Clearance of apoptotic and necrotic cells and its immunological consequences

Krysko, Dmitri V.; D’Herde, Katharina; Vandenabeele, Peter

doi:10.1007/s10495-006-9527-8

Cited by 294 publications

(270 citation statements)

References 193 publications

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“…We showed that apoptotic cells are engulfed by a zipper-like mechanism of phagocytosis ( Figure 1), whereas necrotic cells are internalized by a macropinocytotic mechanism, such that parts of the cell are co-ingested together with extracellular fluid. 8,31,32 In contrast with the initial paradigm, PS exposure mediates recognition and engulfment not only of apoptotic cells, but also of necrotic cells 33,34 and of cells dying from autophagic cell death, 35 indicating that PS-mediated clearance may be a general mechanism irrespective of the way a cell dies. Accordingly, several macrophage receptor systems known to be involved in the engulfment of apoptotic cells also contribute to the uptake of necrotic cells.…”

Section: Positive Regulators Of Uptake Dying Cellmentioning

confidence: 97%

“…For example, C1q, mannose-binding lectin, pentraxin-3, C3, C4, C-reactive protein (an acute phase protein), and thrombospondin bind predominantly to late apoptotic or secondary necrotic cells. 8 Great progress has been achieved during the last decade in unraveling molecules on the surface of apoptotic cells, but it is still not clear how non-apoptotic cells, namely necrotic and autophagic cells, are recognized by macrophages. We showed that apoptotic cells are engulfed by a zipper-like mechanism of phagocytosis ( Figure 1), whereas necrotic cells are internalized by a macropinocytotic mechanism, such that parts of the cell are co-ingested together with extracellular fluid.…”

Section: Positive Regulators Of Uptake Dying Cellmentioning

confidence: 99%

“…8 One of the mechanisms for this protection is related to repelling signals mediated through CD31 (platelet endothelial cell adhesion molecule). CD31 on viable cells homotypically interacts with its identical counterpart on phagocytes, promoting detachment, and preventing engulfment of the viable cells by an active and temperaturedependent mechanism.…”

Section: Negative Regulation Of Dying Cell Uptakementioning

confidence: 99%

“…48 Necrotic cells release massive amount of high mobility group box 1 (HMGB-1) protein, which incites inflammatory responses of macrophages through pathways mediated by Toll-like receptor 2 (TLR2) and TLR4. 8,52 Whether HMGB-1 protein is specifically released by necrotic cells but not by apoptotic or secondary necrotic cells remains controversial. Apparently, in apoptosis and secondary necrosis HMGB-1 remains bound on the DNA.…”

Section: Factors Released By Dying Cellsmentioning

confidence: 99%

See 3 more Smart Citations

From regulation of dying cell engulfment to development of anti-cancer therapy

Krysko

Vandenabeele

2007

Cell Death Differ

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Cell death and efficient engulfment of dying cells ensure tissue homeostasis and is involved in pathogenesis. Clearance of dying cells is a complex and dynamic process coordinated by interplay between ligands on dying cell, bridging molecules, and receptors on engulfing cells. In this review, we will discuss recent advances and significance of molecular changes on the surface of dying cells implicated in their recognition and clearance as well as factors released by dying cells that attract macrophages to the site of cell death. It is now becoming apparent that phagocytes use a specific set of mechanisms to discriminate between live and dead cells, and this phenomenon will be illustrated here. Next, we will discuss potential mechanisms by which removal of dying cells could modulate immune responses of phagocytes, in particular of macrophages. Finally, we will address possible strategies for manipulating the immunogenicity of dying cells in experimental cancer therapies.

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Section: Positive Regulators Of Uptake Dying Cellmentioning

confidence: 97%

Section: Positive Regulators Of Uptake Dying Cellmentioning

confidence: 99%

Section: Negative Regulation Of Dying Cell Uptakementioning

confidence: 99%

Section: Factors Released By Dying Cellsmentioning

confidence: 99%

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From regulation of dying cell engulfment to development of anti-cancer therapy

Krysko

Vandenabeele

2007

Cell Death Differ

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“…Electroporation has been used to transfer plasmid DNA into monocytic cell lines or macrophages with high efficiency (Weir and Meltzer, 1993;Hume et al, 2001). Usually, electroporation causes significant cell death and release of intracellular contents, which is known to induce macrophage responses (Krysko et al, 2006). Moreover, both transfection and electroporation with plasmid DNA containing unmethylated CpG (cytosine followed by guanine) dinucleotides may activate macrophages through Toll-like receptor (TLR)-9 to produce proinflammatory cytokines (Stacey et al, 1996;Sester et al, 1999;Jiang et al, 2006).Thus, the existing methods of plasmid delivery perturb the normal physiological status of the macrophage population and complicate interpretation of the experimental data.…”

Section: Introductionmentioning

confidence: 99%

Dual-promoter lentiviral system allows inducible expression of noxious proteins in macrophages

Hui

Mostoslavsky

Eruslanov

et al. 2008

Journal of Immunological Methods

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In-depth studies of innate immunity require efficient genetic manipulation of macrophages, which is especially difficult in primary macrophages. We have developed a lentiviral system for inducible gene expression both in macrophage cell lines and in primary macrophages. A transgenic mouse strain C3H.TgN(SRA-rtTA) that expresses reverse tetracycline transactivator (rtTA) under the control of macrophage-specific promoter, a modified human scavenger receptor A (SR-A) promoter was generated. For gene delivery, we constructed a dual-promoter lentiviral vector, in which expression of a "gene-of-interest" is driven by a doxycycline-inducible promoter and the expression of a selectable surface marker is driven by an independent constitutive promoter UBC. This vector is used for transduction of bone marrow-derived macrophage precursors. The transduced cells can be enriched to 95-99% purity using marker-specific monoclonal antibodies, expanded and differentiated into mature macrophages or myeloid dendritic cells. We also successfully used this approach for inducible protein expression in hard to transfect macrophage cell lines.Because many proteins, which are expressed by activated or infected macrophages, possess cytotoxic, anti-proliferative or pro-apoptotic activities, generation of stable macrophage cell lines that constitutively express those proteins is impossible. Our method will be especially useful to study immunity-related macrophage proteins in their physiological context during macrophage activation or infection.

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