Suppression of HIV replication in vitro by CpG and CpG conjugated to the non toxic B subunit of cholera toxin

Nowroozalizadeh, Salma; Jansson, Marianne; Adamsson, Jenni; Lindblad, Marianne; Fenyö, Eva Maria; Holmgren, Jan; Harandi, Ali M

Suppression of HIV replication in vitro by CpG and CpG conjugated to the non toxic B subunit of cholera toxin

Mark

Nowroozalizadeh, Salma ^LU ; Jansson, Marianne ^LU ; Adamsson, Jenni ; Lindblad, Marianne ; Fenyö, Eva Maria ^LU ; Holmgren, Jan and Harandi, Ali M (2008) In Current HIV Research 6(3). p.230-238

Abstract: Administration of oligodeoxynucleotides (ODNs) containing CpG motifs generates a rapid and potent response of CC-chemokines, known as ligands of the HIV-1 co-receptor CCR5, in the murine female genital tract. The present study explored the potential HIV inhibitory activities of different human CpG prototypes either alone or conjugated to the non-toxic subunit of cholera toxin (CTB). Results showed that in vitro replication of both HIV-1 and HIV-2 can be suppressed by different human CpG prototypes. Importantly, the conjugation of CpG ODN to CTB (CTB-CpG) enhanced the antiviral activity of CpG against primary HIV-1 isolates of both R5 and X4 phenotypes in peripheral blood mononuclear cells (PBMC) as well as U87.CD4 co-receptor indicator... (More); Administration of oligodeoxynucleotides (ODNs) containing CpG motifs generates a rapid and potent response of CC-chemokines, known as ligands of the HIV-1 co-receptor CCR5, in the murine female genital tract. The present study explored the potential HIV inhibitory activities of different human CpG prototypes either alone or conjugated to the non-toxic subunit of cholera toxin (CTB). Results showed that in vitro replication of both HIV-1 and HIV-2 can be suppressed by different human CpG prototypes. Importantly, the conjugation of CpG ODN to CTB (CTB-CpG) enhanced the antiviral activity of CpG against primary HIV-1 isolates of both R5 and X4 phenotypes in peripheral blood mononuclear cells (PBMC) as well as U87.CD4 co-receptor indicator cells. CTB-CpGs triggered higher amounts of MIP-1 alpha, and MIP-1 beta in PBMC than the corresponding CpG ODNs, which may explain the superior antiviral effect of CTB-CpG against R5 virus in PBMC. Incubation of PBMC with CpG ODN and CTB-CpG did not alter surface expression of HIV-1 receptors indicating that the observed anti-HIV-1 effect is not mediated through down regulation of HIV-1 receptors on target cells. Further, the enhanced antiviral effect of CTB-CpG was dependent on the presence of phosphorothioate backbone in the ODN, whereas the presence of CpG motif in ODNs was dispensable. These results have implications for the development of novel intervention strategies to prevent HIV infection. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1191479

author

Nowroozalizadeh, Salma ^LU ; Jansson, Marianne ^LU ; Adamsson, Jenni ; Lindblad, Marianne ; Fenyö, Eva Maria ^LU ; Holmgren, Jan and Harandi, Ali M

organization

Division of Medical Microbiology

publishing date

2008

type

Contribution to journal

publication status

published

subject

Microbiology in the medical area

keywords

chemokines, CTB, CpG, HIV, antivirals

in

Current HIV Research

volume

6

issue

3

pages

230 - 238

publisher

Bentham Science Publishers

external identifiers

wos:000256616100006
scopus:47749130824

ISSN

1570-162X

DOI

10.2174/157016208784325038

language

English

LU publication?

yes

id

9f375707-5703-4b55-834d-b8d9165917ff (old id 1191479)

date added to LUP

2016-04-01 12:20:36

date last changed

2022-01-27 02:18:51

@article{9f375707-5703-4b55-834d-b8d9165917ff,
  abstract     = {{Administration of oligodeoxynucleotides (ODNs) containing CpG motifs generates a rapid and potent response of CC-chemokines, known as ligands of the HIV-1 co-receptor CCR5, in the murine female genital tract. The present study explored the potential HIV inhibitory activities of different human CpG prototypes either alone or conjugated to the non-toxic subunit of cholera toxin (CTB). Results showed that in vitro replication of both HIV-1 and HIV-2 can be suppressed by different human CpG prototypes. Importantly, the conjugation of CpG ODN to CTB (CTB-CpG) enhanced the antiviral activity of CpG against primary HIV-1 isolates of both R5 and X4 phenotypes in peripheral blood mononuclear cells (PBMC) as well as U87.CD4 co-receptor indicator cells. CTB-CpGs triggered higher amounts of MIP-1 alpha, and MIP-1 beta in PBMC than the corresponding CpG ODNs, which may explain the superior antiviral effect of CTB-CpG against R5 virus in PBMC. Incubation of PBMC with CpG ODN and CTB-CpG did not alter surface expression of HIV-1 receptors indicating that the observed anti-HIV-1 effect is not mediated through down regulation of HIV-1 receptors on target cells. Further, the enhanced antiviral effect of CTB-CpG was dependent on the presence of phosphorothioate backbone in the ODN, whereas the presence of CpG motif in ODNs was dispensable. These results have implications for the development of novel intervention strategies to prevent HIV infection.}},
  author       = {{Nowroozalizadeh, Salma and Jansson, Marianne and Adamsson, Jenni and Lindblad, Marianne and Fenyö, Eva Maria and Holmgren, Jan and Harandi, Ali M}},
  issn         = {{1570-162X}},
  keywords     = {{chemokines; CTB; CpG; HIV; antivirals}},
  language     = {{eng}},
  number       = {{3}},
  pages        = {{230--238}},
  publisher    = {{Bentham Science Publishers}},
  series       = {{Current HIV Research}},
  title        = {{Suppression of HIV replication in vitro by CpG and CpG conjugated to the non toxic B subunit of cholera toxin}},
  url          = {{http://dx.doi.org/10.2174/157016208784325038}},
  doi          = {{10.2174/157016208784325038}},
  volume       = {{6}},
  year         = {{2008}},
}

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Suppression of HIV replication in vitro by CpG and CpG conjugated to the non toxic B subunit of cholera toxin