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Active NON-SBIR/STTR RPGS NIH (US)

Neural Activity Signatures of Tumor Infiltration in the Human Brain

$6.19M USD

Funder NATIONAL INSTITUTE OF NEUROLOGICAL DISORDERS AND STROKE
Recipient Organization Massachusetts General Hospital
Country United States
Start Date Sep 01, 2024
End Date Jul 31, 2029
Duration 1,794 days
Number of Grantees 1
Roles Principal Investigator
Data Source NIH (US)
Grant ID 10942268
Grant Description

ABSTRACT In brain cancer, tumor cells form complex interactions with cells in the brain. Recent studies have revealed a complex interaction between brain cells, or neurons, and tumor cells. Specifically, tumor cells infiltrate healthy brain tissue inducing increased neuron activity and connectivity, particularly among a one

class of brain cells (excitatory neurons), making brain tissue more excitable in the process. This increase in excitability is thought to act as an accelerant for increased tumor infiltration into healthy neural tissue. Conversely, another class of neurons, inhibitory neurons, are degraded during tumor cell infiltration. This

feedback loop leads to further spread of tumor into healthy brain tissue, particularly as the excitation- inhibition balance essential for normal brain function is tipped toward excitation. This imbalance is thought to be a reason for 40-80% of glioma patients developing epilepsy. However, this detailed, intricate, and

devastating process of tumor infiltration has only been detailed through studies in non-human animals and in surgically removed tissue samples, with little to no information on how tumor-induced changes alter activity in the intact human brain. In addition to FDA-approved clinical electrodes, we propose using

cutting edge high-resolution microelectrodes we pioneered for use in the human operating room to sample brain activity in, around, and far from tumor. We will use two types: 1) microelectrodes with 1000 channels printed on ultrathin materials to conforming to the surface of the brain; and 2) Neuropixels

probes which are microelectrodes which can record single cell activity across >300 channels along a probe close to the thickness of a human hair. Recording neural activity altered by tumor infiltration therefore not only offers unprecedented temporal and spatial resolution relative to current clinical

technologies but also fills a scientific gap in capturing ongoing tumor-induced changes in brain activity in the intact human brain. The goal is to provide a high-resolution dynamic physiological map of the tumor and the tumor boundary to better understand tumor infiltration in the intact brain working with patients

already scheduled for neurosurgery for the treatment of tumor following fully informed consent. We predict the tumor boundary can be identified by physiological signatures possibly providing new diagnostic tools providing high resolution information for clinical decisions in the future.

All Grantees

Massachusetts General Hospital

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