Structure-Based Functional Analysis of a Hormone Belonging to an Ecdysozoan Peptide Superfamily: Revelation of a Common Molecular Architecture and Residues Possibly for Receptor Interaction

Overview

Journal Int J Mol Sci

Publisher MDPI

Specialties Biochemistry
Chemistry
Molecular Biology

Date 2021 Oct 23

PMID 34681803

Citations 1

Authors

Yun-Ru Chen

Nai-Wan Hsiao

Yi-Zong Lee

Shiau-Shan Huang

Chih-Chun Chang

Jyuan-Ru Tsai

Hui-Chen Lin

Jean-Yves Toullec

Chi-Ying Lee

Ping-Chiang Lyu

Affiliations

Soon will be listed here.

Abstract

A neuropeptide (Sco-CHH-L), belonging to the crustacean hyperglycemic hormone (CHH) superfamily and preferentially expressed in the pericardial organs (POs) of the mud crab , was functionally and structurally studied. Its expression levels were significantly higher than the alternative splice form (Sco-CHH) in the POs, and increased significantly after the animals were subjected to a hypo-osmotic stress. Sco-CHH-L, but not Sco-CHH, significantly stimulated in vitro the Na, K-ATPase activity in the posterior (6th) gills. Furthermore, the solution structure of Sco-CHH-L was resolved using nuclear magnetic resonance spectroscopy, revealing that it has an -terminal tail, three α-helices (α2, Gly-Asn; α3, His-Gly; and α5, Glu-Arg), and a π-helix (π4, Cys-Tyr), and is structurally constrained by a pattern of disulfide bonds (Cys-Cys, Cys-Cys, and Cys-Cys), which is characteristic of the CHH superfamily-peptides. Sco-CHH-L is topologically most similar to the molt-inhibiting hormone from the Kuruma prawn with a backbone root-mean-square-deviation of 3.12 Å. Ten residues of Sco-CHH-L were chosen for alanine-substitution, and the resulting mutants were functionally tested using the gill Na, K-ATPase activity assay, showing that the functionally important residues (I2, F3, E45, D69, I71, and G73) are located at either end of the sequence, which are sterically close to each other and presumably constitute the receptor binding sites. Sco-CHH-L was compared with other members of the superfamily, revealing a folding pattern, which is suggested to be common for the crustacean members of the superfamily, with the properties of the residues constituting the presumed receptor binding sites being the major factors dictating the ligand-receptor binding specificity.

Citing Articles

analysis of crustacean hyperglycemic hormone family G protein-coupled receptor candidates.

Kozma M, Perez-Moreno J, Gandhi N, Hernandez Jeppesen L, Durica D, Ventura T Front Endocrinol (Lausanne). 2024; 14:1322800.

PMID: 38298185 PMC: 10828670. DOI: 10.3389/fendo.2023.1322800.

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