Your search keyword '"ONCOGENES"' showing total 11,760 results

1. TFE3‐rearranged nonmelanotic renal PEComa: a case series expanding their phenotypic and fusion landscape.

Author

Agaimy, Abbas, Acosta, Andres M, Cheng, Liang, Collins, Katrina, Fridman, Eddie, Schubart, Christoph, Williamson, Sean R, Hartmann, Arndt, and Trpkov, Kiril

Subjects

FLUORESCENCE in situ hybridization, TUBEROUS sclerosis, RENAL cell carcinoma, GENE fusion, PATIENTS

Abstract

Aims: A subset of exceptionally rare primary renal perivascular epithelioid cell tumours (PEComas) that harbour Xp11.2 translocation have been reported, but no larger series devoted to this topic have been published. Methods and Results: We describe the clinicopathological and molecular features of 10 renal PEComas, collected from our routine and consultation files. There were five female and five male patients aged 14–65 (median: 32 years). One patient had a history of childhood neuroblastoma, but no patients were known to have a tuberous sclerosis complex or other hereditary disorder. Complete surgical excision was the treatment for all patients. The available follow‐up in five patients indicated a favourable outcome in 4/5 cases. Tumour size ranged from 2.8 to 15.2 cm (median, 5.2 cm). Immunohistochemistry revealed consistently strong TFE3 expression in all tumours, whereas PAX8 and keratin cocktails were uniformly negative. Other positive markers included HMB45 (7/9 tumours), CathepsinK (7/9 tumours), and CD117 (KIT) (3/5 tumours). TFE3 rearrangements were detected in 8/9 tumours (by targeted RNA sequencing in seven and by FISH in one). The identified fusion partners included SFPQ (n = 2) and one tumour each with ASPSCR1, ZC3H4, MED15, RBMX, and PRCC. One tumour that lacked TFE3 rearrangement by next‐generation sequencing (NGS) and fluorescence in situ hybridization (FISH) revealed a large intrachromosomal deletion involving PKD1 and TSC2 by DNA‐based NGS. Conclusion: This study highlights the morphologic and genetic diversity of TFE3‐rearranged primary renal PEComas and underlines the value of surrogate TFE3 immunohistochemistry in identifying them. The lack of PAX8 and keratin expression represents the mainstay for distinguishing these tumours from MiTF‐associated renal cell carcinomas. In addition, we report rare (ZC3H4, RBMX) and novel (MED15) TFE3 fusion partners in PEComa. [ABSTRACT FROM AUTHOR]

Published

2024

2. "Huanglianjiedu Decoction" Against Pancreatic Adenocarcinoma Proliferation of by Downregulating the PI3K/AKT/mTOR and MAPK/ERK1/2 Signaling Pathways.

Author

Dong, MD, Shu, Xu, MD, Panling, Yang, MD, Peiwen, Jiao, MD, Juying, Cheng, MD, PhD, Chien-shan, and Chen, MD, PhD, Lianyu

Subjects

ADENOCARCINOMA, CHINESE medicine, MITOGEN-activated protein kinases, IN vitro studies, BIOLOGICAL models, RESEARCH funding, PHENOMENOLOGICAL biology, T-test (Statistics), CELL proliferation, HERBAL medicine, ANIMALS, CELLULAR signal transduction, IN vivo studies, BIOCHEMISTRY, DESCRIPTIVE statistics, PANCREATIC tumors, CELL lines, MICE, MASS spectrometry, ONCOGENES, ANALYSIS of variance, TRANSFERASES, STAINS & staining (Microscopy), COMPARATIVE studies, INTERLEUKINS, DISEASE progression

Abstract

Background: Huanglianjiedu decoction (HLJDD) is a classical Traditional Chinese Medicine (TCM) prescription with thousand years of clinical use against various malignancies, including pancreatic adenocarcinoma (PAAD). However, its potential bioactive component and molecular mechanism remains unclear. Aims: This study is to inspect the HLJDD mechanisms of action against PAAD via integrated computational and pharmacochemistry strategy, in vivo and in vitro experiments to validate associated targets and pathways. Methods: A PAAD xenograft model was established by subcutaneous injecting Panc02 cells into C57BL/6 mice. Ultra-high performance liquid chromatography with tandem mass spectrometry (UHPLC-MS/MS) was engaged to determine constituents of HLJDD and assessed for pharmacokinetic scheme using the TCM Systems Pharmacology Platform (TCM-SP). Differentially expressed genes (DEGs) of PAAD was retrieved from the transcriptome dataset GSE43795, followed by recognizing overlapping targets the oncogenes and target genes of PAAD and HLJDD, respectively. Putative signaling pathways of HLJDD in treating PAAD were enriched using KEGG and GO analyses. The anti-PAAD effects of HLJDD was assessed in vivo and in vitro, besides, the potential mechanism was validated using immunoblotting and immunohistochemical assays. Results: HLJDD significantly suppressed the growth of transplanted PAAD tumors, constrained PAAD progression, and induced apoptosis and S-phase arrest. Seventy-five active components meeting the drug-likeness criteria and 278 target genes of HLJDD were identified. KEGG analysis indicated that the top three enriched pathways were cancer, AGE-RAGE signaling, and IL-17 signaling pathways. Disease enrichment analysis highlighted immune, pharmacological, and cancer-related diseases as the top three categories. A total of 47 potential target genes were identified. Immunoblotting revealed that HLJDD inhibited PI3K and MAPK-related signaling pathways, while immunohistochemical staining confirmed that HLJDD suppressed the expression of phosphorylated MAPK and ERK1/2. Conclusion: HLJDD inhibited PAAD in vitro and in vivo via the modulation of multiple mechanisms, including regulation of PI3K/AKT/mTOR and MAPK/ERK1/2 signaling pathways. [ABSTRACT FROM AUTHOR]

Published

2024

3. Cellular SUMO-specific proteases regulate HAdV-C5 E1B-55K SUMOylation and virus-induced cell transformation.

Author

Wing-Hang Ip, Fiedler, Marie, Gornott, Britta, Morische, Malte, Bertzbach, Luca D., and Dobner, Thomas

Subjects

CELL transformation, VIRAL proteins, POST-translational modification, PROTEOLYTIC enzymes, ONCOGENES

Abstract

Various viral proteins are post-translationally modified by SUMO-conjugation during the human adenovirus (HAdV) replication cycle. This modification leads to diverse consequences for target proteins as it influences their intracellular localization or cell transformation capabilities. SUMOylated HAdV proteins include the multifunctional oncoprotein E1B-55K. Our previous research, along with that of others, has demonstrated a substantial influence of yet another adenoviral oncoprotein, E4orf6, on E1B-55K SUMOylation levels. Protein SUMOylation can be reversed by cellular sentrin/SUMO-specific proteases (SENPs). In this study, we investigated the interaction of E1B-55K with cellular SENPs to understand deSUMOylation activities and their consequences for cell transformation mediated by this adenoviral oncoprotein. We show that E1B-55K interacts with and is deSUMOylated by SENP 1, independently of E4orf6. Consistent with these results, we found that SENP 1 prevents E1A/E1Bdependent focus formation in rodent cells. We anticipate these findings to be the groundwork for future studies on adenovirus-host interactions, the mechanisms that underlie E1B-55K SUMOylation, as well as the role of this major adenoviral oncoprotein in HAdV-mediated cell transformation. [ABSTRACT FROM AUTHOR]

Published

2024

4. Potential Role of APC Mutations in the Prognosis and Targeted Therapy of Gastric Adenocarcinoma.

Author

Zhang, Cao, Qin, Jingjing, Zhou, Wenjuan, Huang, Zexuan, Ye, Jingjing, He, Yaqin, and Sahgal, Pranshu

Subjects

ADENOCARCINOMA, STOMACH tumors, GENOMICS, KILLER cells, RESEARCH funding, T cells, CELL proliferation, CANCER patients, GENE expression, ONCOGENES, METABOLISM, ADENOMATOUS polyposis coli, GENETIC mutation, HUMAN genome, CARCINOGENESIS, MOLECULAR biology, DISEASE progression, EOSINOPHILS

Abstract

Background: Adenomatous polyposis coli (APC) gene, an oncogene, has been implicated in stomach adenocarcinoma (STAD), which is a common type of gastric cancer (GC). Although the relationship between APC gene mutations and gastric adenocarcinoma has been comprehensively studied, the potential role of these mutations in the prognosis and targeted therapy remains known. Methods: We utilized The Cancer Genome Atlas (TCGA) database to obtain gene expression matrices, clinical information, and mutation data from patients with STAD. The mutation status of the APC gene was analyzed, and its correlation with tumor mutational burden (TMB), microsatellite instability (MSI), and clinical prognosis in STAD was investigated. Gene set enrichment analysis (GSEA) was conducted to explore the pathological role of APC gene mutations in STAD metabolic pathways. Drug sensitivity analysis was conducted to identify potential targeted antitumor drugs for patients with APC gene mutations in gastric adenocarcinoma. Results: The results revealed that 88% (46/52) of STAD samples had nonsynonymous mutations. The mutation group exhibited a significantly higher TMB than the wild‐type group (p < 0.001), and the percentage of high MSI (MSI‐H) was significantly higher in the mutation group than in the wild‐type group (p < 0.001). Patients with APC mutations had a worse prognosis than those with APC wild‐type (p = 0.009). The APC gene mutation group displayed significant enrichment in amino acids, RNA, and several pathways (|NES| > 1 and nominal p value < 0.01). Compared to the wild‐type group, the mutation group exhibited a higher infiltration proportion of natural killer (NK) cells resting and eosinophils, whereas a lower infiltration proportion of monocytes and resting mast cells (p value < 0.05). AZD5991 exhibited significant sensitivity in patients with STAD carrying APC mutations (p = 0.028). Conclusion:APC gene mutations play a crucial role in the prognosis, molecular characteristics, and potential therapeutic strategies for gastric adenocarcinoma. [ABSTRACT FROM AUTHOR]

Published

2024

5. Overexpression of TPD52L2 in HNSCC: prognostic significance and correlation with immune infiltrates.

Author

Lu, Min, Xia, Haoyu, Xu, Jing, Liao, Zijun, Li, Yuwen, and Peng, Hanwei

Subjects

SQUAMOUS cell carcinoma, PROTEINS, RESEARCH funding, RECEIVER operating characteristic curves, HEAD & neck cancer, POLYMERASE chain reaction, IMMUNE system, CELLULAR signal transduction, CELL motility, GENE expression, IMMUNOHISTOCHEMISTRY, MESSENGER RNA, BIOINFORMATICS, ONCOGENES, WESTERN immunoblotting, SURVIVAL analysis (Biometry), DISEASE progression, PROPORTIONAL hazards models, OVERALL survival

Abstract

Background: Evidence has been presented that the tumor protein D52 (TPD52) family plays a critical role in tumor development and progression. As a member of the TPD52 family, the changes in TPD52L2 gene status are instrumental in kinds of cancer development. However, its effects on patient prognosis and immune infiltration in Head and Neck Squamous Carcinoma (HNSCC) are still poorly understood. Methods: The Tumor Genome Atlas (TCGA), Gene Expression Omnibus (GEO), and c-BioPortal database was used to explore the expression pattern, prognostic value, and variation of gene status in HNSCC. The LinkedOmics database was used to obtain the co-expression genes of TPD52L2 and identify the diagnostic value of TPD52L2 in HNSCC. The correlations between TPD52L2 expression and six main types of immune cell infiltrations and immune signatures were explored using Tumor Immune Estimation Resource (TIMER). The correlation between TPD52L2 expression and immune checkpoint genes (ICGs) was analyzed by TCGA database. Immunohistochemistry (IHC) was performed to validate the expression of three ICGs (PDL1, PDL2, EGFR) and TPD52L2 using 5 paired HNSCC and normal head and neck tissues. Polymerase Chain Reaction (PCR) and Western Blot (WB) of HNSCC and normal head and neck cell lines were performed to verify the high level of TPD52L2 mRNA and protein expression. protein expression of TPD52L2 in pan-cancer was also validated using UALCAN. Results: TPD52L2 was overexpressed in tumor tissues, and it predicted worse survival status in HNSCC. ROC analysis suggested that TPD52L2 had a diagnostic value. Multivariate Cox analysis identified TPD52L2 as an independent negative prognostic marker of overall survival. Functional network analysis suggested that TPD52L2 was associated with immune-related signaling pathways, cell migration pathways, and cancer-related pathways. High expression of TPD52L2 was associated with a more mutant frequency of TP53. Notably, we found that the expression of TPD52L2 was closely negatively correlated with the infiltration levels of 15 types of immune cells and positively correlated with several immune markers. PCR, WB experiments, and UALCAN database verified the high level of TPD52L2 mRNA and protein expression. Conclusion: TPD52L2 is upregulated in HNSCC, which is an independent factor for adverse prognosis prediction. It probably plays a role in the negative regulation of immune cell infiltration. TPD52L2 might be a promising prognostic biomarker and therapeutic target in HNSCC. [ABSTRACT FROM AUTHOR]

Published

2024

6. Importance of Nectin2, NUF2, and Nectin4 Gene Expression in the Pathogenesis of Different Subtypes of Breast Cancer.

Author

Roshanizadeh, Zahra, Haghshenas, Mohammad Reza, Ramezani, Amin, Shajari, Neda, Tahmasebi, Sedigheh, Akrami, Majid, and Ghaderi, Abbas

Subjects

CELL cycle proteins, RESEARCH funding, T-test (Statistics), HORMONE receptor positive breast cancer, PROGESTERONE receptors, BREAST tumors, CELL adhesion molecules, POLYMERASE chain reaction, TUMOR markers, DESCRIPTIVE statistics, GENE expression, ESTROGEN receptors, CASE-control method, ONE-way analysis of variance, ONCOGENES, DATA analysis software, EPIDERMAL growth factor receptors

Abstract

Background: The targeted therapy using breast cancer (BC)-associated biomarkers has significantly minimized the side-effects of BC treatment. This study aims to elucidate the role of Nectin2, NUF2, and Nectin4 gene expression in the pathogenesis of BC. Method: In this case-control study, the expression of Nectin2, Nectin4, and NUF2 genes was investigated through real-time polymerase chain reaction assay in 46 tumor tissues from BC patients and 46 adjacent non-tumorous tissues as a control group. Data were analyzed using SPSS-21 software, employing independent t-tests and oneway ANOVA. A P-value of <0.05 was considered statistically significant. Results: The results demonstrated a significant increase in the expression of the NUF2 gene in tumor tissues compared with adjacent normal tissues (P = 0.005, fold change = 3.7). No statistically significant difference was observed in the expression of Nectin2 and Nectin4 between the tumor and adjacent tissues. However, higher expression of Nectin2 was noted in the early stages of the disease, particularly in subtypes with estrogen receptor-positive (ER+), progesterone receptor positive (PR+), and human epidermal growth factor receptor 2 negative (HER2-). Furthermore, the expression of NUF2 and Nectin4 was elevated in advanced stages and triple-negative BC subtypes. Notably, the expression of these three genes was higher in patients aged ≤ 45 years. Conclusion: The findings suggest that the expression levels of NUF2, Nectin2, and Nectin4 genes may influence the initiation, progression, and pathogenesis of BC subtypes. [ABSTRACT FROM AUTHOR]

Published

2024

7. Antibody-Drug Conjugates and Their Potential in the Treatment of Patients with Biliary Tract Cancer.

Author

Alexander, Shaun, Aleem, Umair, Jacobs, Timothy, Frizziero, Melissa, Foy, Victoria, Hubner, Richard A., and McNamara, Mairéad G.

Subjects

THERAPEUTIC use of antineoplastic agents, THERAPEUTIC use of monoclonal antibodies, BILE duct tumors, TRASTUZUMAB, DRUG approval, ONCOGENES

Abstract

Simple Summary: Survival for patients with biliary tract cancer (BTC) is poor, especially in the advanced stage, where curative treatments are not available. While chemotherapy and immunotherapy are used in standard practice, antibody–drug conjugates (ADCs) have emerged as a novel therapy option. ADCs potentially enhance cancer cell death and reduce side effects. The anti-HER2 ADC Trastuzumab Deruxtecan (T-Dxd) has shown survival benefit for patients whose tumours are HER2-positive, including a subgroup of BTCs. In April 2024, the regulatory authority FDA approved T-Dxd for adults with unresectable or metastatic HER2-positive solid tumours, including BTCs, lacking other treatment options. Ongoing trials are exploring other potentially actionable BTC molecular alterations. This review will discuss the current evidence and ongoing research in this subject area. Background: Biliary tract cancers (BTCs) are aggressive in nature, often presenting asymptomatically until they are diagnosed at an advanced stage. Surgical resection or liver transplantation are potential curative options. However, a large proportion of patients present with incurable locally advanced or metastatic disease and most of these patients are only eligible for palliative chemotherapy or best supportive care. More recently, targeted therapies have proven beneficial in a molecularly selected subgroup of patients with cholangiocarcinoma who have progressed on previous lines of systemic treatment. However, only a minority of patients with BTCs whose tumours harbour specific molecular alterations can access these therapies. Methods: In relation to ADCs, studies regarding use of antibody–drug conjugates in cancer, particularly in BTCs, were searched in Embase (1974 to 2024) and Ovid MEDLINE(R) (1946 to 2024) to obtain relevant articles. Examples of current clinical trials utilising ADC treatment in BTCs were extracted from the ClinicalTrials.gov trial registry. Conclusions: Overall, this review has highlighted that ADCs have shown encouraging outcomes in cancer therapy, and this should lead to further research including in BTCs, where treatment options are often limited. The promising results observed with ADCs in various cancers underscore their potential as a transformative approach in oncology, warranting continued exploration and development and the need for education on the management of their specific toxicities. By addressing current challenges and optimising ADC design and application, future studies could potentially improve treatment outcomes for patients with BTCs and beyond, potentially in both early and advanced stage settings. [ABSTRACT FROM AUTHOR]

Published

2024

8. Systemic Therapy of Gastric Cancer—State of the Art and Future Perspectives.

Author

Lordick, Florian, Rha, Sun Young, Muro, Kei, Yong, Wei Peng, and Lordick Obermannová, Radka

Subjects

THERAPEUTIC use of antineoplastic agents, ESOPHAGEAL physiology, ADENOCARCINOMA, COMBINATION drug therapy, HETEROCYCLIC compounds, STOMACH tumors, MEDICAL quality control, CLINICAL trials, IMMUNOTHERAPY, PROGRAMMED death-ligand 1, ESOPHAGEAL tumors, TREATMENT effectiveness, CANCER patients, TUMOR markers, CONFERENCES & conventions, ADJUVANT chemotherapy, SURGICAL complications, GENE expression, METASTASIS, ONCOGENES, COMBINED modality therapy, TUMOR classification, SURVIVAL analysis (Biometry), PERIOPERATIVE care, PLATINUM

Abstract

Simple Summary: A review of the latest research at PubMed and major cancer conferences was conducted to find out the current treatments for advanced stomach and esophagogastric junction cancers. In the West, neoadjuvant and perioperative chemotherapy is preferred for localized tumors. In East Asia, adjuvant chemotherapy is preferred. Studies are looking at how well immunotherapy and other drugs work in the perioperative setting. To choose the best treatment for advanced gastric cancer, including adenocarcinoma of the esophago-gastric junction, it is important to know biomarkers like HER2 expression, PD-L1 combined positive score (CPS), Claudin 18.2, and microsatellite instability (MSI). The standard first-line therapy is a combination of fluoropyrimidine and a platinum derivative. The choice of chemotherapy with antibodies depends on the biomarker. This article reviews recent clinical trial results and looks at the future of systemic therapy. Background: The prognosis of patients diagnosed with locally advanced and metastatic gastric and esophago-gastric junction cancer is critical. The optimal choice of systemic therapy is essential to optimize survival outcomes. Methods: A comprehensive literature review via PubMed and analysis of major oncology congresses (European Society for Medical Oncology and American Society of Clinical Oncology websites) were conducted to ascertain the current status and latest developments in the systemic treatment of patients with localized or advanced gastric and esophago-gastric junction adenocarcinoma. Results: While neoadjuvant and perioperative chemotherapy for localized tumor stages is the preferred approach in the Western Hemisphere, adjuvant chemotherapy remains the preferred course of action in East Asia. The administration of chemotherapy, typically in the form of combinations comprising platinum and fluoropyrimidine compounds in combination with docetaxel, represents a standard of care. Investigations are underway into the potential of immunotherapy and other biologically targeted agents in the perioperative setting. To select the most appropriate therapy for advanced gastric cancer, including adenocarcinoma of the esophago-gastric junction, it is essential to determine biomarkers such as HER2 expression, PD-L1 combined positive score (CPS) (combined positive score), Claudin 18.2, and microsatellite instability (MSI). In the present clinical context, the standard first-line therapy is a combination of fluoropyrimidine and a platinum derivative. The selection of chemotherapy in combination with antibodies is contingent upon the specific biomarker under consideration. Conclusions: This article reviews the current state of the art based on recent clinical trial results and provides an outlook on the future of systemic therapy. [ABSTRACT FROM AUTHOR]

Published

2024

9. Theranostic Approaches for Gastric Cancer: An Overview of In Vitro and In Vivo Investigations.

Author

Basirinia, Ghazal, Ali, Muhammad, Comelli, Albert, Sperandeo, Alessandro, Piana, Sebastiano, Alongi, Pierpaolo, Longo, Costanza, Di Raimondo, Domenico, Tuttolomondo, Antonino, and Benfante, Viviana

Subjects

IN vitro studies, GLUTATHIONE, STOMACH tumors, RADIATION, IMMUNOTHERAPY, OLIGOPEPTIDES, TREATMENT effectiveness, IN vivo studies, NEOVASCULARIZATION inhibitors, TUMOR markers, ONCOGENES, NANOTECHNOLOGY, GROWTH factors, INDIVIDUALIZED medicine, EARLY diagnosis, ACCURACY, NANOPARTICLES, SENSITIVITY & specificity (Statistics), MOLECULAR pathology, CELL receptors, NEUROTENSIN

Abstract

Simple Summary: Gastric cancer (GC) represents a major global health challenge, ranking as the second leading cause of cancer-related deaths. The high mortality rate is primarily due to late-stage diagnoses, which limit effective treatment options. Recent research emphasizes the development of targeted therapies and radiation immunotherapy as promising alternatives to traditional approaches. The review authors summarize recent advancements in targeted therapies for gastric cancer, focusing on both laboratory and clinical studies. They explore targeted approaches that have shown potential for improving diagnostic accuracy and treatment effectiveness. The findings of this paper may significantly impact the research community by highlighting the importance of personalized medicine in gastric cancer treatment. By identifying specific molecular targets and utilizing nanotechnology for drug delivery, these advancements aim to enhance treatment efficacy while minimizing systemic toxicity. Overall, the review suggests the potential for improved prognosis and treatment strategies through targeted therapies and precision medicine. Gastric cancer (GC) is the second most common cause of cancer-related death worldwide and a serious public health concern. This high death rate is mostly caused by late-stage diagnoses, which lead to poor treatment outcomes. Radiation immunotherapy and targeted therapies are becoming increasingly popular in GC treatment, in addition to surgery and systemic chemotherapy. In this review, we have focused on both in vitro and in vivo research, which presents a summary of recent developments in targeted therapies for gastric cancer. We explore targeted therapy approaches, including integrin receptors, HER2, Claudin 18, and glutathione-responsive systems. For instance, therapies targeting the integrin receptors such as the αvβ3 and αvβ5 integrins have shown promise in enhancing diagnostic precision and treatment efficacy. Furthermore, nanotechnology provides novel approaches to targeted drug delivery and imaging. These include glutathione-responsive nanoplatforms and cyclic RGD peptide-conjugated nanoparticles. These novel strategies seek to reduce systemic toxicity while increasing specificity and efficacy. To sum up, the review addresses the significance of personalized medicine and advancements in gastric cancer-targeted therapies. It explores potential methods for enhancing gastric cancer prognosis and treatment in the future. [ABSTRACT FROM AUTHOR]

Published

2024

10. Post-Transcriptional Modifications to miRNAs Undergo Widespread Alterations, Creating a Unique Lung Adenocarcinoma IsomiRome.

Author

Cohn, David E., Souza, Vanessa G. P., Forder, Aisling, Telkar, Nikita, Stewart, Greg L., and Lam, Wan L.

Subjects

ADENOCARCINOMA, RANDOM forest algorithms, RESEARCH funding, MICRORNA, RESEARCH evaluation, EPIGENOMICS, GENETIC markers, TUMOR suppressor genes, SUPPORT vector machines, ONCOGENES, GENOME editing, GENE expression profiling, LUNG cancer, SEQUENCE analysis

Abstract

Simple Summary: MicroRNAs (miRNAs) play a significant role as epigenetic regulators in cancer. IsomiRs are miRNA molecules that undergo small modifications during miRNA processing, which can affect their stability and their interaction with mRNA targets. While some isomiRs are linked to specific cancers, many, including those in the lung, remain understudied. To address this, small RNA sequencing data from lung adenocarcinoma (LUAD) and adult non-malignant lung (ANL) samples were analyzed to quantify isomiR expression. This analysis identified 16 A-to-I edited isomiRs, 213 5′ isomiRs, 128 3′ adenylated isomiRs, and 100 3′ uridylated isomiRs. A-to-I editing rates correlated with the expression of editing enzymes ADAR and ADARB1, both deregulated in LUAD. LUAD samples had lower A-to-I editing and 3′ adenylation rates compared to ANL. Machine learning models based on isomiR data effectively distinguished ANL from stage I/II LUAD samples, suggesting that isomiRs hold potential as cancer biomarkers. Background: MicroRNAs (miRNAs) modulate the expression of oncogenes and tumor suppressor genes, functioning as significant epigenetic regulators in cancer. IsomiRs are miRNA molecules that have undergone small modifications during miRNA processing. These modifications can alter an isomiR's binding stability with mRNA targets, and certain isomiRs have been implicated in the development of specific cancers. Still, the isomiRomes of many tissues, including the lung, have not been characterized; Methods: In this study, we analyzed small RNA sequencing data for three cohorts of lung adenocarcinoma (LUAD) and adult non-malignant lung (ANL) samples. Results: We quantified isomiR expression and found 16 A-to-I edited isomiRs expressed in multiple cohorts, as well as 213 5′ isomiRs, 128 3′ adenylated isomiRs, and 100 3′ uridylated isomiRs. Rates of A-to-I editing at editing hotspots correlated with mRNA expression of the editing enzymes ADAR and ADARB1, which were both observed to be deregulated in LUAD. LUAD samples displayed lower overall rates of A-to-I editing and 3′ adenylation than ANL samples. Support vector machines and random forest models were trained on one cohort to distinguish ANL and stage I/II LUAD samples using reads per million (RPM) and frequency data for different types of isomiRs. Models trained on A-to-I editing rates at editing hotspots displayed high accuracy when tested on the other two cohorts and compared favorably to classifiers trained on miRNA expression alone; Conclusions: We have identified isomiRs in the human lung and found that their expression differs between non-malignant and tumor tissues, suggesting they hold potential as cancer biomarkers. [ABSTRACT FROM AUTHOR]

Published

2024

11. Eligibility for Adjuvant Cyclin-Dependent Kinase 4/6 Inhibitors in Endocrine Receptor-Positive and HER2-Negative Early Breast Cancer by Age and Type of Surgery.

Author

Houvenaeghel, Gilles, Classe, Jean-Marc, Chauvet, Marie-Pierre, Colombo, Pierre-Emmanuel, Jouve, Eva, Reyal, Fabien, Daraï, Emile, Rouzier, Roman, Faure-Virelizier, Christelle, Gimbergues, Pierre, Coutant, Charles, Mazouni, Chafika, Azuar, Anne-Sophie, Martino, Marc, Bouteille, Catherine, Cohen, Monique, and de Nonneville, Alexandre

Subjects

BREAST cancer prognosis, BREAST tumors, PROTEIN-tyrosine kinase inhibitors, AGE distribution, RETROSPECTIVE studies, TUMOR grading, ADJUVANT chemotherapy, ONCOGENES, HORMONE therapy, MEDICAL records, ACQUISITION of data, CYCLIN-dependent kinases, LUMPECTOMY, CHEMICAL inhibitors

Abstract

Simple Summary: Improved outcomes have been reported with adjuvant treatment combining cyclin-dependent kinase 4/6 inhibitors with endocrine therapy, in high-risk patients with ER-positive and HER2-negative breast cancer, regardless of age. In this real-world data analysis, MonarchE and NataLEE high-risk patients accounted for 9.5% and 33% of patients undergoing upfront surgery, respectively. Significantly higher eligibility rates were observed in patients who underwent a mastectomy, >70 years and ≤40 years for adjuvant abemaciclib and ribociclib, and in patients >80 years for ribociclib. A higher discontinuation rate for abemaciclib was reported in patients ≥65 years and it can be assumed that discontinuation rates may increase with more older patients. If the results of the NataLEE trial translate into clinical practice, the number of patients potentially eligible for adjuvant CDK4/6 inhibitors may increase, especially in the elderly population. Background: Despite early diagnosis, approximately 20% of patients with ER-positive and HER2-negative breast cancer (BC) will experience disease recurrence. Improved survival has been reported with adjuvant treatment combining cyclin-dependent kinase 4/6 inhibitors with endocrine therapy, in high-risk patients with ER-positive and HER2-negative BC, regardless of age. Older patients have higher rates of ER-positive/HER2-negative BC than younger patients. Methods: In this real-world data analysis, MonarchE and NataLEE high-risk patients accounted for 9.5% and 33% of patients undergoing upfront surgery, respectively. Significantly higher eligibility rates were observed in patients who underwent a mastectomy, >70 years and ≤40 years for adjuvant abemaciclib and ribociclib, and in patients >80 years for ribociclib. Results: Eligibility rates in patients ≤40 years and >80 years who underwent mastectomy were 27.8% and 24.7% for abemaciclib, respectively, and 56.6% and 65.2% for ribociclib, respectively. A higher discontinuation rate for abemaciclib was reported in patients aged ≥65 years and it can be assumed that discontinuation rates may increase in even older patients. Conclusions: If the results of the NataLEE trial translate into clinical practice, the number of patients potentially eligible for adjuvant CDK4/6 inhibitors may increase, especially in the elderly population. [ABSTRACT FROM AUTHOR]

Published

2024

12. A Proteomic Analysis of Nasopharyngeal Carcinoma in a Moroccan Subpopulation.

Author

Reffai, Ayman, Hori, Michelle, Adusumilli, Ravali, Bermudez, Abel, Bouzoubaa, Abdelilah, Pitteri, Sharon, Bennani Mechita, Mohcine, and Mallick, Parag

Subjects

BIOLOGICAL models, MITOGEN-activated protein kinases, NF-kappa B, LIQUID chromatography-mass spectrometry, CELL proliferation, TUMOR markers, DESCRIPTIVE statistics, TUMOR grading, CELLULAR signal transduction, IMMUNE system, GENE expression, JANUS kinases, BIOINFORMATICS, PROTEOMICS, GENE expression profiling, FORMALDEHYDE, HISTOLOGICAL techniques, ONCOGENES, DATA analysis software, NASOPHARYNX tumors, MOLECULAR pathology, GENETICS

Abstract

Simple Summary: Nasopharyngeal carcinoma (NPC) is a head and neck cancer that is mainly found in Southeast Asia and North Africa. Most patients with NPC are diagnosed at an advanced stage, which increases the risk of recurrence and metastasis. A cohort of 41 NPC tumor samples from Morocco and North Africa were analyzed using shotgun proteomics. Within the cohort, three proteomically defined clusters were identified. We also examined sex and stage differences from a proteomic perspective. In total, 59 and 26 differentially abundant proteins were identified between male and female patients and patients with early and advanced stages within the cohort. Data were then compared to 21 healthy controls from a prior study. Across the two datasets, 6532 proteins were identified, of which 1507 proteins were differentially abundant between patients and controls. Differentially abundant proteins between tumor and healthy samples included PI3K, MAPK, BCL2, and PPIA proteins, which are involved in various biological pathways related to cell proliferation and growth. This study lays a foundation for both mechanistic and biomarker studies into NPC in Morocco and North African populations. Background: Nasopharyngeal carcinoma (NPC) is a distinct cancer of the head and neck that is highly prevalent in Southeast Asia and North Africa. Though an extensive analysis of environmental and genetic contributors has been performed, very little is known about the proteome of this disease. A proteomic analysis of formalin-fixed paraffin-embedded (FFPE) tissues can provide valuable information on protein expression and molecular patterns for both increasing our understanding of the disease and for biomarker discovery. To date, very few NPC proteomic studies have been performed, and none focused on patients from Morocco and North Africa. Methods: Label-free Liquid Chromatography–Tandem Mass Spectrometry (LC-MS/MS) was used to perform a proteomic analysis of FFPE tissue samples from a cohort of 41 NPC tumor samples of Morocco and North Africa origins. The LC-MS/MS data from this cohort were analyzed alongside 21 healthy controls using MaxQuant 2.4.2.0. A differential expression analysis was performed using the MSstats package in R. Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) functional annotations were carried out using the DAVID bioinformatic tool. Results: 3341 proteins were identified across our NPC cases, revealing three main clusters and five DEPs with prognostic significance. The sex disparity of NPC was investigated from a proteomic perspective in which 59 DEPs were found between males and females, with significantly enriched terms associated with the immune response and gene expression. Furthermore, 26 DEPs were observed between patients with early and advanced stages of NPC with a significant cluster related to the immune response, implicating up-regulated DEPs such as IGHA, IGKC, and VAT1. Across both datasets, 6532 proteins were quantified between NPC patients and healthy controls. Among them, 1507 differentially expressed proteins (DEPs) were observed. GO and KEGG pathway analyses showed enriched terms of DEPs related to increased cellular activity, cell proliferation, and survival. PI3K and MAPK proteins as well as RAC1 BCL2 and PPIA were found to be overexpressed between cancer tissues and healthy controls. EBV infection was also one of the enriched pathways implicating its latent genes like LMP1 and LMP2 that activate several proteins and signaling pathways including NF-Kappa B, MAPK, and JAK-STAT pathways. Conclusion: Our findings unveil the proteomic landscape of NPC for the first time in the Moroccan population. These studies additionally may provide a foundation for identifying potential biomarkers. Further research is still needed to help develop tools for the early diagnosis and treatment of NPC in Moroccan and North African populations. [ABSTRACT FROM AUTHOR]

Published

2024

13. Revisiting HER2 in Prostate Cancer from an Inclusive Perspective: From Biomarkers to Omics.

Author

Mavingire, Nicole, Moore, Janelle C., Johnson, Jabril R., Dwead, Abdulrahman M., Cropp, Cheryl D., Mechref, Yehia, Kobeissy, Firas, Rais-Bahrami, Soroush, and Woods-Burnham, Leanne

Subjects

PATIENT selection, AFRICAN Americans, DRUG resistance in cancer cells, GENETIC markers, HUMAN research subjects, CLINICAL trials, PROSTATE tumors, TUMOR markers, GENE expression, RACE, ONCOGENES, DISEASE progression

Abstract

Simple Summary: HER2 is a well-known driver of worse outcomes for many types of cancer, including prostate cancer. While HER2 has been previously evaluated in prostate cancer bench studies and clinical trials, there has been a lack of diversity in the experimental designs and protocols. For this reason, it has only recently been reported that Black men with prostate cancer may have a higher prevalence of HER2 overexpression. To thoroughly address health inequities that exist for Black men with prostate cancer, it is critical to utilize diverse biospecimens and enroll diverse study participants into studies that evaluate genetic and molecular contributors to worse prognosis for high-risk populations. In this review, we reconsider the role of HER2 in prostate cancer with an approach that incorporates the effects of race and genetic ancestry. Human epidermal growth factor receptor 2 (HER2) is a major driver of disease progression, treatment resistance, and worse survival for patients with various types of cancers, including prostate cancer. However, key bench studies and clinical trials have failed to evaluate the role of HER2 in prostate cancer using racially diverse experimental designs and protocols. This lack of diversity represents what has been the status quo of cancer research in the United States for decades. In the case of prostate cancer, homogenic study designs are problematic as Black men are much more likely to be diagnosed and die from aggressive and incurable forms of the disease. Therefore, the strategic inclusion of biospecimens collected from Black patients as well as the recruitment and enrollment of Black men into prostate cancer clinical trials is necessary to comprehensively evaluate genetic and molecular factors that contribute to variable outcomes in this high-risk population. Additionally, a higher prevalence of HER2 expression in Black men was recently reported in a small cohort of prostate cancer patients and may contribute to worsened prognosis. In this review, we carefully consider the role of HER2 in prostate cancer while, for the first time, taking into account the influences of race and genetic ancestry. [ABSTRACT FROM AUTHOR]

Published

2024

14. Present and Future of Immunotherapy for Triple-Negative Breast Cancer.

Author

Sriramulu, Sushmitha, Thoidingjam, Shivani, Speers, Corey, and Nyati, Shyam

Subjects

COMBINATION drug therapy, ONCOLYTIC virotherapy, PROGESTERONE receptors, RADIOTHERAPY, IMMUNOTHERAPY, BREAST tumors, ANTINEOPLASTIC agents, TREATMENT effectiveness, CANCER vaccines, ESTROGEN receptors, DRUG approval, CANCER chemotherapy, IMMUNE checkpoint inhibitors, MONOCLONAL antibodies, ONCOGENES, CYTOKINES

Abstract

Simple Summary: Immunotherapy has changed the way we treat triple-negative breast cancer (TNBC), a type of breast cancer that does not have common markers like estrogen, progesterone, or HER2. TNBC has the worst outlook among breast cancers, but it may respond better to immunotherapy because it often shows higher levels of PD-L1 and has more immune cells attacking the tumor. Recently, the FDA approved pembrolizumab (Keytruda) combined with chemotherapy for advanced TNBC, offering new hope for patients. However, not all patients respond equally well, mainly because not everyone has high PD-L1 levels. To improve treatment success, combining immunotherapy with other treatments like chemotherapy, targeted therapies, or radiation seems promising. This review explains TNBC and immunotherapy, discusses current and future combination treatment strategies, and explores the challenges and potential new approaches that might soon be available for treating TNBC. Triple-negative breast cancer (TNBC) lacks the expression of estrogen receptors (ERs), human epidermal growth factor receptor 2 (HER2), and progesterone receptors (PRs). TNBC has the poorest prognosis among breast cancer subtypes and is more likely to respond to immunotherapy due to its higher expression of PD-L1 and a greater percentage of tumor-infiltrating lymphocytes. Immunotherapy has revolutionized TNBC treatment, especially with the FDA's approval of pembrolizumab (Keytruda) combined with chemotherapy for advanced cases, opening new avenues for treating this deadly disease. Although immunotherapy can significantly improve patient outcomes in a subset of patients, achieving the desired response rate for all remains an unmet clinical goal. Strategies that enhance responses to immune checkpoint blockade, including combining immunotherapy with chemotherapy, molecularly targeted therapy, or radiotherapy, may improve response rates and clinical outcomes. In this review, we provide a short background on TNBC and immunotherapy and explore the different types of immunotherapy strategies that are currently being evaluated in TNBC. Additionally, we review why combination strategies may be beneficial, provide an overview of the combination strategies, and discuss the novel immunotherapeutic opportunities that may be approved in the near future for TNBC. [ABSTRACT FROM AUTHOR]

Published

2024

15. Ready, Set, Go: Setting Off on the Mission to Target KRAS in Colorectal Cancer.

Author

Pellatt, Andrew J., Bhamidipati, Deepak, and Subbiah, Vivek

Subjects

MISSIONARIES, COLORECTAL cancer, CELLULAR signal transduction, GENE expression, MONOCLONAL antibodies, ONCOGENES, GENETIC mutation, CELL receptors, EPIDERMAL growth factor receptors

Abstract

Understanding the landscape of KRAS mutations in #CRC is crucial with over 2.8M annual diagnoses worldwide. Explore promising therapies and ongoing challenges in this comprehensive review. #CancerResearch #KRAS #ColorectalCancer [ABSTRACT FROM AUTHOR]

Published

2024

16. Targeting KRAS Oncogene for Patients With Colorectal Cancer: A New Step Toward Precision Medicine.

Author

Sahin, Ibrahim Halil, Saridogan, Turcin, Ayasun, Ruveyda, Syed, Masood Pasha, Gorantla, Vikram, Malhotra, Monica, Thomas, Roby, Rhee, John, Zhang, Janie, Hsu, Dennis, Singhi, Aatur D., and Saeed, Anwaar

Subjects

THERAPEUTIC use of antineoplastic agents, CARRIER proteins, COLORECTAL cancer, CANCER patients, TREATMENT effectiveness, ONCOGENES, QUALITY of life, INDIVIDUALIZED medicine, GENETIC mutation, DRUG development, ALLELES, EPIDERMAL growth factor receptors

Abstract

KRAS mutations are common driver oncogenes associated with the development of several solid tumors. KRAS oncogene has been considered a highly challenging target for drug development because of structural features, including the lack of deep groove on its catalytic unit. However, by leveraging cysteine residues, covalent KRAS inhibitors irreversibly trap KRAS G12C mutants in their inactive GDP-bound state. These agents have resulted in significant clinical responses among patients with KRAS G12C-mutant solid tumors, including patients with colorectal cancer (CRC). Other allele-specific inhibitors of KRAS oncogene and panKRAS and panRAS inhibitors are also currently being investigated in clinical trials. This review article overviews recent clinical progress on KRAS G12C targeting for the management of patients with KRAS G12C-mutant CRC and provides an update on other RAS targeting approaches. We also discuss the unique biological features of RAS-mutant CRC, which require the combination of KRAS inhibitors and anti-epidermal growth factor receptor therapy, and elaborate on resistance mechanisms and novel therapeutic avenues that may define future treatment paradigms of patients with RAS-mutant CRC. KRAS oncogene is now actionable: A review of the literature and future therapeutic opportunities. [ABSTRACT FROM AUTHOR]

Published

2024

17. Selection of Germline Genetic Testing Panels in Patients With Cancer: ASCO Guideline Clinical Insights.

Author

Ricker, Charité, Arun, Banu, Pirzadeh-Miller, Sara, Stoffel, Elena Martinez, Messersmith, Hans, and Tung, Nadine

Subjects

TUMOR prevention, MEDICAL protocols, PATIENT selection, PATIENT education, GENETIC markers, HEALTH, FAMILY history (Medicine), DECISION making, INFORMATION resources, ONCOGENES, GENETIC mutation, GENETIC testing

Abstract

The article discusses the recent American Society of Clinical Oncology (ASCO) guidelines on germline genetic testing panels for patients with cancer. It emphasizes the importance of family history in selecting appropriate genes for testing, outlining when and how to use multigene panel testing. It also highlights the need for clinicians to navigate the complexities of testing various genes and the implications of variants of uncertain significance.

Published

2024

18. Quality of life in women with early-stage and metastatic hormone receptor-positive, HER2-negative breast cancer receiving endocrine therapy.

Author

O'Reilly, David, Farooq, Abdul Rehman, Selvadurai, Paul Nevins, Sheehan, Laura, Molan, Karen, Krishnanivas, Bindu, Mullen, Valerie, McMahon, David, Hadi, Danial, Ahmed, Ahmed, Jennings, Maeve, Carroll, Hailey, Chew, Sonya, Macanovic, Bojan, Brown, Ciara O'Hanlon, Noonan, Sinéad A, Reilly, Seamus O, Connolly, Roisin M, Cahir, Caitriona, and Kelly, Catherine M

Subjects

CROSS-sectional method, HORMONE receptor positive breast cancer, PREDICTION models, RESEARCH funding, BREAST tumors, SCIENTIFIC observation, MULTIPLE regression analysis, FISHER exact test, MULTIVARIATE analysis, CHI-squared test, DESCRIPTIVE statistics, QUALITY of life, ONCOGENES, ENDOCRINE diseases, HEALTH outcome assessment, DATA analysis software, NONPARAMETRIC statistics

Abstract

Introduction Early discontinuation of endocrine therapy (ET) is higher among patients with early breast cancer (EBC) compared to patients with metastatic hormone receptor-positive (HR+) breast cancer (MBC). In our clinical experience the reasons for this may include a significant burden of ET side effects impacting quality of life (QOL) in patients with EBC. We hypothesized that QOL is lower in patients with HR + EBC compared to patients with HR + MBC on ET. Methods We conducted a cross-sectional observational study to assess QOL utilizing FACT-ES & EORTC QLQ C30 tools among patients with EBC and MBC receiving ET across 5 Irish hospitals. Results A total of 417 patients were enrolled—EBC (79% n  = 331) and MBC 21% (n  = 86). Using the FACT-ES, we found no difference in overall QOL by stage (139.2 vs 141, P  = .33). Patients with HR + MBC had a lower symptom burden from ET compared to HR + EBC (61.4 vs 54, P  < .01). In adjusted multivariate linear regression models, there was no difference in QOL for patients with EBC and MBC receiving ET. Conclusions There was no significant difference in overall QOL for patients with EBC and MBC. However, patients with EBC experienced more endocrine symptoms. In adjusted multivariate linear regression models, the stage did not predict QOL. Our results suggest that endocrine symptoms are significant contributors to impaired QOL for patients with EBC but the role of other determinants of QOL (eg, stage) is less clear. Future work could include the development of stage-specific QOL tools and utilization of electronic patient-reported outcomes (ePROs) to identify and manage emergent toxicities. [ABSTRACT FROM AUTHOR]

Published

2024

19. The effect of c‐Fos on the prognosis, proliferation, and invasion of oral squamous cell carcinoma.

Author

Peng, Lu, Sun, Ercan, Zhang, Jinfang, Cai, Lanyu, Zheng, Jun, and Zeng, Yan

Subjects

SQUAMOUS cell carcinoma, STATISTICAL correlation, IN vitro studies, MOUTH tumors, CANCER invasiveness, RESEARCH funding, HEAD & neck cancer, CELL proliferation, MICRORNA, TUMOR markers, TRANSCRIPTION factors, CELL motility, CELL lines, GENE expression, IMMUNOHISTOCHEMISTRY, KAPLAN-Meier estimator, BIOINFORMATICS, ONCOGENES, RESEARCH, OXIDOREDUCTASES, PROPORTIONAL hazards models

Abstract

Objective: This study aimed to determine the role of c‐Fos in growth and invasion of oral squamous cell carcinoma (OSCC). Methods: Immunohistochemistry was used to assess c‐Fos expression in 94 OSCC tissues and 30 adjacent normal tissues, the correlation between c‐Fos expression and clinicopathological characteristics was examined, and Kaplan–Meier and Cox analysis were used to investigate the role of c‐Fos in predicting the prognosis of OSCC patients. The effects of c‐Fos on the growth and invasion of OSCC were disclosed by overexpression and knockdown of c‐Fos. Furthermore, based on bioinformatics prediction, the effect of miR‐155‐5p on c‐Fos expression was examined, and dual‐luciferase reporter assay system was used to determine whether miR‐155‐5p regulated the transcriptional activity of c‐Fos in OSCC. Results: c‐Fos was markedly increased in OSCC tissues and cells. c‐Fos upregulation indicates a poor prognosis in OSCC patients, and c‐Fos promotes cell proliferation, migration, and invasion in OSCC. miR‐155‐5p could regulate the expression and the transcriptional activity of c‐Fos by directly targeting the c‐Fos 3′‐UTR. Conclusion: This study demonstrated that c‐Fos contributed to the progression of OSCC and may act as a potential target for OSCC therapy, and a potential prognostic biomarker of OSCC. [ABSTRACT FROM AUTHOR]

Published

2024

20. Predictive Marker of Disease Activity in Breast Cancer Patients with and without Metastasis.

Author

Nourmohammadi, Hassan, Mirbeigi, Syedeh Negin, Nademi, Arash, and Shafiei, Elham

Subjects

RESEARCH funding, BREAST tumors, AGE distribution, RETROSPECTIVE studies, DESCRIPTIVE statistics, METASTASIS, GENE expression, LONGITUDINAL method, ODDS ratio, IMMUNOHISTOCHEMISTRY, ONCOGENES, DATA analysis software, CONFIDENCE intervals, BIOMARKERS

Abstract

Introduction: Levels of the human epidermal growth factor receptor 2 (HER2) gene are low in normal breast tissue, but half of the patients with breast cancer exhibit higher levels of this receptor. The differential expression of the HER2 gene in normal and malignant cells makes it an excellent biomarker for therapeutic purposes. In this study, we evaluated the degree of HER2 overexpression in patients and its relationship with age and the occurrence of metastases. Materials & Methods: In this retrospective, registry-based, two-center cohort study, information on 1500 breast cancer patients recruited from Shahid Mostafa Khomeini Hospital in Ilam Province was collected from 2020 to 2023. Results: The likelihood of metastasis in cancer patients with HER2 gene expression was three times higher (adjusted OR: 2.82; 95% CI: 1.79-3.29; P=0.001). Additionally, the involvement of lymph nodes (adjusted OR: 2.01; 95% CI: 0.87-3.79; P=0.03) was significantly associated with increased metastasis. Conclusion: This study demonstrates that HER2 gene expression and the number of involved lymph nodes are significant prognostic factors that increase the risk of metastasis. Therefore, implementing comprehensive breast cancer screenings can play an important role in the treatment and prevention of metastasis in breast cancer patients. [ABSTRACT FROM AUTHOR]

Published

2024

21. Driver gene alterations in NSCLC patients in southern China and their correlation with clinicopathologic characteristics.

Author

Lingna Deng, Jinbang Li, Zhanlong Qiu, and Yanfen Wang

Subjects

NON-small-cell lung carcinoma, LOGISTIC regression analysis, RAS oncogenes, EPIDERMAL growth factor receptors, ONCOGENES

Abstract

Introduction: In this study, we aimed to explore the relationship between clinicopathological features and driver gene changes in Chinese NSCLC patients. Methods: Amplification refractory mutation system PCR was used to detect the aberrations of 10 driver oncogenes in 851 Chinese NSCLC patients, and their correlation with clinicopathological characteristics was also analyzed. Moreover, three models of logistic regression were used to analyze the association between histopathology and EGFR or KRAS mutations. Results: The top two most frequently aberrant target oncogenes were EGFR (48.06%) and KRAS (9.51%). These were followed by ALK (5.41%), HER2 (2.35%), MET (2.23%), RET (2.11%), ROS1 (1.88%), BRAF (0.47%), NRAS (0.24%), and PIK3CA (0.12%). Additionally, 11 (1.29%) patients had synchronous gene alterations in two genes. The main EGFR mutations were exon 21 L858R and exon 19-Del, which accounted for 45.97% and 42.79% of all EGFR mutations, respectively. Logistic regression analysis showed that the frequency of EGFR mutations was positively correlated with women, non-smokers, lung adenocarcinoma, and invasive nonmucinous adenocarcinoma (IA), and negatively correlated with solid nodule, micro-invasive adenocarcinoma, and solid-predominant adenocarcinoma. KRAS mutations were positively associated with men and longer tumor long diameters and negatively correlated with lung adenocarcinoma (P < 0.05 for all). Conclusion: Our findings suggest that the EGFR mutation frequency was higher in women, non-smokers, lung adenocarcinoma, and the IA subtype in lung adenocarcinoma patients, while the KRAS mutation rate was higher in men and patients with longer tumor long diameter and lower in lung adenocarcinoma patients. [ABSTRACT FROM AUTHOR]

Published

2024

22. Immune‐inflammatory markers and clinical characteristics as predictors of the depth of response and prognosis of patients with PD‐L1 ≥50% metastatic non‐small cell lung cancer receiving first‐line immunotherapy.

Author

Zheng, Xixi, Zhou, Lili, Shi, Hui, An, Juan, Xu, Weiran, Ding, Xiaosheng, Hua, Yichun, Shi, Weiwei, and Li, Xiaoyan

Subjects

NEUTROPHIL lymphocyte ratio, RESEARCH funding, T cells, ACADEMIC medical centers, PROGRAMMED death-ligand 1, IMMUNOTHERAPY, TUMOR markers, CANCER patients, DESCRIPTIVE statistics, RETROSPECTIVE studies, METASTASIS, IMMUNE checkpoint inhibitors, TUMOR suppressor genes, DRUG efficacy, ONCOGENES, MEDICAL records, ACQUISITION of data, INFLAMMATION, LUNG cancer, GENETIC mutation, PROGRESSION-free survival, CONFIDENCE intervals, IMMUNOMODULATORS, OVERALL survival, EPIDERMAL growth factor receptors, EVALUATION, SYMPTOMS

Abstract

Background: Patients with programmed cell death‐ligand 1 (PD‐L1) ≥50% metastatic non‐small cell lung cancer (NSCLC) treated with first‐line immunotherapy showed heterogeneous tumor responses. In this study, we investigated the clinical and immune‐inflammatory markers distinguishing patients with metastatic NSCLC achieving high depth of tumor response (HDPR) from those with non‐high depth of response (NHDPR). The impact of clinical features on the prognosis of patients with PD‐L1 ≥50% were further clarified. Methods: The clinical characteristics and immune‐inflammatory markers of 17 patients with PD‐L1 ≥50% metastatic NSCLC at Beijing Tiantan Hospital between July 2020 and December 2023 were retrospectively analyzed. Results: Among the 17 patients, seven (41.2%) patients achieved HDPR (range: −50%, −72%) and 10 (58.8%) patients achieved NHDPR (range: −13%, −45%). Below normal CD4 + T lymphocytes/CD8 + T lymphocytes (CD4/CD8) ratio (p = 0.01) and oncogenes and/or tumor suppressor gene mutations (TP53/KRAS/EGFR) (p = 0.001) were found enriched for NHDPR compared with HDPR. With a median follow‐up of 26.0 months (range: 17.2–34.8 months), the median progression‐free survival (PFS) following first‐line immunotherapy and overall survival (OS) were 9.0 months (95% CI: 5.0–13.0) and not reached (NR), respectively. The neutrophil‐to‐lymphocyte ratio (NLR) was identified as an independent prognostic factor on first‐line PFS. Patients with an NLR ≥4 exhibited a shorter median PFS (7.0 months vs. NR; p = 0.033; 95% CI: 1.2–80.2) than those with an NLR <4 following first‐line immunotherapy. Conclusions: Among patients with PD‐L1 ≥50% metastatic NSCLC who received first‐line immunotherapy, a lower CD4/CD8 ratio and the presence of genes mutations showed a diminished tumor response and a higher NLR ratio exhibited a worse median PFS. [ABSTRACT FROM AUTHOR]

Published

2024

23. An Autoethnographic Exploration of My Breast Cancer Journey: Egg Freezing, Childfreeness, and "Going Flat".

Author

Pérez-Hernández, Yolinliztli

Subjects

HEALTH literacy, MAMMAPLASTY, UNNECESSARY surgery, BREAST tumors, ETHNOLOGY research, INFERTILITY, BODY image, EXPERIENCE, CISGENDER people, ONCOGENES, MASTECTOMY, CANCER patient psychology, FERTILITY preservation, PATIENT decision making, GENETIC mutation, CHILDLESSNESS

Abstract

In this essay, I discuss my personal experience with breast cancer, exploring three intertwined choices: declining medical egg freezing, choosing not to bear children, and opting out of breast reconstruction after a double mastectomy. Through autoethnography, I narrate how being an immigrant Latina cisgender lesbian in Europe influenced my decision-making processes. Challenging common assumptions about the invariably negative emotional impact on survivors of bilateral mastectomy and infertility, I emphasize the importance for me of minimizing additional pain by eliminating "unnecessary" medical interventions. Likewise, I address concerns about body changes, bodily integrity, and the impact of a positive genetic mutation on my family. My aim is to shed light on knowledge production gaps by sharing my journey from a minority perspective. [ABSTRACT FROM AUTHOR]

Published

2024

24. Analysis of HER2-Low Breast Cancer in Aotearoa New Zealand: A Nationwide Retrospective Cohort Study.

Author

Lasham, Annette, Ramsaroop, Reenadevi, Wrigley, Abbey, and Knowlton, Nicholas

Subjects

THERAPEUTIC use of monoclonal antibodies, RESEARCH funding, BREAST tumors, PSYCHOLOGY of women, RETROSPECTIVE studies, DESCRIPTIVE statistics, REPORTING of diseases, LONGITUDINAL method, ONCOGENES

Abstract

Simple Summary: This research is the first comprehensive study in New Zealand to categorise and examine the characteristics of breast cancer based on HER2 status. We explored three HER2 categories: HER2-zero, HER2-low, and HER2-positive, in women diagnosed with invasive breast cancer. Utilising Te Rēhita Mate Ūtaetae (Breast Cancer Foundation NZ National Register), our study analysed data spanning 21 years, revealing that most women underwent HER2 testing. Significantly, many cases previously not recognised as having significant HER2 levels were in fact HER2-low, qualifying them for newer, targeted drug therapies. These findings are particularly crucial as they suggest that newer therapies could benefit a larger segment of patients, notably those with advanced breast cancer; approximately 60% of these women might now benefit from these innovative HER2-targeted treatments. The study underscores the urgent need for standardised HER2 testing to personalise and optimise treatment, enhancing outcomes for patients with invasive breast cancer. Objectives: To perform the first national analysis of demographic and clinicopathological features associated with the HER2 positive, HER2-low, and HER2-zero invasive breast cancers in New Zealand. The study will reveal the proportion of women who may benefit from new HER2-targeted antibody drug conjugate (ADC) therapies. Methods: Utilising data from Te Rēhita Mate Ūtaetae (Breast Cancer Foundation NZ National Register), the study analysed data from women diagnosed with invasive breast cancer over a 21-year period. The HER2 status of tumours was classified into three categories—HER2-zero, HER2-low, HER2-positive. Results: From 2009–2021, 94% of women underwent HER2 testing, with 14% diagnosed with HER2-positive breast cancer. For advanced-stage disease, 38% of those formerly classified as HER2-negative were reclassified as HER2-low. Including HER2-positive breast cancers, this indicates that 60% of women with advanced breast cancer may potentially benefit from the new HER2-directed ADCs (approximately 120 women per year). Conclusions: The findings suggest a significant proportion of women with invasive breast cancer in New Zealand could benefit from new HER2-targeted treatments. There is a need to standardise HER2 testing to enhance personalised treatment and improve outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

25. FOXM1 Transcriptionally Co-Upregulates Centrosome Amplification and Clustering Genes and Is a Biomarker for Poor Prognosis in Androgen Receptor-Low Triple-Negative Breast Cancer.

Author

Rida, Padmashree, Baker, Sophia, Saidykhan, Adam, Bown, Isabelle, and Jinna, Nikita

Subjects

BREAST cancer prognosis, TUMOR markers, TRANSCRIPTION factors, CELL cycle, GENE expression, CYTOPLASM, ONCOGENES, CELL death, ANDROGEN receptors

Abstract

Simple Summary: Quadruple-negative breast cancer (QNBC; ER−, PR−, HER2−, and AR−) is a highly proliferative subtype of breast cancer that has no targeted treatment options. Chemotherapy, which is toxic to both malignant and healthy cells, is the mainstay treatment for this subpopulation. Centrosome amplification and clustering are cancer cell-specific traits that are upregulated in QNBC relative to other subtypes; thus, centrosome declustering drugs have been suggested to be a promising anticancer therapeutic strategy for this subgroup. However, the targeting of new centrosome biogenesis is neglected, rendering these drugs less effective. Herein, we propose targeting FOXM1, a master transcription regulator that drives the synchronous upregulation of centrosome amplification and clustering genes to circumvent this neglect. We discovered an overdrive of a FOXM1-mediated transcriptional signaling cascade in AR-low relative to AR-high triple-negative breast cancers (TNBCs). Hence, we assert that targeting FOXM1 may be a more efficacious anticancer strategy than centrosome declustering alone, suggesting FOXM1 could be a promising biomarker and actionable target in AR-low TNBC. There are currently no approved targeted treatments for quadruple-negative breast cancer [QNBC; ER−/PR−/HER2−/androgen receptor (AR)−], a subtype of triple-negative breast cancer (TNBC). AR-low TNBC is more proliferative and clinically aggressive than AR-high TNBC. Centrosome amplification (CA), a cancer hallmark, is rampant in TNBC, where it induces spindle multipolarity-mediated cell death unless centrosome clustering pathways are co-upregulated to avert these sequelae. We recently showed that genes that confer CA and centrosome clustering are strongly overexpressed in AR-low TNBCs relative to AR-high TNBCs. However, the molecular mechanisms that index centrosome clustering to the levels of CA are undefined. We argue that FOXM1, a cell cycle-regulated oncogene, links the expression of genes that drive CA to the expression of genes that act at kinetochores and along microtubules to facilitate centrosome clustering. We provide compelling evidence that upregulation of the FOXM1-E2F1-ATAD2 oncogene triad in AR-low TNBC is accompanied by CA and the co-upregulation of centrosome clustering proteins such as KIFC1, AURKB, BIRC5, and CDCA8, conferring profound dysregulation of cell cycle controls. Targeting FOXM1 in AR-low TNBC may render cancer cells incapable of clustering their centrosomes and impair their ability to generate excess centrosomes. Hence, our review illuminates FOXM1 as a potential actionable target for AR-low TNBC. [ABSTRACT FROM AUTHOR]

Published

2024

26. BRAF Inhibition and UVB Light Synergistically Promote Mus musculus Papillomavirus 1-Induced Skin Tumorigenesis.

Author

Dorfer, Sonja, Ressler, Julia Maria, Riebenbauer, Katharina, Kancz, Stefanie, Purkhauser, Kim, Bachmayr, Victoria, Cataisson, Christophe, Kirnbauer, Reinhard, Petzelbauer, Peter, Wiesmueller, Markus, Egg, Maximilian, Hoeller, Christoph, and Handisurya, Alessandra

Subjects

PAPILLOMAVIRUS diseases, PROTEIN kinase inhibitors, MITOGEN-activated protein kinases, SKIN tumors, T-test (Statistics), ULTRAVIOLET radiation, TRANSCRIPTION factors, IN vivo studies, CELLULAR signal transduction, DESCRIPTIVE statistics, ADJUVANT chemotherapy, MICE, KERATINOCYTES, MESSENGER RNA, IMMUNOHISTOCHEMISTRY, SULFONAMIDES, ANIMAL experimentation, ONCOGENES, WESTERN immunoblotting, ONE-way analysis of variance, GENETIC mutation, COMPARATIVE studies, GENOMES

Abstract

Simple Summary: Outgrowth of skin tumors in cancer patients who receive therapies with BRAF inhibitors is frequently observed as an undesired side effect. Infection with certain human papillomaviruses may play a role in BRAF-inhibitor-associated skin tumor development. In this study, the impact of BRAF inhibitors and Ultraviolet B (UVB) light on tumor growth was investigated in laboratory mice after infection of their skin with a murine papillomavirus. We could show that the combination of BRAF inhibitor treatment and UVB exposure resulted in higher numbers of virus-induced tumors compared with virus-infected mice that had received only BRAF inhibitors, only UVB irradiation or no additional treatment. This shows that BRAF inhibitors, particularly when combined with UVB light, support skin tumor growth in mice and may represent a novel way by which BRAF inhibitors contribute to skin cancer development. The development of keratinocytic skin tumors, presumably attributable to paradoxical activation of the MAPK pathway, represents a relevant side effect of targeted therapies with BRAF inhibitors (BRAFis). The role of cutaneous papillomavirus infection in BRAFi-associated skin carcinogenesis, however, is still inconclusive. Employing the Mus musculus papillomavirus 1 (MmuPV1) skin infection model, the impact of BRAFis and UVB exposure on papillomavirus induced skin tumorigenesis was investigated in immunocompetent FVB/NCrl mice. Systemic BRAF inhibition in combination with UVB light induced skin tumors in 62% of the MmuPV1-infected animals. In contrast, significantly fewer tumors were observed in the absence of either BRAF inhibition, UVB irradiation or virus infection, as demonstrated by lesional outgrowth in 20%, 5% and 0% of the mice, respectively. Combinatory exposure to BRAFis and UVB favored productive viral infection, which was shown by high numbers of MmuPV1 genome copies and E1^E4 spliced transcripts and an abundance of E6/E7 oncogene mRNA and viral capsid proteins. BRAF inhibition, but not viral infection or UVB light, activated ERK1/2, whereas γH2AX expression, inducible by UVB light, remained unaltered by BRAFis. These results provide experimental evidence that BRAF inhibition and UVB irradiation synergistically promote MmuPV1-induced skin tumor development in vivo. This indicates an alternative pathway by which papillomavirus skin infection may contribute to BRAFi-associated skin tumorigenesis. [ABSTRACT FROM AUTHOR]

Published

2024

27. Emerging Targets in Non-Small Cell Lung Cancer.

Author

Liu, Louisa, Soler, Joshua, Reckamp, Karen L., and Sankar, Kamya

Subjects

NON-small-cell lung carcinoma, LUNG cancer, DRUG target, ONCOGENES, CLINICAL trials

Abstract

Lung cancer is responsible for a high burden of disease globally. Over the last two decades, the discovery of targetable oncogenic genomic alterations has revolutionized the treatment landscape for early-stage and advanced non-small cell lung cancer (NSCLC). New molecular drivers continue to emerge as promising therapeutic targets, including KRAS non-G12C, RAF/MEK, HER3, Nectin-4, folate receptor alpha, ITGB6, and PRMT5. In this review, we summarize the emerging molecular targets with a potential clinical impact in advanced NSCLC, elaborating on their clinical characteristics and specific mechanisms and molecular pathways for which targeted treatments are currently available. Additionally, we present an aggregate of ongoing clinical trials investigating the available treatment options targeting such alterations, in addition to their current recruitment status and preliminary efficacy data. These advancements may guide further research endeavors and inform future treatment strategies to improve the management of and transform outcomes for patients with advanced NSCLC. [ABSTRACT FROM AUTHOR]

Published

2024

28. Transposable elements alter gene expression and may impact response to cisplatin therapy in ovarian cancer.

Author

Mombach, Daniela Moreira, Mercuri, Rafael Luiz Vieira, Gomes, Tiago Minuzzi Freire da Fontoura, Galante, Pedro A F, and Loreto, Elgion Lucio Silva

Subjects

GENE expression, CANCER genes, ENDOGENOUS retroviruses, OVARIAN cancer, ENDOSCOPIC surgery

Abstract

Cisplatin is widely employed for cancer treatment; therefore, understanding resistance to this drug is critical for therapeutic practice. While studies have delved into differential gene expression in the context of cisplatin resistance, findings remain somewhat scant. We performed a comprehensive investigation of transposable elements (TEs) expression and their impact in host genes in two cisplatin-treated ovarian cancer cell lines. RNA-seq, ATAC-seq, and in-depth bioinformatics analysis were used to compare cisplatin-sensitive and -resistant ovarian cancer cell lines. Our results reveal that cisplatin therapy alters not only the expression of protein-coding genes, but also key TEs, including LINE1, Alu , and endogenous retroviruses, in both cisplatin-sensitive and -resistant cell lines. By co-expressing with downstream genes or by creating chimeric transcripts with host genes at their insertion sites, these TEs seem to control the expression of protein-coding genes, including tumor-related genes. Our model uncovers TEs influencing the expression of cancer genes and cancer pathways. Collectively, our findings indicate that TE alterations associated with cisplatin treatment occur in critical cancer genes and cellular pathways synergically. This research highlights the importance of considering the entire spectrum of transcribed elements in the genome, especially TE expression, for a complete understanding of complex models like cancer response to treatment. [ABSTRACT FROM AUTHOR]

Published

2024

29. WT1 Expression Is Associated with Poor Overall Survival after Azacytidine and DLI in a Cohort of Adult AML and MDS Patients.

Author

Aydin, Semra, Schmitz, Jennifer, Dellacasa, Chiara M., Dogliotti, Irene, Giaccone, Luisa, and Busca, Alessandro

Subjects

MYELODYSPLASTIC syndromes, RED blood cell transfusion, RISK assessment, CYTOGENETICS, AZACITIDINE, BONE marrow cancer, PATHOLOGIC complete response, CANCER patients, DESCRIPTIVE statistics, CELLULAR therapy, TUMOR markers, LONGITUDINAL method, ONCOGENES, NEPHROBLASTOMA, COMPARATIVE studies, CARCINOGENESIS, DISEASE relapse, PROPORTIONAL hazards models, OVERALL survival, DISEASE risk factors, ADULTS

Abstract

Simple Summary: Azacytidine and donor lymphocyte infusions were combined effectively in a single-center high-risk patient cohort (n = 29) for post-transplant relapse of acute myeloid leukemia and myelodysplastic syndrome. Bone marrow Wilms tumor gene 1 (WT1) expression was measured at time of transplant and post-transplant relapse. By using the Cox proportional hazards model, cut-off values for WT1 at both time points were obtained. The disease risk index incorporating initial cytogenetics and the disease stage at transplant as well as WT1 expression was significantly associated with overall survival, indicating that WT1 may represent a minimal residual disease marker in this context of cell therapy response evaluation, especially in high-risk patients currently considered to be in complete remission. Cut-off values for bone marrow WT1 expression for the two decisive treatment time points were proposed. Introduction: Post-transplant relapse of acute myeloid leukemia and myelodysplastic syndrome faces restricted effective salvage regimens. We retrospectively analyzed the use of Azacitidine–donor lymphocyte infusion (AZA/DLI) in this setting. Furthermore, data on bone marrow Wilms tumor gene 1 (WT1) expression were collected. Methods: A Cox proportional hazards model, an outcome-oriented approach for the lowest smoothed plot of the martingale residuals, was performed for the cut-point determination of the respective WT1 expression levels. Finally, a Cox proportional hazards model investigated the association of overall survival (OS) with predictors. Results: An overall response of 41.4% with a median duration of 11.9 months for stable disease and 19.5 months for complete response (CR) patients was achieved. The disease risk index (DRI) high-/very high-risk patients had a shorter OS of 4.4 months than intermediate-risk patients, with 14.5 months, p = 0.007. At transplant, WT1-overexpressing patients (>150 copies) had a shorter median OS of 5.3 months than low-WT1-expressing ones, with 13.5 months, p = 0.024. Furthermore, patients with ≤1000 WT1 copies at relapse had a significantly longer OS with 15.3 months than patients overexpressing WT1, with 4.4 months, p = 0.0002. Conclusions: DRI and WT1 expression associate significantly with OS after AZA/DLI. Hence, WT1 may represent an MRD marker, especially in CR patients at high risk. [ABSTRACT FROM AUTHOR]

Published

2024

30. TP53 Mutation-Mediated Immune Evasion in Cancer: Mechanisms and Therapeutic Implications.

Author

Wang, Chuqi, Tan, Jordan Yong Ming, Chitkara, Nishtha, and Bhatt, Shruti

Subjects

TUMOR genetics, HEMATOPOIETIC stem cell transplantation, KILLER cells, MACROPHAGES, APOPTOSIS, CELL physiology, NEUTROPHILS, IMMUNOTHERAPY, IMMUNE checkpoint inhibitors, ONCOGENES, GENETIC mutation, TUMORS, IMMUNOSUPPRESSION

Abstract

Simple Summary: p53 mutations are prevalent across a variety of human cancers and are regarded as a major obstacle in cancer therapy. These mutations can confer resistance to apoptosis and cell cycle arrest, contributing to multidrug resistance in tumors. Recent studies have uncovered important immunomodulatory functions of p53, but these functions are still underappreciated compared to its other well-known roles. This review aims to summarize the latest literature on immune evasion in p53-mutant tumors and explore the potential of targeting p53 to enhance anti-tumor immunity. Mutation in p53 is the most frequent event in cancer development and a leading cause of cancer therapy resistance due to evasion of the apoptosis cascade. Beyond chemotherapies and radiation therapies, growing evidence indicates that p53-mutant tumors are resistant to a broad range of immune-based therapies, such as immune checkpoint inhibitors, chimeric antigen receptor (CAR) T, and hematopoietic stem cell transplantation (HSCT). This highlights the role of p53 mutations in driving immune evasion of tumor cells. In this review, we first summarize recent studies revealing mechanisms by which p53-mutant tumors evade immune surveillance from T cells, natural killer (NK) cells, and macrophages. We then review how these mutant tumor cells reshape the tumor microenvironment (TME), modulating bystander cells such as macrophages, neutrophils, and regulatory T (Treg) cells to foster immunosuppression. Additionally, we review clinical observations indicative of immune evasion associated with p53 loss or mutations. Finally, we discuss therapeutic strategies to enhance immune response in p53 wild-type (WT) or mutant tumors. [ABSTRACT FROM AUTHOR]

Published

2024

31. A Novel Monoclonal Antibody against PD-1 for the Treatment of Viral Oncogene-Induced Tumors or Other Cancer.

Author

Xu, Xu, Yan, Shih-Long, Yo, Yi-Te, Chiang, Peiyu, Tsai, Chan-Yen, Lin, Lih-Ling, and Qin, Albert

Subjects

THERAPEUTIC use of monoclonal antibodies, IN vitro studies, BIOLOGICAL models, RESEARCH funding, PROGRAMMED death-ligand 1, ANTINEOPLASTIC agents, COLORECTAL cancer, DESCRIPTIVE statistics, MONOCLONAL antibodies, ANTIVIRAL agents, MICE, ONCOGENES, DRUG interactions, ANIMAL experimentation, PRIMATES

Abstract

Simple Summary: Viral infection poses cancer risk and the PD-1/PD-L1 immune check point plays a critical role in this process. Despite the success of the existing anti-PD-1 and PD-L1 antibodies, significant challenges remain due to drug resistance and serious side effects. We have developed a novel anti-PD-1 antibody P1801 which has significant PD-1 blocking and antitumor activities. It displayed unique binding properties distinctive from pembrolizumab and nivolumab with limited ADCC- and CDC-mediated lysis of normal immune cells. We are initiating a Phase 1 clinical study to test its combination use with ropeginterferon alfa-2b, a new-generation interferon-alfa-based therapy which also has antiviral and antitumor activities, for the treatment of cancer. Programmed cell death 1 (PD-1) and programmed death-ligand 1 (PD-L1) interact to form an immune checkpoint fostering viral infection and viral oncogene-induced tumorigenesis. We generated a novel anti-human PD-1, humanized monoclonal antibody P1801 and investigated its pharmacologic, pharmacokinetic (PK), and pharmacodynamic properties. In vitro binding assays revealed that P1801 uniquely binds to human PD-1 and inhibits its interaction with PD-L1/2. It showed a minor effect on the induction of antibody-dependent cell-mediated cytotoxicity (ADCC) and complement-dependent cytotoxicity (CDC). P1801 significantly induced the release of IL-2 from activated T-cells but not from nonactivated T-cells. A dose-dependent linear PK profile was observed for the cynomolgus monkeys treated with repeated doses of P1801 at 5 mg/kg to 200 mg/kg once weekly. A four-week repeat-dose toxicity study revealed that P1801 given weekly was safe and well tolerated at doses ranging from 5 to 200 mg/kg/dose. No pathological abnormalities were noted. In humanized PD-1 mice harboring human PD-L1-expressing colon tumor cells, P1801 administered intraperitoneally twice per week at 12 mg/kg significantly inhibited tumor growth and prolonged mouse survival. P1801 displayed unique binding properties different from pembrolizumab and nivolumab. Therefore, it showed distinctive immunological reactions and significant antitumor activities. We are initiating a Phase 1 clinical study to test its combination use with ropeginterferon alfa-2b, which also has antiviral and antitumor activities, for the treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2024

32. Opportunities and Challenges of Small Molecule Inhibitors in Glioblastoma Treatment: Lessons Learned from Clinical Trials.

Author

Hoosemans, Linde, Vooijs, Marc, and Hoeben, Ann

Subjects

THERAPEUTIC use of antineoplastic agents, COMBINATION drug therapy, GLIOMAS, DRUG resistance in cancer cells, CLINICAL trials, ANTINEOPLASTIC agents, SMALL molecules, CANCER chemotherapy, TUMOR suppressor genes, ONCOGENES, TREATMENT failure, CARCINOGENESIS, DRUG discovery, EVALUATION, PHARMACODYNAMICS

Abstract

Simple Summary: Glioblastoma is the most common brain tumour, with a poor prognosis of about 15 months despite intensive treatment. Many trials have tested new drugs targeting specific genes, but none have succeeded, and treatments have not changed since 2005. This review explores why clinical trials with these drugs failed. It highlights the potential of combining different drugs to overcome resistance and suggests ways to improve future trials. The goal is to understand treatment failures and find new drug combinations to improve survival for GBM patients. Glioblastoma (GBM) is the most prevalent central nervous system tumour (CNS). Patients with GBM have a dismal prognosis of 15 months, despite an intensive treatment schedule consisting of surgery, chemoradiation and concurrent chemotherapy. In the last decades, many trials have been performed investigating small molecule inhibitors, which target specific genes involved in tumorigenesis. So far, these trials have been unsuccessful, and standard of care for GBM patients has remained the same since 2005. This review gives an overview of trials investigating small molecule inhibitors on their own, combined with chemotherapy or other small molecule inhibitors. We discuss possible resistance mechanisms in GBM, focussing on intra- and intertumoral heterogeneity, bypass mechanisms and the influence of the tumour microenvironment. Moreover, we emphasise how combining inhibitors can help overcome these resistance mechanisms. We also address strategies for improving trial outcomes through modifications to their design. In summary, this review aims to elucidate different resistance mechanisms against small molecule inhibitors, highlighting their significance in the search for novel therapeutic combinations to improve the overall survival of GBM patients. [ABSTRACT FROM AUTHOR]

Published

2024

33. Retrieval of the Clipped Axillary Lymph Node and Its Impact on Treatment Decisions.

Author

Detz Jr., David, Hanssen, Diego, Whiting, Junmin, Sun, Weihong, Czerniecki, Brian, Hoover, Susan, Khakpour, Nazanin, Kiluk, John, Laronga, Christine, Mallory, Melissa, Lee, M. Catherine, and Kruper, Laura

Subjects

BREAST tumor treatment, SENTINEL lymph node biopsy, BREAST tumors, AXILLARY lymph node dissection, DECISION making in clinical medicine, CANCER patients, DESCRIPTIVE statistics, METASTASIS, CANCER chemotherapy, COMBINED modality therapy, ONCOGENES

Abstract

Simple Summary: Around 30% of breast cancer patients have axillary lymph node metastases present at the time of diagnosis. Historically, axillary lymph node dissection was performed in these patients with significant morbidity associated with the procedure including permanent lymphedema. These patients are now often treated with neoadjuvant chemotherapy to attempt to downstage the axilla and avoid axillary lymph node dissection. To reduce the false negative rate of a sentinel lymph node biopsy, a targeted axillary dissection is often performed to ensure that biopsy-proven metastatic axillary nodes are removed. The aim of our study was to determine how often the clipped node was also a sentinel lymph node, to identify factors that were associated with pathologic complete response following neoadjuvant chemotherapy, and to assess how the clipped node impacted final treatment decisions. These findings aim to help understand and guide surgeons on axillary evaluation after neoadjuvant chemotherapy. We examined clinically node-positive (cN+) breast cancer patients undergoing neoadjuvant chemotherapy and clipped lymph node (CLN) localization to determine the rate of CLN = non-sentinel lymph node (SLN), the factors associated with cN+ to pN0 conversion, and the treatment impact. We conducted a single institution review of cN+ patients receiving NAC from 2016 to 2022 with preoperative CLN localization (N = 81). Demographics, hormone receptor (HR) and HER2 status, time to surgery, staging, chemotherapy regimen, localization method, pathology, and adjuvant therapy were analyzed. Pathologic complete response (pCR) of the CLN was observed in 41 patients (50.6%): 18.8% HR+/HER2−, 75% HR+/HER2+, 75% HR−/HER2+, and 62.5% triple-negative breast cancer (p-value = 0.006). CLN = SLN in 68 (84%) patients, while CLN = non-SLN in 13 (16%). In 14 (17.3%) patients, the final treatment was altered based on +CLN status: 11 patients underwent axillary lymph node dissection (ALND), and 3 had systemic treatment changes. pCR rates varied, with the highest conversion rates observed in HER2+ disease and the lowest in HR+/HER2− disease. In 2 (2.5%) patients, adjuvant therapy changes were made based on a non-sentinel CLN, while in 97.5% of patients, a SLN biopsy alone represented the status of the axilla. This demonstrates that a +CLN often alters final plans and that, despite also being a SLN in most cases, a subset of patients will be undertreated by SLN biopsy alone. [ABSTRACT FROM AUTHOR]

Published

2024

34. The Impact of Pembrolizumab as a Salvage Therapy Based on HER2 Expression in Advanced Gastric Cancer.

Author

Lim, Sung Hee, Kim, Min Jung, Lee, Jeeyun, Lim, Ho Yeong, Kang, Won Ki, and Kim, Seung Tae

Subjects

STOMACH tumors, SALVAGE therapy, IMMUNE checkpoint inhibitors, GENE expression, IMMUNOHISTOCHEMISTRY, KAPLAN-Meier estimator, ONCOGENES, DRUG efficacy, SURVIVAL analysis (Biometry), PROGRESSION-free survival, DISEASE progression, PHARMACODYNAMICS

Abstract

Simple Summary: This study evaluated the effectiveness of salvage pembrolizumab in advanced gastric cancer (AGC) patients based on HER2 expression. Conducted at Samsung Medical Center from November 2017 to March 2023, it involved 113 patients treated with pembrolizumab. Twelve patients (10.6%) were HER2-positive, and 101 were HER2-negative. Results showed no complete responses among 92 evaluable patients. However, 50% of HER2-positive patients had a partial response compared to 4.9% of HER2-negative patients (p < 0.001). Disease control rates were 70% for HER2-positive and 37.8% for HER2-negative patients (p = 0.086). Median progression-free survival was 5.53 months for HER2-positive patients versus 1.81 months for HER2-negative patients (p = 0.037). This indicates that salvage pembrolizumab monotherapy is more effective in HER2-positive AGC patients. Immune checkpoint inhibitors (ICIs) are used as salvage treatments for advanced gastric cancer (AGC) regardless of HER2 status. This study assessed the efficacy of ICIs based on HER2 expression in AGC patients who received pembrolizumab as salvage monotherapy at Samsung Medical Center from November 2017 to March 2023. HER2 status was determined via immunohistochemistry, and tumor response and survival outcomes were compared accordingly. Among the 113 patients analyzed, with a median age of 61 years and 64.6% being male, 12 patients (10.6%) were HER2-positive, and 101 patients (89.4%) were HER2-negative. Of 92 evaluable patients, none had a complete response. However, 50% of HER2-positive patients had a partial response, compared to 4.9% of HER2-negative patients (p < 0.001). The disease control rate was 70% in HER2-positive and 37.8% in HER2-negative patients (p = 0.086). Median progression-free survival was 5.53 months for HER2-positive patients versus 1.81 months for HER2-negative patients (p = 0.037). Pembrolizumab as a salvage chemotherapy for the treatment of AGC demonstrated superior effectiveness in HER2-positive patients compared with HER2-negative patients. [ABSTRACT FROM AUTHOR]

Published

2024

35. Real-World Cardiotoxicity in Metastatic Melanoma Patients Treated with Encorafenib and Binimetinib.

Author

Pedersen, Sidsel, Nielsen, Marc Østergaard, Donia, Marco, Svane, Inge Marie, Zerahn, Bo, and Ellebaek, Eva

Subjects

HEART physiology, MITOGEN-activated protein kinases, RISK assessment, MELANOMA, PATIENT safety, RESEARCH funding, ANTINEOPLASTIC agents, CANCER patients, RETROSPECTIVE studies, TREATMENT duration, DESCRIPTIVE statistics, METASTASIS, DRUG monitoring, CARDIOTOXICITY, CARDIAC radionuclide imaging, ONCOGENES, MEDICAL records, ACQUISITION of data, TRANSFERASES, GENETIC mutation, CHEMICAL inhibitors

Abstract

Simple Summary: Targeted therapies with BRAF- and MEK-inhibitors have significantly improved outcomes for patients with metastatic melanoma, but they come with a risk of heart-related side effects. This study included 108 real-world patients with metastatic melanoma from Eastern Denmark from 2019–2022 treated with encorafenib and binimetinib. Heart function was monitored with MUGA scans at baseline and every three months. While 18% of the patients experienced minor heart issues without symptoms, only 6% faced major problems, some needing medical intervention. However, no severe heart issues occurred beyond six months of starting the treatment. This suggests that it might be safe to reduce heart monitoring after six to nine months if no issues appear early on. Modern therapies targeting the BRAF gene mutation in advanced melanoma have significantly improved patient outcomes but pose cardiovascular risks. This retrospective study in Eastern Denmark (2019–2022) assessed 108 melanoma patients treated with encorafenib and binimetinib. Patients were monitored for heart function using multigated acquisition (MUGA) scans. The study defined major cardiotoxicity as a decline in left ventricular ejection fraction (LVEF) by more than 10 percentage points to below 50%, and minor cardiotoxicity as a decrease in LVEF by more than 15 points but remaining above 50%. Results showed that 19 patients (18%) developed minor cardiotoxicity and were asymptomatic, while 7 (6%) experienced major cardiotoxicity, with two requiring intervention. Notably, no significant declines in LVEF were observed after six months of treatment. The study concluded that significant cardiotoxicity occurred in 6% of cases, mostly asymptomatic and reversible, and suggests that monitoring LVEF could potentially be reduced after 6–9 months if no early signs of cardiotoxicity are detected. This provides valuable insights into the cardiac safety of these treatments in real-world settings. [ABSTRACT FROM AUTHOR]

Published

2024

36. KIF2C/MCAK a prognostic biomarker and its oncogenic potential in malignant progression, and prognosis of cancer patients: a systematic review and meta-analysis as biomarker.

Author

Kreis, Nina-Naomi, Moon, Ha Hyung, Wordeman, Linda, Louwen, Frank, Solbach, Christine, Yuan, Juping, and Ritter, Andreas

Subjects

TUMOR diagnosis, TUMOR genetics, RESEARCH funding, CELL physiology, TUMOR markers, META-analysis, CANCER patients, SYSTEMATIC reviews, GENE expression, ONCOGENES, CELL death, KINESIN, TUMORS, PROGRESSION-free survival, DISEASE progression, GENOMES, OVERALL survival

Abstract

KIF2C/MCAK (KIF2C) is the most well-characterized member of the kinesin-13 family, which is critical in the regulation of microtubule (MT) dynamics during mitosis, as well as interphase. This systematic review briefly describes the important structural elements of KIF2C, its regulation by multiple molecular mechanisms, and its broad cellular functions. Furthermore, it systematically summarizes its oncogenic potential in malignant progression and performs a meta-analysis of its prognostic value in cancer patients. KIF2C was shown to be involved in multiple crucial cellular processes including cell migration and invasion, DNA repair, senescence induction and immune modulation, which are all known to be critical during the development of malignant tumors. Indeed, an increasing number of publications indicate that KIF2C is aberrantly expressed in multiple cancer entities. Consequently, we have highlighted its involvement in at least five hallmarks of cancer, namely: genome instability, resisting cell death, activating invasion and metastasis, avoiding immune destruction and cellular senescence. This was followed by a systematic search of KIF2C/MCAK's expression in various malignant tumor entities and its correlation with clinicopathologic features. Available data were pooled into multiple weighted meta-analyses for the correlation between KIF2Chigh protein or gene expression and the overall survival in breast cancer, non-small cell lung cancer and hepatocellular carcinoma patients. Furthermore, high expression of KIF2C was correlated to disease-free survival of hepatocellular carcinoma. All meta-analyses showed poor prognosis for cancer patients with KIF2Chigh expression, associated with a decreased overall survival and reduced disease-free survival, indicating KIF2C's oncogenic potential in malignant progression and as a prognostic marker. This work delineated the promising research perspective of KIF2C with modern in vivo and in vitro technologies to further decipher the function of KIF2C in malignant tumor development and progression. This might help to establish KIF2C as a biomarker for the diagnosis or evaluation of at least three cancer entities. [ABSTRACT FROM AUTHOR]

Published

2024

37. High-grade B-cell lymphoma with a quadruple-hit genetic profile including concurrent MYC, BCL2, BCL6, and CCND1 gene rearrangements.

Author

Gagnon, Marie-France, Meyer, Reid G, Weaver, Eric J, Wood, Adam J, Dupuy, Dudley A, Menachery, Sudeep J, Shi, Min, Baughn, Linda B, Ketterling, Rhett P, and Peterson, Jess F

Subjects

PROTEIN metabolism, FLOW cytometry, GENE rearrangement, RARE diseases, GENE expression, ONCOGENES, FLUORESCENCE in situ hybridization, B cell lymphoma, GENETIC profile, PHENOTYPES

Abstract

Several reports of concurrent MYC , BCL2 , BCL6 , and CCND1 rearrangements in high-grade B-cell lymphoma (HGBL) have been recently described. Herein, we aimed to delineate the scope of this entity through a review of HGBL with a "quadruple-hit" genetic profile identified at our institution. We performed a retrospective review (2015-2023) at our institution of B-cell lymphoma (BCL) cases that were evaluated with concurrent MYC , BCL2 , and BCL6 break-apart and IGH::MYC and IGH::CCND1 dual-color dual-fusion fluorescence in situ hybridization studies. Of 203 cases meeting inclusion criteria, 2 (1%) with a quadruple-hit genetic profile were identified. Case 1 represented a 59-year-old female with widespread lymphadenopathy and a diagnosis of HGBL who exhibited primary refractoriness to dose-adjusted etoposide, prednisone, vincristine, cyclophosphamide, doxorubicin, and rituximab (DA-EPOCH-R) chemotherapy. Case 2 represented a 58-year-old male with mediastinal and abdominal lymphadenopathy and a diagnosis of large BCL who died from disease after 1 cycle of DA-EPOCH-R chemotherapy. Similarly, a literature review of 7 previously reported cases of HGBL with a quadruple-hit profile also demonstrated aggressive disease behavior. Our study adds 2 new cases to the rarely encountered quadruple-hit HGBL, and a brief meta-analysis of the 9 available cases indicates aggressive disease behavior conferred by this constellation of genetic events. [ABSTRACT FROM AUTHOR]

Published

2024

38. Multiregion exome sequencing indicates a monoclonal origin of esophageal spindle‐cell squamous cell carcinoma.

Author

Wang, Yulu, Zhu, Qian, Wu, Yaqing, Li, Boyi, Su, Xiaoxing, Xiang, Chan, and Han, Yuchen

Subjects

SQUAMOUS cell carcinoma, CHROMOSOMES, ONCOGENES, CELLULAR signal transduction, MICRODISSECTION

Abstract

Esophageal spindle‐cell squamous cell carcinoma (ESS) is a rare biphasic neoplasm composed of a carcinomatous component (CaC) and a sarcomatous component (SaC). However, the genomic origin and gene signature of ESS remain unclear. Using whole‐exome sequencing of laser‐capture microdissection (LCM) tumor samples, we determined that CaC and SaC showed high mutational commonality, with the same top high‐frequency mutant genes, mutation signatures, and tumor mutation burden; paired samples shared a median of 25.5% mutation sites. Focal gains were found on chromosomes 3q29, 5p15.33, and 11q13.3. Altered genes were mainly enriched in the RTK–RAS signaling pathway. Phylogenetic trees showed a monoclonal origin of ESS. The most frequently mutated oncogene in the trunk was TP53, followed by NFE2L2, KMT2D, and MUC16. Prognostic associations were found for CDC27, LRP2, APC, and SNAPC4. Our data highlight the monoclonal origin of ESS with TP53 as a potent driver oncogene, suggesting new targeted therapies and immunotherapies as treatment options. © 2024 The Pathological Society of Great Britain and Ireland. [ABSTRACT FROM AUTHOR]

Published

2024

39. Targeting KRAS in pancreatic cancer.

Author

STICKLER, SANDRA, RATH, BARBARA, and HAMILTON, GERHARD

Subjects

RAS oncogenes, PANCREATIC cancer, PANCREATIC duct, LUNG cancer, ONCOGENES

Abstract

Pancreatic cancer has a dismal prognosis due to late detection and lack of efficient therapies. The Kirsten rat sarcoma virus (KRAS) oncogene is mutated in up to 90% of all pancreatic ductal adenocarcinomas (PDACs) and constitutes an attractive target for therapy. However, the most common KRAS mutations in PDAC are G12D (44%), G12V (34%) and G12R (20%) that are not amenable to treatment by KRAS G12C-directed cysteine-reactive KRAS inhibitors such as Sotorasib and Adagrasib that exhibit clinical efficacy in lung cancer. KRAS G12C mutant pancreatic cancer has been treated with Sotorasib but this mutation is detected only in 2%-3% of PDAC. Recently, the KRAS G12D-directed MRTX1133 inhibitor has entered clinical trials and more of such inhibitors are in development. The other KRAS mutations may be targeted indirectly via inhibition of the cognate guanosine exchange factor (GEF) Son of Sevenless 1 that drives KRAS. These agents seem to provide the means to target the most frequent KRAS mutations in PDAC and to improve patient outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

40. The role of tazarotene-induced gene 1 in carcinogenesis: is it a tumor suppressor gene or an oncogene?

Author

WANG, CHUN-HUA, WANG, LU-KAI, SHYU, RONG-YAUN, and TSAI, FU-MING

Subjects

TUMOR suppressor genes, GENE expression, CANCER cell growth, ONCOGENES, CANCER genes, VITAMIN A

Abstract

Tazarotene-induced gene 1 (TIG1) is induced by a derivative of vitamin A and is known to regulate many important biological processes and control the development of cancer. TIG1 is widely expressed in various tissues; yet in many cancer tissues, it is not expressed because of the methylation of its promoter. Additionally, the expression of TIG1 in cancer cells inhibits their growth and invasion, suggesting that TIG1 acts as a tumor suppressor gene. However, in some cancers, poor prognosis is associated with TIG1 expression, indicating its protumor growth characteristics, especially in promoting the invasion of inflammatory breast cancer cells. This review comprehensively summarizes the roles of the TIG1 gene in cancer development and details the mechanisms through which TIG1 regulates cancer development, with the aim of understanding its various roles in cancer development. [ABSTRACT FROM AUTHOR]

Published

2024

41. Complete response to capmatinib in a patient with metastatic lung adenocarcinoma harboring CD47-MET fusion: a case report.

Author

Souza, Glaucia Alves de, Dornellas, Debora Maciel Santana, Campregher, Paulo Vidal, Teixeira, Carlos Henrique Andrade, and Schvartsman, Gustavo

Subjects

THERAPEUTIC use of antineoplastic agents, ADENOCARCINOMA, IMMUNOTHERAPY, WHITE people, METASTASIS, CANCER chemotherapy, GENETIC variation, ONCOGENES, LUNG cancer, TRANSFERASES, SEQUENCE analysis

Abstract

Comprehensive genomic profiling is highly recommended for treatment decision in nonsquamous, non-small cell lung cancer (NSCLC). However, rare genomic alterations are still being unveiled, with scarce data to guide therapy. Herein, we describe the treatment journey of a 56-year-old, never-smoker Caucasian woman with a metastatic NSCLC harboring a CD47-MET fusion, initially classified as a variant of unknown significance. She had undergone 3 lines of therapy over the course of 3 years, including chemotherapy, immunotherapy, and anti-angiogenic therapy. After reanalysis of her next-generation sequencing data in our service, the fusion was reclassified as likely oncogenic. The patient was started with fourth-line capmatinib, with a good tolerance so far and a complete metabolic response in the active sites of disease, currently ongoing for 18 months. In conclusion, we highlight the sensitivity of a novel MET fusion to capmatinib and emphasize the need for comprehensive panels in NSCLC and molecular tumor board discussions with specialized centers when rare findings arise. [ABSTRACT FROM AUTHOR]

Published

2024

42. Adjuvant treatment strategy evolution and risk stratification for hormone receptor-positive, human epidermal growth factor receptor-2 negative early breast cancer in China.

Author

Fan, Ying, Ji, Danyang, Jiang, Mingxia, Tan, Yujing, Yang, Yang, Li, Tianyi, Ma, Xiao, and Xu, Binghe

Subjects

BREAST cancer prognosis, BREAST tumor risk factors, MORTALITY risk factors, RISK assessment, AROMATASE inhibitors, HORMONE receptor positive breast cancer, CANCER relapse, RESEARCH funding, ADJUVANT treatment of cancer, EARLY detection of cancer, CHEMORADIOTHERAPY, EVALUATION of medical care, DESCRIPTIVE statistics, LONGITUDINAL method, ONCOGENES, CONFIDENCE intervals, PROGRESSION-free survival, EPIDERMAL growth factor receptors, DISEASE risk factors

Abstract

Background Patients with hormone receptor-positive (HR+), human epidermal growth factor receptor-2 negative (HER2−) early breast cancer (EBC) with high-risk clinicopathological features face an increased risk of recurrence. This study explored the evolving treatment landscape and clinical outcomes in patients with EBC using a nationwide database. Patients and Methods The study cohort comprised HR+/HER2−, stages 1-3, patients with EBC who underwent surgery and received adjuvant endocrine therapy (AET) from January 2013 to March 2021. High-risk patients were defined by ≥4 positive axillary lymph nodes, or 1-3 positive lymph node(s) with at least one high-risk feature (histologic grade 3, tumor size ≥5 cm, or Ki-67 ≥20%). A low-risk cohort included patients not meeting the criteria. Survival analysis was conducted with a cutoff of September 2021. Results The study included 4088 eligible patients (1310 high-risk patients and 2778 low-risk patients). High-risk patients were more likely to receive adjuvant chemotherapy and radiotherapy compared to low-risk patients. From 2013 to 2021, an increasing proportion of patients received aromatase inhibitors and ovarian function suppression as part of their AET. The 2-, 5-, and 7-year invasive disease-free survival for high-risk cohort were 90.67%, 75.26%, and 57.10%, respectively, these rates were notably higher for low-risk cohort at 97.14%, 89.85%, and 84.83%. High-risk patients demonstrated a higher risk of recurrence or death compared with low-risk patients (hazard ratio, 2.38; 95% CI, 1.82-3.12). Conclusion In the setting of standard or even intensive AET, patients with EBC with high-risk features still present high recurrence risk, highlighting the urgent need for innovative adjuvant treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2024

43. Phase II clinical trial of docetaxel and trastuzumab for HER2-positive advanced extramammary Paget's disease (EMPD-HER2DOC).

Author

Hirai, Ikuko, Tanese, Keiji, Nakamura, Yoshio, Fukuda, Keitaro, Ouchi, Takeshi, Hayashida, Tetsu, Kameyama, Kaori, Abe, Takayuki, Amagai, Masayuki, and Funakoshi, Takeru

Subjects

THERAPEUTIC use of antineoplastic agents, DOCETAXEL, ADENOCARCINOMA, COMMUNICABLE diseases, TRASTUZUMAB, PATIENT safety, RESEARCH funding, SKIN diseases, CLINICAL trials, ANTINEOPLASTIC agents, DESCRIPTIVE statistics, GENE expression, METASTASIS, INTRAVENOUS therapy, LONGITUDINAL method, CANCER chemotherapy, ONCOGENES, DRUG efficacy, CONFIDENCE intervals, EPIDERMAL growth factor receptors, NEUTROPENIA, SERUM albumin, EVALUATION

Abstract

Background No consensus has been reached regarding the optimal chemotherapy for metastatic extramammary Paget's disease (EMPD), a rare cutaneous adenocarcinoma, because of the lack of solid evidence from prospective trials. However, the immunohistochemical profile of EMPD reportedly resembles that of breast cancer, particularly in terms of human epidermal growth factor receptor 2 (HER2) expression, suggesting that HER2 is a promising therapeutic target for advanced HER2-positive EMPD. Methods In this phase II single-arm trial, 13 Japanese patients received intravenous trastuzumab (loading dose of 8 mg/kg and maintenance dose of 6 mg/kg) and docetaxel (75 mg/m2) every 3 weeks for up to 2 years. The docetaxel dose was reduced or discontinued according to its toxicity. The primary trial endpoints were objective response rate (ORR) after 3 cycles of treatment and safety throughout the study period. Results All 13 patients completed 3 cycles of combination therapy. The median follow-up was 27.9 months. The ORR was 76.9% (n = 10/13; 90% CI, 50.5-93.4). Frequently observed adverse events were neutropenia (100%), hypoalbuminemia (84.6%), and mucocutaneous infection (84.6%), all of which were well tolerated. Conclusion The combination of docetaxel and trastuzumab demonstrated a favorable clinical effect and acceptable tolerability, which makes it a good treatment option for HER2-positive metastatic EMPD (ClinicalTrials.gov Identifier: UMIN000021311, jRCTs031180073). [ABSTRACT FROM AUTHOR]

Published

2024

44. Exploring a Novel Approach to Spare Classic Chemotherapy in HER2-Low, ER-Positive Breast Cancer Based on Trastuzumab Deruxtecan Combined with Endocrine Therapy.

Author

Scafuri, Luca, Buonerba, Carlo, Di Lauro, Vincenzo, Tortora, Vincenzo, Cascella, Marco, Liguori, Luigi, Sciarra, Antonella, Sabbatino, Francesco, Diana, Anna, Marra, Antonio, Tarantino, Paolo, Trapani, Dario, Giuliano, Mario, Arpino, Grazia, Curigliano, Giuseppe, and Di Lorenzo, Giuseppe

Subjects

THERAPEUTIC use of antineoplastic agents, TRASTUZUMAB, HORMONE receptor positive breast cancer, CLINICAL trials, TREATMENT effectiveness, COMBINED modality therapy, ONCOGENES, HORMONE therapy, DRUG efficacy

Abstract

Background: Breast cancer presents diverse molecular subtypes affecting treatment strategies. Human epidermal growth factor receptor 2 (HER2)-low, hormone receptor-positive (HR+) breast cancer poses a challenge due to limited targeted therapies. Current neoadjuvant treatment primarily utilizes chemotherapy, with conflicting results regarding efficacy in patients with HER2-low breast cancer. Trastuzumab deruxtecan (T-DXd) shows promise in HER2-low metastatic disease, and preliminary evidence suggests synergy with endocrine therapy. Objective: This editorial explores the hypothesis that neoadjuvant T-DXd with or without endocrine therapy offers efficacy in the clinical management of HR+/HER2-low breast cancer. Methods: We propose a phase II study with two treatment arms: T-DXd + letrozole and T-DXd alone. The primary endpoint is the radiological complete response rate. Secondary endpoints include pathological complete response rate, safety, event-free survival, and overall survival. Exploratory analyses will compare the arms to identify potential for optimizing treatment efficacy and minimizing side effects. Conclusions: This study design allows for initial assessment of T-DXd with or without endocrine therapy in the treatment of HER2-low breast cancer. The findings may pave the way for personalized treatment strategies and inform future research, potentially leading to a chemotherapy-sparing approach. [ABSTRACT FROM AUTHOR]

Published

2024

45. Cisplatin Monotherapy as a Treatment Option for Patients with HER-2 Negative Breast Cancer Experiencing Hepatic Visceral Crisis or Impending Visceral Crisis.

Author

Püsküllüoğlu, Mirosława, Pieniążek, Małgorzata, Rudzińska, Agnieszka, Pietruszka, Agnieszka, Pacholczak-Madej, Renata, Grela-Wojewoda, Aleksandra, and Ziobro, Marek

Subjects

BREAST cancer prognosis, HYPERBILIRUBINEMIA, CISPLATIN, BREAST tumors, LOGISTIC regression analysis, TREATMENT effectiveness, RETROSPECTIVE studies, DESCRIPTIVE statistics, CANCER patients, LONGITUDINAL method, CANCER chemotherapy, ODDS ratio, METASTASIS, ONCOGENES, DRUG efficacy, MEDICAL records, ACQUISITION of data, STATISTICS, CONFIDENCE intervals, PROGRESSION-free survival, EPIDERMAL growth factor receptors, OVERALL survival

Abstract

Introduction: Hepatic visceral crisis (VC), characterized by a rapid total bilirubin increase with disease progression, poses a life-threatening risk in advanced breast cancer (ABC). International consensus guidelines define VC and touch on impending VC (IVC). Limited data exist on systemic treatments for hepatic VC/IVC. This study explores the safety and efficacy of cisplatin monotherapy in patients with Human Epidermal Growth Factor Receptor 2- negative breast cancer (BC) and hepatic IVC/VC. Methods: In this retrospective single-center cohort study data of patients treated with cisplatin monotherapy (60–80 mg/m2, every 3–4 weeks) between 2016 and 2023 at a reference Cancer Centre in Southern Poland were analyzed. Results: 33 female patients (24/33 hormonal-positive) with the mean age 53.84 years were included. Participants progressed on median 2 prior palliative systemic treatment lines. In 10/23 patients hepatic VC and in 23/33 IVC (rapid, symptomatic liver progression; extensive liver involvement; alanine or aspartate aminotransferase > 2 × normal limit; significant increases in lactate dehydrogenase, alkaline phosphatase, or gamma-glutamyl transferase) were identified. Median progression-free survival was 1.87 months and median overall survival 2.67 months. 33% of the patients presented stable disease or partial response. Eight patients experienced adverse events grade ≥ 3: in five the dose of cisplatin was reduced; two stopped the treatment. Conclusion: Due to the hepatotoxicity of BC-active drugs, specific recommendations for systemic treatment are scarce. Our study explored cisplatin's potential use, finding it to be a viable option in patients with performance status 0 or 1 experiencing hepatic IVC/VC, irrespective of liver function parameters and other factors. [ABSTRACT FROM AUTHOR]

Published

2024

46. Clinical Characteristics of Children with Nasal BCOR-Rearranged Ewing-like Sarcoma: A Case Report and Literature Review.

Author

Ji, Tingting, Li, Xiaodan, Li, Yanzhen, Zhang, Xuexi, Liu, Qiaoyin, Zhang, Jie, Sun, Nian, Liu, Zhiyong, Liu, Yuwei, Wang, Shengcai, and Ni, Xin

Subjects

NASAL surgery, NASAL cavity, IMMUNOPHENOTYPING, GENE rearrangement, COMPUTED tomography, SYMPTOMS, NASAL tumors, MAGNETIC resonance imaging, ULTRASONIC imaging, NOSE, CANCER chemotherapy, NEEDLE biopsy, ONCOGENES, EWING'S sarcoma, SOFT tissue tumors, CARTILAGE, STAINS & staining (Microscopy), MOLECULAR pathology, CHILDREN

Abstract

Ewing-like sarcomas (ELS) are round cell mesenchymal neoplasms that are highly aggressive to bone and/or soft tissue. However, they rarely occur in the nose, with no reported such cases in the medical literature to date. Here, we reported the case of a two-year-old Chinese boy who presented with a mass in the left nasal cavity. Surprisingly, the final histopathological diagnosis of the nasal mass was determined to be a subtype of ELS, BCOR -rearranged sarcoma. Therefore, we retrospectively analyzed the clinical data of this case and reviewed the relevant literature on ELS and BCOR -rearranged sarcoma. The purpose of this article is to provide new insights into the clinical characteristics of children with BCOR -rearranged Ewing-like sarcoma and to improve the understanding of this disease. [ABSTRACT FROM AUTHOR]

Published

2024

47. Silencing of the long non-coding RNA LINC00265 triggers autophagy and apoptosis in lung cancer by reducing protein stability of SIN3A oncogene.

Author

HUANG, XIAOBI, CHEN, CHUNYUAN, CHEN, YONGYANG, ZHOU, HONGLIAN, CHEN, YONGHUA, HUANG, ZHONG, XIE, YULIU, LIU, BAIYANG, GUO, YUDONG, YANG, ZHIXIONG, CHEN, GUANGHUA, and SU, WENMEI

Subjects

LINCRNA, PROTEIN stability, LUNG cancer, AUTOPHAGY, ONCOGENES

Abstract

Background: Long non-coding RNAs are important regulators in cancer biology and function either as tumor suppressors or as oncogenes. Their dysregulation has been closely associated with tumorigenesis. LINC00265 is upregulated in lung adenocarcinoma and is a prognostic biomarker of this cancer. However, the mechanism underlying its function in cancer progression remains poorly understood. Methods: Here, the regulatory role of LINC00265 in lung adenocarcinoma was examined using lung cancer cell lines, clinical samples, and xenografts. Results: We found that high levels of LINC00265 expression were associated with shorter overall survival rate of patients, whereas knockdown of LINC00265 inhibited proliferation of cancer cell lines and tumor growth in xenografts. Western blot and flow cytometry analyses indicated that silencing of LINC00265 induced autophagy and apoptosis. Moreover, we showed that LINC00265 interacted with and stabilized the transcriptional co-repressor Switch-independent 3a (SIN3A), which is a scaffold protein functioning either as a tumor repressor or as an oncogene in a context-dependent manner. Silencing of SIN3A also reduced proliferation of lung cancer cells, which was correlated with the induction of autophagy. These observations raise the possibility that LINC00265 functions to promote the oncogenic activity of SIN3A in lung adenocarcinoma. Conclusions: Our findings thus identify SIN3A as a LINC00265-associated protein and should help to understand the mechanism underlying LINC00265-mediated oncogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

48. RAS-ON inhibition overcomes clinical resistance to KRAS G12C-OFF covalent blockade.

Author

Nokin, Marie-Julie, Mira, Alessia, Patrucco, Enrico, Ricciuti, Biagio, Cousin, Sophie, Soubeyran, Isabelle, San José, Sonia, Peirone, Serena, Caizzi, Livia, Vietti Michelina, Sandra, Bourdon, Aurelien, Wang, Xinan, Alvarez-Villanueva, Daniel, Martínez-Iniesta, María, Vidal, August, Rodrigues, Telmo, García-Macías, Carmen, Awad, Mark M., Nadal, Ernest, and Villanueva, Alberto

Subjects

NON-small-cell lung carcinoma, PATIENT compliance, RAS oncogenes, ONCOGENES, DISEASE progression

Abstract

Selective KRASG12C inhibitors have been developed to covalently lock the oncogene in the inactive GDP-bound state. Two of these molecules, sotorasib and adagrasib, are approved for the treatment of adult patients with KRASG12C-mutated previously treated advanced non-small cell lung cancer. Drug treatment imposes selective pressures leading to the outgrowth of drug-resistant variants. Mass sequencing from patients' biopsies identified a number of acquired KRAS mutations -both in cis and in trans- in resistant tumors. We demonstrate here that disease progression in vivo can also occur due to adaptive mechanisms and increased KRAS-GTP loading. Using the preclinical tool tri-complex KRASG12C-selective covalent inhibitor, RMC-4998 (also known as RM-029), that targets the active GTP-bound (ON) state of the oncogene, we provide a proof-of-concept that the clinical stage KRASG12C(ON) inhibitor RMC-6291 alone or in combination with KRASG12C(OFF) drugs can be an alternative potential therapeutic strategy to circumvent resistance due to increased KRAS-GTP loading. KRAS G12C mutant selective inhibitors targeting inactive state have been approved for use in non-small cell lung cancer (NSCLC). Here, using models derived from a patient with NSCLC who progressed on sotorasib (KRAS G12C inhibitor), the authors identify increased KRAS GTP loading as an adaptive resistance mechanism which could be targeted with KRAS G12C inhibitors selective to the GTP active state. [ABSTRACT FROM AUTHOR]

Published

2024

49. Neoadjuvant BRAF and MEK inhibitor therapy elicits pathological complete response in stage IIIA non‐small cell lung cancer harboring BRAF V600E mutation: A case report.

Author

Huang, Zhicheng, Wang, Yadong, Li, Bowen, Xu, Yuan, Huang, Guanghua, Song, Yang, Li, Ji, Song, Lan, Wang, Jinhua, Wang, Rongxi, Liang, Naixin, and Li, Shanqing

Subjects

THERAPEUTIC use of antineoplastic agents, PROTEIN kinase inhibitors, PATIENT safety, DISEASE management, IMMUNOTHERAPY, COMPUTED tomography, TREATMENT effectiveness, CANCER patients, ONCOGENES, COMBINED modality therapy, DRUG efficacy, ANAPLASTIC lymphoma kinase, LUNG cancer, GENETIC mutation, TRANSFERASES, EPIDERMAL growth factor receptors

Abstract

In recent years, significant improvement has been made in the management of non‐small cell lung cancer (NSCLC), primarily driven by advances in targeted therapy and immunotherapy. Research on neoadjuvant targeted therapy has also experienced considerable development, primarily directed towards NSCLC harboring epidermal growth factor receptor or anaplastic lymphoma kinase mutations. Nevertheless, there remains a dearth of studies investigating neoadjuvant targeted therapy in the context of BRAF (V‐Raf murine sarcoma viral oncogene homolog B) V600E mutant NSCLC. Herein, we describe the clinical trajectory of a stage IIIA NSCLC patient who underwent a two‐month course of neoadjuvant targeted therapy comprising BRAF and MEK (mitogen‐activated extracellular signal‐regulated kinase) inhibitors prior to surgical intervention, and subsequent postoperative evaluation unveiled a pathological complete response. The case reported here indicates the efficacy and safety of combining BRAF and MEK inhibitors as neoadjuvant targeted therapy in BRAF V600E‐mutant NSCLC and suggests the potential viability of such a therapeutic modality in improving treatment outcomes in this subset of NSCLC. [ABSTRACT FROM AUTHOR]

Published

2024

50. Molecular Profiling of KIT/PDGFRA -Mutant and Wild-Type Gastrointestinal Stromal Tumors (GISTs) with Clinicopathological Correlation: An 18-Year Experience at a Tertiary Center in Kuwait.

Author

Ali, Rola H., Alsaber, Ahmad R., Mohanty, Asit K., Alnajjar, Abdulsalam, Mohammed, Eiman M. A., Alateeqi, Mona, Jama, Hiba, Almarzooq, Ammar, Benobaid, Noelle, Alqallaf, Zainab, Ahmed, Amir A., Bahzad, Shakir, and Alkandari, Mohammad

Subjects

THERAPEUTIC use of antineoplastic agents, GASTROINTESTINAL tumors, RESEARCH funding, STOMACH tumors, PROTEIN-tyrosine kinase inhibitors, TERTIARY care, DESCRIPTIVE statistics, COLORECTAL cancer, RETROSPECTIVE studies, CONNECTIVE tissue tumors, ONCOGENES, GENE expression profiling, INTESTINAL tumors, MEDICAL records, ACQUISITION of data, GENETIC mutation, PERITONEUM tumors, SEQUENCE analysis, SMALL intestine, GENOTYPES, DISEASE progression, SYMPTOMS

Abstract

Simple Summary: Although gastrointestinal stromal tumor (GIST) is a relatively rare mesenchymal neoplasm of the digestive tract, molecular advancements in GISTs over the past two decades have caused a paradigm shift in the field of precision oncology. GISTs are mainly driven by activating mutations in the KIT or PDGFRA oncogenes, rendering them sensitive to targeted therapies. However, there is a significant lack of data from Kuwait that needs to be addressed. We carried out this retrospective analysis of a cohort of 200 GIST patients at the Kuwait Cancer Center to provide much-needed insights into the genetic makeup and clinicopathological characteristics of our population. We detailed the mutational spectrum in KIT and PDGFRA, identified a small subgroup of wild-type tumors, and shed some light on the clinical implications. This study opens the doors for potential larger-scale, multi-institutional outcome studies in the Arabian Gulf region. In gastrointestinal stromal tumors (GISTs), identifying prototypical mutations in the KIT/PDGFRA oncogenes, or in rare alternate genes, is essential for prognostication and predicting response to tyrosine kinase inhibitors. Conversely, wild-type GISTs (WT-GIST), which lack known mutations, have limited treatment options. Data on the mutational landscape of GISTs and their impact on disease progression are very limited in Kuwait. Using a targeted next-generation sequencing panel, we investigated the spectrum and frequency of KIT, PDGFRA, and RAS-pathway-related mutations in 95 out of 200 GISTs diagnosed at Kuwait Cancer Center from 2005 to 2023 and assessed their correlation with clinicopathological parameters. Among the 200 tumors (median age 55 years; 15–91), 54% originated in the stomach, 33% in the small bowel, 7% in the colorectum, 1.5% in the peritoneum, and 4.5% had an unknown primary site. Of the 95 molecularly profiled cases, 88% had a mutation: KIT (61%), PDGFRA (25%), NF1 (2%), and one NTRK1 rearrangement. Ten WT-GISTs were identified (stomach = 6, small bowel = 2, and colorectum = 2). WT-GISTs tended to be smaller (median 4.0 cm; 0.5–8.0) (p = 0.018), with mitosis ≤5/5 mm2, and were of lower risk (p = 0.019). KIT mutations were an adverse indicator of disease progression (p = 0.049), while wild-type status did not significantly impact progression (p = 0.934). The genetic landscape in this cohort mirrors that of global studies, but regional collaborations are needed to correlate outcomes with genetic variants. [ABSTRACT FROM AUTHOR]

Published

2024