Anti-inflammatory and cognitive effects of interferon-β1a (IFNβ1a) in a rat model of Alzheimer’s disease

Mudò, Giuseppa; Frinchi, Monica; Nuzzo, Domenico; Scaduto, P; Plescia, Fulvio; Massenti, Maria Fatima; Carlo, Marta Di; Cannizzaro, Carla; Cassata, Giovanni; Cicero, Luca; Ruscica, Maria; Belluardo, Natale; Grimaldi, Luigi Maria Edoardo

doi:10.1186/s12974-019-1417-4

Cited by 67 publications

(54 citation statements)

References 74 publications

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“…Aβ acts as danger-associated molecular patterns (DAMP) which can bind to different DAMPreceptors, among FPR, which are expressed by microglia and astrocytes [13,14,25,27]. Aß binding to its receptors induced the expression of various pro-inflammatory mediators [68]. In addition, Aβ has been shown to be cleared by microglia in vitro and in vivo through receptor-mediated phagocytosis and degradation [69,70].…”

Section: Discussionmentioning

confidence: 99%

Inhibition of formyl peptide receptors improves the outcome in a mouse model of Alzheimer disease

Schröder

Schaffrath

Welter

et al. 2020

J Neuroinflammation

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Background: An important hallmark of Alzheimer's disease (AD) is the increase of Aβ1-42 burden and its accumulation to senile plaques, leading the reactive gliosis and neurodegeneration. The modulation of glia cell function represents an attractive therapeutic strategy, but is currently limited by an incomplete understanding of its relevance for AD. The chemotactic G-protein coupled formyl peptide receptor (FPR), which is known to modulate Aβ1-42 uptake and signal transduction, might be one candidate molecule regulating glia function in AD. Here, we investigate whether the modulation of FPR exerts beneficial effects in an AD preclinical model. Methods: To address this question, APP/PS1 double-transgenic AD mice were treated for 20 weeks with either the pro-inflammatory FPR agonist fMLF, the FPR1/2 antagonist Boc2 or the anti-inflammatory FPR2 agonist Ac2-26. Spatial learning and memory were evaluated using a Morris water maze test. Immunohistological staining, gene expression studies, and flow cytometry analyses were performed to study neuronal loss, gliosis, and Aß-load in the hippocampus and cortex, respectively. Results: FPR antagonism by Boc2-treatment significantly improved spatial memory performance, reduced neuronal pathology, induced the expression of homeostatic growth factors, and ameliorated microglia, but not astrocyte, reactivity. Furthermore, the elevated levels of amyloid plaques in the hippocampus were reduced by Boc2treatment, presumably by an induction of amyloid degradation. Conclusions: We suggest that the modulation of FPR signaling cascades might be considered as a promising therapeutic approach for alleviating the cognitive deficits associated with early AD. Additional studies are now needed to address the downstream effectors as well as the safety profile of Boc2.

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Section: Discussionmentioning

confidence: 99%

Inhibition of formyl peptide receptors improves the outcome in a mouse model of Alzheimer disease

Schröder

Schaffrath

Welter

et al. 2020

J Neuroinflammation

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“…First, the hypothesis calls for MPN-mutation screening studies among patients with AD and in patient populations which we know have an increased risk of AD as well. Second, considering that treatment with interferon-alpha2 (IFN) normalizes elevated blood cell counts within weeks in the large majority of patients with early stage MPNs (ET, PV, and hyperproliferative myelofibrosis) [63] and interferon-beta most recently has shown potent anti-inflammatory activity in concert with improvement in cognitive function in AD patients [64] and in a rat model [65], studies of the safety and efficacy of interferon-alpha or beta in a larger series of AD patients, preferentially those with early stage disease, might be timely and relevant taking into account that no agents so far have been able to revert disease activity in this devastating disease. Of note, IFN treatment may also impact key factors of utmost pathogenetic importance for AD development, including downregulation of upregulated oxidative stress genes and upregulation of downregulated antioxidative defence genes [66].…”

Section: Discussionmentioning

confidence: 99%

Myeloproliferative blood cancers as a human neuroinflammation model for development of Alzheimer’s disease: evidences and perspectives

Hasselbalch

Skov

Kjær

et al. 2020

J Neuroinflammation

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Chronic inflammation and involvement of myeloid blood cells are associated with the development of Alzheimer's disease (AD). Chronic inflammation is a highly important driving force for the development and progression of the chronic myeloproliferative blood cancers (MPNs), which are characterized by repeated thrombotic episodes years before MPN-diagnosis, being elicited by elevated erythrocytes, leukocytes, and platelets. Mutations in blood cells, the JAK2V617F and TET2-mutations, contribute to the inflammatory and thrombogenic state. Herein, we discuss the MPNs as a human neuroinflammation model for AD development, taking into account the many shared cellular mechanisms for reduction in cerebral blood, including capillary stalling with plugging of blood cells in the cerebral microcirculation. The therapeutic consequences of an association between MPNs and AD are immense, including reduction in elevated cell counts by interferon-alpha2 or hydroxyurea and targeting the chronic inflammatory state by JAK1-2 inhibitors, e.g., ruxolitinib, in the future treatment of AD.

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“…Aβ acts as danger associated molecular patterns (DAMP) which can bind to different DAMP-receptors, among FPR, which are expressed by microglia and astrocytes (13,14,25,27). Aß binding to its receptors induced the expression of various pro-inflammatory mediators (68). In addition, Aβ has been shown to be cleared by microglia in vitro and in vivo through receptor-mediated phagocytosis and degradation (69,70).…”

Section: Discussionmentioning

confidence: 99%

Inhibition of formyl peptide receptors improves the outcome in a mouse model of Alzheimer disease

Schröder

Schaffrath

Welter

et al. 2020

Preprint

View full text Add to dashboard Cite

Background: An important hallmark of Alzheimer's disease (AD) is the increase of Aβ1-42 burden and its accumulation to senile plaques, leading the reactive gliosis and neurodegeneration. The modulation of glia cell function represent an attractive therapeutic strategy, but is currently limited by an incomplete understanding of its relevance for AD. The chemotactic G-protein coupled formyl peptide receptor (FPR), which is known to modulate Aβ1-42 uptake and signal transduction, might be one candidate molecule regulating glia function in AD. Here, we investigate whether the modulation of FPR exerts beneficial effects in an AD preclinical model. Methods: To address this question, APP/PS1 double-transgenic AD mice were treated for 20-weeks with either the pro-inflammatory FPR agonist fMLF, the FPR1/2 antagonist Boc2 or the anti-inflammatory FPR2 agonist Ac2-26. Spatial learning and memory were evaluated using a Morris water maze test. Immunohistological staining, gene expression studies and flow cytometry analyses were performed to study neuronal loss, gliosis and Aß-load in the hippocampus and cortex, respectively. Results: FPR antagonism by Boc2-treatment significantly improved spatial memory performance, reduced neuronal pathology, induced the expression of homeostatic growth factors, and ameliorated microglia, but not astrocyte, reactivity. Furthermore, the elevated levels of amyloid plaques in the hippocampus were reduced by Boc2-treatment, presumably by an induction of amyloid degradation. Conclusions: We suggest that the modulation of FPR signaling cascades might be considered as a promising therapeutic approach for alleviating the cognitive deficits associated with early AD. Additional studies are now needed to address the downstream effectors as well as the safety profile of Boc2.

show abstract

Anti-inflammatory and cognitive effects of interferon-β1a (IFNβ1a) in a rat model of Alzheimer’s disease

Cited by 67 publications

References 74 publications

Inhibition of formyl peptide receptors improves the outcome in a mouse model of Alzheimer disease

Inhibition of formyl peptide receptors improves the outcome in a mouse model of Alzheimer disease

Myeloproliferative blood cancers as a human neuroinflammation model for development of Alzheimer’s disease: evidences and perspectives

Inhibition of formyl peptide receptors improves the outcome in a mouse model of Alzheimer disease

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