Literature DB >> 6495658

Recombination in adenovirus: analysis of crossover sites in intertypic overlap recombinants.

V Mautner, N Mackay.   

Abstract

Overlap recombination has been used as a means of generating intertypic recombinants with crossover sites located within a defined region of the adenovirus genome. Using terminal DNA fragments of adenovirus type 2 and type 5 that overlap within the vicinity of the hexon coding region (51.6-59.7 map units), two different crosses could be studied; in one the overlap entirely encompasses the hexon and there are homologous regions at either side of the overlap where recombination is expected, and in the other only one side of the overlap is capable of sustaining recombination. The overall distribution of crossover sites within the overlap has been determined by restriction endonuclease mapping, and analysed in terms of the extent of homology between Ad2 and Ad5 in this region as defined by the DNA sequences (R. Kinloch, N. Mackay, and V. Mautner (1984). J. Biol. Chem., 259, 6431-6436; G. Akusjärvi, P. Aleström, M. Pettersson, M. Lager, H. Jörnvall, and U. Pettersson (1984). Submitted). Crossovers are found only in regions of relatively high DNA homology, as previously shown for intertypic recombination between temperature-sensitive viruses (M. E. G. Boursnell and V. Mautner (1981). Virology 112, 198-209). The presence of a free DNA end within the heterologous zone is insufficient to overcome the barrier to recombination. In crosses where recombination is confined to a relatively small homologous zone (45.9-53.0 mu) there is no special distribution of crossovers within the interval; no "hot spot" is discernible at the free DNA end, suggesting that a free DNA end is not especially recombinogenic, nor at the junction between the homologous and heterologous zones, suggesting that branch migration up to the heterology does not always occur. A cross designed to furnish evidence for gene conversion gave rise to a "conventional" recombinant with a crossover located within a 21-nucleotide tract of homology.

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Year:  1984        PMID: 6495658     DOI: 10.1016/0042-6822(84)90328-3

Source DB:  PubMed          Journal:  Virology        ISSN: 0042-6822            Impact factor:   3.616


  8 in total

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2.  Computational analysis of human adenovirus type 22 provides evidence for recombination among species D human adenoviruses in the penton base gene.

Authors:  Christopher M Robinson; Jaya Rajaiya; Michael P Walsh; Donald Seto; David W Dyer; Morris S Jones; James Chodosh
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3.  Differential effects of base-pair mismatch on intrachromosomal versus extrachromosomal recombination in mouse cells.

Authors:  A S Waldman; R M Liskay
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4.  Topological requirements for homologous recombination among DNA molecules transfected into mammalian cells.

Authors:  C T Wake; F Vernaleone; J H Wilson
Journal:  Mol Cell Biol       Date:  1985-08       Impact factor: 4.272

5.  Homologous recombination of monkey alpha-satellite repeats in an in vitro simian virus 40 replication system: possible association of recombination with DNA replication.

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6.  Sensitive analysis of genetic heterogeneity of adenovirus types 3 and 7 in the Soviet Union.

Authors:  G I Golovina; F N Zolotaryov; T I Yurlova
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7.  Applying genomic and bioinformatic resources to human adenovirus genomes for use in vaccine development and for applications in vector development for gene delivery.

Authors:  Jason Seto; Michael P Walsh; Padmanabhan Mahadevan; Qiwei Zhang; Donald Seto
Journal:  Viruses       Date:  2010-01-06       Impact factor: 5.818

8.  Genomic analyses of human adenoviruses unravel novel recombinant genotypes associated with severe infections in pediatric patients.

Authors:  Joyce Odeke Akello; Richard Kamgang; Maria Teresa Barbani; Franziska Suter-Riniker; Christoph Aebi; Christian Beuret; Daniel H Paris; Stephen L Leib; Alban Ramette
Journal:  Sci Rep       Date:  2021-12-15       Impact factor: 4.379

  8 in total

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