Your search keyword '"Anticancer drugs"' showing total 4,300 results

1. Evaluation of anticancer therapy-related dermatologic adverse events: Insights from Food and Drug Administration's Adverse Event Reporting System dataset.

Author

Salah, Samir, Kerob, Delphine, Pages Laurent, Cecile, Lacouture, Mario, and Sibaud, Vincent

Abstract

New anticancer therapies have improved patient outcomes but associated dermatologic adverse events (AEs) may cause morbidity and treatment discontinuation. A comprehensive estimation of associations between cancer drugs and skin AEs is lacking. This study utilized the Food and Drug Administartion (FDA)'s Adverse Event Reporting System database (January 2013-September 2022), with 3,399,830 reports involving 3084 drugs and 16,348 AEs. A nearest neighbor matching model was employed to select 10 controls for each case report, utilizing the cosine similarity of demographic and AE severity factors to minimize false positives/negatives. There were 10,698 unique anticancer drugs (n = 212) to skin AE (n = 873) pairs, of which 676 had significant reporting odds ratios (ROR) > 1, comprising 113 drugs and 144 AEs. The minimum ROR was 1.25, and 50% of associations displayed a ROR >10. The most common were rash (51 agents) and dry skin (28 drugs). Methotrexate induced the most distinct AEs (34), then mechlorethamine (33), and vemurafenib (24). Targeted therapies accounted for 49% of pairs, cytotoxic chemotherapies for 35.9%, and immunotherapies for 11%. A total of 113 anticancer drugs were identified as significantly associated with skin AEs, most frequently rash and dry skin. Data are likely under-reported but enable quick postmarketing identification of skin toxicity signals. [ABSTRACT FROM AUTHOR]

Published

2024

2. Cytotoxicity, genotoxicity and mutagenicity of mixed ternary mononuclear Mg complex based on valproic acid with 1,10‐phenanthroline in Saccharomyces cerevisiae and V79 cells.

Author

Vanini, Julia, Rodrigues, Gabriel Berbigier, Juchem, André Luiz Mendes, Guecheva, Temenouga Nikolova, Moura, Sidnei, Dumas, Françoise, Henriques, João Antonio Pêgas, and Oliveira, Iuri Marques

Subjects

*VALPROIC acid, *CENTRAL nervous system diseases, *CYTOTOXINS, *DNA damage, *DNA repair

Abstract

Valproic acid (VA) is a widely used drug for the treatment of diseases affecting the central nervous system. Due to its epigenetic modulatory potential, it has been studied for possible therapeutic application in anticancer therapies. However, the VA exhibits different side effects in its application. Thus, synthetic coordination complexes with valproate can generate promising candidates for new active drugs with reduced toxicity. In this sense, we investigated the genotoxic and mutagenic potential of the sodium valproate and of the mixed ternary mononuclear Mg complex based on VA with 1,10‐phenanthroline (Phen) ligand ‐ [Mg (Valp)2Phen], in Saccharomyces cerevisiae and V79 cells. The MTT and clonal survival assays in V79 cells indicated that the Mg complex has higher cytotoxicity than sodium valproate. A similar cytotoxicity profile is observed in yeast. This fact is possibly due to the intercalation capacity of [Mg(Valp)2Phen], inducing DNA strand breaks, as observed in the comet assay and micronucleus test. In this sense, members of the NER, HR, NHEJ and TLS repair pathways are required for the repair of DNA lesions induced by [Mg(Valp)2Phen]. Interestingly, BER proteins apparently increase the cytotoxic potential of the drug. Furthermore, the [Mg(Valp)2Phen] showed higher cytotoxicity in V79 cells and yeast when compared to sodium valproate indicating applicability as a cytotoxic agent. [ABSTRACT FROM AUTHOR]

Published

2024

3. Plant Metabolomics: The Future of Anticancer Drug Discovery.

Author

Dabbousy, Ranin, Rima, Mohamad, Roufayel, Rabih, Rahal, Mohamad, Legros, Christian, Sabatier, Jean-Marc, and Fajloun, Ziad

Abstract

Drug development from medicinal plants constitutes an important strategy for finding natural anticancer therapies. While several plant secondary metabolites with potential antitumor activities have been identified, well-defined mechanisms of action remained uncovered. In fact, studies of medicinal plants have often focused on the genome, transcriptome, and proteome, dismissing the relevance of the metabolome for discovering effective plant-based drugs. Metabolomics has gained huge interest in cancer research as it facilitates the identification of potential anticancer metabolites and uncovers the metabolomic alterations that occur in cancer cells in response to treatment. This holds great promise for investigating the mode of action of target metabolites. Although metabolomics has made significant contributions to drug discovery, research in this area is still ongoing. In this review, we emphasize the significance of plant metabolomics in anticancer research, which continues to be a potential technique for the development of anticancer drugs in spite of all the challenges encountered. As well, we provide insights into the essential elements required for performing effective metabolomics analyses. [ABSTRACT FROM AUTHOR]

Published

2024

4. Adsorption Characteristics of the Anticancer Drug Hydroxyurea with Armchair BN Graphene Nanoribbons Containing and Lacking Vacancy Defects: Insight via DFT Calculations.

Author

Khudhair, Alaa M. and Ben Ahmed, Ali

Subjects

*ANTINEOPLASTIC agents, *DENSITY functional theory, *BAND gaps, *NANORIBBONS, *DRUG carriers, *NANOCARRIERS

Abstract

The identification of suitable nanocarriers for drug delivery has been a constant area of research and development. Two-dimensional nanomaterials based on graphene have been presented and proven as drug carriers in this instance. In this study, we employed calculations from density functional theory to examine the electronic and adsorption properties of the commonly administered anticancer medication hydroxyurea (HU) on armchair BN graphene nanoribbons with and without vacancy defects. The band gap of the structures, both with and without the presence of an anticancer drug, exhibits semiconductor behavior, with the exception of ABNNR which initially exhibits insulator behavior with a 6.009 eV energy gap, but upon interaction with the HU molecule, the energy disparity diminished to 4.72 eV. With an Eads = − 1.079 eV, the adsorption energy of the HU drug molecule on ABNNR-VN is significantly greater than that of the other complex structures. Based on the computed structural and electronic characteristics, it has been determined that HU/ABNNR-VN exhibits a greater propensity for HU molecule adsorption in comparison to alternative structures. [ABSTRACT FROM AUTHOR]

Published

2024

5. Reevaluating the Mechanistic Insights of α-TOS-Bearing Pt(IV) Anticancer Complexes: A New Perspective from a More In-Depth Knowledge.

Author

Marotta, Carlo, Cirri, Damiano, Funaioli, Tiziana, Gabbiani, Chiara, and Pratesi, Alessandro

Subjects

*CYTOTOXINS, *ANTINEOPLASTIC agents, *PRODRUGS, *RESEARCH personnel, *CLASS actions

Abstract

Pt(IV) prodrugs have been extensively studied over the years with the aim of overcoming the limitations of traditional Pt(II) drugs. In this frame, two cisplatin-based Pt(IV) complexes bearing α-tocopherol succinate (α-TOS, a derivative of vitamin E) in the axial position (namely, [PtCl2(NH3)2(OEt)(α-TOS)] and [PtCl2(NH3)2(α-TOS)2] were reported in recent years and their cytotoxicity was evaluated. In particular, [PtCl2(NH3)2(OEt)(α-TOS)] was reported to be more cytotoxic than [PtCl2(NH3)2(α-TOS)2]. In the present comment paper, reasons for the different cytotoxicity of these complexes are discussed in detail and, more in general, a comprehensive elucidation of the mechanism of action of this class of anticancer Pt(IV) compounds is provided. Hopefully, these findings and the resulting improved knowledge of these drugs will help researchers design new and improved Pt(IV) anticancer drugs. [ABSTRACT FROM AUTHOR]

Published

2024

6. TiO2 Nanotube Arrays Decorated with Graphene/Graphite Oxide Nanocomposite for the Photocatalytic Degradation of Anticancer Drugs in the Aquatic Environment.

Author

Huynh, Thao Phuong, Do, Tho Chau Minh Vinh, and Le, Phuoc Huu

Abstract

In this study, graphene–graphite oxide nanocomposite-decorated TiO2 nanotube arrays (GGO-TNAs) were synthesized by using electrochemical exfoliation and anodizing methods. The influence of GGO content on the material and photocatalytic properties of GGO-TNAs was systematically investigated for the degradation of six anticancer drugsirinotecan, doxorubicin, capecitabine, ifosfamide, cyclophosphamide, and methotrexateusing LC-MS/MS. The efficacy of anticancer drug degradation was evaluated in both pure water and hospital wastewater, with GGO-TNAs showing superior performance compared to TNAs. GGO-TNAs featured well-defined porous TiO2 nanotube arrays (anatase phase, (101) orientation, tube diameter ∼100 nm, thickness ∼16.2 μm) decorated with graphene sheets and graphite oxide particles. By varying the GGO solution concentration (10–40 mg L–1), carbon concentrations in GGO-TNAs ranged from 4.3 to 9.5 at. %. Surface and structural compositions were confirmed by XPS and Raman spectroscopy, while EPR results indicated the generation of highly active •OH and O2•– radicals under UV–vis irradiation. The GGO (20 mg L–1, 6.9 at. % C)-TNAs exhibited the highest photocatalytic activity with first-order rate constants (k) ranging from 4.8 × 10–2 to 40.3 × 10–2 min–1, significantly outperforming TNAs alone (1.2–1.8 times higher). GGO-TNAs retained 97% of their initial efficiency after five cycles of reuse, indicating material stability. The enhanced photocatalytic performance is attributed to improved utilization of visible light, increased generation of photocarriers, and reduced recombination of electron–hole pairs. Furthermore, the relationship between k values and the physicochemical properties of the anticancer drugs was investigated, and a degradation pathway for capecitabine was proposed based on MS spectra analysis. This study demonstrates that GGO-TNAs are highly effective and stable photocatalysts for degrading anticancer drugs in water and wastewater, offering a promising solution for environmental remediation. The enhanced photocatalytic efficiency and reusability of GGO-TNAs highlight their potential for practical water treatment applications. [ABSTRACT FROM AUTHOR]

Published

2024

7. Cancer Patient-Derived Cell-Based Models: Applications and Challenges in Functional Precision Medicine.

Author

Dinić, Jelena, Jovanović Stojanov, Sofija, Dragoj, Miodrag, Grozdanić, Marija, Podolski-Renić, Ana, and Pešić, Milica

Subjects

*INDIVIDUALIZED medicine, *ANTINEOPLASTIC agents, *CANCER treatment, *TREATMENT effectiveness, *DRUG resistance, *CELL culture

Abstract

The field of oncology has witnessed remarkable progress in personalized cancer therapy. Functional precision medicine has emerged as a promising avenue for achieving superior treatment outcomes by integrating omics profiling and sensitivity testing of patient-derived cancer cells. This review paper provides an in-depth analysis of the evolution of cancer-directed drugs, resistance mechanisms, and the role of functional precision medicine platforms in revolutionizing individualized treatment strategies. Using two-dimensional (2D) and three-dimensional (3D) cell cultures, patient-derived xenograft (PDX) models, and advanced functional assays has significantly improved our understanding of tumor behavior and drug response. This progress will lead to identifying more effective treatments for more patients. Considering the limited eligibility of patients based on a genome-targeted approach for receiving targeted therapy, functional precision medicine provides unprecedented opportunities for customizing medical interventions according to individual patient traits and individual drug responses. This review delineates the current landscape, explores limitations, and presents future perspectives to inspire ongoing advancements in functional precision medicine for personalized cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024

8. A Descriptive Review on the Potential Use of Diatom Biosilica as a Powerful Functional Biomaterial: A Natural Drug Delivery System.

Author

Kang, Sunggu, Woo, Yeeun, Seo, Yoseph, Yoo, Daehyeon, Kwon, Daeryul, Park, Hyunjun, Lee, Sang Deuk, Yoo, Hah Young, and Lee, Taek

Subjects

*DRUG delivery systems, *BONE regeneration, *POISONS, *DIATOMS, *ANTINEOPLASTIC agents

Abstract

Although various chemically synthesized materials are essential in medicine, food, and agriculture, they can exert unexpected side effects on the environment and human health by releasing certain toxic chemicals. Therefore, eco-friendly and biocompatible biomaterials based on natural resources are being actively explored. Recently, biosilica derived from diatoms has attracted attention in various biomedical fields, including drug delivery systems (DDS), due to its uniform porous nano-pattern, hierarchical structure, and abundant silanol functional groups. Importantly, the structural characteristics of diatom biosilica improve the solubility of poorly soluble substances and enable sustained release of loaded drugs. Additionally, diatom biosilica predominantly comprises SiO2, has high biocompatibility, and can easily hybridize with other DDS platforms, including hydrogels and cationic DDS, owing to its strong negative charge and abundant silanol groups. This review explores the potential applications of various diatom biosilica-based DDS in various biomedical fields, with a particular focus on hybrid DDS utilizing them. [ABSTRACT FROM AUTHOR]

Published

2024

9. Short Communication: Novel Di- and Triselenoesters as Effective Therapeutic Agents Inhibiting Multidrug Resistance Proteins in Breast Cancer Cells.

Author

Radomska, Dominika, Czarnomysy, Robert, Marciniec, Krzysztof, Nowakowska, Justyna, Domínguez-Álvarez, Enrique, and Bielawski, Krzysztof

Subjects

*DRUG resistance in cancer cells, *TRIPLE-negative breast cancer, *SELENIUM compounds, *MULTIDRUG resistance, *BREAST cancer

Abstract

Breast cancer has the highest incidence rate among all malignancies worldwide. Its high mortality is mainly related to the occurrence of multidrug resistance, which significantly limits therapeutic options. In this regard, there is an urgent need to develop compounds that would overcome this phenomenon. There are few reports in the literature that selenium compounds can modulate the activity of P-glycoprotein (MDR1). Therefore, we performed in silico studies and evaluated the effects of the novel selenoesters EDAG-1 and EDAG-8 on BCRP, MDR1, and MRP1 resistance proteins in MCF-7 and MDA-MB-231 breast cancer cells. The cytometric analysis showed that the tested compounds (especially EDAG-8) are inhibitors of BCRP, MDR1, and MRP1 efflux pumps (more potent than the reference compounds—novobiocin, verapamil, and MK-571). An in silico study correlates with these results, suggesting that the compound with the lowest binding energy to these transporters (EDAG-8) has a more favorable spatial structure affecting its anticancer activity, making it a promising candidate in the development of a novel anticancer agent for future breast cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024

10. Design, synthesis, and biological evaluation of novel halogenated chlorido[N,N′-bis(salicylidene)-1,2-bis(3-methoxyphenyl)ethylenediamine]iron(III) complexes as anticancer agents.

Author

Bernkop-Schnürch, Astrid Dagmar, Huber, Klaus, Clauser, Armida, Cziferszky, Monika, Leitner, Daniel, Talasz, Heribert, Hermann, Martin, Hohloch, Stephan, Gust, Ronald, and Kircher, Brigitte

Subjects

*REACTIVE oxygen species, *MAMMARY glands, *ETHYLENEDIAMINE, *LIGANDS (Biochemistry), *CELL death

Abstract

Iron(III) complexes based on N,N´-bis(salicylidene)ethylenediamine (salene) scaffolds have demonstrated promising anticancer features like induction of ferroptosis, an iron dependent cell death. Since poor cellular uptake limits their therapeutical potential, this study aimed to enhance the lipophilic character of chlorido[N,N′-bis(salicylidene)-1,2-bis(3-methoxyphenyl)ethylenediamine]iron(III) complexes by introducing lipophilicity improving ligands such as fluorine (X1), chlorine (X2) and bromine (X3) in 5-position in the salicylidene moieties. After detailed characterization the binding to nucleophiles, logP values and cellular uptake were determined. The complexes were further evaluated regarding their biological activity on MDA-MB 231 mammary carcinoma, the non-tumorous SV-80 fibroblast, HS-5 stroma and MCF-10A mammary gland cell lines. Stability of the complexes in aqueous and biological environments was proven by the lack of interactions with amino acids and glutathione. Cellular uptake was positively correlated with the logP values, indicating that higher lipophilicity enhanced cellular uptake. The complexes induced strong antiproliferative and antimetabolic effects on MDA-MB 231 cells, but were inactive on all non-malignant cells tested. Generation of mitochondrial reactive oxygen species, increase of lipid peroxidation and induction of both ferroptosis and necroptosis were identified as mechanisms of action. In conclusion, halogenation of chlorido[N,N′-bis(salicylidene)-1,2-bis(3-methoxyphenyl)ethylenediamine]iron(III) complexes raises their lipophilic character resulting in improved cellular uptake. [ABSTRACT FROM AUTHOR]

Published

2024

11. Disproportionality Analysis of Stomatitis Associated with Anticancer Drugs Using the Japanese Adverse Drug Event Report Database.

Author

Hosonaka, Kousuke, Yamaoka, Kenta, Ikeda, Naoe, Uchida, Mayako, Uesawa, Yoshihiro, Takahashi, Kazushige, and Shimizu, Tadashi

Subjects

*STOMATITIS, *DATABASES, *PHARMACOLOGY, *RISK assessment, *DRUG side effects, *ANTINEOPLASTIC agents, *FISHER exact test, *DESCRIPTIVE statistics, *CHI-squared test, *ODDS ratio, *REPORT writing, *DATA analysis software, *CONFIDENCE intervals, *DISEASE risk factors

Abstract

Introduction: Anticancer drug-induced stomatitis can affect a patient's quality of life and the continuation of drug treatment. Although there have been reports of the occurrence of stomatitis associated with anticancer agents in clinical trials, few Japanese participants have been enrolled in clinical trials and have not been sufficiently investigated. In addition, there has been little attention on research on anticancer drugs associated with stomatitis by patient stratification with different carcinogenic sites. Therefore, the aim of this study was to determine the disproportionality associated with stomatitis for various types of anticancer drugs in different types of cancer patients using the Japanese Adverse Drug Event Report (JADER) database. Methods: The aim of this study was to identify the disproportionality of stomatitis by analyzing the type of anticancer drug and cancer patients using the Japanese Pharmacovigilance Database. Data obtained from spontaneous reports of adverse events with more than 10 stomatitis outbreaks reported in the JADER database between April 2004 and March 2023 were analyzed. The safety signal for an adverse event was defined as the lower limit of the 95% confidence interval of the reported odds ratio of >1. Results: There were 6,178 reports of drugs associated with stomatitis. Among these, 41 drugs were suggested to be associated with stomatitis, and 41 drugs were detected as signals. These drugs were classified based on their efficacy: antipyrimidines (six drugs), folate metabolism antagonists (three drugs), alkylating agents (four drugs), platinum (three drugs), topoisomerase inhibitors (three drugs), microtubule inhibitors (three drugs), mammalian target of rapamycin (mTOR) inhibitors (two drugs), kinase inhibitors (seven drugs), anti-growth factor antibodies (five drugs) immune checkpoint inhibitors (one drug), and others (four drugs). Conclusion: The drugs that may be associated with stomatitis were cell cycle-dependent drugs, epidermal growth factor receptor-tyrosine kinase inhibitors, and mTOR inhibitors. Moreover, this study suggested that anti-growth factor antibodies and immune checkpoint inhibitors may be associated with stomatitis development. [ABSTRACT FROM AUTHOR]

Published

2024

12. Vitamin D-metabolizing enzyme CYP24A1 affects oncogenic behaviors of oral squamous cell carcinoma and its prognostic implication.

Author

Nakamori, Yuna, Takasawa, Akira, Takasawa, Kumi, Kyuno, Daisuke, Ono, Yusuke, Magara, Kazufumi, Nakahashi, Naoya, Sekiguchi, Shohei, Tsuchihashi, Kei, Miyazaki, Akihiro, and Osanai, Makoto

Subjects

*SQUAMOUS cell carcinoma, *VITAMIN D, *PROGNOSIS, *OVERALL survival, *ANTINEOPLASTIC agents, *VITAMIN D receptors

Abstract

Vitamin D is an essential molecule for cellular homeostasis, playing a critical role in cell fate decisions including cell proliferation, differentiation, and viability. Accumulating evidence has revealed that expression of the vitamin D-metabolizing enzyme CYP24A1 is dysregulated in different types of human malignancy. CYP24A1 has been shown to be involved in the oncogenic property of a variety of carcinoma cells. However, the pathological relevance of CYP24A1 expression level in human oral malignancy remains to be clarified. In the present study, suppression of CYP24A1 expression in oral squamous cell carcinoma (OSCC) cells increased cell proliferation, invasive activity, colony formation efficacy, and tumor growth in vivo. In addition, knockout of CYP24A1 expression inhibited cell death induced by two different types of anticancer drugs, i.e., fluorouracil and cisplatin. Gene clustering by RNA-sequence analysis revealed that several signaling molecules associated with MYC are involved in CYP24A1-mediated oncogenic behaviors. Furthermore, decreased expression level of CYP24A1 was observed in 124/204 cases (61%) of OSCC and was shown to be associated with short relapse-free and overall survival periods. The results showed that a low expression level of CYP24A1 promotes the oncogenic activity of OSCC and is significantly associated with poor prognosis in patients with this malignancy. [ABSTRACT FROM AUTHOR]

Published

2024

13. Phytochemical‐mediated modulation of autophagy and endoplasmic reticulum stress as a cancer therapeutic approach.

Author

Al Azzani, Mazoun, Nizami, Zohra Nausheen, Magramane, Rym, Sekkal, Mohammed N., Eid, Ali H., Al Dhaheri, Yusra, and Iratni, Rabah

Abstract

Autophagy and endoplasmic reticulum (ER) stress are conserved processes that generally promote survival, but can induce cell death when physiological thresholds are crossed. The pro‐survival aspects of these processes are exploited by cancer cells for tumor development and progression. Therefore, anticancer drugs targeting autophagy or ER stress to induce cell death and/or block the pro‐survival aspects are being investigated extensively. Consistently, several phytochemicals have been reported to exert their anticancer effects by modulating autophagy and/or ER stress. Various phytochemicals (e.g., celastrol, curcumin, emodin, resveratrol, among others) activate the unfolded protein response to induce ER stress‐mediated apoptosis through different pathways. Similarly, various phytochemicals induce autophagy through different mechanisms (namely mechanistic target of Rapamycin [mTOR] inhibition). However, phytochemical‐induced autophagy can function either as a cytoprotective mechanism or as programmed cell death type II. Interestingly, at times, the same phytochemical (e.g., 6‐gingerol, emodin, shikonin, among others) can induce cytoprotective autophagy or programmed cell death type II depending on cellular contexts, such as cancer type. Although there is well‐documented mechanistic interplay between autophagy and ER stress, only a one‐way modulation was noted with some phytochemicals (carnosol, capsaicin, cryptotanshinone, guangsangon E, kaempferol, and δ‐tocotrienol): ER stress‐dependent autophagy. Plant extracts are sources of potent phytochemicals and while numerous phytochemicals have been investigated in preclinical and clinical studies, the search for novel phytochemicals with anticancer effects is ongoing from plant extracts used in traditional medicine (e.g., Origanum majorana). Nonetheless, the clinical translation of phytochemicals, a promising avenue for cancer therapeutics, is hindered by several limitations that need to be addressed in future studies. [ABSTRACT FROM AUTHOR]

Published

2024

14. Liposomal Encapsulation of Different Anticancer Drugs: An Effective Drug Delivery Technique.

Author

Banerjee, Tridib and Sen, Kamalika

Abstract

Drug delivery is the process of introducing bio-active medicinal components into the body of a patient. It is possible to use a variety of natural resources and synthetic materials made from natural resources as the building blocks for creating drug delivery systems (DDs). Liposomal systems are such kinds of DDs consisting of a phospholipid membrane with a hydrophobic tail and a hydrophilic head. Liposomes are lipid-rich spherical or multilayered spherical structures with variations in their size (starting from 2 to > 5000 nm), production techniques, processing, and drug loading. Many advantages of liposomal drug delivery systems over conventional liposomes or free drug treatment of cancer have been discovered as modern drug delivery formulations. Because of their outstanding performance in targeted delivery, liposome nanocarriers have recently displayed excellent drug loading capacity, drug protection, higher bioavailability, enhanced intracellular delivery, and greater therapeutic impact. In this approach, the multifunctional and stimulus-responsive nanocarriers for the drug delivery of cancer treatments improve the effectiveness of treatment, by sustained release of the drug that combats metastases while limiting the systemic negative effects on healthy tissues and organs. This review summarizes the mechanism of liposomal encapsulation of different anticancer drugs, the mechanism of interaction of liposomal anticancer drugs with cancer cells, and also the mechanism of release of drugs from liposomes. The possible disadvantages and future scope of the technique have also been accounted for. [ABSTRACT FROM AUTHOR]

Published

2024

15. A Comprehensive Literature Review on Efficient Synthetic Approaches and Polymorphism of Pazopanib (Votrient), a Tyrosine Kinase Inhibitor.

Author

Chand, Onkar, Chopra, Lalita, and Tiwari, Shashi Kant

Subjects

VASCULAR endothelial growth factors, NEOVASCULARIZATION, TUMOR growth, PYRIMIDINE derivatives, ANTINEOPLASTIC agents

Abstract

Angiogenesis involves the development of new blood vessels from the pre-existing vasculature. In cancer, an inappropriate or pathological angiogenesis reinforces tumor growth by feeding with nutrient and oxygen. Central to the process of angiogenesis is vascular endothelial growth factor (VEGF) and its receptor (VEGFR), as they regulate angiogenesis and vascular permeability. To stop tumor angiogenesis by cutting off the blood supply, a multitude of angiogenesis inhibitors (antiangiogenic agents or anticancer drugs) have been developed. In pursuit of developing an effective angiogenesis inhibitor, a novel pyrimidine derivative, an inhibitor of VEGFR-2 kinase activity later known as "VOTRIENT (Pazopanib)" was developed by GlaxoSmithKline and approved by the FDA in October 2009 for treatment of advanced renal cell cancer. Later, it was also approved by the FDA for the treatment of advanced soft tissue sarcoma in April 2012. In the literature, there are multiple synthetic pathways reported and the present work reviews the literature related to the synthesis of Pazopanib emphasizing applicability at a commercial scale. The main purpose of this review paper is to provide a comprehensive overview of different existing routes of synthesis with relevant comparison, reported polymorphs, and suggesting further development. [ABSTRACT FROM AUTHOR]

Published

2024

16. Modulation of Multidrug Resistance Transporters by Food Components and Dietary Supplements: Implications for Cancer Therapy Efficacy and Safety

Author

Agnieszka Brodzicka, Agnieszka Galanty, and Paweł Paśko

Subjects

MRP2, BCRP, P-gp, natural products, dietary supplements, anticancer drugs, Biology (General), QH301-705.5

Abstract

The aim of this review is to explore how diet and dietary supplements influence the activity of key multidrug resistance (MDR) transporters—MRP2, BCRP, and P-gp. These transporters play a crucial role in drug efflux from cancer cells and significantly affect chemotherapy outcomes. This review focuses on how dietary phytochemicals, such as catechins and quercetin, impact the expression and function of these transporters. Both in vitro and in vivo experiments were examined to assess changes in drug bioavailability and intracellular drug accumulation. The findings show that certain dietary components—such as catechins, flavonoids, resveratrol, curcumin, terpenoids, sterols, and alkaloids—can either inhibit or induce MDR transporter activity, thus influencing the effectiveness of chemotherapy. These results highlight the importance of understanding diet–drug interactions in cancer therapy to improve treatment outcomes and reduce side effects. In conclusion, dietary modifications and supplements should be carefully considered in cancer treatment plans to optimize therapeutic efficacy.

Published

2024

17. Current advances of anticancer drugs based on solubilization technology

Author

Wu Min, Wang LiPing, Li Xiaofang, Zhang Feng, and Jin Xuewen

Subjects

anticancer drugs, anticancer effect, solubilization technology, solubility, bioavailability, Technology, Chemical technology, TP1-1185, Physical and theoretical chemistry, QD450-801

Published

2024

18. A Review of Recent Progress on the Anticancer Activity of Heterocyclic Compounds

Author

Beena Negi and Aarshiya Kwatra

Subjects

N-heterocycles, benzimidazoles, indoles, sulfonamide, pyrimidines, anticancer drugs, Chemistry, QD1-999

Published

2024

19. piscesCSM: prediction of anticancer synergistic drug combinations

Author

Raghad AlJarf, Carlos H. M. Rodrigues, Yoochan Myung, Douglas E. V. Pires, and David B. Ascher

Subjects

Drug combination, Machine learning, Graph-based signatures, Synergistic effects, Anticancer drugs, Information technology, T58.5-58.64, Chemistry, QD1-999

Abstract

Abstract While drug combination therapies are of great importance, particularly in cancer treatment, identifying novel synergistic drug combinations has been a challenging venture. Computational methods have emerged in this context as a promising tool for prioritizing drug combinations for further evaluation, though they have presented limited performance, utility, and interpretability. Here, we propose a novel predictive tool, piscesCSM, that leverages graph-based representations to model small molecule chemical structures to accurately predict drug combinations with favourable anticancer synergistic effects against one or multiple cancer cell lines. Leveraging these insights, we developed a general supervised machine learning model to guide the prediction of anticancer synergistic drug combinations in over 30 cell lines. It achieved an area under the receiver operating characteristic curve (AUROC) of up to 0.89 on independent non-redundant blind tests, outperforming state-of-the-art approaches on both large-scale oncology screening data and an independent test set generated by AstraZeneca (with more than a 16% improvement in predictive accuracy). Moreover, by exploring the interpretability of our approach, we found that simple physicochemical properties and graph-based signatures are predictive of chemotherapy synergism. To provide a simple and integrated platform to rapidly screen potential candidate pairs with favourable synergistic anticancer effects, we made piscesCSM freely available online at https://biosig.lab.uq.edu.au/piscescsm/ as a web server and API. We believe that our predictive tool will provide a valuable resource for optimizing and augmenting combinatorial screening libraries to identify effective and safe synergistic anticancer drug combinations. Scientific contribution This work proposes piscesCSM, a machine-learning-based framework that relies on well-established graph-based representations of small molecules to identify and provide better predictive accuracy of syngenetic drug combinations. Our model, piscesCSM, shows that combining physiochemical properties with graph-based signatures can outperform current architectures on classification prediction tasks. Furthermore, implementing our tool as a web server offers a user-friendly platform for researchers to screen for potential synergistic drug combinations with favorable anticancer effects against one or multiple cancer cell lines.

Published

2024

20. Global burden of anticancer drug-induced acute kidney injury and tubulointerstitial nephritis from 1967 to 2023

Author

Soo-Young Yoon, Sooji Lee, Kyeongmin Lee, Jin Sug Kim, Hyeon Seok Hwang, Andreas Kronbichler, Louis Jacob, Ju-Young Shin, Jin A. Lee, Jaeyu Park, Hyeri Lee, Hayeon Lee, Kyunghwan Jeong, and Dong Keon Yon

Subjects

Anticancer drugs, Acute kidney injury, Tubulointerstitial nephritis, World Health Organization, Medicine, Science

Abstract

Abstract This study aims to figure out the worldwide prevalence of anticancer therapy-associated acute kidney injury (AKI) and tubulointerstitial nephritis (TIN) and the relative risk of each cancer drug. We conducted an analysis of VigiBase, the World Health Organization pharmacovigilance database, 1967–2023 via disproportionate Bayesian reporting method. We further categorized the anticancer drugs into four groups: cytotoxic therapy, hormone therapy, immunotherapy, and targeted therapy. Reporting odds ratio (ROR) and information component (IC) compares observed and expected values to investigate the associations of each category of anticancer drugs with AKI and TIN. We identified 32,722 and 2056 reports (male, n = 17,829 and 1,293) of anticancer therapy-associated AKI and TIN, respectively, among 4,592,036 reports of all-drug caused AKI and TIN. There has been a significant increase in reports since 2010, primarily due to increased reports of targeted therapy and immunotherapy. Immunotherapy exhibited a significant association with both AKI (ROR: 8.92; IC0.25: 3.06) and TIN (21.74; 4.24), followed by cytotoxic therapy (7.14; 2.68), targeted therapy (5.83; 2.40), and hormone therapy (2.59; 1.24) for AKI, and by cytotoxic therapy (2.60; 1.21) and targeted therapy (1.54; 0.61) for TIN. AKI and TIN were more prevalent among individuals under 45 years of age, with a female preponderance for AKI and males for TIN. These events were reported in close temporal relationship after initiation of the respective drug (16.53 days for AKI and 27.97 days for TIN), and exhibited a high fatality rate, with 23.6% for AKI and 16.3% for TIN. These findings underscore that kidney-related adverse drug reactions are of prognostic significance and strategies to mitigate such side effects are required to optimize anticancer therapy.

Published

2024

21. Comprehensive analysis of nationwide anticancer drug-related complications in Korea: incidence, types, and cancer-specific considerations in contemporary oncology.

Author

Jeong, Jonghyun, Park, Soyoung, Heo, Kyu-Nam, Park, Soh Mee, Min, Sangil, Ah, Young-Mi, Han, Ji Min, and Lee, Ju-Yeun

Abstract

Background: The rising global incidence of cancer has increased the demand for chemotherapy, which is a crucial treatment modality. Recent advancements in cancer treatment, including targeted agents and immunotherapy, have introduced complications owing to their specific mechanisms. However, comprehensive studies of the combined complications of these approaches are lacking. Objectives: This study aimed to comprehensively assess and analyze the overall incidence of anticancer drug-related complications in a nationwide patient cohort, utilizing a customized National Health Insurance Sharing Service database in Korea. Design: Retrospective cohort study. Methods: We included patients who were prescribed anticancer drugs (excluding endocrine agents) and diagnosed with cancer. For the type of cancer classification, the International Statistical Classification of Diseases and Related Health Problems, Tenth Revision (ICD-10) was used and anticancer drugs were classified based on the Anatomical Therapeutic Chemical code. We classified cancer into 18 types based on the ICD-10 code and delineated cancer-related complications into 12 categories. Complications included hematological, gastrointestinal, infectious, cardiovascular, major bleeding, endocrine, neurotoxic, nephrotoxic, dermatological, pulmonary, musculoskeletal, and hepatotoxic effects. Result: We included 294,544 patients diagnosed with cancer and administered anticancer drugs between 2016 and 2018, with follow-up continuing until 2021. We identified 486,929 anticancer drug-related complications, with an incidence of 1843.6 per 1000 person-years (PY). Anemia was the most common complication, with a rate of 763.7 per 1000 PY, followed by febrile neutropenia (295.7) and nausea/vomiting (246.9). Several complications peaked during the first months following the initiation of anticancer drug therapy; however, herpes, skin infection, heart failure, and peripheral neuropathy peaked at 6–12 months. Among major cancers, breast cancer had the lowest overall incidence of complications. Targeted therapies revealed lower complication rates than cytotoxic chemotherapy; however, they also required careful monitoring of rash. Conclusion: This study highlights the importance of the proactive management of anticancer drug-related complications for patient care improvement. [ABSTRACT FROM AUTHOR]

Published

2024

22. Exposure–response modelling of osimertinib in patients with non‐small cell lung cancer.

Author

Johnson, Martin, Lin, Yu‐Wei, Schmidt, Henning, Sunnaker, Mikael, Van Maanen, Eline, Huang, Xiangning, Rukazenkov, Yuri, Tomkinson, Helen, and Vishwanathan, Karthick

Subjects

*EPIDERMAL growth factor receptors, *PROTEIN-tyrosine kinase inhibitors, *PROPORTIONAL hazards models, *INTERSTITIAL lung diseases, *OSIMERTINIB

Abstract

Aims Methods Results Conclusions Osimertinib is a third‐generation, irreversible, central nervous system‐active, epidermal growth factor receptor (EGFR) tyrosine kinase inhibitor (TKI) with efficacy in EGFR‐mutated non‐small cell lung cancer (NSCLC). We assessed the relationship between plasma osimertinib levels and its efficacy and safety events.Comprehensive pharmacokinetics exposure–response (E–R) modelling was performed utilizing steady state area under the curve (AUCss) data from first‐line, ≥second‐line and adjuvant studies from the osimertinib clinical development programme (20–240 mg once‐daily dosing; N = 1689 patients). Analyses were conducted for survival using a proportional hazard model; for interstitial lung disease (ILD) and left ventricular ejection fraction (LVEF) events using a penalized logistic regression model and graphical analysis of potential confounding factors; and for rash and diarrhoea events using descriptive analysis.E–R modelling analyses indicated no clear trend of increasing efficacy with increasing osimertinib AUCss; efficacy in all exposure quartiles was significantly better than the control arm (comparator EGFR‐TKI, chemotherapy or placebo) irrespective of treatment line. Model‐based analysis suggested a potential relationship between increased osimertinib exposure and increased probability of ILD events, predominantly in Japanese patients. Additionally, there were increased probabilities of rash or diarrhoea with increasing osimertinib exposure. The probability of LVEF events showed overlapping confidence intervals for osimertinib ≤80 mg and control.E–R modelling in patients with EGFR‐mutated NSCLC demonstrated that increased osimertinib exposure was unlikely to increase efficacy but may increase occurrence of certain adverse events. Hence, long‐term treatment with doses ≥80 mg was not expected to provide additional benefit. [ABSTRACT FROM AUTHOR]

Published

2024

23. The Anticancer Activity of Monosaccharides: Perspectives and Outlooks.

Author

McCallum, Niamh and Najlah, Mohammad

Subjects

*THERAPEUTIC use of antineoplastic agents, *DRUG toxicity, *PHOSPHORYLATION, *GLYCOLYSIS, *CARBOHYDRATES, *CARRIER proteins, *MONOSACCHARIDES, *BIOLOGICAL products, *SOLUBILITY, *CANCER chemotherapy, *ENERGY metabolism, *MOLECULAR structure, *CELL death, *TUMORS, *SYNTHETIC drugs

Abstract

Simple Summary: Despite recent advances in treatment options, such as chemotherapy, cancer continues to be the second-leading cause of death worldwide. Significant hurdles in the success of chemotherapy regimens include severe adverse effects, as well as drug resistance. As such, there is a strong requirement for novel pharmacological interventions in the treatment of cancer. Natural products, such as monosaccharides, are a promising potential treatment option for cancer due to their low toxicity, high solubility, and high specificity for tumour cells. Several naturally occurring and synthetically modified sugars have displayed toxicity in a variety of cancer and tumour cells. A major hallmark of cancer is the reprogramming of cellular metabolism from oxidative phosphorylation (OXPHOS) to glycolysis, a phenomenon known as the Warburg effect. To sustain high rates of glycolysis, cancer cells overexpress GLUT transporters and glycolytic enzymes, allowing for the enhanced uptake and consumption of glucose. The Warburg effect may be exploited in the treatment of cancer; certain epimers and derivatives of glucose can enter cancer cells and inhibit glycolytic enzymes, stunting metabolism and causing cell death. These include common dietary monosaccharides (ᴅ-mannose, ᴅ-galactose, ᴅ-glucosamine, ʟ-fucose), as well as some rare monosaccharides (xylitol, ᴅ-allose, ʟ-sorbose, ʟ-rhamnose). This article reviews the literature on these sugars in in vitro and in vivo models of cancer, discussing their mechanisms of cytotoxicity. In addition to this, the anticancer potential of some synthetically modified monosaccharides, such as 2-deoxy-ᴅ-glucose and its acetylated and halogenated derivatives, is reviewed. Further, this article reviews how certain monosaccharides can be used in combination with anticancer drugs to potentiate conventional chemotherapies and to help overcome chemoresistance. Finally, the limitations of administering two separate agents, a sugar and a chemotherapeutic drug, are discussed. The potential of the glycoconjugation of classical or repurposed chemotherapy drugs as a solution to these limitations is reviewed. [ABSTRACT FROM AUTHOR]

Published

2024

24. Optimization of a Modular Nanotransporter Design for Targeted Intracellular Delivery of Photosensitizer.

Author

Alieva, Rena T., Ulasov, Alexey V., Khramtsov, Yuri V., Slastnikova, Tatiana A., Lupanova, Tatiana N., Gribova, Maria A., Georgiev, Georgii P., and Rosenkranz, Andrey A.

Subjects

*EPIDERMAL growth factor receptors, *DRUG delivery systems, *PHOTOSENSITIZERS, *HETERODIMERS, *MODULAR design

Abstract

Modular nanotransporters (MNTs) are drug delivery systems for targeted cancer treatment. As MNTs are composed of several modules, they offer the advantage of high specificity and biocompatibility in delivering drugs to the target compartment of cancer cells. The large carrier module brings together functioning MNT modules and serves as a platform for drug attachment. The development of smaller-sized MNTs via truncation of the carrier module appears advantageous in facilitating tissue penetration. In this study, two new MNTs with a truncated carrier module containing either an N-terminal (MNTN) or a C-terminal (MNTC) part were developed by genetic engineering. Both new MNTs demonstrated a high affinity for target receptors, as revealed by fluorescent-labeled ligand-competitive binding. The liposome leakage assay proved the endosomolytic activity of MNTs. Binding to the importin heterodimer of each truncated MNT was revealed by a thermophoresis assay, while only MNTN possessed binding to Keap1. Finally, the photodynamic efficacy of the photosensitizer attached to MNTN was significantly higher than when attached to either MNTC or the original MNTs. Thus, this work reveals that MNT's carrier module can be truncated without losing MNT functionality, favoring the N-terminal part of the carrier module due to its ability to bind Keap1. [ABSTRACT FROM AUTHOR]

Published

2024

25. The Role of Inhaled Chitosan-Based Nanoparticles in Lung Cancer Therapy.

Author

Silva, Allana Carvalho, Costa, Mirsiane Pascoal, Zacaron, Thiago Medeiros, Ferreira, Kézia Cristine Barbosa, Braz, Wilson Rodrigues, Fabri, Rodrigo Luiz, Frézard, Frédéric Jean Georges, Pittella, Frederico, and Tavares, Guilherme Diniz

Subjects

*DRUG delivery devices, *SMALL interfering RNA, *POISONS, *CONTROLLED release drugs, *TECHNOLOGICAL innovations, *LUNGS

Abstract

Lung cancer is the leading cause of cancer-related mortality worldwide, largely due to the limited efficacy of anticancer drugs, which is primarily attributed to insufficient doses reaching the lungs. Additionally, patients undergoing treatment experience severe systemic adverse effects due to the distribution of anticancer drugs to non-targeted sites. In light of these challenges, there has been a growing interest in pulmonary administration of drugs for the treatment of lung cancer. This route allows drugs to be delivered directly to the lungs, resulting in high local concentrations that can enhance antitumor efficacy while mitigating systemic toxic effects. However, pulmonary administration poses the challenge of overcoming the mechanical, chemical, and immunological defenses of the respiratory tract that prevent the inhaled drug from properly penetrating the lungs. To overcome these drawbacks, the use of nanoparticles in inhaler formulations may be a promising strategy. Nanoparticles can assist in minimizing drug clearance, increasing penetration into the lung epithelium, and enhancing cellular uptake. They can also facilitate increased drug stability, promote controlled drug release, and delivery to target sites, such as the tumor environment. Among them, chitosan-based nanoparticles demonstrate advantages over other polymeric nanocarriers due to their unique biological properties, including antitumor activity and mucoadhesive capacity. These properties have the potential to enhance the efficacy of the drug when administered via the pulmonary route. In view of the above, this paper provides an overview of the research conducted on the delivery of anticancer drug-loaded chitosan-based nanoparticles incorporated into inhaled drug delivery devices for the treatment of lung cancer. Furthermore, the article addresses the use of emerging technologies, such as siRNA (small interfering RNA), in the context of lung cancer therapy. Particularly, recent studies employing chitosan-based nanoparticles for siRNA delivery via the pulmonary route are described. [ABSTRACT FROM AUTHOR]

Published

2024

26. Electrochemistry as a Powerful Tool for Investigations of Antineoplastic Agents: A Comprehensive Review.

Author

Brycht, Mariola, Poltorak, Lukasz, Baluchová, Simona, Sipa, Karolina, Borgul, Paulina, Rudnicki, Konrad, and Skrzypek, Sławomira

Subjects

*MEDICAL personnel, *SINGLE-stranded DNA, *ANTINEOPLASTIC agents, *DNA, *DRUG interactions

Abstract

Cancer is most frequently treated with antineoplastic agents (ANAs) that are hazardous to patients undergoing chemotherapy and the healthcare workers who handle ANAs in the course of their duties. All aspects related to hazardous oncological drugs illustrate that the monitoring of ANAs is essential to minimize the risks associated with these drugs. Among all analytical techniques used to test ANAs, electrochemistry holds an important position. This review, for the first time, comprehensively describes the progress done in electrochemistry of ANAs by means of a variety of bare or modified (bio)sensors over the last four decades (in the period of 1982–2021). Attention is paid not only to the development of electrochemical sensing protocols of ANAs in various biological, environmental, and pharmaceutical matrices but also to achievements of electrochemical techniques in the examination of the interactions of ANAs with deoxyribonucleic acid (DNA), carcinogenic cells, biomimetic membranes, peptides, and enzymes. Other aspects, including the enantiopurity studies, differentiation between single-stranded and double-stranded DNA without using any label or tag, studies on ANAs degradation, and their pharmacokinetics, by means of electrochemical techniques are also commented. Finally, concluding remarks that underline the existence of a significant niche for the basic electrochemical research that should be filled in the future are presented. [ABSTRACT FROM AUTHOR]

Published

2024

27. A Novel Strategy for Glioblastoma Treatment by Natural Bioactive Molecules Showed a Highly Effective Anti-Cancer Potential.

Author

Giammona, Alessandro, Commisso, Mauro, Bonanomi, Marcella, Remedia, Sofia, Avesani, Linda, Porro, Danilo, Gaglio, Daniela, Bertoli, Gloria, and Lo Dico, Alessia

Abstract

Glioblastoma (GBM) is a severe form of brain tumor that has a high fatality rate. It grows aggressively and most of the time results in resistance to traditional treatments like chemo- and radiotherapy and surgery. Biodiversity, beyond representing a big resource for human well-being, provides several natural compounds that have shown great potential as anticancer drugs. Many of them are being extensively researched and significantly slow GBM progression by reducing the proliferation rate, migration, and inflammation and also by modulating oxidative stress. Here, the use of some natural compounds, such as Allium lusitanicum, Succisa pratensis, and Dianthus superbus, was explored to tackle GBM; they showed their impact on cell number reduction, which was partially given by cell cycle quiescence. Furthermore, a reduced cell migration ability was reported, accomplished by morphological cytoskeleton changes, which even highlighted a mesenchymal–epithelial transition. Furthermore, metabolic studies showed an induced cell oxidative stress modulation and a massive metabolic rearrangement. Therefore, a new therapeutic option was suggested to overcome the limitations of conventional treatments and thereby improve patient outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

28. Fluorinated GlycoNucleoLipid-based hydrogels as new spatiotemporal stimulable DDS.

Author

Gaubert, Alexandra, Castagnet, Thibault, Marsh, Jevon, and Barthélémy, Philippe

Abstract

Achieving a controlled release of several active pharmaceutical ingredients (APIs) remains a challenge for improving their therapeutic effects and reduced their side effects. In the current work, stimulable Drug Delivery Systems (DDS) based on supramolecular hydrogels were designed by combining two APIs featuring anticancer activities, namely the doxorubicin and phenazine 14. In vitro studies revealed promising physicochemical properties for all the investigated API loaded gels. Fluorinated GlycoNucleoLipid (GNF) based supramolecular gels remain stable in the presence of either doxorubicin (Doxo) or phenazine 14 (Phe) as anticancer drugs. Noteworthy, the stiffness of the GNF-based supramolecular gels was enhanced in the presence of both APIs while maintaining their thixotropic properties. We demonstrated that the storage modulus (G') of the GNF gels was increased from 1.3 kPa to 9.3 kPa upon loading of both APIs within the same gels. With a low mechanical stimulation (within the LVR), a passive diffusion out of gels was observed for Dox whereas Phe remained trapped in the GNF gels over several hours. Also, in this work we showed that mechanical stress triggered the release of both Phe and Doxo at different rates. Proof of concept of the dual system sensitive to mechanical stress. [ABSTRACT FROM AUTHOR]

Published

2024

29. piscesCSM: prediction of anticancer synergistic drug combinations.

Author

AlJarf, Raghad, Rodrigues, Carlos H. M., Myung, Yoochan, Pires, Douglas E. V., and Ascher, David B.

Subjects

*ANTINEOPLASTIC combined chemotherapy protocols, *INTERNET servers, *MACHINE learning, *SUPERVISED learning, *COMBINATION drug therapy, *RECEIVER operating characteristic curves, *NOMOGRAPHY (Mathematics)

Abstract

While drug combination therapies are of great importance, particularly in cancer treatment, identifying novel synergistic drug combinations has been a challenging venture. Computational methods have emerged in this context as a promising tool for prioritizing drug combinations for further evaluation, though they have presented limited performance, utility, and interpretability. Here, we propose a novel predictive tool, piscesCSM, that leverages graph-based representations to model small molecule chemical structures to accurately predict drug combinations with favourable anticancer synergistic effects against one or multiple cancer cell lines. Leveraging these insights, we developed a general supervised machine learning model to guide the prediction of anticancer synergistic drug combinations in over 30 cell lines. It achieved an area under the receiver operating characteristic curve (AUROC) of up to 0.89 on independent non-redundant blind tests, outperforming state-of-the-art approaches on both large-scale oncology screening data and an independent test set generated by AstraZeneca (with more than a 16% improvement in predictive accuracy). Moreover, by exploring the interpretability of our approach, we found that simple physicochemical properties and graph-based signatures are predictive of chemotherapy synergism. To provide a simple and integrated platform to rapidly screen potential candidate pairs with favourable synergistic anticancer effects, we made piscesCSM freely available online at https://biosig.lab.uq.edu.au/piscescsm/ as a web server and API. We believe that our predictive tool will provide a valuable resource for optimizing and augmenting combinatorial screening libraries to identify effective and safe synergistic anticancer drug combinations. Scientific contribution: This work proposes piscesCSM, a machine-learning-based framework that relies on well-established graph-based representations of small molecules to identify and provide better predictive accuracy of syngenetic drug combinations. Our model, piscesCSM, shows that combining physiochemical properties with graph-based signatures can outperform current architectures on classification prediction tasks. Furthermore, implementing our tool as a web server offers a user-friendly platform for researchers to screen for potential synergistic drug combinations with favorable anticancer effects against one or multiple cancer cell lines. [ABSTRACT FROM AUTHOR]

Published

2024

30. Di- and Triselenoesters—Promising Drug Candidates for the Future Therapy of Triple-Negative Breast Cancer.

Author

Radomska, Dominika, Czarnomysy, Robert, Szymanowska, Anna, Radomski, Dominik, Chalecka, Magda, Surazynski, Arkadiusz, Domínguez-Álvarez, Enrique, Bielawska, Anna, and Bielawski, Krzysztof

Subjects

*TRIPLE-negative breast cancer, *CANCER cells, *BREAST cancer, *INHIBITION of cellular proliferation, *AMP-activated protein kinases, *CASPASES, *BREAST, *MITOCHONDRIAL membranes

Abstract

Breast cancer is a major malignancy among women, characterized by a high mortality rate. The available literature evidence indicates that selenium, as a trace element, has chemopreventive properties against many types of cancer; as such, compounds containing it in their structure may potentially exhibit anticancer activity. Accordingly, we have undertaken a study to evaluate the effects of novel selenoesters (EDAG-1, -7, -8, -10) on MCF-7 and MDA-MB-231 breast cancer cells. Our analysis included investigations of cell proliferation and viability as well as cytometric determinations of apoptosis/autophagy induction, changes in mitochondrial membrane polarity (ΔΨm), caspase 3/7, 8, and 9 activities, and Bax, Bcl-2, p53, Akt, AMPK, and LC3A/B proteins. The obtained data revealed that the tested derivatives are highly cytotoxic and inhibit cell proliferation even at nanomolar doses (0.41–0.79 µM). Importantly, their strong proapoptotic properties (↑ caspase 3/7) are attributable to the effects on both the extrinsic (↑ caspase 8) and intrinsic (↓ ΔΨm and Bcl-2, ↑ Bax, p53, and caspase 9) pathways of apoptosis. Moreover, the tested compounds are autophagy activators (↓ Akt, ↑ autophagosomes and autolysosomes, AMPK, LC3A/B). In summary, the potent anticancer activity suggests that the tested compounds may be promising drug candidates for future breast cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024

31. Global burden of anticancer drug-induced acute kidney injury and tubulointerstitial nephritis from 1967 to 2023.

Author

Yoon, Soo-Young, Lee, Sooji, Lee, Kyeongmin, Kim, Jin Sug, Hwang, Hyeon Seok, Kronbichler, Andreas, Jacob, Louis, Shin, Ju-Young, Lee, Jin A., Park, Jaeyu, Lee, Hyeri, Lee, Hayeon, Jeong, Kyunghwan, and Yon, Dong Keon

Subjects

*ACUTE kidney failure, *DRUG side effects, *NEPHRITIS, *GROUP psychotherapy

Abstract

This study aims to figure out the worldwide prevalence of anticancer therapy-associated acute kidney injury (AKI) and tubulointerstitial nephritis (TIN) and the relative risk of each cancer drug. We conducted an analysis of VigiBase, the World Health Organization pharmacovigilance database, 1967–2023 via disproportionate Bayesian reporting method. We further categorized the anticancer drugs into four groups: cytotoxic therapy, hormone therapy, immunotherapy, and targeted therapy. Reporting odds ratio (ROR) and information component (IC) compares observed and expected values to investigate the associations of each category of anticancer drugs with AKI and TIN. We identified 32,722 and 2056 reports (male, n = 17,829 and 1,293) of anticancer therapy-associated AKI and TIN, respectively, among 4,592,036 reports of all-drug caused AKI and TIN. There has been a significant increase in reports since 2010, primarily due to increased reports of targeted therapy and immunotherapy. Immunotherapy exhibited a significant association with both AKI (ROR: 8.92; IC0.25: 3.06) and TIN (21.74; 4.24), followed by cytotoxic therapy (7.14; 2.68), targeted therapy (5.83; 2.40), and hormone therapy (2.59; 1.24) for AKI, and by cytotoxic therapy (2.60; 1.21) and targeted therapy (1.54; 0.61) for TIN. AKI and TIN were more prevalent among individuals under 45 years of age, with a female preponderance for AKI and males for TIN. These events were reported in close temporal relationship after initiation of the respective drug (16.53 days for AKI and 27.97 days for TIN), and exhibited a high fatality rate, with 23.6% for AKI and 16.3% for TIN. These findings underscore that kidney-related adverse drug reactions are of prognostic significance and strategies to mitigate such side effects are required to optimize anticancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024

32. Electrochemical Analysis of the Interaction between DNA and Abiraterone D4A Metabolite.

Author

Shumyantseva, V. V., Berezhnova, A. V., Agafonova, L. E., Bulko, T. V., and Veselovsky, A. V.

Subjects

*ELECTROCHEMICAL analysis, *DNA, *GUANINE, *BINDING constant, *CARBON electrodes, *ADENINE, *HYDROGEN bonding interactions

Abstract

The electroanalytical characteristics of double-stranded DNA (dsDNA) and the complex of dsDNA with the anticancer drug metabolite, abiraterone D4A, in the concentration range of 25–200 μM were investigated using differential pulse voltammetry. The effect of D4A on dsDNA was detected by changes in the intensity of the electrochemical oxidation of the heterocyclic bases guanine, adenine, and thymine. This investigation used screen-printed electrodes modified with carbon nanotubes. Binding constants (Kb) for guanine, adenine, and thymine in the dsDNA/D4A complexes were calculated to be 1.1 × 104, 5.5 × 103, and 2.5 × 103 M–1, respectively. The DNA-mediated electrochemical coefficients of the toxic effect were calculated as the ratio of the signal intensities of guanine and adenine in the presence of D4A compared to those without the drug (T, %). Based on an analysis of electrochemical parameters and binding constant values, an assumption was made regarding the mechanism of the interaction between D4A and DNA, predominantly through electrostatic interactions and the formation of hydrogen bonds with the minor groove. Conclusions about the mechanism of the interaction of the abiraterone D4A metabolite with the dsDNA minor groove, obtained by electrochemical methods, were supported by the molecular simulation of the DNA/D4A complex. [ABSTRACT FROM AUTHOR]

Published

2024

33. Quantitative Structure–Property Relationship Analysis in Molecular Graphs of Some Anticancer Drugs with Temperature Indices Approach.

Author

Shi, Xiaolong, Cai, Ruiqi, Ramezani Tousi, Jaber, and Talebi, Ali Asghar

Subjects

*MOLECULAR graphs, *ANTINEOPLASTIC agents, *ALKYLATING agents, *MOLECULAR connectivity index, *BOILING-points, *RALOXIFENE, *METHYLGUANINE

Abstract

The most important application of anticancer drugs in various forms (alkylating agents, hormones agents, and antimetabolites) is the treatment of malignant diseases. Topological indices are widely used in the field of chemical and medical sciences, especially in studying the chemical, biological, clinical, and therapeutic aspects of drugs. In this article, the temperature indices in anticancer drugs molecular graphs such as Carmustine, Convolutamine F, Raloxifene, Tambjamine K, and Pterocellin B were calculated and then analyzed based on physical and chemical properties. The analysis was performed by identifying the best regression models based on temperature indices for six physical and chemical features of anticancer drugs. The results indicated that temperature indices were essential topological indices that predict the properties of anticancer drugs, such as boiling point, flash point, enthalpy, molar refractivity, molar volume, and polarizability. It was also observed that the r value of the regression model was more than 0.6, and the p value was less than 0.05. [ABSTRACT FROM AUTHOR]

Published

2024

34. Targeting Hdm2 and Hdm4 in Anticancer Drug Discovery: Implications for Checkpoint Inhibitor Immunotherapy.

Author

Ntwasa, Monde

Subjects

*IMMUNE checkpoint inhibitors, *TUMOR suppressor proteins, *DRUG discovery, *ANTINEOPLASTIC agents, *DRUG development

Abstract

Hdm2 and Hdm4 are structural homologs that regulate the tumor suppressor protein, p53. Since some tumors express wild-type p53, Hdm2 and Hdm4 are plausible targets for anticancer drugs, especially in tumors that express wild-type p53. Hdm4 can enhance and antagonize the activity of Tp53, thereby playing a critical role in the regulation of p53's activity and stability. Moreover, Hdm2 and Hdm4 are overexpressed in many cancers, some expressing wild-type Tp53. Due to experimental evidence suggesting that the activation of wild-type Tp53 can augment the antitumor activity by some checkpoint inhibitors, drugs targeting Hdm2 and Hdm4 may be strong candidates for combining with checkpoint inhibitor immunotherapy. However, other evidence suggests that the overexpression of Hdm2 and Hdm4 may indicate poor response to immune checkpoint inhibitors. These findings require careful examination and scrutiny. In this article, a comprehensive analysis of the Hdm2/Hdm4 partnership will be conducted. Furthermore, this article will address the current progress of drug development regarding molecules that target the Hdm2/Hdm4/Tp53 partnership. [ABSTRACT FROM AUTHOR]

Published

2024

35. Underlying Mechanisms of Thrombosis Associated with Cancer and Anticancer Therapies.

Author

Pantazi, Despoina, Alivertis, Dimitrios, and Tselepis, Alexandros D.

Abstract

Opinion Statement: Cancer-associated thrombosis (CAT) has been identified as the second most prevalent cause of death after cancer itself. Moreover, the risk of thrombotic events in cancer patients increases due to anticancer drugs, such as tyrosine kinase inhibitors (TKIs). Venous thromboembolism (VTE) as well as arterial thromboembolic (ATE) events are present in CAT. Although VTE occurs more frequently, ATE events are very significant and in some cases are more dangerous than VTE. Guidelines for preventing thrombosis refer mainly VTE as well as the contribution of ATE events. Several factors are involved in thrombosis related to cancer, but the whole pathomechanism of thrombosis is not clear and may differ between patients. The activation of the coagulation system and the interaction of cancer cells with other cells including platelets, endothelial cells, monocytes, and neutrophils are promoted by a hypercoagulable state caused by cancer. We present an update on the pathomechanisms of CAT and the effect of anticancer drugs, mainly targeted therapies with a focus on TKIs. Considering the risk of bleeding associated with anticoagulation in each cancer patient, the anticoagulation strategy may involve the use of FXIa inhibitors, direct oral anticoagulants, and low-molecular-weight heparin. Further research would be valuable in developing strategies for reducing CAT. [ABSTRACT FROM AUTHOR]

Published

2024

36. Generation of Hydrogen Peroxide in Cancer Cells: Advancing Therapeutic Approaches for Cancer Treatment.

Author

Ali, Taufeeque, Li, Daniel, Ponnamperumage, Thilini Nimasha Fernando, Peterson, Alexis Kimberly, Pandey, Jatin, Fatima, Kulsum, Brzezinski, John, Jakusz, Julia Anna Rose, Gao, Hanlun, Koelsch, Gilbert Edward, Murugan, Dhivyashree Senthil, and Peng, Xiaohua

Subjects

*PATIENT safety, *APOPTOSIS, *CELL physiology, *CELL lines, *REACTIVE oxygen species, *HYDROGEN peroxide, *MOLECULAR structure, *TUMORS

Abstract

Simple Summary: Cancer cells grow and divide so rapidly that they are literally engaged in a metabolic marathon—leading to the formation of high levels of reactive oxygen species (ROS). The altered redox balance in cancer cells offers therapeutic opportunities for targeting cancer. Some ROS-targeting strategies attempt to enhance ROS production to inflict lethal cell damage or trigger apoptosis, while other anticancer agents inhibit enzymes that are essential to maintain the redox potential of the cell. One type of ROS that shows potential to be utilized as a treatment mechanism is hydrogen peroxide (H2O2), which can be generated by numerous mechanisms, including metal-based prodrugs, photodynamic therapy, enzymes, nanoparticles, chemical modulators, and various combinations thereof. This review focuses on various chemical agents that induce H2O2-mediated cancer cell death, including their mechanism of function, preclinical and clinical studies, recent advancements, and potential applications as a new and exciting avenue for targeted and efficacious cancer treatment. Cancer cells show altered antioxidant defense systems, dysregulated redox signaling, and increased generation of reactive oxygen species (ROS). Targeting cancer cells through ROS-mediated mechanisms has emerged as a significant therapeutic strategy due to its implications in cancer progression, survival, and resistance. Extensive research has focused on selective generation of H2O2 in cancer cells for selective cancer cell killing by employing various strategies such as metal-based prodrugs, photodynamic therapy, enzyme-based systems, nano-particle mediated approaches, chemical modulators, and combination therapies. Many of these H2O2-amplifying approaches have demonstrated promising anticancer effects and selectivity in preclinical investigations. They selectively induce cytotoxicity in cancer cells while sparing normal cells, sensitize resistant cells, and modulate the tumor microenvironment. However, challenges remain in achieving selectivity, addressing tumor heterogeneity, ensuring efficient delivery, and managing safety and toxicity. To address those issues, H2O2-generating agents have been combined with other treatments leading to optimized combination therapies. This review focuses on various chemical agents/approaches that kill cancer cells via H2O2-mediated mechanisms. Different categories of compounds that selectively generate H2O2 in cancer cells are summarized, their underlying mechanisms and function are elucidated, preclinical and clinical studies as well as recent advancements are discussed, and their prospects as targeted therapeutic agents and their therapeutic utility in combination with other treatments are explored. By understanding the potential of these compounds, researchers can pave the way for the development of effective and personalized cancer treatments. [ABSTRACT FROM AUTHOR]

Published

2024

37. Stress granule-mediated sequestration of EGR1 mRNAs correlates with lomustine-induced cell death prevention.

Author

Leśniczak-Staszak, Marta, Pietras, Paulina, Ruciński, Marcin, Johnston, Ryan, Sowiński, Mateusz, Andrzejewska, Małgorzata, Nowicki, Michał, Gowin, Ewelina, Lyons, Shawn M., Ivanov, Pavel, and Szaflarski, Witold

Subjects

*GENE expression, *CELL death, *STRESS granules, *BCL genes, *GENETIC translation, *DNA, *MESSENGER RNA

Abstract

Some chemotherapy drugs modulate the formation of stress granules (SGs), which are RNA-containing cytoplasmic foci contributing to stress response pathways. How SGs mechanistically contribute to pro-survival or pro-apoptotic functions must be better defined. The chemotherapy drug lomustine promotes SG formation by activating the stress-sensing eIF2a kinase HRI (encoded by the EIF2AK1 gene). Here, we applied a DNA microarray-based transcriptome analysis to determine the genes modulated by lomustine-induced stress and suggest roles for SGs in this process. We found that the expression of the pro-apoptotic EGR1 gene was specifically regulated in cells upon lomustine treatment. The appearance of EGR1-encoding mRNA in SGs correlated with a decrease in EGR1 mRNA translation. Specifically, EGR1 mRNA was sequestered to SGs upon lomustine treatment, probably preventing its ribosome translation and consequently limiting the degree of apoptosis. Our data support the model where SGs can selectively sequester specific mRNAs in a stress-specific manner, modulate their availability for translation, and thus determine the fate of a stressed cell. [ABSTRACT FROM AUTHOR]

Published

2024

38. Structure‐property modeling of pharmacokinetic characteristics of anticancer drugs via topological indices, multigraph modeling and multi‐criteria decision making.

Author

Pandi, Ugasini Preetha, Hayat, Sakander, Marimuthu, Suresh, and Konsalraj, Julietraja

Subjects

*MOLECULAR connectivity index, *MULTIPLE criteria decision making, *ANTINEOPLASTIC agents, *DECISION making, *TOPOLOGICAL degree, *MULTIGRAPH

Abstract

This study presents an in‐depth inquiry into estimating ADME properties for promising anticancer drugs, particularly amino acid‐based alkylating agents, through ev‐ve degree topological indices and QSPR analysis. The aim of the study is to compare multigraph modeling to simple graph modeling in estimating six ADME properties. Results demonstrate that multigraph modeling's superior performance, with notable high correlations such as r=0.926$$ r=0.926 $$ for maximum passive absorption (MPA) using the M‐ev index, compared to simple graph modeling's r=0.68$$ r=0.68 $$ with the M2$$ {M}_2 $$‐ev index. This emphasizes the need for sophisticated modeling techniques in drug development. The primary objective is to compare multigraph and simple graph modeling using topological structure descriptors, followed by QSPR analysis to determine the better approach in estimating ADME properties. MCDM weight allocation techniques validate correlation values, enhancing understanding of estimators and identifying potential drugs. This underscores the importance of considering various MCDM methods and weight allocation approaches for reliable decision‐making in healthcare contexts. [ABSTRACT FROM AUTHOR]

Published

2024

39. Cytotoxic and molecular differences of anticancer agents on 2D and 3D cell culture.

Author

Alwahsh, Mohammad, Al-Doridee, Amani, Jasim, Suhair, Awwad, Oriana, Hergenröder, Roland, and Hamadneh, Lama

Abstract

Background: Cancer and multidrug resistance are regarded as concerns related to poor health outcomes. It was found that the monolayer of 2D cancer cell cultures lacks many important features compared to Multicellular Tumor Spheroids (MCTS) or 3D cell cultures which instead have the ability to mimic more closely the in vivo tumor microenvironment. This study aimed to produce 3D cell cultures from different cancer cell lines and to examine the cytotoxic activity of anticancer medications on both 2D and 3D systems, as well as to detect alterations in the expression of certain genes levels. Method: 3D cell culture was produced using 3D microtissue molds. The cytotoxic activities of colchicine, cisplatin, doxorubicin, and paclitaxel were tested on 2D and 3D cell culture systems obtained from different cell lines (A549, H1299, MCF-7, and DU-145). IC50 values were determined by MTT assay. In addition, gene expression levels of PIK3CA, AKT1, and PTEN were evaluated by qPCR. Results: Similar cytotoxic activities were observed on both 3D and 2D cell cultures, however, higher concentrations of anticancer medications were needed for the 3D system. For instance, paclitaxel showed an IC50 of 6.234 µM and of 13.87 µM on 2D and 3D H1299 cell cultures, respectively. Gene expression of PIK3CA in H1299 cells also showed a higher fold change in 3D cell culture compared to 2D system upon treatment with doxorubicin. Conclusion: When compared to 2D cell cultures, the behavior of cells in the 3D system showed to be more resistant to anticancer treatments. Due to their shape, growth pattern, hypoxic core features, interaction between cells, biomarkers synthesis, and resistance to treatment penetration, the MCTS have the advantage of better simulating the in vivo tumor conditions. As a result, it is reasonable to conclude that 3D cell cultures may be a more promising model than the traditional 2D system, offering a better understanding of the in vivo molecular changes in response to different potential treatments and multidrug resistance development. [ABSTRACT FROM AUTHOR]

Published

2024

40. Drug Delivery Systems of Betulin and Its Derivatives: An Overview.

Author

Jaroszewski, Bartosz, Jelonek, Katarzyna, and Kasperczyk, Janusz

Subjects

DRUG delivery systems, GOLD nanoparticles, BETULIN, CARBON nanotubes, SCIENCE databases

Abstract

Natural origin products are regarded as promising for the development of new therapeutic therapies with improved effectiveness, biocompatibility, reduced side effects, and low cost of production. Betulin (BE) is very promising due to its wide range of pharmacological activities, including its anticancer, antioxidant, and antimicrobial properties. However, despite advancements in the use of triterpenes for clinical purposes, there are still some obstacles that hinder their full potential, such as their hydrophobicity, low solubility, and poor bioavailability. To address these concerns, new BE derivatives have been synthesized. Moreover, drug delivery systems have emerged as a promising solution to overcome the barriers faced in the clinical application of natural products. The aim of this manuscript is to summarize the recent achievements in the field of delivery systems of BE and its derivatives. This review also presents the BE derivatives mostly considered for medical applications. The electronic databases of scientific publications were searched for the most interesting achievements in the last ten years. Thus far, it is mostly nanoparticles (NPs) that have been considered for the delivery of betulin and its derivatives, including organic NPs (e.g., micelles, conjugates, liposomes, cyclodextrins, protein NPs), inorganic NPs (carbon nanotubes, gold NPs, silver), and complex/hybrid and miscellaneous nanoparticulate systems. However, there are also examples of microparticles, gel-based systems, suspensions, emulsions, and scaffolds, which seem promising for the delivery of BE and its derivatives. [ABSTRACT FROM AUTHOR]

Published

2024

41. Recent Development of CDK2 Inhibitors as Anticancer Drugs: An Update (2015–2023)

Author

Yumei Jin, Hao Lu, Hu Ge, Xuben Hou, and Hao Fang

Subjects

cyclin-dependent kinase 2, non-ATP competitive inhibitor, anticancer drugs, Pharmacy and materia medica, RS1-441

Abstract

Cyclin-dependent kinase 2 (CDK2) is a critical regulator of cell division and has emerged as a promising target for anticancer treatment. In this article, we summarize the structural features of CDK2 inhibitors and corresponding binding modes, in particular the noncompetitive binding modes that offer unique advantages for the development of highly selective inhibitors. In addition, we present an overview of the latest advancements in the development of CDK2 inhibitors and discuss the trend in the field. This review provides valuable insights into the structure–activity relationships of the reported CDK2 inhibitors, inspiring the development of potent and selective CDK2 inhibitors in the future.

Published

2024

42. Editorial: Natural products and nanoparticles in cancer treatment: is there a light at the end of the tunnel?

Author

Milica Pešić, Amir Modarresi Chahardehi, Javier Echeverria, and Wamidh H. Talib

Subjects

natural products, nanoparticles, anticancer drugs, cancer treatment, cancer drug resistance, Therapeutics. Pharmacology, RM1-950

Published

2024

43. Editorial: Natural products and nanoparticles in cancer treatment: is there a light at the end of the tunnel?

Author

Pešić, Milica, Chahardehi, Amir Modarresi, Echeverria, Javier, and Talib, Wamidh H.

Subjects

MESENCHYMAL stem cells, IRON oxide nanoparticles, DRUG resistance in cancer cells, CANCER chemotherapy, KREBS cycle

Abstract

This article is an editorial that discusses the potential of natural products and nanoparticles in cancer treatment. It highlights the challenges faced in utilizing natural products for medicinal purposes, such as poor solubility and bioavailability. Nanoparticles, on the other hand, offer unique properties that allow for precise targeting of tumors and reduced impact on healthy tissues. The article also mentions specific studies that explore the application of nanoparticles in targeted therapy for different types of cancer. Overall, the article emphasizes the need for further research in this field to enhance the effectiveness of cancer treatments. [Extracted from the article]

Published

2024

44. Potential Pathways for Chemotherapy-Induced Cognitive Decline

Author

Dahiya, Mini, Yadav, Monu, Sharma, Pratibha, Joon, Priya, Kumar, Anil, Kumar, Deepak, Section editor, Sobti, R. C., editor, Ganguly, Nirmal K., editor, and Kumar, Rakesh, editor

Published

2024

45. Genetic Modulation of Anticancer Drugs Affecting Pharmacokinetic for Safety and Efficacy

Author

Kaushik, Ayansh, Mallan, Sudhanshu, Chib, Shivani, Chauhan, Kanupriya, Singh, Shamsher, Kumar, Anil, Section editor, Kumar, Deepak, Section editor, Sobti, R. C., editor, Ganguly, Nirmal K., editor, and Kumar, Rakesh, editor

Published

2024

46. DNA Cleavage and Cytotoxic Activity of Copper(II) Complexes Based on Reduced Schiff Bases Derived From Salicylaldehyde and Amino Acids

Author

Korcová Jana, Húserková Mária, Lintnerová Lucia, and Valentová Jindra

Subjects

copper(ii) complexes, anticancer drugs, dna cleavage activity, cytotoxicity, Therapeutics. Pharmacology, RM1-950

Abstract

Metal complexes, which, under physiologic conditions, show redox properties and are able to bind to DNA, are great tools to cleave the DNA chain. This aspect is of great importance for their use as antineoplastic drugs. We synthesized ligands derived from short-chain amino acids and from salicylaldehyde. The prepared ligands of the type of reduced Schiff bases were subsequently used for the preparation of copper(II) complexes. The aim of the study was in vitro testing of copper(II) complexes, where it was confirmed that they are capable of cleaving DNA. Their cytotoxic activity was also confirmed by the resazurin redox method on Saccharomyces cerevisiae based on preserved healthy mitochondrial function.

Published

2024

47. A Comprehensive View on Drugs-Induced Cardiotoxicity and Its Prevention

Author

Abdulnaser Ali, Musab Khalaf, and Abdulla A. Ahmad

Subjects

cardiotoxicity, anticancer drugs, cardioprotection, antioxidants, Pharmacy and materia medica, RS1-441

Abstract

Background: The prevention of drug-induced cardiotoxicity is a complicated challenge facing healthcare providers during the last few decades. This challenge is raised from the unclear definition of the term “cardiotoxicity”, the overlapping of the symptoms of heart dysfunction due to the underlying diseases and the used drugs or using a combination of drugs which makes it difficult to distinguish between the side effects of each drug. Objective: This review discusses the most causative agents of cardiotoxicity, and their mechanisms to induce cardiac muscle damage, and finally focuses on the most applicable methods to deal with these dangerous heart problems. Methods: The search method involved electronic databases, including PubMed, Web of Science, Springer, Google Scholar, and others to resume relevant trials of heart disease published in the period between 2010-2023. Conclusion: Cardiotoxicity is a common substantial adverse effect of many drugs including anticancer drugs and others. The prevention methods may include medications, such as (Enalapril or carvedilol), supplementation with antioxidants, or cardioprotective natural products.

Published

2024

48. Comparison of two-dimensional and three-dimensional culture systems and their responses to chemotherapy in cells representing disease progression of high-grade serous ovarian cancer

Author

Naya El Mokbel, Alicia A. Goyeneche, Rewati Prakash, Benjamin N. Forgie, Farah H. Abdalbari, Xing Zeng, Basile Tessier-Cloutier, Shuk On Annie Leung, and Carlos M. Telleria

Subjects

Ultra-low attachment, Anchorage-free, 3D culture, 2D culture, High grade serous ovarian cancer, Anticancer drugs, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

High-grade serous cancer is the most common type of ovarian cancer and is usually diagnosed at advanced stages with high mortality due to recurrence and eventual resistance to standard platinum therapy. The aim of this study was to compare two-dimensional (2D) versus tridimensional (3D) cell culture as a preclinical model of response to carboplatin, paclitaxel and niraparib using PEO1, PEO4 and PEO6 cell lines, which were generated from the same patient along disease progression. Morphologically, cells formed flat adherent layers versus spheroidal structures with different compaction patterns in 2D and 3D respectively. In 2D, apoptosis was rare whereas in 3D cells formed a multilayered structure with an outer layer of live proliferating cells and an inner core of apoptotic cells. Furthermore, a differential capacity to produce ATP was observed among the cell lines in 3D but not in 2D. While response to carboplatin, paclitaxel and niraparib in both settings followed a similar trend, a lower sensitivity was observed in 3D with respect to 2D. Overall, 3D cell culture is likely more reflective of the in vivo cellular tumor behavior and more suitable of therapeutic evaluation given its added complexity absent in 2D.

Published

2024

49. Advances in the delivery of anticancer drugs by nanoparticles and chitosan-based nanoparticles

Author

Prieložná Jarmila, Mikušová Veronika, and Mikuš Peter

Subjects

Anticancer drugs, Organic and inorganic nanoparticles, Lipid and polymeric nanoparticles, Chitosan, Chitosan derivatives, Nanoparticulate drug delivery systems, Pharmacy and materia medica, RS1-441

Abstract

Cancer is the leading cause of death globally, and conventional treatments have limited efficacy with severe side effects. The use of nanotechnology has the potential to reduce the side effects of drugs by creating efficient and controlled anticancer drug delivery systems. Nanoparticles (NPs) used as drug carriers offer several advantages, including enhanced drug protection, biodistribution, selectivity and, pharmacokinetics. Therefore, this review is devoted to various organic (lipid, polymeric) as well as inorganic nanoparticles based on different building units and providing a wide range of potent anticancer drug delivery systems. Within these nanoparticulate systems, chitosan (CS)-based NPs are discussed with particular emphasis due to the unique properties of CS and its derivatives including non-toxicity, biodegradability, mucoadhesivity, and tunable physico-chemical as well as biological properties allowing their alteration to specifically target cancer cells. In the context of streamlining the nanoparticulate drug delivery systems (DDS), innovative nanoplatform-based cancer therapy pathways involving passive and active targeting as well as stimuli-responsive DDS enhancing overall orthogonality of developed NP-DDS towards the target are included. The most up-to-date information on delivering anti-cancer drugs using modern dosage forms based on various nanoparticulate systems and, specifically, CSNPs, are summarised and evaluated concerning their benefits, limitations, and advanced applications.

Published

2024

50. Modulation of the photobehavior of gefitinib and its phenolic metabolites by human transport proteins.

Author

Tamarit, Lorena, El Ouardi, Meryem, Lence, Emilio, Andreu, Inmaculada, González-Bello, Concepcion, Miranda, Miguel A., and Vayá, Ignacio

Subjects

CARRIER proteins, PROTEIN transport, FLUORESCENCE yield, METABOLITES, AMINO acid residues, ALBUMINS

Abstract

The photobiological damage that certain drugs or their metabolites can photosensitize in proteins is generally associated with the nature of the excited species that are generated upon interaction with UVA light. In this regard, the photoinduced damage of the anticancer drug gefitinib (GFT) and its two main photoactive metabolites GFT-M1 and GFT-M2 in cellular milieu was recently investigated. With this background, the photophysical properties of both the drug and its metabolites have now been studied in the presence of the two main transport proteins of human plasma, i.e., serum albumin (HSA) and α1-acid glycoprotein (HAG) upon UVA light excitation. In general, the observed photobehavior was strongly affected by the confined environment provided by the protein. Thus, GFT-M1 (which exhibits the highest phototoxicity) showed the highest fluorescence yield arising from long-lived HSA-bound phenolate-like excited species. Conversely, locally excited (LE) states were formed within HAG, resulting in lower fluorescence yields. The reserve was true for GFT-M2, which despite being also a phenol, led mainly to formation of LE states within HSA, and phenolate-like species (with a minor contribution of LE) inside HAG. Finally, the parent drug GFT, which is known to form LE states within HSA, exhibited a parallel behavior in the two proteins. In addition, determination of the association constants by both absorption and emission spectroscopy revealed that the two metabolites bind stronger to HSA than the parent drug, whereas smaller differences were observed for HAG. This was further confirmed by studying the competing interactions between GFT or its metabolites with the two proteins using fluorescence measurements. These above experimental findings were satisfactorily correlated with the results obtained by means of molecular dynamics (MD) simulations, which revealed the high affinity binding sites, the strength of interactions and the involved amino acid residues. In general, the differences observed in the photobehavior of the drug and its two photoactive metabolites in protein media are consistent with their relative photosensitizing potentials. [ABSTRACT FROM AUTHOR]

Published

2024