Literature DB >> 25987893

Global availability of data on HPV genotype-distribution in cervical, vulvar and vaginal disease and genotype-specific prevalence and incidence of HPV infection in females.

Monika Wagner¹, Liga Bennetts¹, Harshila Patel¹, Sharon Welner¹, Silvia de Sanjose², Thomas W Weiss³.

Abstract

BACKGROUND: Country-level HPV genotyping data may be sought by decision-makers to gauge the genotype-specific burden of HPV-related diseases in their jurisdiction and assess the potential impact of HPV vaccines. We investigated, by country, the availability of published literature on HPV genotypes in cervical, vaginal and vulvar cancers and intraepithelial neoplasms (CINs, VaINs and VINs) and on prevalence and incidence of genital HPV infections among women without clinically manifest disease.
FINDINGS: Primary sources of publications were the PubMed/Medline and EMBASE databases. Original studies or meta-analyses published from 2000, covering genotypes 16 and 18 and at least one of genotypes 31/33/45/52/58, were included. Key exclusion criteria were language not English, cervical lesions not histologically confirmed (cytology only), special populations (e.g., immunocompromised) and, for cervical studies, small population (<50). A total of 727 studies reporting HPV genotype-specific data were identified: 366 for cervical cancers and CINs, 43 for vulvar or vaginal cancers and VINs/VaINs, and 395 and 21 for infection prevalence and incidence, respectively, in general female population samples. A large proportion of studies originated from a small set of countries. Cervical cancer/CIN typing data was scarce for several regions with the highest cervical cancer burden, including Eastern, Middle and Western Africa, Central America, South-East Asia, South Asia, and Eastern Europe. Data for vulvar/vaginal disease was limited outside of Europe and North America.
CONCLUSIONS: Although a large body of published HPV genotype-specific data is currently available, data gaps exist for genotype-specific infection incidence and several world regions with the highest cervical cancer burden.

Entities: Disease Species

Keywords: Cervical cancer; Cervical lesions; Epidemiology; Genital infection; Genotype; Geographic region; HPV

Year: 2015 PMID： 25987893 PMCID： PMC4435914 DOI： 10.1186/s13027-015-0008-y

Source DB: PubMed Journal: Infect Agent Cancer ISSN： 1750-9378 Impact factor: 2.965

Findings

Background

Human papillomaviruses (HPV) belong to the most prevalent sexually transmitted infections worldwide [1], with genotypes 16, 18, 52, 58, 31, 51, and 56 among the most frequently detected in women with normal cervical cytology [2-4]. Globally, approximately 70% of cervical cancers are attributable to genotypes 16 and/or 18, targeted by first-generation HPV vaccines (Gardasil® and Cervarix®), and 90% to 16, 18, 31, 33, 45, 52 or 58, targeted by the 9-valent vaccine (Gardasil® 9) [5]. These genotypes also contribute to the majority of HPV-related vulvar [6-8] and vaginal cancers [7,8]. At the country level, decision-makers are likely to seek data on the local genotype-specific burden of HPV-related diseases for baseline information against which the impact of HPV vaccination may be assessed. Focusing on the 7 high-risk (HR) genotypes covered by the 9-valent vaccine (16, 18, 31, 33, 45, 52 and 58), we investigated, by country, the availability of published literature on HPV genotypes in cervical, vaginal and vulvar cancers and intraepithelial neoplasms (CINs, VaINs and VINs) and on prevalence and incidence of genital HPV infections among women without clinically manifest disease.

Methods

The primary sources of data were the National Library of Medicine’s PubMed/Medline and EMBASE databases. Bibliographies were screened to identify additional sources of information. The literature searches covered literature published from 2000 to May 2014; key search terms included epidemiology, human papillomavirus, genotyping, cervix, vagina, vulva, and intraepithelial lesions, cancer, in various combinations. Publications meeting these criteria were included: original study or meta-analysis reporting (1) HPV genotype distribution in histologically confirmed CINs, VINs or VaINs or cervical, vulvar or vaginal cancers, or (2) genotype-specific genital HPV prevalence or incidence in women without clinically manifest disease (i.e., general populations, screening populations, women with normal cervical cytology, university students, convenience samples). Studies were included if they reported on genotypes 16 and 18, and at least one of the additional HR genotypes covered by the 9-valent vaccine (31, 33, 45, 52, 58). Key exclusion criteria were: publication not in English, small study (n < 50) for prevalence and cervical lesions/cancer studies, special populations (e.g., age <13 or >45 years, pregnant women, sex workers, HIV-infected, immunocompromised), duplicate publication. For each study, data was systematically extracted for country, world region, type and date of study, type of population, age, lesion type, sample type and collection method, HPV assay, number of subjects with valid HPV test results, and HPV genotyping results. Study selection and data extraction were performed by three investigators. One of these investigators performed quality control for accuracy and conformity with selection criteria. Availability of HPV genotyping data was compiled by world region and country [9]. For HPV prevalence studies (in women without clinically manifest disease), in addition to all studies with at least 50 subjects, availability of studies with at least 500 subjects was assessed, as larger studies provide more precise estimates of the prevalence of rare HPV infections. Maps were created using StatPlanet Plus (Version 3.21) visualization software (StatSilk, Melbourne, Australia; http://www.statsilk.com/software/statplanet).

Results

The literature searches yielded 11,474 records, of which 1,765 were screened in full-text and 727 included (Figure 1, Additional file 1). For full-text publications, the most common reason for exclusion was absence of HPV-genotype specific data.

Figure 1

PRISMA diagram of study selection.

PRISMA diagram of study selection. Over one third (n = 256) of all publications originated from just six countries (China, Italy, United States, Brazil, South Korea and Japan). A large body of data (366 publications, Table 1) was available for HPV genotype distribution in at least 50 cervical cancers or CINs, with ten or more studies identified for ten countries (Brazil, China, India, Italy, Japan, Spain, South Korea, Thailand, Taiwan, the United States) (Figure 2). Conversely, no or few (0–2) such studies were identified for Central and Western Asia, most of Africa, particularly Central Africa, and several countries in Europe (mainly Eastern Europe), in Latin America and the Caribbean, and in South and South-East Asia.

Table 1

Distribution of included publications by world region and type of data*

Category of HPV type-specific data	Africa	Asia/Pacific	Europe	Latin America and the Caribbean	Northern America	Multiple world regions	Globally
Any	62	236	236	104	74	19	727
Genital prevalence	38	123	126	65	39	7	395
Genital incidence	4	3	5	3	6	0	21
Cervical lesions or cancers	30	142	107	52	25	11	366
Vulvar or vaginal lesions or cancers	1	4	23	2	9	4	43

Note: Sums of individual columns or rows exceed the total because several publications reported on multiple world regions or types of data.

*Including meta-analyses.

Figure 2

Number of publications, by country, reporting HPV genotype distribution in at least 50 cases of histologically confirmed cervical lesions (CINs) or cervical cancers. Original studies published between January 2000 and May 2014; reporting prevalence data for HPV genotypes 16 and 18 and at least one of genotypes 31, 33, 45, 52 or 58; ≥50 subjects with valid HPV test results; full-text English language publication. CIN: cervical intraepithelial lesion.

Distribution of included publications by world region and type of data* Note: Sums of individual columns or rows exceed the total because several publications reported on multiple world regions or types of data. *Including meta-analyses. Number of publications, by country, reporting HPV genotype distribution in at least 50 cases of histologically confirmed cervical lesions (CINs) or cervical cancers. Original studies published between January 2000 and May 2014; reporting prevalence data for HPV genotypes 16 and 18 and at least one of genotypes 31, 33, 45, 52 or 58; ≥50 subjects with valid HPV test results; full-text English language publication. CIN: cervical intraepithelial lesion. For cervical cancer specifically, 208 publications from 73 countries were identified that reported HPV genotype distribution in at least 50 cases (Figure 3), and four countries (China, Japan, South Korea and the United States) had ten or more such publications. Among the 10 most populous countries, substantial cervical cancer data (≥8 publications) was available for China, the United States, Japan, India, and Brazil, but very limited data (0–2 publications) for Indonesia, Pakistan, Nigeria, Bangladesh and Russia (Figure 3).

Figure 3

Number of publications, by country, reporting HPV genotype distribution in at least 50 cases of histologically confirmed cervical cancers. Original studies published between January 2000 and May 2014; reporting prevalence data for HPV genotypes 16 and 18 and at least one of genotypes 31, 33, 45, 52 or 58; ≥50 subjects with valid HPV test results; full-text English language publication. Forty-three publications were retrieved for vulvar and vaginal cancers and VINs/VaINs. More than half (n = 23) of these studies originated from Europe, with very few available from Africa, Asia/Pacific and Latin America and the Caribbean (Table 1). Among four studies reporting vulvar and vaginal data across world regions, two were meta-analyses [7,8], pooling already existing data, and two were cross-sectional studies that generated new data but did not report country-specific findings [6,10]. A total of 395 publications reported HPV genotype-specific genital prevalence among women without clinically manifest disease. (Most of these referred to cervical infections and a small number to vaginal infections.) For ten countries, including Brazil and Turkey, ten or more such publications were available (Figure 4). However, few publications (0–2) were identified for most countries in Africa (except for those in Eastern Africa as well as Nigeria, Senegal and South Africa), Western Asia, Central Asia, South Asia (except India and Iran), South-East Asia (except Thailand and Vietnam), and Eastern Europe.

Figure 4

Number of publications, by country, reporting HPV genotype-specific genital prevalence among at least 50 women without clinically manifest disease*. Original studies published between January 2000 and May 2014; reporting prevalence data for HPV genotypes 16 and 18 and at least one of genotypes 31, 33, 45, 52 or 58; ≥50 subjects with valid HPV DNA test results; full-text English language publication. *General populations, screening populations, women with normal cervical cytology, or convenience samples. A total of 238 larger prevalence studies, reporting genotype-specific prevalence in at least 500 subjects without clinically manifest disease, were identified for 68 countries, which, however, excluded most countries in Africa (Figure 5), a finding similar to an earlier report on Sub-Saharan Africa [11]. Further, no such large studies were identified for Central Asia and some countries in Latin America and the Caribbean, Europe, and Asia (Figure 5).

Figure 5

Number of publications, by country, reporting HPV genotype-specific genital prevalence among at least 500 women without clinically manifest disease*. Original studies published between January 2000 and May 2014; reporting prevalence data for HPV genotypes 16 and 18 and at least one of genotypes 31, 33, 45, 52 or 58; ≥500 subjects with valid HPV DNA test results; full-text English language publication. *General populations, screening populations, women with normal cervical cytology, or convenience samples.

Discussion and conclusions

Although region- or country-specific differences with respect to individual HPV genotypes exist, a solid body of research indicates that in every world region, taken together, genotypes 16/18/31/33/45/52/58 are responsible for approximately 90% of cervical cancers [12,13]. Nevertheless, decision-makers may seek local data to confirm that certain, maybe less common, vaccine-targeted genotypes circulate in their population, to assess the potential public health impacts of different HPV vaccination options, or to monitor the outcomes of vaccination programs in their jurisdiction. Addressing this need, this study has uncovered a large body of published type-specific data but has also identified significant gaps for several world regions, including those with the highest age-standardized incidence rates of cervical cancer (ASR). Sub-regions that have a notable scarcity of cervical cancer/CIN genotyping data relative to their cervical cancer burden, as estimated by GLOBOCAN 2012 [4], include Eastern Africa (ASR per 100,000 women-years = 42.7), Middle Africa (30.6), Western Africa (29.3), Central America (23.5), South-Eastern Asia (16.3), South-Central Asia including India (19.3), and Central and Eastern Europe (16.3). An additional three sub-regions (Southern Africa, the Caribbean, and South America) have high cervical cancer ASRs (>20) but only a moderate quantity of typing data. There was also scarcity of data for vulvar/vaginal disease, outside of Europe and North America. Globally, cervical cancer ASRs are higher in less developed (15.7) compared to more developed regions (9.9) [4]. Clearly, most regions with the largest discrepancy between cervical cancer burden and availability of genotyping data belong to the less developed subset, where lack of screening and treatment of CIN are major drivers of cervical cancer incidence, and limited research infrastructure and funding are barriers for conducting HPV genotyping studies [14]. An additional finding is that, although there may be ample cervical lesion typing and prevalence data in many jurisdictions, genotype-specific incidence data is limited to few available prospective studies. Data, such as age-specific rates of HPV acquisition, are needed for informing dynamic models to obtain more accurate predictions of the population health impact of vaccination. This study has both strengths and limitations. We did not include anal disease in our study, as anal cancer affects both genders and we intended to focus on females. However, as the burden of anal cancer is reported to be rising in Western countries [15], genotype-specific data on this HPV-related disease may become more important for decision-makers. Consistent with our objective of gauging the quantity of type-specific HPV data available, we excluded studies that reported non-type-specific data or types 16 or 18 only, which represent a large volume of published research in this field (see Figure 1). Also, inclusion was limited to published, English-language, peer-reviewed studies; thus, studies written in local languages or published in report format, for example on government websites, were not included. Limiting inclusion to peer-reviewed publications guarantees a minimum level of quality in the methods and reporting of the studies selected for our analysis. Inclusion of data from histologically-confirmed cervical lesions only (rather than cytologically defined lesions) is also consistent with our focus on higher-quality studies. In conclusion, although a large body of HPV genotype-specific data on distribution in CINs and cervical cancers and female genital prevalence is available, significant data gaps exist for multiple world regions as well as for type-specific incidence. Supplementary Material. Full list of 727 references by world region.

12 in total

Review 1. A systematic review of the prevalence of mucosal and cutaneous human papillomavirus types.

Authors: Davit Bzhalava; Peng Guan; Silvia Franceschi; Joakim Dillner; Gary Clifford
Journal: Virology Date: 2013-08-05 Impact factor: 3.616

Review 2. The increasing incidence of anal cancer: can it be explained by trends in risk groups?

Authors: R P van der Zee; O Richel; H J C de Vries; J M Prins
Journal: Neth J Med Date: 2013-10 Impact factor: 1.422

Review 3. The burden of human papillomavirus infections and related diseases in sub-saharan Africa.

Authors: Hugo De Vuyst; Laia Alemany; Charles Lacey; Carla J Chibwesha; Vikrant Sahasrabuddhe; Cecily Banura; Lynette Denny; Groesbeck P Parham
Journal: Vaccine Date: 2013-12-29 Impact factor: 3.641

4. Human papillomavirus genotype attribution in invasive cervical cancer: a retrospective cross-sectional worldwide study.

Authors: Silvia de Sanjose; Wim Gv Quint; Laia Alemany; Daan T Geraets; Jo Ellen Klaustermeier; Belen Lloveras; Sara Tous; Ana Felix; Luis Eduardo Bravo; Hai-Rim Shin; Carlos S Vallejos; Patricia Alonso de Ruiz; Marcus Aurelho Lima; Nuria Guimera; Omar Clavero; Maria Alejo; Antonio Llombart-Bosch; Chou Cheng-Yang; Silvio Alejandro Tatti; Elena Kasamatsu; Ermina Iljazovic; Michael Odida; Rodrigo Prado; Muhieddine Seoud; Magdalena Grce; Alp Usubutun; Asha Jain; Gustavo Adolfo Hernandez Suarez; Luis Estuardo Lombardi; Aekunbiola Banjo; Clara Menéndez; Efrén Javier Domingo; Julio Velasco; Ashrafun Nessa; Saibua C Bunnag Chichareon; You Lin Qiao; Enrique Lerma; Suzanne M Garland; Toshiyuki Sasagawa; Annabelle Ferrera; Doudja Hammouda; Luciano Mariani; Adela Pelayo; Ivo Steiner; Esther Oliva; Chris Jlm Meijer; Waleed Fahad Al-Jassar; Eugenia Cruz; Thomas C Wright; Ana Puras; Cecilia Ladines Llave; Maria Tzardi; Theodoros Agorastos; Victoria Garcia-Barriola; Christine Clavel; Jaume Ordi; Miguel Andújar; Xavier Castellsagué; Gloria I Sánchez; Andrzej Marcin Nowakowski; Jacob Bornstein; Nubia Muñoz; F Xavier Bosch
Journal: Lancet Oncol Date: 2010-10-15 Impact factor: 41.316

5. Cervical human papillomavirus prevalence in 5 continents: meta-analysis of 1 million women with normal cytological findings.

Authors: Laia Bruni; Mireia Diaz; Xavier Castellsagué; Elena Ferrer; F Xavier Bosch; Silvia de Sanjosé
Journal: J Infect Dis Date: 2010-11-10 Impact factor: 5.226

6. Human papillomavirus infections and vulvar disease development.

Authors: Suzanne M Garland; Ralph P Insinga; Heather L Sings; Richard M Haupt; Elmar A Joura
Journal: Cancer Epidemiol Biomarkers Prev Date: 2009-06 Impact factor: 4.254

7. Prevalence and type distribution of human papillomavirus in carcinoma and intraepithelial neoplasia of the vulva, vagina and anus: a meta-analysis.

Authors: Hugo De Vuyst; Gary M Clifford; Maria Claudia Nascimento; Margaret M Madeleine; Silvia Franceschi
Journal: Int J Cancer Date: 2009-04-01 Impact factor: 7.396

8. Potential impact of a 9-valent HPV vaccine in HPV-related cervical disease in 4 emerging countries (Brazil, Mexico, India and China).

Authors: Beatriz Serrano; Laia Alemany; Patricia Alonso de Ruiz; Sara Tous; Marcus Aurelho Lima; Laia Bruni; Asha Jain; Gary M Clifford; You Lin Qiao; Thomas Weiss; F Xavier Bosch; Silvia de Sanjosé
Journal: Cancer Epidemiol Date: 2014-10-08 Impact factor: 2.984

Review 9. Human papillomavirus type-distribution in vulvar and vaginal cancers and their associated precursors.

Authors: Jennifer S Smith; Danielle M Backes; Brooke E Hoots; Robert J Kurman; Jeanne M Pimenta
Journal: Obstet Gynecol Date: 2009-04 Impact factor: 7.661

10. Potential impact of a nine-valent vaccine in human papillomavirus related cervical disease.

Authors: Beatriz Serrano; Laia Alemany; Sara Tous; Laia Bruni; Gary M Clifford; Thomas Weiss; Francesc Xavier Bosch; Silvia de Sanjosé
Journal: Infect Agent Cancer Date: 2012-12-29 Impact factor: 2.965

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1. Analysis of clinical outcomes of patients with primary rare carcinoma of Bartholin gland: six case series report and review of the literature.

Authors: Kana Wang; Ying Zheng; Longxia Tong; Kaige Pei; Xiang He; Jiawen Zhang
Journal: Transl Cancer Res Date: 2022-06 Impact factor: 0.496

2. High prevalence of human papillomaviruses in Ghanaian pregnant women.

Authors: Marco H Schulze; Fabian M Völker; Raimond Lugert; Paul Cooper; Kai Hasenclever; Uwe Groß; Herbert Pfister; Steffi Silling
Journal: Med Microbiol Immunol Date: 2016-09-06 Impact factor: 3.402

3. Prevalence and genotype distribution of human papillomavirus among women with cervical lesions in Shenzhen city, China.

Authors: Qingfeng Mai; Xiaohan Yang; Huan Cheng; Genghang Wu; Zikun Wu
Journal: Hum Vaccin Immunother Date: 2020-09-22 Impact factor: 3.452

4. Incidence and mortality of cervical cancer in China, 2013.

Authors: Bingbing Song; Chao Ding; Wangyang Chen; Huixin Sun; Maoxiang Zhang; Wanqing Chen
Journal: Chin J Cancer Res Date: 2017-12 Impact factor: 5.087

5. Non-junctional Cx32 mediates anti-apoptotic and pro-tumor effects via epidermal growth factor receptor in human cervical cancer cells.

Authors: Yifan Zhao; Yongchang Lai; Hui Ge; Yunquan Guo; Xue Feng; Jia Song; Qin Wang; Lixia Fan; Yuexia Peng; Minghui Cao; Andrew L Harris; Xiyan Wang; Liang Tao
Journal: Cell Death Dis Date: 2017-05-11 Impact factor: 8.469

Review 6. Retinoic acid receptor beta promoter methylation and risk of cervical cancer.

Authors: Chaninya Wongwarangkana; Nasamon Wanlapakorn; Jira Chansaenroj; Yong Poovorawan
Journal: World J Virol Date: 2018-02-12

7. Trends in Cervical Cancer Mortality in Brazilian Women who are Screened and Not Screened.

Authors: Adriana Cunha Vargas; Catia Dell Agnolo; Willian Augusto de Melo; Fernando Castilho Pelloso; Lander Dos Santos; Maria Dalva de Barros Carvalho; Sandra Marisa Pelloso
Journal: Asian Pac J Cancer Prev Date: 2020-01-01

8. Predictors of cervical cancer screening among Kenyan women: results of a nested case-control study in a nationally representative survey.

Authors: Anne Ng'ang'a; Mary Nyangasi; Nancy G Nkonge; Eunice Gathitu; Joseph Kibachio; Peter Gichangi; Richard G Wamai; Catherine Kyobutungi
Journal: BMC Public Health Date: 2018-11-07 Impact factor: 3.295

9. Correlative analysis of the expression of IL-10 and Ki-67 in human cervical cancer and cervical intraepithelial neoplasias and human papillomavirus infection.

Authors: Zhihong Min; Xiaowen Pu; Zhengrong Gu
Journal: Oncol Lett Date: 2018-09-28 Impact factor: 2.967

10. Analytical performance of a low-cost multiplex polymerase chain reaction human papillomavirus genotyping assay for use in Sub-Saharan Africa.

Authors: Kandali Samwel; Crispin Kahesa; Julius Mwaiselage; Daniela Gonzalez; John T West; Charles Wood; Joel Palefsky; Peter C Angeletti
Journal: J Med Virol Date: 2018-10-22 Impact factor: 2.327