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Restoration of Cyclo-Gly-Pro-induced salivary hyposecretion and submandibular composition by naloxone in mice.

Igor Santana MeloNávylla Candeia-MedeirosJamylle Nunes Souza FerroPolliane Maria Cavalcante-AraújoTales Lyra OliveiraCassio Eráclito Alves SantosLeia Cardoso-SousaEmilia Maria Gomes AguiarStephanie Wutke OliveiraOlagide Wagner CastroRenata Pereira Alves-BalvediLuciano Pereira RodriguesJandir M HickmannDouglas Alexsander AlvesIgor Andrade SantosAna Carolina Gomes JardimWalter Luiz SiqueiraAngelo Ricardo Fávaro PipiLuiz Ricardo GoulartEmiliano de Oliveira BarretoRobinson Sabino Silva
Published in: PloS one (2020)
Cyclo-Gly-Pro (CGP) attenuates nociception, however its effects on salivary glands remain unclear. In this study, we investigated the acute effects of CGP on salivary flow and composition, and on the submandibular gland composition, compared with morphine. Besides, we characterized the effects of naloxone (a non-selective opioid receptor antagonist) on CGP- and morphine-induced salivary and glandular alterations in mice. After that, in silico analyses were performed to predict the interaction between CGP and opioid receptors. Morphine and CGP significantly reduced salivary flow and total protein concentration of saliva and naloxone restored them to the physiological levels. Morphine and CGP also reduced several infrared vibrational modes (Amide I, 1687-1594cm-1; Amide II, 1594-1494cm-1; CH2/CH3, 1488-1433cm-1; C = O, 1432-1365cm-1; PO2 asymmetric, 1290-1185cm-1; PO2 symmetric, 1135-999cm-1) and naloxone reverted these alterations. The in silico docking analysis demonstrated the interaction of polar contacts between the CGP and opioid receptor Cys219 residue. Altogether, we showed that salivary hypofunction and glandular changes elicited by CGP may occur through opioid receptor suggesting that the blockage of opioid receptors in superior cervical and submandibular ganglions may be a possible strategy to restore salivary secretion while maintaining antinociceptive action due its effects on the central nervous system.
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