TERT—Regulation and Roles in Cancer Formation

Dratwa, Marta; Wysoczańska, Barbara; Łacina, Piotr; Kubik, Tomasz; Bogunia‐Kubik, Katarzyna

doi:10.3389/fimmu.2020.589929

Cited by 164 publications

(165 citation statements)

References 210 publications

(291 reference statements)

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“…These mutations result in a new consensus binding site for E-twenty-six (ETS) transcription factors and this may contribute to increased TERT . The ETS transcription factors are downstream targets of the RAS-RAF-MAPK pathways, and TERT promoter mutations are suggested to have synergistic effects with activating BRAF or NRAS mutations to promote tumor cell proliferation [ 21 ]. TERT is involved in the AKT pathway, and plays an important role in cellular immortality [ 6 ].…”

Section: Discussionmentioning

confidence: 99%

“…TERT mRNA overexpression does not completely explain all effects of the TERT promoter mutations in tumorigenesis, and the role of immunohistochemistry in determining the TERT status is still a topic of debate [ 22 ]. Consequently, other undefined or epigenetic mechanisms of TERT -upregulating are expected to exist [ 21 , 23 , 24 ]. While a TERT promoter mutation is not found in conjunctival nevi, it is found in both PAM [ 14 ] and CM [ 6 , 14 ], with increased TERT expression leading to tumor progression [ 6 ].…”

Section: Discussionmentioning

confidence: 99%

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Molecular Genetics of Conjunctival Melanoma and Prognostic Value of TERT Promoter Mutation Analysis

Poppelen

Ipenburg

Bosch

et al. 2021

IJMS

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The aim of this study was exploration of the genetic background of conjunctival melanoma (CM) and correlation with recurrent and metastatic disease. Twenty-eight CM from the Rotterdam Ocular Melanoma Study group were collected and DNA was isolated from the formalin-fixed paraffin embedded tissue. Targeted next-generation sequencing was performed using a panel covering GNAQ, GNA11, EIF1AX, BAP1, BRAF, NRAS, c-KIT, PTEN, SF3B1, and TERT genes. Recurrences and metastasis were present in eight (29%) and nine (32%) CM cases, respectively. TERT promoter mutations were most common (54%), but BRAF (46%), NRAS (21%), BAP1 (18%), PTEN (14%), c-KIT (7%), and SF3B1 (4%) mutations were also observed. No mutations in GNAQ, GNA11, and EIF1AX were found. None of the mutations was significantly associated with recurrent disease. Presence of a TERT promoter mutation was associated with metastatic disease (p-value = 0.008). Based on our molecular findings, CM comprises a separate entity within melanoma, although there are overlapping molecular features with uveal melanoma, such as the presence of BAP1 and SF3B1 mutations. This warrants careful interpretation of molecular data, in the light of clinical findings. About three quarter of CM contain drug-targetable mutations, and TERT promoter mutations are correlated to metastatic disease in CM.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Molecular Genetics of Conjunctival Melanoma and Prognostic Value of TERT Promoter Mutation Analysis

Poppelen

Ipenburg

Bosch

et al. 2021

IJMS

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“…Our study also demonstrated STAT3 activation by hypoxia to be essential for the acquisition of survival and functional benefits of NK cells. STAT3 is known to be an activator of human telomerase reverse transcriptase (hTERT) [ 45 ], and NK cell senescence from mbIL15-mediated expansion can be restored with hTERT gene modification. Since our data showed a reduction in the expression of p21/p53 tumor suppressors [ 46 ], along with a concomitant decrease in p16 mRNAs (data not shown) in hypoxia-exposed NK cells, inhibition of senescence by promoting hTERT activity could also have contributed to the increase in NK cells beyond 20 days of ex-vivo hypoxic NK culture.…”

Section: Discussionmentioning

confidence: 99%

Hypoxia-Driven HIF-1α Activation Reprograms Pre-Activated NK Cells towards Highly Potent Effector Phenotypes via ERK/STAT3 Pathways

Lim

Moon

Shin

et al. 2021

Cancers

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NK cells are the predominant innate lymphocyte subsets specialized to kill malignant tumor cells. In patients with advanced cancer, hypoxic stress shapes NK cells toward tumor-resistant and immunosuppressive phenotypes, hence a strategy to restore NK function is critical for successful tumor immunotherapy. Here, we present evidence that pre-activation and subsequent HIF-1α-dependent metabolic shift of NK cells from oxidative phosphorylation into glycolysis are keys to overcome hypoxia-mediated impairment in NK cell survival, proliferation, and tumor cytotoxicity. Specifically, exposing NK cells to 7–9 days of normoxic culture followed by a pO2 of 1.5% hypoxia led to a highly potent effector phenotype via HIF-1α stabilization and upregulation of its target genes, BNIP3, PDK1, VEGF, PKM2, and LDHA. RNA sequencing and network analyses revealed that concomitant reduction of p21/p53 apoptotic pathways along with upregulation of cell cycle-promoting genes, CCNE1, CDC6, CDC20, and downregulation of cell cycle-arrest genes, CDKN1A, GADD45A, and MDM2 were accountable for superior expansion of NK cells via ERK/STAT3 activation. Furthermore, HIF-1α-dependent upregulation of the NKp44 receptor in hypoxia-exposed NK cells resulted in increased killing against K562, CEM, and A375 tumor targets both in-vitro and in-vivo tumor clearance assays. Therefore, hypoxic exposure on pre-activated proliferating NK cells triggered HIF-1α-dependent pathways to initiate coordinated regulation of cell cycle, apoptosis, and cytotoxicity at the global gene transcription level. Our results uncover a previously unidentified role of HIF-1α-mediated metabolic reprogramming that can reverse impaired NK effector phenotypes to generate requisite numbers of functionally robust NK cells for adoptive cellular therapy for clinical evaluation.

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“…Furthermore, our results indicate that TERT determines the cancerous function of mutant MEG3. Telomerase, an RNA-dependent DNA polymerase with telomerase reverse transcriptase (TERT), regulates cancer formation (54,55).A particular attention is given to the putative connections between TERT transcriptional reactivation and signalling pathways frequently altered in cancer, such as c-MYC, NF-κB and β-Catenin(56). TERT promoter mutations are associated with poor prognosis and cell immortalization in meningioma (57).DNA methylation of the TERT promoter is associated with human cancer(58).TERT and TERC mutations suppress telomerase activity (59).TERT C228T mutation is associated with intravesical recurrence for patients with non-muscle invasive bladder cancer(60).TERC is an RNA component of telomerase and TERC promotes cellular in ammatory response independent of telomerase(61).…”

Section: Discussionmentioning

confidence: 99%

Mutant MEG3 Enhances the Activity of Telomerase by Increasing DNA Damage Repair in Human Liver Cancer Stem Cells

Song

Xie

Qin

et al. 2021

Preprint

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Background: Long noncoding RNAs have recently considered as central regulators in diverse biological processes and emerged as vital players controlling tumorigenesis. Although wild MEG3 acts as a suppressor in several cancers, the function of mutant MEG3 is also unclear during tumorigenesis.Methods: Lentivalus infection,RT-PCR,Western blotting and tumorigenesis test in vitro and in vivo were performed.Results: our results suggest that mutant MEG3 promotes the growth of human liver cancer stem cells in vivo and in vitro.Mechanistically, our results show that mutant MEG3 enhances acetylation modification of HistoneH4 on K16.Then, mutant MEG3 enhances the expression of SETD2 dependent on H4K16Ac.Moreover, mutant MEG3 increases the DNA damage repair through SETD2.Ultimately, mutant MEG3 increases the telomeras activity dependent on DNA damage repair.Strikingly,TERT determines the cancerous function of mutant MEG3 in liver cancer stem cells. Therefore, we shed light on the fact that targeting mutant MEG3 could be a viable approach for cancer treatment.Conclusions: these observations will play an important role in finding effective tumor treatment targets.

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TERT—Regulation and Roles in Cancer Formation

Cited by 164 publications

References 210 publications

Molecular Genetics of Conjunctival Melanoma and Prognostic Value of TERT Promoter Mutation Analysis

Molecular Genetics of Conjunctival Melanoma and Prognostic Value of TERT Promoter Mutation Analysis

Hypoxia-Driven HIF-1α Activation Reprograms Pre-Activated NK Cells towards Highly Potent Effector Phenotypes via ERK/STAT3 Pathways

Mutant MEG3 Enhances the Activity of Telomerase by Increasing DNA Damage Repair in Human Liver Cancer Stem Cells

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