Envelope Formation Is Blocked by Mutation of a Sequence Related to the HKD Phospholipid Metabolism Motif in the Vaccinia Virus F13L Protein

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Journal of Virology, February 1999, p. 1108-1117, Vol. 73, No. 2
0022-538X/99/$00.00+0

Envelope Formation Is Blocked by Mutation of a Sequence Related to the HKD Phospholipid Metabolism Motif in the Vaccinia Virus F13L Protein

Rachel L. Roper and Bernard Moss^*

Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases, Bethesda, Maryland 20892-0445

Received 22 July 1998/Accepted 20 October 1998

The outer envelope of the extracellular form of vaccinia virus is derived from Golgi membranes that have been modified bythe insertion of specific viral proteins, of which the major componentis the 37-kDa, palmitylated, nonglycosylated product of the F13Lgene. The F13L protein contains a variant of the HKD (His-Lys-Asp)motif, which is conserved in numerous enzymes of phospholipidmetabolism. Vaccinia virus mutants with a conservative substitutionof either the K (K314R) or the D (D319E) residue of the F13L proteinformed only tiny plaques similar to those produced by an F13Ldeletion mutant, were unable to produce extracellular envelopedvirions, and failed to mediate low-pH-induced fusion of infectedcells. Membrane-wrapped forms of intracellular virus were rarelydetected in electron microscopic images of cells infected witheither of the mutants. Western blotting and pulse-chase experimentsdemonstrated that the D319E protein was less stable than eitherthe K314R or wild-type F13L protein. Most striking, however, wasthe failure of either of the two mutated proteins to concentratein the Golgi compartment. Palmitylation, oleation, and partitioningof the F13L protein in Triton X-114 detergent were unaffectedby the K314R substitution. These results indicated that the F13Lprotein must retain the K314 and D319 for it to localize in theGolgi compartment and function in membrane envelopment of vacciniavirus.

^* Corresponding author. Mailing address: Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases,Building 4, Room 229, 4 Center Dr. MSC 0445, National Institutesof Health, Bethesda, MD 20892-0445. Phone: (301) 496-9869. Fax:(301) 480-1147. E-mail: bmoss{at}nih.gov.

Journal of Virology, February 1999, p. 1108-1117, Vol. 73, No. 2
0022-538X/99/$00.00+0

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