Population-based surveillance for cervical cancer precursors in three central cancer registries, United States 2009

Elaine W. Flagg; S. Deblina Datta; Mona Saraiya; Elizabeth R. Unger; Edward Peters; Lauren Cole; Vivien W. Chen; Thomas Tucker; Mary Jane Byrne; Glenn Copeland; Won Silva; Meg Watson; Hillard Weinstock

doi:10.1007/s10552-014-0362-x

Population-based surveillance for cervical cancer precursors in three central cancer registries, United States 2009

Elaine W. Flagg, S. Deblina Datta, Mona Saraiya, Elizabeth R. Unger, Edward Peters, Lauren Cole, Vivien W. Chen, Thomas Tucker, Mary Jane Byrne, Glenn Copeland, Won Silva, Meg Watson, Hillard Weinstock

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

12 Scopus citations

Abstract

Purpose: The USA has a well-established network of central cancer registries (CCRs) that collect data using standardized definitions and protocols to provide population-based estimates of cancer incidence. The addition of cervical cancer precursors in select CCR operations would facilitate future studies measuring the population-level impact of human papillomavirus (HPV) vaccine. To assess the feasibility of collecting data on cervical cancer precursors, we conducted a multi-site surveillance study in three state-wide CCRs, to obtain annual case counts and compare rates of precursor lesions to those for invasive cervical cancer. Methods: We developed standardized methods for case identification, data collection and transmission, training and quality assurance, while allowing for registry-specific strategies to accomplish surveillance objectives. We then conducted population-based surveillance for precancerous cervical lesions in three states using the protocols. Results: We identified 5,718 cases of cervical cancer precursors during 2009. Age-adjusted incidence of cervical cancer precursors was 77 (Kentucky), 60 (Michigan), and 54 (Louisiana) per 100,000 women. Highest rates were observed in those aged 20-29 years: 274 (Kentucky), 202 (Michigan), and 196 (Louisiana) per 100,000. The variable with the most missing data was race/ethnicity, which was missing for 13 % of cases in Kentucky, 18 % in Michigan, and 1 % in Louisiana. Overall rates of cervical cancer precursors were over sixfold higher than invasive cervical cancer rates [rate ratios: 8.6 (Kentucky), 8.3 (Michigan), and 6.2 (Louisiana)]. Conclusions: Incorporating surveillance of cervical cancer precursors using existing CCR infrastructure is feasible and results in collection of population-based incidence data. Standardized collection of these data in high-quality registry systems will be useful in future activities monitoring the impact of HPV vaccination across states. As a result of this study, ongoing surveillance of these lesions has now been conducted in four CCRs since 2010.

Original language	English (US)
Pages (from-to)	571-581
Number of pages	11
Journal	Cancer Causes and Control
Volume	25
Issue number	5
DOIs	https://doi.org/10.1007/s10552-014-0362-x
State	Published - May 2014
Externally published	Yes

Keywords

Cervical intraepithelial neoplasia
Epidemiology
Population characteristics
Public health
Sexually transmitted diseases

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1007/s10552-014-0362-x

Cite this

Flagg, E. W., Datta, S. D., Saraiya, M., Unger, E. R., Peters, E., Cole, L., Chen, V. W., Tucker, T., Byrne, M. J., Copeland, G., Silva, W., Watson, M., & Weinstock, H. (2014). Population-based surveillance for cervical cancer precursors in three central cancer registries, United States 2009. Cancer Causes and Control, 25(5), 571-581. https://doi.org/10.1007/s10552-014-0362-x

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title = "Population-based surveillance for cervical cancer precursors in three central cancer registries, United States 2009",

abstract = "Purpose: The USA has a well-established network of central cancer registries (CCRs) that collect data using standardized definitions and protocols to provide population-based estimates of cancer incidence. The addition of cervical cancer precursors in select CCR operations would facilitate future studies measuring the population-level impact of human papillomavirus (HPV) vaccine. To assess the feasibility of collecting data on cervical cancer precursors, we conducted a multi-site surveillance study in three state-wide CCRs, to obtain annual case counts and compare rates of precursor lesions to those for invasive cervical cancer. Methods: We developed standardized methods for case identification, data collection and transmission, training and quality assurance, while allowing for registry-specific strategies to accomplish surveillance objectives. We then conducted population-based surveillance for precancerous cervical lesions in three states using the protocols. Results: We identified 5,718 cases of cervical cancer precursors during 2009. Age-adjusted incidence of cervical cancer precursors was 77 (Kentucky), 60 (Michigan), and 54 (Louisiana) per 100,000 women. Highest rates were observed in those aged 20-29 years: 274 (Kentucky), 202 (Michigan), and 196 (Louisiana) per 100,000. The variable with the most missing data was race/ethnicity, which was missing for 13 % of cases in Kentucky, 18 % in Michigan, and 1 % in Louisiana. Overall rates of cervical cancer precursors were over sixfold higher than invasive cervical cancer rates [rate ratios: 8.6 (Kentucky), 8.3 (Michigan), and 6.2 (Louisiana)]. Conclusions: Incorporating surveillance of cervical cancer precursors using existing CCR infrastructure is feasible and results in collection of population-based incidence data. Standardized collection of these data in high-quality registry systems will be useful in future activities monitoring the impact of HPV vaccination across states. As a result of this study, ongoing surveillance of these lesions has now been conducted in four CCRs since 2010.",

keywords = "Cervical intraepithelial neoplasia, Epidemiology, Population characteristics, Public health, Sexually transmitted diseases",

author = "Flagg, {Elaine W.} and Datta, {S. Deblina} and Mona Saraiya and Unger, {Elizabeth R.} and Edward Peters and Lauren Cole and Chen, {Vivien W.} and Thomas Tucker and Byrne, {Mary Jane} and Glenn Copeland and Won Silva and Meg Watson and Hillard Weinstock",

note = "Funding Information: Acknowledgments Funding for this work was provided by the Centers for Disease Control and Prevention (Contract No. 200-2008-27956).",

year = "2014",

month = may,

doi = "10.1007/s10552-014-0362-x",

language = "English (US)",

volume = "25",

pages = "571--581",

journal = "Cancer Causes and Control",

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T1 - Population-based surveillance for cervical cancer precursors in three central cancer registries, United States 2009

AU - Flagg, Elaine W.

AU - Datta, S. Deblina

AU - Saraiya, Mona

AU - Unger, Elizabeth R.

AU - Peters, Edward

AU - Cole, Lauren

AU - Chen, Vivien W.

AU - Tucker, Thomas

AU - Byrne, Mary Jane

AU - Copeland, Glenn

AU - Silva, Won

AU - Watson, Meg

AU - Weinstock, Hillard

N1 - Funding Information: Acknowledgments Funding for this work was provided by the Centers for Disease Control and Prevention (Contract No. 200-2008-27956).

PY - 2014/5

Y1 - 2014/5

N2 - Purpose: The USA has a well-established network of central cancer registries (CCRs) that collect data using standardized definitions and protocols to provide population-based estimates of cancer incidence. The addition of cervical cancer precursors in select CCR operations would facilitate future studies measuring the population-level impact of human papillomavirus (HPV) vaccine. To assess the feasibility of collecting data on cervical cancer precursors, we conducted a multi-site surveillance study in three state-wide CCRs, to obtain annual case counts and compare rates of precursor lesions to those for invasive cervical cancer. Methods: We developed standardized methods for case identification, data collection and transmission, training and quality assurance, while allowing for registry-specific strategies to accomplish surveillance objectives. We then conducted population-based surveillance for precancerous cervical lesions in three states using the protocols. Results: We identified 5,718 cases of cervical cancer precursors during 2009. Age-adjusted incidence of cervical cancer precursors was 77 (Kentucky), 60 (Michigan), and 54 (Louisiana) per 100,000 women. Highest rates were observed in those aged 20-29 years: 274 (Kentucky), 202 (Michigan), and 196 (Louisiana) per 100,000. The variable with the most missing data was race/ethnicity, which was missing for 13 % of cases in Kentucky, 18 % in Michigan, and 1 % in Louisiana. Overall rates of cervical cancer precursors were over sixfold higher than invasive cervical cancer rates [rate ratios: 8.6 (Kentucky), 8.3 (Michigan), and 6.2 (Louisiana)]. Conclusions: Incorporating surveillance of cervical cancer precursors using existing CCR infrastructure is feasible and results in collection of population-based incidence data. Standardized collection of these data in high-quality registry systems will be useful in future activities monitoring the impact of HPV vaccination across states. As a result of this study, ongoing surveillance of these lesions has now been conducted in four CCRs since 2010.

AB - Purpose: The USA has a well-established network of central cancer registries (CCRs) that collect data using standardized definitions and protocols to provide population-based estimates of cancer incidence. The addition of cervical cancer precursors in select CCR operations would facilitate future studies measuring the population-level impact of human papillomavirus (HPV) vaccine. To assess the feasibility of collecting data on cervical cancer precursors, we conducted a multi-site surveillance study in three state-wide CCRs, to obtain annual case counts and compare rates of precursor lesions to those for invasive cervical cancer. Methods: We developed standardized methods for case identification, data collection and transmission, training and quality assurance, while allowing for registry-specific strategies to accomplish surveillance objectives. We then conducted population-based surveillance for precancerous cervical lesions in three states using the protocols. Results: We identified 5,718 cases of cervical cancer precursors during 2009. Age-adjusted incidence of cervical cancer precursors was 77 (Kentucky), 60 (Michigan), and 54 (Louisiana) per 100,000 women. Highest rates were observed in those aged 20-29 years: 274 (Kentucky), 202 (Michigan), and 196 (Louisiana) per 100,000. The variable with the most missing data was race/ethnicity, which was missing for 13 % of cases in Kentucky, 18 % in Michigan, and 1 % in Louisiana. Overall rates of cervical cancer precursors were over sixfold higher than invasive cervical cancer rates [rate ratios: 8.6 (Kentucky), 8.3 (Michigan), and 6.2 (Louisiana)]. Conclusions: Incorporating surveillance of cervical cancer precursors using existing CCR infrastructure is feasible and results in collection of population-based incidence data. Standardized collection of these data in high-quality registry systems will be useful in future activities monitoring the impact of HPV vaccination across states. As a result of this study, ongoing surveillance of these lesions has now been conducted in four CCRs since 2010.

KW - Cervical intraepithelial neoplasia

KW - Epidemiology

KW - Population characteristics

KW - Public health

KW - Sexually transmitted diseases

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Population-based surveillance for cervical cancer precursors in three central cancer registries, United States 2009

Abstract

Keywords

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