Familial non-medullary thyroid cancer: unraveling the genetic maze

Yang, Samantha Peiling; Ngeow, Joanne

doi:10.1530/erc-16-0067

Cited by 99 publications

(56 citation statements)

References 120 publications

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“…Functional studies have shown the mutant variant increased tumor colony formation and cell migration consistent with the loss of tumor suppressor effect. The HABP2 G534E variant has also been reported in another cohort in the U.S. [106] but not in the Middle Eastern or UK, or Chinese cohorts [102]. The TTF1 germline mutation has been reported in two families with PTC and coexisting multinodular goiter.…”

Section: Familial Non-medullary Thyroid Cancermentioning

confidence: 93%

“…Known familial tumor syndromes that feature thyroid cancer account for only 5% of all familial non-medullary thyroid cancer (FNMTC). These syndromes include familial adenomatous polyposis (Gardner's syndrome), Cowden syndrome, Werner syndrome, Carney complex, and DICER1 mutation syndrome [102]. Much effort to identify susceptibility genes involved in non-syndromic familial thyroid cancer has resulted in the identification of FOXE1, HABP2, and TITF1.…”

Section: Familial Non-medullary Thyroid Cancermentioning

confidence: 99%

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Multi-omics Signatures and Translational Potential to Improve Thyroid Cancer Patient Outcome

Boufraqech

Nilubol

2019

Cancers

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Recent advances in high-throughput molecular and multi-omics technologies have improved our understanding of the molecular changes associated with thyroid cancer initiation and progression. The translation into clinical use based on molecular profiling of thyroid tumors has allowed a significant improvement in patient risk stratification and in the identification of targeted therapies, and thereby better personalized disease management and outcome. This review compiles the following: (1) the major molecular alterations of the genome, epigenome, transcriptome, proteome, and metabolome found in all subtypes of thyroid cancer, thus demonstrating the complexity of these tumors and (2) the great translational potential of multi-omics studies to improve patient outcome.

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Section: Familial Non-medullary Thyroid Cancermentioning

confidence: 93%

Section: Familial Non-medullary Thyroid Cancermentioning

confidence: 99%

Multi-omics Signatures and Translational Potential to Improve Thyroid Cancer Patient Outcome

Boufraqech

Nilubol

2019

Cancers

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“…If the genetic background of DTC is strong, linkage analyses should easily uncover predisposing loci in affected families. However, such linkage analyses have identified only a handful of genes; driver mutations existed in single families and they were absent in sporadic DTC [12]. Therefore, it seems that the genetic predisposition to DTC is probably polygenic with low-penetrance genes involved.…”

Section: Reviewmentioning

confidence: 99%

Clinical implications of GWAS variants associated with differentiated thyroid cancer

Jendrzejewski

Sworczak

Comiskey

et al. 2019

Endokrynologia Polska

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The genetic risk of differentiated thyroid cancer (DTC) probably consists of multiple low-penetrance, single-nucleotide polymorphisms (SNP). Such markers are difficult to uncover by linkage analysis but can be revealed by association studies. Genome-wide association studies (GWASs) have uncovered 31 SNPs associated with DTC. These markers carry a low to moderate risk for DTC, but their cumulative effect increases with each successive risk allele. These data support the important contribution of low penetrance variants in the pathogenesis of DTC. Contrary to somatic mutations such as BRAFV600E, germline variants can be ascertained prior to surgical treatment. Therefore, we hypothesise that GWAS SNPs might impact the clinical course of DTC and we can benefit from this knowledge in choosing a treatment strategy. Several associations between clinical factors and GWAS markers have been reported so far. The most important are associations between rs966423 and mortality (HR = 1.60, p = 0.038), extrathyroidal extension (ETE) (OR = 1.57, p = 0.019); rs965513 and tumour diameter (slope of regression 0.14, p = 0.025), lymph node metastasis (OR = 1.59, p = 0.030) and ETE (OR = 1.29, p = 0.045); rs944289 and distant metastasis (OR = 0.58, p = 0.042); and rs116909374 and lymph node metastasis (OR = 0.61, p = 0.016). These findings show that GWAS SNPs are not only the ignition factors (together with environmental factors) for malignant transformation of thyrocytes but might also impact the clinical course of DTC. Surprisingly, it is not always the risk allele for DTC that is associated with worse clinical outcome. The second interesting observation is that GWAS SNPs show different associations with DTC clinical features depending on their histological subtypes. These point to the complexity of DTC with putatively different roles of genes at different stages of DTC development.

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“…Die Diagnosestellung erfolgt meist im jungen Erwachsenenalter, selten früher oder nach dem 50. LJ [4,22] Bis zu 60 % der Patienten zeigen insbesondere in Kindheit/Adoleszenz eine Schilddrüsenbeteiligung in Form von unspezifischen zystischen Veränderun-gen (75 %), meist follikulären Adenomen (25 %) und selten (<10 %) papillären oder follikulären Karzinomen [19,21].…”

Section: Carney-komplexunclassified

Syndrome mit breitem Tumorspektrum

Steinke‐Lange

Becker

Behnecke

et al. 2017

Medizinische Genetik

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Zusammenfassung Die klinische Diagnose erblicher Tumorsyndrome ist ein wesentlicher Bestandteil der humangenetischen Beratung. Bei seltenen Syndromen, die mit einem breiten Spektrum an Tumoren und phänotypischen Überschneidungen einhergehen, ist dies nicht immer einfach. In diesem Artikel sollen deshalb die typischen und wegweisenden Merkmale der wichtigsten seltenen Tumordispositionssyndrome mit breitem Tumorspektrum herausgearbeitet werden. Hierzu gehören der Carney-Komplex, das Cowden-Syndrom, die juvenile Polyposis, das Li-Fraumeni-Syndrom und das Peutz-Jeghers-Syndrom. Darüber hinaus sind auch die derzeit empfohlenen Früherkennungsuntersuchungen dargestellt, die meist eine interdisziplinäre Betreuung der Patienten erforderlich machen.

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Familial non-medullary thyroid cancer: unraveling the genetic maze

Cited by 99 publications

References 120 publications

Multi-omics Signatures and Translational Potential to Improve Thyroid Cancer Patient Outcome

Multi-omics Signatures and Translational Potential to Improve Thyroid Cancer Patient Outcome

Clinical implications of GWAS variants associated with differentiated thyroid cancer

Syndrome mit breitem Tumorspektrum

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