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BIOMARKER:

AURKA overexpression

i
Other names: AURKA, AIK, ARK1, AurA, BTAK, PPP1R47, STK15, STK6, STK7, Aurora kinase A
Entrez ID:
Related biomarkers:
1m
Palmatine attenuates MYH9 mediated nuclear localization of AURKA to induce G2/M phase arrest in colorectal cancer cells. (PubMed, Int Immunopharmacol)
Taken together, our study revealed that MYH9 as an auxiliary protein for the nuclear localization of AURKA and elucidated the mechanism that PAL reduced nuclear AURKA through inhibiting the interaction of AURKA and MYH9 to induce G2/M phase arrest in CRC cells. Therefore, this study may provide a theoretical basis of PAL for the treatment of CRC.
Journal
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AURKA (Aurora kinase A) • MYH9 (Myosin Heavy Chain 9)
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AURKA overexpression
1m
Post-transcriptional control drives Aurora kinase A expression in human cancers. (PubMed, PLoS One)
hsa-let-7a and APA may also independently contribute to altered AURKA levels. Therefore, we argue that AURKA mRNA and protein expression are often discordant in cancer as a result of dynamic post-transcriptional regulation.
Clinical • Journal
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AURKA (Aurora kinase A)
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AURKA overexpression • AURKA expression
3ms
The significant others of aurora kinase a in cancer: combination is the key. (PubMed, Biomark Res)
By targeting these substrates, it may be possible to disrupt this feedback loop to effectively reverse AURKA levels, thereby providing a promising avenue for developing safer AURKA-targeted therapeutics. Additionally, exploring the synergistic effects of AURKA inhibition with its other oncogenic and/or tumor-suppressor targets could provide further opportunities for developing effective combination therapies against AURKA-driven cancers, thereby maximizing its potential as a critical drug target.
Review • Journal
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AURKA (Aurora kinase A)
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AURKA overexpression • AURKA expression
10ms
AurkA/TPX2 co-overexpression in nontransformed cells promotes genome instability through induction of chromosome mis-segregation and attenuation of the p53 signalling pathway. (PubMed, Biochim Biophys Acta Mol Basis Dis)
Interestingly, the p53/p21 axis response is impaired in AurkA/TPX2 overexpressing cells subjected to different stimuli; consistently, cells acquire increased ability to proliferate after independent induction of mitotic errors, i.e. following nocodazole treatment. Based on our observation that increased levels of the AurkA/TPX2 complex affect chromosome segregation fidelity and interfere with the activation of a pivotal surveillance mechanism in response to altered cell division, we propose that co-overexpression of AurkA and TPX2 per se represents a condition promoting the generation of a genetically unstable context in nontransformed human cells.
Journal
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AURKA (Aurora kinase A) • TPX2 (TPX2 Microtubule Nucleation Factor)
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AURKA overexpression • AURKA expression
10ms
PTEN Deficiency Induces an Extrahepatic Cholangitis-Cholangiocarcinoma Continuum via Aurora kinase A in Mice. (PubMed, J Hepatol)
Pten deficiency in extrahepatic cholangiocytes and peribiliary glands led to a cholangitis-to-cholangiocarcinoma continuum through an Aurka-dependent manner. These findings offer new insights into preventive and therapeutic interventions for extrahepatic CCA.
Preclinical • Journal
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TP53 (Tumor protein P53) • PTEN (Phosphatase and tensin homolog) • AURKA (Aurora kinase A) • PDX1 (Pancreatic And Duodenal Homeobox 1)
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PTEN deletion • AURKA overexpression
10ms
Identification of Hub genes with prognostic values in colorectal cancer by integrated bioinformatics analysis. (PubMed, Cancer Biomark)
The results of GSEA showed that Hub genes and their co-expressed genes mainly participated in chromosome segregation, DNA replication, translational elongation and cell cycle. Overexpression of AURKA, CCNB1, CCNA2 and EXO1 had a better prognosis for CRC and this effect was correlation with gene mutation and infiltration of immune cells.
Journal
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CD8 (cluster of differentiation 8) • AURKA (Aurora kinase A) • CCNA2 (Cyclin A2) • CCNB1 (Cyclin B1)
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AURKA overexpression
12ms
The PIN1-YTHDF1 axis promotes breast tumorigenesis via the mA-dependent stabilization of AURKA mRNA. (PubMed, Arch Pharm Res)
In conclusion, the findings of our study suggest that increased YTHDF1 stability induced by PIN1 promotes breast tumorigenesis via the stabilization of AURKA mRNA. Targeting the PIN1/YTHDF1 axis may represent a novel therapeutic strategy for breast cancer.
Journal
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AURKA (Aurora kinase A) • PIN1 (Peptidylprolyl Cis/Trans Isomerase, NIMA-Interacting 1) • YTHDF1 (YTH N6-Methyladenosine RNA Binding Protein 1)
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AURKA overexpression • AURKA expression
1year
Searching for Natural Aurora a Kinase Inhibitors from Peppers Using Molecular Docking and Molecular Dynamics. (PubMed, Pharmaceuticals (Basel))
We compared our results with anticancer activity studied earlier on MCF-7 cell lines (breast cancer cells). Our research indicates that the compounds contained in peppers can inhibit Aurora A. Further in vitro research is planned to confirm the obtained results.
Journal
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AURKA (Aurora kinase A)
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AURKA overexpression
1year
Unveiling Potential Targeted Therapeutic Opportunities for Co-Overexpressed Targeting Protein for Xklp2 and Aurora-A Kinase in Lung Adenocarcinoma. (PubMed, Mol Biotechnol)
The tyrosine kinase inhibitor (TKI) dacomitinib demonstrated the strong binding potential to hinder TPX2, shielding the AURKA destabilization. This in silico study lays the foundation for repurposing targeted therapeutic options to impede the Protein-Protein Interactions (PPIs) in LUAD progression and aid in future translational investigations.
Journal
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AURKA (Aurora kinase A)
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AURKA overexpression
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Vizimpro (dacomitinib)
over1year
Anlotinib induces apoptosis and second growth/mitosis phase block in cisplatin-resistant ovarian cancer cells via the aurora kinase A/p53 pathway. (PubMed, Hum Exp Toxicol)
This study demonstrated that anlotinib can induce apoptosis and G2/M arrest in cisplatin-resistant ovarian cancer cells through the AURKA/p53 pathway.
Journal
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AURKA (Aurora kinase A) • BAX (BCL2-associated X protein) • CDK1 (Cyclin-dependent kinase 1) • CDKN1A (Cyclin-dependent kinase inhibitor 1A)
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AURKA overexpression • TP53 expression • BAX expression • AURKA expression
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cisplatin • Focus V (anlotinib)
over1year
CDCA2 promotes melanoma progression by inhibiting ubiquitin-mediated degradation of Aurora kinase A. (PubMed, Eur J Cancer)
CDCA2, which was upregulated in melanoma, enhanced AURKA protein stability by inhibiting SMAD specific E3 ubiquitin protein ligase 1-mediated AURKA ubiquitination, thus playing a carcinogenic role in melanoma progression.
Journal
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AURKA (Aurora kinase A) • CDCA2 (Cell Division Cycle Associated 2) • SMURF1 (SMAD Specific E3 Ubiquitin Protein Ligase 1) • UBR5 (Ubiquitin Protein Ligase E3 Component N-Recognin 5)
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AURKA overexpression
over1year
USP21 contributes to the aggressiveness of laryngeal cancer cells by deubiquitinating and stabilizing AURKA. (PubMed, Kaohsiung J Med Sci)
In addition, overexpression of AURKA reversed the effects of USP21 knockdown on cell growth, migration, and invasion. USP21 stabilized AURKA through deubiquitination to promote laryngeal cancer progression.
Journal
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AURKA (Aurora kinase A)
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AURKA overexpression
over1year
Chebulagic acid suppresses gastric cancer by inhibiting the AURKA/β-catenin/Wnt pathway. (PubMed, Front Pharmacol)
CA also inhibited the expression of AURKA and the AURKA/β-catenin/Wnt signaling pathway in vitro and in vivo. Collectively, the present results demonstrated that high expression of AURKA may be an independent factor of poor prognosis in patients with GC, and CA significantly suppressed the tumor biological functions of GC and inhibited the AURKA/β-catenin/Wnt pathway.
Journal
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AURKA (Aurora kinase A)
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AURKA overexpression • AURKA expression
almost2years
Synthetic lethal targeting of AURKA in head and neck squamous cell carcinoma (AACR 2023)
Using viability and clonogenic assays, we have found that the AURKA inhibitor VIC-1911 synergizes with the EGFR inhibitors afatinib and erlotinib in multiple HNSCC cell lines and retains activity in HNSCC cell models selected for resistance to these EGFR inhibitors. Dual inhibition of AURKA in combination with inhibitors of glycolytic enzymes, or enzymes regulating oxidative phosphorylation, showed marked synergy. These and other results investigating AURKA signaling mechanisms in HNSCC demonstrate that the non-canonical functions of AURKA include viable therapeutic targets that can enhance the efficacy of AURKA inhibition in HNSCC.
Synthetic lethality
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AURKA (Aurora kinase A)
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EGFR overexpression • AURKA overexpression
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erlotinib • Gilotrif (afatinib) • VIC-1911
almost2years
AURKA, as a potential prognostic biomarker, regulates autophagy and immune infiltration in nasopharyngeal carcinoma. (PubMed, Immunobiology)
AURKA overexpressed in NPC, which was associated with poor prognosis. Silencing of AURKA inhibited the proliferation and migration of NPC cells. Besides, AURKA might participate in the regulation of both autophagy and immunity in NPC.
Journal
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AURKA (Aurora kinase A)
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AURKA overexpression • AURKA expression
almost2years
Cell cycle kinases (AUKA, CDK1, PLK1) are prognostic biomarkers and correlated with tumor-infiltrating leukocytes in HBV related HCC. (PubMed, J Biomol Struct Dyn)
Furthermore, the expression levels of these genes had a strong correlation with infiltration of immune cells. Our analysis shows that AURKA, CDK1 and PLK1 are correlated with immune infiltration and are the prognostic biomarkers for HBV-induced HCC.Communicated by Ramaswamy H. Sarma.
Journal • Tumor-infiltrating-leukocyte
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AURKA (Aurora kinase A) • PLK1 (Polo Like Kinase 1) • CDK1 (Cyclin-dependent kinase 1)
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AURKA overexpression
2years
The role of AURKA/miR-199b-3p in hepatocellular carcinoma cells. (PubMed, J Clin Lab Anal)
To summarize, this study implied the regulatory mechanism of miR-199b-3p/AURKA axis in HCC, and supplied optional therapeutic targets for HCC patients.
Journal
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AURKA (Aurora kinase A) • MIR199B (MicroRNA 199b)
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AURKA overexpression • miR-199b overexpression • AURKA expression
over2years
Combination of AURKA inhibitor and HSP90 inhibitor to treat breast cancer with AURKA overexpression and TP53 mutations. (PubMed, Med Oncol)
This review describes the research status of AURKA and HSP90 in breast cancer, summarizes the structure, function, and the chaperone cycle of HSP90, elaborates the interrelation between HSP90, mtP53, P53, and AURKA, and proposes the combination of HSP90 inhibitor and AURKA inhibitor to treat breast cancer. Targeting AURKA and HSP90 to treat cancer with AURKA overexpression and TP53 mutations will help improve the specificity and efficiency of breast cancer treatment and solve the problem of drug resistance.
Review • Journal
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HER-2 (Human epidermal growth factor receptor 2) • TP53 (Tumor protein P53)
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TP53 mutation • HER-2 amplification • AURKA overexpression • AURKA expression
over2years
Predicting AURKA as a novel therapeutic target for NPC: A comprehensive analysis based on bioinformatics and validation. (PubMed, Front Genet)
Drug susceptibility analysis found that dacarbazine, R-306465, vorinostat, and other antitumor drugs that act on the cell cycle were closely related to AURKA. We confirmed upregulation of AURKA in NPC tissues. Our results support an oncogenic role of AURKA in the context of NPC, and indicate its potential role as a novel therapeutic target.
Journal
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AURKA (Aurora kinase A) • CD4 (CD4 Molecule)
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AURKA overexpression • AURKA expression
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dacarbazine • Zolinza (vorinostat)
over2years
AURKA is a prognostic potential therapeutic target in skin cutaneous melanoma modulating the tumor microenvironment, apoptosis, and hypoxia. (PubMed, J Cancer Res Clin Oncol)
AURKA is the core hub gene driving the occurrence and development of SKCM, and its expression is regulated by epigenetic modifications. AURKA can regulate the infiltration level of various immune cells in the tumor microenvironment, reshape the immunosuppressive tumor microenvironment, and apoptosis, and hypoxia. Thus, it is a prognostic biomarker and potential therapeutic target in SKCM. ZNC97018978 is an effective and safe inhibitor of AURKA in vitro; its safety and effectiveness in vivo as a potential treatment for cutaneous melanoma should be further determined.
Journal
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CD8 (cluster of differentiation 8) • AURKA (Aurora kinase A) • TGFB1 (Transforming Growth Factor Beta 1)
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AURKA overexpression • AURKA expression
over2years
Induction of Ferroptosis by Ophiopogonin-B Through Regulating the Gene Signature AURKA in NSCLC. (PubMed, Front Oncol)
Overall, our study established a new ferroptosis-related risk prediction model for the prognosis of patients with NSCLC, revealed the enrichment pathways of ferroptosis in NSCLC, and discovered the negative regulation of AURKA in ferroptosis. On this basis, we demonstrated that OP-B can induce ferroptosis in NSCLC and clarified the specific molecular mechanism of OP-B inducing ferroptosis by regulating the expression of AURKA.
Journal • Gene Signature
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AURKA (Aurora kinase A) • SLC7A5 (Solute Carrier Family 7 Member 5) • PHKG2 (Phosphorylase Kinase Catalytic Subunit Gamma 2)
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AURKA overexpression
over2years
Clinical outcomes associated with expression of aurora kinase and p53 family members in muscle-invasive bladder cancer. (PubMed, Mol Clin Oncol)
To the best of our knowledge, the present study was the first to report co-expression of p53 and aurora kinase family members in MIBC, and although wild-type p53 may regulate the aurora kinases in preclinical models, the adverse prognostic value of tumor AURKA overexpression was independent from baseline tumor p53 protein expression in the present cohort. AURKA remains an important prognostic biomarker in patients with MIBC and warrants further evaluation in prospective studies to validate whether baseline AURKA can identify patients that are unlikely to benefit from standard of care with NAC.
Clinical data • Journal
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TP53 (Tumor protein P53) • AURKA (Aurora kinase A) • AURKB (Aurora Kinase B) • TP63 (Tumor protein 63)
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TP53 wild-type • AURKA overexpression • TP53 expression • AURKA expression
over2years
Integrative Analysis for Identification of Therapeutic Targets and Prognostic Signatures in Non-Small Cell Lung Cancer. (PubMed, Bioinform Biol Insights)
On the contrary, high mRNA expressions of CBL, FYN, LRKK2, and SOCS2 were associated with a significantly better prognosis. Furthermore, our drug target analysis for these hub genes suggests a potential use of Trichostatin A, Pracinostat, TGX-221, PHA-793887, AG-879, and IMD0354 antineoplastic agents to reverse the expression of these DEGs in NSCLC patients.
Journal
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CDKN2A (Cyclin Dependent Kinase Inhibitor 2A) • EZH2 (Enhancer of zeste 2 polycomb repressive complex 2 subunit) • AURKA (Aurora kinase A) • CDC20 (Cell Division Cycle 20) • CDK1 (Cyclin-dependent kinase 1) • SOCS2 (Suppressor Of Cytokine Signaling 2) • FYN (FYN Proto-Oncogene, Src Family Tyrosine Kinase)
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AURKA overexpression
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pracinostat (SB939) • PHA 793887 • TGX-221
over2years
Predicting sulforaphane-induced adverse effects in colon cancer patients via in silico investigation. (PubMed, Biomed Pharmacother)
Thus, genome signature of CRC patients could serve as important factor when addressing the risk-to-benefit profile of SFN. Patients with colon cancer and increased expression of TIMP1, CCL20, SPP1, AURKA, CEP55, NEK2, SOX9 and CDK1, or downregulation of CRYAB, PLCE1, MMP28, BMP2 and PLAC8 may not be ideal candidates for SFN chemoprevention.
Clinical • Journal • Adverse events
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SPP1 (Secreted Phosphoprotein 1) • AURKA (Aurora kinase A) • CCL20 (C-C Motif Chemokine Ligand 20) • IL10 (Interleukin 10) • TIMP1 (Tissue inhibitor of metalloproteinases 1) • SOX9 (SRY-Box Transcription Factor 9) • CDK1 (Cyclin-dependent kinase 1) • PLAC8 (Placenta Associated 8) • CEP55 (Centrosomal Protein 55) • RUNX2 (RUNX Family Transcription Factor 2)
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AURKA overexpression • KIM1 expression • TIMP1 expression
almost3years
Targeting AURKA by microRNA-490-3p suppresses gastric cancer cell growth. (PubMed, Histol Histopathol)
MicroRNA-490-3p was likely to restrain the development of GC cells by inhibiting AURKA, and it may be an underlying target for GC treatment.
Journal
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AURKA (Aurora kinase A) • MIR490 (MicroRNA 490)
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AURKA overexpression
3years
Design, Synthesis, and Biochemical Evaluation of New Triazole Derivatives as Aurora-A Kinase Inhibitors. (PubMed, Molecules)
Here, new triazole derivatives were designed as bioisosteric analogues of the known inhibitor JNJ-7706621. The new compounds showed interesting inhibitory activity against Aurora-A kinase, as attested by ICs in the low to submicromolar range.
Journal
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AURKA (Aurora kinase A)
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AURKA overexpression
3years
Defining transcriptomic profiles of breast cancer with early lymph node metastases: A FLEX database sub-study (SABCS 2021)
This study provides a foundation for understanding the mechanisms that promote LN metastasis. Studies have previously correlated LN metastasis with EMT, immune function, and gene overexpression ( BCL2L1, AURKA, CDKN2A, MCL1, MYC ). While we did not find significant differences in these genes, our results indicated similar differentially regulated pathways.
HER-2 (Human epidermal growth factor receptor 2) • CDKN2A (Cyclin Dependent Kinase Inhibitor 2A) • MCL1 (Myeloid cell leukemia 1) • BCL2L1 (BCL2-like 1) • AURKA (Aurora kinase A)
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BCL2L1 overexpression • MCL1 expression • AURKA overexpression
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MammaPrint • BluePrint
over3years
Natural Anthraquinone Compound Emodin as a Novel Inhibitor of Aurora A Kinase: a Pilot Study. (PubMed, Chem Biol Drug Des)
It seems that emodin may have the potential to inhibit cancer cell growth and enhance cisplatin therapy in cancer with resistance. Collectively, our finding reveals a novel AURKA inhibitor, emodin, which may be vulnerable to ovarian cancer therapy in the future.
Clinical • Journal
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AURKA (Aurora kinase A)
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AURKA overexpression
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cisplatin
over3years
Aurora kinase A (AURKA) promotes the progression and imatinib resistance of advanced gastrointestinal stromal tumors. (PubMed, Cancer Cell Int)
These findings indicated that overexpression of AURKA promoted GIST progression and enhanced imatinib resistance, implying that AURKA is a potential therapeutic target for GISTs.
Journal
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AURKA (Aurora kinase A)
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AURKA overexpression • AURKA expression
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imatinib
over3years
[VIRTUAL] In vitro analysis of the combination of APR-246 and carboplatin in triple negative breast cancer (TNBC) and high grade serous ovarian cancer (HGSOC) cell lines and its impact on Aurora kinase A (AURKA)-p53 pathway (ESMO 2021)
Addition of APR246 to carboplatin increased apoptosis in both TNBC and HGSOC cell lines regardless of p53 mutations status in this in vitro study. AURKA and p53 expression was modified after exposure to carbo or combo.
Preclinical
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AURKA (Aurora kinase A)
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TP53 mutation • AURKA overexpression • TP53 expression • AURKA expression
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carboplatin • eprenetapopt (APR-246)
over3years
Nuclear Aurora kinase A triggers programmed death-ligand 1-mediated immune suppression by activating MYC transcription in triple-negative breast cancer. (PubMed, Cancer Commun (Lond))
Nuclear AURKA elevated PD-L1 expression via an MYC-dependent pathway and contributed to immune evasion in TNBC. Therapies targeting nuclear AURKA may restore immune responses against tumors.
Journal • PD(L)-1 Biomarker • IO biomarker
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PD-L1 (Programmed death ligand 1) • MYC (V-myc avian myelocytomatosis viral oncogene homolog) • CD8 (cluster of differentiation 8) • IFNG (Interferon, gamma) • AURKA (Aurora kinase A) • IL2 (Interleukin 2)
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PD-L1 overexpression • MYC overexpression • MYC expression • AURKA overexpression • AURKA expression
over3years
Investigation on the clinical efficacy and mechanism of compound kushen injection in treating esophageal cancer based on multi-dimensional network meta-analysis and in vitro experiment. (PubMed, J Ethnopharmacol)
In this study, network meta-analysis was applied to confirm that Compound Kushen Injection has a curative effect on esophageal cancer and is superior to other anti-tumor Chinese herbal injections. Combined with the network pharmacology and in vitro experiment, the mechanism of Compound Kushen Injection inhibiting the proliferation of esophageal cancer cells by regulating the abnormal expression of EGFR and AURKA was revealed.
Preclinical • Retrospective data • Journal
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EGFR (Epidermal growth factor receptor) • AURKA (Aurora kinase A)
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EGFR expression • EGFR overexpression • AURKA overexpression
over3years
Targeting glioma cells by antineoplastic activity of reversine. (PubMed, Oncol Lett)
In conclusion, reversine potently induced mitotic catastrophe and apoptosis in glioma cells and higher basal levels of aurora kinases and genes responsive to DNA damage and may predict improved antiglioma responses to the drug. Reversine may be a potential novel drug in the antineoplastic arsenal against gliomas.
Journal
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AURKA (Aurora kinase A) • AURKB (Aurora Kinase B)
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AURKA overexpression • AURKA expression
over3years
Kinase inhibitor screening reveals aurora-a kinase is a potential therapeutic and prognostic biomarker of gastric cancer. (PubMed, J Cell Biochem)
Therefore, it is feasible to suggest AURKA as a potential marker of gastric cancer, besides providing robust information for diagnosis and estimated survival of patients. AURKA can be considered a new molecular target used in the prognosis and therapy of gastric cancer.
Journal
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AURKA (Aurora kinase A) • CASP3 (Caspase 3) • CASP7 (Caspase 7)
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AURKA overexpression • AURKA expression
over3years
Repression of the AURKA-CXCL5 axis induces autophagic cell death and promotes radiosensitivity in non-small-cell lung cancer. (PubMed, Cancer Lett)
We further demonstrated that the AURKA-CXCL5 axis played an essential role in NSCLC autophagy and that the activation of cytotoxic autophagy attenuated the malignant biological behavior of NSCLC cells mediated by AURKA-CXCL5. In general, we revealed the role of the AURKA-CXCL5 axis and autophagy in regulating the sensitivity of NSCLC cells to radiotherapy, which may provide potential therapeutic targets and new strategies for combatting NSCLC resistance to radiotherapy.
Journal
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CXCL5 (Chemokine (C-X-C motif) ligand 5)
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AURKA overexpression • AURKA expression
almost4years
[VIRTUAL] AURKA MODULATES TUMORIGENESIS THROUGH REGULATING CANCER STEM-LIKE CELLS IN GASTRIC CANCER (DDW 2021)
Interestingly, AURKA inhibition by alisertib reduced the mRNA expression of SOX9 and tumor size in the TFF1 KO mouse model. Our data indicate that constitutive high levels of AURKA in cancer cells regulate the expression of LGR5, and SOX9, suggesting a positive role for AURKA in expanding and promoting the stem-like properties properties of cancer cells.
PD(L)-1 Biomarker • IO biomarker
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PD-L1 (Programmed death ligand 1) • CD19 (CD19 Molecule) • CD8 (cluster of differentiation 8) • AURKA (Aurora kinase A) • SOX9 (SRY-Box Transcription Factor 9) • LRIG1 (Leucine Rich Repeats And Immunoglobulin Like Domains 1) • TFF1 (Trefoil Factor 1)
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AURKA overexpression • SOX9 expression • AURKA expression
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alisertib (MLN8237)
almost4years
[VIRTUAL] AURORA KINASE A PROMOTES CANCER CELL SURVIVAL BY ACTIVATING UNFOLDED PROTEIN RESPONSE UNDER ONCOGENIC STRESS IN ESOPHAGEAL ADENOCARCINOMA (DDW 2021)
UPR is an important response mechanism that dictates cell fate under ER stress. Our data showed, for the first time, that AURKA activates UPR, promoting cancer cell survival during ER stress in EAC. We have shown that knockdown or inhibition of AURKA can significantly reverse pro-survival UPR signaling mechanisms and decrease cancer cell survival.
PARP Biomarker
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AURKA (Aurora kinase A)
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AURKA overexpression • AURKA expression
almost4years
MiRNA-621 exerts tumor suppressor function in gastric adenocarcinoma by targeting AURKA/GSK-3β pathway. (PubMed, Acta Biochim Pol)
In addition, AURKA overexpression reversed the effect of miR-621 on the growth of cancer cells. Taken together, our results suggest that miR-621 is an important tumor suppressor in gastric cancer and could be a promising target for the cancer treatment.
Journal
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AURKA (Aurora kinase A) • MIR621 (MicroRNA 621)
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AURKA overexpression • AURKA expression