Epidemiologic studies of genital HPV infection in female STD clinic patients and students at the University of Washington have shown no relationship between HPV DNA prevalence in genital specimens and history of sexual exposures - unlike other STDs studied. Use of serology and PCR to detect HPV DNA in oral and genital specimens suggest that infection with """"""""genital"""""""" types of HPV can be detected as early as one year of age. In Project 1, therefore, a study of perinatal and childhood transmission of HPV infection is proposed. 240 pregnant women prior to 20 weeks gestation will be enrolled, evaluated, and followed through pregnancy and the first year after delivery. To assess perinatal transmission, their newborn infants will be periodically examined for HPV infection until 3 years of age. Using serology and PCR, as well as other methods for detection of HPV in mothers and infants, the risk of perinatal transmission in relation to route of delivery and other perinatal obstetric factors will be assessed and HPV types found in mothers and infants will be correlated. To assess intrafamilial transmission during childhood, fathers and siblings will be examined for HPV infection, and siblings will be periodically revaluated over time. In other protocols, members of our study group have specifically analyzed risks and risk factors for perinatal transmission of C. trachomatis, HSV, and HIV,, and have examined prenatal and puerperal manifestations of these infections, as well as CMV and bacterial vaginosis. The proposed study is similar, equally feasible, and will complement Project 2 (a study of sexually acquired HPV in a cohort of sexually inexperienced students); will draw on serologic methods developed in Project 3; and by assessing the effects of pregnancy and lactation on HPV and dysplasia, will be conceptually related to Project 4, which will include analyses of the effects of hormonal factors on HPV-induced neoplasia.

Project Start
Project End
Budget Start
Budget End
Support Year
4
Fiscal Year
1993
Total Cost
Indirect Cost
Name
Fred Hutchinson Cancer Research Center
Department
Type
DUNS #
075524595
City
Seattle
State
WA
Country
United States
Zip Code
98109
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Hagensee, M E; Carter, J J; Wipf, G C et al. (1995) Immunization of mice with HPV vaccinia virus recombinants generates serum IgG, IgM, and mucosal IgA antibodies. Virology 206:174-82
Ostrow, R S; Coughlin, S M; McGlennen, R C et al. (1995) Serological and molecular evidence of rhesus papillomavirus type 1 infections in tissues from geographically distinct institutions. J Gen Virol 76 ( Pt 2):293-9
Baken, L A; Koutsky, L A; Kuypers, J et al. (1995) Genital human papillomavirus infection among male and female sex partners: prevalence and type-specific concordance. J Infect Dis 171:429-32
Xi, L F; Demers, G W; Koutsky, L A et al. (1995) Analysis of human papillomavirus type 16 variants indicates establishment of persistent infection. J Infect Dis 172:747-55
Carter, J J; Hagensee, M B; Lee, S K et al. (1994) Use of HPV 1 capsids produced by recombinant vaccinia viruses in an ELISA to detect serum antibodies in people with foot warts. Virology 199:284-91
McDougall, J K (1994) Immortalization and transformation of human cells by human papillomavirus. Curr Top Microbiol Immunol 186:101-19
Merrick, D T; Gown, A M; Halbert, C L et al. (1993) Human papillomavirus-immortalized keratinocytes are resistant to the effects of retinoic acid on terminal differentiation. Cell Growth Differ 4:831-40
Cook, L S; Koutsky, L A; Holmes, K K (1993) Clinical presentation of genital warts among circumcised and uncircumcised heterosexual men attending an urban STD clinic. Genitourin Med 69:262-4

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