**3. Conclusions**

In our present study, protein – peptide docking technique were accomplished to assess the binding orientations of the seven viral targets from Ebola virus with the 25 selected cell penetrating peptide ligands. Each one of the targets was tightly bound to every 25 different types of CPPs with good score. The E-value scores were very much higher than the previously reported docking studies. Moreover, this research concluded that among all ligands, the CL22, A6 and Res1 peptides interacted efficiently with four of the Ebola proteins and would be considered as potent promising antiviral agents. It is anticipated that this study could pave a way for further in vitro and in vivo investigations to discover new approaches and candidates for Ebola drug design and formulation.
