Creation of Non-Contact Device for Use in Metastatic Melanoma Margin Identification in <i>ex vivo</i> Mouse Brain.

dc.contributor.author

Tucker, Matthew

dc.contributor.author

Lacayo, Matthew

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Joseph, Suzanna

dc.contributor.author

Ross, Weston

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Chongsathidkiet, Pakawat

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Fecci, Peter

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Codd, Patrick J

dc.contributor.editor

Yang, Victor XD

dc.contributor.editor

Kainerstorfer, Jana M

dc.date.accessioned

2023-11-28T16:43:02Z

dc.date.available

2023-11-28T16:43:02Z

dc.date.issued

2022-01

dc.date.updated

2023-11-28T16:42:59Z

dc.description.abstract

Because contemporary intraoperative tumor detection modalities, such as intraoperative MRI, are not ubiquitously available and can disrupt surgical workflow, there is an imperative for an accessible diagnostic device that can meet the surgeon's needs in identifying tissue types. The objective of this paper is to determine the efficacy of a novel non-contact tumor detection device for metastatic melanoma boundary identification in a tissue-mimicking phantom, evaluate the identification of metastatic melanoma boundaries in ex vivo mouse brain tissue, and find the error associated with identifying this boundary. To validate the spatial and fluorescence resolution of the device, tissue-mimicking phantoms were created with modifiable optical properties. Phantom tissue provided ground truth measurements for fluorophore concentration differences with respect to spatial dimensions. Modeling metastatic disease, ex vivo melanoma brain metastases were evaluated to detect differences in fluorescence between healthy and neoplastic tissue. This analysis includes determining required-to-observe fluorescence differences in tissue. H&E staining confirmed tumor presence in mouse tissue samples. The device detected a difference in normalized average fluorescence intensity in all three phantoms. There were differences in fluorescence with the presence and absence of melanin. The estimated tumor boundary of all tissue phantoms was within 0.30 mm of the ground truth tumor boundary for all boundaries. Likewise, when applied to the melanoma-bearing brains from ex vivo mice, a difference in normalized fluorescence intensity was successfully detected. The potential prediction window for the tumor boundary location is less than 1.5 mm for all ex vivo mouse brain tumors boundaries. We present a non-contact, laser-induced fluorescence device that can identify tumor boundaries based on changes in laser-induced fluorescence emission intensity. The device can identify phantom ground truth tumor boundaries within 0.30 mm using instantaneous rate of change of normalized fluorescence emission intensity and can detect endogenous fluorescence differences in melanoma brain metastases in ex vivo mouse tissue.

dc.identifier

1194507

dc.identifier.issn

0277-786X

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1996-756X

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https://hdl.handle.net/10161/29425

dc.language

eng

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SPIE

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Proceedings of SPIE--the International Society for Optical Engineering

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10.1117/12.2608975

dc.subject

Brain metastasis

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Endogenous fluorescence

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Melanoma

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Tumor boundary detection

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Warburg Effect

dc.title

Creation of Non-Contact Device for Use in Metastatic Melanoma Margin Identification in ex vivo Mouse Brain.

dc.type

Journal article

duke.contributor.orcid

Ross, Weston|0009-0002-6214-2189

duke.contributor.orcid

Fecci, Peter|0000-0002-2912-8695

pubs.begin-page

1194507

pubs.organisational-group

Duke

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Pratt School of Engineering

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School of Medicine

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Basic Science Departments

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Clinical Science Departments

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Institutes and Centers

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Integrative Immunobiology

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Biomedical Engineering

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Thomas Lord Department of Mechanical Engineering and Materials Science

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Pathology

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Duke Cancer Institute

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Institutes and Provost's Academic Units

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Initiatives

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Neurosurgery

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Duke Innovation & Entrepreneurship

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Head and Neck Surgery & Communication Sciences

pubs.publication-status

Published

pubs.volume

11945

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