Technical Note: Histological validation of anatomical imaging for breast modeling using a novel cryo-microtome

Anando Sen; Natalie W. Fowlkes; Charles V. Kingsley; Adam M. Kulp; Thomas Huynh; Brandy J. Willis; Kari J. Brewer Savannah; Mary Catherine A. Bordes; Ken Pin Hwang; Molly M. McCulloch; Roger Jason Stafford; Alejandro Contreras; Gregory Reece; Kristy K. Brock

doi:10.1002/mp.15245

Technical Note: Histological validation of anatomical imaging for breast modeling using a novel cryo-microtome

Anando Sen, Natalie W. Fowlkes, Charles V. Kingsley, Adam M. Kulp, Thomas Huynh, Brandy J. Willis, Kari J. Brewer Savannah, Mary Catherine A. Bordes, Ken Pin Hwang, Molly M. McCulloch, Roger Jason Stafford, Alejandro Contreras, Gregory Reece, Kristy K. Brock

Research output: Contribution to journal › Article › peer-review

Abstract

Purpose: Precise correlation between three-dimensional (3D) imaging and histology can aid biomechanical modeling of the breast. We develop a framework to register ex vivo images to histology using a novel cryo-fluorescence tomography (CFT) device. Methods: A formalin-fixed cadaveric breast specimen, including chest wall, was subjected to high-resolution magnetic resonance (MR) imaging. The specimen was then frozen and embedded in an optimal cutting temperature (OCT) compound. The OCT block was placed in a CFT device with an overhead camera and 50 μm thick slices were successively shaved off the block. After each shaving, the block-face was photographed. At select locations including connective/adipose tissue, muscle, skin, and fibroglandular tissue, 20 μm sections were transferred onto cryogenic tape for manual hematoxylin and eosin staining, histological assessment, and image capture. A 3D white-light image was automatically reconstructed from the photographs by aligning fiducial markers embedded in the OCT block. The 3D MR image, 3D white-light image, and photomicrographs were rigidly registered. Target registration errors (TREs) were computed based on 10 pairs of points marked at fibroglandular intersections. The overall MR-histology registration was used to compare the MR intensities at tissue extraction sites with a one-way analysis of variance. Results: The MR image to CFT-captured white-light image registration achieved a mean TRE of 0.73 ± 0.25 mm (less than the 1 mm MR slice resolution). The block-face white-light image and block-face photomicrograph registration showed visually indistinguishable alignment of anatomical structures and tissue boundaries. The MR intensities at the four tissue sites identified from histology differed significantly (p < 0.01). Each tissue pair, except the skin-connective/adipose tissue pair, also had significantly different MR intensities (p < 0.01). Conclusions: Fine sectioning in a highly controlled imaging/sectioning environment enables accurate registration between the MR image and histology. Statistically significant differences in MR signal intensities between histological tissues are indicators for the specificity of correlation between MRI and histology.

Original language	English (US)
Pages (from-to)	7323-7332
Number of pages	10
Journal	Medical physics
Volume	48
Issue number	11
DOIs	https://doi.org/10.1002/mp.15245
State	Published - Nov 2021

Keywords

breast
correlative pathology
novel device
tissue modeling

ASJC Scopus subject areas

Biophysics
Radiology Nuclear Medicine and imaging

MD Anderson CCSG core facilities

Research Animal Support Facility
Small Animal Imaging Facility

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10.1002/mp.15245

Cite this

Sen, A., Fowlkes, N. W., Kingsley, C. V., Kulp, A. M., Huynh, T., Willis, B. J., Brewer Savannah, K. J., Bordes, M. C. A., Hwang, K. P., McCulloch, M. M., Stafford, R. J., Contreras, A., Reece, G., & Brock, K. K. (2021). Technical Note: Histological validation of anatomical imaging for breast modeling using a novel cryo-microtome. Medical physics, 48(11), 7323-7332. https://doi.org/10.1002/mp.15245

Sen, A, Fowlkes, NW, Kingsley, CV, Kulp, AM, Huynh, T, Willis, BJ, Brewer Savannah, KJ, Bordes, MCA, Hwang, KP, McCulloch, MM, Stafford, RJ , Contreras, A , Reece, G & Brock, KK 2021, 'Technical Note: Histological validation of anatomical imaging for breast modeling using a novel cryo-microtome', Medical physics, vol. 48, no. 11, pp. 7323-7332. https://doi.org/10.1002/mp.15245

@article{3cd8e07aa5e94eb080adce2b8c6a11f8,

title = "Technical Note: Histological validation of anatomical imaging for breast modeling using a novel cryo-microtome",

abstract = "Purpose: Precise correlation between three-dimensional (3D) imaging and histology can aid biomechanical modeling of the breast. We develop a framework to register ex vivo images to histology using a novel cryo-fluorescence tomography (CFT) device. Methods: A formalin-fixed cadaveric breast specimen, including chest wall, was subjected to high-resolution magnetic resonance (MR) imaging. The specimen was then frozen and embedded in an optimal cutting temperature (OCT) compound. The OCT block was placed in a CFT device with an overhead camera and 50 μm thick slices were successively shaved off the block. After each shaving, the block-face was photographed. At select locations including connective/adipose tissue, muscle, skin, and fibroglandular tissue, 20 μm sections were transferred onto cryogenic tape for manual hematoxylin and eosin staining, histological assessment, and image capture. A 3D white-light image was automatically reconstructed from the photographs by aligning fiducial markers embedded in the OCT block. The 3D MR image, 3D white-light image, and photomicrographs were rigidly registered. Target registration errors (TREs) were computed based on 10 pairs of points marked at fibroglandular intersections. The overall MR-histology registration was used to compare the MR intensities at tissue extraction sites with a one-way analysis of variance. Results: The MR image to CFT-captured white-light image registration achieved a mean TRE of 0.73 ± 0.25 mm (less than the 1 mm MR slice resolution). The block-face white-light image and block-face photomicrograph registration showed visually indistinguishable alignment of anatomical structures and tissue boundaries. The MR intensities at the four tissue sites identified from histology differed significantly (p < 0.01). Each tissue pair, except the skin-connective/adipose tissue pair, also had significantly different MR intensities (p < 0.01). Conclusions: Fine sectioning in a highly controlled imaging/sectioning environment enables accurate registration between the MR image and histology. Statistically significant differences in MR signal intensities between histological tissues are indicators for the specificity of correlation between MRI and histology.",

keywords = "breast, correlative pathology, novel device, tissue modeling",

author = "Anando Sen and Fowlkes, {Natalie W.} and Kingsley, {Charles V.} and Kulp, {Adam M.} and Thomas Huynh and Willis, {Brandy J.} and {Brewer Savannah}, {Kari J.} and Bordes, {Mary Catherine A.} and Hwang, {Ken Pin} and McCulloch, {Molly M.} and Stafford, {Roger Jason} and Alejandro Contreras and Gregory Reece and Brock, {Kristy K.}",

note = "Funding Information: This research was supported in part by NIH NCI P30 CA016672 correlative pathology platform and used the Small Animal Imaging Facility – correlative pathology core at MD Anderson Cancer Center. Partial support was also provided by the resources of the Image‐Guided Cancer Therapy Research Program, the Helen Black Image‐Guided Fund, and the Tumor Measurement Initiative (all at the University of Texas, MD Anderson Cancer Center). Editorial support was provided by Joseph A Munch, Senior Scientific Editor, Research Medical Library at M D Anderson Cancer Center. Funding Information: This research was supported in part by NIH NCI P30 CA016672 correlative pathology platform and used the Small Animal Imaging Facility – correlative pathology core at MD Anderson Cancer Center. Partial support was also provided by the resources of the Image-Guided Cancer Therapy Research Program, the Helen Black Image-Guided Fund, and the Tumor Measurement Initiative (all at the University of Texas, MD Anderson Cancer Center). Editorial support was provided by Joseph A Munch, Senior Scientific Editor, Research Medical Library at M D Anderson Cancer Center. Publisher Copyright: {\textcopyright} 2021 American Association of Physicists in Medicine",

year = "2021",

month = nov,

doi = "10.1002/mp.15245",

language = "English (US)",

volume = "48",

pages = "7323--7332",

journal = "Medical physics",

issn = "0094-2405",

publisher = "AAPM - American Association of Physicists in Medicine",

number = "11",

}

TY - JOUR

T1 - Technical Note

T2 - Histological validation of anatomical imaging for breast modeling using a novel cryo-microtome

AU - Sen, Anando

AU - Fowlkes, Natalie W.

AU - Kingsley, Charles V.

AU - Kulp, Adam M.

AU - Huynh, Thomas

AU - Willis, Brandy J.

AU - Brewer Savannah, Kari J.

AU - Bordes, Mary Catherine A.

AU - Hwang, Ken Pin

AU - McCulloch, Molly M.

AU - Stafford, Roger Jason

AU - Contreras, Alejandro

AU - Reece, Gregory

AU - Brock, Kristy K.

N1 - Funding Information: This research was supported in part by NIH NCI P30 CA016672 correlative pathology platform and used the Small Animal Imaging Facility – correlative pathology core at MD Anderson Cancer Center. Partial support was also provided by the resources of the Image‐Guided Cancer Therapy Research Program, the Helen Black Image‐Guided Fund, and the Tumor Measurement Initiative (all at the University of Texas, MD Anderson Cancer Center). Editorial support was provided by Joseph A Munch, Senior Scientific Editor, Research Medical Library at M D Anderson Cancer Center. Funding Information: This research was supported in part by NIH NCI P30 CA016672 correlative pathology platform and used the Small Animal Imaging Facility – correlative pathology core at MD Anderson Cancer Center. Partial support was also provided by the resources of the Image-Guided Cancer Therapy Research Program, the Helen Black Image-Guided Fund, and the Tumor Measurement Initiative (all at the University of Texas, MD Anderson Cancer Center). Editorial support was provided by Joseph A Munch, Senior Scientific Editor, Research Medical Library at M D Anderson Cancer Center. Publisher Copyright: © 2021 American Association of Physicists in Medicine

PY - 2021/11

Y1 - 2021/11

N2 - Purpose: Precise correlation between three-dimensional (3D) imaging and histology can aid biomechanical modeling of the breast. We develop a framework to register ex vivo images to histology using a novel cryo-fluorescence tomography (CFT) device. Methods: A formalin-fixed cadaveric breast specimen, including chest wall, was subjected to high-resolution magnetic resonance (MR) imaging. The specimen was then frozen and embedded in an optimal cutting temperature (OCT) compound. The OCT block was placed in a CFT device with an overhead camera and 50 μm thick slices were successively shaved off the block. After each shaving, the block-face was photographed. At select locations including connective/adipose tissue, muscle, skin, and fibroglandular tissue, 20 μm sections were transferred onto cryogenic tape for manual hematoxylin and eosin staining, histological assessment, and image capture. A 3D white-light image was automatically reconstructed from the photographs by aligning fiducial markers embedded in the OCT block. The 3D MR image, 3D white-light image, and photomicrographs were rigidly registered. Target registration errors (TREs) were computed based on 10 pairs of points marked at fibroglandular intersections. The overall MR-histology registration was used to compare the MR intensities at tissue extraction sites with a one-way analysis of variance. Results: The MR image to CFT-captured white-light image registration achieved a mean TRE of 0.73 ± 0.25 mm (less than the 1 mm MR slice resolution). The block-face white-light image and block-face photomicrograph registration showed visually indistinguishable alignment of anatomical structures and tissue boundaries. The MR intensities at the four tissue sites identified from histology differed significantly (p < 0.01). Each tissue pair, except the skin-connective/adipose tissue pair, also had significantly different MR intensities (p < 0.01). Conclusions: Fine sectioning in a highly controlled imaging/sectioning environment enables accurate registration between the MR image and histology. Statistically significant differences in MR signal intensities between histological tissues are indicators for the specificity of correlation between MRI and histology.

AB - Purpose: Precise correlation between three-dimensional (3D) imaging and histology can aid biomechanical modeling of the breast. We develop a framework to register ex vivo images to histology using a novel cryo-fluorescence tomography (CFT) device. Methods: A formalin-fixed cadaveric breast specimen, including chest wall, was subjected to high-resolution magnetic resonance (MR) imaging. The specimen was then frozen and embedded in an optimal cutting temperature (OCT) compound. The OCT block was placed in a CFT device with an overhead camera and 50 μm thick slices were successively shaved off the block. After each shaving, the block-face was photographed. At select locations including connective/adipose tissue, muscle, skin, and fibroglandular tissue, 20 μm sections were transferred onto cryogenic tape for manual hematoxylin and eosin staining, histological assessment, and image capture. A 3D white-light image was automatically reconstructed from the photographs by aligning fiducial markers embedded in the OCT block. The 3D MR image, 3D white-light image, and photomicrographs were rigidly registered. Target registration errors (TREs) were computed based on 10 pairs of points marked at fibroglandular intersections. The overall MR-histology registration was used to compare the MR intensities at tissue extraction sites with a one-way analysis of variance. Results: The MR image to CFT-captured white-light image registration achieved a mean TRE of 0.73 ± 0.25 mm (less than the 1 mm MR slice resolution). The block-face white-light image and block-face photomicrograph registration showed visually indistinguishable alignment of anatomical structures and tissue boundaries. The MR intensities at the four tissue sites identified from histology differed significantly (p < 0.01). Each tissue pair, except the skin-connective/adipose tissue pair, also had significantly different MR intensities (p < 0.01). Conclusions: Fine sectioning in a highly controlled imaging/sectioning environment enables accurate registration between the MR image and histology. Statistically significant differences in MR signal intensities between histological tissues are indicators for the specificity of correlation between MRI and histology.

KW - breast

KW - correlative pathology

KW - novel device

KW - tissue modeling

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Technical Note: Histological validation of anatomical imaging for breast modeling using a novel cryo-microtome

Abstract

Keywords

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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