Human Papilloma Virus: Prevalence, distribution and predictive value to lymphatic metastasis in penile carcinoma

Fonseca, Aluizio Gonçalves da; Soares, Fernando Augusto; Burbano, Rommel Rodriguez; Silvestre, Rodrigo Vellasco; Pinto, Luis Otávio Amaral Duarte

doi:10.1590/S1677-5538.IBJU.2013.04.12

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Original Article • Int Braz J Urol 39 (4) • Jul-Aug 2013 • https://doi.org/10.1590/S1677-5538.IBJU.2013.04.12 copy

Human Papilloma Virus: Prevalence, distribution and predictive value to lymphatic metastasis in penile carcinoma

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Objectives

To evaluate the prevalence, distribution and association of HPV with histological pattern of worse prognosis of penile cancer, in order to evaluate its predictive value of inguinal metastasis, as well as evaluation of other previous reported prognostic factors.

Material and Methods

Tumor samples of 82 patients with penile carcinoma were tested in order to establish the prevalence and distribution of genotypic HPV using PCR. HPV status was correlated to histopathological factors and the presence of inguinal mestastasis. The influence of several histological characteristics was also correlated to inguinal disease-free survival.

Results

Follow-up varied from 1 to 71 months (median 22 months). HPV DNA was identified in 60.9% of sample, with higher prevalence of types 11 and 6 (64% and 32%, respectively). There was no significant correlation of the histological characteristics of worse prognosis of penile cancer with HPV status. Inguinal disease-free survival in 5 years did also not show HPV status influence (p = 0.45). The only independent pathologic factors of inguinal metastasis were: stage T ≥ T1b-T4 (p = 0.02), lymphovascular invasion (p = 0.04) and infiltrative invasion (p = 0.03).

conclusions

HPV status and distribution had shown no correlation with worse prognosis of histological aspects, or predictive value for lymphatic metastasis in penile carcinoma.

Penile Neoplasms; Humans; Prevalence; Lymphatic Metastasis; Biological Markers

INTRODUCTION

Epidermoid carcinoma of penis (ECP) is a rare neoplasm, but with high incidence in underdeveloped countries (¹1. Backes DM, Kurman RJ, Pimenta JM, Smith JS: Systematic review of human papillomavirus prevalence in invasive penile cancer. Cancer Causes Control. 2009; 20: 449-57.). In Brazil, the incidence varies from 2.9 to 6.8 cases/100.000 inhabitants/year (²2. Favorito LA, Nardi AC, Ronalsa M, Zequi SC, Sampaio FJ, Glina S: Epidemiologic study on penile cancer in Brazil. Int Braz J Urol. 2008; 34: 587-91; discussion 591-3.). In an epidemiological study in Pará State, the observed incidence was 5.7 cases/100.000 inhabitants/year (³3. Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90.).

Its etiology is associated with several risk factors, including presence of prepuce, bad hygienic habits, chronic dermatitis and smoking. However, the most extensively studied factor is human papilloma virus infection (HPV) (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.).

HPV has more than 100 subtypes that can be classified as with low (HPVlow) or high risk (HPVhigh) oncogenic potential (⁵5. Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.). Its role in cervical uterine cancer is well established, but its association with ECP is still being discussed.

In patients with ECP, the presence of HPV varies from 15% to 80% suggesting that only a subgroup of these tumors is associated with HPV infection (⁶6. Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50.).

Natural history of the disease is characterized by progressive invasion of surrounding penile tissues, and posteriorly metastatic dissemination to inguinal lymph nodes (⁶6. Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50.). Lymph node involvement is the prognostic factor of worst impact on prognosis of disease-specific survival (⁶6. Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50.) and the analysis of this involvement is very important in order to determine the cure of the disease.

Nowadays, the available methods for staging regional lymph node involvement have low accuracy. For example, Gonzaga-Silva et al., using gamma probe in the sentinel lymph node, showed sensitivity of only 25% and 42.8% of false negative results (⁷7. Gonzaga-Silva LF, Tavares JM, Freitas FC, Tomas Filho ME, Oliveira VP, Lima MV: The isolated gamma probe technique for sentinel node penile carcinoma detection is unreliable. Int Braz J Urol. 2007; 33: 58-63; discussion 64-7.).

The physical exam of inguinal region (inspection and palpation) is also inconclusive, since half the cases with lymph node involvement does not present tumor. Also, 20% of patients without lymph node detected during physical exam present local micrometastasis (⁸8. Pettaway CA, Horenblas S: Penile cancer: incremental insights into etiology, diagnosis, staging, and management. World J Urol. 2009; 27: 139-40.).

Inguinal lymph node involvement is the most accurate method of staging to diagnose occult metastasis. However, it has significant morbidity and does not benefit a relevant subgroup of patients without metastasis (⁸8. Pettaway CA, Horenblas S: Penile cancer: incremental insights into etiology, diagnosis, staging, and management. World J Urol. 2009; 27: 139-40.).

In literature, several histological factors of the primary lesion were identified with predictive value of inguinal metastasis. These include: differentiation grade, tumor staging, and presence of neurovascular and lymph vascular invasion, with independent prognostic importance (⁹9. BE Stephen, BR David, CC Carolyn, GF April, LG Frederick, T Andy, III: AJCC Cancer Staging Manual. Philadelphia, Lippincott. 2010; Seventh Edition, 2010; pp.447.).

Although HPV infection is associated with the most aggressive histological subtypes, its value as a predictive factor of lymph node metastasis and prognosis is still debated (¹⁰10. Cubilla AL: The role of pathologic prognostic factors in squamous cell carcinoma of the penis. World J Urol. 2009; 27: 169-77.).

The present study was conducted in a group of patients from Northern region of Brazil (Pará State), in order to evaluate the prevalence, distribution and association of HPV infection with histological pattern of worse prognosis in ECP and to determine its possible predictive value of lymph node metastasis.

MATERIALS AND METHODS

Patients

This study, as well as its consent inform, was approved by the Local Ethical Committee. Eighty-two patients with ECP were treated at the Hospital Ophir Loyola, Belém - Pará, from 2001 to 2008. The patients were submitted to penile amputation and the analysis of the lymph nodes followed a protocol proposed by the Urologic Department of the Hospital. All patients were prospectively evaluated, by follow-up appointments, medical files charts or telephonic contact of relatives.

Treatment protocol

Lymph node resection was performed after 4 to 6 weeks of the penile surgery. During this interval patients received antibioticotherapy with fluoroquinolones. For the patients with palpable inguinal lymph nodes after the antibiotic treatment it was performed bilateral superficial lymph node resection with freezing histological samples. Patients with T2-T4 staging and/or G2-G3 differentiation grade (according to TNM 2009 UICC System of Staging and Pathology) were also submitted to superficial bilateral lymph node resection.

In the presence of tumor involvement of superficial lymph nodes, radical lymphadenectomy was performed. Pelvic lymphadenectomy was performed in all cases with deep inguinal lymph node invasion.

The surgery was not performed in patients with Tis or T1, G1 staging, without lymph vascular invasion or palpable lymph nodes. These patients followed a careful ambulatory schedule of surveillance for at least five years.

Pathological Analysis

All samples were revised blindly by a single pathologist. The tumors were retrospectively staged according to 2009 TNM System.

Lymph vascular invasion (LVI) was defined as the presence of tumor cells in the interior of lymphatic veins, blood veins or arteries. Perineural invasion (PNI) was determined as the presence of tumor tissue next to peripheral nerve branches. As for invasion, the tumor was considered “infiltrative”, when it was observed the presence of branches of malignant cells within the stroma, or “pushing”, when it was observed an interface between the tumor and the host cells.

Histological subtypes were classified as usual, condylomatous, verrucous, basaloid, papillary, sarcomatoid and acantholysis.

HPV Analysis

This part of the study was developed by the Papilloma Virus Laboratory of Instituto Evandro Chagas, a HPV referential laboratory of Brazilian Ministry of Health.

Parafin blocks were serially cut by microtome and the cuts were used for viral DNA detection.

Samples were submitted to polimerase chain reaction (PCR) using initially human beta globin G73 - 5′GAA GAG GGA AGG ACA GGT AC 3′ e G74 - 5′ CAA CTT CAT CCA CGT TCA CC 3′ (PCR).

Viral gene specific reaction used the initiators GP5+ - 5′ TTT GTT ACT GTG GTA GAT ACT AC 3′ e GP6+ - 5′ GAA AAA TAA ACT GTA AAT CAT ATT C 3′, that were able to amplify a 150pb fragment of the L1 gene, that corresponds to a well preserved region of the virus genome.

After PCR, the identification of the virus was carried out using direct sequencing of the PCR product, using a capillary sequencer ABI 3130 Genetic analyser, Hitachi^©.

The presence of HPV was classified in three subgroups:

HPVhigh - infection by one or more high risk virus

HPVlow - infection by one or more low risk virus

HPVmult - presence of more than one subtype of virus in the sample, whether of high or low risk.

Follow-up and statistical analysis

Follow-up of patients was carried out through periodic ambulatory evaluations, quarterly in the first two years after surgery, and then semiannually.

The presence or absence of HPV infection, as well the presence of subgroups HPVhigh, HPVlow and HPVmult were related to several clinical and pathological variables, using the Chi-Square method or Fisher exact test.

The presence of inguinal metastasis was correlated to: pT, G, LVI, PNI, Infiltratative, Pushing, histological subtype and HPV status, using univariate and multivariate analysis by Cox proportional hazard method.

The analysis of inguinal disease-free interval (IDFI) in five years used the Kaplan-Meier method and the log Rank test. SPSS® 13.0 was used for all analyses, and the result was considered significant if p < 0.05.

RESULTS

Median age of patients was 58 years (22-91 years) and follow-up ranged from 1 to 71 months (median 20 months).

* MISSING SECTION HEADING *

Presence of HPV DNA

HPV DNA was detected in 60.9% (50/82) fixed samples in paraffin. Viral distribution was: HPV11 (64%), HPV6 (32%), HPV16 (30%), HPV53 (18%), HPV33 (4%) and subtypes 18, 68, 45, 51, 52 and 58 (2%).

Subgroups HPVhigh, HPVlow and HPVmult were identified in 12/50 (24%), 25/50 (50%) and 25/50 (50%) respectively. Viral types that predominated in each group were 16, 11 and 11.

Histological characteristics of subgroups HPV positive (HPVhigh, HPVlow and HPVmult) and HPV negative

Patients without HPV infection had predominantly infiltrative invasion. HPV positive group was correlated to more differentiated tumors (Table-1).

Thumbnail

Table 1
- Histopathological characteristics of 82 patients with penile cancer according to HPV positive (n = 50) or negative (n = 32), HPVhigh (n = 12), HPVlow (n = 25) and HPVmult (n = 25) groups.

HPVhigh was associated more frequently to basaloid subtype, and rarely was present in patients with usual pattern. There was also a low prevalence of HVPhigh in patients with more advanced penile carcinoma (Table-1).

Most patients with usual pattern were infected by HPVlow. Condylomatous type was associated more frequently to HPVmult infection (Table-1).

Multiple logistic regression analysis did not show any histological variable independently related to status or HPV subgroup.

Inguinal metastasis-free survival in five years and risk factor, according to histological patterns

It was observed 56% of inguinal involvement of metastasis (46/82 patients). Inguinal metastasis-free survival (IMFS) probability in five years showed no difference between the positive and negative HPV groups (34% × 29%, p = 0.45) - Figure-1.

Figure 1
Inguinal metastasis-free survival after treatment of the primary tumor showed no significant differences between hpv positive tumors (n50/82) or negative hpv tumors (n32/82), p = 0.45.

Likewise, there was no statistical significant difference of IMFS among the groups HPVhigh, HPVlow and HOVmult (Table-2).

Thumbnail

Table 2
- Inguinal metastasis-free survival index in 5 years and risk rate according to clinical and pathological variables – univariate analysis

Univariate analysis of IMFS in five years, according to histopatological patterns, showed that stage T ≥ T1b-T4 (HR = 5.76), LVI (HR = 2.90), PNI (HR = 2.88), and infiltrative invasion (HR = 2.68) were, decreasingly, strong predictors of inguinal metastasis, respectively 82.6% (38/52), 100% (11/11), 94.4% (17/18) and 70.2% (33/47) (Table-2).

Only sarcomatoid subtype was related to regional metastasis (4/5). Papillary subtype showed negative correlation to metastasis in 100% (0/5).

Multivariated analysis showed that T ≥ T1b-T4, LVI and infiltrative invasion were strong independent predictors of inguinal metastasis (Table-3).

Thumbnail

Table 3
- Inguinal metastasis-free survival index in 5 years and risk rate according to clinical and pathological variables - multivariate analysis.

DISCUSSION

The present study is the first scientific report of the presence of HPV and its genotype variants correlated to ECP in a northern state of Brazil, a region with high prevalence of the disease.

In this sample, HPV prevalence in patients with ECP was 60.9%, in accordance to literature. It is reported a variation of 14% to 100% (¹¹11. Miralles-Guri C, Bruni L, Cubilla AL, Castellsagué X, Bosch FX, de Sanjosé S: Human papillomavirus prevalence and type distribution in penile carcinoma. J Clin Pathol. 2009; 62: 870-8.). Miralles-Guri et al. metanalysis in 2009, comprasing 30 studies and 1266 patients with ECP reported a HPV DNA prevalence of 47.9%. In South America, viral DNA was specifically found in 40.7% of tumors (¹²12. Bezerra AL, Lopes A, Santiago GH, Ribeiro KC, Latorre MR, Villa LL: Human papillomavirus as a prognostic factor in carcinoma of the penis: analysis of 82 patients treated with amputation andbilateral lymphadenectomy. Cancer. 2001; 91: 2315-21.).

As for the genotype distribution, in our sample there was a clear prevalence of types 11 and 6, contrary to the previous report of Bezerra et al., that reported an absolute prevalence of type 16 (¹²12. Bezerra AL, Lopes A, Santiago GH, Ribeiro KC, Latorre MR, Villa LL: Human papillomavirus as a prognostic factor in carcinoma of the penis: analysis of 82 patients treated with amputation andbilateral lymphadenectomy. Cancer. 2001; 91: 2315-21.). We also registered infection by multiple HPV genotypes in 30.4% (25/50), contrary to the study by Krustrup et al., that did not show multiple viral infections in their sample (¹³13. Krustrup D, Jensen HL, van den Brule AJ, Frisch M: Histological characteristics of human papilloma-virus-positive and -negative invasive and in situ squamous cell tumours of the penis. Int J Exp Pathol. 2009; 90: 182-9.).

Variations of the reported prevalence of DNA HPV are mainly due to different techniques of sampling, studied population, detection methods, tumoral tissue storage and inclusion of multiple histological subtypes (¹⁴14. Anic GM, Giuliano AR: Genital HPV infection and related lesions in men. Prev Med. 2011; 53: S36-41.).

The role of HPV in epithelium carcinogenesis of uterine cervix is well established. In more than 95% of patients it is observed several high risk subtypes of virus infection (¹⁵15. Rubin MA, Kleter B, Zhou M, Ayala G, Cubilla AL, Quint WG, et al.: Detection and typing of human papillomavirus DNA in penile carcinoma: evidence for multiple independent pathways ofpenile carcinogenesis. Am J Pathol. 2001; 159: 1211-8.); however, in ECP, the viral infection is not mandatory and there are several other causes not related to HPV infection (¹⁵15. Rubin MA, Kleter B, Zhou M, Ayala G, Cubilla AL, Quint WG, et al.: Detection and typing of human papillomavirus DNA in penile carcinoma: evidence for multiple independent pathways ofpenile carcinogenesis. Am J Pathol. 2001; 159: 1211-8.). Relation of genital tumors and HPVhigh is stimulating research and interest of the biological potential viral interference on metastasis and disease prognosis.

Several authors tried to relate viral infection and histological pattern of worse prognosis (¹⁶16. Scheiner MA, Campos MM, Ornellas AA, Chin EW, Ornellas MH, Andrada-Serpa MJ: Human papillomavirus and penile cancers in Rio de Janeiro, Brazil: HPV typing and clinical features. Int Braz J Urol. 2008; 34: 467-74; discussion 475-6.

17. Lont AP, Kroon BK, Horenblas S, Gallee MP, Berkhof J, Meijer CJ, et al.: Presence of high-risk human papillomavirus DNA in penile carcinoma predicts favorable outcome in survival. Int J Cancer. 2006; 119: 1078-81.-¹⁸18. Kirrander P, Kolaric A, Helenius G, Windahl T, Andrén O, Stark JR, et al.: Human papillomavirus prevalence, distribution and correlation to histopathological parameters in a large Swedish cohort ofmen with penile carcinoma. BJU Int. 2011; 108: 355-9.). Scheiner et al. (¹⁶16. Scheiner MA, Campos MM, Ornellas AA, Chin EW, Ornellas MH, Andrada-Serpa MJ: Human papillomavirus and penile cancers in Rio de Janeiro, Brazil: HPV typing and clinical features. Int Braz J Urol. 2008; 34: 467-74; discussion 475-6.), Lont et al. (¹⁷17. Lont AP, Kroon BK, Horenblas S, Gallee MP, Berkhof J, Meijer CJ, et al.: Presence of high-risk human papillomavirus DNA in penile carcinoma predicts favorable outcome in survival. Int J Cancer. 2006; 119: 1078-81.) and Kirrander et al. (¹⁸18. Kirrander P, Kolaric A, Helenius G, Windahl T, Andrén O, Stark JR, et al.: Human papillomavirus prevalence, distribution and correlation to histopathological parameters in a large Swedish cohort ofmen with penile carcinoma. BJU Int. 2011; 108: 355-9.) did not find such evidence. However, Gregoire et al. (¹⁹19. Gregoire L, Cubilla AL, Reuter VE, Haas GP, Lancaster WD: Preferential association of human papillomavirus with high-grade histologic variants of penile-invasive squamous cellcarcinoma. J Natl Cancer Inst. 1995; 87: 1705-9.) and Krustrup et al. (¹³13. Krustrup D, Jensen HL, van den Brule AJ, Frisch M: Histological characteristics of human papilloma-virus-positive and -negative invasive and in situ squamous cell tumours of the penis. Int J Exp Pathol. 2009; 90: 182-9.) reported a significant statistical association between HPVhigh infection and high risk tumors. Our studied showed that the only positive association was between the prevalence of HPVhigh in 75% of basaloid tumors, with worse prognosis. Cubilla et al. (²⁰20. Cubilla AL, Lloveras B, Alejo M, Clavero O, Chaux A, Kasamatsu E, et al.: The basaloid cell is the best tissue marker for human papillomavirus in invasive penile squamous cell carcinoma: a study of202 cases from Paraguay. Am J Surg Pathol. 2010; 34: 104-14.) reported the same association.

Guimaraes et al. evaluated 14 cases of basaloid tumors, and reported 50% of inguinal metastasis. In our sample we observed 75% (3/4 patients) (²¹21. Guimaraes G, Werneck da Cunha I, Soares F, Lopez A, Torres JJ, Chaux A, et al.: WHO histological classiWcation, regional metástasis and outcome in 375 surgically treated patients with penile SCC. Mod Pathol. 2007; 20: 150A.). Despite the small number of patients with this histological subtype of tumor, we believe that this association should be more investigated hereafter.

The recommendations for lymphadenectomies without the presence of inguinal lymph node disease are based upon predictive factors related to the primary lesion, mainly tumor stage and cellular differentiation grade. However, overtreatment can reach 82% of cases (²²22. Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60.). In our sample, this was observed in 88% (30/34) even with the use of a strict protocol. It is necessary to search for non-invasive biomarkers with good accuracy, to predict the risk of metastatic lymph node involvement in patients with penile cancer (²²22. Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60. ²³23. Kroon BK, Valdés Olmos RA, van Tinteren H, Nieweg OE, Horenblas S: Reproducibility of lymphoscintigraphy for lymphatic mapping in patients with penile carcinoma. J Urol. 2005; 174: 2214-7.). In our series, there was no association between the presence or distribution of HPV genotype with lymph node disease, as reported by other authors (¹³13. Krustrup D, Jensen HL, van den Brule AJ, Frisch M: Histological characteristics of human papilloma-virus-positive and -negative invasive and in situ squamous cell tumours of the penis. Int J Exp Pathol. 2009; 90: 182-9. ¹⁹19. Gregoire L, Cubilla AL, Reuter VE, Haas GP, Lancaster WD: Preferential association of human papillomavirus with high-grade histologic variants of penile-invasive squamous cellcarcinoma. J Natl Cancer Inst. 1995; 87: 1705-9.). At present, there are no evidences indicating the use of HPV detection in order to decide to perform lymphadenectomies. Surprisingly, Lont et al., although failed to associate HPV status and lymph node metastasis, showed better specific-disease survival in patients with ECP associated with high risk virus (p = 0.03) (¹⁷17. Lont AP, Kroon BK, Horenblas S, Gallee MP, Berkhof J, Meijer CJ, et al.: Presence of high-risk human papillomavirus DNA in penile carcinoma predicts favorable outcome in survival. Int J Cancer. 2006; 119: 1078-81.). In order to avoid bias in our study, we only evaluated inguinal disease-free survival (IDFI), that did not show differences between HPV positive and negative groups (p = 0.45).

Several pathological and molecular risk factor are being described in order to improve lymph node evaluation (²⁴24. Chaux A, Tamboli P, Ayala A, Soares F, Rodríguez I, Barreto J, et al.: Warty-basaloid carcinoma: clinicopathological features of a distinctive penile neoplasm. Report of 45 cases. Mod Pathol. 2010; 23: 896-904. ²⁵25. Lopes A, Hidalgo GS, Kowalski LP, Torloni H, Rossi BM, Fonseca FP: Prognostic factors in carcinoma of the penis: multivariate analysis of 145 patients treated with amputation and-lymphadenectomy. J Urol. 1996; 156: 1637-42.). Among pathological predictive factors, only PNI, LVI and histological grade are independent factors to predict lymph node involvement (²⁵25. Lopes A, Hidalgo GS, Kowalski LP, Torloni H, Rossi BM, Fonseca FP: Prognostic factors in carcinoma of the penis: multivariate analysis of 145 patients treated with amputation and-lymphadenectomy. J Urol. 1996; 156: 1637-42.). In our study, tumor stage ≥ T1b-T4, LVI, PNI, infiltrative invasion and sarcomatoid histological subtype are the histological factors related to lymph node metastasis in a univariate analysis.

There was no significant difference among the cellular differentiation grades as prognostic factors, in spite of the reduced sample. However, pathological heterogeneity, with more than a grade presented in the same tumor is rarely considered in different studies.

Multivariate regression analysis showed that only ≥ T1b-T4 tumors, LVI and infiltrative pattern were independent factors, and T stage was the most important (HR = 2.67, p = 0.02). The reported differences in several series are mainly caused by methodology, therapeutic approach and heterogeneity of the studied population. These limitations must be contoured in order to obtain a better validation of these risk factors for inguinal metastasis.

CONCLUSIONS

Observed HPV prevalence was similar to previous studies. However, there was a predominance of the low risk viral group. There was no significant association between HPV status or HPV subgroups and histological worse prognostic factors. HPV detection had no use as predictive value of inguinal metastasis. Tumor staging, lymph-vascular invasion and infiltrative pattern were independent risk factors for lymph node involvement.

REFERENCES

¹
Backes DM, Kurman RJ, Pimenta JM, Smith JS: Systematic review of human papillomavirus prevalence in invasive penile cancer. Cancer Causes Control. 2009; 20: 449-57.
²
Favorito LA, Nardi AC, Ronalsa M, Zequi SC, Sampaio FJ, Glina S: Epidemiologic study on penile cancer in Brazil. Int Braz J Urol. 2008; 34: 587-91; discussion 591-3.
³
Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90.
⁴
Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.
⁵
Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.
⁶
Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50.
⁷
Gonzaga-Silva LF, Tavares JM, Freitas FC, Tomas Filho ME, Oliveira VP, Lima MV: The isolated gamma probe technique for sentinel node penile carcinoma detection is unreliable. Int Braz J Urol. 2007; 33: 58-63; discussion 64-7.
⁸
Pettaway CA, Horenblas S: Penile cancer: incremental insights into etiology, diagnosis, staging, and management. World J Urol. 2009; 27: 139-40.
⁹
BE Stephen, BR David, CC Carolyn, GF April, LG Frederick, T Andy, III: AJCC Cancer Staging Manual. Philadelphia, Lippincott. 2010; Seventh Edition, 2010; pp.447.
¹⁰
Cubilla AL: The role of pathologic prognostic factors in squamous cell carcinoma of the penis. World J Urol. 2009; 27: 169-77.
¹¹
Miralles-Guri C, Bruni L, Cubilla AL, Castellsagué X, Bosch FX, de Sanjosé S: Human papillomavirus prevalence and type distribution in penile carcinoma. J Clin Pathol. 2009; 62: 870-8.
¹²
Bezerra AL, Lopes A, Santiago GH, Ribeiro KC, Latorre MR, Villa LL: Human papillomavirus as a prognostic factor in carcinoma of the penis: analysis of 82 patients treated with amputation andbilateral lymphadenectomy. Cancer. 2001; 91: 2315-21.
¹³
Krustrup D, Jensen HL, van den Brule AJ, Frisch M: Histological characteristics of human papilloma-virus-positive and -negative invasive and in situ squamous cell tumours of the penis. Int J Exp Pathol. 2009; 90: 182-9.
¹⁴
Anic GM, Giuliano AR: Genital HPV infection and related lesions in men. Prev Med. 2011; 53: S36-41.
¹⁵
Rubin MA, Kleter B, Zhou M, Ayala G, Cubilla AL, Quint WG, et al.: Detection and typing of human papillomavirus DNA in penile carcinoma: evidence for multiple independent pathways ofpenile carcinogenesis. Am J Pathol. 2001; 159: 1211-8.
¹⁶
Scheiner MA, Campos MM, Ornellas AA, Chin EW, Ornellas MH, Andrada-Serpa MJ: Human papillomavirus and penile cancers in Rio de Janeiro, Brazil: HPV typing and clinical features. Int Braz J Urol. 2008; 34: 467-74; discussion 475-6.
¹⁷
Lont AP, Kroon BK, Horenblas S, Gallee MP, Berkhof J, Meijer CJ, et al.: Presence of high-risk human papillomavirus DNA in penile carcinoma predicts favorable outcome in survival. Int J Cancer. 2006; 119: 1078-81.
¹⁸
Kirrander P, Kolaric A, Helenius G, Windahl T, Andrén O, Stark JR, et al.: Human papillomavirus prevalence, distribution and correlation to histopathological parameters in a large Swedish cohort ofmen with penile carcinoma. BJU Int. 2011; 108: 355-9.
¹⁹
Gregoire L, Cubilla AL, Reuter VE, Haas GP, Lancaster WD: Preferential association of human papillomavirus with high-grade histologic variants of penile-invasive squamous cellcarcinoma. J Natl Cancer Inst. 1995; 87: 1705-9.
²⁰
Cubilla AL, Lloveras B, Alejo M, Clavero O, Chaux A, Kasamatsu E, et al.: The basaloid cell is the best tissue marker for human papillomavirus in invasive penile squamous cell carcinoma: a study of202 cases from Paraguay. Am J Surg Pathol. 2010; 34: 104-14.
²¹
Guimaraes G, Werneck da Cunha I, Soares F, Lopez A, Torres JJ, Chaux A, et al.: WHO histological classiWcation, regional metástasis and outcome in 375 surgically treated patients with penile SCC. Mod Pathol. 2007; 20: 150A.
²²
Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60.
²³
Kroon BK, Valdés Olmos RA, van Tinteren H, Nieweg OE, Horenblas S: Reproducibility of lymphoscintigraphy for lymphatic mapping in patients with penile carcinoma. J Urol. 2005; 174: 2214-7.
²⁴
Chaux A, Tamboli P, Ayala A, Soares F, Rodríguez I, Barreto J, et al.: Warty-basaloid carcinoma: clinicopathological features of a distinctive penile neoplasm. Report of 45 cases. Mod Pathol. 2010; 23: 896-904.
²⁵
Lopes A, Hidalgo GS, Kowalski LP, Torloni H, Rossi BM, Fonseca FP: Prognostic factors in carcinoma of the penis: multivariate analysis of 145 patients treated with amputation and-lymphadenectomy. J Urol. 1996; 156: 1637-42.

Publication Dates

Publication in this collection
Jul-Aug 2013

History

Received
11 Nov 2012
Accepted
25 May 2013

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

DNA-HPV
	HPV+	HPV-	p	HPVHigh	p	HPVlow	p	HPVMult	p
TOTAL	50 (60.9)	32 (39)		12 (50)		25 (50)		25 (50)
T1a	14 (28)	8 (72)		7 (58)		5 (²²22. Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60.)		6 (²²22. Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60.)
T1b-T4	36 (72)	24 (75)	0.73¹	5 (42)	0.01²	2 (⁷7. Gonzaga-Silva LF, Tavares JM, Freitas FC, Tomas Filho ME, Oliveira VP, Lima MV: The isolated gamma probe technique for sentinel node penile carcinoma detection is unreliable. Int Braz J Urol. 2007; 33: 58-63; discussion 64-7.)	0.35¹	1 (⁷7. Gonzaga-Silva LF, Tavares JM, Freitas FC, Tomas Filho ME, Oliveira VP, Lima MV: The isolated gamma probe technique for sentinel node penile carcinoma detection is unreliable. Int Braz J Urol. 2007; 33: 58-63; discussion 64-7.)	0.70²
Grades 1 and 2	36 (72	15 (46)		7 (58)		18 (72)		19 (76)
Grade 3	14 (28)	17 (53)	0.02¹	5 (41)	0.75¹	7 (28)	0.22¹	7 (28)	0.08¹
LVI	8 (¹⁶16. Scheiner MA, Campos MM, Ornellas AA, Chin EW, Ornellas MH, Andrada-Serpa MJ: Human papillomavirus and penile cancers in Rio de Janeiro, Brazil: HPV typing and clinical features. Int Braz J Urol. 2008; 34: 467-74; discussion 475-6.)	3 (⁹9. BE Stephen, BR David, CC Carolyn, GF April, LG Frederick, T Andy, III: AJCC Cancer Staging Manual. Philadelphia, Lippincott. 2010; Seventh Edition, 2010; pp.447.)	0.39¹	3 (¹¹11. Miralles-Guri C, Bruni L, Cubilla AL, Castellsagué X, Bosch FX, de Sanjosé S: Human papillomavirus prevalence and type distribution in penile carcinoma. J Clin Pathol. 2009; 62: 870-8.)	0.20¹	3 (¹¹11. Miralles-Guri C, Bruni L, Cubilla AL, Castellsagué X, Bosch FX, de Sanjosé S: Human papillomavirus prevalence and type distribution in penile carcinoma. J Clin Pathol. 2009; 62: 870-8.)	0.80¹	3 (¹¹11. Miralles-Guri C, Bruni L, Cubilla AL, Castellsagué X, Bosch FX, de Sanjosé S: Human papillomavirus prevalence and type distribution in penile carcinoma. J Clin Pathol. 2009; 62: 870-8.)	0.80¹
PNI	11 (²²22. Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60.)	7 (²¹21. Guimaraes G, Werneck da Cunha I, Soares F, Lopez A, Torres JJ, Chaux A, et al.: WHO histological classiWcation, regional metástasis and outcome in 375 surgically treated patients with penile SCC. Mod Pathol. 2007; 20: 150A.)	0.98¹	1 (¹⁸18. Kirrander P, Kolaric A, Helenius G, Windahl T, Andrén O, Stark JR, et al.: Human papillomavirus prevalence, distribution and correlation to histopathological parameters in a large Swedish cohort ofmen with penile carcinoma. BJU Int. 2011; 108: 355-9.)	0.21¹	6 (¹⁸18. Kirrander P, Kolaric A, Helenius G, Windahl T, Andrén O, Stark JR, et al.: Human papillomavirus prevalence, distribution and correlation to histopathological parameters in a large Swedish cohort ofmen with penile carcinoma. BJU Int. 2011; 108: 355-9.)	0.76¹	5 (¹⁸18. Kirrander P, Kolaric A, Helenius G, Windahl T, Andrén O, Stark JR, et al.: Human papillomavirus prevalence, distribution and correlation to histopathological parameters in a large Swedish cohort ofmen with penile carcinoma. BJU Int. 2011; 108: 355-9.)	0.77¹
INVASION
Infiltrative	24 (48)	23 (71)	0.03²	4 (47)	0.06¹	12 (47)	0.25¹	13 (47)	0.51¹
Pushing	26 (52)	9 (28)		8 (35)		13 (35)		12 (35)
SUBTYPE
Usual	37 (74)	23 (71)	0.83¹	5 (60)	0.000²	23 (60)	0.01¹	18 (60)	0.87¹
Condilomatous	3 (⁶6. Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50.)	1 (³3. Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90.)	0.55¹	1 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	0.54²	0 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	0.17¹	3 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	0.04²
Verrucous	1 (²⁰20. Cubilla AL, Lloveras B, Alejo M, Clavero O, Chaux A, Kasamatsu E, et al.: The basaloid cell is the best tissue marker for human papillomavirus in invasive penile squamous cell carcinoma: a study of202 cases from Paraguay. Am J Surg Pathol. 2010; 34: 104-14.)	2 (⁶6. Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50.)	0.31¹	1 (³3. Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90.)	0.35¹	0 (³3. Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90.)	0.24¹	0 (³3. Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90.)	0.24¹
Basaloid	4 (⁸8. Pettaway CA, Horenblas S: Penile cancer: incremental insights into etiology, diagnosis, staging, and management. World J Urol. 2009; 27: 139-40.)	0 (0)	0.10¹	3 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	0.009²	1 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	0.80¹	1 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	0.80¹
Papillary	2 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	3 (⁹9. BE Stephen, BR David, CC Carolyn, GF April, LG Frederick, T Andy, III: AJCC Cancer Staging Manual. Philadelphia, Lippincott. 2010; Seventh Edition, 2010; pp.447.)	0.32¹	2 (⁵5. Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.)	0.15¹	0 (⁵5. Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.)	0.12²	1 (⁵5. Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.)	0.59¹
Sarcomatoid	2 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.)	3 (⁹9. BE Stephen, BR David, CC Carolyn, GF April, LG Frederick, T Andy, III: AJCC Cancer Staging Manual. Philadelphia, Lippincott. 2010; Seventh Edition, 2010; pp.447.)	0.32¹	0 (⁵5. Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.)	0.33¹	0 (⁵5. Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.)	0.12¹	2 (⁵5. Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.)	0.63¹
Acantholysis	1 (²2. Favorito LA, Nardi AC, Ronalsa M, Zequi SC, Sampaio FJ, Glina S: Epidemiologic study on penile cancer in Brazil. Int Braz J Urol. 2008; 34: 587-91; discussion 591-3.)	0 (0)	0.42¹	0 (¹1. Backes DM, Kurman RJ, Pimenta JM, Smith JS: Systematic review of human papillomavirus prevalence in invasive penile cancer. Cancer Causes Control. 2009; 20: 449-57.)	0.67¹	1 (¹1. Backes DM, Kurman RJ, Pimenta JM, Smith JS: Systematic review of human papillomavirus prevalence in invasive penile cancer. Cancer Causes Control. 2009; 20: 449-57.)	0.12¹	0 (¹1. Backes DM, Kurman RJ, Pimenta JM, Smith JS: Systematic review of human papillomavirus prevalence in invasive penile cancer. Cancer Causes Control. 2009; 20: 449-57.)	0.50¹
pN	29 (58)	17 (53)	0.66¹	6 (46)	0.64¹	15 (46)	0.63¹	12 (46)	0.32¹

	Number of patients	IMFS in 5 years (95%IC) (%)	p Value (Log-Rank test)	Risk rate (IC95%)
pT
T1a	23	59 (45 - 73)	0.002	5.76 (1.78 - 18.64)
T1b-T4	57	26 (19 - 33)
GRADES
1-2	51	34 (25 - 43)	0.42	1.27 (0.70 - 2.31)
3	31	28 (18 - 39)
LVI
Present	11	14 (³3. Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90. ²⁵25. Lopes A, Hidalgo GS, Kowalski LP, Torloni H, Rossi BM, Fonseca FP: Prognostic factors in carcinoma of the penis: multivariate analysis of 145 patients treated with amputation and-lymphadenectomy. J Urol. 1996; 156: 1637-42.)	0.0004	2.90 (1.44 - 5.81)
Absent	71	36 (28 - 43)
PNI
Present	18	14 (⁶6. Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50. ²²22. Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60.)	0.000	2.88 (1.54 - 5.37)
Absent	64	39 (30 - 47)
INVASION
Infiltrative	47	23 (16 - 31)	0.003	2.68 (1.38 - 5.22)
Pushing	35	46 (35 - 57)
SUBTYPE
Usual	60	33 (25 - 41)	0.55	0.81 (0.39 - 1.65)
Condilomatous	4	38 (10 - 66)	0.52	0.53 (0.73 - 3.88)
Verrucous	3	9 (²2. Favorito LA, Nardi AC, Ronalsa M, Zequi SC, Sampaio FJ, Glina S: Epidemiologic study on penile cancer in Brazil. Int Braz J Urol. 2008; 34: 587-91; discussion 591-3. ¹⁵15. Rubin MA, Kleter B, Zhou M, Ayala G, Cubilla AL, Quint WG, et al.: Detection and typing of human papillomavirus DNA in penile carcinoma: evidence for multiple independent pathways ofpenile carcinogenesis. Am J Pathol. 2001; 159: 1211-8.)	0.99	1.00 (0.13 - 7.38)
Basaloid	4	12 (⁹9. BE Stephen, BR David, CC Carolyn, GF April, LG Frederick, T Andy, III: AJCC Cancer Staging Manual. Philadelphia, Lippincott. 2010; Seventh Edition, 2010; pp.447. ¹⁵15. Rubin MA, Kleter B, Zhou M, Ayala G, Cubilla AL, Quint WG, et al.: Detection and typing of human papillomavirus DNA in penile carcinoma: evidence for multiple independent pathways ofpenile carcinogenesis. Am J Pathol. 2001; 159: 1211-8.)	0.24	1.96 (0.60 - 6.45)
Papillary	5	9 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50. ¹³13. Krustrup D, Jensen HL, van den Brule AJ, Frisch M: Histological characteristics of human papilloma-virus-positive and -negative invasive and in situ squamous cell tumours of the penis. Int J Exp Pathol. 2009; 90: 182-9.)	0.02	0.04 (0.00 - 15.59)
Sarcomatoid	5	9 (⁴4. Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50. ¹³13. Krustrup D, Jensen HL, van den Brule AJ, Frisch M: Histological characteristics of human papilloma-virus-positive and -negative invasive and in situ squamous cell tumours of the penis. Int J Exp Pathol. 2009; 90: 182-9.)	0.02	3.02 (1.05 - 8.64)
Acantholysis	1	7 (7 - 7)	0.14	3.88 (0.51 - 29.2)
HPV
Positive	50	34 (25 - 43)	0.45	0.79 (0.43 - 1.46)
Negative	32	29 (18 - 40)

COX multivariate regression analysis – independent risk factors for inguinal metastasis
Variables	Risk rate (IC95%)	“p” value
pT1axpT1b-4 (pT1b-4)	2.67 (1.16 - 6.15)	0.02
LVI +	2.09 (1.03 - 4.22)	0.03
Infiltrative invasion	2.00 (1.00 - 4.03)	0.04

Sociedade Brasileira de Urologia Rua Bambina, 153, 22251-050 Rio de Janeiro RJ Brazil, Tel. +55 21 2539-6787, Fax: +55 21 2246-4088 - Rio de Janeiro - RJ - Brazil
E-mail: brazjurol@brazjurol.com.br

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[1] ¹
Backes DM, Kurman RJ, Pimenta JM, Smith JS: Systematic review of human papillomavirus prevalence in invasive penile cancer. Cancer Causes Control. 2009; 20: 449-57.

[2] ²
Favorito LA, Nardi AC, Ronalsa M, Zequi SC, Sampaio FJ, Glina S: Epidemiologic study on penile cancer in Brazil. Int Braz J Urol. 2008; 34: 587-91; discussion 591-3.

[3] ³
Fonseca AGda, Pinto JASA, Marques MC, Drosdroski FS, Fonseca Neto LORda: Estudo epidemiológico do câncer de pênis no Estado do Pará, Brasil. Rev Pan-Amaz Saude. 2010; 1: 85-90.

[4] ⁴
Bleeker MC, Heideman DA, Snijders PJ, Horenblas S, Dillner J, Meijer CJ: Penile cancer: epidemiology, pathogenesis and prevention. World J rol. 2009; 27: 141-50.

[5] ⁵
Tornesello ML, Duraturo ML, Losito S, Botti G, Pilotti S, Stefanon B, et al.: Human papillomavirus genotypes and HPV16 variants in penile carcinoma. Int J Cancer. 2008; 122: 132-7.

[6] ⁶
Pompeo ACL, Billis A: Carcinoma epidermóide do pênis. Int Braz J Urol. 2003; 29 (Suppl. 1): 44-50.

[7] ⁷
Gonzaga-Silva LF, Tavares JM, Freitas FC, Tomas Filho ME, Oliveira VP, Lima MV: The isolated gamma probe technique for sentinel node penile carcinoma detection is unreliable. Int Braz J Urol. 2007; 33: 58-63; discussion 64-7.

[8] ⁸
Pettaway CA, Horenblas S: Penile cancer: incremental insights into etiology, diagnosis, staging, and management. World J Urol. 2009; 27: 139-40.

[9] ⁹
BE Stephen, BR David, CC Carolyn, GF April, LG Frederick, T Andy, III: AJCC Cancer Staging Manual. Philadelphia, Lippincott. 2010; Seventh Edition, 2010; pp.447.

[10] ¹⁰
Cubilla AL: The role of pathologic prognostic factors in squamous cell carcinoma of the penis. World J Urol. 2009; 27: 169-77.

[11] ¹¹
Miralles-Guri C, Bruni L, Cubilla AL, Castellsagué X, Bosch FX, de Sanjosé S: Human papillomavirus prevalence and type distribution in penile carcinoma. J Clin Pathol. 2009; 62: 870-8.

[12] ¹²
Bezerra AL, Lopes A, Santiago GH, Ribeiro KC, Latorre MR, Villa LL: Human papillomavirus as a prognostic factor in carcinoma of the penis: analysis of 82 patients treated with amputation andbilateral lymphadenectomy. Cancer. 2001; 91: 2315-21.

[13] ¹³
Krustrup D, Jensen HL, van den Brule AJ, Frisch M: Histological characteristics of human papilloma-virus-positive and -negative invasive and in situ squamous cell tumours of the penis. Int J Exp Pathol. 2009; 90: 182-9.

[14] ¹⁴
Anic GM, Giuliano AR: Genital HPV infection and related lesions in men. Prev Med. 2011; 53: S36-41.

[15] ¹⁵
Rubin MA, Kleter B, Zhou M, Ayala G, Cubilla AL, Quint WG, et al.: Detection and typing of human papillomavirus DNA in penile carcinoma: evidence for multiple independent pathways ofpenile carcinogenesis. Am J Pathol. 2001; 159: 1211-8.

[16] ¹⁶
Scheiner MA, Campos MM, Ornellas AA, Chin EW, Ornellas MH, Andrada-Serpa MJ: Human papillomavirus and penile cancers in Rio de Janeiro, Brazil: HPV typing and clinical features. Int Braz J Urol. 2008; 34: 467-74; discussion 475-6.

[17] ¹⁷
Lont AP, Kroon BK, Horenblas S, Gallee MP, Berkhof J, Meijer CJ, et al.: Presence of high-risk human papillomavirus DNA in penile carcinoma predicts favorable outcome in survival. Int J Cancer. 2006; 119: 1078-81.

[18] ¹⁸
Kirrander P, Kolaric A, Helenius G, Windahl T, Andrén O, Stark JR, et al.: Human papillomavirus prevalence, distribution and correlation to histopathological parameters in a large Swedish cohort ofmen with penile carcinoma. BJU Int. 2011; 108: 355-9.

[19] ¹⁹
Gregoire L, Cubilla AL, Reuter VE, Haas GP, Lancaster WD: Preferential association of human papillomavirus with high-grade histologic variants of penile-invasive squamous cellcarcinoma. J Natl Cancer Inst. 1995; 87: 1705-9.

[20] ²⁰
Cubilla AL, Lloveras B, Alejo M, Clavero O, Chaux A, Kasamatsu E, et al.: The basaloid cell is the best tissue marker for human papillomavirus in invasive penile squamous cell carcinoma: a study of202 cases from Paraguay. Am J Surg Pathol. 2010; 34: 104-14.

[21] ²¹
Guimaraes G, Werneck da Cunha I, Soares F, Lopez A, Torres JJ, Chaux A, et al.: WHO histological classiWcation, regional metástasis and outcome in 375 surgically treated patients with penile SCC. Mod Pathol. 2007; 20: 150A.

[22] ²²
Ficarra V, Novara G, Boscolo-Berto R, Artibani W, Kattan MW: How accurate are present risk group assignment tools in penile cancer? World J Urol. 2009; 27: 155-60.

[23] ²³
Kroon BK, Valdés Olmos RA, van Tinteren H, Nieweg OE, Horenblas S: Reproducibility of lymphoscintigraphy for lymphatic mapping in patients with penile carcinoma. J Urol. 2005; 174: 2214-7.

[24] ²⁴
Chaux A, Tamboli P, Ayala A, Soares F, Rodríguez I, Barreto J, et al.: Warty-basaloid carcinoma: clinicopathological features of a distinctive penile neoplasm. Report of 45 cases. Mod Pathol. 2010; 23: 896-904.

[25] ²⁵
Lopes A, Hidalgo GS, Kowalski LP, Torloni H, Rossi BM, Fonseca FP: Prognostic factors in carcinoma of the penis: multivariate analysis of 145 patients treated with amputation and-lymphadenectomy. J Urol. 1996; 156: 1637-42.

Brasil

Brasil

Human Papilloma Virus: Prevalence, distribution and predictive value to lymphatic metastasis in penile carcinoma

Abstract

Objectives

Material and Methods

Results

conclusions

INTRODUCTION

MATERIALS AND METHODS

Patients

Treatment protocol

Pathological Analysis

HPV Analysis

Follow-up and statistical analysis

RESULTS

*** MISSING SECTION HEADING ***

Presence of HPV DNA

Histological characteristics of subgroups HPV positive (HPVhigh, HPVlow and HPVmult) and HPV negative

DISCUSSION

CONCLUSIONS

REFERENCES

Publication Dates

History

* MISSING SECTION HEADING *