Cell fusion induced by ERVWE1 or measles virus causes cellular senescence

Chuprin, Anna; Gal, Hilah; Biron‐Shental, Tal; Biran, Anat; Amiel, Aliza; Rozenblatt, Shmuel; Krizhanovsky, Valery

doi:10.1101/gad.227512.113

Cited by 210 publications

(228 citation statements)

References 63 publications

Supporting

Mentioning

212

Contrasting

Unclassified

Order By: Relevance

“…The human NKG2D ligands primarily consist of MICA, MICB, ULBP1, ULBP2, ULBP3, ULBP4, ULBP5 and ULBP6. The transcriptional up-regulation of MICA and ULBP2 during cell senescence have been reported in senescent-activated hepatic stellate cells, replicative senescent fibroblasts and HUVECs, etoposide-induced senescent fibroblasts, fusioninduced senescent fibroblasts and chemotherapyinduced senescent multiple m yeloma cells (Krizhanovsky et al 2008;Kim et al 2008;Chuprin et al 2013;Soriani et al 2009;Lackner et al 2014). In addition to MICA and ULBP2, microarray analysis of replicative senescent fibroblasts demonstrated an increase in the expression of ULBP1 (2.75-fold) compared to growing cells, in addition to the up-regulation of HLA-E (2-fold) (Lackner et al 2014).…”

Section: The Relationship Between Cell Senescence and Immune Ligand Ementioning

confidence: 96%

“…We define this as a shift from a passive cellular phenotype in terms of immune surveillance to one that actively promotes selfelimination by the immune system. In this model, the secretory phenotype of senescent cells serves to attract immune cells , which then recognize their target via the up-regulated ligands found on their surface (Krizhanovsky et al 2008;Kim et al 2008;Soriani et al 2009;Chuprin et al 2013). …”

mentioning

confidence: 99%

“…However, the length of time within the tissue is clearly a major factor in determining whether the effect of entry into senescence will be beneficial or deleterious to the organism. The appearance of senescent cells in the short-term probably facilitates important physiological functions such as tumour suppression (Braig et al 2005;Chen et al 2005;Michaloglou et al 2005;Collado et al 2005), wound healing (Krizhanovsky et al 2008;Jun et al 2010;Fitzner et al 2012;Kim et al 2013;Demaria et al 2014) and possibly placental development (Chuprin et al 2013;Rajagopalan and Long 2012;Zhang et al 2014). However, senescent cells are known to accumulate in vivo, possibly as a result of impaired immune clearance by an ageing immune system ).…”

mentioning

confidence: 99%

“…mice) do not use it at all (Smith and Kipling 2004;Itahana et al 2004). Oncogene activation (oncogene-induced senescence, OIS) (Serrano et al 1997;Zhu et al 1998), elevated reactive oxygen species (stress-induced premature senescence, SIPS) (Toussaint et al 2000) and cell-cell fusion (Chuprin et al 2013) all trigger entry into a senescent state.…”

mentioning

confidence: 99%

“…Many triggers of cell senescence result in DNA damage in cells in vitro (Di Micco et al 2006;Hewitt et al 2012;Chuprin et al 2013) and in vivo (Herbig et al 2006;Wang et al 2009;Suram et al 2012). This observation gives rise to the important conceptual question of whether the DNA damage response (DDR) is an absolute requirement for immunogenic conversion.…”

mentioning

confidence: 99%

See 4 more Smart Citations

Cellular senescence: from growth arrest to immunogenic conversion

Burton

Faragher

2015

AGE

View full text Add to dashboard Cite

Cellular senescence was first reported in human fibroblasts as a state of stable in vitro growth arrest following extended culture. Since that initial observation, a variety of other phenotypic characteristics have been shown to co-associate with irreversible cell cycle exit in senescent fibroblasts. These include (1) a proinflammatory secretory response, (2) the up-regulation of immune ligands, (3) altered responses to apoptotic stimuli and (4) promiscuous gene expression (stochastic activation of genes possibly as a result of chromatin remodeling). Many features associated with senescent fibroblasts appear to promote conversion to an immunogenic phenotype that facilitates self-elimination by the immune system. Pro-inflammatory cytokines can attract and activate immune cells, the presentation of membrane bound immune ligands allows for specific recognition and promiscuous gene expression may function to generate an array of tissue restricted proteins that could subsequently be processed into peptides for presentation via MHC molecules. However, the phenotypes of senescent cells from different tissues and species are often assumed to be broadly similar to those seen in senescent human fibroblasts, but the data show a more complex picture in which the growth arrest mechanism, tissue of origin and species can all radically modulate this basic pattern. Furthermore, wellestablished triggers of cell senescence are often associated with a DNA damage response (DDR), but this may not be a universal feature of senescent cells. As such, we discuss the role of DNA damage in regulating an immunogenic response in senescent cells, in addition to discussing less established Batypical^senescent states that may occur independent of DNA damage.

show abstract

Section: The Relationship Between Cell Senescence and Immune Ligand Ementioning

confidence: 96%

mentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

See 3 more Smart Citations

Cellular senescence: from growth arrest to immunogenic conversion

Burton

Faragher

2015

AGE

View full text Add to dashboard Cite

show abstract

Preeclampsia and the Kidney: Pathophysiology and Clinical Implications

Dines¹,

Šuvakov²,

Kattah³

et al. 2023

Comprehensive Physiology

View full text Add to dashboard Cite

Impact of Aging and Cellular Senescence in the Pathophysiology of Preeclampsia

Suvakov,

Kattah,

Gojkovic

et al. 2023

Comprehensive Physiology

View full text Add to dashboard Cite

The incidence of hypertensive disorders of pregnancy is increasing, which may be due to several factors, including an increased age at pregnancy and more comorbid health conditions during reproductive years. Preeclampsia, the most severe hypertensive disorder of pregnancy, has been associated with an increased risk of future disease, including cardiovascular and kidney diseases. Cellular senescence, the process of cell cycle arrest in response to many physiologic and maladaptive stimuli, may play an important role in the pathogenesis of preeclampsia and provide a mechanistic link to future disease. In this article, we will discuss the pathophysiology of preeclampsia, the many mechanisms of cellular senescence, evidence for the involvement of senescence in the development of preeclampsia, as well as evidence that cellular senescence may link preeclampsia to the risk of future disease. Lastly, we will explore how a better understanding of the role of cellular senescence in preeclampsia may lead to therapeutic trials. © 2023 American Physiological Society. Compr Physiol 13:5077‐5114, 2023.

show abstract

Cell fusion induced by ERVWE1 or measles virus causes cellular senescence

Cited by 210 publications

References 63 publications

Cellular senescence: from growth arrest to immunogenic conversion

Cellular senescence: from growth arrest to immunogenic conversion

Preeclampsia and the Kidney: Pathophysiology and Clinical Implications

Impact of Aging and Cellular Senescence in the Pathophysiology of Preeclampsia

Contact Info

Product

Resources

About