May 22, 2024

Study finds cervical cancer screening may be safe at longer intervals

Empower health

The risk of detecting cervical precancer eight years after a negative human papillomavirus screening was found to be similar to the risk after three years (the commonly recommended screening interval) after a negative cytology screening, according to results published in Cancer Epidemiology, Biomarkers & Prevention, a journal of the American Association for Cancer Research.

In the last two decades, the United States has been transitioning from cytology to HPV-based screening for cervical cancer. The U.S. Preventive Services Task Force currently recommends one of three options for routine cervical cancer screening: cytology screening every three years, HPV screening every five years or co-testing in which both an HPV and cytology screening are conducted every five years.

Anna Gottschlich, Ph.D., M.P.H.

“There is currently a global shift from conventional cervical cancer screening methods like cytology, or the Pap smear, to HPV-based screening because HPV-based screening has a higher sensitivity to detect precancerous lesions,” said Anna Gottschlich, Ph.D., M.P.H., assistant professor of Oncology at the Wayne State School of Medicine and the Barbara Ann Karmanos Cancer Institute and corresponding author of “Evidence of decreased long-term risk of cervical pre-cancer after negative primary HPV screens compared to negative cytology screens in a longitudinal cohort study. 

“However, some have expressed concern that the longer interval between HPV screens may increase the risk for the development of cervical cancer. These findings should provide assurance that the five-year interval recommended for HPV screening is even safer than the three-year interval for cytology screening,” Dr. Gottschlich added.

Due to available high-performance screening methods, such as the HPV test, and the HPV vaccine, cervical cancer is highly preventable, which is why the World Health Organization has called for the global elimination of cervical cancer by 2030. Even though many high-income countries have established cytology-based screening programs, which have led to decreased rates, many still have rates above the WHO’s elimination threshold goal, including the U.S., where incidence is 7.6 per 100,000 individuals, according to federal statistics. 

As more countries adopt HPV screening programs to accelerate the elimination of cervical cancer, questions remain about the optimal interval between screens, which is why Dr. Gottschlich and her colleagues designed a study to investigate the long-term risk of cervical precancer after negative HPV screening compared to after negative cytology screening. They examined data from four cohorts of women and individuals with a cervix: 5,546 who had one negative HPV screen, 6,624 who had two consecutive negative HPV screens four years apart, 782,297 who had one negative cytology screen and 673,778 who had two consecutive negative cytology screens two to three years apart.

Dr. Gottschlich and colleagues used data from the Canadian HPV For Cervical Cancer Prevention randomized trial conducted between January 2008 and December 2016 and its 14-year longitudinal follow-up FOCAL-DECADE study for the HPV screening cohorts. Data were used from the British Columbia Cervix Screening Program during the same interval for the cytology cohorts. Participants from each cohort were between the ages of 25 and 65 at the initial screen. 
Cumulative risk of cervical intraepithelial neoplasia grades 2 (CIN2), 3 (CIN3) and higher (referred to as CIN2+ or CIN3+)—which are premalignant lesions of cervical cancer—were calculated for each cohort. The risk of CIN2+ eight years after one or two negative HPV tests was similar to that of three years after one or two negative cytology screens. After six years, longer than current five-year guidelines, HPV screens showed lower risk after both one and two negative tests. Risk of CIN3+ was also lower or similar in the HPV cohorts following eight years compared to the cytology cohorts after three years.

While risk for CIN2+ was higher for HPV screening for intervals longer than eight years compared to cytology after three years, the detection of cervical precancer still remained low after negative HPV screening during the 14-year duration of the study and was significantly lower than normal cytology screening.

“HPV screening performs better than cytology by detecting more precancer earlier, which can then be treated earlier,” Dr. Gottschlich said. “We saw that in our study population, even those who had only one negative HPV test were at very low risk for the development of cervical precancer for many years after the negative test.”

She said the results could better inform updated screening guidelines for cervical cancer, but each country or province will need to determine the right guidelines given their populations and resources at their disposal. 

“Policy leaders need to consider a broad array of factors in health decision-making in their settings when considering how to prioritize HPV-based screening over cytology,” Dr. Gottschlich said. “Optimal implementation strategies depend on the kind of screening engagement and resources available in each specific program.” She noted that it is also important to consider the potential loss to follow-up that comes with long screening intervals. “Extending intervals require health system considerations to ensure adequate continued engagement to minimize loss to follow up.”

Longer intervals between testing could allow for the realignment of resources to reach under-screened or unscreened populations and to encourage follow-up, Dr. Gottschlich added. “Screening alone is not sufficient to eliminate cervical cancer. We need to ensure that women who have an abnormal screen have access to diagnostic follow-up and treatment if necessary.”

Limitations of the study include the fact that even though participants in the HPV FOCAL were randomly assigned at the start of the trial, differences in drop-out and screening rates may have made the HPV groups less comparable over the course of the study. Additionally, co-testing was used during exit screens, where two cases of CIN2+ were caught in cytology that were missed by the HPV test. Dr. Gottschlich said this did not affect the main findings as a previous study found that cytology missed over eight times more CIN2+ compared to HPV screening. Also, the study was conducted in well-screened population, so the results are not directly applicable to low-resource settings.

"Research such as this by Dr. Gottschlich, and studies by faculty members conducted at Wayne State University changes the face of medicine for the better contiuously and is a key component of the university's Prosperity Agenda for the greater Detroit region, and empowering health for our urban neighborhoods," said Wael Sakr, M.D., dean of the WSU School of Medicine.

The study was funded by the National Institutes of Health, the Canadian Institutes for Health Research, the Michael Smith Foundation for Health Research and Michael Smith Health Research BC.

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