As an aside, I wonder how much of the effect seen in heterochronic parabiosis is due to organelle transfer?
I think it would be hard to avoid at least some transfer and thus some benefit to the older rats (and harm to the younger ones), and probably happens with every blood transfusion--
In this study, we demonstrated that isolated mitochondria are internalized into cells by simple co-incubation by using genetically labelled mitochondria. Isolated mitochondria were internalized into homogeneic and xenogeneic cells within a few hours of co-incubation. Furthermore, we observed how mitochondria are engulfed by the recipient cells and how they behave inside the cells after internalization by time-lapse video microscopy. We also showed that optimal mitochondrial internalization significantly improves the mitochondrial function in mtDNA-depleted cells, and that these benefits lasted several days. Finally, we demonstrated the possible involvement of macropinocytosis in this process by using various inhibitors of endocytosis....We confirmed that human mitochondria are transferred into rat cells as well as human cells. However, a complete set of cognate chromosomes was necessary for the maintenance of mitochondrial genomes and functions [24]. Mitochondria have co-evolved with their host cells for ages, that is supposed to lead to species-specific compatibility [25] . Therefore, we only conducted interspecies mitochondrial transfer to validate the process and investigated the therapeutic potential of the process by using homogeneic mitochondria.In previous studies, exogenous mitochondria were maintained in the recipient cells for longer periods [26, 27]. In contrast, our study demonstrated that the internalized mitochondria disappeared within a week. In addition, transmission electron microscopy showed that some exogenous DsRed-labelled mitochondria were identified in the autophagosomes after mitochondrial transfer within recipient cells (Fig. S6). Exogenous mitochondria may be selectively degraded after mitochondrial transfer....In this study, the isolated mitochondria-enriched fraction was used for experiments. This fraction also contained various intracellular organelles such as damaged and dysfunctional mitochondria that are proposed to be of no benefit and even harmful to the host cells [34]. A previous study has also indicated that freshly isolated, intact, viable and respiration-competent mitochondria were required to exert a therapeutic effect [13]. Our experiments also revealed that UV-treated mitochondria failed to improve cellular viability in recipient cells.
Edited by Turnbuckle, 14 January 2015 - 01:39 PM.
