Absence of DICER1, CTCF, RPL22, DNMT3A, TRRAP, IDH1 and IDH2 hotspot mutations in patients with various subtypes of ovarian carcinomas

Zou, Yang; Huang, Meizhen; Liu, Faying; Yang, Bicheng; Wang, Liqun; Wang, Feng; Yu, Xiaohong; Wan, Lei; Wan, Xi-di; Xu, Xiaoyun; Li, Wei; Huang, Ouping; He, Ming

doi:10.3892/br.2014.378

Cited by 15 publications

(12 citation statements)

References 39 publications

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“…In recent years, many studies have investigated the molecular basis of ovarian SLCT. Consistent literature data support the role of DICER1 in the disease pathogenesis [13,14,[34][35][36][37][38][39][40][41][42].…”

Section: Discussionsupporting

confidence: 76%

“…In the recent years, many studies have investigated the molecular basis of ovarian SCST [ 34 , 35 , 36 , 37 , 38 , 39 , 40 , 41 , 42 ]. In 2012, using a combination of whole transcriptome and whole exome sequencing analyses, Heravi-Moussavi et al sequenced 14 non-epithelial ovarian tumors identifying closely clustered missense mutations in the region of DICER1 gene encoding the RNase IIIb domain in a total of four samples [ 35 ].…”

Section: Dicer1 Somatic Mutations In Ovarian Sertoli–leydig Cell Tumormentioning

confidence: 99%

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Spectrum of DICER1 Germline Pathogenic Variants in Ovarian Sertoli–Leydig Cell Tumor

Paolis

Paragliola

Concolino

2021

JCM

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Sertoli–Leydig Cell Tumors (SLCTs) are rare ovarian sex cord-stromal neoplasms, which predominantly affect adolescents and young female adults. The SLCTs clinical diagnosis and treatment remains challenging due to the rarity and the varied presentation. A large majority of SLCTs are unilateral, but also bilateral neoplasms have been reported, sometimes in the context of DICER1 syndrome. In fact, the most significant discovery regarding the molecular genetics basis of SLCTs was the finding of somatic and germline pathogenic variants in the DICER1 gene. The DICER1 protein is a key component of the micro-RNA processing pathway. Germline DICER1 pathogenic variants are typically inherited in an autosomal dominant pattern and are most often loss-of-function variants dispersed along the length of the gene. Contrarily, DICER1-related tumors harbor a characteristic missense “RNase IIIb hotspot” mutation occurring in trans, or, less frequently, loss of heterozygosity (LOH) event involving the wild-type allele. While DICER1 mutations have been identified in approximately 60% of SLCTs, especially in the moderately or poorly differentiated types, there are only a few case reports of ovarian SLCT with underlying germline DICER1 mutations. In this review, we focus on the molecular genetic features of SLCT, performing an extensive survey of all germline pathogenic variants modifying the whole sequence of the DICER1 gene. We point out that DICER1 genetic testing, coupled with an accurate variants classification and timely counseling, is of crucial importance in the clinical management of ovarian SLCT-affected patients.

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Section: Discussionsupporting

confidence: 76%

Section: Dicer1 Somatic Mutations In Ovarian Sertoli–leydig Cell Tumormentioning

confidence: 99%

Spectrum of DICER1 Germline Pathogenic Variants in Ovarian Sertoli–Leydig Cell Tumor

Paolis

Paragliola

Concolino

2021

JCM

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“…Examination of copy number loss of DICER in TCGA datasets revealed frequent loss of DICER in high-grade serous EOC, consistent with low levels of expression and association with poor clinical outcome (10). However, DICER functional mutations are not recurrent in high-grade serous ovarian cancer (16, 35, 36). Liang et al (37) studied single nucleotide polymorphisms from 8 miRNA processing genes and 134 microRNA-binding sites in genes in 339 EOC cases and 349 healthy controls.…”

Section: Discussionmentioning

confidence: 99%

The role of MicroRNA molecules and MicroRNA-regulating machinery in the pathogenesis and progression of epithelial ovarian cancer

Wang

Ivan

Hawkins

2017

Gynecologic Oncology

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MicroRNA molecules are small, single-stranded RNA molecules that function to regulate networks of genes. They play important roles in normal female reproductive tract biology, as well as in the pathogenesis and progression of epithelial ovarian cancer. DROSHA, DICER, and Argonaute proteins are components of the microRNA-regulatory machinery and mediate microRNA production and function. This review discusses aberrant expression of microRNA molecules and microRNA-regulating machinery associated with clinical features of epithelial ovarian cancer. Understanding the regulation of microRNA molecule production and function may facilitate the development of novel diagnostic and therapeutic strategies to improve the prognosis of women with epithelial ovarian cancer. Additionally, understanding microRNA molecules and microRNA-regulatory machinery associations with clinical features may influence prevention and early detection efforts.

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“…mRNAs encoding three types of DNA methyltransferase genes and the protein expressed by them are highly expressed (15). Furthermore, a large number of studies indicate that the three can lead to abnormal DNA methylation of suppressor genes in cancer cells and silencing through direct or synergistic effects (15,16). Consequently, DNA transmethylase plays an important role in methylation start-up and maintenance in tumor cells.…”

Section: Discussionmentioning

confidence: 99%

Downregulation of DNMT3a expression increases miR-182-induced apoptosis of ovarian cancer through caspase-3 and caspase-9-mediated apoptosis and DNA damage response

Lü

Wei

2016

Oncology Reports

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In the present study, DNA (cytosine-5)-methyltransferase 3α (DNMT3a) is explored as an anticancer molecule in ovarian cancer treatment, and also the mechanistic link between DNMT3a and its regulatory signaling pathway in Caov-3 cells is provided. Firstly, DNMT3a protein expression in 12 freshly resected ovarian cancer patient tissues and tisssues from 8 ovariectomized patients was assessed. In the ovarian cancer tissues, DNMT3a expression was upregulated and miR-182 expression was downregulated. DNMT3a overexpression inhibited miR-182 expression and caspase-3 and -9 activity and suppressed p53 and c-Myc protein expression in Caov-3 cells. Secondly, miR-182 overexpression increased Caov-3 cell apoptosis, which however was reduced by DNMT3a (DNMT3 plasmid) overexpression. Downregulation of DNMT3a expression activated miR-182 expression and caspase-3 and -9 activity, and promoted p53 and c-Myc protein expression in Caov-3 cells. Collectively, a valuable anticancer mechanism of ovarian cancer was elucidated, by which downregulation of DNMT3a regulated miR-182 via caspase-3 and -9-mediated apoptosis and DNA damage response, which suggests that DNMT3a may be used as a potential strategy for therapeutic intervention in ovarian cancer.

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Absence of DICER1, CTCF, RPL22, DNMT3A, TRRAP, IDH1 and IDH2 hotspot mutations in patients with various subtypes of ovarian carcinomas

Cited by 15 publications

References 39 publications

Spectrum of DICER1 Germline Pathogenic Variants in Ovarian Sertoli–Leydig Cell Tumor

Spectrum of DICER1 Germline Pathogenic Variants in Ovarian Sertoli–Leydig Cell Tumor

The role of MicroRNA molecules and MicroRNA-regulating machinery in the pathogenesis and progression of epithelial ovarian cancer

Downregulation of DNMT3a expression increases miR-182-induced apoptosis of ovarian cancer through caspase-3 and caspase-9-mediated apoptosis and DNA damage response

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