Your search keyword '"Oncogene"' showing total 16,685 results

1. Role of TRIP13 in human cancer development.

Author

Chen, Chaohu, Li, Pan, Fan, Guangrui, Yang, Enguang, Jing, Suoshi, Shi, Yibo, Gong, Yuwen, Zhang, Luyang, and Wang, Zhiping

Abstract

As an AAA + ATPase, thyroid hormone receptor interacting protein 13 (TRIP13) primarily functions in DNA double-strand break repair, chromosome recombination, and cell cycle checkpoint regulation; aberrant expression of TRIP13 can result in chromosomal instability (CIN). According to recent research, TRIP13 is aberrantly expressed in a variety of cancers, and a patient's poor prognosis and tumor stage are strongly correlated with high expression of TRIP13. Tumor cell and subcutaneous xenograft growth can be markedly inhibited by TRIP13 knockdown or TRIP13 inhibitor administration. In the initiation and advancement of human malignancies, TRIP13 seems to function as an oncogene. Based on available data, TRIP13 may function as a biological target and biomarker for cancer. The creation of inhibitors that specifically target TRIP13 may present novel approaches to treating cancer. [ABSTRACT FROM AUTHOR]

Published

2024

2. Biological functions and therapeutic potential of CKS2 in human cancer.

Author

Yueliang Lai and Ye Lin

Subjects

PROGNOSIS, CANCER genes, MOLECULAR diagnosis, BIOLOGY, CELL proliferation

Abstract

The incidence of cancer is increasing worldwide and is the most common cause of death. Identification of novel cancer diagnostic and prognostic biomarkers is important for developing cancer treatment strategies and reducing mortality. Cyclin-dependent kinase subunit 2 (CKS2) is involved in cell cycle and proliferation processes, and based on these processes, CKS2 was identified as a cancer gene. CKS2 is expressed in a variety of tissues in the human body, but its abnormal expression is associated with cancer in a variety of systems. CKS2 is generally elevated in cancer, plays a role in almost all aspects of cancer biology (such as cell proliferation, invasion, metastasis, and drug resistance) through multiple mechanisms regulating certain important genes, and is associated with clinicopathological features of patients. In addition, CKS2 expression patterns are closely related to cancer type, stage and other clinical variables. Therefore, CKS2 is considered as a tool for cancer diagnosis and prognosis and may be a promising tumor biomarker and therapeutic target. This article reviews the biological function, mechanism of action and potential clinical significance of CKS2 in cancer, in order to provide a new theoretical basis for clinical molecular diagnosis, molecular targeted therapy and scientific research of cancer. [ABSTRACT FROM AUTHOR]

Published

2024

3. "The 10th International MDM2 Workshop": Opening up new avenues for MDM2 and p53 research, the First International MDM2 Workshop in Asia.

Author

Ohki, Rieko, Itahana, Koji, and Iwakuma, Tomoo

Subjects

*DRUG discovery, *POSTER presentations, *CANCER research, *RESEARCH institutes

Abstract

The 10th International MDM2 Workshop was held at the National Cancer Center Research Institute (NCCRI) in Tokyo, Japan, from October 15 to 18, 2023. It attracted 166 participants from 12 countries. The meeting featured 52 talks and 41 poster presentations. In the first special session, six invited speakers gave educational and outstanding talks on breakthroughs in MDM2 research. Three keynote speakers presented emerging p53‐independent functions of MDM2/MDM4, functional association of MDM2/p53 with cancer immunity, and drug discovery targeting the MDM2/MDM4‐p53 pathway. Additionally, 19 invited speakers introduced their new findings. Twenty‐one presenters, many of whom were young investigators, postdocs, and students, were selected from submitted abstracts and reported their exciting and unpublished results. For poster presenters, outstanding poster awards were given to the best presenters. There were many inspiring questions and discussions throughout the meeting. Social events like a welcome party, a workshop dinner, and an optional tour enabled further scientific interactions among the participants. The meeting successfully provided an exciting platform for scientific exchange. The experience gained from organizing this meeting will be handed over to the next organizers of the 11th International MDM2 Workshop. [ABSTRACT FROM AUTHOR]

Published

2024

4. Biological functions and therapeutic potential of SRY related high mobility group box 5 in human cancer.

Author

Juan-di Xue, Wan-fang Xiang, Ming-qin Cai, and Xiao-yun Lv

Subjects

SOX transcription factors, CARCINOGENS, TRANSCRIPTION factors, MOLECULAR diagnosis, PROGNOSIS

Abstract

Cancer is a heavy human burden worldwide, with high morbidity and mortality. Identification of novel cancer diagnostic and prognostic biomarkers is important for developing cancer treatment strategies and reducing mortality. Transcription factors, including SRY associated high mobility group box (SOX) proteins, are thought to be involved in the regulation of specific biological processes. There is growing evidence that SOX transcription factors play an important role in cancer progression, including tumorigenesis, changes in the tumor microenvironment, and metastasis. SOX5 is a member of SOX Group D of Sox family. SOX5 is expressed in various tissues of human body and participates in various physiological and pathological processes and various cellular processes. However, the abnormal expression of SOX5 is associated with cancer of various systems, and the abnormal expression of SOX5 acts as a tumor promoter to promote cancer cell viability, proliferation, invasion, migration and EMT through multiple mechanisms. In addition, the expression pattern of SOX5 is closely related to cancer type, stage and adverse clinical outcome. Therefore, SOX5 is considered as a potential biomarker for cancer diagnosis and prognosis. In this review, the expression of SOX5 in various human cancers, the mechanism of action and potential clinical significance of SOX5 in tumor, and the therapeutic significance of Sox5 targeting in cancer were reviewed. In order to provide a new theoretical basis for cancer clinical molecular diagnosis, molecular targeted therapy and scientific research. [ABSTRACT FROM AUTHOR]

Published

2024

5. Molecular Mechanisms of Oncogenesis

Author

Thakur, Kanika, Sharma, Shtakshi, Kumar, Vijay, Kumar, Ravinder, Sobti, Ranbir Chander, editor, Sugimura, Haruhiko, editor, and Sobti, Aastha, editor

Published

2024

6. Long Non-coding RNAs in Cancer

Author

Nadhan, Revathy, Isidoro, Ciro, Song, Yong Sang, Dhanasekaran, Danny N., Sharma, Siddharth, Section editor, Sobti, R. C., editor, Ganguly, Nirmal K., editor, and Kumar, Rakesh, editor

Published

2024

7. High Intrinsic Oncogenic Potential in the Myc-Box-Deficient Hydra Myc3 Protein

Author

Lechable, Marion, Tang, Xuechen, Siebert, Stefan, Feldbacher, Angelika, Fernández-Quintero, Monica L, Breuker, Kathrin, Juliano, Celina E, Liedl, Klaus R, Hobmayer, Bert, and Hartl, Markus

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, Regenerative Medicine, Stem Cell Research, Stem Cell Research - Nonembryonic - Non-Human, Rare Diseases, Cancer, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Animals, Humans, Hydra, Amino Acid Sequence, Genes, myc, Helix-Loop-Helix Motifs, Amino Acids, cancer, cnidaria, development, gene regulation, interstitial stem cell, neurogenesis, oncogene, signal transduction, Biological sciences, Biomedical and clinical sciences

Abstract

The proto-oncogene myc has been intensively studied primarily in vertebrate cell culture systems. Myc transcription factors control fundamental cellular processes such as cell proliferation, cell cycle control and stem cell maintenance. Myc interacts with the Max protein and Myc/Max heterodimers regulate thousands of target genes. The genome of the freshwater polyp Hydra encodes four myc genes (myc1-4). Previous structural and biochemical characterization showed that the Hydra Myc1 and Myc2 proteins share high similarities with vertebrate c-Myc, and their expression patterns suggested a function in adult stem cell maintenance. In contrast, an additional Hydra Myc protein termed Myc3 is highly divergent, lacking the common N-terminal domain and all conserved Myc-boxes. Single cell transcriptome analysis revealed that the myc3 gene is expressed in a distinct population of interstitial precursor cells committed to nerve- and gland-cell differentiation, where the Myc3 protein may counteract the stemness actions of Myc1 and Myc2 and thereby allow the implementation of a differentiation program. In vitro DNA binding studies showed that Myc3 dimerizes with Hydra Max, and this dimer efficiently binds to DNA containing the canonical Myc consensus motif (E-box). In vivo cell transformation assays in avian fibroblast cultures further revealed an unexpected high potential for oncogenic transformation in the conserved Myc3 C-terminus, as compared to Hydra Myc2 or Myc1. Structure modeling of the Myc3 protein predicted conserved amino acid residues in its bHLH-LZ domain engaged in Myc3/Max dimerization. Mutating these amino acid residues in the human c-Myc (MYC) sequence resulted in a significant decrease in its cell transformation potential. We discuss our findings in the context of oncogenic transformation and cell differentiation, both relevant for human cancer, where Myc represents a major driver.

Published

2023

8. KRAS: Biology, Inhibition, and Mechanisms of Inhibitor Resistance

Author

Leonard J. Ash, Ottavia Busia-Bourdain, Daniel Okpattah, Avrosina Kamel, Ariel Liberchuk, and Andrew L. Wolfe

Subjects

KRAS, cancer, immunotherapy, targeted therapy, resistance, oncogene, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

KRAS is a small GTPase that is among the most commonly mutated oncogenes in cancer. Here, we discuss KRAS biology, therapeutic avenues to target it, and mechanisms of resistance that tumors employ in response to KRAS inhibition. Several strategies are under investigation for inhibiting oncogenic KRAS, including small molecule compounds targeting specific KRAS mutations, pan-KRAS inhibitors, PROTACs, siRNAs, PNAs, and mutant KRAS-specific immunostimulatory strategies. A central challenge to therapeutic effectiveness is the frequent development of resistance to these treatments. Direct resistance mechanisms can involve KRAS mutations that reduce drug efficacy or copy number alterations that increase the expression of mutant KRAS. Indirect resistance mechanisms arise from mutations that can rescue mutant KRAS-dependent cells either by reactivating the same signaling or via alternative pathways. Further, non-mutational forms of resistance can take the form of epigenetic marks, transcriptional reprogramming, or alterations within the tumor microenvironment. As the possible strategies to inhibit KRAS expand, understanding the nuances of resistance mechanisms is paramount to the development of both enhanced therapeutics and innovative drug combinations.

Published

2024

9. An oncogene regulating chromatin favors response to immunotherapyOncogene CHAF1A and immunotherapy outcomes

Author

Leqian Ying, Zhangmin Hu, Yi Lu, Qing Tao, Fen Xiong, Yongqian Shu, Yufei Yang, Xuehan Qiao, Chen Peng, Yuchun Jiang, Miao Han, Min Xu, Xiaoqin Li, and Deqiang Wang

Subjects

Cancer, CHAF1A, immune checkpoint, immunotherapy, oncogene, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

ABSTRACTMany biological processes related to cell function and fate begin with chromatin alterations, and many factors associated with the efficacy of immune checkpoint inhibitors (ICIs) are actually downstream events of chromatin alterations, such as genome changes, neoantigen production, and immune checkpoint expression. However, the influence of genes as chromatin regulators on the efficacy of ICIs remains elusive, especially in gastric cancer (GC). In this study, thirty out of 1593 genes regulating chromatin associated with a favorable prognosis were selected for GC. CHAF1A, a well-defined oncogene, was identified as the highest linkage hub gene. High CHAF1A expression were associated with microsatellite instability (MSI), high tumor mutation burden (TMB), high tumor neoantigen burden (TNB), high expressions of PD-L1 and immune effector genes, and live infiltration of immune cells. High CHAF1A expression indicated a favorable response and prognosis in immunotherapy of several cohorts, which was independent of MSI, TMB, TNB, PD-L1 expression, immune phenotype and transcriptome scoring, and improved patient selection based on these classic biomarkers. In vivo, CHAF1A knockdown alone inhibited tumor growth but it impaired the effect of an anti-PD-1 antibody by increasing the relative tumor proliferation rate and decreasing the survival benefit, potentially through the activation of TGF-β signaling. In conclusion, CHAF1A may be a novel biomarker for improving patient selection in immunotherapy.

Published

2024

10. Integrated mutational landscape analysis of poorly differentiated high-grade neuroendocrine carcinoma of the uterine cervix.

Author

Bellonea, Stefania, Jeongb, Kyungjo, Hallec, Mari Kyllesø, Krakstad, Camilla, McNamara, Blair, Greenman, Michelle, Mutlu, Levent, Demirkiran, Cem, Hartwich, Tobias Max Philipp, Yang Yang-Hartwich, Zipponi, Margherita, Buza, Natalia, Pei Hui, Raspagliesi, Francesco, Lopez, Salvatore, Paolini, Biagio, Milione, Massimo, Perrone, Emanuele, Scambia, Giovanni, and Altwerger, Gary

Subjects

*NEUROENDOCRINE tumors, *CERVIX uteri, *EXCISION repair, *HUMAN papillomavirus, *GENE fusion, *GENETIC counseling

Abstract

High-grade neuroendocrine cervical cancers (NETc) are exceedingly rare, highly aggressive tumors. We analyzed 64 NETc tumor samples by whole-exome sequencing (WES). Human papillomavirus DNA was detected in 65.6% (42/64) of the tumors. Recurrent mutations were identified in PIK3CA, KMT2D/MLL2, K-RAS, ARID1A, NOTCH2, and RPL10. The top mutated genes included RB1, ARID1A, PTEN, KMT2D/MLL2, and WDFY3, a gene not yet implicated in NETc. Somatic CNV analysis identified two copy number gains (3q27.1 and 19q13.12) and five copy number losses (1p36.21/5q31.3/6p 22.2/9q21.11/11p15.5). Also, gene fusions affecting the ACLY-CRHR1 and PVT1-MYC genes were identified in one of the eight samples subjected to RNA sequencing. To resolve evolutionary history, multiregion WES in NETc admixed with adenocarcinoma cells was performed (i.e., mixed-NETc). Phylogenetic analysis of mixed-NETc demonstrated that adenocarcinoma and neuroendocrine elements derive from a common precursor with mutations typical of adenocarcinomas. Over one-third (22/64) of NETc demonstrated a mutator phenotype of C > T at CpG consistent with deficiencies in MBD4, a member of the base excision repair (BER) pathway. Mutations in the PI3K/AMPK pathways were identified in 49/64 samples. We used two patient-derived-xenografts (PDX) (i.e., NET19 and NET21) to evaluate the activity of pan-HER (afatinib), PIK3CA (copanlisib), and ATR (elimusertib) inhibitors, alone and in combination. PDXs harboring alterations in the ERBB2/PI3K/AKT/mTOR/ATR pathway were sensitive to afatinib, copanlisib, and elimusertib (P < 0.001 vs. controls). However, combinations of copanlisib/afatinib and copanlisib/elimusertib were significantly more effective in controlling NETc tumor growth. These findings define the genetic landscape of NETc and suggest that a large subset of these highly lethal malignancies might benefit from existing targeted therapies. [ABSTRACT FROM AUTHOR]

Published

2024

11. KRAS: Biology, Inhibition, and Mechanisms of Inhibitor Resistance.

Author

Ash, Leonard J., Busia-Bourdain, Ottavia, Okpattah, Daniel, Kamel, Avrosina, Liberchuk, Ariel, and Wolfe, Andrew L.

Subjects

*RAS oncogenes, *BIOLOGY, *SMALL molecules, *DRUG efficacy, *RESPONSE inhibition

Abstract

KRAS is a small GTPase that is among the most commonly mutated oncogenes in cancer. Here, we discuss KRAS biology, therapeutic avenues to target it, and mechanisms of resistance that tumors employ in response to KRAS inhibition. Several strategies are under investigation for inhibiting oncogenic KRAS, including small molecule compounds targeting specific KRAS mutations, pan-KRAS inhibitors, PROTACs, siRNAs, PNAs, and mutant KRAS-specific immunostimulatory strategies. A central challenge to therapeutic effectiveness is the frequent development of resistance to these treatments. Direct resistance mechanisms can involve KRAS mutations that reduce drug efficacy or copy number alterations that increase the expression of mutant KRAS. Indirect resistance mechanisms arise from mutations that can rescue mutant KRAS-dependent cells either by reactivating the same signaling or via alternative pathways. Further, non-mutational forms of resistance can take the form of epigenetic marks, transcriptional reprogramming, or alterations within the tumor microenvironment. As the possible strategies to inhibit KRAS expand, understanding the nuances of resistance mechanisms is paramount to the development of both enhanced therapeutics and innovative drug combinations. [ABSTRACT FROM AUTHOR]

Published

2024

12. The principles of neoplasia and oncology.

Author

Turnquist, Casmir, Taylor, Thomas RP, Al-Mossawi, Hussein, and Watson, Robert A

Abstract

Cancer is a result of a series of complex occurrences leading to uncontrolled cell growth, including overcoming the key regulators of the cell cycle, invasion of local tissue, establishment of a blood supply and potential spread to distant sites. A potential role for the cancer stem cell in the process of invasion and spread is becoming apparent. Additionally, the importance of some viruses and infections in causing certain cancers is now well understood with the potential for effective vaccine strategies targeting both these pathogens, as well as tumor epitopes. The interplay of cancer biology and the immune system is an area of particular recent interest. A role of innate immune cells such as monocytes in driving cancer processes is now appreciated, while the potential of T cells in cancer surveillance and cytolysis has led to significant advances in medical therapy. [ABSTRACT FROM AUTHOR]

Published

2024

13. A comprehensive review on the use of traditional Chinese medicine for cancer treatment

Author

Neha Yadav, Rohitas Deshmukh, and Rupa Mazumder

Subjects

Chinese medicine, Cancer, Metastasis, Microenvironment, Oncogene, Other systems of medicine, RZ201-999, Therapeutics. Pharmacology, RM1-950

Abstract

Introduction: Healthcare in China has historically relied on Traditional Chinese Medicine (TCM), which has had far-reaching effects on healthcare systems in neighboring nations. TCM has generated anticancer herbal medications. Cancer clinical trials have also examined herbal remedies. Methodology: Web of Science, Scopus, PubMed, and Google Scholar were among the online databases that were searched. Consequently, this review set out to compile a synopsis of the documented phytochemistry and pharmacological activities of the selected plant species. This literature review sought to illuminate TCMadjuvant cancer therapeutic role. New research reveals herbal medicines may inhibit cancer cell migration, adhesion, proliferation, and death. Results: This review aimed to summarise herbs and their TCM processes for chemoprevention and treatment. TCM treatments that target cancer stem cells and alter the tumor microenvironment have also been studied. This review will underpin traditional Chinese medicine cancer therapy research. Discussion: The bioactive chemicals in these herbs have been shown in clinical trials to have a wide range of cancer-fighting properties, with few side effects and a marked improvement in patient's quality of life. Conclusion: Given these benefits, it's clear that incorporating Chinese medicines into cancer care could be a significant step towards a more effective and comprehensive approach to treating the disease.

Published

2024

14. Systematic discovery and functional dissection of enhancers needed for cancer cell fitness and proliferation

Author

Chen, Poshen B, Fiaux, Patrick C, Zhang, Kai, Li, Bin, Kubo, Naoki, Jiang, Shan, Hu, Rong, Rooholfada, Emma, Wu, Sihan, Wang, Mengchi, Wang, Wei, McVicker, Graham, Mischel, Paul S, and Ren, Bing

Subjects

Biochemistry and Cell Biology, Bioinformatics and Computational Biology, Biological Sciences, Cancer, Genetics, Rare Diseases, Human Genome, 1.1 Normal biological development and functioning, Underpinning research, Humans, Enhancer Elements, Genetic, Chromatin, Genome, Human, Transcription Factors, Cell Proliferation, Neoplasms, CP: Cancer, CP: Molecular biology, cell proliferation, functional enhancer, gene regulation, oncogene, Medical Physiology, Biological sciences

Abstract

A scarcity of functionally validated enhancers in the human genome presents a significant hurdle to understanding how these cis-regulatory elements contribute to human diseases. We carry out highly multiplexed CRISPR-based perturbation and sequencing to identify enhancers required for cell proliferation and fitness in 10 human cancer cell lines. Our results suggest that the cell fitness enhancers, unlike their target genes, display high cell-type specificity of chromatin features. They typically adopt a modular structure, comprised of activating elements enriched for motifs of oncogenic transcription factors, surrounded by repressive elements enriched for motifs recognized by transcription factors with tumor suppressor functions. We further identify cell fitness enhancers that are selectively accessible in clinical tumor samples, and the levels of chromatin accessibility are associated with patient survival. These results reveal functional enhancers across multiple cancer cell lines, characterize their context-dependent chromatin organization, and yield insights into altered transcription programs in cancer cells.

Published

2022

15. Polyamines: their significance for maintaining health and contributing to diseases

Author

Mengjuan Xuan, Xinyu Gu, Juan Li, Di Huang, Chen Xue, and Yuting He

Subjects

Polyamine metabolism, Disease, Cancer, Oncogene, Mechanism, Medicine, Cytology, QH573-671

Abstract

Abstract Polyamines are essential for the growth and proliferation of mammalian cells and are intimately involved in biological mechanisms such as DNA replication, RNA transcription, protein synthesis, and post-translational modification. These mechanisms regulate cellular proliferation, differentiation, programmed cell death, and the formation of tumors. Several studies have confirmed the positive effect of polyamines on the maintenance of health, while others have demonstrated that their activity may promote the occurrence and progression of diseases. This review examines a variety of topics, such as polyamine source and metabolism, including metabolism, transport, and the potential impact of polyamines on health and disease. In addition, a brief summary of the effects of oncogenes and signaling pathways on tumor polyamine metabolism is provided. Video Abstract

Published

2023

16. Role of MARCH E3 ubiquitin ligases in cancer development

Author

Behera, Abhayananda, Sachan, Deepanshi, Barik, Ganesh Kumar, and Reddy, Aramati Bindu Madhava

Published

2024

17. NOTCH Signaling Pathway: Occurrence, Mechanism, and NOTCH-Directed Therapy for the Management of Cancer.

Author

Kumari, Lakshmi, Mishra, Lopamudra, Sharma, Yash, Chahar, Kanak, Kumar, Mritunjay, Patel, Preeti, Gupta, Ghanshyam Das, and Kurmi, Balak Das

Subjects

*SULFUR compounds, *ONCOGENES, *CELL receptors, *MONOCLONAL antibodies, *CURCUMIN, *CELLULAR signal transduction, *RESVERATROL, *GENISTEIN, *TUMOR suppressor genes, *TUMORS, *NANOMEDICINE, *ENZYME inhibitors, *PHARMACODYNAMICS, TUMOR genetics

Abstract

It is now well understood that many signaling pathways are vital in carrying out and controlling essential pro-survival and pro-growth cellular functions. The NOTCH signaling pathway, a highly conserved evolutionary signaling pathway, has been thoroughly studied since the discovery of NOTCH phenotypes about 100 years ago in Drosophila melanogaster. Abnormal NOTCH signaling has been linked to the pathophysiology of several diseases, notably cancer. In tumorigenesis, NOTCH plays the role of a "double-edged sword," that is, it may act as an oncogene or as a tumor suppressor gene depending on the nature of the context. However, its involvement in several cancers and inhibition of the same provides targeted therapy for the management of cancer. The use of gamma (γ)-secretase inhibitors and monoclonal antibodies for cancer treatment involved NOTCH receptors inhibition, leading to the possibility of a targeted approach for cancer treatment. Likewise, several natural compounds, including curcumin, resveratrol, diallyl sulfide, and genistein, also play a dynamic role in the management of cancer by inhibition of NOTCH receptors. This review outlines the functions and structure of NOTCH receptors and their associated ligands with the mechanism of the signaling pathway. In addition, it also emphasizes the role of NOTCH-targeted nanomedicine in various cancer treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2024

18. The Multifaceted Role of Human Dickkopf-3 (DKK-3) in Development, Immune Modulation and Cancer.

Author

Mourtada, Jana, Thibaudeau, Chloé, Wasylyk, Bohdan, and Jung, Alain C.

Subjects

*IMMUNOREGULATION, *TISSUE differentiation, *CELLULAR signal transduction, *ONCOGENES, *CELL differentiation, *GENE therapy, *WNT signal transduction

Abstract

The human Dickkopf (DKK) family includes four main secreted proteins, DKK-1, DKK-2, DKK-3, and DKK-4, as well as the DKK-3 related protein soggy (Sgy-1 or DKKL1). These glycoproteins play crucial roles in various biological processes, and especially modulation of the Wnt signaling pathway. DKK-3 is distinct, with its multifaceted roles in development, stem cell differentiation and tissue homeostasis. Intriguingly, DKK-3 appears to have immunomodulatory functions and a complex role in cancer, acting as either a tumor suppressor or an oncogene, depending on the context. DKK-3 is a promising diagnostic and therapeutic target that can be modulated by epigenetic reactivation, gene therapy and DKK-3-blocking agents. However, further research is needed to optimize DKK-3-based therapies. In this review, we comprehensively describe the known functions of DKK-3 and highlight the importance of context in understanding and exploiting its roles in health and disease. [ABSTRACT FROM AUTHOR]

Published

2024

19. Exploring antiproliferative activities and kinase profile of ortho‐substituted N‐(4‐(2‐(benzylamino)‐2‐oxoethyl)phenyl)benzamides.

Author

Muhammad, Yosra A., Omar, Abdelsattar M., Ahmed, Farid, Khayat, Maan T., Malebari, Azizah M., Ibrahim, Sara M., Mass, Shaza A., Elfaky, Mahmoud A., and El‐Araby, Moustafa E.

Subjects

*TUBULINS, *KINASE inhibitors, *KINASES, *CELL lines, *CANCER cells, *BINDING sites, *BENZAMIDE

Abstract

Designing kinase inhibitors that bind to the substrate site of oncogenic kinases in a promising, albeit less explored, approach to kinase inhibition as it was sought to avoid the issue of untoward off‐target modulations. Our previously identified compound KAC‐12 with a meta‐chlorophenyl substitution was an example of this approach. While it showed confirmed inhibitory activity against cancer cells, this substitution shifted the profile of affected targets away from Src/tubulin which were seen with the parent KX‐01. In this paper, we synthesized compounds with ortho‐substitutions, and we investigated the effect of such substitutions on their cellular and subcellular activities. The compound N‐(4‐(2‐(benzylamino)‐2‐oxoethyl)phenyl)‐2‐(morpholine‐4‐carbonyl)benzamide (4) exhibited substantial activities against cell lines such HCT116 (IC50 of 0.97 μM) and IC50 HL60 (2.84 μM). Kinase profiling showed that compound 4 trended consistently with KAC‐12 as it did not affect Src, but it had more impact on members of the Src family of kinases (SFK) such as Yes, Hck, Fyn, Lck, and Lyn. Both compounds exhibited profound downregulation effects on Erk1/2 but differed on others such as GSK3α/β and C‐Jun. Collectively, this study further support to the hypothesis that small structural changes might bring higher changes in their kinome profile. [ABSTRACT FROM AUTHOR]

Published

2024

20. Polyamines: their significance for maintaining health and contributing to diseases.

Author

Xuan, Mengjuan, Gu, Xinyu, Li, Juan, Huang, Di, Xue, Chen, and He, Yuting

Subjects

*POLYAMINES, *POST-translational modification, *DNA replication, *PROTEIN synthesis, *CELL proliferation, *DISEASE progression, *PROGRAMMED cell death 1 receptors

Abstract

Polyamines are essential for the growth and proliferation of mammalian cells and are intimately involved in biological mechanisms such as DNA replication, RNA transcription, protein synthesis, and post-translational modification. These mechanisms regulate cellular proliferation, differentiation, programmed cell death, and the formation of tumors. Several studies have confirmed the positive effect of polyamines on the maintenance of health, while others have demonstrated that their activity may promote the occurrence and progression of diseases. This review examines a variety of topics, such as polyamine source and metabolism, including metabolism, transport, and the potential impact of polyamines on health and disease. In addition, a brief summary of the effects of oncogenes and signaling pathways on tumor polyamine metabolism is provided. 5ikmGssBZD_e4xpSJscY2Y Video Abstract [ABSTRACT FROM AUTHOR]

Published

2023

21. Ca 2+ Signaling and Src Functions in Tumor Cells.

Author

Villalobo, Antonio

Subjects

*CALCIUM ions, *CALMODULIN, *CELL physiology, *PROTEIN-tyrosine kinases, *CELL communication, *KINASES

Abstract

Signaling by calcium ion (Ca2+) plays a prominent role in cell physiology, and these mechanisms are frequently altered in tumor cells. In this review, we consider the interplay of Ca2+ signaling and the functions of the proto-oncogene non-receptor tyrosine kinase c-Src in tumor cells, and the viral oncogenic variant v-Src in transformed cells. Also, other members of the Src-family kinases are considered in this context. The role of Ca2+ in the cell is frequently mediated by Ca2+-binding proteins, where the Ca2+-sensor protein calmodulin (CaM) plays a prominent, essential role in many cellular signaling pathways. Thus, we cover the available information on the role and direct interaction of CaM with c-Src and v-Src in cancerous cells, the phosphorylation of CaM by v-Src/c-Src, and the actions of different CaM-regulated Ser/Thr-protein kinases and the CaM-dependent phosphatase calcineurin on v-Src/c-Src. Finally, we mention some clinical implications of these systems to identify mechanisms that could be targeted for the therapeutic treatment of human cancers. [ABSTRACT FROM AUTHOR]

Published

2023

22. Sterol regulation of developmental and oncogenic Hedgehog signaling

Author

Daggubati, Vikas, Raleigh, David R, and Sever, Navdar

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, Brain Cancer, Rare Diseases, Cancer, Brain Disorders, Underpinning research, 1.1 Normal biological development and functioning, Animals, Carcinogenesis, Hedgehog Proteins, Humans, Oncogene Proteins, Signal Transduction, Smoothened Receptor, Sterols, Medulloblastoma, Basal cell carcinoma, Sonic hedgehog, Sterol-sensing domain, Oncogene, Pharmacology and Pharmaceutical Sciences, Pharmacology & Pharmacy, Biochemistry and cell biology, Pharmacology and pharmaceutical sciences

Abstract

The Hedgehog (Hh) family of lipid-modified signaling proteins directs embryonic tissue patterning and postembryonic tissue homeostasis, and dysregulated Hh signaling drives familial and sporadic cancers. Hh ligands bind to and inhibit the tumor suppressor Patched and allow the oncoprotein Smoothened (SMO) to accumulate in cilia, which in turn activates the GLI family of transcription factors. Recent work has demonstrated that endogenous cholesterol and oxidized cholesterol derivatives (oxysterols) bind and modulate SMO activity. Here we discuss the myriad sterols that activate or inhibit the Hh pathway, with emphasis on endogenous 24(S),25-epoxycholesterol and 3β,5α-dihydroxycholest-7-en-6-one, and propose models of sterol regulation of SMO. Synthetic inhibitors of SMO have long been the focus of drug development efforts. Here, we discuss the possible utility of steroidal SMO ligands or inhibitors of enzymes involved in sterol metabolism as cancer therapeutics.

Published

2022

23. Inflammation and Cancer: Role of Tight Junctions

Author

Pravoverov, Kristina, Barman, Susmita, Gowrikumar, Saiprasad, Fatima, Iram, Yadav, Santosh Kumar, Otte, Megan Lynn, Tamang, Raju Lama, Primeaux, Mark, Singh, Amar Bahadur, Dhawan, Punita, Bhat, Ajaz A., editor, Haris, Mohammad, editor, Macha, Muzafar A., editor, and Dhawan, Punita, editor

Published

2023

24. DEAD-box RNA helicases with special reference to p68: Unwinding their biology, versatility, and therapeutic opportunity in cancer

Author

Shaheda Tabassum and Mrinal K. Ghosh

Subjects

Cancer, DDX5, DEAD-box RNA helicases, Gene expression, Oncogene, Signaling, Medicine (General), R5-920, Genetics, QH426-470

Abstract

In the era of advancement, the entire world continues to remain baffled by the increased rate of progression of cancer. There has been an unending search for novel therapeutic targets and prognostic markers to curb the oncogenic scenario. The DEAD-box RNA helicases are a large family of proteins characterized by their evolutionary conserved D-E-A-D (Asp-Glu-Ala-Asp) domain and merit consideration in the oncogenic platform. They perform multidimensional functions in RNA metabolism and also in the pathology of cancers. Their biological role ranges from ribosome biogenesis, RNA unwinding, splicing, modification of secondary and tertiary RNA structures to acting as transcriptional coactivators/repressors of various important oncogenic genes. They also play a crucial role in accelerating oncogenesis by promoting cell proliferation and metastasis. DDX5 (p68) is one of the archetypal members of this family of proteins and has gained a lot of attention due to its oncogenic attribute. It is found to be overexpressed in major cancer types such as colon, brain, breast, and prostate cancer. It exhibits its multifaceted nature by not only coactivating genes implicated in cancers but also mediating crosstalk across major signaling pathways in cancer. Therefore, in this review, we aim to illustrate a comprehensive overview of DEAD-box RNA helicases especially p68 by focusing on their multifaceted roles in different cancers and the various signaling pathways affected by them. Further, we have also briefly discoursed the therapeutic interventional approaches with the DEAD-box RNA helicases as the pharmacological targets for designing inhibitors to pave way for cancer therapy.

Published

2023

25. Plant homeodomain-finger protein 5A: A key player in cancer progression

Author

Patrick Diaba-Nuhoho

Subjects

Zinc finger, PHF5A, Oncogene, RNA binding, Cancer, Therapeutics. Pharmacology, RM1-950

Abstract

PHF5A is a member of the zinc-finger proteins. To advance knowledge on their role in carcinogenesis, data from experimental studies, animal models and clinical studies in different tumorigenesis have been reviewed. Furthermore, PHF5A as an oncogenic function, is frequently high expressed in tumor cells and a potential prognostic marker for different cancers. PHF5A is implicated in the regulation of cancer cell proliferation, invasion, migration and metastasis. Knockdown of PHF5A prevented the invasion and metastasis of tumor cells. Here, the role of PHF5A in different cancers and their possible mechanism in relation to recent literature is reviewed and discussed. There is an open promising perspective to their therapeutic management for different cancer types.

Published

2023

26. From cultivation to cancer: formation of N-nitrosamines and other carcinogens in smokeless tobacco and their mutagenic implications.

Author

Stanfill, Stephen B., Hecht, Stephen S., Joerger, Andreas C., González, Pablo J., Maia, Luisa B., Rivas, Maria G., Moura, José J. G., Gupta, Alpana K., Le Brun, Nick E., Crack, Jason C., Hainaut, Pierre, Sparacino-Watkins, Courtney, Tyx, Robert E., Pillai, Suresh D., Zaatari, Ghazi S., Henley, S. Jane, Blount, Benjamin C., Watson, Clifford H., Kaina, Bernd, and Mehrotra, Ravi

Subjects

*DNA adducts, *SMOKELESS tobacco, *P53 antioncogene, *RAS oncogenes, *TOBACCO products, *CARCINOGENS

Abstract

Tobacco use is a major cause of preventable morbidity and mortality globally. Tobacco products, including smokeless tobacco (ST), generally contain tobacco-specific N-nitrosamines (TSNAs), such as N′-nitrosonornicotine (NNN) and 4-(methylnitrosamino)-1-(3-pyridyl)-butanone (NNK), which are potent carcinogens that cause mutations in critical genes in human DNA. This review covers the series of biochemical and chemical transformations, related to TSNAs, leading from tobacco cultivation to cancer initiation. A key aim of this review is to provide a greater understanding of TSNAs: their precursors, the microbial and chemical mechanisms that contribute to their formation in ST, their mutagenicity leading to cancer due to ST use, and potential means of lowering TSNA levels in tobacco products. TSNAs are not present in harvested tobacco but can form due to nitrosating agents reacting with tobacco alkaloids present in tobacco during certain types of curing. TSNAs can also form during or following ST production when certain microorganisms perform nitrate metabolism, with dissimilatory nitrate reductases converting nitrate to nitrite that is then released into tobacco and reacts chemically with tobacco alkaloids. When ST usage occurs, TSNAs are absorbed and metabolized to reactive compounds that form DNA adducts leading to mutations in critical target genes, including the RAS oncogenes and the p53 tumor suppressor gene. DNA repair mechanisms remove most adducts induced by carcinogens, thus preventing many but not all mutations. Lastly, because TSNAs and other agents cause cancer, previously documented strategies for lowering their levels in ST products are discussed, including using tobacco with lower nornicotine levels, pasteurization and other means of eliminating microorganisms, omitting fermentation and fire-curing, refrigerating ST products, and including nitrite scavenging chemicals as ST ingredients. [ABSTRACT FROM AUTHOR]

Published

2023

27. Tissue-Specific Tumour Suppressor and Oncogenic Activities of the Polycomb-like Protein MTF2.

Author

Ngubo, Mzwanele, Moradi, Fereshteh, Ito, Caryn Y., and Stanford, William L.

Subjects

*EMBRYONIC stem cells, *EPIGENOMICS, *TRANSCRIPTION factors, *GENE silencing, *PROTEINS, *GENE expression

Abstract

The Polycomb repressive complex 2 (PRC2) is a conserved chromatin-remodelling complex that catalyses the trimethylation of histone H3 lysine 27 (H3K27me3), a mark associated with gene silencing. PRC2 regulates chromatin structure and gene expression during organismal and tissue development and tissue homeostasis in the adult. PRC2 core subunits are associated with various accessory proteins that modulate its function and recruitment to target genes. The multimeric composition of accessory proteins results in two distinct variant complexes of PRC2, PRC2.1 and PRC2.2. Metal response element-binding transcription factor 2 (MTF2) is one of the Polycomb-like proteins (PCLs) that forms the PRC2.1 complex. MTF2 is highly conserved, and as an accessory subunit of PRC2, it has important roles in embryonic stem cell self-renewal and differentiation, development, and cancer progression. Here, we review the impact of MTF2 in PRC2 complex assembly, catalytic activity, and spatiotemporal function. The emerging paradoxical evidence suggesting that MTF2 has divergent roles as either a tumour suppressor or an oncogene in different tissues merits further investigations. Altogether, our review illuminates the context-dependent roles of MTF2 in Polycomb group (PcG) protein-mediated epigenetic regulation. Its impact on disease paves the way for a deeper understanding of epigenetic regulation and novel therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2023

28. The mechanistic insights of the antioxidant Keap1-Nrf2 pathway in oncogenesis: a deadly scenario.

Author

Mukherjee, Anirban Goutam and Gopalakrishnan, Abilash Valsala

Abstract

The Nuclear factor erythroid 2-related factor 2 (Nrf2) protein has garnered significant interest due to its crucial function in safeguarding cells and tissues. The Nrf2 protein is crucial in preserving tissue integrity by safeguarding cells against metabolic, xenobiotic and oxidative stress. Due to its various functions, Nrf2 is a potential pharmacological target for reducing the incidence of diseases such as cancer. However, mutations in Keap1-Nrf2 are not consistently favored in all types of cancer. Instead, they seem to interact with specific driver mutations of tumors and their respective tissue origins. The Kelch-like ECH-associated protein 1 (Keap1)-Nrf2 pathway mutations are a powerful cancer adaptation that utilizes inherent cytoprotective pathways, encompassing nutrient metabolism and ROS regulation. The augmentation of Nrf2 activity elicits significant alterations in the characteristics of neoplastic cells, such as resistance to radiotherapy and chemotherapy, safeguarding against apoptosis, heightened invasiveness, hindered senescence, impaired autophagy and increased angiogenesis. The altered activity of Nrf2 can arise from diverse genetic and epigenetic modifications that instantly impact Nrf2 regulation. The present study aims to showcase the correlation between the Keap1-Nrf2 pathway and the progression of cancers, emphasizing genetic mutations, metabolic processes, immune regulation, and potential therapeutic strategies. This article delves into the intricacies of Nrf2 pathway anomalies in cancer, the potential ramifications of uncontrolled Nrf2 activity, and therapeutic interventions to modulate the Keap1-Nrf2 pathway. [ABSTRACT FROM AUTHOR]

Published

2023

29. Functions, mechanisms, and clinical applications of lncRNA LINC00857 in cancer pathogenesis.

Author

Aldayyeni, Hussein, Hjazi, Ahmed, Shahab, Sana, Gupta, Jitendra, Alsaab, Hashem O., Motea, Yaseen Hasan, alazbjee, Adeeb Abdulally Abdulhussien, Romero-Parra, Rosario Mireya, Obaid, Rasha Fadhel, Hussien, Beneen M., and Hosseini-Fard, Seyed Reza

Subjects

CARCINOGENESIS, CLINICAL medicine, LINCRNA, EPITHELIAL-mesenchymal transition, MEDICAL research

Abstract

Emerging data indicated that long noncoding RNAs (lncRNAs) are crucial players in the biological processes via regulating epigenetics, transcription, and protein translation. A novel lncRNA, LINC00857, was indicated to upregulate in several types of cancer. In addition, LINC00857 was functionally related to the modulation of the cancer-linked behaviors, including invasion, migration, proliferation, epithelial–mesenchymal transition (EMT), cell cycle, and apoptosis. The importance of LINC00857 in cancer onset and development proposed that LINC00857 has major importance in the cancer progression and may be considered as a novel prognostic/diagnostic biomarker as well as a treatment target. Here, we retrospectively investigate the available progress in biomedical research investigating the functions of LINC00857 in cancer, focusing on finding the molecular mechanisms affecting various cancer-related behaviors and exploring its clinical applications. [ABSTRACT FROM AUTHOR]

Published

2023

30. Non-canonical functions of EZH2 in cancer.

Author

Zimmerman, Sarah M., Lin, Phyo Nay, and Souroullas, George P.

Subjects

GENE expression, TRANSCRIPTION factors, CHROMATIN, EPIGENETICS, ONCOGENES

Abstract

Mutations in chromatin modifying genes frequently occur in many kinds of cancer. Most mechanistic studies focus on their canonical functions, while therapeutic approaches target their enzymatic activity. Recent studies, however, demonstrate that non-canonical functions of chromatin modifiers may be equally important and therapeutically actionable in different types of cancer. One epigenetic regulator that demonstrates such a dual role in cancer is the histone methyltransferase EZH2. EZH2 is a core component of the polycomb repressive complex 2 (PRC2), which plays a crucial role in cell identity, differentiation, proliferation, stemness and plasticity. While much of the regulatory functions and oncogenic activity of EZH2 have been attributed to its canonical, enzymatic activity of methylating lysine 27 on histone 3 (H3K27me3), a repressive chromatin mark, recent studies suggest that non-canonical functions that are independent of H3K27me3 also contribute towards the oncogenic activity of EZH2. Contrary to PRC2's canonical repressive activity, mediated by H3K27me3, outside of the complex EZH2 can directly interact with transcription factors and oncogenes to activate gene expression. A more focused investigation into these non-canonical interactions of EZH2 and other epigenetic/chromatin regulators may uncover new and more effective therapeutic strategies. Here, we summarize major findings on the noncanonical functions of EZH2 and how they are related to different aspects of carcinogenesis. [ABSTRACT FROM AUTHOR]

Published

2023

31. Whole-genome characterization of lung adenocarcinomas lacking the RTK/RAS/RAF pathway

Author

Carrot-Zhang, Jian, Yao, Xiaotong, Devarakonda, Siddhartha, Deshpande, Aditya, Damrauer, Jeffrey S, Silva, Tiago Chedraoui, Wong, Christopher K, Choi, Hyo Young, Felau, Ina, Robertson, A Gordon, Castro, Mauro AA, Bao, Lisui, Rheinbay, Esther, Liu, Eric Minwei, Trieu, Tuan, Haan, David, Yau, Christina, Hinoue, Toshinori, Liu, Yuexin, Shapira, Ofer, Kumar, Kiran, Mungall, Karen L, Zhang, Hailei, Lee, Jake June-Koo, Berger, Ashton, Gao, Galen F, Zhitomirsky, Binyamin, Liang, Wen-Wei, Zhou, Meng, Moorthi, Sitapriya, Berger, Alice H, Collisson, Eric A, Zody, Michael C, Ding, Li, Cherniack, Andrew D, Getz, Gad, Elemento, Olivier, Benz, Christopher C, Stuart, Josh, Zenklusen, JC, Beroukhim, Rameen, Chang, Jason C, Campbell, Joshua D, Hayes, D Neil, Yang, Lixing, Laird, Peter W, Weinstein, John N, Kwiatkowski, David J, Tsao, Ming S, Travis, William D, Khurana, Ekta, Berman, Benjamin P, Hoadley, Katherine A, Robine, Nicolas, Network, TCGA Research, Arora, Kanika, Shah, Minita, Shelton, Jennifer, Bowlby, Reanne, Friedl, Verena, Goldman, Mary, Craft, Brian, Heiman, David I, Hajirasouliha, Iman, Ricketts, Camir, Anur, Pavana, Chiotti, Kami E, Caesar-Johnson, Samantha J, Demchok, John A, Ferguson, Martin L, Kemal, Anab, Tarnuzzer, Roy, Wang, Zhining, Yang, Liming, Spellman, Paul T, Raphael, Benjamin, Akbani, Rehan, Zhu, Jingchun, Jones, Steven JM, Shen, Hui, Meyerson, Matthew, Govindan, Ramaswamy, and Imielinski, Marcin

Subjects

Biological Sciences, Cancer Genomics, Human Genome, Rare Diseases, Lung, Lung Cancer, Cancer, Genetics, Biotechnology, 2.1 Biological and endogenous factors, Good Health and Well Being, Adenocarcinoma of Lung, Humans, Kelch-Like ECH-Associated Protein 1, Lung Neoplasms, Tachykinins, Whole Genome Sequencing, TCGA Research Network, TCGA, driver, genome analysis, lung adenocarcinoma, noncoding, oncogene, precision oncology, structural variation, tumor suppressor, whole genome sequencing, Biochemistry and Cell Biology, Medical Physiology, Biological sciences

Abstract

RTK/RAS/RAF pathway alterations (RPAs) are a hallmark of lung adenocarcinoma (LUAD). In this study, we use whole-genome sequencing (WGS) of 85 cases found to be RPA(-) by previous studies from The Cancer Genome Atlas (TCGA) to characterize the minority of LUADs lacking apparent alterations in this pathway. We show that WGS analysis uncovers RPA(+) in 28 (33%) of the 85 samples. Among the remaining 57 cases, we observe focal deletions targeting the promoter or transcription start site of STK11 (n = 7) or KEAP1 (n = 3), and promoter mutations associated with the increased expression of ILF2 (n = 6). We also identify complex structural variations associated with high-level copy number amplifications. Moreover, an enrichment of focal deletions is found in TP53 mutant cases. Our results indicate that RPA(-) cases demonstrate tumor suppressor deletions and genome instability, but lack unique or recurrent genetic lesions compensating for the lack of RPAs. Larger WGS studies of RPA(-) cases are required to understand this important LUAD subset.

Published

2021

32. Dysregulation of hsa-miR-34a and hsa-miR-449a leads to overexpression of PACS-1 and loss of DNA damage response (DDR) in cervical cancer

Author

Veena, Mysore S, Raychaudhuri, Santanu, Basak, Saroj K, Venkatesan, Natarajan, Kumar, Parameet, Biswas, Roopa, Chakrabarti, Rita, Lu, Jing, Su, Trent, Gallagher-Jones, Marcus, Morselli, Marco, Fu, Haiqing, Pellegrini, Matteo, Goldstein, Theodore, Aladjem, Mirit I, Rettig, Matthew B, Wilczynski, Sharon P, Shin, Daniel Sanghoon, and Srivatsan, Eri S

Subjects

Biotechnology, Genetics, Cancer, Aetiology, 2.1 Biological and endogenous factors, DNA Damage, Drug Resistance, Neoplasm, Female, G1 Phase, HeLa Cells, Humans, MicroRNAs, RNA, Neoplasm, S Phase Cell Cycle Checkpoints, Tumor Suppressor Protein p53, Uterine Cervical Neoplasms, Vesicular Transport Proteins, PACS-1, cervical cancer, hsa-miRNA-34a, hsa-miR-449a, DNA damage response, p53 acetylation, nuclear translocation, genome stability, cancer biology, oncogene, tumor, tumor suppressor gene, nuclear transport, trafficking protein, Hela Cells, Chemical Sciences, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology

Abstract

We have observed overexpression of PACS-1, a cytosolic sorting protein in primary cervical tumors. Absence of exonic mutations and overexpression at the RNA level suggested a transcriptional and/or posttranscriptional regulation. University of California Santa Cruz genome browser analysis of PACS-1 micro RNAs (miR), revealed two 8-base target sequences at the 3' terminus for hsa-miR-34a and hsa-miR-449a. Quantitative RT-PCR and Northern blotting studies showed reduced or loss of expression of the two microRNAs in cervical cancer cell lines and primary tumors, indicating dysregulation of these two microRNAs in cervical cancer. Loss of PACS-1 with siRNA or exogenous expression of hsa-miR-34a or hsa-miR-449a in HeLa and SiHa cervical cancer cell lines resulted in DNA damage response, S-phase cell cycle arrest, and reduction in cell growth. Furthermore, the siRNA studies showed that loss of PACS-1 expression was accompanied by increased nuclear γH2AX expression, Lys382-p53 acetylation, and genomic instability. PACS-1 re-expression through LNA-hsa-anti-miR-34a or -449a or through PACS-1 cDNA transfection led to the reversal of DNA damage response and restoration of cell growth. Release of cells post 24-h serum starvation showed PACS-1 nuclear localization at G1-S phase of the cell cycle. Our results therefore indicate that the loss of hsa-miR-34a and hsa-miR-449a expression in cervical cancer leads to overexpression of PACS-1 and suppression of DNA damage response, resulting in the development of chemo-resistant tumors.

Published

2020

33. MYCT1 in cancer development: Gene structure, regulation, and biological implications for diagnosis and treatment

Author

Jianan Xu, Yuanyuan Sun, Weineng Fu, and Shuang Fu

Subjects

MYCT1, Cancer, C-Myc, Oncogene, Tumor suppressor gene, Therapeutics. Pharmacology, RM1-950

Abstract

Myc target 1 (MYCT1), located at 6q25.2, is a crucial player in cancer development. While widely distributed in cells, its subcellular localization varies across different cancer types. As a novel c-Myc target gene, MYCT1 is subject to regulation by multiple transcription factors. Studies have revealed aberrant expression of MYCT1 in various cancers, impacting pivotal biological processes such as proliferation, apoptosis, migration, genomic instability, and differentiation in cancer cells. Additionally, MYCT1 plays a critical role in modulating tumor angiogenesis and remodeling tumor immune responses within the tumor microenvironment. Despite certain debated functions, MYCT1 undeniably holds significance in cancer development. In this review, we comprehensively examine the relationship between MYCT1 and cancer, encompassing gene structure, regulation of gene expression, gene mutation, and biological function, with the aim of providing valuable insights for cancer diagnosis and treatment.

Published

2023

34. Horizontal Transfer of Malignant Traits and the Involvement of Extracellular Vesicles in Metastasis.

Author

Arena, Goffredo O., Forte, Stefano, Abdouh, Mohamed, Vanier, Cheryl, Corbeil, Denis, and Lorico, Aurelio

Subjects

*EXTRACELLULAR vesicles, *CELL transformation, *METASTASIS, *CELL nuclei, *TUMOR suppressor genes, *LARVAL dispersal

Abstract

Metastases are responsible for the vast majority of cancer deaths, yet most therapeutic efforts have focused on targeting and interrupting tumor growth rather than impairing the metastatic process. Traditionally, cancer metastasis is attributed to the dissemination of neoplastic cells from the primary tumor to distant organs through blood and lymphatic circulation. A thorough understanding of the metastatic process is essential to develop new therapeutic strategies that improve cancer survival. Since Paget's original description of the "Seed and Soil" hypothesis over a hundred years ago, alternative theories and new players have been proposed. In particular, the role of extracellular vesicles (EVs) released by cancer cells and their uptake by neighboring cells or at distinct anatomical sites has been explored. Here, we will outline and discuss these alternative theories and emphasize the horizontal transfer of EV-associated biomolecules as a possibly major event leading to cell transformation and the induction of metastases. We will also highlight the recently discovered intracellular pathway used by EVs to deliver their cargoes into the nucleus of recipient cells, which is a potential target for novel anti-metastatic strategies. [ABSTRACT FROM AUTHOR]

Published

2023

35. Deep learning facilitates multi-data type analysis and predictive biomarker discovery in cancer precision medicine

Author

Vivek Bhakta Mathema, Partho Sen, Santosh Lamichhane, Matej Orešič, and Sakda Khoomrung

Subjects

Cancer, Deep learning, Reinforcement learning, Precision medicine, Oncogene, Systems medicine, Biotechnology, TP248.13-248.65

Abstract

Cancer progression is linked to gene-environment interactions that alter cellular homeostasis. The use of biomarkers as early indicators of disease manifestation and progression can substantially improve diagnosis and treatment. Large omics datasets generated by high-throughput profiling technologies, such as microarrays, RNA sequencing, whole-genome shotgun sequencing, nuclear magnetic resonance, and mass spectrometry, have enabled data-driven biomarker discoveries. The identification of differentially expressed traits as molecular markers has traditionally relied on statistical techniques that are often limited to linear parametric modeling. The heterogeneity, epigenetic changes, and high degree of polymorphism observed in oncogenes demand biomarker-assisted personalized medication schemes. Deep learning (DL), a major subunit of machine learning (ML), has been increasingly utilized in recent years to investigate various diseases. The combination of ML/DL approaches for performance optimization across multi-omics datasets produces robust ensemble-learning prediction models, which are becoming useful in precision medicine. This review focuses on the recent development of ML/DL methods to provide integrative solutions in discovering cancer-related biomarkers, and their utilization in precision medicine.

Published

2023

36. Harnessing the MYB-dependent TAL1 5’super-enhancer for targeted therapy in T-ALL

Author

Charlotte Smith, Aurore Touzart, Mathieu Simonin, Christine Tran-Quang, Guillaume Hypolite, Mehdi Latiri, Guillaume P. Andrieu, Estelle Balducci, Marie-Émilie Dourthe, Ashish Goyal, Françoise Huguet, Arnaud Petit, Norbert Ifrah, André Baruchel, Hervé Dombret, Elizabeth Macintyre, Christoph Plass, Jacques Ghysdael, Nicolas Boissel, and Vahid Asnafi

Subjects

Super-enhancer, Oncogene, Targeted therapy, Cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract The acquisition of genetic abnormalities engendering oncogene dysregulation underpins cancer development. Certain proto-oncogenes possess several dysregulation mechanisms, yet how each mechanism impacts clinical outcome is unclear. Using T-cell acute lymphoblastic leukemia (T-ALL) as an example, we show that patients harboring 5’super-enhancer (5’SE) mutations of the TAL1 oncogene identifies a specific patient subgroup with poor prognosis irrespective of the level of oncogene dysregulation. Remarkably, the MYB dependent oncogenic 5’SE can be targeted using Mebendazole to induce MYB protein degradation and T-ALL cell death. Of note Mebendazole treatment demonstrated efficacy in vivo in T-ALL preclinical models. Our work provides proof of concept that within a specific oncogene driven cancer, the mechanism of oncogene dysregulation rather than the oncogene itself can identify clinically distinct patient subgroups and pave the way for future super-enhancer targeting therapy.

Published

2023

37. Residual Neural Network for Predicting Super-Enhancers on Genome Scale

Author

Sabba, Sara, Smara, Meroua, Benhacine, Mehdi, Hameurlaine, Amina, Kacprzyk, Janusz, Series Editor, Gomide, Fernando, Advisory Editor, Kaynak, Okyay, Advisory Editor, Liu, Derong, Advisory Editor, Pedrycz, Witold, Advisory Editor, Polycarpou, Marios M., Advisory Editor, Rudas, Imre J., Advisory Editor, Wang, Jun, Advisory Editor, Lejdel, Brahim, editor, Clementini, Eliseo, editor, and Alarabi, Louai, editor

Published

2022

38. lncRNA PVT1: a novel oncogene in multiple cancers

Author

Ruiming Li, Xia Wang, Chunming Zhu, and Kefeng Wang

Subjects

Long noncoding RNA, PVT1, Oncogene, Cancer, Cytology, QH573-671

Abstract

Abstract Long noncoding RNAs are involved in epigenetic gene modification, including binding to the chromatin rearrangement complex in pre-transcriptional regulation and to gene promoters in gene expression regulation, as well as acting as microRNA sponges to control messenger RNA levels in post-transcriptional regulation. An increasing number of studies have found that long noncoding RNA plasmacytoma variant translocation 1 (PVT1) plays an important role in cancer development. In this review of a large number of studies on PVT1, we found that PVT1 is closely related to tumor onset, proliferation, invasion, epithelial–mesenchymal transformation, and apoptosis, as well as poor prognosis and radiotherapy and chemotherapy resistance in some cancers. This review comprehensively describes PVT1 expression in various cancers and presents novel approaches to the diagnosis and treatment of cancer.

Published

2022

39. Molecular mechanisms of inhibitor of growth (ING) family members in health and malignancy

Author

Mohammad Taheri, Bashdar Mahmud Hussen, Sajad Najafi, Atefe Abak, Soudeh Ghafouri-Fard, Majid Samsami, and Aria Baniahmad

Subjects

ING, Tumor suppressor gene, Cancer, Oncogene, Cellular senescence, Splice variants, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract ING genes belong to family of tumor suppressor genes with regulatory functions on cell proliferation, apoptosis, and cellular senescence. These include a family of proteins with 5 members (ING1-5), which are downregulated in human malignancies and/or affected by pathogenic mutations. ING proteins are highly evolutionarily conserved proteins containing several domains through which bind to chromatin structures by exerting their effects as readers of histone modification marks, and also binding to proteins like p53 involved in biological processes such as cell cycle regulation. Further, they are known as subunits of histone acetylation as well as deacetylation complexes and so exert their regulatory roles through epigenetic mechanisms. Playing role in restriction of proliferative but also invasive potentials of normal cells, INGs are particularly involved in cancer development and progression. However, additional studies and experimental confirmation are required for these models. This paper highlights the potential impact that INGs may have on the development of human cancer and explores what new information has recently arise on the functions of ING genes.

Published

2022

40. Predictive reporter system for investigating dose dependency in oncogene-induced senescence

Author

Chan, Sue Li Adelyne and Narita, Masashi

Subjects

616.99, senescence, cancer, oncogene

Abstract

Oncogene-induced senescence (OIS) is a well-described autonomous tumour suppressor mechanism which removes cells harbouring oncogenic mutations from the proliferation pool. However, senescent cells remain metabolically active and express factors of the senescence-associated secretory phenotype (SASP), which can conversely have a pro-tumorigenic impact on the cellular microenvironment. Yet, aberrant oncogene activation alone is insufficient for triggering OIS, as studies both in vitro and in vivo have demonstrated that low-dose oncogene cells continue proliferating, in some cases proceeding to full malignancy. The molecular mechanisms governing this dose-dependent switch remain unclear. To address this question, we developed a cell system where a constitutively active fluorescence marker (mVenus) stoichiometrically reflects the level of inducible oncogenic HRASG12V. This allows pre-induction sorting into subpopulations expressing differing levels of mVenus, which is reflected in differences in HRAS dose following induction. Using this system, we first validated that subpopulations expressing different levels of RAS are distinct in their proliferative / senescence phenotypes, implying a theoretical, cell-autonomous ‘oncogenic tipping point’ above which cells enter into OIS. We then demonstrate the potential utility of our proposed ‘predictive reporter’ system in addressing gene dose-related biological questions. RNA sequencing of sorted subpopulations demonstrates the effect of RAS dose on gene expression, where between-subpopulation differences suggests that this sorting strategy may serve as a viable intermediate between bulk and single-cell sequencing technologies. These global dose-dependent differences were validated using single-cell RNA sequencing, which also demonstrated transcriptomic heterogeneity that exists independently of RAS dose. Finally, we demonstrate that the reconstruction of subpopulations into a mixed population with cells of varying RAS doses can have implications on phenotype, and that the current system is a flexible tool that facilitates these sorts of ‘cellular ecosystem’ type experiments in vitro.

Published

2019

41. Retinoic acid metabolism in cancer: potential feasibility of retinoic acid metabolism blocking therapy.

Author

Osanai, Makoto, Takasawa, Akira, Takasawa, Kumi, Kyuno, Daisuke, Ono, Yusuke, and Magara, Kazufumi

Subjects

*TRETINOIN, *VITAMIN A, *CYTOCHROME P-450, *METABOLISM, *CELL survival, *ONCOGENES

Abstract

Retinoic acid (RA) is an active metabolite of vitamin A, which is an essential signaling molecule involved in cell fate decisions, such as differentiation, proliferation, and apoptosis, in a wide variety of cell types. Accumulated data have demonstrated that expression of RA-metabolizing enzymes, CYP26A1, B1, and C1 (cytochrome P450, family 26A1, B1, and C1, respectively), protects cells and tissues from exposure to RA through restriction of RA access to transcriptional machinery by converting RA to rapidly excreted derivatives. CYP26 enzymes play similar but separate roles in limiting the consequences of fluctuations in nutritional vitamin A. Recently, we found that RA depletion caused by expression of CYP26A1 promotes malignant behaviors of tumor cells derived from various tissues, implicating CYP26A1 as a candidate oncogene. We also showed that the expression levels of CYP26 enzymes are elevated in various types of cancer. We have provided evidence for oncogenic and cell survival properties of CYP26 enzymes, indicating that these molecules are possible therapeutic targets for CYP26-expressing malignancies. [ABSTRACT FROM AUTHOR]

Published

2023

42. PTEN regulates proliferation and osteogenesis of dental pulp cells and adipogenesis of human adipose‑derived stem cells.

Author

Nowwarote, Nunthawan, Osathanon, Thanaphum, Fournier, Benjamin P.J., Theerapanon, Thanakorn, Yodsanga, Somchai, Kamolratanakul, Paksinee, Porntaveetus, Thantrira, and Shotelersuk, Vorasuk

Subjects

*COWDEN syndrome, *BONE growth, *GENETIC mutation, *CELL physiology, *PHOSPHATASES, *GENETIC variation, *DENTAL pulp, *GENE expression, *CELL proliferation, *RESEARCH funding, *MESENCHYMAL stem cells, *LIPOMA

Abstract

Objective: To investigate the role of phosphatase and tensin homolog (PTEN) in dental pulp cells (hDPs) and adipose‐derived mesenchymal stem cells (hADSCs). Materials and Methods: Genetic variant was identified with exome sequencing. The hDPs isolated from a patient with Cowden syndrome were investigated for their proliferation, osteogenesis, adipogenesis, and gene expression compared with controls. The normal hDPs and hADSCs were treated with the PTEN inhibitor, VO‐OHpic trihydrate (VOT), to investigate the effect of PTEN inhibition. Results: A heterozygous nonsense PTEN variant, c.289C>T (p.Gln97*), was identified in the Cowden patient's blood and intraoral lipomas. The mutated hDPs showed significantly decreased proliferation, but significantly upregulated RUNX2 and OSX expression and mineralization, indicating enhanced osteogenic ability in mutated cells. The normal hDPs treated with VOT showed the decreases in proliferation, colony formation, osteogenic marker genes, alkaline phosphatase activity, and mineral deposition, suggesting that PTEN inhibition diminishes proliferation and osteogenic potential of hDPs. Regarding adipogenesis, the VOT‐treated hADSCs showed a reduced number of cells containing lipid droplets, suggesting that PTEN inhibition might compromise adipogenic ability of hADSCs. Conclusions: PTEN regulates proliferation, enhances osteogenesis of hDPs, and induces adipogenesis of hADSCs. The gain‐of‐function PTEN variant, p.Gln97*, enhances osteogenic ability of PTEN in hDPs. [ABSTRACT FROM AUTHOR]

Published

2023

43. Non-canonical functions of EZH2 in cancer

Author

Sarah M. Zimmerman, Phyo Nay Lin, and George P. Souroullas

Subjects

EZH2, H3K27me3, non-canonical, cancer, oncogene, tumor suppressor, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Mutations in chromatin modifying genes frequently occur in many kinds of cancer. Most mechanistic studies focus on their canonical functions, while therapeutic approaches target their enzymatic activity. Recent studies, however, demonstrate that non-canonical functions of chromatin modifiers may be equally important and therapeutically actionable in different types of cancer. One epigenetic regulator that demonstrates such a dual role in cancer is the histone methyltransferase EZH2. EZH2 is a core component of the polycomb repressive complex 2 (PRC2), which plays a crucial role in cell identity, differentiation, proliferation, stemness and plasticity. While much of the regulatory functions and oncogenic activity of EZH2 have been attributed to its canonical, enzymatic activity of methylating lysine 27 on histone 3 (H3K27me3), a repressive chromatin mark, recent studies suggest that non-canonical functions that are independent of H3K27me3 also contribute towards the oncogenic activity of EZH2. Contrary to PRC2’s canonical repressive activity, mediated by H3K27me3, outside of the complex EZH2 can directly interact with transcription factors and oncogenes to activate gene expression. A more focused investigation into these non-canonical interactions of EZH2 and other epigenetic/chromatin regulators may uncover new and more effective therapeutic strategies. Here, we summarize major findings on the non-canonical functions of EZH2 and how they are related to different aspects of carcinogenesis.

Published

2023

44. Long non-coding RNA MAFG-AS1: A promising therapeutic target for human cancers

Author

Zhiyu Huang, Maoqing Zhang, Jiayue Li, and Chenghua Lou

Subjects

Long non-coding RNA, MAFG-AS1, Cancer, Molecular mechanism, Oncogene, Therapeutics. Pharmacology, RM1-950

Abstract

Long non-coding RNAs (lncRNAs) are commonly known for their important characters in cancer progression. LncRNA MAFG-antisense 1 (AS1) (MAFG-AS1) has been discovered as a novel oncogenic lncRNA for several years. Accumulating data have demonstrated abnormal overexpression of MAFG-AS1 in various human cancers, including breast, bladder, liver, gastric, and lung. Importantly, through regulating various microRNAs and cell signaling pathways, MAFG-AS1 has been demonstrated to exhibit various biological effects, including proliferation, metastasis, and epithelial-mesenchymal transition (EMT). Meanwhile, abnormal overexpression of MAFG-AS1 is closely linked with histological grade, TNM stage, extensive depth of invasion, poor OS, and lymph node metastasis (LNM). In the present review, the authors summarized the previous studies on the biological properties, molecular mechanisms, and clinicopathological characters of MAFG-AS1 in human cancers. In summary, MAFG-AS1 is a promising prognostic biological marker and potential therapeutic target for cancer treatment.

Published

2023

45. Ca2+ Signaling and Src Functions in Tumor Cells

Author

Antonio Villalobo

Subjects

calcium, cancer, calmodulin, oncogene, Src tyrosine kinases, tumor cells, Microbiology, QR1-502

Abstract

Signaling by calcium ion (Ca2+) plays a prominent role in cell physiology, and these mechanisms are frequently altered in tumor cells. In this review, we consider the interplay of Ca2+ signaling and the functions of the proto-oncogene non-receptor tyrosine kinase c-Src in tumor cells, and the viral oncogenic variant v-Src in transformed cells. Also, other members of the Src-family kinases are considered in this context. The role of Ca2+ in the cell is frequently mediated by Ca2+-binding proteins, where the Ca2+-sensor protein calmodulin (CaM) plays a prominent, essential role in many cellular signaling pathways. Thus, we cover the available information on the role and direct interaction of CaM with c-Src and v-Src in cancerous cells, the phosphorylation of CaM by v-Src/c-Src, and the actions of different CaM-regulated Ser/Thr-protein kinases and the CaM-dependent phosphatase calcineurin on v-Src/c-Src. Finally, we mention some clinical implications of these systems to identify mechanisms that could be targeted for the therapeutic treatment of human cancers.

Published

2023

46. Overexpression of long non‐coding RNA NORAD promotes invasion and migration in malignant melanoma via regulating the MIR‐205‐EGLN2 pathway

Author

Chen, Yong, Cao, Ke, Li, Jingjing, Wang, Aijun, Sun, Lichun, Tang, Jintian, Xiong, Wei, Zhou, Xiao, Chen, Xiang, Zhou, Jianda, and Liu, Yan

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biotechnology, Cancer, Genetics, 2.1 Biological and endogenous factors, Aetiology, Animals, Cell Movement, Cell Proliferation, Down-Regulation, Endoplasmic Reticulum Stress, Gene Expression Regulation, Neoplastic, Gene Knockdown Techniques, Heterografts, Humans, Hypoxia-Inducible Factor-Proline Dioxygenases, Male, Melanoma, Mice, Nude, MicroRNAs, Neoplasm Invasiveness, Neoplasm Transplantation, RNA, Long Noncoding, Real-Time Polymerase Chain Reaction, Tumor Cells, Cultured, Up-Regulation, long non-coding RNA, melanoma, microRNA, oncogene, Biochemistry and Cell Biology, Oncology and carcinogenesis

Abstract

Growing evidence suggests that long non-coding RNAs NORAD and miR-205 play a significant role in regulating cancer progression and metastasis. In this study, high expression of NORAD was firstly observed in melanoma tissues and human malignant melanoma cell lines, our aim was to study the interaction of them in the process of invasion and migration of malignant melanoma cells. NORAD, miR-205, and EGLN2 mRNA level in MM cells was detected by qRT-PCR. In situ hybridization (ISH) was performed to detect NORAD expression in MM tissues specimens. Effects of NORAD and miR-205 on Prolyl hydroxylase 2 (EGLN2) expression was explored by western blot in MM cells line. Dual-luciferase reporter assay was performed to verify the interaction relationship between NORAD and miR-205, as well as, miR-205 and EGLN2. Transwell assay was conducted to explore the effects of NORAD and miR-205 in vitro. Xenografts in nude mice experiment were used to confirm the role of NORAD and miR-205 in vivo. In vitro, NORAD knockdown significantly inhibited migration and invasion of malignant melanoma cells and elevated the expression of miR-205, there was an interaction between miR-205 and NORAD in the RNA-induced silencing complex. Upregulation of miR-205 induced significant inhibition of migratory and invasive ability compared with the scrambled control. However, downregulating NORAD largely reversed this effect. Furthermore, the regulatory effects of miR-205 on EGLN2 levels and the induction of endoplasmic reticulum stress were reversed by NORAD. In vivo, deletion of miR-205 induced tumor growth in nude mice. NORAD may play critical roles in tumorigenesis and progression of malignant melanoma by regulating of the miR-205-EGLN2 pathway, and may serve as a new therapeutic target.

Published

2019

47. The X-linked tumor suppressor TSPX downregulates cancer-drivers/oncogenes in prostate cancer in a C-terminal acidic domain dependent manner

Author

Kido, Tatsuo, Li, Yunmin, Tanaka, Yuichiro, Dahiya, Rajvir, and Lau, Yun-Fai Chris

Subjects

Prostate Cancer, Lung Cancer, Cancer, Lung, Genetics, Urologic Diseases, Aging, 2.1 Biological and endogenous factors, Aetiology, TCGA, oncogene, prostate cancer, transcriptome analyses, tumor suppressor, Oncology and Carcinogenesis

Abstract

TSPX is a tumor suppressor gene located at Xp11.22, a prostate cancer susceptibility locus. It is ubiquitously expressed in most tissues but frequently downregulated in various cancers, including lung, brain, liver and prostate cancers. The C-terminal acidic domain (CAD) of TSPX is crucial for the tumor suppressor functions, such as inhibition of cyclin B/CDK1 phosphorylation and androgen receptor transactivation. Currently, the exact role of the TSPX CAD in transcriptional regulation of downstream genes is still uncertain. Using different variants of TSPX, we showed that overexpression of either TSPX, that harbors a CAD, or a CAD-truncated variant (TSPX[∆C]) drastically retarded cell proliferation in a prostate cancer cell line LNCaP, but cell death was induced only by overexpression of TSPX. Transcriptome analyses showed that TSPX or TSPX[∆C] overexpression downregulated multiple cancer-drivers/oncogenes, including MYC and MYB, in a CAD-dependent manner and upregulated various tumor suppressors in a CAD-independent manner. Datamining of transcriptomes of prostate cancer specimens in the Cancer Genome Atlas (TCGA) dataset confirmed the negative correlation between the expression level of TSPX and those of MYC and MYB in clinical prostate cancer, thereby supporting the hypothesis that the CAD of TSPX plays an important role in suppression of cancer-drivers/oncogenes in prostatic oncogenesis.

Published

2019

48. Targeting Oncogenic BRAF: Past, Present, and Future

Author

Zaman, Aubhishek, Wu, Wei, and Bivona, Trever G

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Precision Medicine, Cancer, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Good Health and Well Being, BRAF, oncogene, precision medicine, targeted therapy, drug resistance, Oncology and carcinogenesis

Abstract

Identifying recurrent somatic genetic alterations of, and dependency on, the kinase BRAF has enabled a "precision medicine" paradigm to diagnose and treat BRAF-driven tumors. Although targeted kinase inhibitors against BRAF are effective in a subset of mutant BRAF tumors, resistance to the therapy inevitably emerges. In this review, we discuss BRAF biology, both in wild-type and mutant settings. We discuss the predominant BRAF mutations and we outline therapeutic strategies to block mutant BRAF and cancer growth. We highlight common mechanistic themes that underpin different classes of resistance mechanisms against BRAF-targeted therapies and discuss tumor heterogeneity and co-occurring molecular alterations as a potential source of therapy resistance. We outline promising therapy approaches to overcome these barriers to the long-term control of BRAF-driven tumors and emphasize how an extensive understanding of these themes can offer more pre-emptive, improved therapeutic strategies.

Published

2019

49. miR-106b as an emerging therapeutic target in cancer

Author

Surendra Kumar Sagar

Subjects

Apoptosis, Cancer, Metastases, miRNA, Oncogene, Tumor suppressor, Medicine (General), R5-920, Genetics, QH426-470

Abstract

MicroRNAs (miRNAs) comprise short non-coding RNAs that function in regulating the expression of tumor suppressors or oncogenes and modulate oncogenic signaling pathways in cancer. miRNAs expression alters significantly in several tumor tissues and cancer cell lines. For example, miR-106b functions as an oncogene and increases in multiple cancers. The miR-106b directly targets genes involved in tumorigenesis, proliferation, invasion, migration, and metastases. This review has focused on the miR-106b function and its downstream target in different cancers and provide perspective into how miR-106 regulates cancer cell proliferation, migration, invasion, and metastases by regulating the tumor suppressor genes. Since miRNAs-based therapies are currently being developed to enhance cancer therapy outcomes, miR-106b could be an attractive and prospective candidate in different cancer types for detection, diagnosis, and prognosis assessment in the tumor.

Published

2022

50. A cytoplasmic long noncoding RNA LINC00470 as a new AKT activator to mediate glioblastoma cell autophagy

Author

Liu, Changhong, Zhang, Yan, She, Xiaoling, Fan, Li, Li, Peiyao, Feng, Jianbo, Fu, Haijuan, Liu, Qing, Liu, Qiang, Zhao, Chunhua, Sun, Yingnan, and Wu, Minghua

Subjects

Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Oncology and Carcinogenesis, Brain Disorders, Brain Cancer, Cancer, Orphan Drug, Rare Diseases, Neurosciences, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Autophagy, Cell Line, Tumor, Cytoplasm, Disease Progression, Glioblastoma, Humans, Prognosis, Protein Binding, Proto-Oncogene Proteins c-akt, RNA, Long Noncoding, RNA-Binding Protein FUS, Signal Transduction, LncRNA, AKT activation, Oncogene, GBM, Cardiorespiratory Medicine and Haematology, Cardiovascular medicine and haematology, Oncology and carcinogenesis

Abstract

BackgroundDespite the overwhelming number of investigations on AKT, little is known about lncRNA on AKT regulation, especially in GBM cells.MethodsRNA-binding protein immunoprecipitation assay (RIP) and RNA pulldown were used to confirm the binding of LINC00470 and fused in sarcoma (FUS). Confocal imaging, co-immunoprecipitation (Co-IP) and GST pulldown assays were used to detect the interaction between FUS and AKT. EdU assay, CCK-8 assay, and intracranial xenograft assays were performed to demonstrate the effect of LINC00470 on the malignant phenotype of GBM cells. RT-qPCR and Western blotting were performed to test the effect of LINC00470 on AKT and pAKT.ResultsIn this study, we demonstrated that LINC00470 was a positive regulator for AKT activation in GBM. LINC00470 bound to FUS and AKT to form a ternary complex, anchoring FUS in the cytoplasm to increase AKT activity. Higher pAKT activated by LINC00470 inhibited ubiquitination of HK1, which affected glycolysis, and inhibited cell autophagy. Furthermore, higher LINC00470 expression was associated with GBM tumorigenesis and poor patient prognosis.ConclusionsOur findings revealed a noncanonical AKT activation signaling pathway, i.e., LINC00470 directly interacts with FUS, serving as an AKT activator to promote GBM progression. LINC00470 has an important referential significance to evaluate the prognosis of patients.

Published

2018