Differences of molecular expression mechanisms among neural cell adhesion molecule 1, synaptophysin, and chromogranin A in lung cancer cells

Kashiwagi, Kunihiro; Ishii, Jun; Sakaeda, Masashi; Arimasu, Yuu; Shimoyamada, Hiroaki; Sato, Hidemitsu; Miyata, Chie; Kamma, Hiroshi; Aoki, Ichiro; Yazawa, Takuya

doi:10.1111/j.1440-1827.2011.02781.x

Cited by 27 publications

(33 citation statements)

References 49 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…5 ). Furthermore, chromogranin A, CD56, and synaptophysin, are immunohistochemical markers typically expressed in small cell neuroendocrine carcinomas of the lung [23], [24]. However, both keratin-positive and -negative tumors in the KRAS×KIIf/− mice did not express any of these markers ( Fig.…”

Section: Resultsmentioning

confidence: 99%

Loss of the Keratin Cytoskeleton Is Not Sufficient to Induce Epithelial Mesenchymal Transition in a Novel KRAS Driven Sporadic Lung Cancer Mouse Model

et al. 2013

View full text Add to dashboard Cite

Epithelial-to-mesenchymal transition (EMT), the phenotypical change of cells from an epithelial to a mesenchymal type, is thought to be a key event in invasion and metastasis of adenocarcinomas. These changes involve loss of keratin expression as well as loss of cell polarity and adhesion. We here aimed to determine whether the loss of keratin expression itself drives increased invasion and metastasis in adenocarcinomas and whether keratin loss leads to the phenotypic changes associated with EMT. Therefore, we employed a recently described murine model in which conditional deletion of the Keratin cluster II by Cre-recombinase leads to the loss of the entire keratinmultiprotein family. These mice were crossed into a newly generated Cre-recombinase inducible KRAS-driven murine lung cancer model to examine the effect of keratin loss on morphology, invasion and metastasis as well as expression of EMT related genes in the resulting tumors. We here clearly show that loss of a functional keratin cytoskeleton did not significantly alter tumor morphology or biology in terms of invasion, metastasis, proliferation or tumor burden and did not lead to induction of EMT. Further, tumor cells did not induce synchronously expression of vimentin, which is often seen in EMT, to compensate for keratin loss. In summary, our data suggest that changes in cell shape and migration that underlie EMT are dependent on changes in signaling pathways that cause secondary changes in keratin expression and organization. Thus, we conclude that loss of the keratin cytoskeleton per se is not sufficient to causally drive EMT in this tumor model.

show abstract

Section: Resultsmentioning

confidence: 99%

Loss of the Keratin Cytoskeleton Is Not Sufficient to Induce Epithelial Mesenchymal Transition in a Novel KRAS Driven Sporadic Lung Cancer Mouse Model

et al. 2013

View full text Add to dashboard Cite

show abstract

“…3C). Because the correlation between NCAM and NeuroD1 expression has been made via overexpression data and promoter binding predicted in silico, we investigated whether endogenous NeuroD1 directly bound NCAM promoter elements (24,(32)(33)(34). We found 10 consensus E-box CANNTG binding sites upstream of the transcriptional start site in the NCAM promoter.…”

Section: Neurod1 Regulates Survival and Metastasis Of Neuroendocrine mentioning

confidence: 99%

NeuroD1 regulates survival and migration of neuroendocrine lung carcinomas via signaling molecules TrkB and NCAM

Osborne¹,

Larsen

Shields

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Small-cell lung cancer and other aggressive neuroendocrine cancers are often associated with early dissemination and frequent metastases. We demonstrate that neurogenic differentiation 1 (NeuroD1) is a regulatory hub securing cross talk among survival and migratory-inducing signaling pathways in neuroendocrine lung carcinomas. We find that NeuroD1 promotes tumor cell survival and metastasis in aggressive neuroendocrine lung tumors through regulation of the receptor tyrosine kinase tropomyosinrelated kinase B (TrkB). Like TrkB, the prometastatic signaling molecule neural cell adhesion molecule (NCAM) is a downstream target of NeuroD1, whose impaired expression mirrors loss of NeuroD1. TrkB and NCAM may be therapeutic targets for aggressive neuroendocrine cancers that express NeuroD1.bHLH | SCLC

show abstract

“…demonstrated that ASCL1 directly activates miR‐375 , which functions as a sufficient inducer of neuroendocrine differentiation . ASCL1 was also reported to upregulate synaptophysin and increase tumor‐initiating capacity via upregulation of the candidate stem cell markers CD133 and aldehyde dehydrogenase 1A1 (ALDH1A1) …”

Section: Regulation Of the Neuroendocrine Phenotype Via Specific Tranmentioning

confidence: 99%

“…NeuroD1 expressed in a mouse embryonic carcinoma cell line weakly upregulated primitive neuronal/neuroendocrine cell‐specific transcription factors such as POU3F1, POU3F2, ASCL1, hairy and enhancer of split 5 (HES5), and delta‐like 1 (Dll1) as direct transcriptional targets . SmCCs and LCNECs specifically express NeuroD1; in turn, NeuroD1 directly upregulates neural cell adhesion molecule 1 (NCAM1, also known as CD56) and growth modulating molecule insulin‐like growth factor binding protein 2 (IGFBP2) …”

Section: Regulation Of the Neuroendocrine Phenotype Via Specific Tranmentioning

confidence: 99%

Recent advances in histogenesis research of lung neuroendocrine cancers: Evidence obtained from functional analyses of primitive neural/neuroendocrine cell‐specific transcription factors

Yazawa

2015

Pathology International

Self Cite

View full text Add to dashboard Cite

Small cell carcinoma (SmCC) and large cell neuroendocrine carcinoma (LENEC) are categorized as neuroendocrine cancers (NECs) of the lung and have extremely poor prognoses. The lack of an effective therapeutic strategy against SmCC and LCNEC is a serious issue. Because the regulation of the cellular phenotype is complicated by the actions of various transcription factors, investigations into the function of neural/neuroendocrine cell-specific transcription factors are important for elucidating the cellular characteristics and histogenesis of SmCC and LCNEC and for establishing innovative therapeutic strategies against them. In this review, the functions of ASCL1, NeuroD1, REST, TTF1, and class III/IV POU, that are specifically and highly expressed in lung NECs, are introduced. These transcription factors transactivate and/or transrepress various genes and are involved in neural progenitor phenotyping, neuroendocrine and stem cell marker expression, and epithelial-to-mesenchymal transition. Based on the evidence that certain carcinoids express ASCL1, NeuroD1, TTF1, and class III/IV POU and that lung NECs can develop from non-NE cells/non-NEC cells, the relationships among lung NECs, carcinoid tumors, and non-NECs are discussed. Finally, a model of the histogenesis of lung NECs in view of similarities in the expression of primitive neural/neuroendocrine cell-specific transcription factors is proposed.

show abstract

Differences of molecular expression mechanisms among neural cell adhesion molecule 1, synaptophysin, and chromogranin A in lung cancer cells

Cited by 27 publications

References 49 publications

Loss of the Keratin Cytoskeleton Is Not Sufficient to Induce Epithelial Mesenchymal Transition in a Novel KRAS Driven Sporadic Lung Cancer Mouse Model

Loss of the Keratin Cytoskeleton Is Not Sufficient to Induce Epithelial Mesenchymal Transition in a Novel KRAS Driven Sporadic Lung Cancer Mouse Model

NeuroD1 regulates survival and migration of neuroendocrine lung carcinomas via signaling molecules TrkB and NCAM

Recent advances in histogenesis research of lung neuroendocrine cancers: Evidence obtained from functional analyses of primitive neural/neuroendocrine cell‐specific transcription factors

Contact Info

Product

Resources

About