The potential role of DFNA5, a hearing impairment gene, in p53-mediated cellular response to DNA damage

Masuda, Yoshiko; Futamura, Manabu; Kamino, Hiroki; Nakamura, Yasuyuki; Kitamura, Noriaki; Ohnishi, Shiho; Miyamoto, Yuji; Ichikawa, Hitoshi; Ohta, Tsutomu; Ohki, Masafumi; Kiyono, Tohru; Egami, Hiroshi; Baba, Hideo; Arakawa, Hirofumi

doi:10.1007/s10038-006-0004-6

Cited by 103 publications

(98 citation statements)

References 31 publications

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“…However, since its identification, the small number of papers published on DFNA5 almost all point to a possible involvement in cancer biology. [10][11][12][13][14][15][16] Especially during the last 3 years, DFNA5 emerged from several genomic screens identifying new tumor suppressor genes. Further analysis showed that the DFNA5 gene is epigenetically inactivated in several types of cancer, including gastric, colorectal and breast cancer.…”

Section: Introductionmentioning

confidence: 99%

“…15 These recent data also explain earlier findings that were not well understood at the time, such as the increased resistance to the chemotherapeutic reagent etoposide in melanoma cells with decreased transcription of DFNA5, 11 or the finding that DFNA5 is induced by p53 through a p53-binding site located in intron 1. 12 Webb et al 17 demonstrated that DFNA5 mRNA expression increased after treatment of human acute lymphoblastic leukemia cell lines with the glucocorticoid dexamethasone. This increase was only found in cells that underwent apoptosis in response to glucocorticoid treatment.…”

Section: Introductionmentioning

confidence: 99%

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The DFNA5 gene, responsible for hearing loss and involved in cancer, encodes a novel apoptosis-inducing protein

et al. 2011

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DFNA5 was first identified as a gene causing autosomal dominant hearing loss (HL). Different mutations have been found, all exerting a highly specific gain-of-function effect, in which skipping of exon 8 causes the HL. Later reports revealed the involvement of the gene in different types of cancer. Epigenetic silencing of DFNA5 in a large percentage of gastric, colorectal and breast tumors and p53-dependent transcriptional activity have been reported, concluding that DFNA5 acts as a tumor suppressor gene in different frequent types of cancer. Despite these data, the molecular function of DFNA5 has not been investigated properly. Previous transfection studies with mutant DFNA5 in yeast and in mammalian cells showed a toxic effect of the mutant protein, which was not seen after transfection of the wild-type protein. Here, we demonstrate that DFNA5 is composed of two domains, separated by a hinge region. The first region induces apoptosis when transfected in HEK293T cells, the second region masks and probably regulates this apoptosis inducing capability. Moreover, the involvement of DFNA5 in apoptosis-related pathways in a physiological setting was demonstrated through gene expression microarray analysis using Dfna5 knockout mice. In view of its important role in carcinogenesis, this finding is expected to lead to new insights on the role of apoptosis in many types of cancer. In addition, it provides a new line of evidence supporting an important role for apoptosis in monogenic and complex forms of HL. Keywords: tumor suppressor; hearing loss; apoptosis; dfna5; cancer; GSEA INTRODUCTION DFNA5 first was discovered in a Dutch family with autosomal dominant hearing loss (HL). 1 Not much was known concerning its cellular function and how its function was related to HL. Recently, a novel mutation in DFNA5 has been identified in a Korean family, totaling five families with DFNA5 HL. 2 These families all have different genomic DFNA5 mutations, but in each case the DFNA5 mRNA transcript skips exon 8, resulting in a frameshift and a premature truncation of the protein. [1][2][3][4][5] These findings have led to the hypothesis that DFNA5-associated HL is attributable to a highly specific gain-of-function mutation, in which skipping of one exon causes disease while mutations in other parts of this gene may not result in HL at all. Further experimental evidence for this hypothesis was provided by the finding that transfection of mutant DFNA5 causes cell death in both yeast 6 and mammalian 7 cells and by the discovery of a new DFNA5 mutation. 8 The latter mutation truncated the protein in the fifth exon, but did not segregate with HL and was present in family members with normal hearing. The hypothesis was further corroborated by a mouse that lacked the Dfna5 protein. This knockout (KO) mouse did not display any HL and, as a consequence, was not a suitable animal model to study DFNA5-associated HL. 9 To date, little information is available on the physiological function of DFNA5. However, since its identification, the small num...

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

The DFNA5 gene, responsible for hearing loss and involved in cancer, encodes a novel apoptosis-inducing protein

et al. 2011

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“…We established the p53-knock down (p53-KD) and the control (Cont) cell lines as described previously (3)(4)(5)(6). Briefly, HepG2, LS174T, HCT116 and LC176 cells were infected with SI-MSCV-puro-H1R-p53Ri retrovirus for down-regulation of p53 expression and with SI-MSCV-puro-H1R-control retrovirus for negative control.…”

Section: Rna Interferencementioning

confidence: 99%

“…To identify additional transcriptional targets of p53 in the human genome, we used cDNA microarrays and screened p53-inducible transcripts according to previously described methods (3,5). In these experiments, p21/waf1, whose expression was clearly induced by p53, was used as the positive control; the results indicated that p53 upregulated the expression of approximately 100 genes.…”

Section: Identification Of Tmps As a Novel P53-inducible Genementioning

confidence: 99%

“…Brain-specific angiogenesis inhibitor 1 (BAI1) and thrombospondin 1 (TSP1) suppress angiogenesis and inhibit tumor growth. In our previous studies, we have isolated and characterized additional p53 target genes by using cDNA microarray technology, and we have reported the p53-dependent transcription of genes encoding deafness, autosomal dominant 5 (DFNA5), Semaphorin 3F (SEMA3F), B cell linker protein (BLNK), and unc-5 homolog A (UNC5A) (3)(4)(5)(6). More studies on these target genes would clarify the physiological function of p53 as a tumor suppressor gene.…”

Section: Introductionmentioning

confidence: 99%

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Regulation of apoptosis by p53-inducible transmembrane protein containing sushi domain

Arakara¹

2010

Oncol Rep

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Abstract. The tumor suppressor p53 is a transcription factor that induces the transcription of various target genes in response to DNA damage and it protects the cells from malignant transformation. In this study, we performed cDNA microarray analysis and found that the transmembrane protein containing sushi domain (TMPS) gene, which encodes a putative type I transmembrane protein, is a novel p53-target gene. TMPS contains a sushi domain in the extracellular region, which is associated with protein-protein interaction. TMPS expression is induced by endogenous p53 under genotoxic stress in several cancer cell lines. Reporter assay revealed p53-dependent transactivation of the p53 binding-sites (BSs) located in the intron 1 of TMPS. Chromatin immunoprecipitation (ChIP) assay showed that p53 binds to these BSs in vivo. Overexpression of TMPS induced apoptosis through the activation of caspase-3, 8, and 9 in various cancer cell lines. Moreover, Á-irradiation induced the expression of TMPS mRNA in the spleen and colon of p53 +/+ mice but not in those of p53 -/-mice. These data indicate that TMPS may play a role in p53-dependent apoptosis under DNA damage condition.

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Regulated lytic cell death in breast cancer

Liu

Wang

Xia

et al. 2021

Cell Biology International

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Breast cancer (BC) is a very common cancer among women and one of the primary causes of death in women worldwide. Because BC has different molecular subtypes, the challenges associated with targeted therapy have increased significantly, and the identification of new therapeutic targets has become increasingly urgent. Blocking apoptosis and inhibiting cell death are important characteristics of malignant tumours, including BC. Under adverse conditions, including exposure to antitumour therapy, inhibition of cell death programmes can promote cancerous transformation and the survival of cancer cells. Therefore, inducing cell death in cancer cells is fundamentally important and provides new opportunities for potential therapeutic interventions. Lytic forms of cell death, primarily pyroptosis, necroptosis and ferroptosis, are different from apoptosis owing to their characteristic lysis, that is, the production of cellular components, to guide beneficial immune responses, and the application of lytic cell death (LCD) in the field of tumour therapy has attracted considerable interest from researchers. The latest clinical research results confirm that lytic death signalling cascades involve the BC cell immune response and resistance to therapies used in clinical practice. In this review, we discuss the current knowledge regarding the various forms of LCD, placing a special emphasis on signalling pathways and their implications in BC, which may facilitate the development of novel and optimal strategies for the clinical treatment of BC.

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The potential role of DFNA5, a hearing impairment gene, in p53-mediated cellular response to DNA damage

Cited by 103 publications

References 31 publications

The DFNA5 gene, responsible for hearing loss and involved in cancer, encodes a novel apoptosis-inducing protein

The DFNA5 gene, responsible for hearing loss and involved in cancer, encodes a novel apoptosis-inducing protein

Regulation of apoptosis by p53-inducible transmembrane protein containing sushi domain

Regulated lytic cell death in breast cancer

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