Nitric Oxide Generated by Tumor-Associated Macrophages Is Responsible for Cancer Resistance to Cisplatin and Correlated With Syntaxin 4 and Acid Sphingomyelinase Inhibition

Perrotta, Cristiana; Cervia, Davide; Renzo, Ilaria Di; Moscheni, Claudia; Bassi, Maria Teresa; Campana, Lara; Martelli, Cristina; Catalani, Elisabetta; Giovarelli, Matteo; Zecchini, Silvia; Coazzoli, Marco; Capobianco, Annalisa; Ottobrini, Luisa; Lucignani, Giovanni; Rosa, Patrizia; Rovere‐Querini, Patrizia; Palma, Clara De; Clementi, Emilio

doi:10.3389/fimmu.2018.01186

Cited by 83 publications

(70 citation statements)

References 102 publications

(131 reference statements)

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“…Chemotherapeutic drugs could induce oxidative stress not only contributed to DNA damage and cell cycle arrest, but also was associated with chemoresistance. 37 Together, oxidative stress response has a significant role in chemotherapy resistance. In epithelial ovarian cancer cell lines, acquisition of specific point mutations in key redox enzymes after chemotherapeutics resulted in a boost of oxidative stress and application of antioxidant could regain high sensitivity to chemotherapy.…”

Section: Discussionmentioning

confidence: 99%

Comprehensive analysis of microRNA‐messenger RNA regulatory network in gemcitabine‐resistant bladder cancer cells

Zhang

Chang

Gong

et al. 2018

J of Cellular Biochemistry

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Chemotherapy is still a standard treatment of unresectable bladder cancer or distant metastases. The chemotherapy resistance always occurs after a period of treatment indicating poor prognosis. The current study aimed to explore the molecular mechanism of chemoresistance in bladder cancer cells. The gene expression profiles of GSE77883, including three untreated T24 cells samples and three gemcitabine‐resistant T24 cells samples, was downloaded from Gene Expression Omnibus database. The screening of differentially expressed genes (DEGs), gene function analysis, and interaction prediction between microRNAs (miRNAs) and DEGs were performed by R software. The protein‐protein interaction (PPI) and miRNA‐DEGs networks were constructed and visualized by Cytoscape software. Then, the small molecules, with potential synergistic or antagonistic effects to gemcitabine resistance, were identified using the Connectivity Map database. Finally, gemcitabine‐resistant T24 cell line was established and key genes were validated by quantitative real‐time polymerase chain reaction (qRT‐PCR). In total, 536 upregulated and 513 downregulated genes were screened and mainly enriched in oxidative stress response and signaling pathways related to extracellular matrix–receptor interaction and focal adhesion. PPI network showed interleukin 6, tumor necrosis factor, kinesin family member 11, and BUB1 mitotic checkpoint serine/threonine kinase B were key genes. The miRNA‐DEGs regulatory networks included 18 miRNAs and 185 DEGs, including miR‐182‐5p, miR‐590‐3p, miR‐320a and serum‐ and glucocorticoid‐regulated kinase 1 (SGK1). Then, the related key genes and miRNAs were confirmed by qRT‐PCR. Furthermore, 81 small molecules with antagonistic or synergistic effect to GEM were screened. We have investigated the molecular mechanisms driving GEM‐resistance in bladder cancer cells that would contribute to the development of chemotherapy for advanced bladder cancer.

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Section: Discussionmentioning

confidence: 99%

Comprehensive analysis of microRNA‐messenger RNA regulatory network in gemcitabine‐resistant bladder cancer cells

Zhang

Chang

Gong

et al. 2018

J of Cellular Biochemistry

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“…Prolonged * NO production by iNOS promoted angiogenesis and oral squamous cell carcinoma progression (19). In addition, * NO generation by tumor-associated macrophages prevented tumor cells apoptosis and caused chemoresistance to cisplatin (20). However, in breast, colorectal, epidermoid, head, and neck tumors decrease in tetrahydrobiopterin level causes NOS uncoupling and production of O 2 * À and NOO : instead of NO * to promote tumorigenesis (21).…”

Section: Elevated Rons Generation In Cancermentioning

confidence: 99%

Reactive Oxygen and Nitrogen Species–Induced Protein Modifications: Implication in Carcinogenesis and Anticancer Therapy

2018

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Cancer is a complex disorder extremely dependent on its microenvironment and highly regulated by multiple intracellular and extracellular stimuli. Studies show that reactive oxygen and nitrogen species (RONS) play key roles in cancer initiation and progression. Accumulation of RONS caused by imbalance between RONS generation and activity of antioxidant system (AOS) has been observed in many cancer types. This leads to alterations in gene expression levels, signal transduction pathways, and protein quality control machinery, that is, processes that regulate cancer cell proliferation, migration, invasion, and apoptosis. This review focuses on the latest advancements evidencing that RONS-induced modifications of key redox-sensitive residues in regulatory proteins, that is, cysteine oxidation/Ssulfenylation/S-glutathionylation/S-nitrosylation and tyro-sine nitration, represent important molecular mechanisms underlying carcinogenesis. The oxidative/nitrosative modifications cause alterations in activities of intracellular effectors of MAPK-and PI3K/Akt-mediated signaling pathways, transcription factors (Nrf2, AP-1, NFkB, STAT3, and p53), components of ubiquitin/proteasomal and autophagy/lysosomal protein degradation systems, molecular chaperones, and cytoskeletal proteins. Redox-sensitive proteins, RONSgenerating enzymes, and AOS components can serve as targets for relevant anticancer drugs. Chemotherapeutic agents exert their action via RONS generation and induction of cancer cell apoptosis, while drug resistance associates with RONS-induced cancer cell survival; this is exploited in selective anticancer therapy strategies. Cancer Res; 78(21); 6040-7.

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“…Снижение функциональной активности клеток неспецифического иммунитета некоторыми авторами рассматривается как необходимое условие развития опухоли и метастазов [63]. Однако последние экспериментальные данные показывают, что NO, источником которого является iNOS в опухолеассоциированных макрофагах, способствует усилению резистентности опухоли к терапии цисплатином, и в этом случае подавление синтеза NO ингибиторами, возможно, улучшит результаты химиотерапии [64]. Следует указать на побочные эффекты при использовании малоселективных ингибиторов iNOS, которые могут изменять активность других изоформ NOS -эндотелиальной и нейрональной, нарушая их жизненно важные функции [52].…”

Section: обзорные статьиunclassified

Modulation of the formation of active forms of nitrogen by ingredients of plant products in the inhibition of carcinogenesis

Дерягина¹,

Реутов²

2019

Usp. mol. onkol

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В обзоре анализируются данные литературы и результаты собственных исследований о роли активных форм азота (NO, NO 2 , N 2 O 3) в инициации и прогрессии опухолей. Анализируется возможность модуляции активности индуцибельной NO-синтазы биологически активными компонентами растительных продуктов и их влияние на канцерогенез. Обсуждаются возможные механизмы неоднозначного действия NO и продуктов его метаболизма в канцерогенезе. Обобщение и анализ этих данных позволили сформулировать некоторые принципы применения веществ, модулирующих активность индуцибельной NO-синтазы и влияющих на образование NO и продуктов его метаболизма при ингибировании канцерогенеза.

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Nitric Oxide Generated by Tumor-Associated Macrophages Is Responsible for Cancer Resistance to Cisplatin and Correlated With Syntaxin 4 and Acid Sphingomyelinase Inhibition

Cited by 83 publications

References 102 publications

Comprehensive analysis of microRNA‐messenger RNA regulatory network in gemcitabine‐resistant bladder cancer cells

Comprehensive analysis of microRNA‐messenger RNA regulatory network in gemcitabine‐resistant bladder cancer cells

Reactive Oxygen and Nitrogen Species–Induced Protein Modifications: Implication in Carcinogenesis and Anticancer Therapy

Modulation of the formation of active forms of nitrogen by ingredients of plant products in the inhibition of carcinogenesis

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