Abstract

To begin to address the biology of MCV, we developed viral reporter vectors based on the MCV capsid proteins. We have also developed reporter vectors based on better-studied human polyomaviruses, such as B-K polyomavirus (BKV). Our first application of these new reporter vectors was to quantitate MCV-specific serum antibody responses in human subjects. We found that 88% of a population of healthy adults displayed MCV-specific antibody responses, suggesting that infection with the virus is very common. Interestingly, our analysis revealed that patients with MCC displayed dramatically stronger antibody responses against MCV than control subjects. This suggests that strong MCV-specific antibody responses may serve as a biomarker for MCV-associated diseases. In a separate line of work, we discovered that healthy subjects shed MCV virions from the surface of their skin. The project involved the development of cutting edge methods for random amplification and deep sequencing of the genomic DNA of polyomaviruses, papillomaviruses and other skin-surface microbial DNA. The project led to the discovery of two novel polyomaviruses, human polyomavirus 6 (HPyV6) and HPyV7. More recently we discovered HPyV10 and confirmed the existence of HPyV11. It is not yet clear whether the novel viruses cause any human diseases. However, HPyV6 can be found in skin cancers arising on patients treated with BRAF inhibitors and HPyV7 has recently been found in skin rashes. The remarkable recent success of virus-like particle (VLP) based vaccines against HPV suggests that similar VLP vaccines against polyomaviruses might be similarly effective. Thus, if our work can uncover causal connections between MCV or other HPyVs and major human diseases, such as cancer, it might be possible to rapidly develop a vaccine for preventing any diseases the polyomaviruses might cause. In recent years, our lab has shifted focus toward BK and JC polyomaviruses, which commonly infect the human urinary tract. We are seeking to understand the basic mechanisms through which these two pathogenic human polyomaviruses infect cells and elucidate the mechanisms of antibody-mediated neutralization.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIABC011090-11
Application #
9779789
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
11
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Basic Sciences
Department
Type
DUNS #
City
State
Country
Zip Code

  Publications

Peretti, Alberto; Geoghegan, Eileen M; Pastrana, Diana V et al. (2018) Characterization of BK Polyomaviruses from Kidney Transplant Recipients Suggests a Role for APOBEC3 in Driving In-Host Virus Evolution. Cell Host Microbe 23:628-635.e7
Gupta, Gaurav; Kuppachi, Sarat; Kalil, Roberto S et al. (2018) Treatment for presumed BK polyomavirus nephropathy and risk of urinary tract cancers among kidney transplant recipients in the United States. Am J Transplant 18:245-252
Geoghegan, Eileen M; Pastrana, Diana V; Schowalter, Rachel M et al. (2017) Infectious Entry and Neutralization of Pathogenic JC Polyomaviruses. Cell Rep 21:1169-1179
Geoghegan, Eileen M; Welch, Nicole L; Yabsley, Michael J et al. (2017) Identification of a Second Raccoon-Associated Polyomavirus. Genome Announc 5:
Nguyen, Khang D; Lee, Eunice E; Yue, Yangbo et al. (2017) Human polyomavirus 6 and 7 are associated with pruritic and dyskeratotic dermatoses. J Am Acad Dermatol 76:932-940.e3
Cantalupo, Paul G; Buck, Christopher B; Pipas, James M (2017) Complete Genome Sequence of a Polyomavirus Recovered from a Pomona Leaf-Nosed Bat (Hipposideros pomona) Metagenome Data Set. Genome Announc 5:
Pastrana, Diana V; Ray, Upasana; Magaldi, Thomas G et al. (2016) Erratum for Pastrana et al., BK Polyomavirus Genotypes Represent Distinct Serotypes with Distinct Entry Tropism. J Virol 90:624
Cerqueira, Carla; Pang, Yuk-Ying S; Day, Patricia M et al. (2016) A Cell-Free Assembly System for Generating Infectious Human Papillomavirus 16 Capsids Implicates a Size Discrimination Mechanism for Preferential Viral Genome Packaging. J Virol 90:1096-107
Gupta, Tushar; Robles, Maria Teresa Sáenz; Schowalter, Rachel M et al. (2016) Expression of the small T antigen of Lymphotropic Papovavirus is sufficient to transform primary mouse embryo fibroblasts. Virology 487:112-20
Buck, Christopher B; Van Doorslaer, Koenraad; Peretti, Alberto et al. (2016) The Ancient Evolutionary History of Polyomaviruses. PLoS Pathog 12:e1005574

Showing the most recent 10 out of 40 publications