X-chromosome association study reveals genetic susceptibility loci of nasopharyngeal carcinoma

Zuo, Xiao Yu; Feng, Qi Sheng; Sun, Jian; Wei, Pan; Chin, Yoon Ming; Guo, Yun; Xia, Yunfei; Li, Bo; Xia, Xiao Jun; Jia, Wei‐Hua; Liu, Jing; Khoo, Alan Soo Beng; Mushiroda, Taisei; Ng, Ching Ching; Su, Wen; Zeng, Yi-Xin; Bei, Jin‐Xin

doi:10.1186/s13293-019-0227-9

Cited by 11 publications

(13 citation statements)

References 39 publications

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“…Its incidence is highest among males and its occurrence is particularly frequent in China. An X chromosome-wide association study for SNPs in 1590 Chinese NPC patients and 994 controls revealed an association within the DMD gene (intronic SNP rs5927056, p = 1.49 × 10 − 5 ), which was validated in Taiwanese and Malaysian replication cohorts [ 26 ]. Combination analyses revealed a consistent association in males and showed that the DMD SNP rs5927056 is associated with a reduced risk of NPC (odds ratio: 0.85, p = 9.44 × 10 − 5 ) [ 26 ].…”

Section: Carcinomasmentioning

confidence: 99%

“…An X chromosome-wide association study for SNPs in 1590 Chinese NPC patients and 994 controls revealed an association within the DMD gene (intronic SNP rs5927056, p = 1.49 × 10 − 5 ), which was validated in Taiwanese and Malaysian replication cohorts [ 26 ]. Combination analyses revealed a consistent association in males and showed that the DMD SNP rs5927056 is associated with a reduced risk of NPC (odds ratio: 0.85, p = 9.44 × 10 − 5 ) [ 26 ]. Additionally, NPC risk association with X chromosome SNPs was found to be decreased by 8.3% after excluding rs5927056, suggesting a strong effect of this locus on NPC susceptibility.…”

Section: Carcinomasmentioning

confidence: 99%

“…IF Δ3–29, IF Δ17–30, OOF Δ42–43 Reduced Dp427m expression, Dp71 maintained, Dp116 frequently absent Tumour suppressor role for Dp427 + [ 21 , 43 ] Lymphoma nd DMD downregulated in tumour vs. progenitor cells. DMD upregulated in EBV-positive vs. EBV-negative tumours nd ++ [ 19 , 43 ] Lymphocytic leukaemia nd DMD upregulated Oncogenic ++(+) [ 20 , 43 , 57 – 59 ] Lung adenocarcinoma nd DMD downregulated Oncogenic role for Dp71 ++ [ 24 , 43 ] Gastric adenocarcinoma nd DMD downregulated, attributed to Dp71 Tumour suppressive role for Dp71 ++ [ 25 ] Nasopharyngeal carcinoma Intronic SNP rs5927056 nd nd, SNP associated with reduced risk ++ [ 26 ] Oropharyngeal squamous cell carcinoma nd DMD downregulated Tumour suppressive ++(+) [ 61 , 62 ] Renal cell carcinoma nd …”

Section: Carcinomasmentioning

confidence: 99%

“…Between 2007 and 2011 several studies have emerged showing that muscular dystrophy mouse models are prone to develop spontaneous soft tissue sarcomas (STS) [15][16][17]. Since then, numerous reports, of increasing frequency, have characterised DMD gene mutations and/or expression changes associated with the development, progression and/or survival of patients with a wide range of cancers including sarcomas, carcinomas, melanomas, lymphomas and leukaemia's, as well as brain tumours [18][19][20][21][22][23][24][25][26]. Although a question of cause or effect remains, it is now clear that a role for DMD in cancer extends beyond just myogenic or musculoskeletal tumours and that the ratio of Dp427 to Dp71 may have particular importance.…”

Section: Introductionmentioning

confidence: 99%

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The Duchenne muscular dystrophy gene and cancer

et al. 2020

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Background Mutation of the Duchenne muscular dystrophy (DMD) gene causes Duchenne and Becker muscular dystrophy, degenerative neuromuscular disorders that primarily affect voluntary muscles. However, increasing evidence implicates DMD in the development of all major cancer types. DMD is a large gene with 79 exons that codes for the essential muscle protein dystrophin. Alternative promotor usage drives the production of several additional dystrophin protein products with roles that extend beyond skeletal muscle. The importance and function(s) of these gene products outside of muscle are not well understood. Conclusions We highlight a clear role for DMD in the pathogenesis of several cancers, including sarcomas, leukaemia’s, lymphomas, nervous system tumours, melanomas and various carcinomas. We note that the normal balance of DMD gene products is often disrupted in cancer. The short dystrophin protein Dp71 is, for example, typically maintained in cancer whilst the full-length Dp427 gene product, a likely tumour suppressor, is frequently inactivated in cancer due to a recurrent loss of 5’ exons. Therefore, the ratio of short and long gene products may be important in tumorigenesis. In this review, we summarise the tumours in which DMD is implicated and provide a hypothesis for possible mechanisms of tumorigenesis, although the question of cause or effect may remain. We hope to stimulate further study into the potential role of DMD gene products in cancer and the development of novel therapeutics that target DMD.

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Section: Carcinomasmentioning

confidence: 99%

Section: Carcinomasmentioning

confidence: 99%

Section: Carcinomasmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

The Duchenne muscular dystrophy gene and cancer

et al. 2020

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“…Nasopharyngeal carcinoma (NPC), an epithelial malignancy, is related to Epstein–Barr virus infection [ 1 ]. The pathogenesis of NPC is multifactorial, such as genetic susceptibility [ 2 ], social practices, and environmental factors [ 3 , 4 ]. NPC is frequent in southern China and Southeast Asia with an incidence of 40 cases per 1,00,000 individuals yearly; however, it is infrequent in Western Europe and North America [ 5 ].…”

Section: Introductionmentioning

confidence: 99%

LncRNA FOXD3-AS1/miR-135a-5p function in nasopharyngeal carcinoma cells

Zhang

Xiang

2020

Open Medicine

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This research aimed to illustrate the biological function and associated regulatory mechanism of lncRNA FOXD3-AS1 (FOXD3-AS1) in nasopharyngeal carcinoma (NPC). This research initially found that FOXD3-AS1 was obviously upregulated in NPC cell lines by quantitative reverse transcription polymerase chain reaction (qRT-PCR) detection. Next, the direct target of FOXD3-AS1 was predicted by bioinformatics and further verified by dual-luciferase reporter assay. MiroRNA-135a-5p (miR-135a-5p) was identified as the target gene of FOXD3-AS1 and down-expressed in C666-1 cells compared to NP69. In addition, function assays were conducted in C666-1 cells, including methyl tetrazolium assay, flow cytometry, Caspase3 activity detection, and western blot assay. Our results suggested that miR-135a-5p upregulation inhibited NPC cell growth, enhanced cell apoptosis, promoted Caspase3 activity, increased cleaved-Caspase3, and reduced pro-Caspase3 level. Moreover, we found that FOXD3-AS1 knockdown notably inhibited C666-1 cell proliferation, increased cell apoptosis, enhanced Caspase3 activity, enhanced cleaved-Caspase3 expression, and suppressed pro-Caspase3 level in C666-1 cells. However, these findings were reversed in C666-1 cells by miR-135a-5p mimic co-transfection. To sum up, our data showed that FOXD3-AS1 knockdown regulated cell growth and apoptosis in NCP cells via altering miR-135a-5p expression, suggesting that FOXD3-AS1 might be a therapeutic target for NPC diagnosis and treatment.

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Towards system genetics analysis of head and neck squamous cell carcinoma using the mouse model, cellular platform, and clinical human data

Zohud,

Lone,

Nashef

et al. 2023

Anim Models and Exp Med

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Head and neck squamous cell cancer (HNSCC) is a leading global malignancy. Every year, More than 830 000 people are diagnosed with HNSCC globally, with more than 430 000 fatalities. HNSCC is a deadly diverse malignancy with many tumor locations and biological characteristics. It originates from the squamous epithelium of the oral cavity, oropharynx, nasopharynx, larynx, and hypopharynx. The most frequently impacted regions are the tongue and larynx. Previous investigations have demonstrated the critical role of host genetic susceptibility in the progression of HNSCC. Despite the advances in our knowledge, the improved survival rate of HNSCC patients over the last 40 years has been limited. Failure to identify the molecular origins of development of HNSCC and the genetic basis of the disease and its biological heterogeneity impedes the development of new therapeutic methods. These results indicate a need to identify more genetic factors underlying this complex disease, which can be better used in early detection and prevention strategies. The lack of reliable animal models to investigate the underlying molecular processes is one of the most significant barriers to understanding HNSCC tumors. In this report, we explore and discuss potential research prospects utilizing the Collaborative Cross mouse model and crossing it to mice carrying single or double knockout genes (e.g. Smad4 and P53 genes) to identify genetic factors affecting the development of this complex disease using genome‐wide association studies, epigenetics, microRNA, long noncoding RNA, lncRNA, histone modifications, methylation, phosphorylation, and proteomics.

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X-chromosome association study reveals genetic susceptibility loci of nasopharyngeal carcinoma

Cited by 11 publications

References 39 publications

The Duchenne muscular dystrophy gene and cancer

The Duchenne muscular dystrophy gene and cancer

LncRNA FOXD3-AS1/miR-135a-5p function in nasopharyngeal carcinoma cells

Towards system genetics analysis of head and neck squamous cell carcinoma using the mouse model, cellular platform, and clinical human data

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