<i>CREB3L2-PPARγ</i> Fusion Mutation Identifies a Thyroid Signaling Pathway Regulated by Intramembrane Proteolysis

Lui, Weng‐Onn; Zeng, Lingchun; Rehrmann, Victoria; Deshpande, Seema S.; Tretiakova, Maria; Kaplan, Edwin L.; Leibiger, Ingo B.; Leibiger, Barbara; Enberg, Ulla; Höög, Anders; Larsson, Catharina; Kroll, Todd G.

doi:10.1158/0008-5472.can-08-1085

Cited by 66 publications

(40 citation statements)

References 56 publications

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“…CREB3L2-PPARG t(3;7)(p25;q34) was previously identified in 1 case of follicular thyroid cancer (15). The tumor harboring this fusion in our cohort showed a 3.6-fold increase in PPARG mRNA levels when compared with its matched normal.…”

Section: Screening For Known Genetic Events In Radiation-exposed Pedisupporting

confidence: 54%

Identification of kinase fusion oncogenes in post-Chernobyl radiation-induced thyroid cancers

Ricarte-Filho¹,

Li²,

et al. 2013

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Exposure to ionizing radiation during childhood markedly increases the risk of developing papillary thyroid cancer. We examined tissues from 26 Ukrainian patients with thyroid cancer who were younger than 10 years of age and living in contaminated areas during the time of the Chernobyl nuclear reactor accident. We identified nonoverlapping somatic driver mutations in all 26 cases through candidate gene assays and next-generation RNA sequencing. We found that 22 tumors harbored fusion oncogenes that arose primarily through intrachromosomal rearrangements. Altogether, 23 of the oncogenic drivers identified in this cohort aberrantly activate MAPK signaling, including the 2 somatic rearrangements resulting in fusion of transcription factor ETS variant 6 (ETV6) with neurotrophic tyrosine kinase receptor, type 3 (NTRK3) and fusion of acylglycerol kinase (AGK) with BRAF. Two other tumors harbored distinct fusions leading to overexpression of the nuclear receptor PPARγ. Fusion oncogenes were less prevalent in tumors from a cohort of children with pediatric thyroid cancers that had not been exposed to radiation but were from the same geographical regions. Radiation-induced thyroid cancers provide a paradigm of tumorigenesis driven by fusion oncogenes that activate MAPK signaling or, less frequently, a PPARγ-driven transcriptional program.

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Section: Screening For Known Genetic Events In Radiation-exposed Pedisupporting

confidence: 54%

Identification of kinase fusion oncogenes in post-Chernobyl radiation-induced thyroid cancers

Ricarte-Filho¹,

Li²,

et al. 2013

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“…19 Another type of the PPARg gene fusion, CREB3L2/ PPARg, has been reported in 1 out of 42 follicular carcinomas. 64 …”

Section: Pax8/pparcmentioning

confidence: 99%

Molecular analysis of thyroid tumors

2011

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“…In addition, most studies have shown that this rearrangement is also seen in follicular adenomas at 2-13% frequency, and in papillary carcinomas with follicular variants at 1-5% frequency [111][112][113]. Rarely, in 1 out of 42 follicular carcinomas, another type of gene rearrangement of PPAR␥ with CREB3L2 (CREB3L2/PPAR ␥) was observed [114].…”

Section: Pax8/pparγ Rearrangementmentioning

confidence: 99%