In MS, the precise distribution of different laminin isoforms is reported to be important for integrin-mediated leucocyte extravasation to the active lesion, where ‘perivascular cuffs’ of inflammatory infiltrates
specifically associate with patches of laminin α4 but not laminin α5 expression [347,348]. In the chronic lesion, increased perivascular expression of fibrillar collagens (types I, III and V) and the SLRPs decorin and biglycan was suggested to reduce monocytic expression of the leucocyte attractant chemokine CCL2 (MCP1) [349]. Similarly to the approaches discussed earlier with regards to traumatic CNS injury, manipulating the BMN 673 cost ECM therefore a represents a potential therapeutic strategy to overcome Palbociclib nmr demyelination (recently reviewed in [350]). Indeed, reduction of CSPG synthesis using xyloside, in vivo, was shown to increase OPC and oligodendrocyte numbers in lesions and improve remyelination in a lysolecithin murine model [351]. Thus, there is promise for future studies to apply ECM modification strategies to models
of MS and it will be of great interest to determine whether these strategies can improve disease pathology and lead to functional repair. The ECM plays a critical role during development and following disease or injury to the CNS. Rather than mere provision of a supportive
environment, the ECM is actively involved in many fundamental processes such as cell signalling, axon guidance and synaptic plasticity. Following disease or damage to the CNS, the composition tuclazepam of the ECM can prove detrimental to axonal regeneration, plasticity and repair. Manipulating the ECM represents a powerful therapeutic approach, with the aim of recapitulating beneficial processes that occur during development and/or reducing negative remodelling after injury, either by targeting specific ECM components or by global targeting of families of ECM molecules. There is now much pre-clinical evidence to suggest that beneficial outcomes can be achieved following traumatic brain and spinal cord injury with therapies involving matrix manipulation and encouragingly, some of these strategies are progressing closer to clinical application. We may only be beginning to understand the complexities of ECM interactions in neurodegenerative disorders but it appears that manipulations of the ECM may well have wide applications in future strategies to promote repair following CNS injury or disease. “
“F. Mori, K. Tanji, Y. Miki, A. Kakita, H. Takahashi and K.