Nasal administration of the neuroprotective candidate NeuroEPO to healthy volunteers: a randomized, parallel, open-label safety study

Santos-Morales, Orestes; Díaz-Machado, Alina; Jiménez-Rodríguez, Daise; Pomares-Iturralde, Yaisel; Festary-Casanovas, Tatiana; González-Delgado, Carlos A.; Pérez-Rodríguez, Sonia; Alfonso-Muñoz, Eulalia; Viada-González, Carmen; Piedra-Sierra, Patricia; García-García, Idrian; Amaro-González, Daniel; García-Rodríguez, Julio César; Sosa-Testé, I.; Lagarto-Parra, Alicia; L, Barrero-Viera; David-Baldo, Marlene; Tamayo-Rodríguez, Maura; Rivero-Vázquez, Ivonne; González-Gamiz, Gricel; Martín-Trujillo, Alis; Rodríguez-Fernández, Yasmila; Luz, Ana Alfa Ledo-de la; Álvarez-Delgado, Maylén; Álvarez, Ivón Howland; Cruz-Gómez, Yolanda

doi:10.1186/s12883-017-0908-0

Cited by 25 publications

(28 citation statements)

References 32 publications

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“…In human, a first evaluation on healthy human volunteers 27 indicated that 0.5 and 1 mg of Neuro‐EPO every 8 h during 4 days were well tolerated and had no erythropoiesis effect. More clinical trials at similar dosage are ongoing against stroke (acute treatment 1‐mg Neuro‐EPO by nasal route every 8 h for 3 days) and against long‐term neurodegenerative disease on mild–moderate Alzheimer patients and Parkinson patients 28,29 .…”

Section: Detection After a Single In Administrationmentioning

confidence: 99%

Detection of a nonerythropoietic erythropoietin, Neuro‐EPO, in blood after intranasal administration in rat

Martin¹,

Audran²,

Ericsson³

et al. 2020

Drug Testing and Analysis

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Nonerythropoietic erythropoietins (EPOs) are investigated for their high antioxidant properties. A new drug candidate under clinical investigation to treat brain diseases is Neuro‐EPO, produced by selecting EPO isoforms with low sialic acid content. Intranasal administration allows to bypass the blood–brain barrier to get a fast and concentrated delivery to the brain. The aims of this project were to characterize Neuro‐EPO with anti‐doping methods used to detect conventional recombinant EPOs (isoelectric focusing [IEF] and sodium dodecyl sulfate–polyacrylamide gel electrophoresis [SDS‐PAGE]) and to evaluate the window of detection of Neuro‐EPO in brain and blood (plasma) after a single intranasal administration in rats. Neuro‐EPO drug analyzed by IEF‐PAGE presented a very basic profile completely detected only when using a 2–8 or 2–10 pH gradient instead of the conventional 2–6 pH gradient. Its profile consisted in six main bands that did not interfere with endogenous EPO profile from human or rat. After SDS‐PAGE, a broad band was detected for Neuro‐EPO in the same area as endogenous EPO, making Neuro‐EPO identification very difficult by this approach. Therefore, IEF was the method for identification chosen after administration in rats. Neuro‐EPO was clearly identified in blood 2 and 6 h after the delivery. Fainter signals were obtained between 12 and 48 h, but some characteristic very basic bands remained detectable. Surprisingly, brain extracts did not show the presence of Neuro‐EPO even 2 h after administration, indicating a fast degradation or elimination from the brain to the bloodstream. This experiment indicated that detection of Neuro‐EPO after intranasal delivery should be possible for a few days.

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Section: Detection After a Single In Administrationmentioning

confidence: 99%

Detection of a nonerythropoietic erythropoietin, Neuro‐EPO, in blood after intranasal administration in rat

Martin¹,

Audran²,

Ericsson³

et al. 2020

Drug Testing and Analysis

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show abstract

“…Further advances have been made also concerning administration route. Intranasal formulations of EPO and EPO-analogs have been developed in order to avoid repeated injections or high-dose systemic administration (Genc et al, 2011; Santos-Morales et al, 2017). Indeed, the nasal route can bypass the blood brain barrier with an optimal distribution in the cerebrospinal fluid and negligible flow in the systemic circulation, thus potentially hampering unwanted side effects (Genc et al, 2011).…”

Section: Erythropoietin As Therapeutic Compoundmentioning

confidence: 99%

Erythropoietin and Friedreich Ataxia: Time for a Reappraisal?

Boesch

Indelicato

2019

Front. Neurosci.

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Friedreich ataxia (FRDA) is a rare neurological disorder due to deficiency of the mitochondrial protein frataxin. Frataxin deficiency results in impaired mitochondrial function and iron deposition in affected tissues. Erythropoietin (EPO) is a cytokine which was mostly known as a key regulator of erythropoiesis until cumulative evidence showed additional neurotrophic and neuroprotective properties. These features offered the rationale for advancement of EPO in clinical trials in different neurological disorders in the past years, including FRDA. Several mechanisms of action of EPO may be beneficial in FRDA. First of all, EPO exposure results in frataxin upregulation in vitro and in vivo . By promoting erythropoiesis, EPO influences iron metabolism and induces shifts in iron pool which may ameliorate conditions of free iron excess and iron accumulation. Furthermore, EPO signaling is crucial for mitochondrial gene activation and mitochondrial biogenesis. Up to date nine clinical trials investigated the effects of EPO and derivatives in FRDA. The majority of these studies had a proof-of-concept design. Considering the natural history of FRDA, all of them were too short in duration and not powered for clinical changes. However, these studies addressed significant issues in the treatment with EPO, such as (1) the challenge of the dose finding, (2) stability of frataxin up-regulation, (3) continuous versus intermittent stimulation with EPO/regimen, or (4) tissue changes after EPO exposure in humans in vivo (muscle biopsy, brain imaging). Despite several clinical trials in the past, no treatment is available for the treatment of FRDA. Current lines of research focus on gene therapy, frataxin replacement strategies and on regulation of key metabolic checkpoints such as NrF2. Due to potential crosstalk with all these mechanisms, interventions on the EPO pathway still represent a valuable research field. The recent development of small EPO mimetics which maintain cytoprotective properties without erythropoietic action may open a new era in EPO research for the treatment of FRDA.

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“…There are already a few clinical studies exploring the intranasal route for a variety of inflammatory acute and chronic neurological conditions that require considerable systemic exposure . These studies are summarized in Table .…”

Section: Anti‐neuroinflammatory Treatment In Sepsismentioning

confidence: 99%

Sepsis: developing new alternatives to reduce neuroinflammation and attenuate brain injury

Meneses

Cárdenas

Espinosa

et al. 2018

Annals of the New York Academy of Sciences

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Sepsis occurs when a systemic infection induces an uncontrolled inflammatory response that results in generalized organ dysfunction. The exacerbated peripheral inflammation can induce, in turn, neuroinflammation which may result in severe impairment of the central nervous system (CNS). Indeed, the ensuing blood–brain barrier disruption associated with sepsis promotes glial activation and starts a storm of proinflammatory cytokines in the CNS that leads to brain dysfunction in sepsis survivors. Endotoxic shock induced in mice by peripheral injection of lipopolysaccharides closely resembles the peripheral and central inflammation observed in sepsis. In this review, we provide an overview of the neuroinflammatory features in sepsis and of recent progress toward the development of new anti‐neuroinflammatory therapies seeking to reduce mortality and morbidity in sepsis survivors.

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Nasal administration of the neuroprotective candidate NeuroEPO to healthy volunteers: a randomized, parallel, open-label safety study

Cited by 25 publications

References 32 publications

Detection of a nonerythropoietic erythropoietin, Neuro‐EPO, in blood after intranasal administration in rat

Detection of a nonerythropoietic erythropoietin, Neuro‐EPO, in blood after intranasal administration in rat

Erythropoietin and Friedreich Ataxia: Time for a Reappraisal?

Sepsis: developing new alternatives to reduce neuroinflammation and attenuate brain injury

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