Both methods present advantages and disadvantages. In solid pieces of tissue, neurones are mixed together Crizotinib with glial populations, which could help the maturation of the tissue in the host brain [145]. Importantly, with the latter approach, cells do not undergo mechanical stress, trauma or necrosis due to axotomy, although cell death may still occur upon dissection
of the tissue [146]. On the other hand, cell suspensions, which require the mechanical dissociation of the tissue with potential accompanying cell damage, are surgically easier to implant in the brain. Dissociated cells are also more likely to be integrated in the host brain and to form afferent and efferent connections with the latter [147]. However, the trituration of the tissue leads to the destruction of the donor vasculature leaving the graft to rely strictly on the vascular supply of the host [90,148,149]. Solid pieces Pexidartinib in vivo of tissue maintain their own angioarchitecture and will more readily anastomose with surrounding vessels [114,148,150,151]. Finally, cell suspensions trigger a weaker inflammatory response, in part because they are injected through a smaller cannula than solid grafts [139]. In clinical trials, the cell suspensions utilized were not completely dissociated and small clusters of cells were maintained, introducing a source of variability with regard to the effective number of cells implanted
between transplants. However, the method of cell suspension seems to yield a better outcome [139]. The regime of immunosuppression is another parameter that may be predictive of graft outcome and one that is intermingled with the cellular and molecular immune/inflammatory responses against grafted tissue (Table 1).
The early work on transplantation in animal models of disease demonstrated that the long-term survival of dopaminergic xenografts (mouse to rat and human to rat) was improved when the immunosuppressive drug cyclosporine A was administered to the recipient animal, even for a short period of time [152,153]. However, halting cyclosporine treatment reduced functional effects of grafted tissue at later time points (6 months), although the improvement of the behavioural phenotype of the immunosuppressed animals was still greater than in non-immunosuppressed Tyrosine-protein kinase BLK animals [154]. Clinically, the withdrawal of immunosuppression coincided with the decline of beneficial effects in PD patients [155]. It was suggested that this could reflect graft rejection, although grafts survival was confirmed both by PET scans of Fluoro-dopa uptake and later by post-mortem histological analysis [155], similarly to previous reports [156]. In other PD cases, the withdrawal of the immunotherapy treatment did not lead to graft rejection [157,158]. Two independent reports have further described grafts survival in the absence of any immunosuppressive treatment [109,159].