Lokale Applikation von Mitoxantron beim inoperablen, stenosierenden Oesophaguskarzinom

Hoffmanns, Hans; G, Altmeier

doi:10.1159/000215955

Cited by 4 publications

(2 citation statements)

References 5 publications

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“…MIT is FDA-approved for the treatment of numerous human cancers, but not yet for esophageal cancer [ 24 ]. It has been reported to induce transitory subjective and objective response without significant local or systemic side effects in five patients with inoperable, recurrent esophageal cancer after local administration [ 42 ]. Mechanistically, MIT mainly acts through intercalation with the DNA molecule, which in turn causes single- and double-stranded disruptions and suppresses DNA repair via inhibition of topoisomerase II.…”

Section: Discussionmentioning

confidence: 99%

Small molecule screen identifies pyrimethamine as an inhibitor of NRF2-driven esophageal hyperplasia

Paiboonrungruang,

Xiong,

Lamson

et al. 2023

Redox Biology

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Section: Discussionmentioning

confidence: 99%

Small molecule screen identifies pyrimethamine as an inhibitor of NRF2-driven esophageal hyperplasia

Paiboonrungruang,

Xiong,

Lamson

et al. 2023

Redox Biology

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“…To the best of our knowledge, very little data has been reported regarding the efficacy of mitoxantrone in esophageal cancer. Hoffmanns et al performed a preliminary clinical study, which demonstrated the efficacy of mitoxantrone in five inoperable, recurrent esophageal carcinoma patients [ 45 ]. In each patient, they observed transitory subjective and objective responses.…”

Section: Discussionmentioning

confidence: 99%

Genome-Wide DNA Methylation and Gene Expression Profiling Characterizes Molecular Subtypes of Esophagus Squamous Cell Carcinoma for Predicting Patient Survival and Immunotherapy Efficacy

Zheng

Gao

et al. 2022

Cancers

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Background: Immunotherapy is recently being used to treat esophageal squamous cell carcinoma (ESCC); however, response and survival benefits are limited to a subset of patients. A better understanding of the molecular heterogeneity and tumor immune microenvironment in ESCC is needed for improving disease management. Methods: Based on the DNA methylation and gene expression profiles of ESCC patients, we identify molecular subtypes of patients and construct a predictive model for subtype classification. The clinical value of molecular subtypes for the prediction of immunotherapy efficacy is assessed in an independent validation cohort of Chinese ESCC patients who receive immunotherapy. Results: We identify two molecular subtypes of ESCC (S1 and S2) that are associated with distinct immune-related pathways, tumor microenvironment and clinical outcomes. Accordingly, S2 subtype patients had a poorer prognosis. A 15-gene expression signature is developed to classify molecular subtypes with an overall accuracy of 94.7% (89/94, 95% CI: 0.880–0.983). The response rate of immunotherapy is significantly higher in the S1 subtype than in the S2 subtype patients (68.75% vs. 25%, p = 0.028). Finally, potential target drugs, including mitoxantrone, are identified for treating patients of the S2 subtype. Conclusions: Our findings demonstrated that the identified molecular subtypes constitute a promising prognostic and predictive biomarker to guide the clinical care of ESCC patients.

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Magenkarzinome

Raab¹

1991

Palliative Krebstherapie

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Lokale Applikation von Mitoxantron beim inoperablen, stenosierenden Oesophaguskarzinom

Cited by 4 publications

References 5 publications

Small molecule screen identifies pyrimethamine as an inhibitor of NRF2-driven esophageal hyperplasia

Small molecule screen identifies pyrimethamine as an inhibitor of NRF2-driven esophageal hyperplasia

Genome-Wide DNA Methylation and Gene Expression Profiling Characterizes Molecular Subtypes of Esophagus Squamous Cell Carcinoma for Predicting Patient Survival and Immunotherapy Efficacy

Magenkarzinome

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