Characterization of Tissue Plasminogen Activator Expression and Trafficking in the Adult Murine Brain.
Tamara K StevensonDaniel A LawrencePublished in: eNeuro (2018)
Tissue plasminogen activator (tPA) is an immediate-early gene important for regulating physiological processes like synaptic plasticity and neurovascular coupling. It has also been implicated in several pathological processes including blood-brain barrier (BBB) permeability, seizure progression, and stroke. These varied reports suggest that tPA is a pleiotropic mediator whose actions are highly compartmentalized in space and time. The specific localization of tPA, therefore, can provide useful information about its function. Accordingly, the goal of this study was to provide a detailed characterization of tPA's regional, cellular, and subcellular localization in the brain. To achieve this, two new transgenic mouse lines were utilized: (1) a PlatβGAL reporter mouse, which houses the β-galactosidase gene in the tPA locus and (2) a tPABAC-Cerulean mouse, which has a cerulean-fluorescent protein fused in-frame to the tPA C-terminus. Using these two transgenic reporters, we show that while tPA is expressed throughout most regions of the adult murine brain, it appears to be preferentially targeted to fiber tracts in the limbic system. In the hippocampus, confocal microscopy revealed tPA-Cerulean (tPA-Cer) puncta localized to giant mossy fiber boutons (MFBs) and astrocytes in stratum lucidum. With amplification of the tPA-Cer signal, somatically localized tPA was also observed in the stratum oriens (SO)/alveus layer of both CA1 and CA3 subfields. Coimmunostaining of tPA-Cer and interneuronal markers indicates that these tPA-positive cell bodies belong to a subclass of somatostatin (SST)/oriens-lacunosum moleculare (O-LM) interneurons. Together, these data imply that tPA's localization is differentially regulated, suggesting that its neuromodulatory effects may be compartmentalized and specialized to cell type.
Keyphrases
- blood brain barrier
- cerebral ischemia
- healthcare
- white matter
- poor prognosis
- single cell
- drug delivery
- palliative care
- social media
- multiple sclerosis
- mesenchymal stem cells
- bone marrow
- binding protein
- deep learning
- cognitive impairment
- artificial intelligence
- protein protein
- adverse drug
- genome wide identification
- long non coding rna