New Trends in Identification and Characterization of Venom Components

A special issue of Toxins (ISSN 2072-6651). This special issue belongs to the section "Animal Venoms".

Deadline for manuscript submissions: closed (31 March 2023) | Viewed by 3072

Special Issue Editors


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Guest Editor
National Natural Toxins Research Center, Texas A&M University-Kingsville, Kingsville, TX 78363, USA
Interests: snake venom toxins; pathophysiology; recombinant proteins; molecular mechanisms of action; envenomation; proteomics; vascular permeability; extracellular vesicle; inflammatory responses; signaling pathways
Special Issues, Collections and Topics in MDPI journals

E-Mail Website
Guest Editor
National Natural Toxins Research Center, Texas A&M University-Kingsville, Kingsville, TX, USA
Interests: snake venom; phospholipases A2; inflammation; immune response; coagulation; hemostasis; pathophysiology; antivenoms; recombinant protein; molecular mechanisms of action; envenomation; proteomics

Special Issue Information

Dear Colleagues,

Animal venoms are rich sources of bioactive molecules, displaying a variety of molecular targets and functions. Many toxins have been identified and characterized by venomous animals such as scorpions, spiders, honeybees, and snails, and most of these are from snakes. Each component in the venom has different targets and interferes with the normal biological functions of the target cells, tissues, organs, and physiological systems and can cause severe consequences to human health. Due to their pharmacological activities, several venom components are extensively studied and can be used as diagnostic tools and therapeutic agents. Over the years, more species of venomous animals have been reported, leading to the enormous diversity of unstudied venoms. The advent of more sophisticated identification and characterization techniques has accelerated a more comprehensive knowledge of the venom composition and unveiled the pharmacological complexity of venoms. The exploration of new venom components contributes not only to understanding the pathophysiological changes observed after envenomation but also offers an exciting new avenue for studying venom evolution and toxicology, as well as the discovery of novel pharmacological tools and drug candidates. This Special Issue of Toxins welcomes contributions to the development of innovative approaches, advanced instrumental techniques, and methods to identify and characterize the venom components.

Dr. Montamas Suntravat
Dr. Emelyn Salazar
Guest Editors

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Keywords

  • identification and characterization
  • venomous animals
  • venom components
  • toxin
  • mechanism of action
  • venom secretions

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Published Papers (1 paper)

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Research

30 pages, 5095 KiB  
Article
A Combined Bioassay and Nanofractionation Approach to Investigate the Anticoagulant Toxins of Mamba and Cobra Venoms and Their Inhibition by Varespladib
by Arif Arrahman, Taline D. Kazandjian, Kristina B. M. Still, Julien Slagboom, Govert W. Somsen, Freek J. Vonk, Nicholas R. Casewell and Jeroen Kool
Toxins 2022, 14(11), 736; https://doi.org/10.3390/toxins14110736 - 27 Oct 2022
Cited by 6 | Viewed by 2631
Abstract
Envenomation by elapid snakes primarily results in neurotoxic symptoms and, consequently, are the primary focus of therapeutic research concerning such venoms. However, mounting evidence suggests these venoms can additionally cause coagulopathic symptoms, as demonstrated by some Asian elapids and African spitting cobras. This [...] Read more.
Envenomation by elapid snakes primarily results in neurotoxic symptoms and, consequently, are the primary focus of therapeutic research concerning such venoms. However, mounting evidence suggests these venoms can additionally cause coagulopathic symptoms, as demonstrated by some Asian elapids and African spitting cobras. This study sought to investigate the coagulopathic potential of venoms from medically important elapids of the genera Naja (true cobras), Hemachatus (rinkhals), and Dendroaspis (mambas). Crude venoms were bioassayed for coagulant effects using a plasma coagulation assay before RPLC/MS was used to separate and identify venom toxins in parallel with a nanofractionation module. Subsequently, coagulation bioassays were performed on the nanofractionated toxins, along with in-solution tryptic digestion and proteomics analysis. These experiments were then repeated on both crude venoms and on the nanofractionated venom toxins with the addition of either the phospholipase A2 (PLA2) inhibitor varespladib or the snake venom metalloproteinase (SVMP) inhibitor marimastat. Our results demonstrate that various African elapid venoms have an anticoagulant effect, and that this activity is significantly reduced for cobra venoms by the addition of varespladib, though this inhibitor had no effect against anticoagulation caused by mamba venoms. Marimastat showed limited capacity to reduce anticoagulation in elapids, affecting only N. haje and H. haemachatus venom at higher doses. Proteomic analysis of nanofractionated toxins revealed that the anticoagulant toxins in cobra venoms were both acidic and basic PLA2s, while the causative toxins in mamba venoms remain uncertain. This implies that while PLA2 inhibitors such as varespladib and metalloproteinase inhibitors such as marimastat are viable candidates for novel snakebite treatments, they are not likely to be effective against mamba envenomings. Full article
(This article belongs to the Special Issue New Trends in Identification and Characterization of Venom Components)
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