Structure–activity relationship of contractile effects induced by helicokinins in the isolated gut of the lepidopteran caterpillar Spodoptera frugiperda

The diuretic helicokinins YFSPWG-amide (Hez KI), VRFSPWG-amide (Hez KII) and KVKFSAWG-amide (Hez KIII) are potent contractants of the isolated gut of the caterpillar Spodoptera frugiperda at doses ranging from 0.1 to 10 nM. In comparison, the pentapeptide FSPWG-amide was a full agonist with greatly...

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Bibliographic Details
Published in:Journal of insect physiology 2002, Vol.48 (1), p.75-82
Main Authors: Howarth, C.J, Prince, R.I, Dyker, H, Lösel, P.M, Seinsche, A, Osborne, R.H
Format: Article
Language:English
Subjects:
Gut bioassay
Helicokinins
Lepidoptera
Noctuidae
Spodoptera frugiperda
Structure–activity relationship
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Summary:The diuretic helicokinins YFSPWG-amide (Hez KI), VRFSPWG-amide (Hez KII) and KVKFSAWG-amide (Hez KIII) are potent contractants of the isolated gut of the caterpillar Spodoptera frugiperda at doses ranging from 0.1 to 10 nM. In comparison, the pentapeptide FSPWG-amide was a full agonist with greatly reduced potency while SPWG-amide and PWG-amide were weak partial agonists. Substitution of individual amino acids in Hez KI with alanine revealed that replacement of the [phenylalanine 2] residue caused a large fall in potency while replacement of [tryptophan 5] residue caused complete loss of myogenic activity. The striking fall in potency of YASPWG-amide and the lack of activity of YFSPAG-amide confirm the requirement for aromatic groups in positions 2 and 3 of the core pentapeptide as well as supporting the ideas that the active core of these peptides adopts a β-turn when interacting with receptors, bringing together the [Phe] and [Trp] residues that are critical for activity. Neither the pentapeptide proctolin nor the potent mammalian gut contractant Substance P were able to cause contraction when applied to caterpillar gut tissue. Incubation of isolated gut tissue in the phosphodiesterase inhibitor theophylline (10–100 μM) caused significant potentiation of the response to applied Hez KI. Conversely, in the presence of the L-type Ca 2+ channel blocker verapamil (10 μM–1 mM) or Co 2+ (1–50 mM) the contractile effects of Hez KI were attentuated significantly. These data suggest that the gut of S. frugiperda contains G-protein-linked kinin receptors that utilise cyclic AMP as their second messenger system and cause contraction by promoting the entry of extracellular Ca 2+.
ISSN:0022-1910
1879-1611
DOI:10.1016/S0022-1910(01)00147-0