23 results on '"Israel, Mathilde R."'
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2. Topical Oxaliplatin Produces Gain- and Loss-of-Function in Multiple Classes of Sensory Afferents
3. Low potency inhibition of NaV1.7 by externally applied QX-314 via a depolarizing shift in the voltage-dependence of activation
4. Australian funnel-web spiders evolved human-lethal δ-hexatoxins for defense against vertebrate predators
5. Animal toxins — Nature’s evolutionary-refined toolkit for basic research and drug discovery
6. Manipulation of a spider peptide toxin alters its affinity for lipid bilayers and potency and selectivity for voltage-gated sodium channel subtype 1.7
7. Toxins as tools: Fingerprinting neuronal pharmacology
8. The pharmacology of voltage-gated sodium channel activators
9. NaV1.7 as a pain target – From gene to pharmacology
10. Passive transfer of fibromyalgia symptoms from patients to mice
11. δ-Conotoxin SuVIA suggests an evolutionary link between ancestral predator defence and the origin of fish-hunting behaviour in carnivorous cone snails
12. Sodium Channels and Venom Peptide Pharmacology
13. Pain-causing stinging nettle toxins target TMEM233 to modulate NaV1.7 function.
14. Neurotoxic peptides from the venom of the giant Australian stinging tree
15. Characterization of Synthetic Tf2 as a NaV1.3 Selective Pharmacological Probe
16. Na V 1.6 regulates excitability of mechanosensitive sensory neurons
17. Chapter Three - Sodium Channels and Venom Peptide Pharmacology
18. The E15R Point Mutation in Scorpion Toxin Cn2 Uncouples Its Depressant and Excitatory Activities on Human NaV1.6
19. Multiple sodium channel isoforms mediate the pathological effects of Pacific ciguatoxin-1
20. NaV1.6 regulates excitability of mechanosensitive sensory neurons.
21. The E15R Point Mutation in Scorpion Toxin Cn2 Uncouples Its Depressant and Excitatory Activities on Human NaV1.6.
22. The E15R Point Mutation in Scorpion Toxin Cn2 Uncouples Its Depressant and Excitatory Activities on Human NaV1.6
23. Characterization of Synthetic Tf2 as a Na V 1.3 Selective Pharmacological Probe.
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