O papilomavirus humano e lesões do colo uterino

Rosa, Maria Inês da

January 2007

Analisamos uma coorte de mulheres no sul do Brasil, com objetivo de identificar associações epidemiológicas para persistência e cura da infecção pelo HPV e realizamos uma metanálise para determinar a acurácia da telomerase nas lesões precursoras do câncer cervical. Métodos: O estudo de coorte foi iniciado em fevereiro de 2003. Foram coletados espécimes cervicais para citologia oncótica e para detecção do DNA HPV na entrada do estudo e no seguimento. O desfecho foi dividido em quatro categorias: (1) persistência, (2) conversão (3) cura. A quarta categoria (referência) eram mulheres negativas no início que permaneceram negativas. Foram usados o teste χ2 de Pearson, regressão logística multinomial e Kaplan- Meier para análise estatística. Para a metanálise foram incluídos estudos que comparavam o teste de telomerase (TRAP) e anatomopatológicos, obtidos por biópsias cervicais para diagnóstico de lesões cervicais. Resultados: A Incidência de HPV foi 12,3%. O HPV16 foi o tipo mais encontrado (18,6%), entre as 501 mulheres do estudo.Trinta e quatro mulheres (6,78%) ficaram persistentemente infectadas pelo HPV, estando essa categoria associada à idade da sexarca inferior a 21 anos (OR = 3,14, IC 95%, 1,43-6,87) e a quatro ou mais parceiros durante a vida (OR = 2,48 IC 95%, 1,14-5,41). No período mediano de 19 meses, 80,7 % das mulheres tinham curado o HPV, a cura foi significativamente associado à cor preta (OR= 3,44 IC 95%, 1,55-7,65), co-infecção com C. trachomatis no arrolamento (OR= 3,26, IC 95%, 1,85-5,76) e história de já ter realizado exame de Papanicolaou (OR= 3,48, IC 95%, 1,51- 8,00). Na metanálise dez estudos foram analisados, os quais incluíram 1069 mulheres. Para lesões intraepiteliais de baixo grau (LIEBG) vs. normal ou lesões benignas, encontrou-se uma positividade do teste da telomerase, sendo que o resultado da odds ratio para diagnóstico (DOR) foi de (DOR = 3,2, IC 95%,1,9-5,6). Nas lesões intraepiteliais de alto grau (LIEAG) vs LIEBG, normal ou benigna: (DOR = 5,8, IC 95%, 3.1-10). )]. Encontrou-se uma DORelevada de 8,1 (IC 95%: 3,2-20) nas lesões de câncer cervical vs LIEAG. Da mesma forma, nas lesões de câncer cervical vs. LIEBG, a razão de chance foi elevada, com uma DOR de 40,9 (IC 95%: 18,2-91). Conclusões: A persistência da infecção pelo HPV foi associada com a sexarca precoce e ao número de parceiros sexuais na vida, sugerindo que estratégias de orientação sexual podem modificar as taxas de persistência do HPV. A associação da cura do HPV com história prévia de realização de Papanicolaou salienta a importância de aprimorar os programas de rastreamento de câncer cervical. Futuros estudos da associação de infecções ginecológicas com cura da infecção pelo HPV são necessários. Na metanálise nossos dados suportam a corrente hipótese da atividade da telomerase como um evento precoce na carcinogênese e que poderia estar associado ao início e à progressão de lesões cervicais. / We analysed a cohort of women in Southern Brazil with the aim to identify epidemiological correlates for persistence and clearance of cervical HPV infection. A quantitative systematic review was performed to estimate the accuracy of telomerase assay in cervical lesions. Methods: A cohort study was started on February 2003. Cervical smears were collected to perform Pap cytology and HPV DNA detection at baseline and during the follow up. The outcome was constructed in four categories (1) persistence of HPV DNA; (2) conversion; (3) clearance of HPV. Pearson’s χ2 test, multinomial logistic regression and univariate analysis using the log-rank test were performed. Meta-analysis studies that evaluated the telomerase test (telomerase repeated amplification protocol) for the diagnosis of cervix lesions and compared it to paraffin-embedded sections as the diagnostic standard were included. Results: Incidence of HPV DNA: 12.3%. HPV16 was the most frequent type (18.6%) among 501 women in the study. Thirty-four women were persistently infected with HPV, which was associated with age below 21 years at first intercourse (OR 3.14, 95% CI, 1.43-6.87) and ≥ 4 sexual partners during lifetime (OR 2.48, 95% CI, 1.14-5.41). In a median period of 19 months, 80.7% of women had clearance of HPV, which was associated with black race (OR 3.44, 95% CI, 1.55-7.65), co-infection with C. trachomatis at baseline (OR 3.26, 95% CI, 1.85-5.76) and history of previous Pap smear (OR 3.48, 95% CI, 1.51-8.00). In meta-analysis ten studies were analyzed, which included 1,069 women. The diagnostic odds ratio (DOR) for a positive telomerase test for Lo-SIL vs. normal or benign lesions was 3.2 (95% CI, 1.9-5.6). The DOR for a positive telomerase test for Hi-SIL vs. Lo-SIL, normal or benign lesions was 5.8 (95% CI, 3.1-10). For cervix cancer vs. Hi-SIL, the DOR for a positive telomerase test was 8.1 (95% CI, 3.2-20.3) and for cervix cancer vs. Lo-SIL, normal or benign lesions, it was 40.9 (95% CI, 18.2-91). Conclusions: Persistence of HPV infection wasassociated with early age at first intercourse and number of sexual partners during lifetime, suggesting that strategies for sexual orientation may modify the rates of HPV persistence. The association of HPV clearance with a history of previous Pap smear screening highlights the importance of improving cervical screening programs. Further studies on the association of gynaecological infections with HPV clearance are needed. In meta-analysis our data support the current hypothesis that telomerase may activate an early event in cervical carcinogenesis, that could be associated with the initiation and progression of cervical lesions.

Infecções por papillomavirus

Neoplasias do colo do útero

Fatores de risco

Metanálise

Telomerase

Human papillomavirus infection

Cervix cancer

Gynaecological infections

HPV clearance

Risk factors

Accuracy

Diagnosis

Meta-analysis

Systematic review

Telomerase

Associação entre polimorfismos de genes do sistema imunológico (IL-10, TNF-a) e a infecção por HPV nos diferentes graus de lesões cervicais

Igansi, Cristine Nascente

January 2009

Estudos epidemiológicos e moleculares têm sugerido que o HPV é o principal fator de risco para o desenvolvimento de lesões malignas na cérvice uterina. E, sendo o número de infecções extremamente maior do que o número de casos de câncer cervical, este fato nos leva à investigação de outros fatores associados, como por exemplo, a predisposição imunológica do hospedeiro. Este estudo tem como objetivo avaliar a associação dos polimorfismos (-1082A/G) e (-308 A/G), localizados nos genes da IL-10 e TNF-α, respectivamente, com a infecção genital pelo Papilomavírus Humano (HPV), incluindo os tipos oncogênicos HPV-16, 18 e 31, visto que, estas citocinas são moléculas importantes na resposta imune contra infecções virais. Trata-se de um estudo de casos e controles. O grupo controle foi composto por 211 mulheres, que apresentavam resultado negativo para infecção genital por HPV, identificada através da técnica de Reação em Cadeia da Polimerase (PCR) e exame citopatológico sem alterações. Já os casos, corresponderam a 84 mulheres com infecção genital por HPV e resultado anatomopatológico alterado. A técnica de amplificação refratária de mutações (ARMS-PCR) foi utilizada para a identificação dos polimorfismos. Regressão logística múltipla foi utilizada para verificar a associação das variáveis estudadas com o desfecho (infecção genital pelo HPV).O cálculo de Equilíbrio de Hardy-Weinberg foi utilizado para verificar se as freqüências alélicas e gentotípicas observadas estão de acordo com as esperadas na população em estudo. Para os resultados de IL-10, a freqüência genotípica observada nos casos foi de 11,9% (AA), 28,6% (AG) e 59,5% (GG); a freqüência alélica foi de 26,0% para A e 74,0% para G. No grupo controle, a freqüência genotípica encontrada foi 22,8% (AA), 48,8% (AG) e 28,4% (GG); a freqüência alélica foi de 47,0% para A e 53,0% para G. Houve diferença significativa entre os grupos estudados, tanto para a freqüência alélica quanto para a genotípica (p<0,0001). Entre as mulheres com infecção, encontramos associação das lesões intraepiteliais escamosas de baixo grau (LGSIL) com o genótipo GG (p=0,02). As variáveis idade (RC=4,70; IC95%: 2,61-8,40), co-infecção por HIV (RC=11,21; IC95%:1,002-125,33) e o genótipo GG (RC=4,22; IC95%: 1,84-9,61) permaneceram independentemente associados ao desfecho (infecção genital pelo HPV). Para TNF-α, a homozigosidade do alelo G (genótipo GG) foi encontrada em maior freqüência nos casos (36,9%), seguido por 35,7% do genótipo AA e 27,4% do genótipo AG. Houve diferença significativa entre os grupos estudados, tanto para a freqüência alélica (p<0,0002) quanto para a genotípica: AA (p=0,03), AG e GG (p<0,0001). Analisando a associação com lesões cervicais e tipos oncogênicos, encontramos associação entre o genótipo GG e LGSIL (p<0,01). O genótipo GG está associado ao tipo oncogênico HPV-16 (p<0,05), e à co-infecção pelo vírus HIV (p<0,001). As variáveis idade (RC=3,46; IC95%: 1,89-6,33), os genótipos AG (RC=9,21; IC95%: 4,29-19,75) e AA (RC=2,73; IC95%: 1,25-6,00) permaneceram independentemente associados ao desfecho (infecção genital pelo HPV). Com estes resultados, é possível sugerir que a predisposição determinada geneticamente para a produção de altos níveis de IL-10 e TNF-α parece estar associada à infecção genital pelo HPV, mostrando a importância da resposta imunológica do hospedeiro no processo de infecção e na progressão das lesões cervicais geradas pelo Papilomavírus Humano. / Molecular and epidemiological studies have suggested that HPV is the most important risk factor for the development of malignant lesions in the uterine cervix. The fact that the number of HPV infections is extremely greater than the number of cervical cancer cases leads us to the investigation of other risk factors, such as the predisposition of the host immune. The present study aimed to evaluate the influence of genetic polymorphisms (-1082A/G) and (-308A/G), located in the genes of IL-10 and TNF-α, respectively, with the genital HPV infection, including oncogenic HPV-16, 18 and 31, since these cytokines are important molecules in the immune response against viral infections. This is a case-control study. The control group was composed by 211 women, who have tested negative for HPV genital infection by the Polymerase Chain Reaction (PCR) technique, and who had normal cytologic results. Cases were 84 women with HPV genital infection and abnormal anatomopathological results. The technique of amplification refractory mutation system (ARMS-PCR) was used to identify the polymorphisms. Multiple logistic regression was used to verify the association between the study factors and the outcome (genital infection by HPV). The Hardy-Weinberg equilibrium was used to verify whether the observed allelic and genotypic frequencies were according with the expected in the studied population. For the results of IL-10, the genotypic frequencies observed in the group of women with infection was 11.9% (AA), 28,6% (AG) and 59.5% (GG), the allelic frequency was 26.0% for 74.0% for A and G. In the control group, the frequency was found genotypical 22.8% (AA), 48.8% (AG) and 28.4% (GG), the allelic frequency was 47.0% to 53.0% for A and G. There were significant differences between groups, both for the allelic frequency as for the genotypic (p<0.0001). Among women with infection, we found association of injuries LGSIL with the GG genotype (p=0021). The variables age (OR=4.70; 95%IC: 2.61-8.40), HIV co-infection (OR=11.21; 95%IC: 1.002-125,33), and genotype GG (OR=4.22; 95%IC: 1.84-9.61) remained independently associated to the outcome (genital HPV infection). For TNF-α analysis, the genotypic frequencies observed in the group of patients was 22.0% (AA), 69.0% (AG) and 8.0% (GG), the allelic frequency was 57.0% and 43.0% for A to G. In the control group, the frequency genotype was found 35.0% (AA), 27.0% (AG) and 36.0% (GG), the allelic frequency was 49.0% for A and 51.0% for G. There were significant differences between groups, both for the allelic frequency (p<0.0002) and to the genotypic: AA (p=0.03), AG e GG (p<0.0001). Analysing the association with cervical lesions and with high-risk type, there was found a significant association, between the genotype GG and LGSIL (p<0.01). The genotype GG is associated with the HPV-16 infection (p<0.05) and with the HIV virus co-infection (p<0001). The variables age (OR=3.46; 95%IC: 1.89-6.33), genotypes AG (OR=9.21; 95%IC: 4.29-19.75) and AA (OR=2.73; 95%IC: 1.25- 6.00) remained independently associated to the outcome (genital HPV infection). The results suggest that the genetically determined predisposition to produce high levels of IL- 10 and TNF-α may be related to the genital HPV infection showing the importance of the host immune response in the progression of cervical lesions caused by the Human Papillomavirus.

Papillomavirus humano

Polimorfismo genético

Neoplasias do colo do útero

Infecções por papillomavirus

Lesões

Fator de necrose tumoral alfa

Interleucina-10

HPV

Polymorphism

IL-10

TNF-α

Cervical cancer

Associação entre o papiloma vírus humano e o carcinoma epidermóide de orofaringe : um estudo de caso-controle

Schwartsmann, Carla Cuenca

January 2013

Introdução: A incidência do carcinoma epidermóide de orofaringe (CEO) aumentou em todo o mundo nos últimos 30 anos. Estudos identificaram o papiloma vírus humano (HPV) como um fator de risco para essa neoplasia. Objetivos: O objetivo do presente estudo foi verificar a frequência do HPV em pacientes com CEO e em pacientes sem neoplasia maligna e avaliar a existência de uma diferença estatisticamente significativa na frequência do HPV entre os dois grupos. O objetivo secundário foi estudar a correlação entre a infecção pelo HPV e a localização do tumor na orofaringe, o estadiamento clínico e o grau de diferenciação tumoral. Métodos: Foi realizado um estudo de caso-controle com 59 pacientes com CEO e 54 pacientes sem neoplasia, no qual foram analisados os blocos de parafina contendo material tumoral e tecido não neoplásico. Foram analisadas respectivamente a frequência do HPV e sua atividade viral utilizando a técnica de hibridização in situ cromogênica (CISH) para HPV de baixo risco (BR) e alto risco (AR) e a expressão imunoistoquímica da proteína P16. Resultados: A frequência do HPV foi maior no grupo caso em comparação ao grupo controle quando utilizamos a expressão imunoistoquímica da proteína P16 como método de detecção isolado (OR=10,3; P<0,001) e quando utilizamos a CISH e a expressão imunoistoquímica da proteína P16 em conjunto (OR=21,4; P<0,001). A CISH isoladamente não mostrou uma diferença estatisticamente significativa na frequência do HPV entre os grupos estudados (P=0,572). A localização tumoral na orofaringe e o estadiamento clínico não mostraram correlação com a infecção pelo HPV em nenhum dos métodos utilizados, assim como o grau de diferenciação tumoral (P>0,20). Conclusão: Utilizando-se a técnica de imunoistoquímica para P16 isolada ou combinada com a técnica de CISH, observou-se uma maior positividade para o HPV no grupo de pacientes com CEO. A localização do tumor na orofaringe, o estadiamento clínico e o grau de diferenciação tumoral não tiveram correlação com a positividade para o HPV. / Introduction: The incidence of oropharyngeal squamous cell carcinoma (OSCC) has increased worldwide over the last 30 years. Studies have identified human papillomavirus (HPV) infection as a risk factor for OSCC. Objectives: To compare the frequency of HPV infection in patients with OSCC and patients with benign oral or oropharyngeal disease and ascertain whether a statistically significant difference in HPV frequency exists between these two groups. As a secondary objective, to assess potential correlations between HPV positivity, anatomic site of OSCC, tumor staging, and degree of tumor differentiation. Methods: Case-control study. The sample comprised 59 patients with OSCC and 54 non-OSCC controls who underwent surgery for benign oral or oropharyngeal conditions. Paraffin-embedded specimens from cases and controls were tested for HPV positivity by chromogenic in situ hybridization (CISH) for low-risk (LR) and high-risk (HR) HPV, and HPV activity was assessed by P16 immunohistochemistry (IHC). Results: The frequency of HPV positivity was higher in the case group than in the control group when assessed by P16 IHC alone (OR=10.3, P<0.001) or by CISH and P16 IHC in combination (OR=21.4, P<0.001). CISH alone did not detect any significant between-group difference in HPV frequency (P=0.572). Tumor site, staging, and differentiation did not correlate with HPV positivity with any of the methods employed (P>0.20). Conclusion: Using a P16 IHC assay alone or combined with CISH, the authors showed a higher rate of HPV positivity among patients with OSCC, as compared with patients with benign disease. Tumor site within the oropharynx, tumor stage, and degree of differentiation did not correlate with HPV positivity.

Carcinoma de células escamosas

Hibridização in situ

Imunoistoquímica

Papillomavirus humano 16

Tonsila palatina

Squamous cell carcinoma

In situ hybridization

Immunohistochemistry

Oropharynx

Human papillomavirus 16

Palatine tonsil

Avaliação da prevalência do Papíloma Humano (HPV) em saliva de pacientes portadores do HIV

AZEVEDO, Karinne Silva

27 August 2015

Submitted by Fabio Sobreira Campos da Costa (fabio.sobreira@ufpe.br) on 2016-12-12T14:11:56Z No. of bitstreams: 2 license_rdf: 1232 bytes, checksum: 66e71c371cc565284e70f40736c94386 (MD5) DISSERTACAO PARA BIBLIOTECA CENTRAL - KARINNE AZEVEDO.pdf: 2052240 bytes, checksum: fba514c37249c7db73fcf51a37fa21ff (MD5) / Made available in DSpace on 2016-12-12T14:11:56Z (GMT). No. of bitstreams: 2 license_rdf: 1232 bytes, checksum: 66e71c371cc565284e70f40736c94386 (MD5) DISSERTACAO PARA BIBLIOTECA CENTRAL - KARINNE AZEVEDO.pdf: 2052240 bytes, checksum: fba514c37249c7db73fcf51a37fa21ff (MD5) Previous issue date: 2015-08-27 / CAPES / Identificar a presença dos sorotipos de alto risco do Papilomavírus Humano (HPV) na saliva de pacientes portadores do vírus HIV. A amostra de 90 pacientes foi oriunda de dois centros de referência em tratamento de ISTs da cidade do Recife, PE, Brasil. Uma entrevista foi realizada para identificar o perfil da amostra, sendo realizada uma coleta de saliva empregando tubos falcon e solução para bochecho com sacarose a 5%, com posterior armazenamento em freezer a -20°C para rastreamento do HPV e genotipagem para o sorotipo 16 e 18 por PCR convencional. Na amostra predominou a presença do sexo masculino 59 de 90 (65,6%), com idade média de 38,8 anos, variando entre 18 e 69 anos, renda familiar média de 1,95 Salários Mínimos (DP = 1,37). A prevalência de HPV nesta amostra foi de 23 de 90 (25,6%) e dos sorotipos 16 e 18 foi 8 de 90 (8,9%). A co-infecção por HPV é comumente observada em pacientes portadores de HIV. / To identify the presence of high-risk serotypes human papillomavirus (HPV) in patients with sexually transmitted infections (STIs). A sample of 90 patients were from two referral hospitals in treatment of STIs. An interview was conducted to identify the sample’s profile a saliva collections being perfomed using falcon tubs and mount rinse with 5% sucrose, subsequente storage in a freezer at -20ºC for HPV screening and genotyping for serotype 16 and 18 by conventional PCR. In the sample predominant male presence 59 of 90 (65.6%) with mean age of 38.8 years, ranging between 18 and 69 years, average family income of 1.95 minimum wages (SD = 1, 37). The prevalence of HPV in this sample was 23 of 90 (25.6%) and the serotype HPV 16 and 18 was 8 of 90 (8.9%). Co-infection with HPV is commonly observed in HIV patients.

Papilomavírus Humano 16

Papilomavírus Humano 18

Infecções por HIV

Infecções Sexualmente Transmissíveis

Papilomaviridae

Human Papillomavirus 16

Human Papillomavirus 18

HIV Infections

Sexually Transmitted Diseases

Papilomaviridae

Prevalência de infecção por HPV em jovens primíparas e fatores associados / Prevalence of HPV infection in young primiparous women and associated factors

Cristina Helena Rama

21 July 2009

Introdução: A infecção genital pelo papilomavírus humano (HPV) é um fator necessário para o desenvolvimento do câncer cervical. Vacinas para prevenir a infecção pelos tipos de alto risco HPV 16 e 18 foram desenvolvidas e idealmente devem ser administradas antes da exposição ao HPV através do contato sexual. As variações na prevalência do HPV e na de seus tipos específicos em diferentes populações podem influenciar as recomendações da vacina contra o HPV em diferentes locais. A vacinação após o primeiro parto poderia ser uma estratégia em potencial para atingir mulheres jovens e saudáveis, dependendo da proporção de mulheres desse grupo ainda não infectadas pelos tipos de alto risco, HPV 16 e 18. Objetivos: O objetivo principal deste estudo foi determinar a prevalência genital do DNA de tipos específicos do HPV e avaliar a associação dessa infecção com fatores de risco selecionados em mulheres após o primeiro parto, usuárias de uma maternidade pública. Métodos: Esse estudo transversal foi realizado no Hospital Maternidade Leonor Mendes de Barros (HMLMB), uma das maiores maternidades públicas da cidade de São Paulo. Durante junho de 2006 até fevereiro de 2007, 301 primíparas de 15-24 anos, cujos partos ocorreram no referido Hospital, foram incluídas no estudo entre 43 e 60 dias após o parto. Na detecção de DNA do HPV extraído das células cervicais esfoliadas foi utilizado protocolo padrão da Reação em Cadeia por Polimerase (PCR), utilizando primers PGMY09/11. Para estimar a associação da infecção por HPV com fatores de risco selecionados, foi calculada a Razão de Prevalência (RP) e o intervalo de 95% de confiança [IC]; o ajuste foi realizado utilizando-se o Modelo Linear Generalizado (MLG) com distribuição binomial e função de ligação logarítmica. Resultados: O DNA do HPV foi detectado em 58,5% (IC 95% 52,7%-64,0%) das jovens mulheres. Os tipos de HPV mais comumente encontrados foram: HPV 16, HPV 51, HPV 52, HPV 58 e HPV 71. A prevalência dos tipos de HPV incluídos nas vacinas profiláticas foi: HPV 16 - 12,0%, HPV 18 - 2,3% e HPV 6+11 - 4,3%. Os tipos de alto risco de HPV foram encontrados em 133 (44,2%) mulheres, enquanto 43 delas (14,3%) apresentaram somente tipos de HPV de baixo risco. Cento e duas mulheres (33,9%) foram positivas para apenas um tipo de HPV; entretanto, 43 (14,3%) apresentaram dois tipos, e 31 (10,3%) apresentaram três ou mais tipos virais. A análise multivariada revelou que somente a idade (p=0,020) e o hábito de fumar (p <0,001) foram fatores de risco independentemente associados com a infecção por HPV. Conclusões: Essas adolescentes e jovens primíparas apresentaram elevada prevalência de infecção genital por tipos de alto risco do HPV, mostrando que constituem um grupo de risco para o desenvolvimento de câncer cervical. Contudo, apenas 17,3% apresentaram pelo menos um dos quatro tipos virais presentes na vacina quadrivalente (HPV 6, 11, 16 ou 18), 13,3% apresentaram infecção pelos tipos HPV 16 ou 18, e somente 1,0% apresentou concomitantemente infecção por esses dois tipos virais de alto risco presentes nas vacinas. Portanto, esse estudo indica que a grande maioria dessas jovens primíparas poderia ainda se beneficiar da imunização (catch-up) contra o HPV e constitui um grupo que deve ser alvo de programas efetivos de prevenção primária e secundária para o câncer cervical / Introdution: Genital infection by human papillomavirus (HPV) is a necessary factor in the development of cervical cancer. Vaccines to prevent infection by high risk HPV genotypes 16 and 18 were developed and ideally should be administered before exposure to HPV through sexual contact. Variations in HPV prevalence in different populations and of specific HPV types could affect vaccine recommendations in different settings. Vaccination after first delivery could be a potential strategy for reaching healthy young women depending on the baseline prevalence of high risk genotypes 16 and 18 in this target group. Objectives: The main objective of this study was to determine genital type specific HPV DNA prevalence and selected risk factors associated with HPV infection after the delivery of the first child among young women in a public maternity. Methods: This cross-sectional study was carried out at Hospital Maternidade Leonor Mendes de Barros (HMLMB), one of the largest public maternity hospitals in Sao Paulo. During June 2006 to February 2007, 301 primiparous women aged 15-24 years, who gave birth at that hospital, were included in the study between 43 and 60 days after delivery. Detection of HPV DNA in cervical specimens was performed using a standardized polymerase chain reaction (PCR) protocol with PGMY09/11 primers. To estimate the association of HPV infection with selected risk factors, prevalence ratios (PR) and 95% confidence interval [CI] were estimated using a Generalized Linear Model (GLM) with binomial distribution and log link function. Results: Any HPV DNA was detected in 58.5% (95% CI 52.7%-64.0%) of the enrolled young women. Most common types of HPV found were: HPV16, HPV51, HPV52, HPV58 and HPV71. The overall prevalence of HPV types targeted by the HPV prophylactic vaccines was: HPV16 - 12.0%, HPV18 -2.3% and HPV 6+11- 4.3%. High-risk HPV types were found in 133 (44.2%) women, whereas 43 women (14.3%) had only low-risk HPV types. One hundred and two women (33.9%) were positive for one HPV type only; however, 43 (14.3%) had two types, and 31 (10.3%) had three or more types detected. The multivariate analysis revealed that only age (p for trend =0.020) and smoking habits (p <0.001) were risk factors independently associated with HPV infection. Conclusions: These adolescents and young primiparous women had high cervical HPV prevalence, suggesting that this is a high risk group for cervical cancer development. Nevertheless, 17.3% were positive to any of the four HPV types included in HPV vaccines (HPV6, 11, 16 or 18), with 13.3% positive for HPV 16 or 18, and only 1.0% of them had both vaccine related oncogenic HPV types. Thus, this study supports that the most part of young primiparous women could benefit from catch-up HPV vaccination, and represents a target group for effective primary and secondary cervical cancer prevention programs

Infecções por papilomavírus

Período pós-parto

Vacinas contra papilomavírus

Papillomavirus infections

Papillomavirus vaccines

Postpartum period

Análise clínica e molecular de pacientes não tabagistas e não etilistas com carcinoma epidermóide de cabeça e pescoço / Clinical and molecular analysis of non smoking and non drinking patients with head and neck squamous cell carcinoma

Raquel Ajub Moysés

08 April 2011

O carcinoma epidermóide de cabeça e pescoço (CECP) é um problema de saúde relevante no mundo, por sua prevalência e agressividade. Os papéis do tabaco e do álcool estão bem definidos na sua etiologia, mas uma minoria crescente dos pacientes acometidos pela doença não é tabagista ou etilista. A infecção pelo papilomavirus humano (HPV) parece ser responsável por parte desses casos. Sugere-se que o CECP que acomete pacientes não tabagistas e não etilistas (NTNE) tenha processos carcinogênicos e evolução clínica distintos daqueles de pacientes tabagistas e etilistas (TE). Os objetivos desse estudo foram verificar se os aspectos demográficos, clínicos e histopatológicos de pacientes com CECP são diferentes conforme os hábitos tabágico e etílico; verificar se os CECPs de pacientes NTNE e TE diferem em relação à positividade para HPV; e comparar a sobrevida específica pela doença e a expressão de marcadores biológicos em amostras tumorais e de mucosa normal do trato aerodigestório de pacientes NTNE e de pacientes TE. Para tanto, realizamos estudo transversal de pacientes com carcinomas epidermóides de cavidade oral (exceto lábio), orofaringe, laringe e hipofaringe, prospectivamente incluídos em um banco de tumores de CECP de 2001 a 2009, pelo grupo de pesquisa multi-institucional GENCAPO. Seus dados demográficos, clínicos e patológicos foram analisados conforme os hábitos de tabagismo e etilismo. Através de análise de pareamento, pacientes NTNE e TE foram comparados em relação à sobrevida, à positividade para o HPV no tumor por reação em cadeia da polimerase (PCR) e aos marcadores imunohistoquímicos p53, FHIT, Ki-67, VEGF, EGFR e p16 tanto em amostras tumorais como de epitélio não tumoral. Dos 1633 pacientes selecionados, 80 eram NTNE (4,9%), 1374 TE (84,1%), 140 tabagistas atuais ou no passado mas não etilistas (TNE:8,6%) e 39 apenas etilistas atuais ou no passado, mas não tabagistas (NTE:2,4%). O grupo de pacientes NTNE constituiu-se principalmente por mulheres, preferencialmente idosas, com tumores da cavidade oral, diferentemente de pacientes tabagistas e/ou etilistas (p<0,001). Considerando os diferentes padrões de hábitos, pacientes TE eram geralmente mais jovens (p<0,001), pacientes TNE apresentaram proporcionalmente mais tumores de laringe (p<0,001) e pacientes NTNE apresentaram menor número de parentes de primeiro grau tabagistas (p<0,001). Observou-se um provável efeito do álcool na ocorrência de metástases ganglionares (p<0,001), enquanto o tabaco pareceu relacionar-se a menor grau de diferenciação tumoral à histologia e a menores índices de massa corpórea (p<0,001). Detectou-se a presença de material genético do HPV em 32,8% dos tumores de pacientes NTNE. Desses tumores positivos para o HPV, metade apresentou também hiperexpressão pelo p16. Foi observado menor risco de óbito pela doença em pacientes NTNE quando apresentavam expressão tumoral intensa do p16 (p=0,011 / RR = 0,07; IC 0,01-0,55) e menor sobrevida se apresentavam marcação pelo FHIT em camada basal de margem não tumoral (p= 0,031). Ao comparar pacientes NTNE e TE, não se observaram diferenças na sobrevida específica pela doença ou na positividade para o HPV de forma independente de sexo, idade, sítio tumoral, grau de diferenciação, variante morfológica, estádio T e presença de metástases linfonodais. Pacientes NTNE apresentaram marcação nuclear pelo FHIT em camada basal menos frequentemente do que pacientes TE (p=0,021) / Head and neck squamous cell carcinoma (HNSCC) is a major health problem worldwide, due to its prevalence and aggressiveness. The role of tobacco and alcohol in its etiology is well established; however, a growing minority of patients with HNSCC neither smokes nor consumes alcohol. Human Papillomavirus (HPV) infection seems to be responsible for some of these cases. It is suggested that HNSCC affecting non smoking and non drinking (NSND) patients has different carcinogenesis and outcomes than those in smoking and drinking (SD) subjects. The objectives of this study were to test if demographic, clinical and pathological aspects of patients with HNSCC vary according to smoking and drinking habits; to test if HNSCC in NSND and SD patients differ in terms of HPV positivity; and to compare NSND and SD patients with HNSCC according to survival and biomarkers in tumor and mucosal samples of the aerodigestive tract. We conducted a cross-sectional study of patients with oral cavity (lips excluded), oropharynx, larynx and hypopharynx tumors prospectively included in a multi-institutional HNSCC tumor bank - GENCAPO, from January 2001 to February 2009. Demographic, clinical and pathological data were analyzed in regards of smoking and drinking habits. Using matched-pair analysis, we compared NSND and SD patients in relation to disease-free survival, HPV positivity through polymerase chain reaction (PCR) and Immunohistochemical staining of p53, FHIT, Ki-67, VEGF, EGFR and p16 biomarkers in tumor and mucosal samples. From 1633 patients, 80 were NSND (4.9%), 1374 SD (84.1%), 140 current or past smokers, but non drinkers (SND:8.6%) and 39 current or past drinkers, but non smokers (NSD:2.4%). NSND patients were most frequently women, remarkably elderly, with oral cavity cancers more commonly than the other groups (p<0.001).Comparing to the other groups, SD patients were younger (p<0.001); SND patients were more frequently affected by larynx tumors (p<0.001) and NSND patients had fewer smoking first degree relatives (p<0.001). We observed that alcohol may influence the presence on node metastasis (p<0.001) whereas tobacco may be related to less differentiated tumors and lower body mass indexes (p<0.001). We found HPV DNA in 32.8% of tumors of NSND subjects. Half of the HPV positive tumors were also positive for p16 staining. A lower risk of death from disease was observed among NSND patients with intense p16 staining (p=0.011 / RR = 0.07; CI 0.01-0.55) and lower survival rates in patients with positive nuclear staining for FHIT at the basal layer of mucosal epithelium (p=0.031). We found no differences in disease-free survival of NSND and SD patients in an independent manner of gender, age, tumor site, differentiation grade at histology, pathological variants, T stage and the presence of node metastasis. NSND patients presented less frequently with nuclear staining for FHIT at the basal layer of mucosal epithelium than SD patients (p=0.021)

Alcoolismo

Análise de sobrevida

Carcinoma de células escamosas

Imunoistoquímica

Neoplasias de cabeça e pescoço

Papillomavirus humano

Tabagismo

Alcoholism

Carcinoma squamous cell

Head and neck neoplasms

Human papillomavirus

Immunohistochemistry

Smoking

Survival analysis

Infection with high risk Human Papillomavirus (HRHPV) among HIV-positive women: epidemiology, natural history and impact of combined antiretroviral therapy / Infection par le papillomavirus à haut risque chez les femmes VIH-positives: épidémiologie, histoire naturelle et impact des thérapies antirétrovirales combinées

Konopnicki, Deborah

26 June 2014

L’infection persistante par les papillomavirus (HPV) dits « à haut risque » induit le cancer du col. Chez les femmes infectées par le VIH, les infections par ces HPV oncogènes et les lésions associées, allant des dysplasies au cancer invasif, sont plus fréquentes, plus sévères et de moins bon pronostic que chez les femmes non porteuses du VIH. Etonnamment, alors qu’il a été clairement établi que l’importance de la pathologie liée à HPV est directement proportionnelle au degré d’immunodépression des patientes porteuses du VIH, il n’a pas pu être démontré qu’un traitement antirétroviral efficace contre le VIH permettant d’améliorer l’immunité, diminue l’infection par ces HPV. <p>Entre janvier 2002 et décembre 2012, nous avons constitué une cohorte prospective de dépistage et de suivi de l’infection cervicale par HPV à haut risque incluant plus de 900 femmes traitées à la consultation du Centre de Référence SIDA de l’hôpital Saint-Pierre. Nos résultats montrent que chez ces femmes pour la plupart d’origine Africaine et traitée avec succès pour le VIH depuis plusieurs années, la prévalence et l’incidence de l’infection par HPV oncogène sont beaucoup plus importantes que dans la population belge générale ou que chez les femmes séropositives vivant dans d’autres pays occidentaux. Grâce à un suivi longitudinal de plusieurs années, nous avons pu démontrer que le risque d’être infectée par un HPV oncogène est significativement réduit sous trithérapie anti-VIH sous réserve d’obtenir une charge virale indétectable à <50 cp/ml pendant plus de 3 ans ou une restauration immunitaire à >500 lymphocytes CD4+/µL pendant plus d’un an et demi. Ces résultats ont été confirmés dans l’analyse que nous avons faite sur les nombreuses dysplasies cervicales également retrouvées dans notre cohorte. Enfin, nous avons trouvé que la distribution des génotypes d’HPV de nos patientes est similaire à celle trouvée en Afrique sub-saharienne impliquant que la couverture offerte par les vaccins anti-HPV varie entre moins de 30% pour les vaccins bi- ou quadrivalent actuellement disponibles à 80% pour le vaccin nanovalent en développement. Notre travail met en lumière l’étendue particulièrement importante de l’infection par HPV à haut risque chez les femmes séropositives vivant en Belgique et offre de nouveaux éléments de réflexion afin d’adapter à leurs particularités les recommandations belges et les critères de remboursement à la fois pour le dépistage du cancer cervical et la vaccination anti-HPV.<p>/<p>Persistent infection with human papillomavirus (HPV) called “at high risk” induces cervical cancer. In HIV-positive women, infection with these oncogenic HPV and HPV-induced lesions ranging from cervical dysplasia to invasive cancer are more frequent, more severe and have a worst outcome than in HIV-negative women. An intriguing paradox is that, although it has been clearly demonstrated that high risk HPV infection and associated diseases are increased by progressive immune deficiency, the introduction of efficient therapy against HIV leading to improved immunity has not been associated with a decrease in oncogenic HPV infection or HPV-induced lesions.<p>Between January 2002 and December 2012, we have built a prospective cohort to screen and follow-up cervical infection by high risk HPV in more than 900 women treated for HIV in the AIDS Reference centre of Saint-Pierre Hospital. We have shown that among these women mainly from Sub-Saharan African origin and successfully treated for HIV for several years, the prevalence and incidence rate of high risk HPV are much higher than in the general population from Belgium or in HIV-positive women from other western countries. After several years of longitudinal follow up, we have demonstrated that the risk of infection by oncogenic HPV is significantly reduced by efficient therapy against HIV provided that HIV viral load has been sustainly suppressed below 50 cp/ml for more than 3 years or that immunity has been increased more than 500 CD4+T cells/µl for more than 1.5 years. These results have been confirmed in the analysis on cervical dysplasia which is also very prevalent in our cohort. At last, we have found that the HPV genotype distribution in our population is very similar to the one found in Sub-Saharan Africa. We have estimated that the coverage offered by the vaccines against HPV in our cohort is less than 30% for the currently available bi- or quadrivalent vaccine but reaches 80% with the future nanovalent vaccine. Our results highlight many differences in the HPV infection and associated diseases in HIV-positive women compared to HIV-negative women; these differences should be taken into account to adapt to our specific population the current Belgian guidelines or the reimbursement criteria on cervical screening and on vaccines against HPV. <p> / Doctorat en Sciences médicales / info:eu-repo/semantics/nonPublished

Médecine pathologie humaine

Papillomavirus diseases

HIV-positive women

Antiretroviral agents

Dysplasia

Maladies à papillomavirus

Séropositives

Antirétroviraux

Dysplasie

women

HIV

cervical cancer

cervical dysplasia

HPV

genotype

Analyse et caractérisation moléculaire de l'hypoxie intratumorale de carcinomes épidermoïdes de l'oropharynx / Analysis and molecular characterisation of tumor hypoxia in the oropharyngeal squamous cell carcinoma

Hanns, Elodie

18 September 2014

Les carcinomes épidermoïdes des voies aéro-digestives supérieures (VADS) se situent au sixième rang des cancers les plus fréquents dans le monde. Ces tumeurs sont liés à deux facteurs de risque : l’intoxication éthylo-tabagique (80% des cas) et l’infection de l’épithélium des VADS par les papillomavirus humain (HPV) à haut risque oncogène (20% des cas). Ces derniers définissent une sous-population de patients de meilleur pronostic. Une des hypothèses actuellement étudiées, afin d’expliquer la survie améliorée des patients HPV positifs, serait une hypoxie moindre dans ces tumeurs. En effet, les tumeurs des VADS sont fréquemment hypoxiques, et l’hypoxie intratumorale est un facteur de mauvais pronostic. Dans une première partie de cette thèse, nous avons entrepris une caractérisation moléculaire de l’hypoxie intratumorale dans les tumeurs humaines oropharyngées en fonction du statut HPV. Il apparaît que les tumeurs HPV positives présentent un statut hypoxique moindre comparées aux tumeurs HPV négatives. Ces tumeurs se caractérisent également par une abondante vascularisation intratumorale, qui pourrait être à l’origine de ce statut hypoxique moindre. Dans une deuxième partie, nous avons étudié l’adaptation à l’hypoxie de la lignée cellulaire HPV négative SQ20B et la lignée cellulaire HPV positive SCC90. De plus, des modèles de xénogreffes ont été établis à partir de ces mêmes lignées cellulaires et ont été analysés du point de vue de l’hypoxie intratumorale. De façon comparable aux tumeurs HPV positives, les xénogreffes obtenus à partir de la lignée SCC90 montre un statut hypoxique réduit comparés aux xénogreffes SQ20B. Les deux lignées cellulaires s’adaptent également différemment en hypoxie in vitro. La réponse à l’hypoxie dans la lignée SCC90 semble plus dynamique. En effet, la lignée SCC90 tente de s’adapter et de répondre à cet environnement hypoxique en induisant de fort niveau d’expression de gènes comparée à la lignée SQ20B. / Head and neck squamous cell carcinoma (HNSCC) represents the sixth most common malignancy worldwide. The major risk factors for HNSCC identified are tobacco use and alcohol consumption (80% of all HNSCC), which seem to have a synergistic effect. A subgroup of HNSCCs (20% of cases), particularly those of the oropharynx, is caused by infection with high-risk types of human papillomavirus (HPV). Human papillomavirus HPV-related oropharyngeal squamous cell carcinoma defines a distinct clinical subgroup of head and neck cancer patients with improved prognosis. Currently, one of the several hypothesis studied to account for their improved survival outcomes could be a distinct hypoxia status compared to their HPV-negative counterpart. Indeed, tumour hypoxia is common in solid tumours including head and neck tumours, and hypoxia is a well-known poor prognosis factor. In first part of this thesis, we have performed a molecular characterisation of tumor hypoxia on cohort of oropharyngeal tumours according to HPV status of the patients. The results support the hypothesis that HPV-related tumours display a lesser hypoxia status compared to HPV-negative oropharyngeal tumours. These HPV-related tumours also characterize by an abundant tumour vascularisation, which could be responsible for a lesser hypoxia status. In a second part, we have studied the ability of the adaptation to hypoxia of the HPV-positive SCC90 cell line and HPV-negative SQ20B cell line. Furthermore, HPV-positive and HPV-negative HNSCC xenograft models have been established and have been analysed about tumor hypoxia. Similar to HPV-related HNSCC, tumours-derived HPV positive cell lines display a reduced hypoxic status compared to tumours-derived HPV negative cell lines. The two cell lines adapt also differently to in vitro hypoxia. In the HPV-positive cell line, the hypoxia response pathways could be more dynamics. Indeed, SCC90 cell lines attempt to adapt and to reply to hypoxic environment inducing highly expression of all of the hypoxia related genes compared to SQ20B cell lines.

Cancer des VADS

Oropharynx

Papillomavirus humain

Hypoxie tumorale

Head and neck squamous cell carcinoma

Oropharyngeal squamous cell carcinoma

Human papillomavirus

Hypoxia

572.8

616.99

Occurrence of high risk human papillomaviruses and cervical cancer among fertile-aged women in Finland

Laukkanen, P. (Päivi)

04 December 2012

Abstract High risk human papilloma virus (hrHPV) infection is a necessary but not a sufficient cause of cervical cancer. In Finland, since 1990 the incidence of cervical cancer has increased among women younger than 40 years of age despite a nationwide screening programme. In this thesis, the overall objective is to address the role of possible, earlier hrHPV epidemic in this increased incidence of cervical cancer. The target population includes all fertile-aged women in Finland during 1983–2006. The actual study population comprised all women with a minimum of two pregnancies within five years and under 32 years of age in 1983–1997 and under 29 years of age in 1995–2003 identified from the Finnish Maternity Cohort (FMC). From this subpopulation, two subcohorts were selected for hrHPV antibody analysis by random sampling stratified by age and calendar time. All cases of cervical cancer diagnosed for women under 50 years of age during 1983–2002 and 1986–2006 were identified from the Finnish Cancer Registry. The case-cohort design, used for estimating population attributable fractions (PAF) associated with hrHPV, included the cases of cervical cancer and the first subcohort of FMC. A steady annual increase of 0.7% per year in the incidence of HPV16 was estimated to have taken place in Finland from 1983 to 1997 among the 23–31-year-old women with at least two pregnancies. The estimated seroprevalence of HPV16 increased from 17% to 24%, respectively. The PAF of hrHPV exposures in squamous cell carcinoma of the uterine cervix (SCC) was estimated as 73% (95% CI: 13% to 93%). For 26–31-year-old women born in the 1960s and 1970s the incidence of SCC was roughly double compared with women born in the late 1950s. Mathematical modelling indicated that changes in the sexual behaviour partly accounted for the increase seen in the incidence of cervical cancer in the 1990s. The findings of this thesis indicate that growth in the background exposure to HPV16 preceded the increase of incidence of cervical cancer in Finland. At younger birth cohorts, the increase of the incidence of SCC is visible among fertile-aged women in Finland. Whether overall screening starting at 25 years of age, higher participation rate for cervical screening or HPV vaccination of early adolescents is the future solution to lowering the incidence of cervical cancer among young women remains to be seen. / Tiivistelmä Ihmisen papilloomaviruksen (HPV), erityisesti korkean riskin tyypin (hrHPV), aiheuttama infektio on kohdunkaulan syövän välttämätön, mutta ei riittävä syytekijä. Suomessa vuoden 1990 jälkeen kohdunkaulan syövän ilmaantuvuus on valtakunnallisesta seulonnasta huolimatta noussut alle 40-vuotiailla naisilla. Tämän väitöskirjan tavoitteena on osoittaa, mikä rooli mahdollisella aiemmalla hrHPV-epidemialla on kyseiseen kohdunkaulan syövän ilmaantuvuuden kasvuun. Tutkimuksen kohdeväestöön kuuluvat kaikki lisääntymisikäiset suomalaiset naiset. Varsinainen tutkimusväestö koostui kaikista vuosina 1983–97 alle 32-vuotiaana ja vuosina 1995–2003 alle 29-vuotiaana kaksi kertaa raskaana olleista naisista, jotka identifioitiin Suomen äitikohortista (FMC). Tästä joukosta valittiin satunnaisotannalla kaksi alikohorttia hrHPV-laboratorioanalyysejä varten. Kaikki vuosina 1983–2002 ja 1986–2006 kohdunkaulan syöpädiagnoosin alle 50-vuotiaana saaneet naiset poimittiin Suomen syöpärekisteristä. Tapaus-kohorttiasetelma, jota käytettiin hrHPV altistukseen liittyvien väestösyyosuuksien (PAF) estimoinnissa, sisälsi kohdunkaulan syöpätapaukset ja ensimmäisen alikohortin. Suomalaisten 23–31 -vuotiaiden, vähintään kahdesti raskaana olleiden, naisten vuosittainen HPV16-ilmaantuvuus kasvoi tasaisesti 0.7&#160;% per vuosi ajanjaksolla 1983–1997. Vastaavasti HPV16:n vallitsevuus kasvoi 17 prosentista 24 prosenttiin. Kohdunkaulan levyepiteelisyövän hrHPV-altistukseen liittyvän PAF:n estimoitiin olevan 73&#160;% (95&#160;%:n luottamusväli 13–93&#160;%). Levyepiteelisyövän ilmaantuvuus oli suunnilleen kaksinkertainen 1960- ja 1970-luvulla syntyneillä naisilla, heidän ollessaan 26–31 -vuotiaita, verrattuna 1950-luvulla syntyneisiin samanikäisiin naisiin. Matemaattisen mallinnuksen tulosten perusteella kohdunkaulan syövän ilmaantuvuuden nousu 1990- luvulla selittyy ainakin osittain sukupuolikäyttäytymisen muutoksilla. Tämän väitöskirjan tulokset osoittavat, että kasvanut HPV16-virukselle altistuminen edelsi kohdunkaulan syövän ilmaantuvuuden nousua Suomessa. Levyepiteelisyövän ilmaantuvuuden nousu nuorimmissa syntymäkohorteissa on nähtävissä lisääntymisikäisillä naisilla Suomessa. Tulevaisuudessa nähdään, onko seulonnan aloittaminen 25-vuotiaana, korkeampi seulontaan osallistumisosuus vai nuorten aikuisten HPV-rokottaminen ratkaisu nuorten naisten kohdunkaulan syövän ilmaantuvuuden vähentämiseksi.

cohort studies

human papillomavirus 16

incidence

papillomavirus infections

squamous cell carcinoma

stastitical models

uterine cervical neoplasms

epidemiologia

kohdunkaulansyöpä

kohorttitutkimus

papilloomavirus

tilastolliset mallit

Evaluación costo-efectividad de dos alternativas de vacunación para el virus del papiloma humano en la prevención del cáncer cervical uterino

Bolaños-Díaz, Rafael, Tejada, Romina A, Beltrán, Jessica, Escobedo-Palza, Seimer

09 1900

Objetivos. Determinar la relación costo-efectividad de la vacunación contra el (virus del papiloma humano) VPH y el tamiz de lesiones cervicales, frente a un programa de tamiz solo. Materiales y métodos. Se realizó una evaluación costo-efectividad y se empleó un modelo de Markov, con un horizonte temporal de 70 años y tres alternativas de prevención para el (cáncer del cuello uterino) CCU (tamiz solo, tamiz + vacuna bivalente, y tamiz + vacuna cuadrivalente), en una cohorte hipotética de niñas de diez años, desde la perspectiva del Ministerio de Salud. Resultados. La vacunación contra el VPH y tamiz es más costo-efectiva que el tamiz solo a partir de una voluntad de pago de S/ 2000 (USD 1 290,32). En el análisis determinístico, la vacuna bivalente es marginalmente más costo-efectiva que la vacuna cuadrivalente (S/ 48 [USD 30,97] frente a S/ 166 [USD 107,10] por AVAC, respectivamente). Sin embargo, en el análisis probabilístico ambas intervenciones generan nubes de puntos superpuestos, con una tendencia de la vacuna cuadrivalente a ser más costo-efectiva. Es decir, ambas son costo-efectivas y, por ende, intercambiables. El modelo fue especialmente sensible a variaciones de la cobertura y en la prevalencia de infección persistente por genotipos oncológicos no incluidos en la vacuna. Conclusiones. A partir de una disponibilidad de pago de S/ 2000 [USD 1 290,32] el tamiz y la vacunación son más costo-efectivos que el tamiz solo. La diferencia de costo-efectividad entre ambas vacunas carece de robustez probabilística y ambas vacunas pueden considerarse intercambiables desde la perspectiva costo-efectividad. / Objectives. To determine the cost-effectiveness of human papillomavirus (HPV) vaccination and cervical lesion screening versus screening alone for the prevention of uterine cervical cancer (UCC). Materials and methods. This cost-effectiveness evaluation from the perspective of the Ministry of Health employed a Markov model with a 70-year time horizon and three alternatives for UCC prevention (screening alone, screening + bivalent vaccine, and screening + quadrivalent vaccine) in a hypothetical cohort of 10-year-old girls. Results. Our model, which was particularly sensitive to variations in coverage and in the prevalence of persistent infection by oncologic genotypes not included in the vaccine, revealed that HPV vaccination and screening is more cost-effective than screening alone, assuming a payment availability from S/ 2 000 (US dollars (USD) 1 290.32) per subject. In the deterministic analysis, the bivalent vaccine was marginally more cost-effective than the quadrivalent vaccine (S/ 48 [USD 30.97] vs. S/ 166 [USD 107.10] per quality-adjusted life-year, respectively). However, in the probabilistic analysis, both interventions generated clouds of overlapping points and were thus cost-effective and interchangeable, although the quadrivalent vaccine tended to be more cost-effective. Conclusions. Assuming a payment availability from S/ 2000 [USD 1,290.32], screening and vaccination were more cost-effective than screening alone. The difference in cost-effectiveness between the two vaccines lacked probabilistic robustness, and therefore the vaccines can be considered interchangeable from a cost-effectiveness perspective.

Vacunas contra papillomavirus

Neoplasias del cuello uterino

Condiloma acuminado

Análisis costo-beneficio

Papillomavirus vaccines

Cervical intraepithelial neoplasia

Condylomata acuminata

Cost-benefit analysis