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      Network-based therapeutic approach for brain ischemia: A broad therapy for a specific patient

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            Abstract

            Despite years of efforts, translational stroke research has yield to no neuroprotective therapy. Moreover, only single-drug targets remain hitherto being pursued whilst we know that complex diseases are defined by multitarget modules which should be tackled simultaneously ( Fig. 1A). Therefore, we here propose a network-based approach for multi-target identification based on human disease genes linked to ischemic stroke, in combination with a network pharmacology, drug repurposing therapeutic approach. Indeed, network pharmacology exploits this concept by simultaneously targeting several components of an impaired signalling pathway, using mechanistically related and thus synergistic drugs with a maximal therapeutic effect. Upon stroke, the proposed in silico-based network pharmacology therapy significantly improved reduced infarct volume in line with improved neuro-motor functioning until 14 days after stroke induction ( Fig. 1B-C). RNA sequencing and subsequent gene set enrichment analysis revealed an upregulation of genes modulating synaptic plasticity, while neuroinflammatory and infiltration-related pathways were significantly downregulated ( Fig. 1D). In line with these findings, histological assessment confirmed a reduced neuronal cell death, astrogliosis, microglia activation in the penumbra. This blood-brain barrier stabilising effect was associated with a diminished abundance of infiltrated immune cells during the sub-acute phase after cerebral ischaemia and furthermore decreased concentration of pro-inflammatory cytokines such as TNF-α and GM-CSF in treated animals. However, it remains evident that not all stroke patients suffer from the same dysregulated mechanisms upon stroke. Then, we propose to combine a network pharmacology therapeutic approach with diagnostic endothenotyping of patients who could maximally benefit from our proposed therapy; thus ensuring a personalised, mechanism-based, synergistic therapy with a quick access to the pharmaceutic market.

            Content

            Author and article information

            Conference
            RExPO Conference Series
            REPO4EU
            10 May 2024
            Affiliations
            [1 ] University Hospital Essen ( https://ror.org/02na8dn90)
            [2 ] Maastricht University ( https://ror.org/02jz4aj89)
            Author notes
            Author information
            https://orcid.org/0000-0002-0935-074X
            Article
            10.58647/REXPO.24000061.v4
            47553695-e7ec-45a1-83f9-7f82410c8d79

            This work has been published open access under Creative Commons Attribution License CC BY 4.0 , which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. Conditions, terms of use and publishing policy can be found at www.scienceopen.com .

            RExPO24
            3
            Munich, Germany
            3-5 July 2024
            History
            : 3 May 2024
            Categories

            The datasets generated during and/or analysed during the current study are available from the corresponding author on reasonable request.
            Pharmacology & Pharmaceutical medicine
            Brain ischemia,Network pharmacology,Drug repurposing,Disease module,Synergy

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