The Nature of the DNA Associated with Incomplete Particles of Adenovirus Type 2

Khittoo, Govindranathsing; Weber, Joseph

doi:10.1099/0022-1317-54-2-343

Cited by 11 publications

(7 citation statements)

References 11 publications

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“…In addition to the empty capsids that lack any DNA, two classes of assembly intermediates, called light and heavy, exist in virus-infected cells. The light assembly intermediates are associated with DNA fragments derived from the left end of viral genome (Daniell, 1976 ; Khittoo and Weber, 1981 ). Interestingly, the light intermediates range in density from 1.29 g/cm 3 (empty capsids) to 1.34 g/cm 3 (mature virions), with longer DNA fragments associated with the particles of higher densities (Tibbetts, 1977 ).…”

Section: Evidence For Sequential Assembly Of Advmentioning

confidence: 99%

Components of Adenovirus Genome Packaging

Ahi

Mittal

2016

Front. Microbiol.

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Adenoviruses (AdVs) are icosahedral viruses with double-stranded DNA (dsDNA) genomes. Genome packaging in AdV is thought to be similar to that seen in dsDNA containing icosahedral bacteriophages and herpesviruses. Specific recognition of the AdV genome is mediated by a packaging domain located close to the left end of the viral genome and is mediated by the viral packaging machinery. Our understanding of the role of various components of the viral packaging machinery in AdV genome packaging has greatly advanced in recent years. Characterization of empty capsids assembled in the absence of one or more components involved in packaging, identification of the unique vertex, and demonstration of the role of IVa2, the putative packaging ATPase, in genome packaging have provided compelling evidence that AdVs follow a sequential assembly pathway. This review provides a detailed discussion on the functions of the various viral and cellular factors involved in AdV genome packaging. We conclude by briefly discussing the roles of the empty capsids, assembly intermediates, scaffolding proteins, portal vertex and DNA encapsidating enzymes in AdV assembly and packaging.

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Section: Evidence For Sequential Assembly Of Advmentioning

confidence: 99%

Components of Adenovirus Genome Packaging

Ahi

Mittal

2016

Front. Microbiol.

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“…In view of the findings of Hammarskjold & Winberg (1980), that packaging of Ad 16 DNA is dependent on a sequence at the left end of the genome, it is not surprising that the discrete fragments from IP contain only left end sequences. Tibbetts (1977) and Khittoo & Weber (1981) suggested that IP-containing left end fragments may be assembly intermediates whose unprotected DNA was digested during purification, leaving the left end sequences protected within the capsid. An alternative theory is that subgenomic fragments are generated in infected cells from both ends of the genome and that the left end fragments are selectively packaged (Daniell & Mullenbach, 1978).…”

Section: Discussionmentioning

confidence: 99%

“…IP containing subgenomic DNA have been reported for a subgroup A adenovirus serotype 12 (Adl2) (Burlingham et al, 1974), subgroup B serotypes 3, 7 and 16 (Prage et al, 1972;Daniell, 1976;Hammarskjold et al, 1977;Tibbetts, 1977;Hammarskjold & Winberg, 1980) and subgroup C serotype 2 (Burlingham et al, 1974;Daniell, 1976;Khittoo & Weber, 1981). Group B adenoviruses produce large quantities of incomplete particles and analysis of the DNA by gel electrophoresis has shown that it is more heterogeneous in size than the DNA from IP of Ad2 (Daniell, 1976;Tibbetts, 1977;Hammarskjold & Winberg, 1980).…”

Section: Introductionmentioning

confidence: 99%

“…Group B adenoviruses produce large quantities of incomplete particles and analysis of the DNA by gel electrophoresis has shown that it is more heterogeneous in size than the DNA from IP of Ad2 (Daniell, 1976;Tibbetts, 1977;Hammarskjold & Winberg, 1980). Restriction endonuclease analysis and blot hybridization experiments have shown that subgenomic DNA from IP originates from the left end of the genome (Daniell, 1976;Tibbetts, 1977;Hammarskjold & Winberg, 1980;Khittoo & Weber, 1981), whereas DNA from cells infected with Ad2, Ad3 or Ad 16 mapped to both left and right ends of the genome (Hammarskjold & Winberg, 1980;Daniell & Mullenbach, 1978;Rajagopalan & Chinnadurai, 1979). This suggested that a sequence at the left end of the genome may be involved in encapsidation.…”

Section: Introductionmentioning

confidence: 99%

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Discrete Subgenomic DNA Fragments in Incomplete Particles of Adenovirus Type 2

Brown

Weber

1982

Journal of General Virology

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SUMMARYDiscrete subgenomic DNA fragments were found in three out of thirty-two preparations of adenovirus type 2 incomplete particles grown in human Hep-2 cells and examined over the course of 1 year. One preparation contained three fragments corresponding to 5, 14 and 19 % of the genome, another contained a 37 % fragment and the third a 40% fragment. Each fragment hybridized exclusively to the left end of the genome. Digestion of the nick-translated 37% fragment with HindIII confirmed that it contained the 1eft 37.3% of the genome. Synthesis of these fragments was not dependent on high input multiplicity of infection. Comparable fragments were not found in unpackaged DNA from the corresponding infected cells. This is consistent with the hypothesis that such fragments are generated during virus assembly or, alternatively, may reflect the very small proportion of these fragments relative to the pool of unpackaged DNA within the cells. The possibility that they are generated by errors in DNA replication is discussed.

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“…During the late phase of infection, pulse-labelling experiments suggest that many of these proteins are first assembled into empty shell precursor particles called top components (TC) due to their light density in equilibrium gradients (Ishibashi & Maizel, 1974;Rosenwirth et al, 1974). Such particles contain proteins II, III, Ilia, IV, V, PVI, PVIII, IX and very little DNA (Edvardsson et al, 1976;Khittoo & Weber, 1977, 1981Persson et al, 1979). In addition to evidence from pulse-chase experiments, the following suggest that TC are precursors to complete virions: (i) several temperature-sensitive (ts) mutants (2ts4, 2ts112, 2tsl01, 5ts58) accumulate TC; (ii) TC contain precursor proteins (PVI, PVIII); (iii) the TC accumulated by some mutants can be chased into complete virions (Chee-Sheung & Ginsberg, 1982;D'Halluin et al, 1978).…”

mentioning

confidence: 99%

The Role of Phosphorylation and Core Protein V in Adenovirus Assembly

Weber¹,

Khittoo²

1983

Journal of General Virology

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SUMMARYThe role of phosphorylation and the minor core protein V in adenovirus type 2 assembly was examined. Comparison of the phosphoprotcin composition of top components (TC), young virions and mature virions of wild-type and assembly mutants showed specific changcs related to virus assembly and maturation. TC were identified as precursors of young virions which contain two molccular weight forms of core protein V, one of which is phosphorylatcd. Conversion of TC into young virions by DNA encapsidation resulted in the loss of the unphosphorylated form of protein V, and subsequent maturation to old virions resulted in thc dephosphorylation of the core protein. This last step is blocked by the tsl mutation which inactivates the viral endoproteinase.

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The Nature of the DNA Associated with Incomplete Particles of Adenovirus Type 2

Cited by 11 publications

References 11 publications

Components of Adenovirus Genome Packaging

Components of Adenovirus Genome Packaging

Discrete Subgenomic DNA Fragments in Incomplete Particles of Adenovirus Type 2

The Role of Phosphorylation and Core Protein V in Adenovirus Assembly

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