Targeting Neuroinflammation in Brain Cancer: Uncovering Mechanisms, Pharmacological Targets, and Neuropharmaceutical Developments.
Mahmoud S. Alghamri,Brandon L. McClellan,Margaret S. Hartlage,Santiago Haase,Syed M Faisal,Rohit Thalla,Ali Dabaja,Kaushik Banerjee,Stephen Carney,Anzar A. Mujeeb,Michael R. Olin,James J. Moon,Anna Schwendeman,Pedro R. Lowenstein,Maria G. Castro +14 more
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TLDR
Glioblastomas are one of the most lethal types of cancers accounting for ~80% of all central nervous system (CNS) primary malignancies [1, as discussed by the authors.Abstract:
Gliomas are one of the most lethal types of cancers accounting for ~80% of all central nervous system (CNS) primary malignancies [1; 2]. Amongst gliomas, glioblastomas (GBM) are the most aggressive, characterized by a median patient survival of fewer than 15 months. Recent molecular characterization studies uncovered the genetic signatures and methylation status of gliomas and correlate these with clinical prognosis [2]. The most relevant molecular characteristics for the new glioma classification are IDH mutation, chromosome 1p/19q deletion, histone mutations, and other genetic parameters such as ATRX loss, TP53, and TERT mutations, as well as DNA methylation levels. Similar to other solid tumors, glioma progression is impacted by the complex interactions between the tumor cells and immune cells within the tumor microenvironment. The immune system’s response to cancer can impact the glioma’s survival, proliferation, and invasiveness. Salient characteristics of gliomas include enhanced vascularization, stimulation of a hypoxic tumor microenvironment, increased oxidative stress, and an immune suppressive milieu. These processes promote the neuro-inflammatory tumor microenvironment which can lead to the loss of blood-brain barrier (BBB) integrity. The consequences of a compromised BBB are deleteriously exposing the brain to potentially harmful concentrations of substances from the peripheral circulation, adversely affecting neuronal signaling, and abnormal immune cell infiltration; all of which can lead to disruption of brain homeostasis. In this review, we first describe the unique features of inflammation in CNS tumors. We then discuss the mechanisms of tumor-initiating neuro-inflammatory microenvironment and its impact on tumor invasion and progression. Finally, we also discuss potential pharmacological interventions that can be used to target neuro-inflammation in gliomas.read more
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TSPO PET signal using [18F]GE180 is associated with survival in recurrent gliomas
S. Quach,Adrien Holzgreve,Lena Kaiser,Marcus Unterrainer,Franziska J. Dekorsy,Debie Nelwan,L. Bartos,S V Kirchleitner,Jonathan Weller,Lorraine Weidner,Maximilian Niyazi,Viktoria Ruf,Jochen Herms,Sophia Stöcklein,Christian H. Wetzel,Markus J. Riemenschneider,Louisa V Baumgarten,Niklas Thon,Matthias Brendel,Rainer Rupprecht,Peter Bartenstein,Jörg C. Tonn,Nathalie L. Albert +22 more
TL;DR: In this paper , the authors correlated the TSPO positron emission tomography (PET) signal using [18F]GE180 in a large cohort of recurrent glioma patients with their clinical outcome.
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Development of immunotherapy for high-grade gliomas: Overcoming the immunosuppressive tumor microenvironment
Andrea Franson,Brandon L. McClellan,María Luisa Varela,Andrea Comba,Mohammad Faisal Syed,Kaushik Banerjee,Ziwen Zhu,Nazareno González,Marianela Candolfi,Pedro R. Lowenstein,Maria G. Castro +10 more
TL;DR: A review of the TME and immunotherapy development in HGG with a specific focus on glioblastoma multiforme (GBM) as well as additional discussion in the context of the pediatric HGG diagnoses of diffuse midline glioma (DMG) and diffuse hemispheric gliomas (DHG).
Journal ArticleDOI
The complex interactions between the cellular and non-cellular components of the brain tumor microenvironmental landscape and their therapeutic implications
Syed M. Faisal,Andrea Comba,María Luisa Varela,Anna E Argento,Emily K. Brumley,Clifford Abel,Maria G. Castro,Pedro R. Lowenstein +7 more
TL;DR: The complexity of the interactions between the cellular and non-cellular components of the TME and advances in the field as a whole are discussed to guide the development of safe and effective therapeutic strategies against brain cancer.
Journal ArticleDOI
Choroid plexus-derived extracellular vesicles exhibit brain targeting characteristics.
Marie Pauwels,Junhua Xie,Adam Ceroi,Sriram Balusu,Jonas Castelein,Elien Van Wonterghem,Griet Van Imschoot,Andrew D. Ward,Trevelyan R. Menheniott,Oskar Gustafsson,Francis Combes,Samir El Andaloussi,Niek N. Sanders,Imre Mäger,Lien Van Hoecke,Roosmarijn E. Vandenbroucke +15 more
TL;DR: In this paper , extracellular vesicles (EVs) make up a natural mechanism for information transfer between cells and across cell layers, has stimulated interest in their potential use as drug delivery platform.
Posted ContentDOI
Targeted nanocarriers coopting pulmonary leukocytes for drug delivery to the injured brain
Patrick M. Glassman,Jiaying Nong,Jacob W. Myerson,Viviana Zuluaga-Ramirez,Alba Rodriguez-Garcia,Alvin J. Mukalel,Serena Omo-Lamai,Landis R. Walsh,Raisa Yu Kiseleva,Carlos H. Villa,Colin F. Greineder,Scott E. Kasner,Drew Weissman,Michael J. Mitchell,Silvia Muro,Yuri Persidsky,Jacob S. Brenner,Vladimir R. Muzykantov,Oscar A. Marcos-Contreras +18 more
TL;DR: Coopting the natural homing of WBC from the lungs via ICAM-targeting to injured brain is an attractive strategy for precise interventions for treatment of acute brain injuries.
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