Improvement of cognitive functions in chronic schizophrenic patients by recombinant human erythropoietin

Ehrenreich, Hannelore; Hinze-Selch, D.; Stawicki, Sabina; Aust, Carlotta; Knolle-Veentjer, S.; Wilms, S.; Heinz, G.; Erdag, S.; Jahn, Henriette; Degner, Detlef; Ritzén, Martin; Mohr, Alexander T.; Wagner, Michael; Schneider, Udo; Bohn, Manfred A.; Huber, Martin; Czernik, Adelheid; Pollmächer, Thomas; Maier, Wolfgang; Sirén, Anna‐Leena; Klosterkötter, Joachim; Falkai, Peter; Rüther, Eckart; Aldenhoff, Josef B.; Krampe, Henning

doi:10.1038/sj.mp.4001907

Cited by 244 publications

(216 citation statements)

References 65 publications

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“…High-dose EPO (40,000 IU intravenously), applied over 12 weeks on a weekly basis, led to significant improvement of schizophrenia-relevant cognitive performance as compared to placebo-treated patients. 124 In addition to the stepwise improvement in cognitive performance, we found that EPO was able to delay progression of cortical gray matter loss in chronic schizophrenic patients, as determined by most comprehensive, voxel-based morphometrical MRI analysis (manuscript in preparation). In this respect, EPO-induced prevention of brain atrophy, as observed in rodent studies, 86 could be nicely reproduced in man.…”

Section: Schizophreniamentioning

confidence: 84%

“…To our knowledge, no EPO variants other than rhEPO itself have thus far been published in relation to the treatment of human nervous system diseases. The only studies published so far reporting on efficacy of rhEPO in human brain diseases are our own studies on ischemic stroke, schizophrenia and MS. 69,119,124 …”

Section: Erythropoietin As Neuroprotective/ Neuroregenerative Treatmementioning

confidence: 99%

“…27 From 2003 to 2005, we performed a double-blind, placebo-controlled multicenter trial (phase IIb) on EPO add-on treatment in chronic schizophrenic men displaying a defined cognitive deficit. 124 Participating centers included Göttingen, Kiel, Homburg, Cologne and Marburg. High-dose EPO (40,000 IU intravenously), applied over 12 weeks on a weekly basis, led to significant improvement of schizophrenia-relevant cognitive performance as compared to placebo-treated patients.…”

Section: Schizophreniamentioning

confidence: 99%

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Therapeutic Potential of Erythropoietin and its Structural or Functional Variants in the Nervous System

et al. 2009

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Summary:The growth factor erythropoietin (EPO) and erythropoietin receptors (EPOR) are expressed in the nervous system. Neuronal expression of EPO and EPOR peaks during brain development and is upregulated in the adult brain after injury. Peripherally administered EPO, and at least some of its variants, cross the blood-brain barrier, stimulate neurogenesis, neuronal differentiation, and activate brain neurotrophic, antiapoptotic, anti-oxidant and anti-inflammatory signaling. These mechanisms underlie their tissue protective effects in nervous system disorders. As the tissue protective functions of EPO can be separated from its stimulatory action on hematopoiesis, novel EPO derivatives and mimetics, such as asialo-EPO and carbamoylated EPO have been developed. While the therapeutic potential of the novel EPO derivatives continues to be characterized in preclinical studies, the experimental findings in support for the use of recombinant human (rh)EPO in human brain disease have already been translated to clinical studies in acute ischemic stroke, chronic schizophrenia, and chronic progressive multiple sclerosis. In this review article, we assess the studies on EPO and, in particular, on its structural or functional variants in experimental models of nervous system disorders, and we provide a short overview of the completed and ongoing clinical studies testing EPO as neuroprotective/neuroregenerative treatment option in neuropsychiatric disease.

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Section: Schizophreniamentioning

confidence: 84%

Section: Erythropoietin As Neuroprotective/ Neuroregenerative Treatmementioning

confidence: 99%

Section: Schizophreniamentioning

confidence: 99%

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Therapeutic Potential of Erythropoietin and its Structural or Functional Variants in the Nervous System

et al. 2009

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“…Therefore, sustained or increased brain BDNF by exogenous rhEPO co-treatment has the potential to prevent and/or reverse neuropathological events in schizophrenia (Glantz et al, 2006). In support of this possibility, a recent clinical add-on therapy, rhEPO with antipsychotic medication, showed significant improvement in cognitive function in chronic schizophrenia patients (Ehrenreich et al, 2007). In addition, rhEPO has therapeutic advantages over other neurotrophic factors in terms of delivery to their target cells in the brain and clinical tolerability (Abicht and Lochmuller, 1999;Horina et al, 1991).…”

Section: Discussionmentioning

confidence: 97%

“…Furthermore, a recent study by Ehrenreich et al, 2007 has shown that rhEPO improves cognitive functions in chronic schizophrenic patients. We recently reported that HAL and olanzapine have distinct temporal effects on the expression of EPO and its receptor in adult rat brain .…”

Section: Introductionmentioning

confidence: 99%

Erythropoietin Prevents Haloperidol Treatment-Induced Neuronal Apoptosis through Regulation of BDNF

Pillai

Dhandapani

Pillai

et al. 2007

Neuropsychopharmacol

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Functional alterations in the neurotrophin, brain-derived neurotrophic factor (BDNF) have recently been implicated in the pathophysiology of schizophrenia. Furthermore, animal studies have indicated that several antipsychotic drugs have time-dependent (and differential) effects on BDNF levels in the brain. For example, our previous studies in rats indicated that chronic treatment with the conventional antipsychotic, haloperidol, was associated with decreases in BDNF (and other neurotrophins) in the brain as well as deficits in cognitive function (an especially important consideration for the therapeutics of schizophrenia). Additional studies indicate that haloperidol has other deleterious effects on the brain (eg increased apoptosis). Despite such limitations, haloperidol remains one of the more commonly prescribed antipsychotic agents worldwide due to its efficacy for the positive symptoms of schizophrenia and its low cost. Interestingly, the hematopoietic hormone, erythropoietin, in its recombinant human form rhEPO has been reported to increase the expression of BDNF in neuronal tissues and to have neuroprotective effects. Such observations provided the impetus for us to investigate in the present study whether co-treatment of rhEPO with haloperidol could sustain the normal levels of BDNF in vivo in rats and in vitro in cortical neuronal cultures and further, whether BDNF could prevent haloperidol-induced apoptosis through the regulation of key apoptotic/antiapoptotic markers. The results indicated that rhEPO prevented the haloperidol-induced reduction in BDNF in both in vivo and in vitro experimental conditions. The sustained levels of BDNF in rats with rhEPO prevented the haloperidol-induced increase in caspase-3 (po0.05) and decrease in Bcl-xl (po0.01) protein levels. Similarly, in vitro experiments showed that rhEPO prevented (po0.001) the haloperidol-induced neuronal cell death as well as the decrease in Bcl-xl levels (po0.01). These findings may have significant implications for the development of neuroprotective strategies to improve clinical outcomes when antipsychotic drugs are used chronically.

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Calcium channel blockers for antipsychotic-induced tardive dyskinesia

Essali

Soares‐Weiser

Adams

2018

Cochrane Database of Systematic Reviews

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Cochrane Database of Systematic Reviews a er three to four weeks' treatment (MD -0.71, 95% CI -2.68 to 1.26, very low quality evidence). Only one study randomising 20 participants reported on adverse events, and reported that there were no adverse events with flunarizine or with placebo (very low quality evidence). One study with 18 participants reported no events of deterioration in mental state with diltiazem or with placebo (very low quality evidence). No studies reported on acceptability of treatment or on social confidence, social inclusion, social networks or personalised quality of life outcomes designated important to patients. Authors' conclusionsAvailable evidence from randomised controlled trials is extremely limited and very low quality, conclusions cannot be drawn. The e ects of calcium channel blockers for antipsychotic-induced tardive dyskinesia are unknown. Their use is experimental and should only be given in the context of well-designed randomised trials.

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Improvement of cognitive functions in chronic schizophrenic patients by recombinant human erythropoietin

Cited by 244 publications

References 65 publications

Therapeutic Potential of Erythropoietin and its Structural or Functional Variants in the Nervous System

Therapeutic Potential of Erythropoietin and its Structural or Functional Variants in the Nervous System

Erythropoietin Prevents Haloperidol Treatment-Induced Neuronal Apoptosis through Regulation of BDNF

Calcium channel blockers for antipsychotic-induced tardive dyskinesia

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