Tumor necrosis factor receptor expression and signal transduction in HIV-1-infected cells

Salvatore T. Butera; Beverly D. Roberts; Kwan Leung; Gary J. Nabel; Thomas M. Folks

Tumor necrosis factor receptor expression and signal transduction in HIV-1-infected cells

Salvatore T. Butera, Beverly D. Roberts, Kwan Leung, Gary J. Nabel, Thomas M. Folks

Research output: Contribution to journal › Article › peer-review

Abstract

Objective: To examine the inter-relationship between HIV-1 infection and the cell surface receptors for tumor necrosis factor (TNF)-α, an immunoregulatory cytokine that can enhance HIV-1 replication. Design: Infected promyelocytic and promonocytic cells were examined because they normally express both types of TNF receptors. Methods: TNF receptor surface expression was determined by specific monoclonal antibody recognition and flow cytometry, and signal transduction was detected by gel shift analysis. HIV-1 activation and expression was quantitated by reverse transcriptase assay. Results: In the OM-10.1 promyelocytic model of chronic infection, TNF-α-induced HIV-1 expression also resulted in a substantial increase in 75 kd TNF receptor (TR75) expression although 55 kD TNF receptor (TR55) levels were not dramatically altered. A series of uninfected parental HL-60 subclones all reduced TR75 surface expression in response to TNF-α treatment. Enhanced TR75 expression on OM-10.1 cells followed the same TNF-α-dose dependency as that observed for HIV-1 production. An increase in TR75 expression was also evident during the peak of an acute HIV-1 infection of HL-60 promyelocytes. Although TR55 expression was unaltered during TNF-α-induced HIV activation, this receptor was still involved in the viral activation process. Antibody cross-linking of TR55, in the absence of exogenous TNF-α, induced maximal HIV-1 expression, an up-modulation of surface TR75, and nuclear NF-NB activity in OM-10.1 cultures. Surprisingly, this was the case even when an antagonistic anti-TR55 antibody was used. Anti-TR55 antibody cross-linking in chronically infected U1 promonocytic cultures could only partially substitute for TNF-α-induced HIV-1 expression. Conclusions: Our results demonstrated that HIV-1 infection can selectively influence the surface expression of TNF receptors, potentially influencing its own expression and altering normal immunoregulatory signal transduction.

Original language	English (US)
Pages (from-to)	911-918
Number of pages	8
Journal	AIDS
Volume	7
Issue number	7
State	Published - 1993
Externally published	Yes

Keywords

Agonistic/antagonistic antibodies
Latent/inducible HIV-1 infection
NF-NB activity
Tumor necrosis factor receptor

ASJC Scopus subject areas

Immunology
Immunology and Allergy

Cite this

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title = "Tumor necrosis factor receptor expression and signal transduction in HIV-1-infected cells",

abstract = "Objective: To examine the inter-relationship between HIV-1 infection and the cell surface receptors for tumor necrosis factor (TNF)-α, an immunoregulatory cytokine that can enhance HIV-1 replication. Design: Infected promyelocytic and promonocytic cells were examined because they normally express both types of TNF receptors. Methods: TNF receptor surface expression was determined by specific monoclonal antibody recognition and flow cytometry, and signal transduction was detected by gel shift analysis. HIV-1 activation and expression was quantitated by reverse transcriptase assay. Results: In the OM-10.1 promyelocytic model of chronic infection, TNF-α-induced HIV-1 expression also resulted in a substantial increase in 75 kd TNF receptor (TR75) expression although 55 kD TNF receptor (TR55) levels were not dramatically altered. A series of uninfected parental HL-60 subclones all reduced TR75 surface expression in response to TNF-α treatment. Enhanced TR75 expression on OM-10.1 cells followed the same TNF-α-dose dependency as that observed for HIV-1 production. An increase in TR75 expression was also evident during the peak of an acute HIV-1 infection of HL-60 promyelocytes. Although TR55 expression was unaltered during TNF-α-induced HIV activation, this receptor was still involved in the viral activation process. Antibody cross-linking of TR55, in the absence of exogenous TNF-α, induced maximal HIV-1 expression, an up-modulation of surface TR75, and nuclear NF-NB activity in OM-10.1 cultures. Surprisingly, this was the case even when an antagonistic anti-TR55 antibody was used. Anti-TR55 antibody cross-linking in chronically infected U1 promonocytic cultures could only partially substitute for TNF-α-induced HIV-1 expression. Conclusions: Our results demonstrated that HIV-1 infection can selectively influence the surface expression of TNF receptors, potentially influencing its own expression and altering normal immunoregulatory signal transduction.",

keywords = "Agonistic/antagonistic antibodies, Latent/inducible HIV-1 infection, NF-NB activity, Tumor necrosis factor receptor",

author = "Butera, {Salvatore T.} and Roberts, {Beverly D.} and Kwan Leung and Nabel, {Gary J.} and Folks, {Thomas M.}",

year = "1993",

language = "English (US)",

volume = "7",

pages = "911--918",

journal = "AIDS",

issn = "0269-9370",

publisher = "Lippincott Williams and Wilkins",

number = "7",

}

TY - JOUR

T1 - Tumor necrosis factor receptor expression and signal transduction in HIV-1-infected cells

AU - Butera, Salvatore T.

AU - Roberts, Beverly D.

AU - Leung, Kwan

AU - Nabel, Gary J.

AU - Folks, Thomas M.

PY - 1993

Y1 - 1993

N2 - Objective: To examine the inter-relationship between HIV-1 infection and the cell surface receptors for tumor necrosis factor (TNF)-α, an immunoregulatory cytokine that can enhance HIV-1 replication. Design: Infected promyelocytic and promonocytic cells were examined because they normally express both types of TNF receptors. Methods: TNF receptor surface expression was determined by specific monoclonal antibody recognition and flow cytometry, and signal transduction was detected by gel shift analysis. HIV-1 activation and expression was quantitated by reverse transcriptase assay. Results: In the OM-10.1 promyelocytic model of chronic infection, TNF-α-induced HIV-1 expression also resulted in a substantial increase in 75 kd TNF receptor (TR75) expression although 55 kD TNF receptor (TR55) levels were not dramatically altered. A series of uninfected parental HL-60 subclones all reduced TR75 surface expression in response to TNF-α treatment. Enhanced TR75 expression on OM-10.1 cells followed the same TNF-α-dose dependency as that observed for HIV-1 production. An increase in TR75 expression was also evident during the peak of an acute HIV-1 infection of HL-60 promyelocytes. Although TR55 expression was unaltered during TNF-α-induced HIV activation, this receptor was still involved in the viral activation process. Antibody cross-linking of TR55, in the absence of exogenous TNF-α, induced maximal HIV-1 expression, an up-modulation of surface TR75, and nuclear NF-NB activity in OM-10.1 cultures. Surprisingly, this was the case even when an antagonistic anti-TR55 antibody was used. Anti-TR55 antibody cross-linking in chronically infected U1 promonocytic cultures could only partially substitute for TNF-α-induced HIV-1 expression. Conclusions: Our results demonstrated that HIV-1 infection can selectively influence the surface expression of TNF receptors, potentially influencing its own expression and altering normal immunoregulatory signal transduction.

AB - Objective: To examine the inter-relationship between HIV-1 infection and the cell surface receptors for tumor necrosis factor (TNF)-α, an immunoregulatory cytokine that can enhance HIV-1 replication. Design: Infected promyelocytic and promonocytic cells were examined because they normally express both types of TNF receptors. Methods: TNF receptor surface expression was determined by specific monoclonal antibody recognition and flow cytometry, and signal transduction was detected by gel shift analysis. HIV-1 activation and expression was quantitated by reverse transcriptase assay. Results: In the OM-10.1 promyelocytic model of chronic infection, TNF-α-induced HIV-1 expression also resulted in a substantial increase in 75 kd TNF receptor (TR75) expression although 55 kD TNF receptor (TR55) levels were not dramatically altered. A series of uninfected parental HL-60 subclones all reduced TR75 surface expression in response to TNF-α treatment. Enhanced TR75 expression on OM-10.1 cells followed the same TNF-α-dose dependency as that observed for HIV-1 production. An increase in TR75 expression was also evident during the peak of an acute HIV-1 infection of HL-60 promyelocytes. Although TR55 expression was unaltered during TNF-α-induced HIV activation, this receptor was still involved in the viral activation process. Antibody cross-linking of TR55, in the absence of exogenous TNF-α, induced maximal HIV-1 expression, an up-modulation of surface TR75, and nuclear NF-NB activity in OM-10.1 cultures. Surprisingly, this was the case even when an antagonistic anti-TR55 antibody was used. Anti-TR55 antibody cross-linking in chronically infected U1 promonocytic cultures could only partially substitute for TNF-α-induced HIV-1 expression. Conclusions: Our results demonstrated that HIV-1 infection can selectively influence the surface expression of TNF receptors, potentially influencing its own expression and altering normal immunoregulatory signal transduction.

KW - Agonistic/antagonistic antibodies

KW - Latent/inducible HIV-1 infection

KW - NF-NB activity

KW - Tumor necrosis factor receptor

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M3 - Article

C2 - 8395188

AN - SCOPUS:0027249180

SN - 0269-9370

VL - 7

SP - 911

EP - 918

JO - AIDS

JF - AIDS

IS - 7

ER -

Tumor necrosis factor receptor expression and signal transduction in HIV-1-infected cells

Abstract

Keywords

ASJC Scopus subject areas

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