Efficient functional neutralization of lethal peptide toxins in vivo by oligonucleotides
Medical means to save the life of human patients affected by drug abuse, envenomation or critical poisoning are currently limited. While the compounds at risks are most often well identified, particularly for bioterrorism, chemical intervention to counteract the toxic effects of the ingested/injected compound(s) is restricted to the use of antibodies. Herein, we illustrate that DNA aptamers, targeted to block the pharmacophore of a poisonous compound, represent a fast-acting and reliable method of neutralization in vivo that possesses efficient and long-lasting life-saving properties. For this proof of concept, we used one putative bioweapon, $\alpha$C-conotoxin PrXA, a marine snail ultrafast-killing paralytic toxin, to identify peptide-binding DNA aptamers. We illustrate that they can efficiently neutralize the toxin-induced (i) displacement of [125I]-$\alpha$-bungarotoxin binding onto nicotinic receptors, (ii) inhibition of diaphragm muscle contraction, and (iii) lethality in mice. Our results demonstrate the preclinical value of DNA aptamers as fast-acting, safe and cheap antidotes to lethal toxins at risk of misuse in bioterrorism and offer hope for an alternative method than donor sera to treat cases of envenomation.
Références
- Titre
- Efficient functional neutralization of lethal peptide toxins in vivo by oligonucleotides
- Type de publication
- Article de revue
- Année de publication
- 2017
- Auteurs
- El-Aziz, Tarek Mohamed Ab, Ravelet Corinne, Molgo Jordi, Fiore Emmanuelle, Pale Simon, Amar Muriel, Al-Khoury Sawsan, Dejeu Jérôme, Fadl Mahmoud, Ronjat Michel, Taiwe Germain Sotoing, Servent Denis, Peyrin Eric, and De Waard Michel
- Revue
- Sci. Rep.
- Volume
- 7
- Pagination
- 7202
- ISSN
- 2045-2322
Soumis le 18 mai 2018