Your search keyword '"Saqlain Suleman"' showing total 2 results

1. HIV- 1 lentivirus tethering to the genome is associated with transcription factor binding sites found in genes that favour virus survival

Author

Saqlain Suleman, Annette Payne, Johnathan Bowden, Sharmin Al Haque, Marco Zahn, Serena Fawaz, Mohammad S. Khalifa, Susan Jobling, David Hay, Matteo Franco, Raffaele Fronza, Wei Wang, Olga Strobel-Freidekind, Annette Deichmann, Yasuhiro Takeuchi, Simon N. Waddington, Irene Gil-Farina, Manfred Schmidt, and Michael Themis

Subjects

Binding Sites, Virus Integration, Lentivirus, Induced Pluripotent Stem Cells, IS- insertion site, pTFBS- predicted transcription factor binding site, HIV Infections, LV- lentiviral vectors, Mice, stem-cell differentiation, Genetics, HIV-1, Molecular Medicine, Humans, Animals, cancer, genetics, Molecular Biology, Transcription Factors

Abstract

Data availability: The databases generated during an/or analysed during the current study are available from the corresponding author on reasonable request. Copyright © The Author(s) 2022. Lentiviral vectors (LV) are attractive for permanent and effective gene therapy. However, integration into the host genome can cause insertional mutagenesis highlighting the importance of understanding of LV integration. Insertion site (IS) tethering is believed to involve cellular proteins such as PSIP1/LEDGF/p75, which binds to the virus pre-integration complexes (PICs) helping to target the virus genome. Transcription factors (TF) that bind both the vector LTR and host genome are also suspected influential to this. To determine the role of TF in the tethering process, we mapped predicted transcription factor binding sites (pTFBS) near to IS chosen by HIV-1 LV using a narrow 20 bp window in infected human induced pluripotent stem cells (iPSCs) and their hepatocyte-like cell (HLC) derivatives. We then aligned the pTFBS with these sequences found in the LTRs of native and self-inactivated LTRs. We found significant enrichment of these sequences for pTFBS essential to HIV-1 life cycle and virus survival. These same sites also appear in HIV-1 patient IS and in mice infected with HIV-1 based LV. This in silco data analysis suggests pTFBS present in the virus LTR and IS sites selected by HIV-1 LV are important to virus survival and propagation. NC3Rs CRACK IT Challenge 21: InMutagene award, sponsored by GSK and Novartis.

Published

2022

2. Rapid and inexpensive purification of adenovirus vectors using an optimised aqueous two-phase technology

Author

Michael Themis, Rajvinder Karda, Simon N. Waddington, Kuteiba Schrubaji, Saqlain Suleman, Peter Hewitson, Svetlana Ignatova, Chrysovalanto Filippou, and Jonathan Huddleston

Subjects

endocrine system, Technology, COVID-19 Vaccines, animal diseases, viruses, Genetic Vectors, Vectors in gene therapy, Biology, Virus, Adenoviridae, adenovirus type 5, chemistry.chemical_compound, viral vector purification, Plasmid, In vivo, vaccine, Virology, PEG ratio, Humans, caesium chloride, Cytotoxicity, Downstream processing, Chromatography, aqueous two-phase partitioning system, SARS-CoV-2, virus diseases, COVID-19, HEK293 Cells, chemistry, Caesium chloride

Abstract

Copyright © 2021 The Author(s). Adenoviruses (AdVs) are used as gene therapy vectors to treat human diseases and as vaccines against COVID-19. AdVs are produced by transfecting human embryonic kidney 239 (HEK293) or PER.C6 virus producer cells with AdV plasmid vectors or infecting these cells withcell lysates containing replication-defective AdV. Cell lysates can be purified further by caesium chloride or chromatographic protocols to research virus seed stocks (RVSS) for characterisation to high quality master virus seed stocks (MVSS) and working virus seed stocks (WVSS) before downstream production of pure, high titre AdV. Lysates are poorly infectious, block filtration columns and have limited storage capability. Aqueous two-phase systems (ATPS) are an alternative method for AdV purification that rapidly generates cleaner RVSS for characterisation to MVSS. After testing multiple ATPS formulations, an aqueous mixture of 20 % PEG 600 and 20 % (NH4)2SO4 (w/w) was found most effective for AdV partitioning, producing up to 97+3% yield of high-titre virus that was devoid of aggregates both effective in vitro and in vivo with no observable cytotoxicity. Importantly, AdV preparations stored at −20 °C or 4 °C show negligible loss of titre and are suitable for downstream processing to clinical grade to support the need for AdV vaccines. Brunel University London Brief award.

Published

2020