Genital and oral human papillomavirus infection in a patient from the group of women who have sex with women

Reis, Helena Lucia B. dos; Ferreira, Dennis Carvalho; Forattini, Aline Garcia; Souza, Philippe Godefroy; Curvelo, Jose Alexandre da Rocha; Passos, Mauro Romero Leal

doi:10.1590/S1807-59322010001200025

LETTER TO THE EDITOR

Genital and oral human papillomavirus infection in a patient from the group of women who have sex with women

Helena Lucia B. dos Reis^I; Dennis Carvalho Ferreira^II; Aline Garcia Forattini^III; Philippe Godefroy Souza^IV; Jose Alexandre da Rocha Curvelo^V; Mauro Romero Leal Passos^I

^IUniversidade Federal Fluminense - UFF - Setor de Doenças Sexualmente Transmissíveis, Niterói, Brazil

^IIUniversidade Federal do Rio de Janeiro - Institute of Microbiology Professor Paulo de Goes, Rio de Janeiro, Brazil

^IIIUniversidade Federal do Espírito Santo, Ginecologia/Obstetricia Hospital Universitário Cassiano Antonio de Moraes (HUCAM), Vitória, Espirito Santo. E-mail: hbarroso@unimedvitoria.com.br. Tel.: 55 27 3335 7180

^IVUniversidade Federal Fluminense, Setor de DST, Niterói, Brazil

^VUniversidade Federal do Rio de Janeiro, Institute of Microbiology Professor Paulo de Goes, Rio de Janeiro, Brazil

CASE REPORT

A 21-year-old self-declared lesbian patient of African descent was referred to a sexually transmitted disease (STD) center at the Federal Fluminense University (UFF) from a private clinic with a case of genital warts of 1 year's duration. The patient, who denied tobacco use but admitted social alcohol use, had been in a stable homosexual relationship for the previous 16 months, and routinely performs unprotected oral sex on her partner. She had been previously treated with trichloroacetic acid (TCA) 90% throughout the year with no signs of improvement. She presented with multiple, large, and hardened genital warts (Fig. 1) and a single, small lesion on her lower lip (Fig. 2). The lower lip lesion was first noticed by the patient approximately 30 days before her consultation. She had been treated with TCA 90% applied to the genital area for 4 weeks, without any noticeable clinical improvement; a biopsy was then carried out on both the genital area and the lips. Twenty-one days after the procedure, the genital lesions disappeared completely. Laboratory examinations were ordered (anti-HIV and Venereal Disease Research Laboratory), both of which tested negative; an examination of the larynx was also normal. The patient's partner was also tested. Her hymen was found to be intact and no alterations were found in the colposcopy examination.

Both women denied past history of STDs and heterosexual intercourse; although they did declare previous relationships with digital-vaginal and digital-anal practices, as well as vulvar and oral-to-oral contact. Biopsy results for lesions of the lips and vulva revealed condylomata acuminata (Figs 3 and 4). Polymerase chain reaction (PCR) tests for human papillomavirus (HPV) were performed on both lesions but the viral subtype was not defined. Specific orientations were offered to these women who are now symptom-free, and follow-up was undertaken by the STD center.

DISCUSSION

This case report clearly illustrates the need for specific orientation about HPV infection targeted at women who have sex with women (WSW), in view of their behavioral pattern and HPV infection pattern. Intact hymen poses a challenge for HPV screening and colposcopy, as demonstrated in the present case. Even though research has indicated that many WSW have had prior sexual intercourse with men or are self-declared bisexual (53-99%),^5,6 as indicated in a study conducted in Seattle, WA, this study showed that 86% of WSW confirmed having had sex with a male partner, and, of these, 24% reported sexual intercourse with men in the previous year;² our patient, who is WSW with intact hymen, may form yet another subgroup within the WSW subgroup.

Among the sexual practices reported, the most common are oral-vaginal sex, oral-to-oral sex, which was the case for our study subject, digital-vaginal and digital-anal sex and the use of sex toys. Any of these practices, if unprotected, would theoretically facilitate STD transmission, including HPV.^2,7

Our patient presented two clinical manifestations of HPV infection, namely oral and genital warts. Both her lesions were confirmed by histological studies, unlike her partner, whose examination results were negative. This fact highlights the challenge faced for breaking the HPV transmission cycle, since the incubation period of this virus varies or may even be indeterminate, resulting in a long period of time between infection and presentation of clinical signs by patients.³ Patients with a history of lesbianism in a long, steady relationship may feel uneasy in reporting previous sexual partners, which makes it harder to obtain a reliable history.

The fact that HPV types 6 and 16 have already been found in WSW, together with the example provided in our case, indicates the need for methods to effectively prevent HPV transmission, such as the use of gloves, plastic barriers and condoms.^2,8 The isolation of HPV from sexual fomites⁹ and from fingers¹⁰ of patients with genital warts adds to the idea that this virus can be sexually transmitted between women.

Among the most common viral subtypes found in genital warts were 31/33/35/39 for both WSW who deny any prior sexual contact with men and for those WSW who reported no sexual contact with men in the previous year. In the latter group, however, subtype 16 was found to be the most prevalent.²

Another important factor in the follow-up of these patients is the availability of records of their former and current sexual partners, as the information obtained may contribute to better outcomes. Our subject has undergone regular follow-up visits, varying from monthly to yearly check-ups in order to keep an accurate record of the case.

The clinical management of oral and genital warts aims at the removal of lesions, which can be done through the use of either TCA 60-90%, podophyllin resin 10-25%, or imiquimod 5% cream. A surgical approach would involve any of the following: tangential scissor excision, tangential shave excision, curettage, electrosurgery, or laser surgery.

The choice of treatment should be based on the number of lesions, their localization and size, costs, and resources available. When there are few lesions present, surgical removal is indicated, especially when histological studies are desirable.^1,11 These data are consistent with the treatment course adopted; incision biopsy was performed on the patient's genital warts after three sessions of TCA 90% and an excision biopsy was performed on the lip lesion. It should be pointed out that our patient had already been treated with TCA 90% for genital warts for approximately 1 year prior to her referral to UFF. It should also be noted that 21 days after the biopsy, the vulvar lesions had disappeared completely. It is important to emphasize the relationship between local immune factors and the viral agent, since it might be the case that the inflammation process evoked by the biopsy was a key element for viral suppression.¹²

In general, none of the available treatments are 100% effective for every patient because HPV acquires different forms of resistance in different organisms. In other words, each case should be evaluated individually, before establishing the therapeutic course. The individual immune response plays a key role in both the elimination of the virus and in the reduction of recurrence.¹³ Patients should be informed that post-treatment recurrence may be as high as 30%, most cases of which are seen after the first 3 months of treatment.¹⁴ This emphasizes the need for WSW patients to undergo routine pap smears, along with a thorough clinical examination, including the oral cavity, in the same way as heterosexual women do. This will significantly contribute to the prevention of cervical cancer, a disease closely associated with HPV infection and which accounts for one of the two most prevalent forms of cancer in Brazilian women.^15,16

Various types of HPV has been described with oncogenic potential and associated with oral lesions. Squamous papilloma (SP), condyloma acuminatum (CA) and focal epithelial hyperplasy are the most frequent pathological entities associated with HPV, and this virus has been identified and correlated to lichen planus, vulgar pemphigus, squamous cell carcinoma (SCC), and verrucose carcinoma (VC).^11,17,18 This infection often occurs on oral mucosa and the sites most involved are labial mucosa, with 55% of cases, the palate, jugal mucosa, gums, tonsils, uvula and roof of the mouth.¹⁹ Careful clinical history, oral examination, and histopathology may lead to correct diagnosis and treatment, as showed by the present report

Owing to the oncogenic role of certain types of HPV, the relation between this virus and carcinogenesis in oral mucosa is still controversial. Various studies have identified HPV in biopsies of oral SCC and VC.^19,20 Oral HPV infection is associated with oropharyngeal cancer among subjects with or without established risk factors of tobacco and alcohol use.^19,11

In an attempt to protect women from cervical cancer, much research is now devoted towards the development of effective HPV vaccines.²¹ These vaccines, however, will have a prophylactic goal and be targeted at patients who have not had prior exposition to the virus.^3,17 However important these new developments are, the need for routine HPV screening remains critical, as does the need for creating and/or strengthening HPV awareness among all WSW.

¹
Brasil. Ministério da Saúde. Secretaria de Projetos Especiais de Saúde. Coordenação de Doenças Sexualmente Transmissíveis e AIDS. Manual de Controle das Doenças Sexualmente Transmissíveis. 3rd edn. Brasília: 1999. pp. 95-100.
2. Marrazzo JM, Koutsky LA, Stine KL, Kuypers JM, Grubert TA, Galloways DA, et al. Genital human papillomavirus infection in women who have sex with women. J Infect Dis. 1998;178:1604-9, doi: 10.1086/314494.
3. Tovar JM, Bazaldua OV, Vargas L, Reile E. Human papillomavirus, cervical cancer, and the vaccines. Postgrad Med. 2008;120:79-84, doi: 10.- 3810/pgm.2008.07.1794.
4. Marazzo JM, Coffey P, Bingham A. Sexual practices, risk perception and knowledge of sexually transmitted disease risk among lesbian and bisexual women. Perspect Sex Reprod Health. 2005;37:6-12, doi: 10.1363/-3700605.
5. O'Hanlan KA. Lesbian health and homophobia. Curr Prob Obstet Gynecol Fertil 1995;18:93-136.
6. Laumann EO, Gagnon JH, Michael RT, Michaels S. The social organization of sexuality: sexual practices in the United States. Chicago: University of Chicago Press. 1994;295.
7. Eaton L, Kalichman S, Cain D, Cherry C, Pope H, Fuhrel A, et al. Perceived prevalence and risks for human papillomavirus (HPV) infection among women who have sex with women. J Womens Health (Larchmt). 2008;17:75-83, doi: 10.1089/jwh.2006.0256.
8. Bailey JV, Kavanagh J, Owen C, McLean KA, Skinner CJ. Lesbian and cervical screening. Br J Gen Pract. 2000;50:481-2.
9. Ferenczy A, Bergueron C, Richart RM. Human papillomavirus DNA in fomites on objects used the management of patients with genital human papillomavirus infections. Obstet Gynecol. 1989;74:950-4.
10. Sonnex C, Strauss S, Gray JJ. Detection of human papillomavirus DNA on the fingers of patients with genital warts. STI. 1999;75:317-9.
11. Castro TMPG, Neto CER, Scala KA, Scala WA. Manifestações orais associadas ao papilomavírus humano (HPV) conceitos atuais: revisão bibliograífica. Rev Bras Otorrinolaringol. 2004;70:546-50.
12. Trottier H, Franco EL. The epidemiology of genital human papillomavirus infection. Vaccine. 2006;24(Suppl)1:S1-S15.
13. Ellerbrock TV, Chiasson MA, Bush TJ, Sun XW, Sawo D, Brudney K, et al. Incidence of cervical squamous intraepithelial lesions in HIV-infected women. JAMA. 2000;283:1031-7, doi: 10.1001/jama.283.8.1031.
14. Centers for Disease Control and Prevention, Workowski KA, Berman SM. Sexually transmitted diseases treatment guidelines, 2006. MMWR Recomm Rep. 2006;55(RR-11):1-94.
¹⁵
Brasil. Ministério da Saúde. Instituto Nacional do Cancer-INCA. Estimativas da incidência e mortalidade por cancer. Rio de Janeiro: INCA. 2003;92.
16. Terai M, Takagi M. Human papillomavirus in the oral cavity. Oral Med Pathol. 2001;6:1-12, doi: 10.3353/omp.6.1.
17. Reis HLB, Rabelo PC, Santana MRF, Ferreira DC, Filho AC. Oral squamous papilloma and condyloma acuminatum as manifestations of buccal-genital infection by human papillomavirus. Indian J Sex Transm Dis AIDS. 2009;30:40-2, doi: 10.4103/0253-7184.55484.
18. Ferreira DC, Curvelo JAR, Passos MRL. Open questions on carcinogenesis of oral cancer: Interaction between the environmental and genetic aspects. IJDR. 2009;20:249.
19. D'Souza G, Kreimer AR, Viscidi R, Pawlita M, Fakhry C, Koch WM, et al. Case-control study of human papillomavirus and oropharyngeal cancer. N Engl J Med. 2007;356:1944-56, doi: 10.1056/NEJMoa065497.
20. Ward KA, Napier SS, Winter PC, Maw RD, Dinsmore WW. Detection of human papilloma virus DNA sequences in oral squamous cell papillomas by the polymerase chain reaction. Oral Surg Oral Med Oral Pathol Oral Radiol Endod. 1995;80:63-6, doi: 10.1016/S1079-2104(95)80017-4.
21. Aligieri P. Pais e meídicos precisam conhecer e recomendar as vacinas contra HPV. Rev Assoc Med Bras. 2007;53:283., doi: 10.1590/S0104-42302007000400001

Publication Dates

Publication in this collection
21 Mar 2011
Date of issue
2010

This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

[1] ¹
Brasil. Ministério da Saúde. Secretaria de Projetos Especiais de Saúde. Coordenação de Doenças Sexualmente Transmissíveis e AIDS. Manual de Controle das Doenças Sexualmente Transmissíveis. 3rd edn. Brasília: 1999. pp. 95-100.

[2] 2. Marrazzo JM, Koutsky LA, Stine KL, Kuypers JM, Grubert TA, Galloways DA, et al. Genital human papillomavirus infection in women who have sex with women. J Infect Dis. 1998;178:1604-9, doi: 10.1086/314494.

[3] 3. Tovar JM, Bazaldua OV, Vargas L, Reile E. Human papillomavirus, cervical cancer, and the vaccines. Postgrad Med. 2008;120:79-84, doi: 10.- 3810/pgm.2008.07.1794.

[4] 4. Marazzo JM, Coffey P, Bingham A. Sexual practices, risk perception and knowledge of sexually transmitted disease risk among lesbian and bisexual women. Perspect Sex Reprod Health. 2005;37:6-12, doi: 10.1363/-3700605.

[5] 5. O'Hanlan KA. Lesbian health and homophobia. Curr Prob Obstet Gynecol Fertil 1995;18:93-136.

[6] 6. Laumann EO, Gagnon JH, Michael RT, Michaels S. The social organization of sexuality: sexual practices in the United States. Chicago: University of Chicago Press. 1994;295.

[7] 7. Eaton L, Kalichman S, Cain D, Cherry C, Pope H, Fuhrel A, et al. Perceived prevalence and risks for human papillomavirus (HPV) infection among women who have sex with women. J Womens Health (Larchmt). 2008;17:75-83, doi: 10.1089/jwh.2006.0256.

[8] 8. Bailey JV, Kavanagh J, Owen C, McLean KA, Skinner CJ. Lesbian and cervical screening. Br J Gen Pract. 2000;50:481-2.

[9] 9. Ferenczy A, Bergueron C, Richart RM. Human papillomavirus DNA in fomites on objects used the management of patients with genital human papillomavirus infections. Obstet Gynecol. 1989;74:950-4.

[10] 10. Sonnex C, Strauss S, Gray JJ. Detection of human papillomavirus DNA on the fingers of patients with genital warts. STI. 1999;75:317-9.

[11] 11. Castro TMPG, Neto CER, Scala KA, Scala WA. Manifestações orais associadas ao papilomavírus humano (HPV) conceitos atuais: revisão bibliograífica. Rev Bras Otorrinolaringol. 2004;70:546-50.

[12] 12. Trottier H, Franco EL. The epidemiology of genital human papillomavirus infection. Vaccine. 2006;24(Suppl)1:S1-S15.

[13] 13. Ellerbrock TV, Chiasson MA, Bush TJ, Sun XW, Sawo D, Brudney K, et al. Incidence of cervical squamous intraepithelial lesions in HIV-infected women. JAMA. 2000;283:1031-7, doi: 10.1001/jama.283.8.1031.

[14] 14. Centers for Disease Control and Prevention, Workowski KA, Berman SM. Sexually transmitted diseases treatment guidelines, 2006. MMWR Recomm Rep. 2006;55(RR-11):1-94.

[15] ¹⁵
Brasil. Ministério da Saúde. Instituto Nacional do Cancer-INCA. Estimativas da incidência e mortalidade por cancer. Rio de Janeiro: INCA. 2003;92.

[16] 16. Terai M, Takagi M. Human papillomavirus in the oral cavity. Oral Med Pathol. 2001;6:1-12, doi: 10.3353/omp.6.1.

[17] 17. Reis HLB, Rabelo PC, Santana MRF, Ferreira DC, Filho AC. Oral squamous papilloma and condyloma acuminatum as manifestations of buccal-genital infection by human papillomavirus. Indian J Sex Transm Dis AIDS. 2009;30:40-2, doi: 10.4103/0253-7184.55484.

[18] 18. Ferreira DC, Curvelo JAR, Passos MRL. Open questions on carcinogenesis of oral cancer: Interaction between the environmental and genetic aspects. IJDR. 2009;20:249.

[19] 19. D'Souza G, Kreimer AR, Viscidi R, Pawlita M, Fakhry C, Koch WM, et al. Case-control study of human papillomavirus and oropharyngeal cancer. N Engl J Med. 2007;356:1944-56, doi: 10.1056/NEJMoa065497.

[20] 20. Ward KA, Napier SS, Winter PC, Maw RD, Dinsmore WW. Detection of human papilloma virus DNA sequences in oral squamous cell papillomas by the polymerase chain reaction. Oral Surg Oral Med Oral Pathol Oral Radiol Endod. 1995;80:63-6, doi: 10.1016/S1079-2104(95)80017-4.

[21] 21. Aligieri P. Pais e meídicos precisam conhecer e recomendar as vacinas contra HPV. Rev Assoc Med Bras. 2007;53:283., doi: 10.1590/S0104-42302007000400001

Brasil

Brasil

Genital and oral human papillomavirus infection in a patient from the group of women who have sex with women

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