Aberrant expression of LMO4 induces centrosome amplification and mitotic spindle abnormalities in breast cancer cells

Montanez‐Wiscovich, Marjorie; Shelton, Melissa D.; Seachrist, Darcie D.; Lozada, Kristen L.; Johnson, Emhonta; Miedler, John D.; Abdul‐Karim, Fadi W.; Visvader, Jane E.; Keri, Ruth A.

doi:10.1002/path.2762

Cited by 22 publications

(17 citation statements)

References 53 publications

(85 reference statements)

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“…LIM domain only 4 (LMO4) expression is frequently elevated in breast cancer (34). Additional experiments in breast cancer cells from various subtypes demonstrated that LMO4 induced cyclin D1 and cyclin E1 expression to promote cell cycle progression and facilitate cell proliferation (35). The expression of LMO4 was regulated by miR-409-3p in colorectal cancer (50).…”

Section: Discussionmentioning

confidence: 99%

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Long non‑coding RNA SNHG1 promotes breast cancer progression by regulation of LMO4

Xiong

Feng

et al. 2020

Oncol Rep

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Long non-coding RNA (lncRNA) small nucleolar RNA host gene 1 (SNHG1) was reported to be a critical regulator of tumorigenesis and is frequently deregulated in several cancer types. However, the exact mechanism by which SNHG1 contributes to breast cancer progression has not been fully elucidated. The identification of the molecular mechanism of SNHG1 is important for understanding the development of breast cancer and for improving the prognosis of the patients with this disease. In the present study, increased expression levels of SNHG1 were noted in breast cancer tumors following analysis of differentially expressed lncRNAs between 1,063 tumor and 102 normal tissues derived from The Cancer Genome Atlas Breast Invasive Carcinoma (TCGA-BRCA) dataset. This finding was further validated using 50 pairs of normal and tumor tissues that were collected from patients with breast cancer. Notably, SNHG1 expression was significantly correlated with estrogen receptor (ER)/progesterone receptor (PR) negative status (ER -/PR -) and advanced clinical stage in breast cancer tissues. Knockdown of SNHG1 led to cell growth arrest, cell cycle redistribution and cell migration inhibition of breast cancer cells. The miRDB database predicted that miR-573 interacts with SNHG1. RT-PCR confirmed the negative regulation of miR-573 levels by SNHG1 in breast cancer cells and the Dual-luciferase reporter assay confirmed their complementary binding. The repression of miR-573 by SNGH1 decreased LIM domain only 4 (LMO4) mRNA and protein expression levels in the breast cancer cell lines tested and induced the expression of cyclin D1 and cyclin E. In vitro experiments indicated that LMO4 overexpression could reverse siSNHG1-induced cell growth arrest, cell cycle redistribution and inhibition of cell migration in breast cancer cells. Moreover, the tumor xenograft model indicated that SNHG1 knockdown inhibited MDA-MB-231 growth in vivo and LMO4 overexpression reversed the tumor growth inhibition induced by SNHG1 knockdown. The present study demonstrated that SNHG1 acts as a novel oncogene in breast cancer via the SNHG/miR-573/LMO4 axis and that it could be a promising therapeutic target for patients with breast cancer.

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Section: Discussionmentioning

confidence: 99%

“…6A). LMO4 is a transcription factor that activates cyclin D1 and E1 transcription and mediates cell cycle progression (35). Knockdown of SNHG1 reduced cyclin D1 and cyclin E1 mRNA levels (Fig.…”

Section: Snhg1 Knockdown Downregulates Lmo4 Expression and The Expresmentioning

confidence: 99%

Long non‑coding RNA SNHG1 promotes breast cancer progression by regulation of LMO4

Xiong

Feng

et al. 2020

Oncol Rep

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“…It has been reported that LMO4 plays a crucial role in the centrosome cycle as well as cell cycle progression in breast cancer cells. It can regulate several cell cycle-related genes, including cyclin D1, cyclin E, p21, p27 and BRCA1 (11,18). Strikingly, growing evidence indicates that LMO4 can modulate progression of breast cancer cell cycle by indirectly enhancing the expression of G 1 cyclins, such as cyclin D1 and cyclin E, and contributes to the growth of multiple breast cancer cells (19–21).…”

Section: Introductionmentioning

confidence: 99%

The oncoprotein HBXIP activates transcriptional coregulatory protein LMO4 via Sp1 to promote proliferation of breast cancer cells

Lin¹,

Li²,

Liu

et al. 2013

Carcinogenesis

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Hepatitis B X-interacting protein (HBXIP) is an important oncoprotein that plays critical role in the development of cancer. In this study, we report that HBXIP activates LIM-only protein 4 (LMO4), a transcriptional coregulatory protein, in promotion of cell proliferation. We observed that the messenger RNA (mRNA) expression levels of HBXIP were positively associated with those of LMO4 in clinical breast cancer tissues. We further identified that HBXIP upregulated LMO4 at the levels of promoter, mRNA and protein in MCF-7 and LM-MCF-7 breast cancer cell lines. The expression of cyclin D1 and cyclin E, downstream effectors of LMO4, could be upregulated by HBXIP through LMO4. Then, chromatin immunoprecipitation (ChIP) assay revealed that HBXIP was able to interact with the promoter region of LMO4. Electrophoretic mobility shift assay showed that HBXIP occupied the -237/-206 region of LMO4 promoter containing Sp1 binding element. The mutant of Sp1 binding site in the LMO4 promoter impeded the interaction of HBXIP with the promoter. Co-immunoprecipitation, ChIP and luciferase reporter gene assays showed that HBXIP activated LMO4 promoter through binding to Sp1. In function, flow cytometry, 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide, 5-ethynyl-2'-deoxyuridine (EdU) incorporation assays and animal transplantation assays demonstrated that HBXIP-enhanced cell proliferation of breast cancer through upregulating LMO4 in vitro and in vivo. Thus, we concluded that oncoprotein HBXIP is able to activate the transcriptional coregulatory protein LMO4 through transcription factor Sp1 in promotion of proliferation of breast cancer cells. HBXIP may serve as a driver gene to activate transcription in the development of cancer.

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“…Recently, it was reported that LMO4 is a downstream target of ERBB-2 and its signaling protein PI3K and is essential for ERBB2-mediated proliferation and cell cycle progression in ERBB-2-dependent breast cancer cells (Montañez-Wiscovich et al, 2009). Pathological results also showed that the aberrant expression of LMO4 on the centrosome cycle promoted LMO4-induced breast cancer formation (Montañez-Wiscovich et al, 2010). Increasing evidence suggested that the LIM domain of LMO4 protein acted as a docking site for the assembly of multiprotein complexes including HEN1 (Manetopoulos et al, 2003), CtBP-interacting protein and BRCA1 complex (Sum et al, 2002), ERα and MTA1 complex (Singh et al, 2005), Clim-2/ldb-1/Nl1 (Sugihara et al, 1998), DEAF1 (Hahm et al, 2004), peroxisome proliferation-activated receptor-γ (PPARγ) (Schock et al, 2008), cAMP response element-binding protein (CREB) complex (Kashani et al, 2006), glycoprotein 130 complex (Novotny-Diermayr et al, 2005), and transcription modulator Cited2 (Michell et al, 2010), which provided further compelling evidence for LMO4 playing a significant role in cells.…”

Section: Discussionmentioning

confidence: 97%

LMO4 inhibits p53-mediated proliferative inhibition of breast cancer cells through interacting p53

et al. 2012

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Aberrant expression of LMO4 induces centrosome amplification and mitotic spindle abnormalities in breast cancer cells

Cited by 22 publications

References 53 publications

Long non‑coding RNA SNHG1 promotes breast cancer progression by regulation of LMO4

Long non‑coding RNA SNHG1 promotes breast cancer progression by regulation of LMO4

The oncoprotein HBXIP activates transcriptional coregulatory protein LMO4 via Sp1 to promote proliferation of breast cancer cells

LMO4 inhibits p53-mediated proliferative inhibition of breast cancer cells through interacting p53

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