PDE7 inhibitor TC3.6 ameliorates symptomatology in a model of primary progressive multiple sclerosis
Abstract
Background and PurposecAMP plays an important role in the transduction of signalling pathways involved in neuroprotection and immune regulation. Control of the levels of this nucleotide by inhibition of cAMP-specific PDEs such as PDE7 may affect the pathological processes of neuroinflammatory diseases like multiple sclerosis (MS). In the present study, we evaluated the therapeutic potential of the selective PDE7 inhibitor, TC3.6, in a model of primary progressive multiple sclerosis (PPMS), a rare and severe variant of MS. Experimental ApproachTheiler's murine encephalomyelitis virus-induced demyelinated disease (TMEV-IDD) is one of the models used to validate the therapeutic efficacy of new drugs in MS. As recent studies have analysed the effect of PDE7 inhibitors in the EAE model of MS, here the TMEV-IDD model was used to test their efficacy in a progressive variant of MS. Mice were subjected to two protocols of TC3.6 administration: on the pre-symptomatic phase and once the disease was established. Key ResultsTreatment with TC3.6 ameliorated the disease course and improved motor deficits of infected mice. This was associated with down-regulation of microglial activation and reduced cellular infiltrates. Decreased expression of pro-inflammatory mediators such as COX-2 and the cytokines, IL-1, TNF-, IFN- and IL-6 in the spinal cord of TMEV-infected mice was also observed after TC3.6 administration. ConclusionThese findings support the importance of PDE7 inhibitors, and specifically TC3.6, as a novel class of agents with therapeutic potential for PPMS. Preclinical studies are needed to determine whether their effects translate into durable clinical benefits.
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Título según WOS: | ID WOS:000359295200005 Not found in local WOS DB |
Título de la Revista: | BRITISH JOURNAL OF PHARMACOLOGY |
Volumen: | 172 |
Número: | 17 |
Editorial: | WILEY-BLACKWELL |
Fecha de publicación: | 2015 |
Página de inicio: | 4277 |
Página final: | 4290 |
DOI: |
10.1111/bph.13192 |
Notas: | ISI |