SDF-1α stimulates JNK3 activity via eNOS-dependent nitrosylation of MKP7 to enhance endothelial migration

Pi, Xinchun; Wu, Yaxu; Ferguson, James E.; Portbury, Andrea L.; Patterson, Cam

doi:10.1073/pnas.0809568106

Cited by 74 publications

(60 citation statements)

References 43 publications

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“…Although it has been reported that ADM promotes angiogenesis in vitro through the activation of some signaling pathways (38), the nature of TAM-derived ADM and its mechanism involved in angiogenesis and tumor growth merit further studies. The activation of eNOS in endothelial cells is an important intracellular signaling event for angiogenesis (40)(41)(42). VEGF, similar to ADM, is a proangiogenic factor, which enhances angiogenesis through the activation of eNOS signaling pathway (43).…”

Section: Discussionmentioning

confidence: 99%

Tumor-Associated Macrophages Promote Angiogenesis and Melanoma Growth via Adrenomedullin in a Paracrine and Autocrine Manner

Chen

Huang

Bong

et al. 2011

Clinical Cancer Research

180

185

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Purpose: Elevated numbers of tumor-associated macrophages (TAM) in the tumor microenvironment are often correlated with poor prognosis in melanoma. However, the mechanisms by which TAMs modulate melanoma growth are still poorly understood. This study was aimed at examining the function and mechanism of TAM-derived adrenomedullin (ADM) in angiogenesis and melanoma growth.Experimental Design: We established in vitro and in vivo models to investigate the relationship between TAMs and ADM in melanoma, the role and mechanism of ADM in TAM-induced angiogenesis and melanoma growth. The clinical significance of ADM and its receptors was evaluated using melanoma tissue microarrays.Results: ADM was expressed by infiltrating TAMs in human melanoma, and its secretion from macrophages was upregulated upon coculture with melanoma cells, or with melanoma cells conditioned media. Meanwhile, TAMs enhanced endothelial cell migration and tubule formation and also increased B16/F10 tumor growth. Neutralizing ADM antibody and ADM receptor antagonist, AMA, attenuated TAM-induced angiogenesis in vitro and melanoma growth in vivo, respectively. Furthermore, ADM promoted angiogenesis and melanoma growth via both the paracrine effect, mediated by the endothelial nitric oxide synthase signaling pathway, and the autocrine effect, which stimulated the polarization of macrophages toward an alternatively activated (M2) phenotype. Finally, immunofluorescence analysis on human melanomas showed that the expression of ADM in TAMs and its receptors was greatly increased compared with adjacent normal skins.Conclusion: Our study reveals a novel mechanism that TAMs enhance angiogenesis and melanoma growth via ADM and provides potential targets for melanoma therapies.

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Section: Discussionmentioning

confidence: 99%

Tumor-Associated Macrophages Promote Angiogenesis and Melanoma Growth via Adrenomedullin in a Paracrine and Autocrine Manner

Chen

Huang

Bong

et al. 2011

Clinical Cancer Research

180

185

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“…11 This pathway is regulated by eNOS at several levels: CXCR4 signaling is eNOS dependent, and upregulation of matrix metalloproteinase-9 and release of soluble kit ligand are impaired in eNOSknockout mice. 12,13 Interestingly, a single dose of AMD injected under steady-state conditions has been shown to increase circulating levels of SDF-1 and to mobilize hematopoietic progenitors through CXCR4-dependent active secretion of SDF-1 by BM stromal cells.…”

Section: How Can a Short-acting Drug Antagonizing Cxcr4 Develop Sustamentioning

confidence: 99%

A Quick Fix?

Limbourg

2013

Circulation

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“…40,41 Additionally, JNK1 dominant-negative expression suppresses the VEGF-induced proliferation and migration of endothelial cells. 42 JNK3 also promotes endothelial cell migration to facilitate angiogenesis 43 ( Fig. 1).…”

Section: Jnk Isoforms Increase Angiogenesismentioning

confidence: 99%

“…Recently, the influence of JNK3 in the circulatory system, including its importance in angiogenesis, was demonstrated. 43 JNK3 is inactivated by promoter methylation in a variety of cancer cell lines, both immune and epithelial in origin. 111 Its function in the prevention of cytokine-mediated apoptosis in pancreatic β-cells has also been noted recently.…”

Section: Differential Roles For Jnk Isoformsmentioning

confidence: 99%

“…89 If JNKdependent CCL2 production occurs in secondary site cells or in CTCs during metastasis, then this will recruit VEGF-secreting macrophages, leading to endothelial barrier disruption and tumor cell extravasation. Considering the role of JNK3 in endothelial cell mobilization during angiogenesis, 43 it may also contribute to barrier disruption during extravasation (Fig. 2).…”

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confidence: 99%

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c-Jun N-Terminal Kinases Mediate a Wide Range of Targets in the Metastatic Cascade

2013

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Disseminated cancer cells rely on intricate interactions among diverse cell types in the tumor-associated stroma, vasculature, and immune system for survival and growth. Ubiquitous expression of c-Jun N-terminal kinase (jnk) genes in various cell types permits their control of metastasis. In early stages of metastasis, JNKs affect tumor-associated inflammation and angiogenesis as well as tumor cell migration and intravasation. Within the tumor stroma, JNKs are essential for the release of growth factors that promote epithelial-to-mesenchymal transition (EMT) in tumor cells. JNK3, the least ubiquitous isoform, facilitates angiogenesis by increasing endothelial cell migration. Importantly, JNK expression in tumor cells integrates stromal signals to promote tumor cell invasion. However, JNK isoforms differentially regulate migration toward the endothelial barrier. Once tumor cells enter the bloodstream, JNKs increase circulating tumor cell (CTC) survival and homing to tissues. By promoting fibrosis, JNKs improve CTC attachment to the endothelium. Once anchored, JNKs stimulate EMT to facilitate tumor cell extravasation and enhance the secretion of endothelial barrier disrupters. Tumor cells attract barrier-disrupting macrophages by JNK-dependent transcription of macrophage chemoattractant molecules. In the secondary tissue, JNKs are instrumental in the premetastatic niche and stimulate tumor cell proliferation. JNK expression in cancer cells stimulates tissue-remodeling macrophages to improve tumor colonization. However, in T-cells, JNKs alter cytokine production that increases tumor surveillance and inhibits the recruitment of tissue-remodeling macrophages. Therapeutically targeting JNKs for metastatic disease is attractive considering their promotion of metastasis; however, specific JNK tools are needed to determine their definitive actions within the context of the entire metastatic cascade.

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SDF-1α stimulates JNK3 activity via eNOS-dependent nitrosylation of MKP7 to enhance endothelial migration

Cited by 74 publications

References 43 publications

Tumor-Associated Macrophages Promote Angiogenesis and Melanoma Growth via Adrenomedullin in a Paracrine and Autocrine Manner

Tumor-Associated Macrophages Promote Angiogenesis and Melanoma Growth via Adrenomedullin in a Paracrine and Autocrine Manner

A Quick Fix?

c-Jun N-Terminal Kinases Mediate a Wide Range of Targets in the Metastatic Cascade

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