MYBL1 rearrangements and MYB amplification in breast adenoid cystic carcinomas lacking the MYB–NFIB fusion gene

Kim, Ji Sun; Geyer, Felipe C.; Martelotto, Luciano G.; Ng, Charlotte K.Y.; Lim, Raymond S.; Selenica, Pier; Li, Anqi; Pareja, Fresia; Fusco, Nicola; Edelweiss, Marcia; Kumar, Rahul; Gularte‐Mérida, Rodrigo; Forbes, Andre Neil; Khurana, Ekta; Mariani, Odette; Badve, Sunil; Vincent‐Salomon, Anne; Norton, Larry; Reis‐Filho, Jorge S.; Weigelt, Britta

doi:10.1002/path.5006

Cited by 80 publications

(56 citation statements)

References 39 publications

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“…Nuclear factors and their receptors are indispensable in the development of tumor growth, metastasis and epithelial-mesenchymal transition (EMT) in several types of cancers (8). Nuclear factor I/B (NFIB) is a recently discovered member of the nuclear factor family (which includes NFI-A, B and X) and emerging evidence has shown that NFIB, besides functioning during normal somatic development, is also involved in the generation and progression of various types of cancer, including small-cell lung cancer, melanoma and breast cancer, through different molecular mechanisms such as forming the oncogenic NFIB-MYB gene fusion or increasing the chromatin accessibilities of its downstream targets (9)(10)(11). Nevertheless, research on the functions and involvement of NFIB on the development of GC has not been reported yet.…”

Section: Introductionmentioning

confidence: 99%

NFIB promotes cell growth, aggressiveness, metastasis and EMT of gastric cancer through the Akt/Stat3 signaling pathway

Zhu

Liu

et al. 2018

Oncol Rep

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Nuclear factor I/B (NFIB) plays a crucial role in the progression of several types of cancers. However, its role in gastric cancer (GC) remains unclear. The present study revealed that NFIB was highly expressed in GC tissues and was positively associated with the clinicopathological features of GC patients. Downregulation of NFIB inhibited the tumor growth, migration and aggression of MKN45 and HGC27 cells in vitro. In addition, NFIB expression promoted epithelial‑mesenchymal transition (EMT), which was accompanied with decreased E‑cadherin and increased vimentin expression. Since AKT and Stat3 play an important role in EMT and tumor progression, we examined whether there is a correlation between NFIB and AKT/Stat3 signaling pathways in GC. Our results revealed that NFIB exhibits its oncogenic functions in GC development by regulating the phosphorylation of both AKT and Stat3 molecules. Knocking down the NFIB expression may enhance the phosphorylation of AKT while inhibiting the Stat3 phosphorylation, suggesting that the AKT/Stat3 signaling pathway may be the downstream target of NFIB with which it exerts its roles on GC development. These results revealed that NFIB promotes tumor growth and aggressiveness of GC. In addition, downregulation of NFIB alters the protein kinase B/signal transducers and activators of transcription 3 (AKT/Stat3) axis, which could be a potential molecular mechanism for precise target treatment of GC.

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Section: Introductionmentioning

confidence: 99%

NFIB promotes cell growth, aggressiveness, metastasis and EMT of gastric cancer through the Akt/Stat3 signaling pathway

Zhu

Liu

et al. 2018

Oncol Rep

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“…Our results are in line with this study and support the use of MYB IHC as a useful adjunct to establishing the diagnosis of adenoid cystic carcinoma in the breast as well as non‐breast sites. Recent genetic investigations demonstrate that alternative mechanisms for MYB pathway activation including MYB amplification or rearrangement of MYBL1 (a closely related gene with similar function) may be present in a considerable number of ACC cases that lack the classic MYB–NFIB translocation . These provide a logical potential explanation for the observations that MYB expression by immunohistochemistry may be more sensitive for ACC of the breast compared to FISH.…”

Section: Discussionmentioning

confidence: 99%

MYB rearrangement and immunohistochemical expression in adenomyoepithelioma of the breast: a comparison with adenoid cystic carcinoma

et al. 2018

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Our results indicate that AMEs do not harbour MYB gene rearrangement. IHC for MYB may be helpful in diagnosing FISH-negative cases of ACC, particularly the diagnostically more difficult solid variants. However, weak to moderate MYB expression in a subset of AMEs highlights not only a potential diagnostic pitfall, but also shared pathophysiology with ACC worth investigating further at the genomic level.

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“…Salivary gland ACC is driven by the MYB-NFIB gene fusion in the majority of cases, which has also been demonstrated in breast and lacrimal gland ACC, although much fewer cases have been examined (28,29,33,34,161,207). Recently, the identification of the MYBL1-NFIB gene fusion was shown to account for a subset of salivary gland and breast ACC without MYB-NFIB or the expression of MYB protein, whereas MYBL1 is yet to be shown to be involved in lacrimal gland ACC (21,30). We identified a spectrum of genetic abnormalities in salivary gland ACC, including MYB amplification (5 0 ), isolated MYB rearrangement (MYB-X), MYB-NFIB, MYBL1-NFIB, and isolated NFIB rearrangement (NFIB-X).…”

Section: Discussionmentioning

confidence: 99%

Molecular features of adenoid cystic carcinoma with an emphasis on microRNAexpression

Andreasen

2018

APMIS

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MYBL1 rearrangements and MYB amplification in breast adenoid cystic carcinomas lacking the MYB–NFIB fusion gene

Cited by 80 publications

References 39 publications

NFIB promotes cell growth, aggressiveness, metastasis and EMT of gastric cancer through the Akt/Stat3 signaling pathway

NFIB promotes cell growth, aggressiveness, metastasis and EMT of gastric cancer through the Akt/Stat3 signaling pathway

MYB rearrangement and immunohistochemical expression in adenomyoepithelioma of the breast: a comparison with adenoid cystic carcinoma

Molecular features of adenoid cystic carcinoma with an emphasis on microRNAexpression

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