Flipping the molecular switch for innate protection and repair of tissues: Long-lasting effects of a non-erythropoietic small peptide engineered from erythropoietin

Collino, Massimo; Thiemermann, Christoph; Cerami, Anthony; Brines, Michael

doi:10.1016/j.pharmthera.2015.02.005

Cited by 77 publications

(78 citation statements)

References 97 publications

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“…5 Although parallel assessments of lower limb distal IENFD did not show a similar change, quantification of new nerve fiber growth within the epidermis using GAP-43 immunostaining also supported a cibinetide-related increase in small nerve fiber regeneration. This observation is strengthened further by the significant positive correlation noted between changes in CNFA and GAP-43 þ fiber length.…”

Section: Discussionmentioning

confidence: 83%

“…9 Despite a short plasma half-life, cibinetide triggers sustained biological effects when concentrations exceed the low nanomolar affinity of the receptor. 5 Notably, in a mouse model of diabetic SNFL, daily administration of cibinetide reversed neuronal dystrophy. 7 In neuropathic states the transient receptor potential vanilloid-1 (TRPV1) ion channel, a key integrator of nociception and neurogenic inflammation, undergoes upregulation and sensitization in peripheral small nerve fibers and central pain pathways.…”

Section: Minute Walk Test [6mwt])mentioning

confidence: 99%

“…This system is activated by the innate repair receptor (IRR) comprised of b common (CD131) and erythropoietin receptor subunits, which signals via janus kinase-2 and multiple downstream intracellular molecular pathways. 5 IRR activation promotes tissue protection and repair in a wide variety of preclinical models, 5 including neuropathy. [6][7][8] Cibinetide (ARA 290; helix B surface peptide) is a novel 11 amino acid peptide with high affinity and selectivity for the IRR.…”

Section: Minute Walk Test [6mwt])mentioning

confidence: 99%

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Cibinetide Improves Corneal Nerve Fiber Abundance in Patients With Sarcoidosis-Associated Small Nerve Fiber Loss and Neuropathic Pain

Culver

Dahan

Bajorunas

et al. 2017

Invest. Ophthalmol. Vis. Sci.

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PURPOSE. Sarcoidosis frequently is complicated by small nerve fiber loss (SNFL), which can be quantified using corneal confocal microscopy (CCM). Prior studies suggest that the innate repair receptor agonist cibinetide reverses corneal nerve loss. This phase 2b, 28-day, randomized trial of 64 subjects with sarcoid-associated SNFL and neuropathic pain assessed the effect of cibinetide on corneal nerve fiber area (CNFA) and regenerating intraepidermal fibers (GAP-43 þ ) as surrogate endpoints for disease modification, pain severity, and functional capacity (6-minute walk test [6MWT]).METHODS. Cibinetide (1, 4, or 8 mg/day) was compared to placebo. The primary study endpoint was a change in CNFA at 28 days.RESULTS. The placebo-corrected mean change from baseline CNFA (lm 2 ) at day 28 was 109 (95% confidence interval [CI], À429, 647), 697 (159, 1236; P ¼ 0.012), and 431 (À130, 992) in the 1, 4, and 8 mg groups, respectively. Intraepidermal GAP-43 þ fibers increased in the 4 mg group (P ¼ 0.035). Further, changes in CNFA correlated with changes in GAP-43 þ (q ¼ 0.575; P ¼ 0.025) and 6MWT (q ¼ 0.645; P ¼ 0.009). Pain improved significantly in all groups, with subjects having moderate-severe pain reporting a clinically meaningful placebocorrected decrease in pain intensity in the 4 mg group (P ¼ 0.157).CONCLUSIONS. Cibinetide significantly increased small nerve fiber abundance in the cornea and skin, consistent with a disease modifying effect. The relationships between CNFA and other clinical measures of disease support its use as a surrogate endpoint to assess potential disease modifying therapies for neuropathy.

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Section: Discussionmentioning

confidence: 83%

Section: Minute Walk Test [6mwt])mentioning

confidence: 99%

Section: Minute Walk Test [6mwt])mentioning

confidence: 99%

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Cibinetide Improves Corneal Nerve Fiber Abundance in Patients With Sarcoidosis-Associated Small Nerve Fiber Loss and Neuropathic Pain

Culver

Dahan

Bajorunas

et al. 2017

Invest. Ophthalmol. Vis. Sci.

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“…The nature of the neuroprotective Epo receptor is currently debated. As non-erythropoietic candidate receptors, common β chain receptor/classical EpoR heteromers expressed in the nervous system (Brines and Cerami, 2005; Collino et al, 2015) and bone tissue (Duedal Rölfing et al, 2014) and leukemia inhibitory factor LIFR/DC130 expressed in neuronal and other cell lines (Bonnas, 2012) are discussed. However, even within a particular tissue such as the nervous system, the expression of Epo receptors may depend on cell type, developmental stage, physiological condition and actual as well as previous exposure to challenging stimuli (Sinor and Greenberg, 2000; Brines and Cerami, 2005; Shein et al, 2005; Um et al, 2007; Sanchez et al, 2009).…”

Section: Introductionmentioning

confidence: 99%

The Insect Ortholog of the Human Orphan Cytokine Receptor CRLF3 Is a Neuroprotective Erythropoietin Receptor

Hahn

Knorr

Liebig

et al. 2017

Front. Mol. Neurosci.

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The cytokine erythropoietin (Epo) mediates various cell homeostatic responses to environmental challenges and pathological insults. While stimulation of vertebrate erythrocyte production is mediated by homodimeric “classical” Epo receptors, alternative receptors are involved in neuroprotection. However, their identity remains enigmatic due to complex cytokine ligand and receptor interactions and conflicting experimental results. Besides the classical Epo receptor, the family of type I cytokine receptors also includes the poorly characterized orphan cytokine receptor-like factor 3 (CRLF3) present in vertebrates including human and various insect species. By making use of the more simple genetic makeup of insect model systems, we studied whether CRLF3 is a neuroprotective Epo receptor in animals. We identified a single ortholog of CRLF3 in the beetle Tribolium castaneum, and established protocols for primary neuronal cell cultures from Tribolium brains and efficient in vitro RNA interference. Recombinant human Epo as well as the non-erythropoietic Epo splice variant EV-3 increased the survival of serum-deprived brain neurons, confirming the previously described neuroprotective effect of Epo in insects. Moreover, Epo completely prevented hypoxia-induced apoptotic cell death of primary neuronal cultures. Knockdown of CRLF3 expression by RNA interference with two different double stranded RNA (dsRNA) fragments abolished the neuroprotective effect of Epo, indicating that CRLF3 is a crucial component of the insect Epo-responsive receptor. This suggests that a common urbilaterian ancestor of the orphan human and insect cytokine receptor CRLF3 served as a neuroprotective receptor for an Epo-like cytokine. Our work also suggests that vertebrate CRLF3, like its insect ortholog, might represent a tissue protection-mediating receptor.

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“…The addition of ARA 290 significantly suppressed caspase 3/7 activity after co-culturing with proinflammatory cytokines compared to the vehicle-treated control group. Mechanistically, ARA 290 exerts anti-inflammatory, antiapoptotic, and tissue-protective effects through its interaction with the IRR [35][36][37] and subsequently suppresses the nuclear factor-κB-driven gene transcription of pro-inflammatory mediators, which leads to the phosphorylation of endothelial nitric oxide synthase and other signaling systems [35,38,39]. Exposure of proinflammatory cytokines causes IRR expression on the cell surface [24] and therefore the addition of ARA 290 could activate this receptor to prevent cytokine-induced damage and apoptosis.…”

Section: Discussionmentioning

confidence: 99%

An Engineered Innate Repair Receptor Agonist, ARA 290, Protects Rat Islets from Cytokine-induced Apoptosis

Watanabe¹,

Saito²,

Wallmo³

et al. 2016

J Diabetes Metab

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The efficacy of pancreatic islet transplantation (PITx) is reduced due to severe inflammatory responses triggered by the islet isolation and transplantation procedures. ARA 290, an innate repair receptor agonist, has anti-apoptotic and anti-inflammatory properties and it has been shown to improve clinical symptoms caused by inflammation in sarcoidosis patients and type 2 diabetes. We here investigated whether ARA 290 treatment would improve the efficacy of PITx in a rat pancreatic islet transplantation model. For islets co-cultured with proinflammatory cytokines, addition of ARA290 showed better viability [percent of naïve control in MTT assay: 54.6 ± 5.2 vs. 75.2 ± 6.4], insulin release [stimulation index in static glucose stimulated insulin secretion tests of 1.05 ± 0.63 vs. 2.61 ± 0.89], and reduced apoptosis [caspase3/7 activity182 ± 18 vs. 152 ± 18 luminescence/dsDNA(ng)] (islets with cytokines vs. islets with ARA290+cytokines, respectively, all p<0.05). In order to mimic the clinical situation, islets were isolated after prolonged cold ischemia (18 h). The addition of ARA 290 into preservation solution, however, did not improve islet yields or function. As a marginal syngeneic PITx, 220 syngeneic rat islets were transplanted under the kidney capsule of streptozotocin-induced diabetic rats and the recipients were treated with ARA 290 (120 µg/kg/day) for two weeks after PITx. In this model, no beneficial effect of ARA 290 treatment was observed. Our results indicated that ARA 290 protected rat pancreatic islets from cytokine-induced damage and apoptosis, but did not improve PITx perhaps due to poor penetration of ARA290 into transplant site or low IRR expression. ARA 290 could be useful as an agent to reduce islet injury caused by severe inflammation.

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Flipping the molecular switch for innate protection and repair of tissues: Long-lasting effects of a non-erythropoietic small peptide engineered from erythropoietin

Cited by 77 publications

References 97 publications

Cibinetide Improves Corneal Nerve Fiber Abundance in Patients With Sarcoidosis-Associated Small Nerve Fiber Loss and Neuropathic Pain

Cibinetide Improves Corneal Nerve Fiber Abundance in Patients With Sarcoidosis-Associated Small Nerve Fiber Loss and Neuropathic Pain

The Insect Ortholog of the Human Orphan Cytokine Receptor CRLF3 Is a Neuroprotective Erythropoietin Receptor

An Engineered Innate Repair Receptor Agonist, ARA 290, Protects Rat Islets from Cytokine-induced Apoptosis

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