamorphosis are important physiological processes in insects that are tightly controlled by ecdysone receptor (EcR) through the 20‐hydroxyecdysone (20E) signaling pathway. EcR is a steroid nuclear receptor (SR). Several FK506‐binding proteins (FKBPs) have been identified from the mammal SR complex, and are thought to be involved in the subcellular trafficking of SR. However, their roles in insects are poorly understood. To explore whether FKBPs are involved in insect molting or metamorphosis, we injected an FKBP inhibitor (FK506) into a lepidopteran insect, Spodoptera litura , and found that molting was inhibited in 61.11% of the larvae, and that the time for larvae to pupate was significantly extended. A total of 10 FKBP genes were identified from the genome of S. litura and were clustered into 2 distinct groups, according to their subcellular localization, with FKBP13 and FKBP14 belonging to the endoplasmic reticulum (ER) group and with the other members belonging to the cytoplasmic (Cy) group. All the CyFKBP s were significantly upregulated in the prepupal or pupal stages, with the opposite being observed for the ER group members. FK506 completely blocked the transfer of EcR to the nucleus under 20E induction, and significantly downregulated the transcriptional expression of many 20E signaling genes. A similar phenomenon was observed after RNA interference of 2 CyFKBP s ( FKBP45 and FKBP12b ), but not for FKBP13 . Taken together, our data indicate that the cytoplasmic FKBPs, especially FKBP45 and FKBP12b, mediate the nuclear localization of EcR, thereby regulating the 20E signaling and ultimately affecting molting and metamorphosis in insects.
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