Human papillomavirus genotype distribution in Ethiopia: an updated systematic review

Cervical cancer is the most common malignancy impacting women and families globally. Today, more women are dying of cervical cancer than are dying of complications during childbirth. In 2020, an estimated 604,237 women were diagnosed with cervical cancer globally, representing 6.5% of all female cancers. In same year, the disease killed an estimated 341,843 women, 90% of whom were in less-developed regions of the world, where access to prevention, screening, and treatment services are severely limited [1]. In 2030, the annual number of new cases and death from cervical cancer has been projected to increase to 700, 000 and 400, 000, respectively [2, 3]. The global burden of cervical cancer (close to 90%) occurs in developing countries. The highest burden was reported in sub-Saharan lacking well-organized screening and Human papillomavirus (HPV) vaccination programs [2, 4‐6].

Cervical cancer imposes an enormous burden in Ethiopia. The incidence and prevalence of the disease are increasing because of the growth and aging of the population, as well as an increasing prevalence of well-established risk factors [7]. According to the international agency for research on cancer assessments, the estimated number of new cervical cancer cases was 7500 in 2020 and it will be increased to 15,300 in 2040 in Ethiopia. Similarly, the mortality from the disease will increase from 5340 in 2020 to 11,000 in 2040 yearly [3]. Cervical cancer is becoming a major cause of morbidity and mortality among women in Ethiopia as the country cannot sustain proven cervical cancer prevention strategies [6].

Etiologically > 99% of cervical cancer cases are associated with genital infection with High-Risk type HPV infections. It is the most common viral infection of the reproductive tract [8, 9] that most women are experience soon after they become sexually active [10]. Persistent infection with HR-HPV is the primary cause of cervical cancer [11, 12]. More than 200 different HPVs have been characterized and completely sequenced to date. Of all types of HPVs, about 30 to 40 are sexually transmitted and infect the genital areas of both men and women [13‐17]. HPVs are categorized according to their oncogenic potential. The HR-HPV types that include HPV16, 18, 31, 33, 35, 39, 45, 51, 52, 56, 58, 68 and 59. These are considered to be high-risk due to their strong implication in carcinogenesis, particularly the malignant progression of cervical tumors. Some other groups are classified as potential or probable high risk (pHR) types, including HPV 26, 53, 66, 70, 73, and 82. Studies showed that HPV 16 and 18 are the well-known oncogenic causing > 70% of all cervical cancer burdens worldwide [8, 18, 19].

The recognition of HPVs as a primary etiologic agent for human cancers has increased their medical importance and stimulated research into developing strategies for screening, diagnosis, prevention and treatment of HPV-associated diseases [20, 21]. Despite the high burden of cervical cancer related morbidity and mortality in Ethiopia, systematically compiled nationwide data on HPV genotypes distribution among Ethiopian women is limited. Therefore, this review was an update of our previous report [22] with more additional data describing the genotype distribution of HPVs in Ethiopia, where the finding would play a great role as an input for optimal vaccination and HPV-based cervical screening strategies.

The objective of this review was to describe the genotype distribution of Human papillomaviruses among women with different kinds of cervical lesions in Ethiopia.

Because of the considerable geographical differences in the HPV genotype distribution globally, data on HPV genotyping for a specific nation is important for vaccination and support cervical cancer screening policies  to improve the effectiveness of screening programs and reduce overtreatment [35]. However, currently there is limited data on the countrywide genotype distribution of HPVs in Ethiopia.

In the present review, the detection of HPV among women who were selected from the general population was between 19.9 and 23.2%. Likewise, the prevalence of HPV from woman with different kinds of cervical dysplasia was between 13.7 and 93%. A global-based review by Forman et al. showed that the prevalence of HPV was between 11 and 12% (with higher rates, 24%, in sub-Saharan Africa) in women without cervical abnormalities [36]. The detection of HPV increases in women with cervical pathology in proportion to the severity of the lesions, which supports our finding. Forman et al., in their global-based review, also reported close to 90% detection of HPV from women with different grades of cervical abnormalities [36]. In addition, a review by Pend et al. also showed HPV prevalence to be 84.8% from different kinds of cervical lesions among Asian women [37].

In our review, the proportions of high-risk, possible/probable high-risk and low-risk HPVs were at 77.5% (1493), 9.4% (182) and 10.1% (195), respectively. A recent meta-analysis by Ogembo et al. showed that the proportion of HR-HPV was 42.2% in Eastern Africa [38]. On the contrary, a similar review that report HPV profiling from women in India, Bangladesh, Sri Lanka and Nepal reported the proportion of HR-HPV types at 97% [39]. The difference might be due to population and geographic variations. The predominantly identified genotypes were HPV 16 (37.3%), HPV 52 (6.8%), HPV 35 (4.8%), HPV 18 (4.4%) and HPV 56 (3.9%). Some of other high-risk HPV groups include HPV 31 (3.8%), HPV 45 (3.5%), HPV 58 (3.1%), HPV 59 (2.3%), and HPV 68 (2.3%). These findings are essentially necessary to predict how HPV vaccination and HPV-based screening will impact cervical cancer prevention in Ethiopia. This infers that further HPV vaccine studies in Ethiopia should mainly target the first few predominant genotypes [22].

Based on similar review reports in different parts of the globe, the genotype distribution of HPVs in different countries from different kinds of cervical lesions is presented in Table 2 for comparison.

As it is indicated in the table, HPV 16 is the most common genotype consistently reported globally as an important cause of cervical abnormalities. Variation in the other types of HPV genotype distribution across the above studies is likely attributable to differences in population, the severity of cervical lesions, age at screening initiation, frequency, coverage, and follow-up rates of women with cervical abnormalities [22, 43]. Besides, the difference might also be associated with ethnic differences, geographical locations and the sexual behavior of their male partners [44‐46].

Among HR-HPV groups HPV 16 and 18 are commonly implicated in cervical malignancies globally. In this review, the combined prevalence of HPV 16/18 was at 53.7%. Similarly, a review by Ogembo et al. showed that HPV16/18 was 45.1% from high-grade cervical lesions and 67.7% of invasive cervical cancer among African women [38]. Among HPV positive cases, the co-prevalence of HPV 16/18 was reported differently in different countries such as; 60% (in Israel) in both pre-neoplastic lesions and cervical cancer [41], 87.5% (in Central and Eastern Europe) [47], 80% (India) among high-grade cervical lesions [39]. In Italy, HPV 16 (64%) and HPV 18 (7%) were frequently reported from women with abnormal cervical cytology [48]. A review by Guan et al. revealed that HPV 16 positivity increased steeply from normal to high-grade cervical lesions [49]. Accordingly, a vaccine mixes and HPV-based screening tests should always include this genotype although some low-grade cervical lesions associated with certain other HR-HPVs may preferentially progress to cervical cancer [22, 50]. Our review would envisage the future impact of broadly identified genotypes (HPV16, 52 and 35) in vaccination and HPV-based screening in Ethiopia.

The Ethiopian Ministry of Health started vaccinating school girls aged 14 years using Gardasil-4™ (HPV 6, 11, 16, 18) since 2018.  HPV-based screening based on the detection of HPV16/18 oncoproteins, and most recently HPV DNA test were employed. This implies that vaccinating girls using Gardasil-4^TM and screening women for cervical lesions using HPV16/18 oncoproteins significantly reduce the number of girls who might be protected, and women who might be missed by screening, respectively as the important HPV genotypes circulating in the country are not considered very well. Most developed countries are currently using otherwise the nonavalent Gardasil®9 (6, 11, 16, 18, 31, 33, 45, 52, and 58) vaccine that targets close to 90% of all HR-HPVs [51] which is essentially an ideal type of vaccine for Ethiopians as well based our review finding. However, it might have a financial implication.

This systematic review will be an important input to revise the current vaccination and HPV-based screening program of Ethiopia. The review includes studies from different settings and study participants, which enable us to appreciate a better picture of HPV genotypes distribution in Ethiopia. However, the review result should be interpreted in light of a few limitations. Because of the absence of studies from some parts of the country, our finding could compromise to gain  the overall picture of the HPV genotype distribution in overall Ethiopia. The other possible shortcoming of our review is the variations of HPV genotyping methods and the study participants included by the studies.

In this review, HR-HPV genotypes were predominantly identified from different kinds of cervical samples. HPV 16 in particular, but also HPV 52, 35 and HPV 18, requires special attention while designing vaccination and HPV-based cervical cancer screening programs in Ethiopia. Additional data are needed to strengthen this finding and emphasize the nationwide HPV map to broadly introduce, implement and sustain effective cervical cancer prevention and control programs in the country.