Implications of telomerase reverse transcriptase in tumor metastasis.

Metastasis is the main culprit of the great majority of cancerrelated deaths. However, the complicated process of the invasion-metastasis cascade remains the least understood aspect of cancer biology. Telomerase plays a pivotal role in bypassing cellular senescence and sustaining the cancer progression by maintaining telomere homeostasis and genomic integrity. Telomerase reverse transcriptase (TERT) exerts a series of fundamental functions that are independent of its enzymatic cellular activity, including proliferation, inflammation, epithelia-mesenchymal transition (EMT), angiogenesis, DNA repair, and gene expression. Accumulating evidence indicates that TERT may facilitate most steps of the invasion-metastasis cascade. In this review, we summarize important advances that have revealed some of the mechanisms by which TERT facilitates tumor metastasis, providing an update on the non-canonical functions of telomerase beyond telomere maintaining. [BMB Reports 2020; 53(9): 458-465].

INTRODUCTION

Telomerase is a large ribonucleoprotein complex responsible for adding telomeric repeats to the 3’ ends of chromosomes, thereby alleviating the telomere attrition from each round of replication (1, 2). Telomerase is essentially composed of the TERT and telomerase RNA component (TR), which serves as a template for the TERT to synthesize telomeric repeats. hTR is ubiquitously expressed in both normal cells and cancer cells. Conversely, hTERT is repressed in normal cells, re-activated in 85-90% of cancer types, and closely associated with telomerase activity in cancers, suggesting that TERT is the determinant for telomerase activity, which makes telomerase an attractive therapeutic target (3-6).

Tumor metastasis, termed the invasion-metastasis cascade, is a multi-step process that involves dissemination of cancer cells from primary tumors to distant organs and their subsequent seeding of new tumor colonies into foreign soil (7). The invasion-metastasis cascade is a succession of cell-biology events: (a) local invasion of primary tumor cells into the adjacent parenchyma through the surrounding extracellular matrix and stromal cell layers, (b) intravasation of invasive tumor cells into the circulatory system, (c) survival and dissemination during hematogenous transit through the vascula-ture, (d) arrest at distant organs, (e) extravasation of tumor cells from the microvasculature into the adjacent parenchyma of distant organ sites, (f) formation of micrometastase colonies in the parenchyma of distant tissues, and (g) growth of micrometastase colonies and establishment of a full-fledged tumor at the distant site (7). Metastatic disease is largely incurable because of it is complex and systemic and resists current therapeutic strategies, which results in more than 90% of deaths of cancer-associated patients (8). Recently, a growing number of evidence suggests that TERT may play a pivotal role in the invasion-metastasis cascade. Here, we highlight the functional regulation of TERT in each step of the tumor metastasis, which providing new insights for understanding tumor metastasis and developing new diagnostic and therapeutic strategies.

TERT AND LOCAL INVASION

Primary tumor cells breach the basement membrane (BM) and enter into the surrounding tumor-associated stroma, which leads to the first step in tumor metastasis. It has been demonstrated that metalloproteinases (MMPs), which disintegrate the extracellular matrix and promotes tumor cell invasion. Therefor, MMPs are key factors for determining the invasive potential of cells (9). It has been shown that hTERT associates with the expression of MMPs in many tumor entities. For example, knockdown hTERT in oral squamous-cell carcinoma decreases the MMP2 and MMP9 expression, thereby inhibiting invasiveness (10). Moreover, hTERT promotes the invasive ability of the cell by regulating MMP9 expression in a NF-κB-dependent manner independently of its catalytic activity in osteosarcoma and cervical carcinoma cell line, such as U2OS and HeLa (11). Importantly, Ghosh et al. revealed that TERT directly regulates NF-κB-dependent transcription (11, 12). To mention briefly, TERT interacts with NF-κB p65 and binds many NF-κB targeting genes, such as IL6, IL8, and TNFα, which are critical for inflammatory response (12). IL6 and TNFα play a central role in linking inflammation and cancer (13). It’s worth noticing that IL-6 can act as an inducer of EMT in breast cancer cells (14). Ectopic expression of IL-6 in breast adenocarcinoma cells induces an EMT phenotype by upregulating vimentin, N-cadherin, Snail and Twist. It’s important to mention that TNFα enhances the invasive property of renal carcinoma cells by inducing EMT through Snail or ZEB1/ZEB2 (15, 16). EMT is believed to be an important step in the conversion of primary cancer cells into a migratory population capable of systemic metastasis (17-19). Thus, it seems that TERT contributes to the formation of migratory cell by inducing EMT in a NF-κB-dependent manner. Interestingly, one study demonstrated that hTERT directly stimulates EMT of gastric cancer cells by occupying the promoter of vimentin in cooperation with β-catenin and in a telomere-independent manner (20). Collectively, hTERT promotes the invasiveness of cancer cells by inducing an extracellular protease and EMT program in a NF-κB-dependent transcription manner. However, the detailed mechanisms by which TERT regulate NF-κB for primary tumor cells in local invasion remains to be revealed. TERT can use other extracellular proteases to remodel the ECM, thereby promoting the invasiveness of cells. It has been shown that cathepsins and heparanase can cleave the E-cadherin, a key cell-cell adhesion molecule, and degrade heparan sulfate proteoglycans (HSPG) secreted by ECM and BM, respectively, enabling primary tumor cells to cross the adjacent parenchyma (21-25). Importantly, Young et al. found that hTERT activates tumor invasi-veness by upregulating cathepsin D via early growth response 1 (EGR-1) in oral squamous-cell carcinoma cells (22). Tang et al. found that hTERT expression is highly associated with an advanced TNM stage and lymphatic metastasis in gastric cancers. They further revealed that hTERT promotes gastric cancer-cell invasion and metastasis by cooperating with c-Myc to induce the expression of Hpa (23). These findings suggest that TERT may facilitate invasion of primary tumor cells via cathepsins and heparanase. However, this hypothesis needs more experimental support. Furthermore, whether TERT regulates the expression of cathepsins and heparanase dependent on its catalytic activity remains to be answered. Recently, studies demonstrated that TERT promote gastric cancer invasion by upregulating the expression of ITGB1 (Integrin b1) adhesion molecules for cancer cells and the extracellular matrix (26, 27). The hTERT-MDM2 complex enhances the ubiquitin-me-diated degradation of FOXO3a, alleviating FOXO3a-repressed ITGB1 expression, which eventually leads to the upregulation of ITGB1. Both hTERT and ITGB1 were highly expressed in the advanced tumor-node metastases (TNM) stage group and the lymphatic metastasis positive group. The group of higher expression of both hTERT and ITGB1 is linked to the worst survival rate in gastric-cancer patients. These findings suggest that TERT may contribute to tumor metastasis via ITGB1. Early studies showed that Integrin β1 is a critical effector in promoting invasion by the primary tumor cells and cancer metastasis, which further supports that ITGB1 is a driver in tumor metastasis (28, 29).

Recently, Chen et al. showed that hTERT promotes the invasion of colorectal cancer cells by increasing chemokine CCL2 expression in collaboration with the b-catenin/TCF-4 complex. They further found that MDSCs accumulated in areas where hTERT and CCL2 were colocalized (30). Early studies revealed that primary tumor cells can use CCL2 to recruit MDSCs, regulatory T cells (TRegs) and tumor associate macrophage (TAM) to evade immune surveillance, which is a crucial step for preparing a metastatic journey to start the invasion-metastasis cascade (31-35). These results suggest that hTERT may also play a regulatory role in the recruitment of myeloid-derived suppressor cells (MDSCs) and evasion of tumor immunity.

TERT AND INTRAVASATION

Intravasation is local invasive cancer cells entering into the lumina of lymphatic or blood vessels to disseminate throughout the body before adhering to the endothelial cells lining the microvasculature (36). Tumor-associated microvasculature, generated by the process of angiogenesis, harbors the weak interactions between adjacent endothelial cells and the absence of extensive pericyte coverage, which are considered to facilitate intravasation (7). Therefore, the mechanics of intravasation are likely to be strongly influenced by angiogenesis. It has been well established that vascular endothelial growth factor (VEGF) is a key inducer in angiogenesis, which can stimulate tumor cells to form new blood vessels within their local microenvironment via neoangiogenesis (9). Importantly, it has been shown that hTERT induces VEGF gene expression independently of its telomerase reverse transcriptase activity, which provides a cornerstone for hTERT driving angiogenesis (37). Liu et al. reported that hTERT induces VEGF gene expression by occupying the VEGF promoter in cooperation with Sp1 (38). They further found that TERT promotes the vascular tube formation and deficiency of TERT-compromised tumor growth and vascular development. Furthermore, hTERT expression is positively correlated with VEGF in patient samples. These findings suggest that TERT may facilitate the intravasation by inducing angiogenesis. It has been previously reported that VEGF can induce hTERT and telomerase activity (39, 40). There may be a positive regulatory feedback circuit between hTERT and VEGF that has a collaborative role in tumorigenesis and cancer progression. Besides VEGF, sufficient studies showed that MMPs are involved in angiogenesis-dependent intravasation and metastasis, and that MMPs can directly or indirectly affect the VEGF-mediated development of angiogenic vasculature. These findings suggest that TERT may also contri-bute to the induction of intravasation and metastasis-sustaining neo-vasculature via MMPs. A growing number of studies showed that TNF-β promote intravasation (41, 42). In order to identify the role of mTert in prostate-cancer progression, Ding et al. compared an mTert-deficiency mouse (G3/4-LSL-mTert−/−-Pten/p53) with an mTert knock-in mouse (G3/4-LSL-mTert+/+-Pten/p53) and found that the TNF-β/Smad4 pathway is required for mTERT-mediated bone metastasis (43). It seems that mTert acts as an active driver for tumor metastasis in a telomere-based crisis. We can assume that the TNF-β/Smad4 pathway may be implicated in the process of intravasation. However, the mechanisms by which mTERT regulate TNF-β in bone metastasis need to be discovered.

TERT AND CIRCULATING TUMOR CELLS’ (CTCS) SURVIVAL IN CIRCULATION

The bloodstream represents a hostile environment for CTCs, exposing various cellular stresses that include oxidative stress and endoplasmic reticulum (ER) stress (7, 44, 45). It has been found by using animal models (46) that less than 0.02% of tumor cells in circulation can survive to form metastasis. To survive and disseminate in the circulation, CTCs not only induce survival-related pathways and the EMT program, but also interact with bioactive factors and stroma cells to facilitate their passage to extravasation at distant sites (8, 44). Tumor cells and tumor-associated stromal cells secrete abundant reactive oxygen species (ROS) into the tumor microenvironment (47). ROS exerts an important role in cellular activities, including genomic instability, cell death, and cellular senescence (48). CTCs use multiple pathways to adapt to the increased ROS, including modification of metabolism and up-regulation of β-hemoglobin (49, 50). More recently, evidence showed that oxidative stress inhibits distant metastasis (49, 51). To mention briefly, several studies demonstrated that TERT alleviates the production of ROS, improves mitochondrial function, and inhibits ROS-induced apoptosis in cancer cells (52-54). Moreover, CTCs are also exposed to various stress stimuli that activate the unfolded protein response (UPR), a homeostatic pathway, that is mainly composed of the IRE1α-xbp1, ATF6, and PERK-eIF2α pathways and orchestrates several events to restore the ER folding capacity or can induce cell death when restoration fails (47, 55). Importantly, we previous reported that ER stress promotes hTERT expression in both human cancer cells and murine neural cells, which protects cells from ER stress-induced cell death (56). Moreover, over-expression of hTERT reduces ER stress-induced cell death, which is independent of catalytically active enzymes or DNA damage signaling, whereas depletion of hTERT sensitizes cells to undergo apoptosis under ER stress. Additionally, Yu et al. demonstrated that CTCs of breast tumors exhibit combinations of epithelial and mesenchymal traits, suggesting an important role for EMT in the blood-borne dissemination of human breast cancer (57). It seems reasonable that TERT may protect CTCs from oxidative stress or ER stress. So far, the mechanisms by which oxidative stress or ER stress regulates the CTCs survival are largely unknown. As mentioned above, there are less than 0.02% of tumor cells that can survive in circulating blood, which leads to a big bottleneck in collecting enough CTCs.

TERT AND EXTRAVASATION

CTCs may cross from vessel lumina into the tissue parenchyma by traversing the endothelial cell and pericyte layers, which is considered as extravasation (58). Accordingly, CTCs secret a series of factors to affect the microenvironments and promote vascular hyperpermeability, which leads to tumor cells across the barriers to extravasation in tissues (58). For example, it has been demonstrated that VEGF promotes the process of extravasation by inducing pulmonary hyperpermeability, which was prior to the arrival of CTCs in the lungs (59, 60). Moreover, MMPs facilitate the extravasation of breast tumor cells by disrupting pulmonary vascular endothelial cell-cell junctions (42, 61). Given that TERT can induce the expression of MMPs and VEGF, these findings suggest that TERT may contribute to the process of extravasation during metastasis. VEGF and MMPs may promote the processes of both intravasation and extravasation, suggesting that certain traits which were favorable previously in the process of tumor invasion also prove useful at the later steps in the invasion-metastasis cascade. However, the mechanisms by which TERT regulates the extravasation need to be addressed. Recently, studies have demonstrated that CCL2 promotes the extravasation and subsequent metastatic growth by directly increasing the vascular permeability in lung parenchyma (58, 62). Moreover, inflammatory monocytes facilitate the extravasation of breast carcinoma cells via a CCL2-dependent mechanism (62). It has been reported that hTERT promotes invasion and migration of colon-cancer cells by upregulating expression of CCL2 (30). Therefore, we speculate that TERT may contribute to the extravasation via CCL2. Taken together, TERT could induce VEGF, CCL2, and MMPs expression and enhance the vascular hyperpermeability, thereby promoting the intravasation. However, the detailed mechanisms by which TERT regulates the intravasation remain to be found.

IMPLICATIONS OF TERT IN MICROMETASTASIS FORMATION AND MACROMETASTATIC GROWTH

Cancer cells extravasate into the parenchyma of target tissues and start colonization after CTCs are arrested in capillaries at distant sites. Disseminated tumor cells (DTCs) land in a new tissue microenvironment, where they lack the familiar stromal cells, growth factors, cytokines, and ECM constituents that had been present in the primary tumor site (7). Hence, most DTCs arrive at the metastatic site as solitary tumor cells and have to resume growth to develop a new colony and establish a micrometastasis. Otherwise, they will die or enter dormancy (63). Early studies demonstrated that the ratio between the p38 mitogen-activated protein kinase (p38) and extracellular signal-regulated kinase1/2 (ERK1/2) determines whether DTCs enter proliferation or dormancy (63-65). The activities of p38 and ERK are regulated by altered intrinsic signaling pathways and external dormancy-inducing signals (65-72). Of note, the property of tumor initiation in cancer stem cells (CSCs) is a prerequisite for successfully forming a metastatic colony (7). Interestingly, Okamoto et al. revealed that hTERT forms a complex with nucleolar GTP-binding protein nucleostemin (GNL3L/NS) and BRG1, which act in a telomere-independent manner to maintain the state of tumor-initiating cells or cancer stem cells (73). Thus, we speculate that TERT may drive DTCs in the status of cancer stem cells, which contributes to the formation of metastastic colonies. Moreover, some studies have demonstrated that external dormancy-inducing signals, including bone morphogenetic protein (BMP) ligand 7 (BMP7) and TNF-β, induce dormancy of tumor cells (65, 69). Importantly, Lucy et al. revealed that BMP7 negatively regulates telomere maintenance by suppressing hTERT, inducing cervical tumor-growth arrest (74). Li et al. found that TNF-β suppresses TERT expression by Smad3 interacting with c-Myc and TERT promoter (75). Given that BMP7, TNF-β, and hTERT are impor-tant for underpinning cancer stem-cells renewal and proliferation, we speculate that the functional regulation of hTERT by BMP7 or TNF-β may take an important role in establishing a balance between tumor dormancy and metastatic colonies’ growth. Interestingly, Xu’s lab reported that hTERT promotes in vivo tumorigenesis and metastastic colonies of gastric-cancer cells (20). It’s the first direct evidence to support the assumption that hTERT facilitates the formation of metastastic colonies. The detailed mechanisms by which TERT maintains the dormancy of DTCs and promotes micrometastasis remain to be discovered.

IMPLICATIONS OF TERT PROMOTER MUTATION IN TUMOR METASTASIS

The TERT promoter hotspot mutations (C228T and C250T) have been widely investigated and identified as driver mutations with different frequencies from undetectable to 85% in various human cancer types (76, 77). Clinically, tumor samples carrying TERT promoter mutations promote the expression of TERT mRNA and telomerase activity compared to those having a wild-type promoter (78). Through experimentation, the introduction of either -124C > T or -146C > T into the TERT promoter reporter significantly increases the promoter activity (77, 79). It has been reported that GA-binding proteins were specifically recruited to the TERT mutant promoter compared to the wild-type TERT promoter, which enhances TERT transcription and telomerase activity (79). Therefore, it has been considered that the interaction between GA-binding proteins and the TERT promoter mutations forms a novel mechanism for telomerase activation in malignant transformation. It’s interesting that accumulating evidence showed that TERT promoter mutations associate tumor metastasis with several cancer types, including melanoma, thyroid cancer, urothelial carcinomas, and glioblastomas. First, it has been reported that a higher frequency of TERT promoter mutations was observed in metastatic tissues than in primary melanomas. These mutations were associated with shorter survival or short disease-free survival in melanomas, suggesting the functional role of TERT promoter mutations in the metastatic process of melanoma cells (80). Second, it has been demonstrated that TERT promoter mutations are associated with distant metastasis, worse prognostic features, poor survival, and worse response to treatment in thyroid cancer (81-86). Third, evidence showed that TERT promoter mutations are related to distant metastases in glioblastomas and urothelial carcinomas (87). It’s worth mentioning that the simultaneous mutation of BRAF/RAS and TERT promoter leads a high aggressiveness in thyroid cancer, melanoma, and lung cancer with different mechanisms being identified. For example, it has been proposed KRAS activates the expression of TERT by promoting the activity of RAS/MEK pathway, which leads aggressiveness of lung cancer cells (88). Moreover, Liu et al. demonstrated a novel mechanism for the activation of mutant TERT by the BRAF V600E/MAP kinase pathway through FOS/GABP in human cancer (89, 90). In summary, TERT promoter mutations that are implicated in the tumor metastasis and mechanisms by which TERT promoter mutations regulate the tumor metastasis are largely unidentified.

CONCLUDING REMARKS

In the past few years, sufficient evidence indicates that TERT has non-canonical functions beyond telomere maintenance in several important cellular processes, including cell proliferation, inflammation, apoptosis, EMT, cell adhesion and migration, angiogenesis, DNA damage response, and transcriptional regulation of target genes (5, 91, 92). As summarized in this review, accumulating studies have revealed that TERT may facilitate most steps of invasion-metastasis cascade as summarized in Fig. 1 including:

Fig. 1

TERT facilitates the invasion-metastasis cascade. TERT promotes local invasion via MMPs, NF-κB, EMT, and ITGB1. TERT promotes intravasation via TGF-β and VEGF. TERT promotes CTCs survival in circulation via EMT and anti-oxidative stress and ER stress-induced apoptosis. TERT promotes extravasation via VEGF, MMPs, and CCL2. TERT promotes the formation of micrometastasis and the macrometastatic growth partially through EMT and hTERT/GNL3L/NS/BRG1 complex. The actions of TERT implicated in tumor metastasis are described in the text. ECM, extracellular matrix. BM, basement membrane.

(1) Promotes local invasion of primary cancer cells by using different factors and cellular programs, mainly including NF-κB, MMPs, EMT, and ITGB1.

(2) Promotes the intravasation through VEGF and TNF-β.

(3) Promotes CTCs survival by using an EMT program or anti-oxidative stress or ER stress-induced apoptosis.

(4) Promotes the extravasation through tumor-secreted VEGF, MMPs, and CCL2.

(5) Promotes micrometastasis formation and macrometastatic growth, in which EMT, hTERT/GNL3L/NS/BRG1 complex, and external dormancy-inducing signals (such as, BMP7 and TNF-β) are involved.

TERT may facilitate the invasion metastasis cascade, which suggests that TERT is a new diagnostic and attractive therapeutic target in tumor metastasis. In line with this hypothesis, several approaches have been adopted, including oligonucleotides (e.g., GRN163L), small-molecule inhibitors (e.g., BIBR1532), and anti-telomerase immune-therapeutics (GRVAC1, GV1001 and Vx001), to selectively induce apoptosis and cell death in cancer cells (93). GRN163L can efficiently target glioblastoma tumor-initiating cells, which leads to a decreased proliferation and tumor growth (94). Similarly, clinical trial results demonstrated that a vaccine (GV1001, hTERT peptide) is a promising as a telomerase-targeting vaccine and can stimulate CD4+ and CD8+ responses in telomerase-positive tumors, showing minimal effects on normal cells and no autoimmunity (93). However, metastatic disease is complex and systemic and resists most of current therapeutic strategies, which are closely affected by the tumor microenvironment, which plays a vital role in determining the success of therapeutic vaccination, but the mechanisms by which TERT is employed in the metastatic microenvironment are poorly understood. Thus, it’s urgent to arrive at a precise understanding of the contribution of TERT in each step of the invasion-metastasis cascade.

It has been extensively studied how TERT promotes invasion by cancer cells. However, the detailed functional aspects and mechanisms by which TERT regulates the local invasion of primary tumor cells remain to be identified. Importantly, studies have shown that preparation for a metastatic journey, which is involved in evasion of tumor immunity and pre-metastatic niche, is a crucial step for primary tumors to start the invasion-metastasis cascade (31, 32). More questions need to be answered in the future:

(1) Whether TERT regulates the functional aspects of immune cells to affect the tumor invasion, including TAMs, TANs, MDSCs, Treg, and B cells.

(2) Whether TERT regulates the cytotoxicity of NK cells and CD8 T cells.

(3) Whether TERT promoter mutations (C228T and C250T) regulate the immune cells and the cytotoxicity of NK cells and CD8 T cells (76, 77).

Metastatic colonization may require several years or decades to complete, which provides a key therapeutic window for targeting metastatic colonization (95). Targeting CSCs may alleviate metastatic colonization (7). Importantly, several studies have suggested that TERT takes an important role in maintaining the state of CSCs and dormancy of DTCs via the TERT-GNL3L-BRG1 complex and external dormancy-inducing signals (65, 69, 73). However, more questions need to be answered:

(1) Whether both TERT and the TERT-GNL3L-BRG1 complex regulate the dormancy of DTCs.

(2) Mechanisms by which TERT regulates the external dormancy-inducing signals, including BMP7 and TNFβ.

(3) The detailed mechanism by which TERT promotes meta-stastic colonies of gastric cancer cells (20).