TGLI1 transcription factor mediates breast cancer brain metastasis via activating metastasis-initiating cancer stem cells and astrocytes in the tumor microenvironment

Sirkisoon, Sherona; Carpenter, Richard L.; Rimkus, Tadas; Doheny, Daniel; Zhu, Dongqin; Aguayo, Noah R.; Xing, Fei; Chan, Michael D.; Ruiz, Jimmy; Metheny-Barlow, Linda J.; Strowd, Roy E.; Lin, Jiayuh; Regua, Angelina T.; Arrigo, Austin; Anguelov, Marlyn; Pasche, Boris; Debinski, Waldemar; Watabe, Kounosuke; Lo, Hui-Wen

doi:10.1038/s41388-019-0959-3

Cited by 65 publications

(68 citation statements)

References 40 publications

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“…We have optimized conditions to reliably separate two GLI1 isoforms by SDS-PAGE and validated custom-made antibodies to specifically detect tGLI1. However, the difficulty in separating the two proteins could mean that functions previously ascribed to GLI1 are actually due to tGLI1-specific activity [25,33]. Our laboratory, and others, have shown the tGLI1 variant to be expressed in most GBM specimens and patient-derived xenografts, but undetectable in normal brain cells or tissues [24,26,27,29].…”

Section: Glioblastomamentioning

confidence: 90%

“…GLI1 proteins regulate the expression of the pluripotency factors Nanog, octamer binding transcription factor 4 (OCT4), SOX2, WNT-2, CD44, and Kruppel-like factor 4 (KLF4) [148,165,167,168]. Recently, we have shown the novel tGLI1 isoform to promote the glioma stem cell population via upregulation of CD44 and the breast cancer stem cell population through upregulation of CD44, Nanog, OCT4, and Sox2 (Section 6) [31,33]. These data demonstrate that amplified SHH signaling is important for the self-renewal and maintenance of CSCs.…”

Section: Cancer Stem Cellsmentioning

confidence: 99%

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Hedgehog Signaling and Truncated GLI1 in Cancer

Doheny

Manore

Wong

et al. 2020

Cells

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108

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The hedgehog (HH) signaling pathway regulates normal cell growth and differentiation. As a consequence of improper control, aberrant HH signaling results in tumorigenesis and supports aggressive phenotypes of human cancers, such as neoplastic transformation, tumor progression, metastasis, and drug resistance. Canonical activation of HH signaling occurs through binding of HH ligands to the transmembrane receptor Patched 1 (PTCH1), which derepresses the transmembrane G protein-coupled receptor Smoothened (SMO). Consequently, the glioma-associated oncogene homolog 1 (GLI1) zinc-finger transcription factors, the terminal effectors of the HH pathway, are released from suppressor of fused (SUFU)-mediated cytoplasmic sequestration, permitting nuclear translocation and activation of target genes. Aberrant activation of this pathway has been implicated in several cancer types, including medulloblastoma, rhabdomyosarcoma, basal cell carcinoma, glioblastoma, and cancers of lung, colon, stomach, pancreas, ovarian, and breast. Therefore, several components of the HH pathway are under investigation for targeted cancer therapy, particularly GLI1 and SMO. GLI1 transcripts are reported to undergo alternative splicing to produce truncated variants: loss-of-function GLI1ΔN and gain-of-function truncated GLI1 (tGLI1). This review covers the biochemical steps necessary for propagation of the HH activating signal and the involvement of aberrant HH signaling in human cancers, with a highlight on the tumor-specific gain-of-function tGLI1 isoform.

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Section: Glioblastomamentioning

confidence: 90%

Section: Cancer Stem Cellsmentioning

confidence: 99%

Hedgehog Signaling and Truncated GLI1 in Cancer

Doheny

Manore

Wong

et al. 2020

Cells

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108

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“…42 TGLI1 may also contribute to radioresistance by increasing stemness and creating a "metastasis-friendly" microenvironment through activation of astrocytes. 42 Fatty acid binding protein 7 (FABP-7) is a lipid binding protein found specifically in the brain. However, FABP-7 is also expressed in BC cells, particularly Recent progress in the field of cell-and viral-based therapeutics has also been applied to HER2+ BCBrM.…”

Section: Mouse Models Of Her2+ Bcbrmmentioning

confidence: 99%

HER2‐positive breast cancer brain metastasis: A new and exciting landscape

Zimmer

Swearingen²,

Anders³

2020

Cancer Reports

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Background: Brain metastases (BrM) incidence is 25% to 50% in women with advanced human epidermal growth factor receptor 2 (HER2)-positive breast cancer. Radiation and surgery are currently the main local treatment approaches for central nervous system (CNS) metastases. Systemic anti-HER2 therapy following a diagnosis of BrM improves outcomes. Previous preclinical data has helped elucidate HER2 brain trophism, the blood-brain/blood-tumor barrier(s), and the brain tumor microenvironment, all of which can lead to development of novel therapeutic options. Recent findings: Several anti-HER2 agents are currently available and reviewed here, some of which have recently shown promising effects in BrM patients, specifically. New strategies driven by and focusing on brain metastasis-specific genomics, immunotherapy, and preventive strategies have shown promising results and are under development. Conclusions: The field of HER2+ breast cancer, particularly for BrM, continues to evolve as new therapeutic strategies show promising results in recent clinical trials. Increasing inclusion of patients with BrM in clinical studies, and a focus on assessing their outcomes both intracranially and extracranially, is changing the landscape for patients with HER2+ CNS metastases by demonstrating the ability of newer agents to improve outcomes.

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“…Cancer stem cells (CSCs) contributed to metastasis, recurrence and drug resistance in cancers [11][12][13][14], and previous data suggested that CSCs enrichment contributed to cisplatin-resistance in GC cells [17,18]. Therefore, elimination of CSCs will help to improve chemo-sensitivity in GC cells [19].…”

Section: Discussionmentioning

confidence: 99%

“…Cancer stem cells (CSCs) were a subgroup of cancer cells characterized by high self-renewal abilities [11,12], which sustained the heterogeneity of tumor cells and contributed to metastasis and bad prognosis in GC patients [13,14]. In addition, recent data indicated that CSCs were pivotal for sustaining cisplatinresistance in multiple cancers, such as head and neck squamous cell carcinoma (HNSCC) [15], lung cancer [16] and GC [17,18].…”

Section: Introductionmentioning

confidence: 99%

Low-dose Diosbulbin-B (DB) Regulates Tumor-Intrinsic PD-L1/NLRP3 Signaling Pathway to Increase Cisplatin-Sensitivity in Gastric Cancer (GC)

Qiu

Xue

2020

Preprint

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Background: Generation of cisplatin (DDP)-resistance by gastric cancer (GC) cells seriously limits the therapeutic efficacy of this drug in clinic, and recent data suggested that Diosbulbin-B (DB), the main anti-tumor compound of Dioscorea bulbifera L, was effective to improve cisplatin-sensitivity in GC cells. However, the underlying mechanisms are still largely unknown.Methods: Genes expressions were determined by Real-Time qPCR and Western Blot. Cell viability was evaluated by cell counting kit-8 and trypan blue staining assay. Annexin V-FITC/PI double staining assay was used to examine cell apoptosis. The Spheroid formation assay was used to evaluated cell stemness. Immunohistochemistry (IHC) was employed to examine the expressions and localization of Ki67 protein in mice tumor tissues.Results: Here we found that low-dose DB (12.5 μM) downregulated PD-L1 to activate NLRP3-medicated pyroptosis, and inhibited cancer stem cells (CSCs) properties, to sensitize cisplatin-resistant GC (CR-GC) cells to cisplatin. Mechanistically, the CR-GC cells were obtained, and either low-dose DB or cisplatin alone had little effects on cell viability in CR-GC cells, while low-dose DB significantly induced apoptotic cell death in cisplatin treated CR-GC cells. In addition, low-dose DB triggered cell pyroptosis in CR-GC cells stimulated with cisplatin, which were abrogated by silencing NLRP3. Next, CSCs tended to be enriched in CR-GC cells, instead of their parental cisplatin-sensitive GC (CS-GC) cells, and low-dose DB (12.5 μM) inhibited spheroid formation and stemness biomarkers (CD44, CD133, SOX2, OCT4 and Nanog) expressions to eliminate CSCs in CR-GC cells, which were reversed by upregulating programmed death ligand-1 (PD-L1). Furthermore, we proved that PD-L1 negatively regulated NLRP3 in CR-GC cells, and low-dose DB (12.5 μM) activated NLRP3-mediated pyroptotic cell death in cisplatin treated CR-GC cells by downregulating PD-L1. Also, low-dose DB aggravated the inhibiting effects of cisplatin on tumorigenesis of CR-GC cells in vivo. Conclusions: Collectively, low-dose DB (12.5 μM) regulated intrinsic PD-L1/NLRP3 pathway to improve cisplatin-sensitivity in CR-GC cells, and this study provided alternative therapy treatments for GC.

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TGLI1 transcription factor mediates breast cancer brain metastasis via activating metastasis-initiating cancer stem cells and astrocytes in the tumor microenvironment

Cited by 65 publications

References 40 publications

Hedgehog Signaling and Truncated GLI1 in Cancer

Hedgehog Signaling and Truncated GLI1 in Cancer

HER2‐positive breast cancer brain metastasis: A new and exciting landscape

Low-dose Diosbulbin-B (DB) Regulates Tumor-Intrinsic PD-L1/NLRP3 Signaling Pathway to Increase Cisplatin-Sensitivity in Gastric Cancer (GC)

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