Novel replication-incompetent adenoviral B-group vectors: high vector stability and yield in PER.C6 cells.

نویسندگان

  • M Havenga
  • R Vogels
  • D Zuijdgeest
  • K Radosevic
  • S Mueller
  • M Sieuwerts
  • F Weichold
  • I Damen
  • J Kaspers
  • A Lemckert
  • M van Meerendonk
  • R van der Vlugt
  • L Holterman
  • D Hone
  • Y Skeiky
  • R Mintardjo
  • G Gillissen
  • D Barouch
  • J Sadoff
  • J Goudsmit
چکیده

Adenoviral vectors based on adenovirus type 35 (rAd35) have the advantage of low natural vector immunity and induce strong, insert-specific T- and B-cell responses, making them prime-candidate vaccine carriers. However, severe vector-genome instability of E1-deleted rAd35 vectors was observed, hampering universal use. The instability of E1-deleted rAd35 vector proved to be caused by low pIX expression induced by removal of the pIX promoter, which was located in the E1B region of B-group viruses. Reinsertion of a minimal pIX promoter resulted in stable vectors able to harbour large DNA inserts (> 5 kb). In addition, it is shown that replacement of the E4-Orf6 region of Ad35 by the E4-Orf6 region of Ad5 resulted in successful propagation of an E1-deleted rAd35 vector on existing E1-complementing cell lines, such as PER.C6 cells. The ability to produce these carriers on PER.C6 contributes significantly to the scale of manufacturing of rAd35-based vaccines. Next, a stable rAd35 vaccine was generated carrying Mycobacterium tuberculosis antigens Ag85A, Ag85B and TB10.4. The antigens were fused directly, resulting in expression of a single polyprotein. This vaccine induced dose-dependent CD4+ and CD8+ T-cell responses against multiple antigens in mice. It is concluded that the described improvements to the rAd35 vector contribute significantly to the further development of rAd35 carriers for mass-vaccination programmes for diseases such as tuberculosis, AIDS and malaria.

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عنوان ژورنال:
  • The Journal of general virology

دوره 87 Pt 8  شماره 

صفحات  -

تاریخ انتشار 2006