Digestion of Chromatin in Apoptotic Cell Microparticles Prevents Autoimmunity

Sisirak, Vanja; Sally, Benjamin; D’Agati, Vivette D.; Martinez‐Ortiz, Wilnelly; Özçakar, Z. Bı̇rsı̇n; David, J. Hearn; Rashidfarrokhi, Ali; Yeste, Ada; Panea, Casandra; Chida, Asiya Seema; Bogunovic, Milena; Ivanov, Ivaylo I.; Quintana, Francisco J.; Sanz, Iñaki; Elkon, Keith B.; Tekin, Mustafa; Yalçınkaya, Fatoş; Cardozo, Timothy; Clancy, Robert M.; Buyon, Jill P.; Reizis, Boris

doi:10.1016/j.cell.2016.05.034

Cited by 346 publications

(484 citation statements)

References 45 publications

Supporting

Mentioning

449

Contrasting

Unclassified

Order By: Relevance

“…Perhaps cavity dwelling macrophages can be recruited to dying cells in their cavities as well as neighboring organs. As cavity resident cells these macrophage populations may also have limited exposure to circulating proteins, such as DNASE1L3, which digests DNA in microparticles released from ACs (Sisirak et al, 2016), One interesting possibility is that cavity resident macrophages utilize additional mechanisms to limit responses to ACs because of reduced DNase activity in these compartments.…”

Section: Discussionmentioning

confidence: 99%

Tissue-Resident Macrophages Are Locally Programmed for Silent Clearance of Apoptotic Cells

et al. 2017

View full text Add to dashboard Cite

SUMMARY Although apoptotic cells (ACs) contain nucleic acids that can be recognized by Toll-like receptors (TLRs), engulfment of ACs does not initiate inflammation in healthy organisms. Here we identified macrophage populations that continually engulf ACs in distinct tissues and found that these macrophages shared characteristics compatible with immunologically silent clearance of ACs, including high expression of AC recognition receptors, low expression of TLR9, and reduced TLR responsiveness to nucleic acids. Removal from tissues resulted in loss of many of these characteristics and the ability to generate inflammatory responses to AC-derived nucleic acids, suggesting that cues from the tissue microenvironment program macrophages for silent AC clearance. The transcription factors KLF2 and KLF4 controlled the expression of many genes within this AC clearance program. The coordinated expression of AC receptors with genes that limit responses to nucleic acids may thus represent a central feature of tissue macrophages that ensures maintenance of homeostasis.

show abstract

Section: Discussionmentioning

confidence: 99%

Tissue-Resident Macrophages Are Locally Programmed for Silent Clearance of Apoptotic Cells

et al. 2017

View full text Add to dashboard Cite

show abstract

“…Bone marrow-derived DCs exposed to acetylated nucleosomes undergo maturation and activate syngenic T cells. Apoptotic microparticles, which expose modified nucleosomes at the cell surface (123-125), are found in both SLE patients and mice (125-127). Apoptotic microparticles from MRL/ lpr mice express elevated levels of modified chromatin and induce enhanced maturation of DCs than BALB/c mice (125).…”

Section: Apoptosis-associated Histone Modifications In Lnmentioning

confidence: 99%

“…Apoptotic microparticles from MRL/ lpr mice express elevated levels of modified chromatin and induce enhanced maturation of DCs than BALB/c mice (125). DNASE1L3 is a serum enzyme that is critical for the degradation of chromatin in microparticles precluding autoantibody recognition of microparticle DNA and humans and mice lacking DNASE1L3 develop SLE-like disease (127-131). Microparticles from SLE patients express apoptosis-related histone modifications while these were absent in microparticles from healthy individuals (126).…”

Section: Apoptosis-associated Histone Modifications In Lnmentioning

confidence: 99%

Cell death in the pathogenesis of systemic lupus erythematosus and lupus nephritis

Mistry

Kaplan

2017

Clinical Immunology

157

137

View full text Add to dashboard Cite

Nephritis is one of the most severe complications of systemic lupus erythematosus (SLE). One key characteristic of lupus nephritis (LN) is the deposition of immune complexes containing nucleic acids and/or proteins binding to nucleic acids and autoantibodies recognizing these molecules. A variety of cell death processes are implicated in the generation and externalization of modified nuclear autoantigens and in the development of LN. Among these processes, apoptosis, primary and secondary necrosis, NETosis, necroptosis, pyroptosis, and autophagy have been proposed to play roles in tissue damage and immune dysregulation. Cell death occurs in healthy individuals during conditions of homeostasis yet autoimmunity does not develop, at least in part, because of rapid clearance of dying cells. In SLE, accelerated cell death combined with a clearance deficiency may lead to the accumulation and externalization of nuclear autoantigens and to autoantibody production. In addition, specific types of cell death may modify autoantigens and alter their immunogenicity. These modified molecules may then become novel targets of the immune system and promote autoimmune responses in predisposed hosts. In this review, we examine various cell death pathways and discuss how enhanced cell death, impaired clearance, and post-translational modifications of proteins could contribute to the development of lupus nephritis.

show abstract

“…DNASE1L3, a circulating DNase produced primarily by macrophages and DC, digests the genomic DNA in apoptotic cell derived membrane-bound vesicles called microparticles (246). These microparticles are smaller than apoptotic bodies and can be found in the plasma of SLE patients bound to IgG to form a type of immune complex that may contribute to pathogenesis (247, 248).…”

Section: Degradation Of Apoptotic Cell Dnamentioning

confidence: 99%

“…These microparticles are smaller than apoptotic bodies and can be found in the plasma of SLE patients bound to IgG to form a type of immune complex that may contribute to pathogenesis (247, 248). A highly basic C-terminal peptide in DNASE1L3 enables its association with liposomes encapsulating DNA (249), and this property of DNASE1L3 is thought to enable its digestion of surface-exposed chromatin exposed on microparticles thereby preventing autoantibody binding (246, 250). Dnase1l3 -deficient mice develop antibodies to dsDNA and chromatin and exhibit features of SLE including glomerulonephritis (246).…”

Section: Degradation Of Apoptotic Cell Dnamentioning

confidence: 99%

The many ways tissue phagocytes respond to dying cells

Blander

2017

Immunological Reviews

View full text Add to dashboard Cite

Summary Apoptosis is an important component of normal tissue physiology, and the prompt removal of apoptotic cells is equally essential to avoid the undesirable consequences of their accumulation and disintegration. Professional phagocytes are highly specialized for engulfing apoptotic cells. The recent ability to track cells that have undergone apoptosis in situ has revealed a division of labor among the tissue resident phagocytes that sample them. Macrophages are uniquely programmed to process internalized apoptotic cell-derived fatty acids, cholesterol and nucleotides, as a reflection of their dominant role in clearing the bulk of apoptotic cells. Dendritic cells carry apoptotic cells to lymph nodes where they signal the emergence and expansion of highly suppressive regulatory CD4 T cells. A broad suppression of inflammation is executed through distinct phagocyte-specific mechanisms. A clever induction of negative regulatory nodes is notable in dendritic cells serving to simultaneously shut down multiple pathways of inflammation. Several of the genes and pathways modulated in phagocytes in response to apoptotic cells have been linked to chronic inflammatory and autoimmune diseases such as atherosclerosis, inflammatory bowel disease and systemic lupus erythematosus. Our collective understanding of old and new phagocyte functions after apoptotic cell phagocytosis demonstrates the enormity of ways to mediate immune suppression and enforce tissue homeostasis.

show abstract

Digestion of Chromatin in Apoptotic Cell Microparticles Prevents Autoimmunity

Cited by 346 publications

References 45 publications

Tissue-Resident Macrophages Are Locally Programmed for Silent Clearance of Apoptotic Cells

Tissue-Resident Macrophages Are Locally Programmed for Silent Clearance of Apoptotic Cells

Cell death in the pathogenesis of systemic lupus erythematosus and lupus nephritis

The many ways tissue phagocytes respond to dying cells

Contact Info

Product

Resources

About