Volume of preclinical xenograft tumors is more accurately assessed by ultrasound imaging than manual caliper measurements

Gregory D. Ayers; Eliot T. McKinley; Ping Zhao; Jordan M. Fritz; Rebecca E. Metry; Brenton C. Deal; Katrina M. Adlerz; Robert J. Coffey; H. Charles Manning

doi:10.7863/jum.2010.29.6.891

Volume of preclinical xenograft tumors is more accurately assessed by ultrasound imaging than manual caliper measurements

Gregory D. Ayers, Eliot T. McKinley, Ping Zhao, Jordan M. Fritz, Rebecca E. Metry, Brenton C. Deal, Katrina M. Adlerz, Robert J. Coffey, H. Charles Manning

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

79 Scopus citations

Abstract

Objective: The volume of subcutaneous xenograft tumors is an important metric of disease progression and response to therapy in preclinical drug development. Noninvasive imaging technologies suitable for measuring xenograft volume are increasingly available, yet manual calipers, which are susceptible to inaccuracy and bias, are routinely used. The goal of this study was to quantify and compare the accuracy, precision, and inter-rater variability of xenograft tumor volume assessment by caliper measurements and ultrasound imaging. Methods: Subcutaneous xenograft tumors derived from human colorectal cancer cell lines (DLD1 and SW620) were generated in athymic nude mice. Experienced independent reviewers segmented 3-dimensional ultrasound data sets and collected manual caliper measurements resulting in tumor volumes. Imaging- and caliper-derived volumes were compared with the tumor mass, the reference standard, determined after resection. Bias, precision, and inter-rater differences were estimated for each mouse among reviewers. Bootstrapping was used to estimate mean and confidence intervals of variance components, intraclass correlation coefficients (ICCs), and confidence intervals for each source of variation. Results: The average deviation from the true volume and inter-rater differences were significantly lower for ultrasound volumes compared with caliper volumes (P = .0005 and .001, respectively). Reviewer ICCs for ultrasound and caliper measurements were similarly low (1%), yet caliper volume variance was 1.3-fold higher than for ultrasound. Conclusions: Ultrasound imaging more accurately, precisely, and reproducibly reflects xenograft tumor volume than caliper measurements. These data suggest that preclinical studies using the xenograft burden as a surrogate end point measured by ultrasound imaging require up to 30% fewer animals to reach statistical significance compared with analogous studies using caliper measurements.

Original language	English (US)
Pages (from-to)	891-901
Number of pages	11
Journal	Journal of Ultrasound in Medicine
Volume	29
Issue number	6
DOIs	https://doi.org/10.7863/jum.2010.29.6.891
State	Published - Jun 1 2010
Externally published	Yes

Keywords

Colorectal cancer
Preclinical mouse models
Tumor burden
Ultrasound imaging
Xenograft

ASJC Scopus subject areas

Radiological and Ultrasound Technology
Radiology Nuclear Medicine and imaging

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10.7863/jum.2010.29.6.891

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@article{631eeeed0a1043d7b8de404d947509c1,

title = "Volume of preclinical xenograft tumors is more accurately assessed by ultrasound imaging than manual caliper measurements",

abstract = "Objective: The volume of subcutaneous xenograft tumors is an important metric of disease progression and response to therapy in preclinical drug development. Noninvasive imaging technologies suitable for measuring xenograft volume are increasingly available, yet manual calipers, which are susceptible to inaccuracy and bias, are routinely used. The goal of this study was to quantify and compare the accuracy, precision, and inter-rater variability of xenograft tumor volume assessment by caliper measurements and ultrasound imaging. Methods: Subcutaneous xenograft tumors derived from human colorectal cancer cell lines (DLD1 and SW620) were generated in athymic nude mice. Experienced independent reviewers segmented 3-dimensional ultrasound data sets and collected manual caliper measurements resulting in tumor volumes. Imaging- and caliper-derived volumes were compared with the tumor mass, the reference standard, determined after resection. Bias, precision, and inter-rater differences were estimated for each mouse among reviewers. Bootstrapping was used to estimate mean and confidence intervals of variance components, intraclass correlation coefficients (ICCs), and confidence intervals for each source of variation. Results: The average deviation from the true volume and inter-rater differences were significantly lower for ultrasound volumes compared with caliper volumes (P = .0005 and .001, respectively). Reviewer ICCs for ultrasound and caliper measurements were similarly low (1%), yet caliper volume variance was 1.3-fold higher than for ultrasound. Conclusions: Ultrasound imaging more accurately, precisely, and reproducibly reflects xenograft tumor volume than caliper measurements. These data suggest that preclinical studies using the xenograft burden as a surrogate end point measured by ultrasound imaging require up to 30% fewer animals to reach statistical significance compared with analogous studies using caliper measurements.",

keywords = "Colorectal cancer, Preclinical mouse models, Tumor burden, Ultrasound imaging, Xenograft",

author = "Ayers, {Gregory D.} and McKinley, {Eliot T.} and Ping Zhao and Fritz, {Jordan M.} and Metry, {Rebecca E.} and Deal, {Brenton C.} and Adlerz, {Katrina M.} and Coffey, {Robert J.} and Manning, {H. Charles}",

year = "2010",

month = jun,

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doi = "10.7863/jum.2010.29.6.891",

language = "English (US)",

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TY - JOUR

T1 - Volume of preclinical xenograft tumors is more accurately assessed by ultrasound imaging than manual caliper measurements

AU - Ayers, Gregory D.

AU - McKinley, Eliot T.

AU - Zhao, Ping

AU - Fritz, Jordan M.

AU - Metry, Rebecca E.

AU - Deal, Brenton C.

AU - Adlerz, Katrina M.

AU - Coffey, Robert J.

AU - Manning, H. Charles

PY - 2010/6/1

Y1 - 2010/6/1

N2 - Objective: The volume of subcutaneous xenograft tumors is an important metric of disease progression and response to therapy in preclinical drug development. Noninvasive imaging technologies suitable for measuring xenograft volume are increasingly available, yet manual calipers, which are susceptible to inaccuracy and bias, are routinely used. The goal of this study was to quantify and compare the accuracy, precision, and inter-rater variability of xenograft tumor volume assessment by caliper measurements and ultrasound imaging. Methods: Subcutaneous xenograft tumors derived from human colorectal cancer cell lines (DLD1 and SW620) were generated in athymic nude mice. Experienced independent reviewers segmented 3-dimensional ultrasound data sets and collected manual caliper measurements resulting in tumor volumes. Imaging- and caliper-derived volumes were compared with the tumor mass, the reference standard, determined after resection. Bias, precision, and inter-rater differences were estimated for each mouse among reviewers. Bootstrapping was used to estimate mean and confidence intervals of variance components, intraclass correlation coefficients (ICCs), and confidence intervals for each source of variation. Results: The average deviation from the true volume and inter-rater differences were significantly lower for ultrasound volumes compared with caliper volumes (P = .0005 and .001, respectively). Reviewer ICCs for ultrasound and caliper measurements were similarly low (1%), yet caliper volume variance was 1.3-fold higher than for ultrasound. Conclusions: Ultrasound imaging more accurately, precisely, and reproducibly reflects xenograft tumor volume than caliper measurements. These data suggest that preclinical studies using the xenograft burden as a surrogate end point measured by ultrasound imaging require up to 30% fewer animals to reach statistical significance compared with analogous studies using caliper measurements.

AB - Objective: The volume of subcutaneous xenograft tumors is an important metric of disease progression and response to therapy in preclinical drug development. Noninvasive imaging technologies suitable for measuring xenograft volume are increasingly available, yet manual calipers, which are susceptible to inaccuracy and bias, are routinely used. The goal of this study was to quantify and compare the accuracy, precision, and inter-rater variability of xenograft tumor volume assessment by caliper measurements and ultrasound imaging. Methods: Subcutaneous xenograft tumors derived from human colorectal cancer cell lines (DLD1 and SW620) were generated in athymic nude mice. Experienced independent reviewers segmented 3-dimensional ultrasound data sets and collected manual caliper measurements resulting in tumor volumes. Imaging- and caliper-derived volumes were compared with the tumor mass, the reference standard, determined after resection. Bias, precision, and inter-rater differences were estimated for each mouse among reviewers. Bootstrapping was used to estimate mean and confidence intervals of variance components, intraclass correlation coefficients (ICCs), and confidence intervals for each source of variation. Results: The average deviation from the true volume and inter-rater differences were significantly lower for ultrasound volumes compared with caliper volumes (P = .0005 and .001, respectively). Reviewer ICCs for ultrasound and caliper measurements were similarly low (1%), yet caliper volume variance was 1.3-fold higher than for ultrasound. Conclusions: Ultrasound imaging more accurately, precisely, and reproducibly reflects xenograft tumor volume than caliper measurements. These data suggest that preclinical studies using the xenograft burden as a surrogate end point measured by ultrasound imaging require up to 30% fewer animals to reach statistical significance compared with analogous studies using caliper measurements.

KW - Colorectal cancer

KW - Preclinical mouse models

KW - Tumor burden

KW - Ultrasound imaging

KW - Xenograft

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EP - 901

JO - Journal of Ultrasound in Medicine

JF - Journal of Ultrasound in Medicine

IS - 6

ER -

Volume of preclinical xenograft tumors is more accurately assessed by ultrasound imaging than manual caliper measurements

Abstract

Keywords

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