Molecular dynamics simulation and purification of chimeric L1/L2 protein from human papillomavirus type 52 expressed in Escherichia coli BL21 (DE3)

Al Adawiah, Rabiyah and Zaenal Mustopa, Apon and Budiarti, Sri and Nur Umami, Rifqiyah and Hertati, Ai and Irawan, Herman and Ikramullah, Muh. Chaeril and Arwansyah, Arwansyah and Mamangkey, Jendri and Kartikasari, Isti and Salahudin Darusman, Huda (2024) Molecular dynamics simulation and purification of chimeric L1/L2 protein from human papillomavirus type 52 expressed in Escherichia coli BL21 (DE3). Journal of Immunoassay and Immunochemistry, 45 (5). pp. 395-414. ISSN 1532-1819

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Abstract

The available prophylactic vaccines for human papillomavirus (HPV) in the market are only effective against specific types of HPV, rendering them ineffective for other types of HPV infections. The objective of this research is to investigate the stability of the recombinant protein constructed, namely chimeric L1/L2 protein from HPV type 52, with improved cross-neutralization ability. The 3D model, predicted using Alphafold, Robetta, I-Tasser, and refined with Galaxy Refinement, is validated using Ramachandran plot analysis. The stability is verified through molecular dynamics simulations, considering parameters such as RMSD, RMSF, Rg, and SASA, where stable conditions are observed. The chimeric L1/L2 protein from HPV type 52 is purified using affinity chromatography, and the His-tag is cleaved using SUMO protease to obtain pure chimeric protein with the size of ~ 55 kDa. Western blot analysis confirms binding to anti-L1 HPV type 52 polyclonal antibody. The obtained vaccine candidate can be utilized as an effective prophylactic vaccine against HPV.

Item Type: Article
Uncontrolled Keywords: HPV; molecular dynamics; purification; vaccine
Subjects: Medicine & Biology > Cytology, Genetics, & Molecular Biology
Depositing User: Saepul Mulyana
Date Deposited: 08 Dec 2025 06:00
Last Modified: 08 Dec 2025 06:00
URI: https://karya.brin.go.id/id/eprint/55714

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