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Neuronal exposure induces neurotransmitter signaling and synaptic mediators in tumors early in brain metastasis.


ABSTRACT:

Background

Brain metastases (BM) are responsible for neurological decline and poor overall survival. Although the pro-metastatic roles of glial cells, and the acquisition of neuronal attributes in established BM tumors have been described, there are no studies that investigate the initial interplay between neurons and brain-seeking tumor cells. The aim of this study was to characterize early tumor-neuron interactions and the induced CNS-adaptive changes in tumor cells prior to macro-colonization.

Methods

Utilizing pure neuronal cultures and brain-naïve and patient-derived BM tumor cells, we surveyed the early induction of mediators of neurotransmitter (NT) and synaptic signaling in breast and lung tumor cells. Reliance on microenvironmental GABA in breast-to-brain metastatic cells (BBMs) was assessed in vitro and in vivo.

Results

Coculture with neurons induces early expression of classical NT receptor genes (HTR4, GRIA2, GRIN2B, GRM4, GRM8, DRD1) and neuronal synaptic mediators (CNR1, EGR2, ARC, NGFR, NRXN1) in breast and lung cancer cells. NT-dependent classification of tumor cells within the neuronal niche shows breast cancer cells become GABAergic responsive brain metastases (GRBMs) and transition from relying on autocrine GABA, to paracrine GABA from adjacent neurons; while autocrine Dopaminergic breast and lung tumor cells persist. In vivo studies confirm reliance on paracrine GABA is an early CNS-acclimation strategy in breast cancer. Moreover, neuronal contact induces early resurgence in Reelin expression in tumor cells through epigenetic activation, facilitating CNS adaptation.

Conclusion

Tumor-neuron interactions allow for CNS adaptation early in the course of brain metastasis.

SUBMITTER: Deshpande K 

PROVIDER: S-EPMC9159425 | biostudies-literature | 2022 Jun

REPOSITORIES: biostudies-literature

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Publications

Neuronal exposure induces neurotransmitter signaling and synaptic mediators in tumors early in brain metastasis.

Deshpande Krutika K   Martirosian Vahan V   Nakamura Brooke Naomi BN   Iyer Mukund M   Julian Alex A   Eisenbarth Rachel R   Shao Ling L   Attenello Frank F   Neman Josh J  

Neuro-oncology 20220601 6


<h4>Background</h4>Brain metastases (BM) are responsible for neurological decline and poor overall survival. Although the pro-metastatic roles of glial cells, and the acquisition of neuronal attributes in established BM tumors have been described, there are no studies that investigate the initial interplay between neurons and brain-seeking tumor cells. The aim of this study was to characterize early tumor-neuron interactions and the induced CNS-adaptive changes in tumor cells prior to macro-colo  ...[more]

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