Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience

SIGNIFICANCE: High grade serous ovarian cancer is the most deadly gynecological cancer, and it is now believed that most cases originate in the fallopian tubes (FTs). Early detection of ovarian cancer could double the 5-year survival rate compared with late-stage diagnosis. Autofluorescence imaging...

Descripción completa

Detalles Bibliográficos
Autores principales: Rocha, Andrew D., Drake, William K., Rice, Photini F., Long, Dilara J., Shir, Hasina, Walton, Ryan H. M., Reed, Mary N., Galvez, Dominique, Gorman, Taliah, Heusinkveld, John M., Barton, Jennifer K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Society of Photo-Optical Instrumentation Engineers 2023
Materias:
Special Section on Selected Topics in Biophotonics: Translating Novel Photonics Technology into Clinical Applications
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10423010/
https://www.ncbi.nlm.nih.gov/pubmed/37577082
http://dx.doi.org/10.1117/1.JBO.28.12.121206
_version_ 1785089353624584192
author Rocha, Andrew D.
Drake, William K.
Rice, Photini F.
Long, Dilara J.
Shir, Hasina
Walton, Ryan H. M.
Reed, Mary N.
Galvez, Dominique
Gorman, Taliah
Heusinkveld, John M.
Barton, Jennifer K.
author_facet Rocha, Andrew D.
Drake, William K.
Rice, Photini F.
Long, Dilara J.
Shir, Hasina
Walton, Ryan H. M.
Reed, Mary N.
Galvez, Dominique
Gorman, Taliah
Heusinkveld, John M.
Barton, Jennifer K.
author_sort Rocha, Andrew D.
collection PubMed
description SIGNIFICANCE: High grade serous ovarian cancer is the most deadly gynecological cancer, and it is now believed that most cases originate in the fallopian tubes (FTs). Early detection of ovarian cancer could double the 5-year survival rate compared with late-stage diagnosis. Autofluorescence imaging can detect serous-origin precancerous and cancerous lesions in ex vivo FT and ovaries with good sensitivity and specificity. Multispectral fluorescence imaging (MFI) can differentiate healthy, benign, and malignant ovarian and FT tissues. Optical coherence tomography (OCT) reveals subsurface microstructural information and can distinguish normal and cancerous structure in ovaries and FTs. AIM: We developed an FT endoscope, the falloposcope, as a method for detecting ovarian cancer with MFI and OCT. The falloposcope clinical prototype was tested in a pilot study with 12 volunteers to date to evaluate the safety and feasibility of FT imaging prior to standard of care salpingectomy in normal-risk volunteers. In this manuscript, we describe the multiple modifications made to the falloposcope to enhance robustness, usability, and image quality based on lessons learned in the clinical setting. APPROACH: The [Formula: see text] diameter falloposcope was introduced via a minimally invasive approach through a commercially available hysteroscope and introducing a catheter. A navigation video, MFI, and OCT of human FTs were obtained. Feedback from stakeholders on image quality and procedural difficulty was obtained. RESULTS: The falloposcope successfully obtained images in vivo. Considerable feedback was obtained, motivating iterative improvements, including accommodating the operating room environment, modifying the hysteroscope accessories, decreasing endoscope fragility and fiber breaks, optimizing software, improving fiber bundle images, decreasing gradient-index lens stray light, optimizing the proximal imaging system, and improving the illumination. CONCLUSIONS: The initial clinical prototype falloposcope was able to image the FTs, and iterative prototyping has increased its robustness, functionality, and ease of use for future trials.
format Online
Article
Text
id pubmed-10423010
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Society of Photo-Optical Instrumentation Engineers
record_format MEDLINE/PubMed
spelling pubmed-104230102023-08-13 Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience Rocha, Andrew D. Drake, William K. Rice, Photini F. Long, Dilara J. Shir, Hasina Walton, Ryan H. M. Reed, Mary N. Galvez, Dominique Gorman, Taliah Heusinkveld, John M. Barton, Jennifer K. J Biomed Opt Special Section on Selected Topics in Biophotonics: Translating Novel Photonics Technology into Clinical Applications SIGNIFICANCE: High grade serous ovarian cancer is the most deadly gynecological cancer, and it is now believed that most cases originate in the fallopian tubes (FTs). Early detection of ovarian cancer could double the 5-year survival rate compared with late-stage diagnosis. Autofluorescence imaging can detect serous-origin precancerous and cancerous lesions in ex vivo FT and ovaries with good sensitivity and specificity. Multispectral fluorescence imaging (MFI) can differentiate healthy, benign, and malignant ovarian and FT tissues. Optical coherence tomography (OCT) reveals subsurface microstructural information and can distinguish normal and cancerous structure in ovaries and FTs. AIM: We developed an FT endoscope, the falloposcope, as a method for detecting ovarian cancer with MFI and OCT. The falloposcope clinical prototype was tested in a pilot study with 12 volunteers to date to evaluate the safety and feasibility of FT imaging prior to standard of care salpingectomy in normal-risk volunteers. In this manuscript, we describe the multiple modifications made to the falloposcope to enhance robustness, usability, and image quality based on lessons learned in the clinical setting. APPROACH: The [Formula: see text] diameter falloposcope was introduced via a minimally invasive approach through a commercially available hysteroscope and introducing a catheter. A navigation video, MFI, and OCT of human FTs were obtained. Feedback from stakeholders on image quality and procedural difficulty was obtained. RESULTS: The falloposcope successfully obtained images in vivo. Considerable feedback was obtained, motivating iterative improvements, including accommodating the operating room environment, modifying the hysteroscope accessories, decreasing endoscope fragility and fiber breaks, optimizing software, improving fiber bundle images, decreasing gradient-index lens stray light, optimizing the proximal imaging system, and improving the illumination. CONCLUSIONS: The initial clinical prototype falloposcope was able to image the FTs, and iterative prototyping has increased its robustness, functionality, and ease of use for future trials. Society of Photo-Optical Instrumentation Engineers 2023-08-12 2023-12 /pmc/articles/PMC10423010/ /pubmed/37577082 http://dx.doi.org/10.1117/1.JBO.28.12.121206 Text en © 2023 The Authors https://creativecommons.org/licenses/by/4.0/Published by SPIE under a Creative Commons Attribution 4.0 International License. Distribution or reproduction of this work in whole or in part requires full attribution of the original publication, including its DOI.
spellingShingle Special Section on Selected Topics in Biophotonics: Translating Novel Photonics Technology into Clinical Applications
Rocha, Andrew D.
Drake, William K.
Rice, Photini F.
Long, Dilara J.
Shir, Hasina
Walton, Ryan H. M.
Reed, Mary N.
Galvez, Dominique
Gorman, Taliah
Heusinkveld, John M.
Barton, Jennifer K.
Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience
title Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience
title_full Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience
title_fullStr Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience
title_full_unstemmed Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience
title_short Iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience
title_sort iterative prototyping based on lessons learned from the falloposcope in vivo pilot study experience
topic Special Section on Selected Topics in Biophotonics: Translating Novel Photonics Technology into Clinical Applications
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10423010/
https://www.ncbi.nlm.nih.gov/pubmed/37577082
http://dx.doi.org/10.1117/1.JBO.28.12.121206
work_keys_str_mv AT rochaandrewd iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT drakewilliamk iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT ricephotinif iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT longdilaraj iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT shirhasina iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT waltonryanhm iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT reedmaryn iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT galvezdominique iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT gormantaliah iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT heusinkveldjohnm iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience
AT bartonjenniferk iterativeprototypingbasedonlessonslearnedfromthefalloposcopeinvivopilotstudyexperience

Ejemplares similares