Author
Listed:
- Tae Jin Kim
(Cheil General Hospital and Women’s Healthcare Center, College of Medicine, Kwandong University)
- Hyun-Tak Jin
(Research Institute, Genexine Inc., Korea Bio Park)
- Soo-Young Hur
(Seoul St Mary’s Hospital, College of Medicine, The Catholic University of Korea)
- Hyun Gul Yang
(Pohang University of Science and Technology)
- Yong Bok Seo
(Pohang University of Science and Technology)
- Sung Ran Hong
(Cheil General Hospital and Women’s Healthcare Center, College of Medicine, Kwandong University)
- Chang-Woo Lee
(Samsung Biomedical Research Institute, Sungkyunkwan University School of Medicine)
- Suhyeon Kim
(Samsung Biomedical Research Institute, Sungkyunkwan University School of Medicine)
- Jung-Won Woo
(Research Institute, Genexine Inc., Korea Bio Park)
- Ki Seok Park
(Research Institute, Genexine Inc., Korea Bio Park)
- Youn-Young Hwang
(Research Institute, Genexine Inc., Korea Bio Park)
- Jaehan Park
(Research Institute, Genexine Inc., Korea Bio Park)
- In-Ho Lee
(Cheil General Hospital and Women’s Healthcare Center, College of Medicine, Kwandong University)
- Kyung-Taek Lim
(Cheil General Hospital and Women’s Healthcare Center, College of Medicine, Kwandong University)
- Ki-Heon Lee
(Cheil General Hospital and Women’s Healthcare Center, College of Medicine, Kwandong University)
- Mi Seon Jeong
(Laboratory of R&D for Genomics, Cheil General Hospital and Women’s Healthcare Center, College of Medicine, Kwandong University)
- Charles D. Surh
(Pohang University of Science and Technology
Academy of Immunology and Microbiology, Institute of Basic Science)
- You Suk Suh
(Research Institute, Genexine Inc., Korea Bio Park)
- Jong Sup Park
(Seoul St Mary’s Hospital, College of Medicine, The Catholic University of Korea)
- Young Chul Sung
(Research Institute, Genexine Inc., Korea Bio Park
Pohang University of Science and Technology)
Abstract
Here, we demonstrate that electroporation-enhanced immunization with a rationally designed HPV DNA vaccine (GX-188E), preferentially targeting HPV antigens to dendritic cells, elicits a significant E6/E7-specific IFN-γ-producing T-cell response in all nine cervical intraepithelial neoplasia 3 (CIN3) patients. Importantly, eight out of nine patients exhibit an enhanced polyfunctional HPV-specific CD8 T-cell response as shown by an increase in cytolytic activity, proliferative capacity and secretion of effector molecules. Notably, seven out of nine patients display complete regression of their lesions and viral clearance within 36 weeks of follow up. GX-188E administration does not elicit serious vaccine-associated adverse events at all administered doses. These findings indicate that the magnitude of systemic polyfunctional CD8 T-cell response is the main contributing factor for histological, cytological and virological responses, providing valuable insights into the design of therapeutic vaccines for effectively treating persistent infections and cancers in humans.
Suggested Citation
Tae Jin Kim & Hyun-Tak Jin & Soo-Young Hur & Hyun Gul Yang & Yong Bok Seo & Sung Ran Hong & Chang-Woo Lee & Suhyeon Kim & Jung-Won Woo & Ki Seok Park & Youn-Young Hwang & Jaehan Park & In-Ho Lee & Kyu, 2014.
"Clearance of persistent HPV infection and cervical lesion by therapeutic DNA vaccine in CIN3 patients,"
Nature Communications, Nature, vol. 5(1), pages 1-14, December.
Handle:
RePEc:nat:natcom:v:5:y:2014:i:1:d:10.1038_ncomms6317
DOI: 10.1038/ncomms6317
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