Temozolomide, Procarbazine and Nitrosoureas in the Therapy of Malignant Gliomas: Update of Mechanisms, Drug Resistance and Therapeutic Implications

Kaina, Bernd

doi:10.3390/jcm12237442

Cited by 7 publications

(8 citation statements)

References 175 publications

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“…Many studies have shown that different mechanisms are involved in TMZ sensitivity or resistance. Various anticancer drugs have been used to increase the sensitivity of cancer cells to TMZ therapy py [ 57 , 58 ]. Oxyphyllanene B can cause TMZ sensitivity by overexpressing PACS2, which can interfere with and impair connection between the endoplasmic reticulum and mitochondria [ 50 ].…”

Section: Temozolomide In Chemotherapy: From History To Molecular Mech...mentioning

confidence: 99%

The landscape of circRNAs in gliomas temozolomide resistance: Insights into molecular pathways

Mafi,

Hedayati,

Kahkesh

et al. 2024

Non-coding RNA Research

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Section: Temozolomide In Chemotherapy: From History To Molecular Mech...mentioning

confidence: 99%

The landscape of circRNAs in gliomas temozolomide resistance: Insights into molecular pathways

Mafi,

Hedayati,

Kahkesh

et al. 2024

Non-coding RNA Research

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“…TMZ is, in clinical use, part of the standard of care for the chemoradiation treatment of glioblastoma (GBM). Its primary cytotoxic mode of action is methylation of the O6-position of guanine, which results in DNA double-strand breaks and subsequent apoptosis [ 28 ]. However, this process does not work in cells that express the DNA repair protein O6-methylguanine-DNA methyltransferase (MGMT), because MGMT is able to effectively remove the methyl group from the O6-position of guanine, thereby disposing of the toxic lesion and providing chemoresistance [ 29 ].…”

Section: Introductionmentioning

confidence: 99%

Activation of Epstein–Barr Virus’ Lytic Cycle in Nasopharyngeal Carcinoma Cells by NEO212, a Conjugate of Perillyl Alcohol and Temozolomide

Hartman-Houstman,

Swenson,

Minea

et al. 2024

Cancers

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The Epstein–Barr virus (EBV) is accepted as a primary risk factor for certain nasopharyngeal carcinoma (NPC) subtypes, where the virus persists in a latent stage which is thought to contribute to tumorigenesis. Current treatments are sub-optimal, and recurrence occurs in many cases. An alternative therapeutic concept is aimed at triggering the lytic cycle of EBV selectively in tumor cells as a means to add clinical benefit. While compounds able to stimulate the lytic cascade have been identified, their clinical application so far has been limited. We are developing a novel anticancer molecule, NEO212, that was generated by covalent conjugation of the alkylating agent temozolomide (TMZ) to the naturally occurring monoterpene perillyl alcohol (POH). In the current study, we investigated its potential to trigger the lytic cycle of EBV in NPC cells in vitro and in vivo. We used the established C666.1 cell line and primary patient cells derived from the brain metastasis of a patient with NPC, both of which harbored latent EBV. Upon treatment with NEO212, there was an increase in EBV proteins Zta and Ea-D, key markers of the lytic cycle, along with increased levels of CCAAT/enhancer-binding protein homologous protein (CHOP), a marker of endoplasmic reticulum (ER) stress, followed by the activation of caspases. These effects could also be confirmed in tumor tissue from mice implanted with C666.1 cells. Towards a mechanistic understanding of these events, we used siRNA-mediated knockdown of CHOP and inclusion of anti-oxidant compounds. Both approaches blocked lytic cycle induction by NEO212. Therefore, we established a sequence of events, where NEO212 caused reactive oxygen species (ROS) production, which triggered ER stress and elevated the levels of CHOP, which was required to stimulate the lytic cascade of EBV. Inclusion of the antiviral agent ganciclovir synergistically enhanced the cytotoxic impact of NEO212, pointing to a potential combination treatment for EBV-positive cancers which should be explored further. Overall, our study establishes NEO212 as a novel agent able to stimulate EBV’s lytic cycle in NPC tumors, with implications for other virus-associated cancers.

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“…Gliom present a more alkaline environment compared to surrounding healthy brain cells, le ing to drug activation [1,3,4,7,8] almost exclusively in the tumor cells [1,7,8,13,14]. Mor ver, senescence induced by TMZ is another phenomenon that should also be mention TMZ senescent GB cells overexpress NF-kB and lead to inflammatory cytokines' prod tion, such as IL6 and IL8; thus, these cells seem not to be eliminated after TMZ and rad therapy and tend to be present even in recurrence of the tumor, with a not yet fully cla fied role [15]. Due to the highly heterogeneous and mutation-prone nature of GB, resistance to TMZ is developed and accounts for over 50% of GB patients that eventually fail to respond to the therapy [16].…”

Section: Introductionmentioning

confidence: 99%

“…Moreover, senescence induced by TMZ is another phenomenon that should also be mentioned. TMZ senescent GB cells overexpress NF-kB and lead to inflammatory cytokines’ production, such as IL6 and IL8; thus, these cells seem not to be eliminated after TMZ and radiotherapy and tend to be present even in recurrence of the tumor, with a not yet fully clarified role [ 15 ].…”

Section: Introductionmentioning

confidence: 99%

Overcoming Resistance to Temozolomide in Glioblastoma: A Scoping Review of Preclinical and Clinical Data

Smerdi,

Moutafi,

Kotsantis

et al. 2024

Life

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Glioblastoma (GB) is the most common and most aggressive primary brain tumor in adults, with an overall survival almost 14.6 months. Optimal resection followed by combined temozolomide chemotherapy and radiotherapy, also known as Stupp protocol, remains the standard of treatment; nevertheless, resistance to temozolomide, which can be obtained throughout many molecular pathways, is still an unsurpassed obstacle. Several factors influence the efficacy of temozolomide, including the involvement of other DNA repair systems, aberrant signaling pathways, autophagy, epigenetic modifications, microRNAs, and extracellular vesicle production. The blood–brain barrier, which serves as both a physical and biochemical obstacle, the tumor microenvironment’s pro-cancerogenic and immunosuppressive nature, and tumor-specific characteristics such as volume and antigen expression, are the subject of ongoing investigation. In this review, preclinical and clinical data about temozolomide resistance acquisition and possible ways to overcome chemoresistance, or to treat gliomas without restoration of chemosensitinity, are evaluated and presented. The objective is to offer a thorough examination of the clinically significant molecular mechanisms and their intricate interrelationships, with the aim of enhancing understanding to combat resistance to TMZ more effectively.

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Temozolomide, Procarbazine and Nitrosoureas in the Therapy of Malignant Gliomas: Update of Mechanisms, Drug Resistance and Therapeutic Implications

Cited by 7 publications

References 175 publications

The landscape of circRNAs in gliomas temozolomide resistance: Insights into molecular pathways

The landscape of circRNAs in gliomas temozolomide resistance: Insights into molecular pathways

Activation of Epstein–Barr Virus’ Lytic Cycle in Nasopharyngeal Carcinoma Cells by NEO212, a Conjugate of Perillyl Alcohol and Temozolomide

Overcoming Resistance to Temozolomide in Glioblastoma: A Scoping Review of Preclinical and Clinical Data

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