Objective: To describe the characteristics of short interfering double stranded RNA （dsRNA） against hepatitis C virus （HCV） and to find out the determining factors in design for desirable inhibitory efficacy. Methods: The data were collected and analyzed by retrieval of 229 published short dsRNAs designed for degradation of HCV RNA. Results: Statistical analyses showed that the most frequently involved short dsRNAs were directing against 5′NTR/core and genotype 1b

accounting for 64.2% and 69.9%

respectively. Inhibitory efficacy varied with the structural characteristics of short dsRNAs

of which the most potential were those directed against HCV core region with inhibitory efficacy of 70.2%. Moreover

the mean inhibitory efficacy of short dsRNAs with GC contents from 30% to 52% was higher than that of those with GC contents out of this range. Conclusion: Based on this pooled data in a relatively large sample

the present results provided clues to design for short dsRNAs with more potent inhibitory efficacy.