Pharmacological reversal of a pain phenotype in iPSC-derived sensory neurons and patients with inherited erythromelalgia

Cao, Lishuang; McDonnell, Aoibhinn; Nitzsche, Anja; Alexandrou, Aristos J.; Saintot, Pierre-Philippe; Loucif, Alexandre; Brown, Adam R.; Young, Gareth T.; Mis, Malgorzata A.; Randall, Andrew D.; Waxman, Stephen G.; Stanley, P; Kirby, Simon; Tarabar, Sanela; Gutteridge, Alex; Butt, Richard P.; McKernan, Ruth M.; Whiting, Paul J.; Ali, Zahid; Bilsland, James; Stevens, Edward B.

doi:10.1126/scitranslmed.aad7653

Cited by 160 publications

(182 citation statements)

References 29 publications

(57 reference statements)

Supporting

Mentioning

163

Contrasting

Order By: Relevance

“…While efficacy in the OD1 model, as well as emerging positive clinical trial results with small molecule aryl sulfonamides56, suggest that Na V 1.7 inhibitors may be efficacious in IEM or PEPD, our results reveal that acute administration of peripherally restricted Na V 1.7 inhibitors alone may not have broad efficacy in inflammatory pain. The efficacy of peripherally restricted Na V 1.7 inhibitors in other pain types, such as neuropathic pain, remains to be determined, and underscores the need for further studies to determine how, or whether, Nav1.7 blockade will reduce pain in humans.…”

Section: Discussionmentioning

confidence: 61%

Pharmacological characterisation of the highly NaV1.7 selective spider venom peptide Pn3a

Deuis

Dekan

Wingerd

et al. 2017

Sci Rep

Self Cite

126

185

View full text Add to dashboard Cite

Human genetic studies have implicated the voltage-gated sodium channel NaV1.7 as a therapeutic target for the treatment of pain. A novel peptide, μ-theraphotoxin-Pn3a, isolated from venom of the tarantula Pamphobeteus nigricolor, potently inhibits NaV1.7 (IC50 0.9 nM) with at least 40–1000-fold selectivity over all other NaV subtypes. Despite on-target activity in small-diameter dorsal root ganglia, spinal slices, and in a mouse model of pain induced by NaV1.7 activation, Pn3a alone displayed no analgesic activity in formalin-, carrageenan- or FCA-induced pain in rodents when administered systemically. A broad lack of analgesic activity was also found for the selective NaV1.7 inhibitors PF-04856264 and phlotoxin 1. However, when administered with subtherapeutic doses of opioids or the enkephalinase inhibitor thiorphan, these subtype-selective NaV1.7 inhibitors produced profound analgesia. Our results suggest that in these inflammatory models, acute administration of peripherally restricted NaV1.7 inhibitors can only produce analgesia when administered in combination with an opioid.

show abstract

Section: Discussionmentioning

confidence: 61%

Pharmacological characterisation of the highly NaV1.7 selective spider venom peptide Pn3a

Deuis

Dekan

Wingerd

et al. 2017

Sci Rep

Self Cite

126

185

View full text Add to dashboard Cite

show abstract

“…However, although several selective Nav1.7 inhibitors have been described in the literature101112, none have fully recapitulated the dramatic analgesia observed in Nav1.7-null subjects1112 and clinical progress has been slow1314. While the absence of efficacy has discouraged many in the field, and led some to question the drugabililty of Nav1.7, one possible explanation is that the pharmacological tools utilized provided sub-optimal block of Nav1.7.…”

mentioning

confidence: 99%

Insensitivity to pain induced by a potent selective closed-state Nav1.7 inhibitor

Flinspach

Piekarz

et al. 2017

Sci Rep

108

141

View full text Add to dashboard Cite

Pain places a devastating burden on patients and society and current pain therapeutics exhibit limitations in efficacy, unwanted side effects and the potential for drug abuse and diversion. Although genetic evidence has clearly demonstrated that the voltage-gated sodium channel, Nav1.7, is critical to pain sensation in mammals, pharmacological inhibitors of Nav1.7 have not yet fully recapitulated the dramatic analgesia observed in Nav1.7-null subjects. Using the tarantula venom-peptide ProTX-II as a scaffold, we engineered a library of over 1500 venom-derived peptides and identified JNJ63955918 as a potent, highly selective, closed-state Nav1.7 blocking peptide. Here we show that JNJ63955918 induces a pharmacological insensitivity to pain that closely recapitulates key features of the Nav1.7-null phenotype seen in mice and humans. Our findings demonstrate that a high degree of selectivity, coupled with a closed-state dependent mechanism of action is required for strong efficacy and indicate that peptides such as JNJ63955918 and other suitably optimized Nav1.7 inhibitors may represent viable non-opioid alternatives for the pharmacological treatment of severe pain.

show abstract

“…iPSCs can be used to draw associations between genotype and drug responses and to identify biomarkers to inform patient selection for enrollment in clinical trials 109–111 . For example, the pharmacological reversal, using a selective sodium-channel blocker, of a hyperexcitability phenotype in sensory neurons derived from iPSCs from patients with the pain disorder inherited erythromelalgia was found to correlate with patient responses and specific patient mutations 111 .…”

Section: Applications Of Ipscs In Basic and Translational Cancer Resementioning

confidence: 99%

“…For example, the pharmacological reversal, using a selective sodium-channel blocker, of a hyperexcitability phenotype in sensory neurons derived from iPSCs from patients with the pain disorder inherited erythromelalgia was found to correlate with patient responses and specific patient mutations 111 . For such applications to materialize, large and diverse collections of cancer-derived iPSCs, capturing a range of cancer types and genotypes, will need to be assembled.…”

Section: Applications Of Ipscs In Basic and Translational Cancer Resementioning

confidence: 99%

Patient-derived induced pluripotent stem cells in cancer research and precision oncology

Papapetrou

2016

Nat Med

130

108

View full text Add to dashboard Cite

Together with recent advances in the processing and culture of human tissue, bioengineering, xenotransplantation and genome editing, Induced pluripotent stem cells (iPSCs) present a range of new opportunities for the study of human cancer. Here we discuss the main advantages and limitations of iPSC modeling, and how the method intersects with other patient-derived models of cancer, such as organoids, organson-chips and patient-derived xenografts (PDXs). We highlight the opportunities that iPSC models can provide beyond those offered by existing systems and animal models and present current challenges and crucial areas for future improvements toward wider adoption of this technology.

show abstract

Pharmacological reversal of a pain phenotype in iPSC-derived sensory neurons and patients with inherited erythromelalgia

Cited by 160 publications

References 29 publications

Pharmacological characterisation of the highly NaV1.7 selective spider venom peptide Pn3a

Pharmacological characterisation of the highly NaV1.7 selective spider venom peptide Pn3a

Insensitivity to pain induced by a potent selective closed-state Nav1.7 inhibitor

Patient-derived induced pluripotent stem cells in cancer research and precision oncology

Contact Info

Product

Resources

About