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Proteomic Analysis of Heloderma horridum horridum Venom: Assessment to Its Transcriptome and Newfound Proteins.

Gisela J Lino-LópezEliel Ruiz-MayJosé M Elizalde-ContrerasJuana M Jiménez-VargasArmando Rodríguez-VázquezGabino González-CarrilloEsaú Bojórquez-VelázquezPatricia E García-VillalvazoManuel de J Bermúdez-GuzmánRocio Zatarain-PalaciosOscar F Vázquez-VuelvasLaura Leticia Valdez-VelazquezGerardo Corzo
Published in: Journal of proteome research (2024)
Heloderma horridum horridum , a venomous reptile native to America, has a venom with potential applications in treating type II diabetes. In this work, H. h. horridum venom was extracted, lyophilized, and characterized using enzymatic assays for hyaluronidase, phospholipase, and protease. Proteomic analysis of the venom was conducted employing bottom-up/shotgun approaches, SDS-PAGE, high-pH reversed-phase chromatography, and fractionation of tryptic peptides using nano-LC-MS/MS. The proteins found in H. h. horridum venom were reviewed according to the classification of the transcriptome previously reported. The proteomic approach identified 101 enzymes, 36 other proteins, 15 protein inhibitors, 11 host defense proteins, and 1 toxin, including novel venom components such as calcium-binding proteins, phospholipase A2 inhibitors, serpins, cathepsin, subtilases, carboxypeptidase-like, aminopeptidases, glycoside hydrolases, thioredoxin transferases, acid ceramidase-like, enolase, multicopper oxidases, phosphoglucose isomerase (PGI), fructose-1,6-bisphosphatase class 1, pentraxin-related, peptidylglycine α-hydroxylating monooxygenase/peptidyl-hydroxyglycine α-amidating lyase, carbonic anhydrase, acetylcholinesterase, dipeptidylpeptidase, and lysozymes. These findings contribute to understanding the venomous nature of H. h. horridum and highlight its potential as a source of bioactive compounds. Data are available via PRoteomeXchange with the identifier PXD052417.
Keyphrases
  • gene expression
  • type diabetes
  • cardiovascular disease
  • single cell
  • rna seq
  • genome wide
  • hydrogen peroxide
  • electronic health record
  • binding protein
  • weight loss
  • tandem mass spectrometry
  • human health