p38α and p38γ Mediate Oncogenic ras-induced Senescence through Differential Mechanisms

Kwong, Jinny; Hong, Lian; Long, Rong; Deng, Qingdong; Han, Jiahuai; Sun, Peiqing

doi:10.1074/jbc.m808327200

Cited by 72 publications

(66 citation statements)

References 64 publications

(96 reference statements)

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“…Recent studies have demonstrated that MAPK signaling pathways play a major role in regulating cell-cycle reentry and oncogenic ras-induced senescence. [39][40][41] The results of the present study show clearly that human Treg cells modulated the specific MAPK p38 and ERK1/2 signaling pathways selectively in responder T cells. In addition, our in vitro and in vivo studies suggest that specific MAPK signaling pathway inhibition in responder T cells can prevent the induction of T-cell senescence mediated by Treg cells.…”

mentioning

confidence: 69%

“…39,40 It has been reported that ERK1/2 and p38 activation can induce p21-dependent G 1 cell-cycle arrest. 41 Therefore, in the present study, we investigated whether human Treg-induced naive T-cell cycle G 0 /G 1 arrest and conversion of naive CD4 ϩ T cells into senescent T cells involved MAPK signaling modulation.…”

Section: Human Treg Cells Induce the Selective Modulation Of Mapk P38mentioning

confidence: 99%

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Human regulatory T cells induce T-lymphocyte senescence

Huang

Hsueh

et al. 2012

Blood

129

276

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IntroductionRegulatory T (Treg) cells play a central role in controlling immune tolerance and homeostasis of the immune system, preventing autoimmune diseases, and limiting chronic inflammatory diseases. 1,2 However, Treg cells can also inhibit effective immune responses against cancer and various pathogen infections. [3][4][5] Therefore, it is critical to better define the suppressive mechanisms used by Treg cells in order to develop effective approaches for their clinical manipulation for therapeutic intervention. Significant progress has been made in delineating the molecules and mechanisms that Treg cells use to mediate suppression. [6][7][8] These mechanisms include suppression by inhibitory cytokines and secreted molecules, 9 by cytolysis or apoptosis of target cells, [10][11][12] by consumption of limiting growth factors and metabolic disruption, [12][13][14] and/or by affecting dendritic cell functions. 15 The majority of previous studies were performed in animal models, so whether these mechanisms are also used by human Treg cells is still under investigation. In addition, the fate and function of responder T cells suppressed by Treg cells is unclear.Cellular senescence was described initially more than 40 years ago in human fibroblasts with limited passages in cell culture. 16 It is now well known that senescent cells have permanent cell-cycle arrest but remain viable and metabolically active and possess unique transcriptional profiles and gene-regulation signatures. 17 There are 2 major categories of cellular senescence: replicative senescence (also known as telomere-dependent senescence) [18][19][20] and premature senescence (also known as extrinsic senescence or telomere-independent senescence). 17,[21][22][23] Recent studies suggest that replicative senescence also occurs in the human immune system. Accumulation of senescent CD8 ϩ T cells has been found in persons during normal aging, in younger persons with chronic viral infections, and in patients with certain types of cancers. [24][25][26][27] Senescent CD8 ϩ T cells show functional changes and have defective killing abilities due to the loss of perforin and granzyme or have defects in signaling of granule exocytosis. 28,29 Furthermore, senescent CD8 ϩ T cells have negative regulatory functions that reduce the effects of immunization and vaccinations and prolong the survival of allografts. 26,30 Improved understanding of the molecular mechanisms used in the generation of senescent T cells and their functional alterations will open new avenues to restoring T-cell function and will help in the design of novel vaccines for infectious diseases and cancers.In the present study, we explored the suppressive mechanisms used by human Treg cells and investigated the fate of Treg-treated responder T cells and found that treatment with CD4 ϩ CD25 hi naturally occurring Treg cells can induce naive/effector T-cell senescence. We further identified the molecular signaling that controls the process of T-cell senescence and characterized these senescent T cells....

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mentioning

confidence: 69%

Section: Human Treg Cells Induce the Selective Modulation Of Mapk P38mentioning

confidence: 99%

Human regulatory T cells induce T-lymphocyte senescence

Huang

Hsueh

et al. 2012

Blood

129

276

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“…This hypothesis is supported by the finding that the progeny of LKS + cells cultured with SB exhibited significantly less SA-bgal staining and expression of p16 mRNA than those without SB. SA-b-gal is a widely used biomarker of senescent cells [34] and increased expression of p16 has been implicated in the induction of cellular senescence down-stream of p38 activation [26,33]. In addition, a significant fewer apoptotic cells were detected in LKS + cells cultured with SB than the cells without SB, indicating that p38 inhibition can also inhibit HSC apoptosis.…”

Section: Discussionmentioning

confidence: 99%

“…The mechanisms by which p38 inhibition promotes HSC self-renewal and ex vivo expansion may be attributable primarily to the inhibition of cellular senescence, because it has been shown that p38 functions as a key molecule mediating diverse stimuli-induced cellular senescence via upregulation of p16 in a variety of cells, including HSCs [14,15,32,33]. This hypothesis is supported by the finding that the progeny of LKS + cells cultured with SB exhibited significantly less SA-bgal staining and expression of p16 mRNA than those without SB.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of p38 Mitogen-Activated Protein Kinase Promotes Ex Vivo Hematopoietic Stem Cell Expansion

Wang

Kellner

Liu

et al. 2011

Stem Cells and Development

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Hematopoietic stem cell (HSC) self-renewal is tightly regulated by a complex crosstalk between many cellintrinsic regulators and a variety of extrinsic signals from the stem cell niche. In this study, we examined whether the p38 mitogen-activated protein kinase (p38) is one of the intrinsic regulators that can negatively regulate HSC self-renewal in vitro and whether inhibition of p38 activity with a small molecule inhibitor can promote HSC expansion ex vivo. The results from this study showed that sorted mouse bone marrow Lin -Sca1 + c-kit + cells (LSK + cells) exhibited selective activation of p38 after culture in a serum-free medium supplemented with 100 ng/mL stem cell factor, thrombopoietin, and Flt3 ligand. The activation of p38 was associated with a significant reduction in HSCs and induction of apoptosis and cellular senescence in LSK + cells and their progeny. Addition of the specific p38 inhibitor SB203580 (SB, 5 mM) to the culture inhibited the activation of p38 in LSK + cells, which led to increase in HSC self-renewal and ex vivo expansion as shown by the cobblestone area forming cell assay, competitive repopulation, and serial transplantation. The increase in HSC expansion is likely attributable to SB-mediated inhibition of HSC apoptosis and senescence and upregulation of HoxB4 and CXCR4. These findings suggest that p38 plays an important role in the regulation of HSC self-renewal in vitro and inhibition of p38 activation with a small molecule inhibitor may represent a novel approach to promote ex vivo expansion of HSCs.

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“…These variants had acquired increased autophosphorylation activity (Fig. 6B) (13) sufficient to elevate their catalytic activities (15,18,30,31). We thus coincubated the Histagged WT or active variants of each p38 isoform with increasing amounts of their GST-tagged KD counterpart (Fig.…”

Section: P38␤mentioning

confidence: 99%

p38β Mitogen-Activated Protein Kinase Modulates Its Own Basal Activity by Autophosphorylation of the Activating Residue Thr180 and the Inhibitory Residues Thr241 and Ser261

Beenstock

Melamed

Mooshayef

et al. 2016

Molecular and Cellular Biology

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e Many enzymes are self-regulated and can either inhibit or enhance their own catalytic activity. Enzymes that do both are extremely rare. Many protein kinases autoactivate by autophosphorylating specific sites at their activation loop and are inactivated by phosphatases. Although mitogen-activated protein kinases (MAPKs) are usually activated by dual phosphorylation catalyzed by MAPK kinases (MAPKKs), the MAPK p38␤ is exceptional and is capable of self-activation by cis autophosphorylation of its activation loop residue T180. We discovered that p38␤ also autophosphorylates in trans two previously unknown sites residing within a MAPK-specific structural element known as the MAPK insert: T241 and S261. Whereas phosphorylation of T180 evokes catalytic activity, phosphorylation of S261 reduces the activity of T180-phosphorylated p38␤, and phosphorylation of T241 reduces its autophosphorylation in trans. Both phosphorylations do not affect the activity of dually phosphorylated p38␤. T241 of p38␤ is found phosphorylated in vivo in bone and muscle tissues. In myogenic cell lines, phosphorylation of p38␤ residue T241 is correlated with differentiation to myotubes. T241 and S261 are also autophosphorylated in intrinsically active variants of p38␣, but in this protein, they probably play a different role. We conclude that p38␤ is an unusual enzyme that automodulates its basal, MAPKK-independent activity by several autophosphorylation events, which enhance and suppress its catalytic activity.

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p38α and p38γ Mediate Oncogenic ras-induced Senescence through Differential Mechanisms

Cited by 72 publications

References 64 publications

Human regulatory T cells induce T-lymphocyte senescence

Human regulatory T cells induce T-lymphocyte senescence

Inhibition of p38 Mitogen-Activated Protein Kinase Promotes Ex Vivo Hematopoietic Stem Cell Expansion

p38β Mitogen-Activated Protein Kinase Modulates Its Own Basal Activity by Autophosphorylation of the Activating Residue Thr180 and the Inhibitory Residues Thr241 and Ser261

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