A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation

William K.C. Park; David R. Mills; Sierin Lim; Barindra Sana; Victoria E. Frank; Brendan M. Kenyon; Michael P. Primmer; Jarod B. Paul; Greyson L. Baird; Edward Walsh; Damian E. Dupuy

doi:10.1117/12.2250041

A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation

William K.C. Park^*, David R. Mills, Sierin Lim, Barindra Sana, Victoria E. Frank, Brendan M. Kenyon, Michael P. Primmer, Jarod B. Paul, Greyson L. Baird, Edward Walsh, Damian E. Dupuy

^*Corresponding author for this work

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution

Abstract

Purpose: A ferritin-containing nanoparticle conjugated with a target-specific antibody was investigated as a MRI contrast agent for tumor detection. A genetically modified ferritin to markedly improve Fe (III) payload (up to 7,000 Fe ions), was chemically tethered to a monoclonal antibody against rat Nectin-like molecule 5 (Necl-5). Necl-5 is a cell surface glycoprotein that is highly expressed on the cell surface of many common epithelial cancers, including prostate cancer. It was previously demonstrated that this novel nanoconjugate agent exhibited effective in vitro targeting of Necl- 5 expressing tumor cells and exhibited strong MRI contrast characteristics via shortening of T₂. Here, we demonstrate that the nanoconjugate-Necl-5 interaction can be exploited to target and detect tumor in vivo by MRI. Procedure: Using an in vivo tumor model (i.e., tumor size 0.5^-1 cm, immunodeficient beige/nude/xid mouse, xenograft injection with transformed rat prostate cells), efficacy of the conjugate targeting the tumor was examined. We used two injection strategies, a direct and a tail vein injection (0.8 mg, 300 μL per subject). Pre-injection baseline and postinjection scans were performed with the following spin-echo sequence parameters: Field of view = 90x53mm, reconstruction matrix size = 192x114, slice thickness = 1mm (10 slices), repetition time (TR) = 2070 ms, echo times (TE) = 11-198 ms in 11ms steps (18 echoes), number of averages = 2, acquisition time per scan = 7min 56s. Results: All T₂ data obtained were converted to R₂ for demonstration purposes (R₂ = 1/T₂). The tail vein injected conjugate significantly increased R₂ response (22.9 ± 5.2 s^-1) as compared to control (13.5 ±1.7 s^-1) at 4 h. The weaker R₂ increase was noted (15.2 ± 2.0 s^-1) at 24 h. No notable changes in R₂ were observed in surrounding tissues regardless the stages of the measurement. We also measured the initial conjugate kinetics for both injection methods with respect to the ability of targeting the tumor. Direct injection of the nanoconjugate in to the center of the tumor showed a stronger and more rapid increase in R2 than the tail vein injection. Conclusion: The nanoconjugate interacts strongly and selectively in situ with Necl-5 overexpressing tumor cells. Direct injection of the nanoconjugate into the body of the tumor caused a more significant in situ R₂ increase in MRI than the tail vein injection. Varying degrees of R₂ increase within the tumor mass is likely to represent different distribution patterns of the conjugate, reflective of tumor heterogeneity.

Original language	English
Title of host publication	Energy-Based Treatment of Tissue and Assessment IX
Editors	Thomas P. Ryan
Publisher	SPIE
ISBN (Electronic)	9781510605732
DOIs	https://doi.org/10.1117/12.2250041
Publication status	Published - 2017
Externally published	Yes
Event	Energy-Based Treatment of Tissue and Assessment IX - San Francisco, United States Duration: Jan 29 2017 → Jan 30 2017

Publication series

Name	Progress in Biomedical Optics and Imaging - Proceedings of SPIE
Volume	10066
ISSN (Print)	1605-7422

Conference

Conference	Energy-Based Treatment of Tissue and Assessment IX
Country/Territory	United States
City	San Francisco
Period	1/29/17 → 1/30/17

Bibliographical note

Publisher Copyright:
© 2017 SPIE.

ASJC Scopus Subject Areas

Electronic, Optical and Magnetic Materials
Atomic and Molecular Physics, and Optics
Biomaterials
Radiology Nuclear Medicine and imaging

Keywords

Electromagnetic field
Ferritin
Microwave energy
Monoclonal antibody
Nanoconjugate
Necl-5
Self-assembly
T and T (R and R)
Xenograft

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1117/12.2250041

Cite this

Park, W. K. C., Mills, D. R., Lim, S., Sana, B., Frank, V. E., Kenyon, B. M., Primmer, M. P., Paul, J. B., Baird, G. L., Walsh, E., & Dupuy, D. E. (2017). A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation. In T. P. Ryan (Ed.), Energy-Based Treatment of Tissue and Assessment IX Article 100660H (Progress in Biomedical Optics and Imaging - Proceedings of SPIE; Vol. 10066). SPIE. https://doi.org/10.1117/12.2250041

Park, William K.C. ; Mills, David R. ; Lim, Sierin et al. / A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen : A potential thermal accelerant for microwave ablation. Energy-Based Treatment of Tissue and Assessment IX. editor / Thomas P. Ryan. SPIE, 2017. (Progress in Biomedical Optics and Imaging - Proceedings of SPIE).

@inproceedings{d88a48bf0f98499e86dd76a71c149302,

title = "A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation",

abstract = "Purpose: A ferritin-containing nanoparticle conjugated with a target-specific antibody was investigated as a MRI contrast agent for tumor detection. A genetically modified ferritin to markedly improve Fe (III) payload (up to 7,000 Fe ions), was chemically tethered to a monoclonal antibody against rat Nectin-like molecule 5 (Necl-5). Necl-5 is a cell surface glycoprotein that is highly expressed on the cell surface of many common epithelial cancers, including prostate cancer. It was previously demonstrated that this novel nanoconjugate agent exhibited effective in vitro targeting of Necl- 5 expressing tumor cells and exhibited strong MRI contrast characteristics via shortening of T2. Here, we demonstrate that the nanoconjugate-Necl-5 interaction can be exploited to target and detect tumor in vivo by MRI. Procedure: Using an in vivo tumor model (i.e., tumor size 0.5-1 cm, immunodeficient beige/nude/xid mouse, xenograft injection with transformed rat prostate cells), efficacy of the conjugate targeting the tumor was examined. We used two injection strategies, a direct and a tail vein injection (0.8 mg, 300 μL per subject). Pre-injection baseline and postinjection scans were performed with the following spin-echo sequence parameters: Field of view = 90x53mm, reconstruction matrix size = 192x114, slice thickness = 1mm (10 slices), repetition time (TR) = 2070 ms, echo times (TE) = 11-198 ms in 11ms steps (18 echoes), number of averages = 2, acquisition time per scan = 7min 56s. Results: All T2 data obtained were converted to R2 for demonstration purposes (R2 = 1/T2). The tail vein injected conjugate significantly increased R2 response (22.9 ± 5.2 s-1) as compared to control (13.5 ±1.7 s-1) at 4 h. The weaker R2 increase was noted (15.2 ± 2.0 s-1) at 24 h. No notable changes in R2 were observed in surrounding tissues regardless the stages of the measurement. We also measured the initial conjugate kinetics for both injection methods with respect to the ability of targeting the tumor. Direct injection of the nanoconjugate in to the center of the tumor showed a stronger and more rapid increase in R2 than the tail vein injection. Conclusion: The nanoconjugate interacts strongly and selectively in situ with Necl-5 overexpressing tumor cells. Direct injection of the nanoconjugate into the body of the tumor caused a more significant in situ R2 increase in MRI than the tail vein injection. Varying degrees of R2 increase within the tumor mass is likely to represent different distribution patterns of the conjugate, reflective of tumor heterogeneity.",

keywords = "Electromagnetic field, Ferritin, Microwave energy, Monoclonal antibody, Nanoconjugate, Necl-5, Self-assembly, T and T (R and R), Xenograft",

author = "Park, {William K.C.} and Mills, {David R.} and Sierin Lim and Barindra Sana and Frank, {Victoria E.} and Kenyon, {Brendan M.} and Primmer, {Michael P.} and Paul, {Jarod B.} and Baird, {Greyson L.} and Edward Walsh and Dupuy, {Damian E.}",

note = "Publisher Copyright: {\textcopyright} 2017 SPIE.; Energy-Based Treatment of Tissue and Assessment IX ; Conference date: 29-01-2017 Through 30-01-2017",

year = "2017",

doi = "10.1117/12.2250041",

language = "English",

series = "Progress in Biomedical Optics and Imaging - Proceedings of SPIE",

publisher = "SPIE",

editor = "Ryan, {Thomas P.}",

booktitle = "Energy-Based Treatment of Tissue and Assessment IX",

address = "United States",

}

Park, WKC, Mills, DR, Lim, S, Sana, B, Frank, VE, Kenyon, BM, Primmer, MP, Paul, JB, Baird, GL, Walsh, E & Dupuy, DE 2017, A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation. in TP Ryan (ed.), Energy-Based Treatment of Tissue and Assessment IX., 100660H, Progress in Biomedical Optics and Imaging - Proceedings of SPIE, vol. 10066, SPIE, Energy-Based Treatment of Tissue and Assessment IX, San Francisco, United States, 1/29/17. https://doi.org/10.1117/12.2250041

A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation. / Park, William K.C.; Mills, David R.; Lim, Sierin et al.
Energy-Based Treatment of Tissue and Assessment IX. ed. / Thomas P. Ryan. SPIE, 2017. 100660H (Progress in Biomedical Optics and Imaging - Proceedings of SPIE; Vol. 10066).

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution

TY - GEN

T1 - A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen

T2 - Energy-Based Treatment of Tissue and Assessment IX

AU - Park, William K.C.

AU - Mills, David R.

AU - Lim, Sierin

AU - Sana, Barindra

AU - Frank, Victoria E.

AU - Kenyon, Brendan M.

AU - Primmer, Michael P.

AU - Paul, Jarod B.

AU - Baird, Greyson L.

AU - Walsh, Edward

AU - Dupuy, Damian E.

PY - 2017

Y1 - 2017

N2 - Purpose: A ferritin-containing nanoparticle conjugated with a target-specific antibody was investigated as a MRI contrast agent for tumor detection. A genetically modified ferritin to markedly improve Fe (III) payload (up to 7,000 Fe ions), was chemically tethered to a monoclonal antibody against rat Nectin-like molecule 5 (Necl-5). Necl-5 is a cell surface glycoprotein that is highly expressed on the cell surface of many common epithelial cancers, including prostate cancer. It was previously demonstrated that this novel nanoconjugate agent exhibited effective in vitro targeting of Necl- 5 expressing tumor cells and exhibited strong MRI contrast characteristics via shortening of T2. Here, we demonstrate that the nanoconjugate-Necl-5 interaction can be exploited to target and detect tumor in vivo by MRI. Procedure: Using an in vivo tumor model (i.e., tumor size 0.5-1 cm, immunodeficient beige/nude/xid mouse, xenograft injection with transformed rat prostate cells), efficacy of the conjugate targeting the tumor was examined. We used two injection strategies, a direct and a tail vein injection (0.8 mg, 300 μL per subject). Pre-injection baseline and postinjection scans were performed with the following spin-echo sequence parameters: Field of view = 90x53mm, reconstruction matrix size = 192x114, slice thickness = 1mm (10 slices), repetition time (TR) = 2070 ms, echo times (TE) = 11-198 ms in 11ms steps (18 echoes), number of averages = 2, acquisition time per scan = 7min 56s. Results: All T2 data obtained were converted to R2 for demonstration purposes (R2 = 1/T2). The tail vein injected conjugate significantly increased R2 response (22.9 ± 5.2 s-1) as compared to control (13.5 ±1.7 s-1) at 4 h. The weaker R2 increase was noted (15.2 ± 2.0 s-1) at 24 h. No notable changes in R2 were observed in surrounding tissues regardless the stages of the measurement. We also measured the initial conjugate kinetics for both injection methods with respect to the ability of targeting the tumor. Direct injection of the nanoconjugate in to the center of the tumor showed a stronger and more rapid increase in R2 than the tail vein injection. Conclusion: The nanoconjugate interacts strongly and selectively in situ with Necl-5 overexpressing tumor cells. Direct injection of the nanoconjugate into the body of the tumor caused a more significant in situ R2 increase in MRI than the tail vein injection. Varying degrees of R2 increase within the tumor mass is likely to represent different distribution patterns of the conjugate, reflective of tumor heterogeneity.

AB - Purpose: A ferritin-containing nanoparticle conjugated with a target-specific antibody was investigated as a MRI contrast agent for tumor detection. A genetically modified ferritin to markedly improve Fe (III) payload (up to 7,000 Fe ions), was chemically tethered to a monoclonal antibody against rat Nectin-like molecule 5 (Necl-5). Necl-5 is a cell surface glycoprotein that is highly expressed on the cell surface of many common epithelial cancers, including prostate cancer. It was previously demonstrated that this novel nanoconjugate agent exhibited effective in vitro targeting of Necl- 5 expressing tumor cells and exhibited strong MRI contrast characteristics via shortening of T2. Here, we demonstrate that the nanoconjugate-Necl-5 interaction can be exploited to target and detect tumor in vivo by MRI. Procedure: Using an in vivo tumor model (i.e., tumor size 0.5-1 cm, immunodeficient beige/nude/xid mouse, xenograft injection with transformed rat prostate cells), efficacy of the conjugate targeting the tumor was examined. We used two injection strategies, a direct and a tail vein injection (0.8 mg, 300 μL per subject). Pre-injection baseline and postinjection scans were performed with the following spin-echo sequence parameters: Field of view = 90x53mm, reconstruction matrix size = 192x114, slice thickness = 1mm (10 slices), repetition time (TR) = 2070 ms, echo times (TE) = 11-198 ms in 11ms steps (18 echoes), number of averages = 2, acquisition time per scan = 7min 56s. Results: All T2 data obtained were converted to R2 for demonstration purposes (R2 = 1/T2). The tail vein injected conjugate significantly increased R2 response (22.9 ± 5.2 s-1) as compared to control (13.5 ±1.7 s-1) at 4 h. The weaker R2 increase was noted (15.2 ± 2.0 s-1) at 24 h. No notable changes in R2 were observed in surrounding tissues regardless the stages of the measurement. We also measured the initial conjugate kinetics for both injection methods with respect to the ability of targeting the tumor. Direct injection of the nanoconjugate in to the center of the tumor showed a stronger and more rapid increase in R2 than the tail vein injection. Conclusion: The nanoconjugate interacts strongly and selectively in situ with Necl-5 overexpressing tumor cells. Direct injection of the nanoconjugate into the body of the tumor caused a more significant in situ R2 increase in MRI than the tail vein injection. Varying degrees of R2 increase within the tumor mass is likely to represent different distribution patterns of the conjugate, reflective of tumor heterogeneity.

KW - Electromagnetic field

KW - Ferritin

KW - Microwave energy

KW - Monoclonal antibody

KW - Nanoconjugate

KW - Necl-5

KW - Self-assembly

KW - T and T (R and R)

KW - Xenograft

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DO - 10.1117/12.2250041

M3 - Conference contribution

AN - SCOPUS:85020312180

T3 - Progress in Biomedical Optics and Imaging - Proceedings of SPIE

BT - Energy-Based Treatment of Tissue and Assessment IX

A2 - Ryan, Thomas P.

PB - SPIE

Y2 - 29 January 2017 through 30 January 2017

ER -

Park WKC, Mills DR, Lim S, Sana B, Frank VE, Kenyon BM et al. A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation. In Ryan TP, editor, Energy-Based Treatment of Tissue and Assessment IX. SPIE. 2017. 100660H. (Progress in Biomedical Optics and Imaging - Proceedings of SPIE). doi: 10.1117/12.2250041

A ferritin-containing nanoconjugate as MRI image-guidance to target Necl-5, a tumor-surface antigen: A potential thermal accelerant for microwave ablation

Abstract

Publication series

Conference

Bibliographical note

ASJC Scopus Subject Areas

Keywords

UN SDGs

Access to Document

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