Potential predictive biomarker for response to radiotherapy and CXCL12 inhibition in glioblastoma in the phase I/II GLORIA trial.

Giordano, Frank A.; Layer, Julian Philipp; Friker, Lea Lydia; Turiello, Roberta; Corvino, Dillon; Zeyen, Thomas; Schaub, Christina; Mueller, Wolf; Sperk, Elena; Schmeel, Leonard Christopher; Sahm, Katharina; Kebir, Sied; Hambsch, Peter; Pietsch, Torsten; Bisdas, Sotirios; Glas, Martin; Seidel, Clemens; Herrlinger, Ulrich; Hölzel, Michael

doi:10.1200/jco.2023.41.16_suppl.2048

Cited by 2 publications

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“…To date, just one clinical trial has assayed aptamers for GB treatment (NCT04121455). The first and only clinical trial to date using aptamer NOX-A12 in GB patients showed promising results and was well tolerated with no dose-limiting toxicities or treatment-related deaths, which is specifically interesting because it has been assayed in GB patients with unmethylated promoters [ 945 ]. The addition of the CXCL12 inhibitor NOX-A12 (olaptesed pegol) to SOC and BEV led to an overall OS rate of 83% (n = 5/6) at a median follow-up of 15 months in ndGB patients, according to preliminary data from an expansion arm of the phase 1/2 GLORIA trial [ 945 ].…”

Section: Nanotherapiesmentioning

confidence: 99%

Glioblastoma Therapy: Past, Present and Future

Obrador,

Moreno-Murciano,

Oriol-Caballo

et al. 2024

IJMS

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Glioblastoma (GB) stands out as the most prevalent and lethal form of brain cancer. Although great efforts have been made by clinicians and researchers, no significant improvement in survival has been achieved since the Stupp protocol became the standard of care (SOC) in 2005. Despite multimodality treatments, recurrence is almost universal with survival rates under 2 years after diagnosis. Here, we discuss the recent progress in our understanding of GB pathophysiology, in particular, the importance of glioma stem cells (GSCs), the tumor microenvironment conditions, and epigenetic mechanisms involved in GB growth, aggressiveness and recurrence. The discussion on therapeutic strategies first covers the SOC treatment and targeted therapies that have been shown to interfere with different signaling pathways (pRB/CDK4/RB1/P16ink4, TP53/MDM2/P14arf, PI3k/Akt-PTEN, RAS/RAF/MEK, PARP) involved in GB tumorigenesis, pathophysiology, and treatment resistance acquisition. Below, we analyze several immunotherapeutic approaches (i.e., checkpoint inhibitors, vaccines, CAR-modified NK or T cells, oncolytic virotherapy) that have been used in an attempt to enhance the immune response against GB, and thereby avoid recidivism or increase survival of GB patients. Finally, we present treatment attempts made using nanotherapies (nanometric structures having active anti-GB agents such as antibodies, chemotherapeutic/anti-angiogenic drugs or sensitizers, radionuclides, and molecules that target GB cellular receptors or open the blood–brain barrier) and non-ionizing energies (laser interstitial thermal therapy, high/low intensity focused ultrasounds, photodynamic/sonodynamic therapies and electroporation). The aim of this review is to discuss the advances and limitations of the current therapies and to present novel approaches that are under development or following clinical trials.

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Section: Nanotherapiesmentioning

confidence: 99%

Glioblastoma Therapy: Past, Present and Future

Obrador,

Moreno-Murciano,

Oriol-Caballo

et al. 2024

IJMS

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Immunotherapeutic Strategies for the Treatment of Glioblastoma: Current Challenges and Future Perspectives

Salvato,

Marchini

2024

Cancers

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Despite decades of research and the best up-to-date treatments, grade 4 Glioblastoma (GBM) remains uniformly fatal with a patient median overall survival of less than 2 years. Recent advances in immunotherapy have reignited interest in utilizing immunological approaches to fight cancer. However, current immunotherapies have so far not met the anticipated expectations, achieving modest results in their journey from bench to bedside for the treatment of GBM. Understanding the intrinsic features of GBM is of crucial importance for the development of effective antitumoral strategies to improve patient life expectancy and conditions. In this review, we provide a comprehensive overview of the distinctive characteristics of GBM that significantly influence current conventional therapies and immune-based approaches. Moreover, we present an overview of the immunotherapeutic strategies currently undergoing clinical evaluation for GBM treatment, with a specific emphasis on those advancing to phase 3 clinical studies. These encompass immune checkpoint inhibitors, adoptive T cell therapies, vaccination strategies (i.e., RNA-, DNA-, and peptide-based vaccines), and virus-based approaches. Finally, we explore novel innovative strategies and future prospects in the field of immunotherapy for GBM.

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Potential predictive biomarker for response to radiotherapy and CXCL12 inhibition in glioblastoma in the phase I/II GLORIA trial.

Cited by 2 publications

References 0 publications

Glioblastoma Therapy: Past, Present and Future

Glioblastoma Therapy: Past, Present and Future

Immunotherapeutic Strategies for the Treatment of Glioblastoma: Current Challenges and Future Perspectives

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