Role of chromosomal instability in cancer progression

Sarah E McClelland

doi:10.1530/erc-17-0187

Role of chromosomal instability in cancer progression

Endocrine Related Cancer ◽

10.1530/erc-17-0187 ◽

2017 ◽

Vol 24 (9) ◽

pp. T23-T31 ◽

Cited By ~ 30

Author(s):

Sarah E McClelland

Keyword(s):

Cancer Cells ◽

Cancer Progression ◽

Chromosomal Instability ◽

Genetic Material ◽

The Body ◽

Haploid Number ◽

Normal Cells ◽

Structural Alterations ◽

Novel Approaches

Cancer cells often displaychromosomal instability(CIN), a defect that involves loss or rearrangement of the cell’s genetic material – chromosomes – during cell division. This process results in the generation of aneuploidy, a deviation from the haploid number of chromosomes, and structural alterations of chromosomes in over 90% of solid tumours and many haematological cancers. This trait is unique to cancer cells as normal cells in the body generally strictly maintain the correct number and structure of chromosomes. This key difference between cancer and normal cells has led to two important hypotheses: (i) cancer cells have had to overcome inherent barriers to changes in chromosomes that are not tolerated in non-cancer cells and (ii) CIN represents a cancer-specific target to allow the specific elimination of cancer cells from the body. To exploit these hypotheses and design novel approaches to treat cancer, a full understanding of the mechanisms driving CIN and how CIN contributes to cancer progression is required. Here, we will discuss the possible mechanisms driving chromosomal instability, how CIN may contribute to the progression at multiple stages of tumour evolution and possible future therapeutic directions based on targeting cancer chromosomal instability.

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Cancer Fighting SiRNA-RRM2 Loaded Nanorobots

Pharmaceutical Nanotechnology ◽

10.2174/2211738508666200128120142 ◽

2020 ◽

Vol 8 (2) ◽

pp. 79-90

Author(s):

Arjun Sharma ◽

Pravir Kumar ◽

Rashmi K. Ambasta

Keyword(s):

Cancer Therapy ◽

Dna Synthesis ◽

Cancer Progression ◽

Sirna Delivery ◽

Predictive Marker ◽

The Body ◽

Tumor Site ◽

Target Delivery ◽

Target Effect

Background: Silencing of several genes is critical for cancer therapy. These genes may be apoptotic gene, cell proliferation gene, DNA synthesis gene, etc. The two subunits of Ribonucleotide Reductase (RR), RRM1 and RRM2, are critical for DNA synthesis. Hence, targeting the blockage of DNA synthesis at tumor site can be a smart mode of cancer therapy. Specific targeting of blockage of RRM2 is done effectively by SiRNA. The drawbacks of siRNA delivery in the body include the poor uptake by all kinds of cells, questionable stability under physiological condition, non-target effect and ability to trigger the immune response. These obstacles may be overcome by target delivery of siRNA at the tumor site. This review presents a holistic overview regarding the role of RRM2 in controlling cancer progression. The nanoparticles are more effective due to specific characteristics like cell membrane penetration capacity, less toxicity, etc. RRM2 have been found to be elevated in different types of cancer and identified as the prognostic and predictive marker of the disease. Reductase RRM1 and RRM2 regulate the protein and gene expression of E2F, which is critical for protein expression and progression of cell cycle and cancer. The knockdown of RRM2 leads to apoptosis via Bcl2 in cancer. Both Bcl2 and E2F are critical in the progression of cancer, hence a gene that can affect both in regulating DNA replication is essential for cancer therapy. Aim: The aim of the review is to identify the related gene whose silencing may inhibit cancer progression. Conclusion: In this review, we illuminate the critical link between RRM-E2F, RRM-Bcl2, RRM-HDAC for the therapy of cancer. Altogether, this review presents an overview of all types of SiRNA targeted for cancer therapy with special emphasis on RRM2 for controlling the tumor progression.

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The wages of CIN

The Journal of Cell Biology ◽

10.1083/jcb.200801030 ◽

2008 ◽

Vol 180 (4) ◽

pp. 661-663 ◽

Cited By ~ 12

Author(s):

Karen W. Yuen ◽

Arshad Desai

Keyword(s):

Cancer Cells ◽

Solid Tumors ◽

Chromosomal Instability ◽

Chromosome Instability ◽

Spindle Checkpoint ◽

Human Cells ◽

Normal Cells ◽

Chromosome Missegregation ◽

Cell Biol ◽

The Relationship

Aneuploidy and chromosome instability (CIN) are hallmarks of the majority of solid tumors, but the relationship between them is not well understood. In this issue, Thompson and Compton (Thompson, S.L., and D.A. Compton. 2008. Examining the link between chromosomal instability and aneuploidy in human cells. J. Cell. Biol. 180:665–672) investigate the mechanism of CIN in cancer cells and find that CIN arises primarily from defective kinetochore–spindle attachments that evade detection by the spindle checkpoint and persist into anaphase. They also explore the consequences of artificially elevating chromosome missegregation in otherwise karyotypically normal cells. Their finding that induced aneuploidy is rapidly selected against suggests that the persistence of aneuploid cells in tumors requires not only chromosome missegregation but also additional, as yet poorly defined events.

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MATHEMATICAL MODELLING OF CANCER CELL INVASION OF TISSUE: THE ROLE OF THE UROKINASE PLASMINOGEN ACTIVATION SYSTEM

Mathematical Models and Methods in Applied Sciences ◽

10.1142/s0218202505000947 ◽

2005 ◽

Vol 15 (11) ◽

pp. 1685-1734 ◽

Cited By ~ 169

Author(s):

M. A. J. CHAPLAIN ◽

G. LOLAS

Keyword(s):

Cancer Cells ◽

Cancer Cell ◽

Cell Invasion ◽

The Body ◽

Plasminogen Activation ◽

Cancer Cell Invasion ◽

Plasminogen Activation System ◽

Activation System ◽

Spatio Temporal

The growth of solid tumours proceeds through two distinct phases: the avascular and the vascular phase. It is during the latter stage that the insidious process of cancer invasion of peritumoral tissue can and does take place. Vascular tumours grow rapidly allowing the cancer cells to establish a new colony in distant organs, a process that is known as metastasis. The progression from a single, primary tumour to multiple tumours in distant sites throughout the body is known as the metastatic cascade. This is a multistep process that first involves the over-expression by the cancer cells of proteolytic enzyme activity, such as the urokinase-type plasminogen activator (uPA) and matrix metalloproteinases (MMPs). uPA itself initiates the activation of an enzymatic cascade that primarily involves the activation of plasminogen and subsequently its matrix degrading protein plasmin. Degradation of the matrix then enables the cancer cells to migrate through the tissue and subsequently to spread to secondary sites in the body. In this paper we consider a mathematical model of cancer cell invasion of tissue (extracellular matrix) which focuses on the role of the plasminogen activation system. The model consists of a system of reaction-diffusion-taxis partial differential equations describing the interactions between cancer cells, urokinase plasminogen activator (uPA), uPA inhibitors, plasmin and the host tissue. The focus of the modelling is on the spatio-temporal dynamics of the uPA system and how this influences the migratory properties of the cancer cells through random motility, chemotaxis and haptotaxis. The results obtained from numerical computations carried out on the model equations produce rich, dynamic heterogeneous spatio-temporal solutions and demonstrate the ability of rather simple models to produce complicated dynamics, all of which are associated with tumour heterogeneity and cancer cell progression and invasion.

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How Antimalarials and Antineoplastic Drugs can Interact in Combination Therapies: a Perspective on the Role of PPT1 Enzyme

Current Drug Metabolism ◽

10.2174/1389200222666211118114057 ◽

2021 ◽

Vol 22 ◽

Author(s):

Diana Duarte ◽

Nuno Vale

Keyword(s):

Cancer Cells ◽

Cancer Progression ◽

Antineoplastic Agents ◽

Antimalarial Drugs ◽

Antineoplastic Drugs ◽

Anticancer Effects ◽

Different Types ◽

Important Pathway ◽

Palmitoyl Protein Thioesterase

: Antimalarial drugs from different classes have demonstrated anticancer effects in different types of cancer cells, but their complete mode of action in cancer remains unknown. Recently, several studies reported the important role of palmitoyl-protein thioesterase 1 (PPT1), a lysosomal enzyme, as the molecular target of chloroquine and its derivates in cancer. It was also found that PPT1 is overexpressed in different types of cancer, such as breast, colon, etc. Our group has found a synergistic interaction between antimalarial drugs, such as mefloquine, artesunate and chloroquine and antineoplastic drugs in breast cancer cells, but the mechanism of action was not determined. Here, we describe the importance of autophagy and lysosomal inhibitors in tumorigenesis and hypothesize that other antimalarial agents besides chloroquine could also interact with PPT1 and inhibit the mechanistic target of rapamycin (mTOR) signalling, an important pathway in cancer progression. We believe that PPT1 inhibition results in changes in the lysosomal metabolism that result in less accumulation of antineoplastic drugs in lysosomes, which increases the bioavailability of the antineoplastic agents. Taken together, these mechanisms help to explain the synergism of antimalarial and antineoplastic agents in cancer cells.

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Role of Integrins in Resistance to Therapies Targeting Growth Factor Receptors in Cancer

Cancers ◽

10.3390/cancers11050692 ◽

2019 ◽

Vol 11 (5) ◽

pp. 692 ◽

Cited By ~ 16

Author(s):

Elisabete Cruz da Silva ◽

Monique Dontenwill ◽

Laurence Choulier ◽

Maxime Lehmann

Keyword(s):

Cancer Cells ◽

Cancer Progression ◽

Tyrosine Kinases ◽

Treatment Options ◽

Cancer Cell Proliferation ◽

Remarkable Feature ◽

Rtk Signaling ◽

Intracellular Signal ◽

New Treatment

Integrins contribute to cancer progression and aggressiveness by activating intracellular signal transduction pathways and transducing mechanical tension forces. Remarkably, these adhesion receptors share common signaling networks with receptor tyrosine kinases (RTKs) and support their oncogenic activity, thereby promoting cancer cell proliferation, survival and invasion. During the last decade, preclinical studies have revealed that integrins play an important role in resistance to therapies targeting RTKs and their downstream pathways. A remarkable feature of integrins is their wide-ranging interconnection with RTKs, which helps cancer cells to adapt and better survive therapeutic treatments. In this context, we should consider not only the integrins expressed in cancer cells but also those expressed in stromal cells, since these can mechanically increase the rigidity of the tumor microenvironment and confer resistance to treatment. This review presents some of these mechanisms and outlines new treatment options for improving the efficacy of therapies targeting RTK signaling.

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Spatiotemporal pH Heterogeneity as a Promoter of Cancer Progression and Therapeutic Resistance

Cancers ◽

10.3390/cancers11071026 ◽

2019 ◽

Vol 11 (7) ◽

pp. 1026 ◽

Cited By ~ 13

Author(s):

David E. Korenchan ◽

Robert R. Flavell

Keyword(s):

Cancer Cells ◽

Cancer Progression ◽

Co2 Exchange ◽

Therapeutic Resistance ◽

Slow Time ◽

Phenotypic Changes ◽

Ph Buffering ◽

Available Technology ◽

Kinetics Of

Dysregulation of pH in solid tumors is a hallmark of cancer. In recent years, the role of altered pH heterogeneity in space, between benign and aggressive tissues, between individual cancer cells, and between subcellular compartments, has been steadily elucidated. Changes in temporal pH-related processes on both fast and slow time scales, including altered kinetics of bicarbonate-CO2 exchange and its effects on pH buffering and gradual, progressive changes driven by changes in metabolism, are further implicated in phenotypic changes observed in cancers. These discoveries have been driven by advances in imaging technologies. This review provides an overview of intra- and extracellular pH alterations in time and space reflected in cancer cells, as well as the available technology to study pH spatiotemporal heterogeneity.

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Vimentin filaments drive migratory persistence in polyploidal cancer cells

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.2011912117 ◽

2020 ◽

Vol 117 (43) ◽

pp. 26756-26765

Author(s):

Botai Xuan ◽

Deepraj Ghosh ◽

Joy Jiang ◽

Rachelle Shao ◽

Michelle R. Dawson

Keyword(s):

Cancer Cells ◽

Cancer Progression ◽

Structural Integrity ◽

Single Cell Analysis ◽

Critical Role ◽

Critical Function ◽

Rna Knockdown ◽

Interfering Rna ◽

The Impact

Polyploidal giant cancer cells (PGCCs) are multinucleated chemoresistant cancer cells found in heterogeneous solid tumors. Due in part to their apparent dormancy, the effect of PGCCs on cancer progression has remained largely unstudied. Recent studies have highlighted the critical role of PGCCs as aggressive and chemoresistant cancer cells, as well as their ability to undergo amitotic budding to escape dormancy. Our recent study demonstrated the unique biophysical properties of PGCCs, as well as their unusual migratory persistence. Here we unveil the critical function of vimentin intermediate filaments (VIFs) in maintaining the structural integrity of PGCCs and enhancing their migratory persistence. We performed in-depth single-cell analysis to examine the distribution of VIFs and their role in migratory persistence. We found that PGCCs rely heavily on their uniquely distributed and polarized VIF network to enhance their transition from a jammed to an unjammed state to allow for directional migration. Both the inhibition of VIFs with acrylamide and small interfering RNA knockdown of vimentin significantly decreased PGCC migration and resulted in a loss of PGCC volume. Because PGCCs rely on their VIF network to direct migration and to maintain their enlarged morphology, targeting vimentin or vimentin cross-linking proteins could provide a therapeutic approach to mitigate the impact of these chemoresistant cells in cancer progression and to improve patient outcomes with chemotherapy.

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Metabolic cooperation between cancer and non-cancerous stromal cells is pivotal in cancer progression

Tumor Biology ◽

10.1177/1010428318756203 ◽

2018 ◽

Vol 40 (2) ◽

pp. 101042831875620 ◽

Cited By ~ 11

Author(s):

Filipa Lopes-Coelho ◽

Sofia Gouveia-Fernandes ◽

Jacinta Serpa

Keyword(s):

Cancer Cells ◽

Cancer Progression ◽

Stromal Cells ◽

Inflammatory Cells ◽

Metabolic Adaptation ◽

Metabolic Cooperation ◽

Metabolic Remodeling ◽

Organ Tissue ◽

Cancerous Cells

The way cancer cells adapt to microenvironment is crucial for the success of carcinogenesis, and metabolic fitness is essential for a cancer cell to survive and proliferate in a certain organ/tissue. The metabolic remodeling in a tumor niche is endured not only by cancer cells but also by non-cancerous cells that share the same microenvironment. For this reason, tumor cells and stromal cells constitute a complex network of signal and organic compound transfer that supports cellular viability and proliferation. The intensive dual-address cooperation of all components of a tumor sustains disease progression and metastasis. Herein, we will detail the role of cancer-associated fibroblasts, cancer-associated adipocytes, and inflammatory cells, mainly monocytes/macrophages (tumor-associated macrophages), in the remodeling and metabolic adaptation of tumors.

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The Functional Role of MnSOD as a Biomarker of Human Diseases and Therapeutic Potential of a New Isoform of a Human Recombinant MnSOD

BioMed Research International ◽

10.1155/2014/476789 ◽

2014 ◽

Vol 2014 ◽

pp. 1-11 ◽

Cited By ~ 19

Author(s):

Antonella Borrelli ◽

Antonietta Schiattarella ◽

Patrizia Bonelli ◽

Franca Maria Tuccillo ◽

Franco Maria Buonaguro ◽

...

Keyword(s):

Cancer Cells ◽

Manganese Superoxide Dismutase ◽

Therapeutic Potential ◽

Human Diseases ◽

Leader Peptide ◽

X Rays ◽

Normal Cells ◽

Initial Application ◽

Prevention Of Cancer

Reactive oxygen species (ROS) are generated as a consequence of metabolic reactions in the mitochondria of eukaryotic cells. This work describes the role of the manganese superoxide dismutase (MnSOD) as a biomarker of different human diseases and proposes a new therapeutic application for the prevention of cancer and its treatment. The paper also describes how a new form of human MnSOD was discovered, its initial application, and its clinical potentials. The MnSOD isolated from a human liposarcoma cell line (LSA) was able to kill cancer cells expressing estrogen receptors, but it did not have cytotoxic effects on normal cells. Together with its oncotoxic activity, the recombinant MnSOD (rMnSOD) exerts a radioprotective effect on normal cells irradiated with X-rays. The rMnSOD is characterized by the presence of a leader peptide, which allows the protein to enter cells: this unique property can be used in the radiodiagnosis of cancer or chemotherapy, conjugating radioactive substances or chemotherapic drugs to the leader peptide of the MnSOD. Compared to traditional chemotherapic agents, the drugs conjugated with the leader peptide of MnSOD can selectively reach and enter cancer cells, thus reducing the side effects of traditional treatments.

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EDD1 predicts prognosis and regulates gastric cancer growth in vitro and in vivo via miR-22

Biological Chemistry ◽

10.1515/hsz-2015-0279 ◽

2016 ◽

Vol 0 (0) ◽

Author(s):

Min Yang ◽

Nan Jiang ◽

Qi-wei Cao ◽

Qing Sun

Keyword(s):

Gastric Cancer ◽

Cancer Cells ◽

Cancer Progression ◽

Patient Survival ◽

Underlying Mechanism ◽

Gastric Cancer Cells ◽

Cancer Tissues

Abstract Gastric cancer is the most common digestive malignant tumor worldwild. EDD1 was reported to be frequently amplified in several tumors and played an important role in the tumorigenesis process. However, the biological role and potential mechanism of EDD1 in gastric cancer remains poorly understood. In this study, we are aim to investigate the effect of EDD1 on gastric cancer progression and to explore the underlying mechanism. The results showed the significant up-regulation of EDD1 in -gastric cancer cell tissues and lines. The expression level of EDD1 was also positively associated with advanced clinical stages and predicted poor overall patient survival and poor disease-free patient survival. Besides, EDD1 knockdown markedly inhibited cell viability, colony formation, and suppressed tumor growth. Opposite results were obtained in gastric cancer cells with EDD1 overexpression. EDD1 knockdown was also found to induce gastric cancer cells apoptosis. Further investigation indicated that the oncogenic role of EDD1 in regulating gastric cancer cells growth and apoptosis was related to its PABC domain and directly through targeting miR-22, which was significantly down-regulated in gastric cancer tissues. Totally, our study suggests that EDD1 plays an oncogenic role in gastric cancer and may be a potential therapeutic target for gastric cancer.

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