A dimorphism shift of hepatitis B virus capsids in response to ionic conditions. Academic Article uri icon


  • The dimorphism of HBV capsids (coexistence of T = 3 and T = 4 capsids) was found to be regulatable by controlling the rate of capsid nucleation using cations such as K+ or Ca2+: a quick addition of highly concentrated monovalent and/or multivalent counter-cations resulted in a morphism transition from a thermodynamically more stable, T = 4 capsid-dominant state (>80% of total capsids) to a new state containing 1:1 amounts of T = 3 and T = 4 capsids. These results suggested that the salts with strong charge screening ability could narrow the difference in nucleation energy barriers between the two states, which were not inter-convertible once formed. The effect of salts was more significant than other factors such as pH or protein concentration in achieving such a dimorphism shift. The general mechanism of HBV capsid dimorphism described here provides a new perspective in understanding the virus assembly during infection and directing the design of non-infectious capsids for nanotechnology applications.

published proceedings

  • Nanoscale

author list (cited authors)

  • Sun, X., Li, D., Wang, Z., Liu, Q., Wei, Y., & Liu, T.

citation count

  • 5

complete list of authors

  • Sun, Xinyu||Li, Dong||Wang, Zhaoshuai||Liu, Qiao||Wei, Yinan||Liu, Tianbo

publication date

  • September 2018