Prostaglandin E2 reduces radiation-induced epithelial apoptosis through a mechanism involving AKT activation and bax translocation

Tessner, Teresa G.; Muhale, Filipe; Riehl, Terrence E.; Anant, Shrikant; Stenson, William F.

doi:10.1172/jci200422218

Cited by 33 publications

(23 citation statements)

References 51 publications

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“…COX‐2, an enzyme that catalyzes the formation of prostaglandins, affects tumor cell proliferation and host immune response and is undetectable in most of the normal tissue. Evidence from clinical and preclinical studies indicates that COX‐2‐derived prostaglandins participate in carcinogenesis, suppression of host immunity, apoptosis inhibition, angiogenesis, and tumor cell invasiveness and metastasis . Our previous studies showed that a high expression of COX‐2 is associated with the recurrence and a poor prognosis of patients with NPC, and COX‐2 may play a critical role in chemotherapeutic resistance in NPC via the inhibition of chemotherapy‐induced senescence via the inactivation of p53 .…”

Section: Discussionmentioning

confidence: 99%

High COX‐2 expression in cancer‐associated fibiroblasts contributes to poor survival and promotes migration and invasiveness in nasopharyngeal carcinoma

Zhu

Chen

Zeng

et al. 2019

Molecular Carcinogenesis

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Nasopharyngeal carcinoma (NPC) has the highest rate of metastasis among head and neck cancers, and distant metastasis is the major reason for treatment failure. We have previously shown that high cyclooxygenase‐2 (COX‐2) expression is associated with a poor prognosis of patients with NPC and inhibits chemotherapy‐induced senescence in NPC cells. In this study, we found that COX‐2 was upregulated in cancer‐associated fibroblasts (CAFs) derived from NPC by RNA‐Seq. Furthermore, elevated COX‐2 expression in CAF was detected in NPC patients with poor survival and distant metastasis by using immunohistochemistry. Then, we identified that COX‐2 is highly expressed in CAF at the distant metastasis site in seven paired NPC patients. High expression of COX‐2 and secretion of prostaglandin E2, a major product catalyzed by COX‐2 in fibroblasts, promotes migration and invasiveness of NPC cells in vitro. On the contrary, inhibition of COX‐2 has the opposite effect in vitro as well as in the COX‐2−/− mouse with the lung metastasis model in vivo. Mechanistically, we discovered that COX‐2 elevates tumor necrosis factor‐α expression in CAF to promote NPC cell migration and invasiveness. Overall, our results identified a novel target in CAF promoting NPC metastasis. Our findings suggested that high expression of COX‐2 in CAF may serve as a new prognostic indicator for NPC metastasis and provide the possibility of targeting CAF for treating advanced NPC.

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Section: Discussionmentioning

confidence: 99%

High COX‐2 expression in cancer‐associated fibiroblasts contributes to poor survival and promotes migration and invasiveness in nasopharyngeal carcinoma

Zhu

Chen

Zeng

et al. 2019

Molecular Carcinogenesis

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“…95,[98][99][100] Expression of COX-2 specifically in IMCs protects mice from tissue damage and mucosal repair caused by irradiation, DSS administration, or biopsy injury. 25,101,102 Expression of COX-2 by IMCs is regulated by cytokines (such as TNF and IL-1), microbial products (such as lipoproteins), and growth factors (such as insulin-like growth factor 2 messenger RNA binding protein 1 [IGF2BP1] and FGF9). [25][26][27]103,104 Interestingly, mesenchymal stem cells in the lamina propria express the highest levels of COX-2 and localize to sites of injury where they reposition themselves to mediate tissue repair via MYD88 signaling.…”

Section: Prostaglandin-endoperoxide Synthase 2 (Ptgs2 or Cyclooxygenamentioning

confidence: 99%

Mesenchymal Cells in Colon Cancer

et al. 2017

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Mesenchymal cells in the intestine comprise a variety of cell types of diverse origins, functions, and molecular markers. They provide mechanical and structural support and have important functions during intestinal organogenesis, morphogenesis, and homeostasis. Recent studies of the human transcriptome have revealed their importance in the development of colorectal cancer, and studies from animal models have provided evidence for their roles in the pathogenesis of colitis-associated cancer and sporadic colorectal cancer. Mesenchymal cells in tumors, called cancer-associated fibroblasts, arise via activation of resident mesenchymal cell populations and the recruitment of bone marrow-derived mesenchymal stem cells and fibrocytes. Cancer-associated fibroblasts have a variety of activities that promote colon tumor development and progression; these include regulation of intestinal inflammation, epithelial proliferation, stem cell maintenance, angiogenesis, extracellular matrix remodeling, and metastasis. We review the intestinal mesenchymal cell-specific pathways that regulate these processes, with a focus on their roles in mediating interactions between inflammation and carcinogenesis. We also discuss how increasing our understanding of intestinal mesenchymal cell biology and function could lead to new strategies to identify and treat colitis-associated cancers.

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“…Together, they play a vital role in the production of prostaglandins that can have both growth-stimulatory and antiapoptotic effects (25). Ptgs1 and -2 have also been shown to play a significant role in protection of the intestine from both irradiation and DSS-mediated damage (24,26,27), primarily though the production of PGE 2 . Recently PGE 2 was shown to transactivate the canonical Wnt signaling pathway (28).…”

Section: Introductionmentioning

confidence: 99%

Myd88-dependent positioning of Ptgs2-expressing stromal cells maintains colonic epithelial proliferation during injury

Brown¹,

Riehl²,

Walker³

et al. 2007

J. Clin. Invest.

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237

205

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We identified cellular and molecular mechanisms within the stem cell niche that control the activity of colonic epithelial progenitors (ColEPs) during injury. Here, we show that while WT mice maintained ColEP proliferation in the rectum following injury with dextran sodium sulfate, similarly treated Myd88 -/-(TLR signaling-deficient) and prostaglandin-endoperoxide synthase 2 -/-(Ptgs2 -/-) mice exhibited a profound inhibition of epithelial proliferation and cellular organization within rectal crypts. Exogenous addition of 16,16-dimethyl PGE 2 (dmPGE 2 ) rescued the effects of this injury in both knockout mouse strains, indicating that Myd88 signaling is upstream of Ptgs2 and PGE 2 . In WT and Myd88 -/-mice, Ptgs2 was expressed in scattered mesenchymal cells. Surprisingly, Ptgs2 expression was not regulated by injury. Rather, in WT mice, the combination of injury and Myd88 signaling led to the repositioning of a subset of the Ptgs2-expressing stromal cells from the mesenchyme surrounding the middle and upper crypts to an area surrounding the crypt base adjacent to ColEPs. These findings demonstrate that Myd88 and prostaglandin signaling pathways interact to preserve epithelial proliferation during injury using what we believe to be a previously undescribed mechanism requiring proper cellular mobilization within the crypt niche.

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Prostaglandin E2 reduces radiation-induced epithelial apoptosis through a mechanism involving AKT activation and bax translocation

Cited by 33 publications

References 51 publications

High COX‐2 expression in cancer‐associated fibiroblasts contributes to poor survival and promotes migration and invasiveness in nasopharyngeal carcinoma

High COX‐2 expression in cancer‐associated fibiroblasts contributes to poor survival and promotes migration and invasiveness in nasopharyngeal carcinoma

Mesenchymal Cells in Colon Cancer

Myd88-dependent positioning of Ptgs2-expressing stromal cells maintains colonic epithelial proliferation during injury

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