MUTATIONS IN THE CYTOPLASMIC DOMAIN OF THE FUSION GLYCOPROTEIN OF NEWCASTLE-DISEASE VIRUS DEPRESS SYNCYTIA FORMATION

被引：49

作者：

SERGEL, T ^{[1
]}

MORRISON, TG ^{[1
]}

机构：

[1] UNIV MASSACHUSETTS,SCH MED,DEPT MOLEC GENET & MICROBIOL,WORCESTER,MA 01655

来源：

VIROLOGY | 1995年 / 210卷 / 02期

关键词：

D O I：

10.1006/viro.1995.1343

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

The role of the cytoplasmic domain of the Newcastle disease virus fusion protein in syncytia formation was explored by characterizing the intracellular processing and activities of proteins with deletions and point mutations in this region. Deletion of the entire domain (amino acids 523 to 553) resulted in a protein which was minimally proteolytically cleaved and had no syncytia forming activity. Deletion of the carboxy terminal half of the domain (amino acids 540 to 553) resulted in a protein that was normally processed but had no syncytia forming activity. Deletion of amino acids 547 to 553 resulted in a protein with approximately 30% wild-type levels of activity while deletion of amino acids 550 to 553 yielded a protein with wild-type activity. The results suggested that amino acids 540 to 550 are important for syncytia formation and this conclusion was supported by two internal deletions as well as point mutations in this region. Mutation of two cysteine residues in and adjacent to the transmembrane domain, which are potential sites for fatty acid acylation, had no effect on syncytia formation either singly or in combination. (C) 1995 Academic Press, Inc.

引用

页码：264 / 272

页数：9

共 36 条

[1]

BRODY BA, 1993, J VIROL, V68, P4620

[2] A LEUCINE ZIPPER STRUCTURE PRESENT IN THE MEASLES-VIRUS FUSION PROTEIN IS NOT REQUIRED FOR ITS TETRAMERIZATION BUT IS ESSENTIAL FOR FUSION [J].

BUCKLAND, R ;

MALVOISIN, E ;

BEAUVERGER, P ;

WILD, F .

JOURNAL OF GENERAL VIROLOGY, 1992, 73 :1703-1707

[3] CELL-FUSION BY THE ENVELOPE GLYCOPROTEINS OF PERSISTENT MEASLES VIRUSES WHICH CAUSED LETHAL HUMAN BRAIN DISEASE [J].

CATTANEO, R ;

ROSE, JK .

JOURNAL OF VIROLOGY, 1993, 67 (03) :1493-1502

[4] THE CYTOPLASMIC DOMAIN OF SIMIAN IMMUNODEFICIENCY VIRUS TRANSMEMBRANE PROTEIN MODULATES INFECTIVITY [J].

CHAKRABARTI, L ;

EMERMAN, M ;

TIOLLAIS, P ;

SONIGO, P .

JOURNAL OF VIROLOGY, 1989, 63 (10) :4395-4403

[5] HEPTAD REPEAT SEQUENCES ARE LOCATED ADJACENT TO HYDROPHOBIC REGIONS IN SEVERAL TYPES OF VIRUS FUSION GLYCOPROTEINS [J].

CHAMBERS, P ;

PRINGLE, CR ;

EASTON, AJ .

JOURNAL OF GENERAL VIROLOGY, 1990, 71 :3075-3080

[6] FATTY-ACID MODIFICATION OF NEWCASTLE-DISEASE VIRUS GLYCOPROTEINS [J].

CHATIS, PA ;

MORRISON, TG .

JOURNAL OF VIROLOGY, 1982, 43 (01) :342-347

[7] TRUNCATION OF THE HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 TRANSMEMBRANE GLYCOPROTEIN CYTOPLASMIC DOMAIN BLOCKS VIRUS INFECTIVITY [J].

DUBAY, JW ;

ROBERTS, SJ ;

HAHN, BH ;

HUNTER, E .

JOURNAL OF VIROLOGY, 1992, 66 (11) :6616-6625

[8] SIV ADAPTION TO HUMAN-CELLS [J].

HIRSCH, VM ;

EDMONDSON, P ;

MURPHEYCORB, M ;

ARBEILLE, B ;

JOHNSON, PR ;

MULLINS, JI .

NATURE, 1989, 341 (6243) :573-574

[9] STUDIES ON THE FUSION PEPTIDE OF A PARAMYXOVIRUS FUSION GLYCOPROTEIN - ROLES OF CONSERVED RESIDUES IN CELL-FUSION [J].

HORVATH, CM ;

LAMB, RA .

JOURNAL OF VIROLOGY, 1992, 66 (04) :2443-2455

[10]

KOCH N, 1986, J BIOL CHEM, V261, P3434

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