Molecular cloning and functional characterization of the diapause hormone receptor in the corn earworm Helicoverpa zea

被引:33
作者
Jiang, Hongbo [1 ]
Wei, Zhaojun [1 ]
Nachman, Ronald J. [2 ]
Park, Yoonseong [1 ]
机构
[1] Kansas State Univ, Dept Entomol, Manhattan, KS 66506 USA
[2] USDA, Southern Plains Agr Res Ctr, Areawide Pest Management Res, College Stn, TX 77845 USA
关键词
GPCR; Neuropeptide; Insect; Peptidomimetic; BIOSYNTHESIS-ACTIVATING NEUROPEPTIDE; PROTEIN-COUPLED RECEPTORS; ORIENTAL TOBACCO BUDWORM; HELIOTHIS-VIRESCENS; PUPAL DIAPAUSE; PK/PBAN ANALOG; IDENTIFICATION; PEPTIDES; EXPRESSION; FAMILY;
D O I
10.1016/j.peptides.2013.11.005
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The diapause hormone (DH) in the heliothine moth has shown its activity in termination of pupal diapause, while the orthology in the silkworm is known to induce embryonic diapause. In the current study, we cloned the diapause hormone receptor from the corn earworm Helicoverpa zea (HzDHr) and tested its ligand specificities in a heterologous reporter system. HzDHr was expressed in Chinese Hamster Ovary (CHO) cells, which were co-transfected with the aequorin reporter, and was used to measure the ligand activities. A total of 68 chemicals, including natural DH analogs and structurally similar peptide mimetics, were tested for agonistic and antagonistic activities. Several peptide mimetics with a 2-amino7-bromofluorene-succinoyl (2Abf-Suc) N-terminal modification showed strong agonistic activities; these mimetics included 2Abf-Suc-F[dA]PRLamide, 2Abf-Suc-F[dR]PRLamide, 2Abf-Suc-FKPRLamide and 2Abf-Suc-FGPRLamide. Antagonistic activity was found in the ecdysis triggering hormone in Drosophila melanogaster (FFLKITKNVPRLamide). Interestingly, HzDHr does not discriminate between DH (WFGPRLamide C-terminal motif) and another closely related endogenous peptide, pyrokinin 1 (FXPRXamide; a C-terminal motif that is separate from WFGPRLamide). We provide large-scale in vitro data that serve as a reference for the development of agonists and antagonists to disrupt the DH signaling pathway. (c) 2013 Elsevier Inc. All rights reserved.
引用
收藏
页码:243 / 249
页数:7
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