Journal article

Synthesis, conformation, and activity of human insulin-like peptide 5 (INSL5)

MA Hossain, RAD Bathgate, CK Kong, F Shabanpoor, S Zhang, LM Haugaard-Jönsson, KJ Rosengren, GW Tregear, JD Wade

Chembiochem | WILEY-BLACKWELL | Published : 2008

DOI: 10.1002/cbic.200800113

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Abstract

Insulin-like peptide 5 (INSL5) was first identified through searches of the expressed sequence tags (EST) databases. Primary sequence analysis showed it to be a prepropeptide that was predicted to be processed in vivo to yield a two-chain sequence (A and B) that contained the insulin-like disulfide cross-links. The high affinity interaction between INSL5 and the receptor RXFP4 (GPCR142) coupled with their apparent coevolution and partially overlapping tissue expression patterns strongly suggest that INSL5 is an endogenous ligand for RXFP4. Given that the primary function of the INSL5-RXFP4 pair remains unknown, an effective means of producing sufficient quantities of this peptide and its ana..

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University of Melbourne Researchers

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Keywords

34 Chemical Sciences
Chain Combination
Solid-Phase Synthesis
In-Vitro
Science & Technology
Rxfp4
Biochemistry & Molecular Biology
Biotechnology
Chemistry, Medicinal
Chemical-Synthesis
Peptides
Pharmacology & Pharmacy
Synthesis
Human Relaxin
3405 Organic Chemistry
Insulin-Like Peptides
Aspartimide Formation
Biological-Activity
Gene
Life Sciences & Biomedicine
Circular Dichroism
Difficult Sequences
Mouse Relaxin