Early adoption of innovation in HPV prevention strategies: closing the gap in cervical cancer

Ishika Mahajan^1†, Amogh Kadam^2†, Lucy McCann^3,4†, Aruni Ghose^3,5,6,7,8†, Katie Wakeham^3,7,9, Navjot Singh Dhillon¹⁰, Susannah Stanway^7,11, Stergios Boussios^{5,12,13,14,15}, Soirindhri Banerjee¹⁶, Ashwini Priyadarshini¹⁷, Bhawna Sirohi^7,18*, Julie S Torode^19* and Swarupa Mitra^20*

¹Department of Oncology, Lincoln County Hospital, United Lincolnshire Hospitals NHS Trust, Lincoln, Lincolnshire, UK

²Government Cuddalore Medical College and Hospital, Chidambaram, India

³Department of Oncology, Barts Cancer Centre, St. Bartholomew’s Hospital, Barts Health NHS Trust, London, UK

⁴Centre for Primary Care, Wolfson Institute of Population Health, Queen Mary University, London, UK

⁵Department of Medical Oncology, Medway NHS Foundation Trust, Gillingham, Kent, UK

⁶Centre for Cancer Biomarkers and Biotherapeutics, Barts Cancer Institute, Queen Mary University of London, London, UK

⁷United Kingdom and Ireland Global Cancer Network

⁸Prevention, Screening and Early Detection Network, European Cancer Organisation, Brussels, Belgium

⁹Radiotherapy UK

¹⁰Department of General Surgery, Pilgrim Hospital, United Lincolnshire Hospitals NHS Trust, Boston, Lincolnshire, UK

¹¹Department of Medical Oncology, The Royal Marsden NHS Foundation Trust, London, UK

¹²Faculty of Life Sciences and Medicine, School of Cancer and Pharmaceutical Sciences, King’s College London, London, UK

¹³Kent and Medway Medical School, University of Kent, Canterbury, UK

¹⁴Faculty of Medicine, Health and Social Care, Canterbury Christ Church University, Canterbury, UK

¹⁵AELIA Organisation, Thessaloniki, Greece

¹⁶Department of Radiation Oncology, IPGMER and SSKM Hospital, Kolkata, India

¹⁷Department of Preventive and Social Medicine, VMMC and Safdarjung Hospital, New Delhi, India

¹⁸Department of Medical Oncology, BALCO Medical Centre, Vedanta Medical Research Foundation, Chattisgarh, India

¹⁹Institute of Cancer Policy, Centre for Cancer, Society & Public Health, King’s College London, London, UK

²⁰Department of Radiation Oncology, Fortis Medical Research Institute, Gurgaon, India

^†All authors contributed equally

^*Joint Senior Authors

Abstract

Cervical cancer (CC) is one of the highest prevailing causes of female cancer-related mortality globally. A significant discrepancy in incidence has been noted between high and low-middle-income countries. The origins of CC have been accredited to the human papillomavirus (HPV) with serotypes 16 and 18 being the most prevalent. HPV vaccines, with 90%–97% efficacy, have proven safe and currently function as the primary prevention method. In addition, secondary prevention by timely screening can potentially increase the 5-year survival rate by >90%. High-precision HPV DNA testing has proven to be both highly sensitive and specific for early detection and is advocated by the WHO. Lack of public awareness, poor screening infrastructure and access to vaccines, socio-cultural concerns, along with economic, workforce-associated barriers and the presence of marginalised communities unable to access services have contributed to a continued high incidence. This article comprehensively analyses the efficacy, coverage, benefits and cost-effectiveness of CC vaccines and screening strategies including the transition from cytological screening to HPV self-sampling, while simultaneously exploring the real-world disparities in their feasibility. Furthermore, it calls for the implementation of population-based approaches that address the obstacles faced in approaching the WHO 2030 targets for CC elimination.

Keywords: cervical cancer, screening, HPV, Pap, primary prevention, secondary prevention, vaccine, population health, elimination

Correspondence to: Aruni Ghose
Email: aruni.ghose1@gmail.com

Published: 11/09/2024
Received: 30/03/2024

Publication costs for this article were supported by ecancer (UK Charity number 1176307).

Copyright: © the authors; licensee ecancermedicalscience. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Introduction

Cervical cancer (CC) is the fourth highest cause of cancer-related mortality among women worldwide. In 2020, 604,100 new CC cases were reported with over 341,000 fatalities [1]. The human papilloma virus (HPV), a DNA virus, is the predominant causal agent of CC [2] (Figure 1). Twelve oncogenic strains of HPV have been identified as group 1 carcinogens or high risk by the International Agency for Research on Cancer [3], with serotypes 16 and 18 accounting for about 70% of CC cases [4].

Significant disparities between economically developing and developed countries exist regarding incidence (18.8 versus 11.3 per 100,000) and mortality (12.4 versus 5.2 per 100,000). This variance is directly driven by the disproportion in the availability of prevention and screening technologies and resources [5]. Ninety percent of deaths attributable to CC occur in low- and middle-income countries (LMICs), especially in sub-Saharan Africa, Melanesia, South-East Asia and South America [6]. Malawi in sub-Saharan Africa has the world’s highest CC incidence and mortality [7].

CC prevention requires a dual-pronged approach via screening and vaccination. Vaccination or primary prevention of CC started in 2007, but by 2020 it had been introduced as a prevention strategy in only 57% of countries worldwide [8, 9]. The full effect of vaccination can be seen only in the years following implementation as it prevents the natural history of the disease.

Screening achieves short-term goals through early detection of CC or premalignant lesions [10]. In the long term, sustained high coverage of vaccination, creates a population that is protected from high-risk diseases. There is thus a decreased screening requirement [11].

Despite the possibility of being able to achieve near complete prevention of disease, efforts to lower the incidence to the global elimination goals are forestalled, broadly due to a lack of public awareness or poor access to the vaccine, poor screening program infrastructure and insubstantial utilisation of strategies in LMICs secondary to cost and human resource factors [6, 12].

Figure 1. This figure shows onco-pathogenesis of CC due to HPV.

In a groundbreaking effort to eliminate CC entirely, the WHO launched a global strategy in November 2020. This ambitious plan, known as the ‘90-70-90 strategy’, aims to vaccinate 90% of girls against HPV by age 15, ensure 70% of women have access to accurate and reliable screening tests for CC by age 35 and again by 45 and guarantee 90% of women diagnosed with CC receive proper treatment, including both pre-cancerous and invasive stages, by the year 2030 [13].

Our review article comprehensively impresses on population-based strategies for primary and secondary prevention of CC (Figure 2). It also explores the hurdles in the path towards achieving the WHO 2030 targets, paving the way to elimination. We also aim to elaborate on the success of vaccination and screening programs in some countries, hoping to extrapolate these to the high-burden, low-reach zones.

HPV vaccination: the primary prevention

Primary prevention strategies against CC focus on prophylactic vaccination as the most effective form of long-term primary prevention of CC [14].

Three HPV vaccines are used most widely: Cervarix (a bivalent vaccine targeting HPV 16 and 18), Gardasil (a quadrivalent targeting 6/11/16/18) and Gardasil 9 (nonavalent targeting 6/11/16/18/31/33/45/52/58). These prevent about 70% to 90% of CC cases depending on the type used [15–17]. Recent developments have led to multiple other vaccines completing clinical trials in China and India (Table 1).

Since first licensure in 2006, HPV vaccination has been recommended for global use in females between 11 and 12 years by the US Centers for Disease Control and Prevention (CDC)’s Advisory Committee on Immunisation Practices [8, 9]. Over time, emerging evidence has led to adaptation of these global vaccination recommendations to improve cost-effectiveness and coverage. Recent evidence from Scandinavian countries suggests optimal effectiveness around adolescence or younger [18]. Beyond the age of 26, the efficacy and cost-effectiveness are poor, as people have often already potentially been exposed to HPV [19].

HPV is implicated in several non-CCs in both women and men, specifically anal, oropharyngeal, penile, vaginal and vulvar cancer. Even with the introduction of a national vaccine program for HPV for women and girls in most developed countries, the male vaccine program is yet to be established as a stronghold for prevention [20]. However, in 2016 WHO formulated public health recommendations which were extended to include vaccination rollout for boys and catch-up schemes for adults due to its cross-cover for non-cervical pathologies. This was based on high coverage in girls, i.e., ≥80% to be the most cost-effective means to achieve herd effect [21]. As per 2022 data, Canada, Denmark, Norway and Chile had achieved ≥ 80% coverage of first-dose vaccination in boys, with the USA, Argentina, Australia, Italy, New Zealand and the UK following behind with >50% coverage [22].

Figure 2. This figure is a conceptual diagram summarising the two main strategies for CC prevention.

Table 1. This table demonstrates characteristics of currently licenced HPV prophylactic vaccinations [15–17, 25, 53].

Efficacy

The efficacy of two- and three-dose HPV vaccination regimens have been rigorously assessed in large cohorts, both pre- and post-licensure. Initially, the WHO recommended a 3-dose schedule. In 2014, this shifted to a two-dose series spaced 6–12 months apart. More recently, a review of the evidence led to the Strategic Advisory Group of Experts on Immunization supporting both single and two-dose HPV vaccination schedules due to their comparable individual effectiveness and ease in programme implementation [23].

In 2018, the WHO commissioned an independent systematic review to assess the potential protection of the vaccine and the benefit it has on public health [24]. Across 26 trials (73,428 participants), they concluded with high-certainty evidence that HPV vaccines are protective against cervical precancers in adolescent females aged 15–26. As per protocol analysis, all licensed vaccines have proven similar successful efficacy [25]. However, Gardasil 9 has the potential to prevent 90% of CCs due to the additional strains it covers [26]. In addition to protecting the individual, there is also strong evidence that HPV vaccination offers herd immunity when sufficient population coverage is reached, further enhancing its efficacy [11].

The Kenya single-dose HPV-vaccine efficacy trial found that a single dose of Gardasil 9 produced an efficacy of over 97%, which was similar to that found in their trial assessing the triple dose regimen [27]. Early data from the Dose Reduction Immunobridging and Safety Study trial supports these findings, demonstrating that antibody avidity is the same in groups treated with single-, two- and three-dose regimens [28].

Safety

HPV vaccines have been consistently proven safe for over 15 years in rigorous independent analyses of large cohorts. This has included regular assessment by the Global Advisory Committee on Vaccine Safety from 2007 to 2015, which has repeatedly concluded no evidence of association with adverse effects [29]. In an independent analysis, deaths within the vaccine were deemed to be unrelated to the administration of the vaccine [24].

Coverage and effectiveness

As with many public health strategies, efficacy and safety in a clinical trial setting do not equate to effectiveness in real-life settings. Despite its licensure over 15 years ago, population coverage remains suboptimal. Current public HPV programmes cover less than a third of those eligible for the vaccine [29, 30]. A combination of barriers has led to poor uptake of vaccines, including problems with demand, supply and affordability which vary substantially depending on the setting.

Where vaccine programmes have been implemented effectively, the benefits are already seen. The UK has one of the most effective national vaccination programmes globally. In the 13 years since its implementation in 2008, it has substantially reduced CC incidence to near elimination [31]. However, this is not the case globally. While the majority of high-income countries (HICs) have >75% coverage, there remain some which have lagged. Japan is an HIC which has seen dramatic changes in vaccine uptake. The changes in recommendations from the Ministry of Health in 2013 led to a decline in coverage to a low of 0.3% in 2016 [32]. Since then, rectifications in recommendations in 2021 mean that the rates have improved [33]. We are yet to see any cancer spikes due to the lag time between HPV infection and CC presentation. However, this waiver in vaccine implementation is estimated to have resulted in around 5,000 preventable deaths [32].

Globally, there is vast inter- and intra-country variation, with the most significant disparity being between LMICs and HICs (Figure 3). Vaccination coverage tends to correlate with socioeconomic deprivation both between and within countries [34, 35]. In many LMICs, initial dose coverage of >70% was seen; however, this dropped with subsequent doses, with the third dose coverage being only around 30%. The ill-sustained impact is likely due to funding momentum failing and a dearth of sustainable programmes [36]. Furthermore, there is a large vaccination gap between urban and rural areas. Bolivia and Honduras are both exceptions which have achieved almost two-thirds coverage, sustainably maintained [34, 37]. All ten countries with the highest age-standardised rates of CC mortality are within West Africa, where national vaccination implementation has been slow [38]. This stems from a poor vaccine acceptance rate including poor information, safety, fertility and promiscuity concerns. In contrast, in Southeast Asia, vaccine uptake increased significantly once it was offered for free [39]. Altogether, the barriers to successful vaccination programs in LMICs are complex and vary depending on multiple factors including cultural, financial and environmental [34, 35].

The COVID-19 pandemic significantly disrupted routine vaccination programs worldwide. Studies from countries such as Brazil and the United Kingdom documented substantial declines in HPV vaccine doses administered during lockdowns and social distancing measures [40, 41]. A modelling study in the US predicted a 75% reduction in HPV vaccination during the first wave of COVID-19 [42].

Figure 3. The world map above shows the available data for vaccination cover of the first dose of the HPV vaccine in girls till the year 2022 [22, 30] (The areas shaded in purple depicts the areas which have started vaccination programs from 2019, but do not have adequate national data available).

Disruptions stemmed from several factors. School closures, a common strategy to curb COVID-19 spread, hindered school-based vaccination programs, a crucial delivery channel for HPV vaccines [42]. Healthcare system resource constraints further hampered routine vaccinations, with staff and facilities diverted to COVID-19 response efforts [43]. Additionally, vaccine hesitancy may have increased due to pandemic anxieties and misinformation [42].

Despite the challenges, some countries like Israel maintained or even increased HPV vaccination rates during the pandemic [44]. This suggests the importance of robust vaccination programs and effective communication strategies to mitigate disruption.

Even after restrictions have been lifted, the pandemic has continued to have residual disruption to vaccine supply and demand [45]. Recovery efforts are underway. The WHO emphasizes the need for catch-up programs to address vaccination gaps and restore pre-pandemic coverage levels [43]. Additionally, promoting HPV vaccination alongside COVID-19 vaccination campaigns can improve efficiency and reach [46].

Cost effectiveness

The cost-effectiveness of HPV vaccinations has been proven consistently. In a multi-country meta-analysis Rosettie et al [47] assessed incremental cost-effectiveness ratios (ICERs) for HPV vaccination in 195 countries and found a mean of US$ 4,217 per DALY averted (95% uncertainty interval: US$773–13,448) globally. This was significantly lower for certain regions, particularly in LMICs. ICER was reduced with values of US$706 per DALY averted (95% UI: $130–2,245) in Southern Asia and Sub-Saharan Africa [47]. This means that although individual mortality and morbidity benefits may be modest, there is substantial financial benefit to the implementation of HPV vaccinations at a global level.

Notably, the level of cost-effectiveness can vary depending on various factors including vaccine delivery method, number of vaccines given and target population, with young women and men having sex with men being the most effective cohort. Similarly, vaccinating those at older ages provides less cost-effectiveness due to the limited benefit [48].

Using the UK as a case study, an analysis was provided by Datta et al [49] Vaccinating girls provides significant health benefits at a reasonable cost. Threshold prices of £56–£108 per dose imply the healthcare system would see this as worthwhile. With a lower discount rate (1.5%), i.e., when future health benefits of preventing penile and throat cancers are valued more highly, vaccinating both sexes becomes cost-effective. At a higher discount rate (3.5%), vaccinating both sexes is less cost-effective than girls alone (£25–£53 threshold price). This is mainly due to herd immunity: vaccinating girls significantly reduces HPV transmission, indirectly protecting boys [49].

As discussed previously, various alterations of vaccination strategies have been made in recent years to improve ICER, such as the delivery of a single vaccination and combining vaccine delivery with that of other vaccinations [50].

Another consideration of cost-effectiveness is the cost per unit of each dose. Unit dosing is dependent on several factors, further complicating cost-effectiveness decisions within countries. For instance, the nonavalent vaccine Gardasil 9, is priced higher for full doses compared to the bi- and quadrivalent cervical vaccines. This means that in some countries, it is not cost-effective when the other vaccination options are, despite its coverage over more strains [51].

Similarly, prices of the same vaccine vary between different countries. While those within the GAVI Alliance are offered a sustainable supply of low-cost vaccines, the same vaccines can be over 20 times more expensive in developed countries [34]. Thus, countries such as Vietnam rely on qualifying for GAVI-priced vaccines to have sufficient cost-effectiveness to justify funding cervical vaccination programmes [52].

Middle-income countries that do not qualify for GAVI subsidies are most at risk of not being able to afford comprehensive vaccination programmes, often referred to as the ‘missing middle’. Despite the limited support, by 2020 around half of these countries had managed to implement a vaccination programme, with many more developing pilots [51]. In 2022, India achieved market authorisation of the novel vaccine Cervavac, which covers the same four strains as Gardasil. This offers a more affordable vaccine to India’s population; costing approximately 200–400 rupees (or 3.5 EUR), compared to the alternatives which are around 10 times the price [53, 54]. Such opportunities must be welcomed and encouraged to maximise protection.

Despite its proven safe, efficacious existence for a significant time, the coverage and cost-effectiveness of the HPV vaccines remain substantially sub-optimal.

People living with HIV (PLHIV)

HPV vaccination is crucial in PLHIV due to their increased susceptibility to HPV-related cancers. The WHO, the CDC and the British HIV Association recommend HPV vaccination in this population [55–57].

Studies have shown that the HPV vaccine is immunogenic in PLHIV [58, 59]. However, the magnitude of the immune response may be lower compared to the general population, particularly in individuals with advanced HIV disease or low CD4 counts [59, 60].

Available evidence suggests that the HPV vaccine can still be protective against HPV infection and related pre-cancerous lesions in PLHIV [60, 61]. However, long-term efficacy data and data on the prevention of invasive cancers specifically in this population are still limited [60, 61]. Ongoing research is crucial to fully understand its long-term impact and the potential need for different vaccination strategies in this population.

PLHIV are recommended to receive HPV vaccination according to the standard recommendations for the general population (typically 2 or 3 doses depending on age at initiation). However, some guidelines, like the CDC’s, recommend initiating vaccination as early as 9 years of age for individuals with HIV, considering potential immune system compromise [56]. The Canadian Paediatric Society suggests a 3-dose regimen for immunocompromised individuals to ensure optimal immune response [62]. Despite the guidelines, achieving optimal HPV vaccination coverage among HIV-positive individuals remains a challenge.

CC screening: the secondary prevention

Secondary prevention or screening programs aim to reduce morbidity and mortality associated with CC by increased detection of precursor lesions and early identification of invasive carcinoma [63]. If recognised early, the 5-year survival rate of women diagnosed with invasive CC is 92% as compared to 58% and 18% for locally advanced and metastatic stages, respectively [1].

Screening tools: transition from cytology to HPV testing

The Pap smear

Since its introduction in the 1940s, papanicolaou smear has been the most widely used tool for the detection of precancerous cervical lesions. It led to a greater than 70% decrease in the mortality associated with CC in the US [64]. However, a nationwide study in the UK found its sensitivity to be 55.4% and specificity to be 96.8% [65]. A meta-analysis further compared 11 separate studies with a cumulative of 39,050 participants to find that sensitivity and specificity estimates of cytology ranged from 0.43 to 0.94 and 0.78 to 0.98, respectively. The pooled sensitivity and specificity were 0.70 and 0.95, respectively. While specificity remained consistent over several studies, the sensitivity was widely variable [66]. To balance this inconsistency in sensitivity, a lifetime of repeat testing is warranted. In low-resource settings where regular testing is difficult due to limited access and knowledge about CC screening, this poses a significant hurdle. Another caveat is their implementation. Pap smears are labour intensive and require repeat testing, trained personnel to conduct and interpret the test, equipment and other resources. All of these are a lacuna in many regions of the world [67]. Adoption of a cytology (Pap smear)-based screening program in a few LMICs has shown little benefit, with an unchanged mortality rate after 5 years. This was likely due to the above-mentioned constraints, low-quality smears and the inability to allocate adequate capital to ensure high-quality standards [68].

Visual inspection

To overcome the aforementioned gap and to adopt a screen-and-treat approach, visual inspection with acetic acid (VIA) became the preferred CC screening modality in LMICs. The sensitivity and specificity estimates after comparing 11 studies were found to be 0.17–1.00 and 0.08–0.95, respectively. The pooled sensitivity and specificity were 0.77 and 0.82, respectively [66]. Visual inspection techniques can be performed relatively more efficiently than other modalities in low-resource settings as they require a simpler infrastructure, are not specialist-intensive and are significantly cheaper. Other advantages for high-burden zones are that VIA only takes a few minutes to perform, and the results can be immediately interpreted, negating the need for time-consuming laboratory processing [69]. It was also found that visual inspection methods had higher sensitivity than cytology testing, detecting more high-grade CIN in several studies conducted in India [70]. However, this ability to detect a greater number of positive cases is a double-edged sword. It was found that when compared to cytology or HPV testing, VIA led to a much higher number of false positives and subsequent overtreatment [66]. While VIA appears to be a good alternative to the Pap smear in LMICs, it comes with significant challenges of scaling up. A variance of sensitivity is also seen in older women with other endocervical lesions. Moreover, factors such as age, parity and underlying cervical disease also affect the positive predictive value [70]. There is also a significant difference in accuracy when visual inspection is performed by physicians (30.2% positivity) versus nurses (36.3% positivity), highlighting the significance of the subjective nature of the evaluation [71]. Vedantham et al [72] uncovered a remarkable difference in positivity rates (4% to 31%) when similarly qualified gynaecologists conducted testing and the greatest variation was seen between the two doctors that had received the most training. They also found that the positivity rates increased for disease-negative women with cervical inflammation (6.1%–15.5% (p-value < 0.001) [72].

HPV testing

The shortcomings of cytology and visual inspection techniques along with the realisation that oncogenic strains of HPV are responsible for over 95% of CC led to the introduction of HPV DNA testing in CC screening programs [73] (Table 2).

Initially, HPV assays were integrated into clinical practice to triage minor cytological abnormalities, then along with cytology as co-testing and now most recently as a stand-alone primary screening tool [69]. The latest WHO guidelines recommend HPV DNA detection as the modality of choice for primary CC screening in women of the general population and also those that live with HIV, over cytology and VIA. It advocates the screening to begin by the age of 30 and until age 50 with screening intervals of 5 or 10 years [74]. An HPV DNA test looks for the presence of viral DNA in the cervical cells [75]. HPV testing is comparable in accuracy to the other commonly employed modalities for the detection of cervical precancerous lesions among women. It detects high-grade precancerous lesions (CIN3) earlier than cytology, thereby increasing the likelihood of treatment before progression to invasive cancer. A follow-up of four randomised control trials found that HPV testing offers 60%–70% more protection against invasive cancer than cytology [76]. Additionally, a single round of HPV DNA testing has been shown to increase the number of cases detected and lead to a reduction in the progression to advanced cancer and mortality [77].

The sensitivity and specificity of singular HPV DNA testing were found to be 0.64–1.00 and 0.56–0.97, respectively. The pooled sensitivity of 15 studies was 0.94 and specificity was 0.88 [64]. The ATHENA Study conducted in the US found that HPV testing detected 64.2% more CIN3 when compared to cytology and 22.5% more CIN3 than a co-testing strategy. This stark difference was seen when baseline testing was done and also on an annual follow-up done for 3 years subsequently. It was also noted that HPV Testing had the highest 3-year adjusted sensitivity when compared to cytology (47.8%); and co-testing (61.7%) for CIN 3. Moreover, a negative HPV test had a much lower risk of CIN3 as compared to a negative cytology report. Out of all the women with a positive CIN3 over 3 years, 47.3% had an initial negative cytology report while only 9.8% had an initial negative high-risk HPV test [78].

Table 2. This table summarises the pooled sensitivity and specificity of the various screening strategies discussed [66, 79, 93].

Co-testing versus stand-alone testing

Co-testing refers to testing for HPV DNA and cytology from a single sample collected by a clinician. It takes longer and is more expensive when compared to a single HPV test alone. HPV testing had a sensitivity of 90% and 95% for detecting underlying CIN2+ and CIN3+, respectively. Adding cytological testing to it leads to an increase in average sensitivity of only 5% for CIN2+ and 2% for CIN3+ along with a marked decrease in the specificity 0.95 and 0.93, respectively [79]. The added sensitivity benefitted very few women, as little as five women per million per year [80]. Another study found that in comparison, stand-alone testing was superior to co-testing using both Pap smear and liquid-based cytology. Co-testing with Pap also had higher false positive results and more referrals to colposcopy [81]. A study that compared the long-term emergence of pre-cancer and cancer in negative tests found that primary HPV tests done every 3 years provided similar, if not more, reassurance than co-testing every 5 years. The risk for HPV testing and co-testing was as follows, CIN3: 0.069% versus 0.19%, (p < 0.0001) and invasive cancer: 0.011% versus 0.020%, (p < 0.0001) [82]. There is an insignificant difference in the cumulative risk of invasive carcinoma for a double negative result (HPV and cytology) as compared to a single HPV negative result in the long run [79]. Additionally, an HPV-negative/cytology-positive result only led to a minor increase in the detection of precancerous lesions (3.5%) and cancer (5.9%) [80].

The small increase in sensitivity afforded by co-testing is inadequate to justify the difficulties posed by it, thus stand-alone HPV testing should be considered as the superior screening tool over co-testing.

DNA versus mRNA testing

WHO recommends countries that are starting screening programs begin with HPV testing and encourages others to transition to the same as soon as feasible. However, HPV mRNA testing can be a suitable alternative. The increased expression of the mRNA coding for E6/E7 proteins, which are essential for CC pathogenesis, shows a higher risk for cancer. These tests primarily detect the presence of E6/E7 mRNA of oncogenic HPV types and thus could be a more specific predictor for cancer risk [83]. In comparison to DNA testing, mRNA testing was discovered to be similarly sensitive and more specific with a relative sensitivity and specificity of 0.98 and 1·03 for CIN2+. A 4–7-year relative sensitivity analysis showed similar values in the range of 0.91–1.05 when compared to DNA testing. The commonly used APTIMA test had a lower sensitivity for self-collected samples and hence use could be limited to clinical settings [84].

The consideration of mRNA in primary CC screening is due to its increased specificity compared to DNA testing. A few separate studies that evaluated the role of mRNA as the primary screening tool found that it produces results similar to HPV DNA testing programs [85, 86]. However, a reduction in colposcopy referrals that is expected of a modality with higher specificity was not observed [86]. That combined with the finding that solitary mRNA screening would miss 3% of patients with CIN 3 when compared to DNA testing has led to some reluctance to shift to mRNA testing [87]. An interesting application was noted by a group that tried mRNA triage on DNA-positive cases. Both tests were performed on the same sample. It was found this co-testing strategy led to a 54.5% reduction in colposcopy referrals and was more cost-effective when compared to stand-alone DNA testing [88]. The most conclusive evidence for the debate between mRNA versus DNA comes from the WHO recommendations which firmly advocate for the HPV DNA test as the first-line primary screening tool. It suggests that mRNA may be used as an alternative when the samples are collected by the clinician and there exists the capacity to repeat testing at 5-year intervals [74].

Self sampling

HPV self-sampling (HPV SS) is a process by which a woman can use a testing kit (options available to programmes include lavage, brush, swab, or vaginal patch) to collect a cervicovaginal sample that is sent for laboratory analysis. The test cannot diagnose CC but will identify if a woman is infected with a high-risk HPV by detecting viral DNA [89]. Rolling out self-sampling kits in bulk as part of the CC screening program led to an increase of 10% in test coverage in just a year in Sweden. It was well accepted by the target population due to its ease of use and is recommended due to the lower costs associated with it [90].

Non-responders are screening-eligible women who do not participate in routine CC screening programs. Non-responders are significant because 50% of all positive cases from the UK, USA and Netherlands are seen in women with no history of screening. HPV SS can be a possible solution to fill this gap [91]. Many women are reluctant to participate in clinical conducted programs because there is a fear of pain, embarrassment and invasion of privacy, particularly related to the pelvic examination using a speculum. Often, religious/cultural sentiments and a lack of access to healthcare centres prevent interested women from attaining necessary screening interventions. HPV SS is a unique solution to this multifaceted problem because the test can be done easily, in private and without any pain [92].

A 2014 meta-analysis that pooled data from 36 studies revealed that HPV SS could detect 76% of CIN2 and CIN3. The pooled absolute specificity for CIN2+ was 86% and for CIN3 was 87% [93]. The pooled sensitivity and specificity of self-collected samples were slightly lower than that of clinician-collected samples (12% reduction in sensitivity for CIN2+) [94]. This gap can further be bridged by the usage of polymerase chain reaction (PCR)-based HPV testing which has similar sensitivities across both scenarios [93].

The MARCH randomised control trial assessed the value of HPV SS and compared it to cytology in Mexico. They found HPV SS to be 3.4 times more sensitive and it detected 4.2 times more invasive cancer than cytology. One drawback was the lower positive predictive value of the test, but it makes up for it with higher sensitivity. In low-resource settings, cytology-based programs are not as successful due to restricted infrastructure. Women in these regions typically get tested only a handful of times in their lifetimes and hence benefit from a more sensitive test [95].

Due to its comparable clinical accuracy, lower cost and better acceptability, HPV SS can potentially become an important add-on strategy for women who do not participate in routine screening.

A population-based cervical screening program

Population-based screening programs require that a target group be identified and invited to participate. In opportunistic screening, the healthcare provider or patients must take the initiative to do screening as per the guidelines (Table 3) [96]. The WHO advocates for the adoption of large-scale, national population-based screen-and-treat programs. The present guideline demands for screening at least 70% of women by the age of 35 and then again by 45 (with 90% follow up when cervical disease is identified), working toward a 2030 goal of elimination of CC [6, 97, 98].

The WHO CC Elimination Modelling Consortium was developed in 2020 and includes the 90-70-90 triple intervention coverage targets, i.e., scaling up of HPV vaccination, twice-lifetime cervical screening, treatment of CIN and invasive cancer to 90%, 70% and 90%, respectively [6, 97, 98]. This model was used to predict CC-related mortality in 78 LMICs. Vaccination alone would reduce mortality by 0.1%, 61.7% and 89.5% by 2030, 2070 and 2120, respectively. Integrating twice lifetime screening and treatment would increase those figures to 34.2%, 92.3% and 98.6%, respectively. Moreover, by 2030, half and one-third of CC related deaths could be avoided in sub-Saharan Africa and South Asia respectively, in sync with the UN sustainable development goals [97]. In another analysis of the model, girls-only vaccination (age 9 at catch up to age 14) yielded elimination in 60% LMICs with threshold incidence ≤4/100,000, 99% LMICs with incidence ≤10/100,000 and 87% LMICs with ≥85% reduction of threshold incidence. Superimposing twice-lifetime screening achieved 100% elimination in all these 3 groups [98].

Akin to the WHO, the Canadian Partnership Against Cancer [99] developed an action plan for a 90-90-90 target by 2030 to eliminate CC by 2040 projecting itself as the first nation to do so. Strategies include scaling up HPV vaccination, primary HPV screening and follow-up of abnormal results. In Australia, a modelling study revealed that courtesy of high coverage of vaccination and screening, the age-standardised annual incidence is <6/100,000 by 2020 and <4/100,000 by 2028. Regarding mortality, the trend indicates an age-standardised annual mortality rate of 1/100,000 [100]. The US-based Cancer Intervention and Surveillance Modelling Network predicted that by 2038–2046, a threshold CC incidence of < 4/100,000 is feasible. Elimination could be pre poned to 2028–2033 provided there is higher screening coverage [101].

Cost effectiveness

When compared to visual inspection and cytology, HPV DNA cervical sampling is the most cost-efficient choice (Table 4). Not only is it the most affordable, but it also provides the greatest average reduction in cancer risk over a lifetime when compared to other tests. This can be illustrated from data collected in three countries – India, Nicaragua and Uganda. Indian analysis found that HPV Testing done thrice in a lifetime (at 30, 35 and 40 years) had an ICER of I$ 1600 per year of life saved (YLS) with the highest life expectancy gains and a reduction of 48.7% in lifetime risk of cancer. Similar statistics were observed in Nicaragua (I$1200 per YLS) and Uganda (I$420 per YLS) [110]. A Colombian study discovered cytology done at 3-year intervals to be the most expensive modality and HPV DNA testing repeated 5 years to be the cheapest along with an expected reduction in mortality from 69% to 81% [111]. An El Salvadorian study came to a similar conclusion that HPV Testing followed by cryotherapy was the most effective (reduction in cancer risk by 58.5%) and most cost-effective (US$490 per YLS) modality for CC screening [112]. A study conducted in Thailand assessed the cost effectiveness of using the detection of HPV p16/18 as the primary screening test as opposed to conventional cytology and found it to be a more sensitive (82.65% versus 55.85%, respectively) test while maintaining the specificity (96.47 versus 95.48%, respectively) and reduced false positives. All these factors make it a more cost-effective and well-rounded option with an ICER of $1395 per QALY gained [113].

The above evidence talks about the cost effectiveness of HPV testing by illustrating values of ICER per YLS and QALY while the following shines a light on the amount per detected lesion. According to the FOCAL trial conducted in Canada, HPV testing followed by reflexive cytology identified more lesions and was associated with a lower cost per detected lesion ($7551) as compared to the control group that received just cytology ($8325) [114]. Another study conducted in Thailand compared the ICER in terms of cost per detected case of CIN2 and found HPV testing to dominate over cytology. The cost per detected case was found to be $1219.9 [115]. A modelling study in the Netherlands concluded that the total costs fell by 21% and the cost per QALY gained was €12,225 (46% less) for HPV testing as compared to €22,678 for the cytology program [116]. Another HIC model-based study conducted by the NHS estimated annual savings of £13 million on average if a switch was made to HPV testing [117].

Even in settings where an established cytology-based screening program already exists, switching over to a hybrid strategy (cytology till age 29 and HPV Testing thereafter) will save funds with the money spent to obtain 1 year with the quality of life being under the willingness to pay threshold (negative ICER of US$ 37.87) [118].

Table 4. This table demonstrates the cost effectiveness of HPV testing strategies over cytology [110–116].

Table 4. This table demonstrates the cost effectiveness of HPV testing strategies over cytology [110–116].

Coverage and effectiveness

The average percentage of 55 LMICs for women screened for CC was 44%. Much improvement needs to happen to reach the WHO 2030 goal of 70% screening coverage. Among the LMICs, Latin America and the Caribbean nations had the highest numbers (country-level median of 84.6% – IQR, 65.7%–91.1%; range, 11.7%–97.4%) while Sub-Saharan Africa lags severely behind with the global lowest screening coverage (country-level median, 16.9%; IQR, 3.7%–31.0%; range, 0.9%–50.8%) [119].

Some outliers from the LMIC group have shown an increasing trend in screening coverage despite many challenges. Notably, countries like Taiwan, Portugal, Mexico, Argentina and El Salvador show promising results. Africa, Botswana and Costa Rica have shown good progress. All these outliers have a well-executed population-based national screening program with HPV testing at the helm of it as the primary screening modality. The lifetime screening percentages for Botswana and El Salvador are 50% and 95%, respectively. Costa Rica has shown commendable growth in recent years with 77% of women having undergone screening in the past 5 years [6]. The success of the Latin American nations can be attributed to the presence of national CC screening programs that provide free-of-cost services to women at the local level [120]. Taiwan after implementing a national program has seen a reduction in invasive cancer by 47.8% during 1995–2006 [119]. Hence, while the developed nations predictably show an improving graph due to their higher expenditure, bridging the gap in LMICs is not an impossible task.

Regarding coverage for PLHIV, WHO guidelines provide special considerations. Testing commences from the age of 25 with a primary HPV DNA test. If positive, then a secondary test of either partial genotyping, colposcopy, VIA, or cytology is performed to triage women. This screen, triage and treat approach is to be repeated every 3–5 years till the age of 50 [74]. The factors that are shown to increase participation in screening programs are formal education, and knowledge and awareness of CC, its risk factors and severity. Women who had the aforementioned factors were around 3.5 times more likely to be screened [121]. Another fix could be the implementation of self-sampling for PLHIV as many are unable to access screening clinics due to HIV-associated stigma. Studies find it has good acceptability. Over 90% of PLHIV included in a study said self-sampling was comfortable and were willing to try it again. However, many also prefer clinician-collected samples as they trust trained professionals over themselves for sample collection [120–122].

The possible effect of vaccination on screening is noteworthy. According to Wilyman [123], HPV vaccination may decrease the rate of abnormal Pap tests and ultimately weaken the positive predictive value of cytology. Hence, once HPV vaccination becomes a routine practice, the HPV test may be considered as a primary screening procedure and cytology for women thereafter who test HPV positive. Other considerations may include delaying the initial screening to 25 years of age and reducing the frequency of screening [123].

A substantial challenge to CC screening in recent times has been the COVID-19 pandemic. Screening rates plummeted by 94% post movement restriction orders. After lifting restrictions, the screening numbers were 35% less than pre-pandemic trends. A comparative model-based analysis done to assess the future impact of COVID-19 disruptions showed that women screened with cytology alone would show the greatest increase in cancer incidence [124]. It also revealed that delaying screening in previously HPV-negative women would not have a significant impact. A risk-based approach for prioritising patients (versus an algorithm-based strategy), with an HPV-based screening program with special emphasis on self-collected HPV testing and integration of telehealth is recommended [125]. Having mentioned the aforesaid, in the setting of a fear of entering public spaces, HPV SS testing kits delivered at the doorstep are predicted to increase the population uptake of screening [89].

People living with HIV

CC screening guidelines for PLHIV differ slightly from the general population due to their increased risk of developing CC [126].

The American College of Obstetricians and Gynecologists (ACOG) recommends initiating screening earlier for HIV-positive women, starting at age 21 [127]. This recommendation aligns with guidelines from other organisations like the CDC [128].

Screening frequency may be increased compared to the general population. ACOG suggests Pap smears every 6 months for the first 2 years followed by yearly Pap smears or co-testing (Pap smear and HPV test) every 3 years thereafter, depending on individual risk factors [127]. The CDC also suggests similar increased screening frequency for high-risk individuals, including those with HIV [128].

HPV testing may play a more prominent role in screening for HIV-positive individuals. Co-testing is being increasingly recommended as it can improve the detection of pre-cancerous lesions even in the presence of abnormal Pap smears that might be misleading due to immune system issues in HIV [127, 129, 130].

Early detection and intervention are crucial for preventing CC in this high-risk population. The adapted screening guidelines aim to balance the need for increased vigilance with minimizing unnecessary procedures while considering the potential for inconclusive Pap smears due to immune system factors.

Conclusion

The dramatic disparity in incidence rates between HICs and LMICs is primarily due to differential access to effective screening and preventive treatment; similar disparities also exist within countries. As HPV vaccinations are practically feasible and cost-effective, increasing acceptance and coverage should be a public health priority. While the context-specific barriers should be addressed, there is a clear need for regular monitoring and sustained funding within all HIC and LMIC settings to ensure progress is sustained. The efficacy of single-dose schedules has the potential to accelerate progress considerably in the coming years; they will massively enhance cost-effectiveness, simplify delivery schedules and enhance coverage. On another note, HPV testing for primary screening dominates other strategies (i.e., it is more effective and cost effective) and, therefore, if implemented properly with regular testing and stringent quality assurance checks, it could become a well-rounded and universal option with cost-effectiveness and optimum therapeutic value for LMICs and HICs alike. However, vaccines should not substitute screening and vice-versa – a combined approach is needed to combat this global problem. It is undoubtedly the need of the hour as international gaps are threatened to widen secondary to the lag in LMICs.

Acknowledgments

Nil.

Conflicts of interest

No conflict of interest.

Funding

No funding.

Author contributions

Conceptualisation and design – AG, KW, SS, BS, SM.

Data collection and assembly – IM, AK, LM, AG, SB1, SB2.

Data analysis and interpretation - IM, AK, LM, AG, KW, NSD, SS, BS, JST, SM.

Manuscript writing – IM, AK, LM, KW, NSD.

Final approval of manuscript – All authors.

References

1. Sung H, Ferlay J, and Siegel RL, et al (2021) Global cancer statistics 2020: GLOBOCAN estimates of incidence and mortality worldwide for 36 cancers in 185 countries CA Cancer J Clin 71(3) 209–249 https://doi.org/10.3322/caac.21660 PMID: 33538338

2. Bosch FX, Burchell AN, and Schiffman M, et al (2008) Epidemiology and natural history of human papillomavirus infections and type-specific implications in cervical neoplasia Vaccine 26(Suppl 10) K1–K16 https://doi.org/10.1016/j.vaccine.2008.05.064 PMID: 18847553

3. IARC Working Group on the Evaluation of Carcinogenic Risks to Humans (2007) Human papillomaviruses IARC Monogr Eval Carcinog Risks Hum 90 1–636

4. Cohen PA, Jhingran A, and Oaknin A, et al (2019) Cervical cancer Lancet 393(10167) 169–182 https://doi.org/10.1016/S0140-6736(18)32470-X PMID: 30638582

5. Ferlay J, Colombet M, and Soerjomataram I, et al (2021) Cancer statistics for the year 2020: an overview Int J Cancer 149(4) 778–789 https://doi.org/10.1002/ijc.33588

6. World Health Organization (2020) Global Strategy to Accelerate the Elimination of Cervical Cancer as a Public Health Problem (Geneva: World Health Organization)

7. Arbyn M, Weiderpass E, and Bruni L, et al (2020) Estimates of incidence and mortality of cervical cancer in 2018: a worldwide analysis Lancet Glob Health 8(2) e191–e203 https://doi.org/10.1016/S2214-109X(19)30482-6 PMCID: 7025157

8. Gultekin M, Ramirez PT, and Broutet N, et al (2020) World Health Organization call for action to eliminate cervical cancer globally Int J Gynecol Cancer 30(4) 426–427 https://doi.org/10.1136/ijgc-2020-001285 PMID: 32122950

9. Bruni L, Saura-Lázaro A, and Montoliu A, et al (2021) HPV vaccination introduction worldwide and WHO and UNICEF estimates of national HPV immunization coverage 2010-2019 Prev Med 144 106399 https://doi.org/10.1016/j.ypmed.2020.106399

10. World Health Organization (2014) Comprehensive Cervical Cancer Control: a Guide to Essential Practice 2nd edn (Geneva: World Health Organization)

11. Drolet M, Bénard É, and Pérez N, et al (2019) Population-level impact and herd effects following the introduction of human papillomavirus vaccination programmes: updated systematic review and meta-analysis Lancet 394(10197) 497–509 https://doi.org/10.1016/S0140-6736(19)30298-3 PMID: 31255301 PMCID: 7316527

12. de Martel C, Plummer M, and Vignat J, et al (2017) Worldwide burden of cancer attributable to HPV by site, country and HPV type Int J Cancer 141(4) 664–670 https://doi.org/10.1002/ijc.30716 PMID: 28369882 PMCID: 5520228

13. Cervical Cancer [Internet] (Geneva: World Health Organization) [https://www.who.int/news-room/fact-sheets/detail/cervical-cancer?gad_source=1&gclid=Cj0KCQiAz8GuBhCxARIsAOpzk8xAqe75HoWimxKt47QvQ7_kNLCb__HOSDqoNR8tvk2NJY77Hzm9B7UaAhJqEALw_wcB] Date accessed: 07/05/24

14. Senkomago V, Henley SJ, and Thomas CC, et al (2019) Human papillomavirus-attributable cancers – United States, 2012–2016 MMWR Morb Mortal Wkly Rep 68(33) 724–728 https://doi.org/10.15585/mmwr.mm6833a3 PMID: 31437140 PMCID: 6705893

15. GlaxoSmithKline (2023) FDA Approves Cervarix, GlaxoSmithKline’s Cervical Cancer Vaccine (Brentford: GlaxoSmithKline) [https://www.gsk.com/en-gb/media/press-releases/fda-approves-cervarix-glaxosmithkline-s-cervical-cancer-vaccine/] Date accessed: 18/03/23

16. Centres for Disease Control and Prevention (2024) Human Papillomavirus (HPV) Vaccine [https://www.cdc.gov/vaccinesafety/vaccines/hpv-vaccine.html] Date accessed: 05/03/24

17. Zou Z, Fairley CK, and Ong JJ, et al (2020) Domestic HPV vaccine price and economic returns for cervical cancer prevention in China: a cost-effectiveness analysis Lancet Glob Health 8(10) e1335–e1344 https://doi.org/10.1016/S2214-109X(20)30277-1 PMID: 32971056

18. Dehlendorff C, Sparén P, and Baldur-Felskov B, et al (2018) Effectiveness of varying number of doses and timing between doses of quadrivalent HPV vaccine against severe cervical lesions Vaccine 36(43) 6373–6378 https://doi.org/10.1016/j.vaccine.2018.09.011 PMID: 30249423

19. Kim JJ, Simms KT, and Killen J, et al (2021) Human papillomavirus vaccination for adults aged 30 to 45 years in the United States: a cost-effectiveness analysis PLoS Med 18(3) e1003534 https://doi.org/10.1371/journal.pmed.1003534 PMID: 33705382 PMCID: 7951902

20. Newman PA, Logie CH, and Doukas N, et al (2013) HPV vaccine acceptability among men: a systematic review and meta-analysis Sex Transm Infect 89(7) 568–574 https://doi.org/10.1136/sextrans-2012-050980 PMID: 23828943 PMCID: 3812849

21. World Health Organization (2016) Guide to Introducing HPV Vaccine Into National Immunization Programmes (Geneva: World Health Organization)

22. Human Papillomavirus (HPV) Vaccination Coverage [Internet] (Geneva: World Health Organization) [https://immunizationdata.who.int/pages/coverage/hpv.html?GROUP=Countries&ANTIGEN=&YEAR=&CODE=] Date accessed: 07/03/24

23. World Health Organization (2022) Highlights from the Meeting of the Strategic Advisory Group of Experts (SAGE) on Immunization (Geneva: World Health Organization) [https://cdn.who.int/media/docs/default-source/reproductive-health/sage_april2022meetinghighlights_11apr2022_final.pdf?sfvrsn=21bcfb4f_3] Date accessed: 20/02/24

24. Arbyn M, Xu L, and Simoens C, et al (2018) Prophylactic vaccination against human papillomaviruses to prevent cervical cancer and its precursors Cochrane Database Syst Rev 5(5) CD009069 PMID: 29740819 PMCID: 6494566

25. Bergman H, Buckley BS, and Villanueva G, et al (2019) Comparison of different human papillomavirus (HPV) vaccine types and dose schedules for prevention of HPV-related disease in females and males Cochrane Database Syst Rev 2019(11) CD013479 PMID: 31755549 PMCID: 6873216

26. Yang DY and Bracken K (2016) Update on the new 9-valent vaccine for human papillomavirus prevention Can Fam Physician 62(5) 399–402 PMID: 27255620 PMCID: 4865336

27. Barnabas RV, Brown ER, and Onono MA, et al (2022) Efficacy of single-dose HPV vaccination among young African women NEJM Evid 1(5) EVIDoa2100056 https://doi.org/10.1056/EVIDoa2100056 PMID: 35693874 PMCID: 9172784

28. Watson-Jones D, Changalucha J, and Whitworth H, et al (2022) Immunogenicity and safety of one-dose human papillomavirus vaccine compared with two or three doses in Tanzanian girls (DoRIS): an open-label, randomised, non-inferiority trial Lancet Glob Health 10(10) e1473–e1484 https://doi.org/10.1016/S2214-109X(22)00309-6 PMID: 36113531 PMCID: 9638030

29. Meeting of the global advisory committee on vaccine safety, 7–8 June 2017 (2017) Wkly Epidemiol Rec 92(28) 393–402

30. UNICEF (2019) Human Papillomavirus Vaccine: Supply and Demand Update (New York: UNICEF)

31. Falcaro M, Castañon A, and Ndlela B, et al (2021) The effects of the national HPV vaccination programme in England, UK, on cervical cancer and grade 3 cervical intraepithelial neoplasia incidence: a register-based observational study Lancet 398(10316) 2084–2092 https://doi.org/10.1016/S0140-6736(21)02178-4 PMID: 34741816

32. Simms KT, Hanley SJB, and Smith MA, et al (2020) Impact of HPV vaccine hesitancy on cervical cancer in Japan: a modelling study Lancet Public Health 5(4) e223–e234 https://doi.org/10.1016/S2468-2667(20)30010-4 PMID: 32057317

33. Ministry of Health, Labour and Welfare of Japan (2023) HPV Vaccine Adverse Event Reports in the National Committee on Vaccine Safety (Tokyo: Ministry of Health, Labour and Welfare of Japan) [https://www.mhlw.go.jp/stf/shingi/shingi-kousei_284075.html] Date accessed: 20/02/23

34. Gallagher KE, Howard N, and Kabakama S, et al (2017) Lessons learnt from human papillomavirus (HPV) vaccination in 45 low- and middle-income countries PLoS One 12(6) e0177773 https://doi.org/10.1371/journal.pone.0177773 PMID: 28575074 PMCID: 5456063

35. Spayne J and Hesketh T (2021) Estimate of global human papillomavirus vaccination coverage: analysis of country-level indicators BMJ Open 11(9) e052016 https://doi.org/10.1136/bmjopen-2021-052016 PMID: 34475188 PMCID: 8413939

36. Dorji T, Nopsopon T, and Tamang ST, et al (2021) Human papillomavirus vaccination uptake in low-and middle-income countries: a meta-analysis EClinicalMedicine 34 100836 https://doi.org/10.1016/j.eclinm.2021.100836 PMID: 33997733 PMCID: 8102703

37. World Cancer Research Fund International (2024) Cervical Cancer Statistics (London: World Cancer Research Fund International) [https://www.wcrf.org/cancer-trends/cervical-cancer-statistics/] Date accessed: 20/02/24

38. Wilson R (2021) HPV vaccine acceptance in West Africa: a systematic literature review Vaccine 39(37) 5277–5284 https://doi.org/10.1016/j.vaccine.2021.06.074 PMID: 34366143

39. Wijayanti KE, Schütze H, and MacPhail C, et al (2021) Parents’ knowledge, beliefs, acceptance and uptake of the HPV vaccine in members of The Association of Southeast Asian Nations (ASEAN): a systematic review of quantitative and qualitative studies Vaccine 39(17) 2335–2343 https://doi.org/10.1016/j.vaccine.2021.03.049 PMID: 33781598

40. Silva TM, Nogueira de Sá AC, and Beinner MA, et al (2022) Impact of the COVID-19 pandemic on human papillomavirus vaccination in Brazil Int J Public Health 67 1604224 https://doi.org/10.3389/ijph.2022.1604224 PMID: 35431762 PMCID: 9008128

41. Rai Y, Webster H, and Tessier E, et al (2020) Human papillomavirus (HPV) vaccination coverage in adolescent females and males in England: academic year 2019 to 2020 Health Prot Rep 14(19) 1–5

42. Daniels V, Saxena K, and Roberts C, et al (2021) Impact of reduced human papillomavirus vaccination coverage rates due to covid-19 in the United States: a model based analysis Vaccine 39(20) 2731–2735 https://doi.org/10.1016/j.vaccine.2021.04.003 PMID: 33875269 PMCID: 8023201

43. WHO Immunization Data Portal [Internet] (Geneva: World Health Organization) [https://immunizationdata.who.int/] Date accessed: 07/03/24

44. Lavie M, Lavie I, and Laskov I, et al (2023) Impact of Covid-19 pandemic on human papillomavirus vaccine uptake in Israel J Low Genit Tract Dis 27(2) 168–172 https://doi.org/10.1097/LGT.0000000000000729 PMID: 36815631 PMCID: 10026726

45. Smith DL and Perkins RB (2022) Low rates of HPV vaccination and cervical cancer screening: challenges and opportunities in the context of the COVID-19 pandemic Prev Med 159 107070 https://doi.org/10.1016/j.ypmed.2022.107070 PMID: 35461955 PMCID: 9022394

46. Considerations for Integrating COVID-19 Vaccination with Other Childhood and Adolescent Immunizations: Interim Guidance (Geneva: World Health Organization) [https://www.who.int/publications-detail-redirect/9789240064454] Date accessed: 02/03/24

47. Rosettie KL, Joffe JN, and Sparks GW, et al (2021) Cost-effectiveness of HPV vaccination in 195 countries: a meta-regression analysis PLoS One 16(12) e0260808 https://doi.org/10.1371/journal.pone.0260808 PMID: 34928971 PMCID: 8687557

48. Tran PT, Riaz M, and Chen Z, et al (2022) An umbrella review of the cost effectiveness of human papillomavirus vaccines Clin Drug Investig 42(5) 377–390 https://doi.org/10.1007/s40261-022-01155-5 PMID: 35488964

49. Datta S, Pink J, and Medley GF, et al (2019) Assessing the cost-effectiveness of HPV vaccination strategies for adolescent girls and boys in the UK BMC Infect Dis 19(1) 552 https://doi.org/10.1186/s12879-019-4108-y PMID: 31234784 PMCID: 6591963

50. Prem K, Choi YH, and Bénard É, et al (2021) Global impact and cost-effectiveness of one-dose versus two-dose human papillomavirus vaccination schedules: a comparative modelling analysis MedRxiv

51. Jiang Y, Ni W, and Wu J (2019) Cost-effectiveness and value-based prices of the 9-valent human papillomavirus vaccine for the prevention of cervical cancer in China: an economic modelling analysis BMJ Open 9(11) e031186 https://doi.org/10.1136/bmjopen-2019-031186 PMID: 31767588 PMCID: 6886925

52. Van Minh H, My NTT, and Jit M (2017) Cervical cancer treatment costs and cost-effectiveness analysis of human papillomavirus vaccination in Vietnam: a PRIME modeling study BMC Health Serv Res 17(1) 353 https://doi.org/10.1186/s12913-017-2297-x PMID: 28506297 PMCID: 5433243

53. The Lancet Oncology (2022) HPV vaccination in south Asia: new progress, old challenges Lancet Oncol 23(10) 1233 https://doi.org/10.1016/S1470-2045(22)00567-8 PMID: 36174615

54. Burki TK (2023) India rolls out HPV vaccination Lancet Oncol 24(4) e147 https://doi.org/10.1016/S1470-2045(23)00118-3 PMID: 36934729

55. World Health Organization (2020) Human Papillomavirus (HPV) Vaccines: WHO Position Paper (Geneva: World Health Organization)

56. Centers for Disease Control and Prevention (2023) HPV Vaccination for People with HIV

57. BHIVA guidelines on the use of vaccines in HIV-positive adults 2015 [Internet] [https://www.bhiva.org/vaccination-guidelines] Date accessed: 07/03/24

58. Losada C, Samaha H, and Scherer EM, et al (2023) Efficacy and durability of immune response after receipt of HPV vaccines in people living with HIV Vaccines 11(6) 1067 https://doi.org/10.3390/vaccines11061067 PMID: 37376456 PMCID: 10301114

59. Staadegaard L, Rönn MM, and Soni N, et al (2022) Immunogenicity, safety, and efficacy of the HPV vaccines among people living with HIV: a systematic review and meta-analysis eClinicalMedicine 52 101585 https://doi.org/10.1016/j.eclinm.2022.101585 PMID: 35936024 PMCID: 9350866

60. Zizza A, Banchelli F, and Guido M, et al (2021) Efficacy and safety of human papillomavirus vaccination in HIV-infected patients: a systematic review and meta-analysis Sci Rep 11(1) 4954 https://doi.org/10.1038/s41598-021-83727-7 PMID: 33654181 PMCID: 7925667

61. Human papillomavirus [Internet] (2012) [https://www.ecdc.europa.eu/en/human-papillomavirus] Date accessed: 07/03/24

62. Johnson N (2020) Comprehensive sexual health assessments for adolescents Paediatr Child Health 25(8) 551 https://doi.org/10.1093/pch/pxaa122 PMID: 33365110 PMCID: 7739542

63. Shieh Y, Eklund M, and Sawaya GF, et al (2016) Population-based screening for cancer: hope and hype Nat Rev Clin Oncol 13(9) 550–565 https://doi.org/10.1038/nrclinonc.2016.50 PMID: 27071351 PMCID: 6585415

64. Safaeian M, Solomon D, and Castle PE (2007) Cervical cancer prevention – cervical screening: science in evolution Obstet Gynecol Clin North Am 34(4) 739–760, ix https://doi.org/10.1016/j.ogc.2007.09.004 PMID: 18061867 PMCID: 2762353

65. Mayrand MH, Duarte-Franco E, and Rodrigues I, et al (2007) Human papillomavirus DNA versus Papanicolaou screening tests for cervical cancer N Engl J Med 357(16) 1579–1588 https://doi.org/10.1056/NEJMoa071430 PMID: 17942871

66. Mustafa RA, Santesso N, and Khatib R, et al (2016) Systematic reviews and meta-analyses of the accuracy of HPV tests, visual inspection with acetic acid, cytology, and colposcopy Int J Gynaecol Obstet 132(3) 259–265 https://doi.org/10.1016/j.ijgo.2015.07.024 PMID: 26851054

67. Catarino R, Petignat P, and Dongui G, et al (2015) Cervical cancer screening in developing countries at a crossroad: emerging technologies and policy choices World J Clin Oncol 6(6) 281–290 https://doi.org/10.5306/wjco.v6.i6.281 PMID: 26677441 PMCID: 4675913

68. Sankaranarayanan R, Budukh AM, and Rajkumar R (2001) Effective screening programmes for cervical cancer in low- and middle-income developing countries Bull World Health Organ 79(10) 954–962 PMID: 11693978 PMCID: 2566667

69. Bedell SL, Goldstein LS, and Goldstein AR, et al (2020) Cervical cancer screening: past, present, and future Sex Med Rev 8(1) 28–37 https://doi.org/10.1016/j.sxmr.2019.09.005

70. Srivastava AN, Misra JS, and Srivastava S, et al (2018) Cervical cancer screening in rural India: status & current concepts Indian J Med Res 148(6) 687–696 https://doi.org/10.4103/ijmr.IJMR_5_17

71. Silkensen SL, Schiffman M, and Sahasrabuddhe V, et al (2018) Is it time to move beyond visual inspection with acetic acid for cervical cancer screening? Glob Health Sci Pract 6(2) 242–246 https://doi.org/10.9745/GHSP-D-18-00206 PMID: 29959268 PMCID: 6024629

72. Vedantham H, Silver MI, and Kalpana B, et al (2010) Determinants of VIA (Visual inspection of the cervix after acetic acid application) positivity in cervical cancer screening of women in a Peri-urban area in Andhra Pradesh, India Cancer Epidemiol Biomarkers Prev 19(5) 1373–1380 https://doi.org/10.1158/1055-9965.EPI-09-1282 PMID: 20447927 PMCID: 2913449

73. Bosch FX, Lorincz A, and Muñoz N, et al (2002) The causal relation between human papillomavirus and cervical cancer J Clin Pathol 55(4) 244–265 https://doi.org/10.1136/jcp.55.4.244 PMID: 11919208 PMCID: 1769629

74. World Health Organization (2021) WHO Guideline for Screening and Treatment of Cervical Pre-Cancer Lesions for Cervical Cancer Prevention 2nd edn (Geneva: World Health Organization)

75. Hillyar CR, Kanabar SS, and Pufal KR, et al (2022) A systematic review and meta-analysis of the diagnostic effectiveness of human papillomavirus methylation biomarkers for detection of cervical cancer Epigenomics 14(18) 1055–1072 https://doi.org/10.2217/epi-2022-0160 PMID: 36169190

76. Ronco G, Dillner J, and Elfström KM, et al (2014) Efficacy of HPV-based screening for prevention of invasive cervical cancer: follow-up of four European randomised controlled trials Lancet 383(9916) 524–532 https://doi.org/10.1016/S0140-6736(13)62218-7

77. Sankaranarayanan R, Nene BM, and Shastri SS, et al (2009) HPV screening for cervical cancer in rural India N Engl J Med 360(14) 1385–1394 https://doi.org/10.1056/NEJMoa0808516 PMID: 19339719

78. Wright TC, Stoler MH, and Behrens CM, et al (2015) Primary cervical cancer screening with human papillomavirus: end of study results from the ATHENA study using HPV as the first-line screening test Gynecol Oncol 136(2) 189–197 https://doi.org/10.1016/j.ygyno.2014.11.076 PMID: 25579108

79. Arbyn M, Ronco G, and Anttila A, et al (2012) Evidence regarding human papillomavirus testing in secondary prevention of cervical cancer Vaccine 30(Suppl 5) F88–F99 https://doi.org/10.1016/j.vaccine.2012.06.095 PMID: 23199969

80. Schiffman M, Kinney WK, and Cheung LC, et al (2018) Relative performance of HPV and cytology components of cotesting in cervical screening J Natl Cancer Inst 110(5) 501–508 https://doi.org/10.1093/jnci/djx225 PMCID: 6279277

81. Liang LA, Einzmann T, and Franzen A, et al (2021) Cervical cancer screening: comparison of conventional Pap Smear Test, liquid-based cytology, and human papillomavirus testing as stand-alone or cotesting strategies Cancer Epidemiol Biomarkers Prev 30(3) 474–484 https://doi.org/10.1158/1055-9965.EPI-20-1003

82. Gage JC, Schiffman M, and Katki HA, et al (2014) Reassurance against future risk of precancer and cancer conferred by a negative human papillomavirus test J Natl Cancer Inst 106(8) dju153 https://doi.org/10.1093/jnci/dju153 PMID: 25038467 PMCID: 4111283

83. Ratnam S, Coutlee F, and Fontaine D, et al (2011) Aptima HPV E6/E7 mRNA test is as sensitive as hybrid capture 2 assay but more specific at detecting cervical precancer and cancer J Clin Microbiol 49(2) 557–564 https://doi.org/10.1128/JCM.02147-10 PMCID: 3043526

84. Arbyn M, Simon M, and de Sanjosé S, et al (2022) Accuracy and effectiveness of HPV mRNA testing in cervical cancer screening: a systematic review and meta-analysis Lancet Oncol 23(7) 950–960 https://doi.org/10.1016/S1470-2045(22)00294-7 PMID: 35709810

85. Sørbye SW, Fismen S, and Gutteberg TJ, et al (2016) Primary cervical cancer screening with an HPV mRNA test: a prospective cohort study BMJ Open 6(8) e011981 https://doi.org/10.1136/bmjopen-2016-011981 PMID: 27515759 PMCID: 4985920

86. Maggino T, Sciarrone R, and Murer B, et al (2016) Screening women for cervical cancer carcinoma with a HPV mRNA test: first results from the Venice pilot program Br J Cancer 115(5) 525–532 https://doi.org/10.1038/bjc.2016.216 PMID: 27490801 PMCID: 4997543

87. Giorgi Rossi P, Ronco G, and Mancuso P, et al (2022) Performance of HPV E6/E7 mRNA assay as primary screening test: results from the NTCC2 trial Int J Cancer 151(7) 1047–1058 https://doi.org/10.1002/ijc.34120 PMID: 35579975

88. Zappacosta R, Gatta DM, and Marinucci P, et al (2015) Role of E6/E7 mRNA test in the diagnostic algorithm of HPV-positive patients showing ASCUS and LSIL: clinical and economic implications in a publicly financed healthcare system Expert Rev Mol Diagn 15(1) 137–150 https://doi.org/10.1586/14737159.2015.961915

89. Yeh PT, Kennedy CE, and de Vuyst H, et al (2019) Self-sampling for human papillomavirus (HPV) testing: a systematic review and meta-analysis BMJ Glob Health 4(3) e001351 https://doi.org/10.1136/bmjgh-2018-001351 PMID: 31179035 PMCID: 6529022

90. Regional Committee for Europe, 72nd session (2022) Seventy-Second Regional Committee for Europe: Tel Aviv, 12–14 September 2022: Roadmap to Accelerate the Elimination of Cervical Cancer as a Public Health Problem in the WHO European Region 2022–2030 (Geneva: World Health Organization, Regional Office for Europe)

91. Bais AG, van Kemenade FJ, and Berkhof J, et al (2007) Human papillomavirus testing on self-sampled cervicovaginal brushes: an effective alternative to protect nonresponders in cervical screening programs Int J Cancer 120(7) 1505–1510 https://doi.org/10.1002/ijc.22484 PMID: 17205514

92. Wong EL, Cheung AW, and Wong AY, et al (2020) Acceptability and feasibility of HPV self-sampling as an alternative primary cervical cancer screening in under-screened population groups: a cross-sectional study Int J Environ Res Public Health 17(17) 6245 https://doi.org/10.3390/ijerph17176245 PMID: 32867315 PMCID: 7503998

93. Arbyn M, Verdoodt F, and Snijders PJ, et al (2014) Accuracy of human papillomavirus testing on self-collected versus clinician-collected samples: a meta-analysis Lancet Oncol 15(2) 172–183 https://doi.org/10.1016/S1470-2045(13)70570-9 PMID: 24433684

94. Gupta S, Palmer C, and Bik EM, et al (2018) Self-sampling for human papillomavirus testing: increased cervical cancer screening participation and incorporation in International Screening Programs Front Public Health 6 77 https://doi.org/10.3389/fpubh.2018.00077 PMID: 29686981 PMCID: 5900042

95. Lazcano-Ponce E, Lorincz AT, and Cruz-Valdez A, et al (2011) Self-collection of vaginal specimens for human papillomavirus testing in cervical cancer prevention (MARCH): a community-based randomised controlled trial Lancet 378(9806) 1868–1873 https://doi.org/10.1016/S0140-6736(11)61522-5 PMID: 22051739

96. Wang W, Arcà E, and Sinha A, et al (2022) Cervical cancer screening guidelines and screening practices in 11 countries: a systematic literature review Prev Med Rep 28 101813 https://doi.org/10.1016/j.pmedr.2022.101813 PMID: 35637896 PMCID: 9142642

97. Canfell K, Kim JJ, and Brisson M, et al (2020) Mortality impact of achieving WHO cervical cancer elimination targets: a comparative modelling analysis in 78 low-income and lower-middle-income countries Lancet 395(10224) 591–603 https://doi.org/10.1016/S0140-6736(20)30157-4 PMID: 32007142 PMCID: 7043006

98. Brisson M, Kim JJ, and Canfell K, et al (2020) Impact of HPV vaccination and cervical screening on cervical cancer elimination: a comparative modelling analysis in 78 low-income and lower-middle-income countries Lancet 395(10224) 575–590 https://doi.org/10.1016/S0140-6736(20)30068-4 PMID: 32007141 PMCID: 7043009

99. Canadian Partnership Against Cancer (2024) Action Plan for the Elimination of Cervical Cancer in Canada, 2020-2030 [https://www.partnershipagainstcancer.ca/topics/elimination-cervical-cancer-action-plan/] Date accessed: 06/02/24

100. Hall MT, Simms KT, and Lew JB, et al (2019) The projected timeframe until cervical cancer elimination in Australia: a modelling study Lancet Public Health 4(1) e19–e27 https://doi.org/10.1016/S2468-2667(18)30183-X

101. Burger EA, Smith MA, and Killen J, et al (2020) Projected time to elimination of cervical cancer in the USA: a comparative modelling study Lancet Public Health 5(4) e213–e222 https://doi.org/10.1016/S2468-2667(20)30006-2 PMID: 32057315 PMCID: 8715100

102. US Preventive Services Task Force, Curry SJ, and Krist AH, et al (2018) Screening for cervical cancer: US preventive services task force recommendation statement JAMA 320(7) 674–686 https://doi.org/10.1001/jama.2018.10897 PMID: 30140884

103. American College of Obstetricians and Gynecologists (2021) Updated Cervical Cancer Screening Guidelines. Practice Advisory (Washington: American College of Obstetricians and Gynecologists)

104. American Cancer Society (2021) The American Cancer Society Guidelines for the Prevention and Early Detection of Cervical Cancer (Atlanta: American Cancer Society)

105. von Karsa L, Arbyn M, and De Vuyst H, et al (2015) European guidelines for quality assurance in cervical cancer screening. Summary of the supplements on HPV screening and vaccination Papillomavirus Res 1 22–31 https://doi.org/10.1016/j.pvr.2015.06.006

106. Australian Institute of Health and Welfare (2021) Cancer in Australia 2021. Cancer Series no. 133. Cat. no. CAN 144 (Canberra: Australian Institute of Health and Welfare)

107. Public Health England (2021) NHS Cervical Screening (CSP) Programme: Detailed Information (London: Public Health England)

108. IARC Working Group on the Evaluation of Cancer-Preventive Interventions (2022) IARC Handbooks of Cancer Prevention, Volume 18: Cervical Cancer Screening (Lyon: International Agency for Research on Cancer)

109. Ministry of Health and Family Welfare, Government of India (2016) Operational Framework – Management of Common Cancers (New Delhi: Ministry of Health and Family Welfare, Government of India)

110. Campos NG, Tsu V, and Jeronimo J, et al (2015) When and how often to screen for cervical cancer in three low- and middle-income countries: a cost-effectiveness analysis Papillomavirus Res 1 38–58 https://doi.org/10.1016/j.pvr.2015.05.003

111. Andrés-Gamboa O, Chicaíza L, and García-Molina M, et al (2008) Cost-effectiveness of conventional cytology and HPV DNA testing for cervical cancer screening in Colombia Salud Publica Mex 50(4) 276–285 https://doi.org/10.1590/S0036-36342008000400005 PMID: 18670718

112. Campos NG, Maza M, and Alfaro K, et al (2019) The cost-effectiveness of implementing HPV testing for cervical cancer screening in El Salvador Int J Gynaecol Obstet 145(1) 40–46 https://doi.org/10.1002/ijgo.12773 PMID: 30702142 PMCID: 6988124

113. Termrungruanglert W, Khemapech N, and Tantitamit T, et al (2019) Cost effectiveness analysis of HPV primary screening and dual stain cytology triage compared with cervical cytology J Gynecol Oncol 30(2) e17 https://doi.org/10.3802/jgo.2019.30.e17 PMID: 30740950 PMCID: 6393632

114. Cromwell I, Smith LW, and van der Hoek K, et al (2021) Cost-effectiveness analysis of primary human papillomavirus testing in cervical cancer screening: results from the HPV FOCAL trial Cancer Med 10(9) 2996–3003 https://doi.org/10.1002/cam4.3864 PMID: 33811457 PMCID: 8085916

115. Termrungruanglert W, Khemapech N, and Tantitamit T, et al (2017) Cost-effectiveness analysis study of HPV testing as a primary cervical cancer screening in Thailand Gynecol Oncol Rep 22 58–63 https://doi.org/10.1016/j.gore.2017.09.007 PMID: 29034308 PMCID: 5633754

116. Jansen E, Naber SK, and Aitken CA, et al (2021) Cost-effectiveness of HPV-based cervical screening based on first year results in the Netherlands: a modelling study BJOG 128(3) 573–582 https://doi.org/10.1111/1471-0528.16400 PMCID: 7818441

117. Bains I, Choi YH, and Soldan K, et al (2019) Clinical impact and cost-effectiveness of primary cytology versus human papillomavirus testing for cervical cancer screening in England Int J Gynecol Cancer ijgc-2018-000161

118. Vale DB, Silva MT, and Discacciati MG, et al (2021) Is the HPV-test more cost-effective than cytology in cervical cancer screening? An economic analysis from a middle-income country PLoS One 16(5) e0251688 https://doi.org/10.1371/journal.pone.0251688 PMID: 33989331 PMCID: 8121350

119. Lemp JM, De Neve JW, and Bussmann H, et al (2020) Lifetime prevalence of cervical cancer screening in 55 low- and middle-income countries JAMA 324(15) 1532–1542 https://doi.org/10.1001/jama.2020.16244 PMID: 33079153 PMCID: 7576410

120. National Cancer Institute: Surveillance, Epidemiology and End Results Program (2024) Cancer Stat Facts: Cervical Cancer [https://seer.cancer.gov/statfacts/html/cervix.html] Date accessed: 23/02/24

121. Dessalegn Mekonnen B (2020) Cervical cancer screening uptake and associated factors among HIV-positive women in Ethiopia: a systematic review and meta-analysis Adv Prev Med 2020 7071925 https://doi.org/10.1155/2020/7071925 PMID: 32879739 PMCID: 7448202

122. Asare M, Abah E, and Obiri-Yeboah D, et al (2022) HPV self-sampling for cervical cancer screening among women living with HIV in low- and middle-income countries: what do we know and what can be done? Healthcare (Basel) 10(7) 1270 https://doi.org/10.3390/healthcare10071270 PMID: 35885798 PMCID: 9317927

123. Wilyman J (2013) HPV vaccination programs have not been shown to be cost-effective in countries with comprehensive Pap screening and surgery Infect Agent Cancer 8(1) 21 https://doi.org/10.1186/1750-9378-8-21 PMID: 23758803 PMCID: 3698073

124. Burger EA, Sy S, and Kim JJ (2020) Impact of COVID-19-related care disruptions on cervical cancer screening in the United States, annual society of medical decision making meeting (Virtual)

125. Wentzensen N, Clarke MA, and Perkins RB (2021) Impact of COVID-19 on cervical cancer screening: challenges and opportunities to improving resilience and reduce disparities Prev Med 151 106596 https://doi.org/10.1016/j.ypmed.2021.106596 PMID: 34217415 PMCID: 8241689

126. Lacey CJN (2019) HPV vaccination in HIV infection Papillomavirus Res 8 100174 https://doi.org/10.1016/j.pvr.2019.100174 PMID: 31252073 PMCID: 6603434

127. Updated cervical cancer screening guidelines [Internet] [https://www.acog.org/clinical/clinical-guidance/practice-advisory/articles/2021/04/updated-cervical-cancer-screening-guidelines] Date accessed: 08/03/24

128. HPV Vaccination Recommendations [Internet] (Atlanta: Centers for Disease Control and Prevention) [https://www.cdc.gov/vaccines/vpd/hpv/hcp/recommendations.html] Date accessed: 08/03/24

129. Cervical cancer-health professional version [Internet] [https://www.cancer.gov/types/cervical/hp] Date accessed: 08/03/24

130. Cervical Cancer [Internet] (2023) (Atlanta: Centers for Disease Control and Prevention) [https://www.cdc.gov/cancer/cervical/index.htm] Date accessed: 08/03/24