**4.1. Transport of cargoes**

In RanGTPase system, Ran-binding protein 1 (RanBP1) which is cytoplasmic localized binds RanGTP and eases the RanGAP-dependent conversion of RanGTP to RanGDP [29]. This indicates that RanBP1 catalyses the cytoplasmic disassembly of RanGTP–transport receptor complexes. These complexes are kinetically so stable that RanGAP alone fails to trigger GTP hydrolysis [30-32]. RanBP2 [33] is a major constituent of the cytoplasmic filaments of NPCs and exhibits similar functions as RanBP1. It has four RanBP1 homology domains and forms a stable complex with sumoylated RanGAP [34,35], in order to dismantle the RanGTP–transport receptor complexes that exit the nucleus. Importin- and exportin-mediated transport cycles can accumulate cargoes against gradients of chemical activity, which is an energy-dependent process. The RanGTPase system hydrolyses one GTP molecule per transport cycle, and a number of evidences suggest that this contains the sole input of metabolic energy [36-39]. We have successfully identified all the required key components in the *T. brucei* nuclear transport. Whether their functionalities *in vivo* are consensus with the known ones still remains to be further investigated.
