Clinical Validation of a Vaginal Cervical Cancer Screening Self-Collection Method for At-Home Use A Nonrandomized Clinical Trial

Megan B. Fitzpatrick; Catherine M. Behrens; Karl Hibler; Courtney Parsons; Clair Kaplan; Ronald Orso; Lamar Parker; Lisa Memmel; Ann Collins; Colleen McNicholas; La Shonda Crane; Youri Hwang; Elizabeth Sutton; Jenell Coleman; Lindsay Kuroki; Kimberly Harshberger; Sigrid Williams; Ashley Jennings; Frank Buccini; Laura Gillis; Akiva P. Novetsky; David Hawkes; Marion Saville; Trena Depel; Emeline Aviki; Sangini S. Sheth; Christine Conageski

doi:10.1001/jamanetworkopen.2025.11081

Clinical Validation of a Vaginal Cervical Cancer Screening Self-Collection Method for At-Home Use A Nonrandomized Clinical Trial

Megan B. Fitzpatrick
, Catherine M. Behrens
, Karl Hibler
, Courtney Parsons
, Clair Kaplan
, Ronald Orso
, Lamar Parker
, Lisa Memmel
, Ann Collins
, Colleen McNicholas
, La Shonda Crane
, Youri Hwang
, Elizabeth Sutton
, Jenell Coleman
, Lindsay Kuroki
, Kimberly Harshberger
, Sigrid Williams
, Ashley Jennings
, Frank Buccini
, Laura Gillis

Akiva P. Novetsky, David Hawkes, Marion Saville, Trena Depel, Emeline Aviki, Sangini S. Sheth, Christine Conageski

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

6 Scopus citations

Abstract

IMPORTANCE One-quarter of US women who are at risk for cervical cancer delay screening. Self-collected (SC) cervical screening was recently US Food and Drug Administration (FDA)-approved in the US for use in a health care setting only; an at-home SC option is crucial to address clinic-related barriers to screening. OBJECTIVE To clinically validate the use of an SC device that was designed for optimal at-home performance, safety, ease-of-use, and dry storage and transport. DESIGN, SETTING, AND PARTICIPANTS This nonrandomized clinical trial used a prospective method comparison study design. Participants aged 25 to 65 years were recruited from 16 clinical sites in the US including community and academic practices from November 20, 2023, to April 5, 2024. Data analysis was conducted from April to August 2024. INTERVENTION Eligible participants collected a sample with the SC method, followed by a clinician-collected (CC) sample. The SC sample was eluted into PreservCyt at the laboratory and both samples were tested on an FDA-approved high risk human papillomavirus (hrHPV) test approved for primary screening. Participants were followed up for safety and completed usability and screening preference surveys. MAIN OUTCOME AND MEASURES The primary outcome measures were positive percentage agreement (PPA) and negative percentage agreement for detection of hrHPV between the SC and CC samples. Other study measures included clinical sensitivity for high grade cervical dysplasia and usability. RESULTS Of 609 screening-eligible participants, 599 (262 aged 30-39 years [43.7%]; 583 identified as female [97.3%]) had paired SC-CC samples, of which 582 had valid paired samples included in the end point analysis. Among the 582 evaluable paired samples, the PPA between SC compared with paired CC samples for detection of hrHPV was 95.2% (95% CI, 92.1%-97.1%; 278 of 292 participants). The absolute clinical sensitivity for detection of high-grade cervical dysplasia was 95.8% (95% CI, 86.0%-98.8%; 46 of 48 participants), equivalent to the CC (relative sensitivity, 1.00). Nearly all participants (555 of 601 participants [92.3%]) reported that the device instructions were easy or very easy to understand and also that they would choose SC if they knew the results were comparable to CC results (560 of 602 participants [93.0%]). CONCLUSIONS AND RELEVANCE In this nonrandomized clinical trial, SC samples collected with the device showed equivalent clinical sensitivity and exceeded the PPA end point for cervical screening. This SC method was found to be easy to use and to be a preferred option with high clinical performance intended for use in an at-home setting.

Original language	English
Article number	e2511081
Journal	JAMA Network Open
Volume	8
Issue number	5
DOIs	https://doi.org/10.1001/jamanetworkopen.2025.11081
State	Published - May 2025

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10.1001/jamanetworkopen.2025.11081

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Fitzpatrick, M. B., Behrens, C. M., Hibler, K., Parsons, C., Kaplan, C., Orso, R., Parker, L., Memmel, L., Collins, A., McNicholas, C., Crane, L. S., Hwang, Y., Sutton, E., Coleman, J., Kuroki, L., Harshberger, K., Williams, S., Jennings, A., Buccini, F., ... Conageski, C. (2025). Clinical Validation of a Vaginal Cervical Cancer Screening Self-Collection Method for At-Home Use A Nonrandomized Clinical Trial. JAMA Network Open, 8(5), Article e2511081. https://doi.org/10.1001/jamanetworkopen.2025.11081

@article{dc535dcec1464a0a8593abf242bd418c,

title = "Clinical Validation of a Vaginal Cervical Cancer Screening Self-Collection Method for At-Home Use A Nonrandomized Clinical Trial",

abstract = "IMPORTANCE One-quarter of US women who are at risk for cervical cancer delay screening. Self-collected (SC) cervical screening was recently US Food and Drug Administration (FDA)-approved in the US for use in a health care setting only; an at-home SC option is crucial to address clinic-related barriers to screening. OBJECTIVE To clinically validate the use of an SC device that was designed for optimal at-home performance, safety, ease-of-use, and dry storage and transport. DESIGN, SETTING, AND PARTICIPANTS This nonrandomized clinical trial used a prospective method comparison study design. Participants aged 25 to 65 years were recruited from 16 clinical sites in the US including community and academic practices from November 20, 2023, to April 5, 2024. Data analysis was conducted from April to August 2024. INTERVENTION Eligible participants collected a sample with the SC method, followed by a clinician-collected (CC) sample. The SC sample was eluted into PreservCyt at the laboratory and both samples were tested on an FDA-approved high risk human papillomavirus (hrHPV) test approved for primary screening. Participants were followed up for safety and completed usability and screening preference surveys. MAIN OUTCOME AND MEASURES The primary outcome measures were positive percentage agreement (PPA) and negative percentage agreement for detection of hrHPV between the SC and CC samples. Other study measures included clinical sensitivity for high grade cervical dysplasia and usability. RESULTS Of 609 screening-eligible participants, 599 (262 aged 30-39 years [43.7\%]; 583 identified as female [97.3\%]) had paired SC-CC samples, of which 582 had valid paired samples included in the end point analysis. Among the 582 evaluable paired samples, the PPA between SC compared with paired CC samples for detection of hrHPV was 95.2\% (95\% CI, 92.1\%-97.1\%; 278 of 292 participants). The absolute clinical sensitivity for detection of high-grade cervical dysplasia was 95.8\% (95\% CI, 86.0\%-98.8\%; 46 of 48 participants), equivalent to the CC (relative sensitivity, 1.00). Nearly all participants (555 of 601 participants [92.3\%]) reported that the device instructions were easy or very easy to understand and also that they would choose SC if they knew the results were comparable to CC results (560 of 602 participants [93.0\%]). CONCLUSIONS AND RELEVANCE In this nonrandomized clinical trial, SC samples collected with the device showed equivalent clinical sensitivity and exceeded the PPA end point for cervical screening. This SC method was found to be easy to use and to be a preferred option with high clinical performance intended for use in an at-home setting.",

author = "Fitzpatrick, \{Megan B.\} and Behrens, \{Catherine M.\} and Karl Hibler and Courtney Parsons and Clair Kaplan and Ronald Orso and Lamar Parker and Lisa Memmel and Ann Collins and Colleen McNicholas and Crane, \{La Shonda\} and Youri Hwang and Elizabeth Sutton and Jenell Coleman and Lindsay Kuroki and Kimberly Harshberger and Sigrid Williams and Ashley Jennings and Frank Buccini and Laura Gillis and Novetsky, \{Akiva P.\} and David Hawkes and Marion Saville and Trena Depel and Emeline Aviki and Sheth, \{Sangini S.\} and Christine Conageski",

note = "Publisher Copyright: {\textcopyright} 2025 Fitzpatrick MB et al.",

year = "2025",

month = may,

doi = "10.1001/jamanetworkopen.2025.11081",

language = "English",

volume = "8",

journal = "JAMA Network Open",

issn = "2574-3805",

number = "5",

}

Fitzpatrick, MB, Behrens, CM, Hibler, K, Parsons, C, Kaplan, C, Orso, R, Parker, L, Memmel, L, Collins, A, McNicholas, C, Crane, LS, Hwang, Y, Sutton, E, Coleman, J, Kuroki, L, Harshberger, K, Williams, S, Jennings, A, Buccini, F, Gillis, L, Novetsky, AP, Hawkes, D, Saville, M, Depel, T, Aviki, E, Sheth, SS & Conageski, C 2025, 'Clinical Validation of a Vaginal Cervical Cancer Screening Self-Collection Method for At-Home Use A Nonrandomized Clinical Trial', JAMA Network Open, vol. 8, no. 5, e2511081. https://doi.org/10.1001/jamanetworkopen.2025.11081

TY - JOUR

T1 - Clinical Validation of a Vaginal Cervical Cancer Screening Self-Collection Method for At-Home Use A Nonrandomized Clinical Trial

AU - Fitzpatrick, Megan B.

AU - Behrens, Catherine M.

AU - Hibler, Karl

AU - Parsons, Courtney

AU - Kaplan, Clair

AU - Orso, Ronald

AU - Parker, Lamar

AU - Memmel, Lisa

AU - Collins, Ann

AU - McNicholas, Colleen

AU - Crane, La Shonda

AU - Hwang, Youri

AU - Sutton, Elizabeth

AU - Coleman, Jenell

AU - Kuroki, Lindsay

AU - Harshberger, Kimberly

AU - Williams, Sigrid

AU - Jennings, Ashley

AU - Buccini, Frank

AU - Gillis, Laura

AU - Novetsky, Akiva P.

AU - Hawkes, David

AU - Saville, Marion

AU - Depel, Trena

AU - Aviki, Emeline

AU - Sheth, Sangini S.

AU - Conageski, Christine

PY - 2025/5

Y1 - 2025/5

N2 - IMPORTANCE One-quarter of US women who are at risk for cervical cancer delay screening. Self-collected (SC) cervical screening was recently US Food and Drug Administration (FDA)-approved in the US for use in a health care setting only; an at-home SC option is crucial to address clinic-related barriers to screening. OBJECTIVE To clinically validate the use of an SC device that was designed for optimal at-home performance, safety, ease-of-use, and dry storage and transport. DESIGN, SETTING, AND PARTICIPANTS This nonrandomized clinical trial used a prospective method comparison study design. Participants aged 25 to 65 years were recruited from 16 clinical sites in the US including community and academic practices from November 20, 2023, to April 5, 2024. Data analysis was conducted from April to August 2024. INTERVENTION Eligible participants collected a sample with the SC method, followed by a clinician-collected (CC) sample. The SC sample was eluted into PreservCyt at the laboratory and both samples were tested on an FDA-approved high risk human papillomavirus (hrHPV) test approved for primary screening. Participants were followed up for safety and completed usability and screening preference surveys. MAIN OUTCOME AND MEASURES The primary outcome measures were positive percentage agreement (PPA) and negative percentage agreement for detection of hrHPV between the SC and CC samples. Other study measures included clinical sensitivity for high grade cervical dysplasia and usability. RESULTS Of 609 screening-eligible participants, 599 (262 aged 30-39 years [43.7%]; 583 identified as female [97.3%]) had paired SC-CC samples, of which 582 had valid paired samples included in the end point analysis. Among the 582 evaluable paired samples, the PPA between SC compared with paired CC samples for detection of hrHPV was 95.2% (95% CI, 92.1%-97.1%; 278 of 292 participants). The absolute clinical sensitivity for detection of high-grade cervical dysplasia was 95.8% (95% CI, 86.0%-98.8%; 46 of 48 participants), equivalent to the CC (relative sensitivity, 1.00). Nearly all participants (555 of 601 participants [92.3%]) reported that the device instructions were easy or very easy to understand and also that they would choose SC if they knew the results were comparable to CC results (560 of 602 participants [93.0%]). CONCLUSIONS AND RELEVANCE In this nonrandomized clinical trial, SC samples collected with the device showed equivalent clinical sensitivity and exceeded the PPA end point for cervical screening. This SC method was found to be easy to use and to be a preferred option with high clinical performance intended for use in an at-home setting.

AB - IMPORTANCE One-quarter of US women who are at risk for cervical cancer delay screening. Self-collected (SC) cervical screening was recently US Food and Drug Administration (FDA)-approved in the US for use in a health care setting only; an at-home SC option is crucial to address clinic-related barriers to screening. OBJECTIVE To clinically validate the use of an SC device that was designed for optimal at-home performance, safety, ease-of-use, and dry storage and transport. DESIGN, SETTING, AND PARTICIPANTS This nonrandomized clinical trial used a prospective method comparison study design. Participants aged 25 to 65 years were recruited from 16 clinical sites in the US including community and academic practices from November 20, 2023, to April 5, 2024. Data analysis was conducted from April to August 2024. INTERVENTION Eligible participants collected a sample with the SC method, followed by a clinician-collected (CC) sample. The SC sample was eluted into PreservCyt at the laboratory and both samples were tested on an FDA-approved high risk human papillomavirus (hrHPV) test approved for primary screening. Participants were followed up for safety and completed usability and screening preference surveys. MAIN OUTCOME AND MEASURES The primary outcome measures were positive percentage agreement (PPA) and negative percentage agreement for detection of hrHPV between the SC and CC samples. Other study measures included clinical sensitivity for high grade cervical dysplasia and usability. RESULTS Of 609 screening-eligible participants, 599 (262 aged 30-39 years [43.7%]; 583 identified as female [97.3%]) had paired SC-CC samples, of which 582 had valid paired samples included in the end point analysis. Among the 582 evaluable paired samples, the PPA between SC compared with paired CC samples for detection of hrHPV was 95.2% (95% CI, 92.1%-97.1%; 278 of 292 participants). The absolute clinical sensitivity for detection of high-grade cervical dysplasia was 95.8% (95% CI, 86.0%-98.8%; 46 of 48 participants), equivalent to the CC (relative sensitivity, 1.00). Nearly all participants (555 of 601 participants [92.3%]) reported that the device instructions were easy or very easy to understand and also that they would choose SC if they knew the results were comparable to CC results (560 of 602 participants [93.0%]). CONCLUSIONS AND RELEVANCE In this nonrandomized clinical trial, SC samples collected with the device showed equivalent clinical sensitivity and exceeded the PPA end point for cervical screening. This SC method was found to be easy to use and to be a preferred option with high clinical performance intended for use in an at-home setting.

UR - https://www.scopus.com/pages/publications/105005821811

U2 - 10.1001/jamanetworkopen.2025.11081

DO - 10.1001/jamanetworkopen.2025.11081

M3 - Article

C2 - 40388167

AN - SCOPUS:105005821811

SN - 2574-3805

VL - 8

JO - JAMA Network Open

JF - JAMA Network Open

IS - 5

M1 - e2511081

ER -

Clinical Validation of a Vaginal Cervical Cancer Screening Self-Collection Method for At-Home Use A Nonrandomized Clinical Trial

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