Accelerated neutrophil apoptosis in the acquired immunodeficiency syndrome.

Pitrak, David; Tsai, H.; Mullane, Kathleen M.; Sutton, Sarah H.; Stevens, Paul

doi:10.1172/jci119096

Cited by 132 publications

(110 citation statements)

References 32 publications

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“…Neutrophils enter the bloodstream and tissues as terminally differentiated cells, which are unable to self-renew and have the shortest half-life of all circulating leukocytes. After leaving the bone marrow, neutrophils are programmed to die within about 24 h as a result of constitutive and spontaneous apoptosis [3][4][5], a controlled biological process leading to the physiological death of the cell, and characterized by cell shrinkage, chromatin condensation, and internucleosomal DNA degradation, widely considered to be a biochemical hallmark of apoptosis [6].…”

Section: Introductionmentioning

confidence: 99%

Expression of genes involved in initiation, regulation, and execution of apoptosis in human neutrophils and during neutrophil differentiation of HL-60 cells

Santos-Beneit

Mollinedo

2000

Journal of Leukocyte Biology

107

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Neutrophils possess a very short lifespan, dying by apoptosis. HL-60 cells undergo apoptosis after neutrophil differentiation with dimethyl sulfoxide (DMSO). We have found that the onset of apoptosis in neutrophil-differentiating HL-60 cells correlates with the achievement of an apoptosis-related gene expression pattern similar to that of peripheral blood mature neutrophils. Using reverse transcriptase-polymerase chain reaction, cloning, and sequencing techniques, we have found that HL-60 cells express bak, bik, bax, bad, bcl-2, bcl-x L , bcl-w, bfl-1, fas, and caspases 1-4 and 7-10. After DMSO treatment, bak, bcl-w, bfl-1, fas, and caspases 1 and 9 were up-regulated, whereas bik, bcl-2, and caspases 2, 3, and 10 were down-regulated at different degrees, achieving mRNA expression levels that correlated with those detected in peripheral blood neutrophils. Caspase-2 mRNA and protein expression was drastically reduced after HL-60 cell differentiation, being absent in both HL-60-differentiated neutrophils and mature neutrophils, whereas caspase-3 and -10 mRNA and protein expression were diminished upon HL-60 cell differentiation until achieving the respective levels found in mature neutrophils. Bak and bfl-1 mRNA levels were largely increased during DMSO-induced differentiation of HL-60 cells, and these genes were the bcl-2 family members that were expressed most abundantly in mature neutrophils. Bcl-2 overexpression or caspase inhibition prevented differentiation-induced apoptosis in HL-60 cells, but not their differentiation capability. Neutrophil spontaneous apoptosis was also blocked by the caspase inhibitor z-Asp-2,6-dichlorobenzoyloxymethylketone. Peripheral blood neutrophils expressed bak, bad, bcl-w, bfl-1, fas, and caspases 1, 3, 4, and 7-10, but hardly expressed bcl-2, bcl-x L , bik, bax, and caspase-2. These results suggest that the above gene expression changes in neutrophil-differentiating HL-60 cells may play a role in the acquisition of the neutrophil apoptotic features. J. Leukoc. Biol. 67: 712-724; 2000.

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Section: Introductionmentioning

confidence: 99%

Expression of genes involved in initiation, regulation, and execution of apoptosis in human neutrophils and during neutrophil differentiation of HL-60 cells

Santos-Beneit

Mollinedo

2000

Journal of Leukocyte Biology

107

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“…The modulation of neutrophil apoptosis in RSV infection in vivo may regulate the epithelial damage induced by neutrophils. To date, however, there are no published studies of neutrophil apoptosis in RSV infection, although a recent study shows that HIV infection accelerates neutrophil apoptosis [11].…”

Section: Introductionmentioning

confidence: 99%

“…On the other hand, because apoptotic neutrophils are functionally impaired [32], accelerated neutrophil apoptosis in vivo may contribute to the risk of secondary infection [11], which has been associated with RSV infection [33,34]. In addition, although in this study neutrophil apoptosis due to RSV infection was investigated, it is likely that other respiratory viral infections could have a similar effect.…”

mentioning

confidence: 99%

The apoptosis of neutrophils is accelerated in respiratory syncytial virus (RSV)-induced bronchiolitis

Wang

Smith

Lovejoy

et al. 1998

Clinical and Experimental Immunology

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SUMMARYNeutrophils are the predominant inflammatory cell in the lung tissues and airways in RSV infection, and can augment the epithelial cell damage induced by RSV. Neutrophil apoptosis has been suggested to be a mechanism to reduce the potential for tissue injury. The apoptosis of neutrophils from nasopharyngeal aspirates (NPA) (n ¼ 19) and peripheral blood (PB) of infants with RSV bronchiolitis (n ¼ 11) and PB from healthy controls (n ¼ 9) was investigated. Monoclonal antibody against CD95 (Fas) and a binding protein Annexin V were used to determine the apoptosis of neutrophils. The expression of CD11b and CD18 on neutrophils was also detected with flow cytometry. The mean fluorescence intensity (MFI) of CD95 on neutrophils from RSV þ NPA was increased compared with cells from control PB (73·6 Ϯ 7·6 versus 31·5 Ϯ 4·3); the MFI of Annexin V, CD11b and CD18 on neutrophils from RSV þ NPA was upregulated compared with cells from both control PB (105·3 Ϯ 18·1 versus 11·8 Ϯ 1·5; 1683 Ϯ 153·3 versus 841·1 Ϯ 72·3; 517 Ϯ 50·5 versus 147 Ϯ 8·7, respectively) and RSV þ PB (105·3 Ϯ 18·1 versus 35·8 Ϯ 4·1; 1683 Ϯ 153·3 versus 818 Ϯ 141·2; 517 Ϯ 50·5 versus 260 Ϯ 25·8, respectively). Furthermore, the percentage of neutrophils expressing Annexin V and the MFI of CD18 on neutrophils from RSV þ PB were increased compared with neutrophils from control PB. In addition, both CD11b (MFI) and CD18 (MFI) correlated with Annexin V (MFI) on neutrophils. We conclude that neutrophil apoptosis in RSV bronchiolitis is accelerated; and CD11b/CD18 may play an important role in RSV infection by influencing neutrophil apoptosis.

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“…It is well established that dendritic cells (DCs) are involved early in HIV-1 transmission (Granelli-Piperno et al, 1998;Manel et al, 2010;Tsunetsugu-Yokota et al, 1997). It is also known that CD4TL, more particularly the Th17 mucosal subset (Cecchinato and Franchini, 2010;Cecchinato et al, 2008;Elhed and Unutmaz, 2010;Favre et al, 2009;Milush et al, 2011;Paiardini, 2010) are dysregulated (Elbim et al, 2009;Hofman et al, 1999;Okada, Takei, and Tashiro, 1997;Okada, Takei, and Tashiro, 1998;Pitrak et al, 1996;Roilides et al, 1993;Roilides et al, 1990;Szelc et al, 1992;Thorsen, Busch-Sorensen, and Sondergaard, 1989) in pathogenic HIV-1/SIV infection (Brenchley et al, 2008;Elbim et al, 2009;Elbim et al, 2008;Favre et al, 2009). A rapid decrease thus occurs in the numbers of both infected and uninfected CD4TL within the very first weeks of infection.…”

Section: Rapid Depletion Of Cd4tl During Primary Infectionmentioning

confidence: 99%

Exosomes Decrease In Vitro Infectivity of HIV-1 Preparations: Implication for CD4+T Lymphocyte Depletion In Vivo

Subra¹,

Burelout²,

Sophie³

et al. 2011

Understanding HIV/AIDS Management and Care - Pandemic Approaches in the 21st Century

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Accelerated neutrophil apoptosis in the acquired immunodeficiency syndrome.

Cited by 132 publications

References 32 publications

Expression of genes involved in initiation, regulation, and execution of apoptosis in human neutrophils and during neutrophil differentiation of HL-60 cells

Expression of genes involved in initiation, regulation, and execution of apoptosis in human neutrophils and during neutrophil differentiation of HL-60 cells

The apoptosis of neutrophils is accelerated in respiratory syncytial virus (RSV)-induced bronchiolitis

Exosomes Decrease In Vitro Infectivity of HIV-1 Preparations: Implication for CD4+T Lymphocyte Depletion In Vivo

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