HPV Virology and Treatment

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Introduction

HPV currently infects twenty million Americans and about another six million become infected each year. Today, at least fifty percent of sexually active men and women get HPV during their lifetime (40). As one can see, this sexually transmitted disease is among the most prevalent in America, which explains the importance of understand the disease. Human papillomavirus (HPV) or the “wart virus” is a virus belonging to its own family, papillomaviridae. There are more than a 100 types of HPV and as reflected in its name, species specific for humans. There are two types, cutaneous or mucocutaneous, based upon its tissue tropism or predilection for infecting specific areas of the human body. Human papillomavirus infections are diagnosed worldwide, account for the most common sexually transmitted disease worldwide, and have been associated with both cutaneous and mucocutaneous cancers prompting attempts to prevent infections using vaccines. In short, it has become a global health infection warranting every effort to control and eradicate it.


Electron micrograph of the Ebola Zaire virus. This was the first photo ever taken of the virus, on 10/13/1976. By Dr. F.A. Murphy, now at U.C. Davis, then at the CDC.


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The Virology of HPV

Virology/Oncogenesis/Molecular detection

HPV is a double-stranded DNA, non-enveloped capsid virus. It has 7900 base pairs which have 90% homology between the types (1). The base pairs are arranged in a circle which includes the codes for two key proteins known as L1 and L2 (2). These two proteins act as the “immunogene” which is required for self-assembly and the infectivity protein, respectively (2,3). The virus is transmitted between humans through breaks within the epidermis of the skin. Once the virus enters the skin, it attaches to a component of skin stem cells known as the tissue-specific heparin sulfate proteoglycans (4,5,6). Differentiation of the virus then occurs within the squamous keratinocyte (7), replicates, proliferates, and then moves to the next cell. It is the persistence of HPV within the squamous which poses the greatest risk for malignant degeneration. [See the figure from Robert W. Trindle, Nature Reviews Cancer 2:59-64, 2002]

BiologyofHPVF1.jpg


HPV types are differentiated by their associations with specific types of human cancers. For example, HPV 16 and 18 are most frequently associated with cervical cancer (8). HPV 16 accounts for up to 50% of HPV causing cervical and anal cancers worldwide (8,9,10). In addition of those viruses associated with penile cancer, 70% are of the HPV 16 phenotype and occurs 6 times higher in males with histories of venereal warts or condylomata accuminata.

HPVs have been proven to be the causative agents of other epithelial cancers. The proof that these viruses indeed are the causative agents is based upon the following observations (11):

1)HPV DNA has been found within cancer biopsies 2)known viral oncogenes E6 and E7 are found in cancer material 3)genes E6 and E7 code for proteins which are growth-regulators in host cells 4)E6 and E7 gene expression have been identified in cervical cancer immortalized cell lines(12) 5)epidemiologic investigations have identified HPV as a major factor for the development of cervical cancer 6)species specific papillomaviruses cause cancer in experimental animal models including the rabbit and cow; and human neonatal foreskin infected with HPV-16 and placed in severe combined immunodeficient mice form intraepithelial neoplasms (Mandel)

Molecular pathogenesis of skin cancer implicates HPV-E6 gene product binding to the human p53 tumor suppressor protein as the initial event (13-16). The p53 protein is a negative regulator the cell cycle transformation step between G0/G1 to the S phase. By degrading the p53 protein cell growth is directly impeded. E7 appears to exert an anti-cell death (anti-apoptotic) effect in cells through mutations in the p53 protein (17, 18) by interfering with the G1 or arrest phase of the cell cycle. Thus, both genes negatively impact normal cell cycles causing an unregulated, unimpeded cell growth, i.e. cancer transformation.

HPV is now generally detected in human tissue by various molecular biologic techniques including in situ hybridization (ISH), Southern transfer hybridization (STH), hybrid capture (HC), dot blot (DB), filter hybridization (FH), or polymerase chain reaction (PCR) (19). ISH is sensitive and can be performed directly on infected tissue specimens. It is both tedious and less sensitive than PCR and HC and thus rarely used. DB, FH, and STH are reserved for research studies and are capable of providing separations among the HPV types. HC requires a long single-stranded RNA probe to hybridize with a whole HPV genome in solution. This test enables identification of specific HPVs and quantifies them. It currently is the only method approved by the Federal Drug Administration in the United States for detection of HPV in cervical samples. PCR remains the most sensitive method for detection. It utilizes a specific primer sequence for a specific type of HPV which as a result can be used to verify links between the virus and various types of human cancers.

The Epidemiology of HPV

Epidemiology

HPV is both ubiquitous and ever prevalent in humans worldwide. A worldwide investigation of over 150,000 women with normal Pap smears (cervical cytology) revealed HPV prevalence at approximately 10% (20). Of all the regions of the world, African remains the continent with the highest prevalence of HPV infections (22% of the women examined) and incidence of the carcinogenic HPV types, 16 and 18. [See the figure from Lancet Infect Dis. de Sanjose et al. 207(7):453-459, 2007]

WorldPrevalenceofHPV.jpg

Prevalence of cervical HPV infections peaks by age 30 years then drops quickly. This corresponds to the greatest periods of sexual activity among women (21). Of interest is the finding women in Europe are more likely to become infected with HPV 16 than those in Sub-Saharan Africa (22). In certain African countries such as Uganda, HPV prevalence can exceed 75% although the major types were equally distributed between 16, 18, 51 and 52. In the United States 75-80% of sexually active adults acquire anon-genital infections by the age of 50 years (23). The highest prevalence group (45%) was women between the ages of 20 and 24 years. A study of approximately 250 female college students found as many as 29% developed an HPV infection after their first sexual encounter (24). It is important to note that most infections are transient. One study of 431 women, half of whom had anal HPV, found that 60% had cleared their infections within 15 months after detection (25). Chronic infections are more likely associated with those of the cervix and may account for the greater incidence of cervical cancer versus anal cancer due to HPV.

Males are also at risk for HPV infections with prevalence rates between 1-70% (26). Risk factors include sexual behavior (men having sex with men vs. heterosexual men), circumcision, condom use, prior STDs (sexually transmitted diseases), race and ethnicity (27,28). Among HIV negative homosexual men the prevalence rate is approximately 50% whereas in heterosexual males, cigarette smokes and those who had intercourse with multiple female partners were associated with higher rates. Condom use was associated with the lowest prevalent rates. Again, in males like females infections were cleared within 12 months in as many as 75% of those originally infected (29). Circumcision confers an advantage for clearing the infection by almost 6-fold within 12 months versus in non-circumcised males (30).

Sample Section 3


Include some current research in each section.

Conclusion


Overall paper length should be approximately 2,000 to 2,500 words.
Include at least two data figures.
Use professional sources, including at least two research studies. Public Health Measures Against HPV

References

General reviews:

Mandell, Douglas, and Bennett’s Principles and Practice of Infectious Disease. 7th Ed. 2009. Churchill Livingstone, Philadelphia. V.2. Chapter 144: Papillomaviruses. Section Eds. William Bounez and Richard C. Reichman.

Wheeler, CM. Natural history of human papillomavirus infections, cytologic and histologic abnormalities, and cancer. Obstr Gynecol Clin. 35 (4) Dec 2008; pp.519-536.

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J Virol 2003; 77:13125. 7) Doorbar, J. Molecular biology of human papillomavirus infection and cervical cancer. Clin Sci (Lond)2006; 110:525. 8) Bosch, FX, Manos, MM, Munoz, N, et al. Prevalence of human papillomavirus in cervical cancer: a worldwide perspective. International biological study on cervical cancer (IBSCC) study group. J Natl Cancer Inst 2001; 93:315. 9) Zaki, SR, Judd, R, Coffield, LM, et al. Human papillomavirus infection and anal carcinoma. Retropsective analysis by in-situ hybridization and the polymerase chain reaction. Am J Pathol 1992;140:1345. 10) Frisch, M, Glimelius, B, van den Brule, et al. Sexually transmitted infection as a cause of anal cancer. N Engl J Med 1997; 337:1350. 11) Zur Hausen, H. Papillomaviruses causing cancer: evasion from host-cell control in early events in carcinogenesis. J Natl Cancer Inst 2000; 92:690. 12) Schlegel, R. Papillomaviruses and human cancer. Semin Virol 1990; 1:297. 13) Vogelstein, B, Fearon, ER, Kern SE, et al. Allelotype of colorectal carcinomas. Science 1989; 244: 207. 14) Masuda, H, Miller, C, Koeffler, HP, et al. Rearrangement of the p53 gene in human osteogenic sarcoma. Proc Natl Acad Sci USA 1987; 84:7716. 15) Hinds, P, Finlay, C, Levine, AJ. Mutilation is required to activate the p53 gene for cooperation with the ras oncogene and transformation. J Virol 1989; 63:739. 16) Dupuy, C, Buzoni-Gatel, D, Touze, A, et al. Cell mediated immunity induced in mice by HPV 16 L1 virus like particles. Microb Pathog 1997; 22:219. 17) Puthenveettil, JA, Frederickson, SM, Reznikoff, CA. Apoptosis in human papillomavirus 16 E7-, but not E6-immortalized human uroepithelial cells. Oncogene 1996; 13:1123. 18) Magal, SS, Jackman, A, Pei, XF, et al. Induction of apoptosis in human keratinocytes containing mutated p53 alleles and its inhibition by both the E6 and E7 oncoproteins. Int J Cancer 1998; 75:96. 19) Lorincz, AT. Molecular methods for the detection of human papillomavirus infection. Obstet Gynecol Clin North Am 1996; 23:707. 20) De Sanjose, S, Diaz, M, Castellsague, X, et al. Worldwide prevalence and genotype distribution of cervical human papillomavirus DNA in women with normal cytology: a meta-analysis. Lancet Infect Dis 2007; 7:453. 21) Wright, TC Jr, Schiffman, M. Adding a test for human papillomavirus DNA to cervical-cancer screening. N Engl J Med 2003: 348:489. 22) Clifford, GM, Gallus, S, Herrero, R, et al. Worldwide distribution of human papillomavirus types in cytologically normal women in the International Agency for Research on Cancer HPV prevalence surveys: a pooled analysis. Lancet 2005; 366: 991. 23) Workowski, KA, Berman, SM. Sexually transmitted diseases treatment guidelines, 2006. MMWR Recomm Rep 2006; 55:1. 24) Winer, RL, Feng, Q, Hughes, JP, et al. Risk of female human papillomavirus acquisition associated with first male sex partner. J Infect Dis 2008; 197: 297. 25) Shvetsov, YB, Hernandez, BY, McDuffie, K, et al. Duration and clearance of anal human papilloavirus (HPV) infection among women: the Hawaii HPV cohort study. Clin Infect Dis 2009; 48:536. 26) Goodman, MT, Shvetsov, SB, McDuffie, K, et al. Acquisition of anal human papillomavirus (HPV) infection in women: the Hawaii HPV Cohort Study. J Infect Dis 2008; 197:957. 27) Baldwin, SB, Wallace, DR, Papenfuss, MR, et al. Condom use and other factors affecting penile human papillomavirus detection in men attending a sexually transmitted disease clinic. Sex Transm Dis 2004; 31:601. 28) Castellsague, X, Bosch, F, Munoz, N, et al. Male circumcision, penile human papillomavirus infection, and cervical cancer in female partners. N Engl J Med 2002; 346: 1105. 29) Guiliano, AR, Lu, B, Nielson, CM, et al. Age-specific prevalence, incidence, and duration of human papillomavirus infections in a cohort of 290 US men. J Infect Dis 2009; 199:1. 30) Lu, B, Wu, Y, Nielson, CM, et al. Factors associated with acquisition and clearance of human papillomavirus infection in a cohort of US men: a prospective study. J Infect Dis 2009; 199:362. 31) Allen, AL, Siegfried, EC. What’s new in human papillomavirus infection. Curr Opin Pediatr 2000; 12:365. 32) Beutner, KR. Nongenital human papillomavirus infections. Clin Lab Med 2000; 20:423. 33) Koutsky, L. Epidemiology of genital human papillomavirus infection. Am J Med 1997; 102:3. 34) Kjaer, SK, Tran, TN, Sparen, P, et al. The burden of genital warts: a study of nearly 70,000 women from the general female population in the 4 Nordic countries. J Infect Dis 2007; 196:1447. 35) Franco, EL, Duarte-Franco, E, Ferenczy, A. Cervical cancer: epidemiology, prevention, and the role of human papillomavirus infection. CMAJ 2001; 164:1017. 36) Petersen, BL, Buchwald, C, Gerstoft, J, et al. An aggressive and invasive growth of juvenile papillomas involving the total respiratory tract. J Laryngol Otol 1998; 112:1101. 37) Sterling, JC, Handfield-Jones, S, Hudson, PM. Guidelines for the management of cutaneous warts. Br J Dermatol 2001; 144:4. 38) Auborn, KJ, Carter, TH. Treatment of human papillomavirus gynecologic infections. Clin Lab Med 2000; 20: 407. 39) Steinbrook, R. The potential of human papillomavirus vaccines. N Engl J Med 2006; 354:1109. 40) "STD Facts- Human Papillomavirus." Center for Disease Control and Prevention. Center for Disease Control and Prevention, Apr. 2008. Web. 19 Nov. 2009. <http://www.cdc.gov/std/HPV/STDFact-HPV.htm>.