The significance of TNFAIP8 in prostate cancer response to radiation and docetaxel and disease recurrence

Zhang, Chuanbo; Kallakury, Bhaskar; Ross, Jeffrey S.; Mewani, Rajshree R.; Sheehan, Christine E.; Sakabe, Isamu; Luta, George; Kumar, Deepak; Yadavalli, Sivaramakrishna; Starr, Joshua; Sreenath, Taduru; Srivastava, Shiv; Pollard, Harvey B.; Eidelman, Ofer; Srivastava, Meera; Kasid, Usha N.

doi:10.1002/ijc.27996

Cited by 60 publications

(65 citation statements)

References 39 publications

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“…The last exon is common, whereas usage of other exons differs across variants (Supplementary Figure S1). Several reports have shown that TNFAIP8 is overexpressed in human cancers, [3][4][5]8,[19][20][21][22] yet none of these publications have used methods with adequate specificity to discriminate among TNFAIP8 variants. In order to determine the expression patterns of the variants in human tumors compared with normal tissue, we analyzed cataloged RNA-sequencing (RNA-seq) data from primary human tumor and normal tissue for 11 cancer types in The Cancer Genome Atlas (TCGA) (Figure 1a and Supplementary Figure S2A).…”

Section: Resultsmentioning

confidence: 99%

“…Of interest, TNFAIP8 has been proposed to be a scaffolding protein, and both p53 and PCNA were previously identified as potential TNFAIP8-binding partners. 4 It is thus intriguing to consider the possibility that v2 binding may possibly regulate access of acetylases and/or deacetylases to p53. TNFAIP8 could also conceivably regulate the activity of a signaling protein or transcription factor (other than p53 (Figure 5e)) that regulates PCNA expression.…”

Section: Discussionmentioning

confidence: 99%

“…The last exon is common, whereas usage of other exons differs across variants (Supplementary Figure S1). Several reports have shown that TNFAIP8 is overexpressed in human cancers, [3][4][5]8,[19][20][21][22] yet none of these publications have used methods with adequate specificity to discriminate among Abbreviations: BrdU, 5-bromo-2'-deoxyuridine; ChIP-seq, chromatin immunoprecipitation sequencing; DOX, doxorubicin; Gadd45A, growth arrest and DNA damageinducible 45a; H3K4me1, histone H3 mono-methylation on lysine 4; H3K4me3, histone H3 tri-methylation on lysine 4; H3K27ac, histone H3 acetylation on lysine 27; p53RE, p53 response element; PCNA, proliferating cell nuclear antigen; Scri, cells expressing scrambled shRNA; shRNA, short hairpin RNA; TCGA, The Cancer Genome Atlas; TNFAIP8, tumor necrosis factor-α-induced protein 8; TP8i, cells expressing TNFAIP8 shRNA …”

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confidence: 99%

“…1,2 Although little is known about TNFAIP8, it has recently been found to be overexpressed in a wide range of human cancers. Some studies have suggested protumor functions for TNFAIP8, including enhancement of cell survival, proliferation, and metastasis [3][4][5][6][7][8][9] and resistance to cancer chemotherapeutics in mice. 4,10 Nonetheless, nothing is known about how TNFAIP8 influences responses to DNA damage in cancer cells.…”

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confidence: 99%

“…Some studies have suggested protumor functions for TNFAIP8, including enhancement of cell survival, proliferation, and metastasis [3][4][5][6][7][8][9] and resistance to cancer chemotherapeutics in mice. 4,10 Nonetheless, nothing is known about how TNFAIP8 influences responses to DNA damage in cancer cells. Moreover, several transcript variants from the TNFAIP8 gene were recently registered in the NCBI reference sequence database, but no study to date has differentiated among them or defined the factors that govern their expression.…”

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The novel p53 target TNFAIP8 variant 2 is increased in cancer and offsets p53-dependent tumor suppression

et al. 2016

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Tumor necrosis factor-α-induced protein 8 (TNFAIP8) is a stress-response gene that has been associated with cancer, but no studies have differentiated among or defined the regulation or function of any of its several recently described expression variants. We found that TNFAIP8 variant 2 (v2) is overexpressed in multiple human cancers, whereas other variants are commonly downregulated in cancer (v1) or minimally expressed in cancer or normal tissue (v3-v6). Silencing v2 in cancer cells induces p53-independent inhibition of DNA synthesis, widespread binding of p53, and induction of target genes and p53-dependent cell cycle arrest and DNA damage sensitization. Cell cycle arrest induced by v2 silencing requires p53-dependent induction of p21. In response to the chemotherapeutic agent doxorubicin, p53 regulates v2 through binding to an intragenic enhancer, together indicating that p53 and v2 engage in complex reciprocal regulation. We propose that TNFAIP8 v2 promotes human cancer by broadly repressing p53 function, in essence offsetting p53-dependent tumor suppression. Cell Death and Differentiation (2017) 24, 181-191; doi:10.1038/cdd.2016 published online 11 November 2016 Tumor necrosis factor-α-induced protein 8 (TNFAIP8) is the founding member of a recently described family of environmental stress response genes that are induced by TNFα. TNFAIP8 has been shown to promote or inhibit apoptosis, depending on cell type and context. 1,2 Although little is known about TNFAIP8, it has recently been found to be overexpressed in a wide range of human cancers. Some studies have suggested protumor functions for TNFAIP8, including enhancement of cell survival, proliferation, and metastasis [3][4][5][6][7][8][9] and resistance to cancer chemotherapeutics in mice. 4,10Nonetheless, nothing is known about how TNFAIP8 influences responses to DNA damage in cancer cells. Moreover, several transcript variants from the TNFAIP8 gene were recently registered in the NCBI reference sequence database, but no study to date has differentiated among them or defined the factors that govern their expression.The tumor suppressor p53 is a transcription factor that regulates many biological processes through its target gene network. Some of the well-characterized p53 target genes including p21/CDKN1A, growth arrest and DNA damageinducible 45a (GADD45A) and Bcl-2-like protein 4 (BAX) together promote senescence, cell cycle arrest, and apoptosis, all of which may contribute to the tumor suppressing functions of p53. 11,12Additional noncanonical tumorsuppressive pathways from p53 have recently been identified. [13][14][15] Improved characterization of the p53 DNAbinding sequence with modern sequencing techniques has led to the identification of a rapidly expanding list of p53 target genes. [16][17][18] Continued identification of these genes and characterization of their mechanisms of regulation and function will be critical to a full understanding of p53 and for full realization of opportunities to intervene upon p53 in cancer.Here, we identify ...

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

“…The last exon is common, whereas usage of other exons differs across variants (Supplementary Figure S1). Several reports have shown that TNFAIP8 is overexpressed in human cancers, [3][4][5]8,[19][20][21][22] yet none of these publications have used methods with adequate specificity to discriminate among Abbreviations: BrdU, 5-bromo-2'-deoxyuridine; ChIP-seq, chromatin immunoprecipitation sequencing; DOX, doxorubicin; Gadd45A, growth arrest and DNA damageinducible 45a; H3K4me1, histone H3 mono-methylation on lysine 4; H3K4me3, histone H3 tri-methylation on lysine 4; H3K27ac, histone H3 acetylation on lysine 27; p53RE, p53 response element; PCNA, proliferating cell nuclear antigen; Scri, cells expressing scrambled shRNA; shRNA, short hairpin RNA; TCGA, The Cancer Genome Atlas; TNFAIP8, tumor necrosis factor-α-induced protein 8; TP8i, cells expressing TNFAIP8 shRNA …”

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confidence: 99%

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confidence: 99%

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confidence: 99%

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The novel p53 target TNFAIP8 variant 2 is increased in cancer and offsets p53-dependent tumor suppression

et al. 2016

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TNFAIP8 regulates Hippo pathway through interacting with LATS1 to promote cell proliferation and invasion in lung cancer

Tang

Zhao

et al. 2017

Molecular Carcinogenesis

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TNFAIP8 is associated with prognosis of several human malignancies. However, the molecular mechanism of TNFAIP8 in lung cancer remains unknown. In our study, we found TNFAIP8 could enhance TEAD luciferase activity and inhibits the activity of Hippo pathway. TNFAIP8 also increased cyclin D1, CDK6, and decreased p27 in lung cancer cells. In addition, TNFAIP8 increased total YAP protein and promoted nuclear localization of YAP. More importantly, YAP depletion blocked the role of TNFAIP8 on cell cycle-related proteins and TEAD luciferase activity, revealing that TNFAIP8 regulates Hippo pathway in a YAP-dependend manner. Further experiments identified that TNFAIP8 depletion enhanced LATS1 phosphorylation and TNFAIP8 overexpression decreased phosphorylated LAST1 level. LATS1 siRNA treatment reversed the effects of TNFAIP8 plasmid or siRNA on cell cycle proteins. Besides, immunofluorescence and co-immunoprecipitation demonstrated the interaction between TNFAIP8 and LATS1 in H460 and H1299 cells, suggesting that TNFAIP8 regulates Hippo signaling through its interaction with LATS1. Colony formation assays and transwell assays showed that YAP or LATS1 depletion reversed the positive effect of TNFAIP8 on cell proliferation and invasion. TNFAIP8 overexpression could increase MMP-7 and TNFAIP8 depletion could decrease MMP-7 at both protein and mRNA levels, without significant changes of E-cadherin, N-cadherin, and Vimentin. Collectively, the present study provides a novel finding that TNFAIP8 regulates Hippo pathway through interacting with LATS1 to promote cell proliferation and invasion in lung cancer. TNFAIP8 may serve as a candidate biomarker for poor prognosis and a target for new therapies.

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Transcriptome and Proteome Analyses of TNFAIP8 Knockdown Cancer Cells Reveal New Insights into Molecular Determinants of Cell Survival and Tumor Progression

Day

Mewani

Starr

et al. 2016

Methods in Molecular Biology

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Tumor necrosis factor-α-inducible protein 8 (TNFAIP8) is the first discovered oncogenic and an anti-apoptotic member of a conserved TNFAIP8 or TIPE family of proteins. TNFAIP8 mRNA is induced by NF-kB, and overexpression of TNFAIP8 has been correlated with poor prognosis in many cancers. Downregulation of TNFAIP8 expression has been associated with decreased pulmonary colonization of human tumor cells, and enhanced sensitivities of tumor xenografts to radiation and docetaxel. Here we have investigated the effects of depletion of TNFAIP8 on the mRNA, microRNA and protein expression profiles in prostate and breast cancers and melanoma. Depending on the tumor cell type, knockdown of TNFAIP8 was found to be associated with increased mRNA expression of several antiproliferative and apoptotic genes (e.g., IL-24, FAT3, LPHN2, EPHA3) and fatty acid oxidation gene ACADL, and decreased mRNA levels of oncogenes (e.g., NFAT5, MALAT1, MET, FOXA1, KRAS, S100P, OSTF1) and glutamate transporter gene SLC1A1. TNFAIP8 knockdown cells also exhibited decreased expression of multiple onco-proteins (e.g., PIK3CA, SRC, EGFR, IL5, ABL1, GAP43), and increased expression of the orphan nuclear receptor NR4A1 and alpha 1 adaptin subunit of the adaptor-related protein complex 2 AP2 critical to clathrin-mediated endocytosis. TNFAIP8-centric molecules were found to be predominately implicated in the hypoxia-inducible factor-1α (HIF-1α) signaling pathway, and cancer and development signaling networks. Thus TNFAIP8 seems to regulate the cell survival and cancer progression processes in a multifaceted manner. Future validation of the molecules identified in this study is likely to lead to new subset of molecules and functional determinants of cancer cell survival and progression.

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The significance of TNFAIP8 in prostate cancer response to radiation and docetaxel and disease recurrence

Cited by 60 publications

References 39 publications

The novel p53 target TNFAIP8 variant 2 is increased in cancer and offsets p53-dependent tumor suppression

The novel p53 target TNFAIP8 variant 2 is increased in cancer and offsets p53-dependent tumor suppression

TNFAIP8 regulates Hippo pathway through interacting with LATS1 to promote cell proliferation and invasion in lung cancer

Transcriptome and Proteome Analyses of TNFAIP8 Knockdown Cancer Cells Reveal New Insights into Molecular Determinants of Cell Survival and Tumor Progression

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