Molecular profiling related to poor prognosis in thyroid carcinoma. Combining gene expression data and biological information

Montero‐Conde, Cristina; Martín‐Campos, Jesús M.; Lerma, Enrique; Gimenez, Gabriel; Martínez-Guitarte, José-Luis; Combalía, Neus; Montaner, David; Matías‐Guiu, Xavier; Dopazo, Joaquı́n; Leiva, Alberto de; Robledo, Mercedes; Mauricio, Dı́dac

doi:10.1038/sj.onc.1210792

Cited by 83 publications

(64 citation statements)

References 42 publications

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“…46 However, approximately 2% to 5% of MEN2 families do not have RET mutations, and many cases of sporadic MTC do not carry RET mutations. 47,48 The absence of RET mutations suggests the existence of additional loci predisposing to MEN2 and sporadic MTC. Other genes, including those encoding components of the retinoblastoma (RB) and P53 tumorsuppressor pathways and RAS proto-oncogene may be involved in MTC formation.…”

Section: Cancermentioning

confidence: 99%

RET gene mutations (genotype and phenotype) of multiple endocrine neoplasia type 2 and familial medullary thyroid carcinoma

Krampitz

Norton

2014

Cancer

114

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The rapid technical advances in molecular biology and accelerating improvements in genomic and proteomic diagnostics have led to increasingly personalized strategies for cancer therapy. Such an approach integrates the genomic, proteomic, and molecular information unique to the individual to provide an accurate genetic diagnosis, molecular risk assessment, informed family counseling, therapeutic profiling, and early preventative management that best fits the particular needs of each patient. The discovery of mutations in the RET proto-oncogene resulting in variable onset and severity of multiple endocrine neoplasia type 2 (MEN2) was the first step in developing direct genetic testing for at-risk individuals. Patients with germline RET mutations may undergo risk assessment and appropriate intervention based on specific mutations. Moreover, family members of affected individuals receive counseling based on understanding of the genetic transmission of the disease. Increasingly, clinicians are able to make therapeutic choices guided by an informative biomarker code. Improvements in detection and management of patients with MEN2 resulting from understanding of the RET proto-oncogene are evidence of the benefits of personalized cancer medicine. This review describes the discovery of the RET proto-oncogene, the association between genotype and phenotype, and the role of mutation analysis on diagnosis and treatment of MEN2. Cancer 2014;120:1920-31.

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Section: Cancermentioning

confidence: 99%

RET gene mutations (genotype and phenotype) of multiple endocrine neoplasia type 2 and familial medullary thyroid carcinoma

Krampitz

Norton

2014

Cancer

114

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“…The over-expression of PKB in poorly differentiated thyroid carcinomas was first demonstrated by Rodrigues et al (2007b), who emphasized the importance of the MAP kinase pathway in the progression of thyroid carcinomas. Montero-Conde et al (2008) investigated differentiated and undifferentiated thyroid tumors by using cDNA microarrays and also reported significant changes in the expression of genes of the MAPK pathway, as well as those of the TGFb pathway, focal adhesion, and activation of actin polymerization and cell cycle. Ito et al (2009) reported the co-expression of S100A8 and A100A9, which represent the S100 calcium-binding proteins A8 and A9, in undifferentiated thyroid carcinomas, and the lack of S100A8 expression and a weak expression of S100A9 in PDTC, and lack of these proteins in well-differentiated DTC.…”

Section: Transcriptome Of Pdtc and Undifferentiated Thyroid Cancer Inmentioning

confidence: 99%

Gene expression profile of human thyroid cancer in relation to its mutational status

Rusinek

Szpak‐Ulczok²,

Jarząb³

2011

Journal of Molecular Endocrinology

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This review describes the gene expression profile changes associated with the presence of different mutations that contribute to thyroid cell carcinogenesis. The results are discussed in the context of thyroid cancer biology and of the implications for disease prognosis, while the diagnostic aspect has been omitted. For papillary thyroid cancer (PTC), the most characteristic gene expression profile is associated with the presence of BRAF mutation. BRAF-associated PTC differ profoundly from RET/PTC or RAS-associated cancers. Simultaneously, they retain many characteristic gene expression features common for all PTCs, induced by the alternative mutations activating MAPK pathway. Although the difference between papillary and follicular thyroid cancer (FTC) is significant at the gene expression profile level, surprisingly, the RAS-related signature of FTC is not well specified. PAX8/peroxisome proliferator-activated receptor g (PPARg) rearrangements, which occur in FTC as an alternative to the RAS mutation, are associated with specific changes in gene expression. Furthermore, the difference between well-differentiated thyroid cancers and poorly differentiated and anaplastic thyroid cancers is mainly a reflection of tumor degree of differentiation and may not be attributed to the presence of characteristic mutations.

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“…10 Taking advantage of the available data from mRNA and miRNA expression from the same tumors, MirRGate, a specific tool for miRNA targets' identification, was used for target prediction (http://mirgate.bioinfo.cnio.es/API/). The miRNA was considered regulatory if its expression was negatively correlated with that of the target mRNA as assessed by Pearson's correlation test.…”

Section: Statistical Analysesmentioning

confidence: 99%

“…Similarly to other genomic features, [8][9][10] the miRNA expression fingerprints have been shown to be subtype-and driver alteration-specific (reviewed in Pallante et al 11 ). Moreover, the role of polymorphisms in the complementary sites of target mRNAs was initially proposed in the context of papillary carcinomas, 12 and polymorphisms in the miRNA sequence itself were shown to be predisposing to thyroid cancer, 13 highlighting the role of miRNAs in thyroid tumorigenesis.…”

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confidence: 99%

MicroRNA deep-sequencing reveals master regulators of follicular and papillary thyroid tumors

et al. 2015

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MicroRNA deregulation could be a crucial event in thyroid carcinogenesis. However, current knowledge is based on studies that have used inherently biased methods. Thus, we aimed to define in an unbiased way a list of deregulated microRNAs in well-differentiated thyroid cancer in order to identify diagnostic and prognostic markers. We performed a microRNA deep-sequencing study using the largest well-differentiated thyroid tumor collection reported to date, comprising 127 molecularly characterized tumors with follicular or papillary patterns of growth and available clinical follow-up data, and 17 normal tissue samples. Furthermore, we integrated microRNA and gene expression data for the same tumors to propose targets for the novel molecules identified. Two main microRNA expression profiles were identified: one common for follicular-pattern tumors, and a second for papillary tumors. Follicular tumors showed a notable overexpression of several members of miR-515 family, and downregulation of the novel microRNA miR-1247. Among papillary tumors, top upregulated microRNAs were miR-146b and the miR-221~222 cluster, while miR-1179 was downregulated. BRAF-positive samples displayed extreme downregulation of miR-7 and -204. The identification of the predicted targets for the novel molecules gave insights into the proliferative potential of the transformed follicular cell. Finally, by integrating clinical follow-up information with microRNA expression, we propose a prediction model for disease relapse based on expression of two miRNAs (miR-192 and let-7a) and several other clinicopathological features. This comprehensive study complements the existing knowledge about deregulated microRNAs in the development of well-differentiated thyroid cancer and identifies novel markers associated with recurrence-free survival.

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Molecular profiling related to poor prognosis in thyroid carcinoma. Combining gene expression data and biological information

Cited by 83 publications

References 42 publications

RET gene mutations (genotype and phenotype) of multiple endocrine neoplasia type 2 and familial medullary thyroid carcinoma

RET gene mutations (genotype and phenotype) of multiple endocrine neoplasia type 2 and familial medullary thyroid carcinoma

Gene expression profile of human thyroid cancer in relation to its mutational status

MicroRNA deep-sequencing reveals master regulators of follicular and papillary thyroid tumors

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