Infectious rotavirus enters cells by direct cell membrane penetration, not by endocytosis.

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J Virol. 1988 April; 62(4): 1136-1144

Infectious rotavirus enters cells by direct cell membrane penetration, not by endocytosis.

K T Kaljot, R D Shaw, D H Rubin and H B Greenberg

Department of Medicine, Stanford University School of Medicine, California 95305.

ABSTRACT

Rotaviruses are icosahedral viruses with a segmented, double-strandedRNA genome. They are the major cause of severe infantile infectiousdiarrhea. Rotavirus growth in tissue culture is markedly enhancedby pretreatment of virus with trypsin. Trypsin activation isassociated with cleavage of the viral hemagglutinin (viral protein3 [VP3]; 88 kilodaltons) into two fragments (60 and 28 kilodaltons).The mechanism by which proteolytic cleavage leads to enhancedgrowth is unknown. Cleavage of VP3 does not alter viral bindingto cell monolayers. In previous electron microscopic studiesof infected cell cultures, it has been demonstrated that rotavirusparticles enter cells by both endocytosis and direct cell membranepenetration. To determine whether trypsin treatment affectedrotavirus internalization, we studied the kinetics of entryof infectious rhesus rotavirus (RRV) into MA104 cells. Trypsin-activatedRRV was internalized with a half-time of 3 to 5 min, while nonactivatedvirus disappeared from the cell surface with a half-time of30 to 50 min. In contrast to trypsin-activated RRV, loss ofnonactivated RRV from the cell surface did not result in theappearance of infection, as measured by plaque formation. Endocytosisinhibitors (sodium azide, dinitrophenol) and lysosomotropicagents (ammonium chloride, chloroquine) had a limited effecton the entry of infectious virus into cells. Purified trypsin-activatedRRV added to cell monolayers at pH 7.4 medicated 51Cr, [14C]choline,and [3H]inositol released from prelabeled MA104 cells. Thisrelease could be specifically blocked by neutralizing antibodiesto VP3. These results suggest that MA104 cell infection followsthe rapid entry of trypsin-activated RRV by direct cell membranepenetration. Cell membrane penetration of infectious RRV isinitiated by trypsin cleavage of VP3. Neutralizing antibodiescan inhibit this direct membrane penetration.

J Virol. 1988 April; 62(4): 1136-1144

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