Process development for an effective COVID-19 vaccine candidate harboring recombinant SARS-CoV-2 delta plus receptor binding domain produced by Pichia pastoris

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作者
Sibel Kalyoncu
Semiramis Yilmaz
Ayca Zeybek Kuyucu
Dogu Sayili
Olcay Mert
Hakan Soyturk
Seyda Gullu
Huseyin Akinturk
Erhan Citak
Merve Arslan
Melda Guray Taskinarda
Ibrahim Oguzhan Tarman
Gizem Yilmazer Altun
Ceren Ozer
Ridvan Orkut
Aysegul Demirtas
Idil Tilmensagir
Umur Keles
Ceren Ulker
Gizem Aralan
Yavuz Mercan
Muge Ozkan
Hasan Onur Caglar
Gizem Arik
Mehmet Can Ucar
Muzaffer Yildirim
Tugce Canavar Yildirim
Dilara Karadag
Erhan Bal
Aybike Erdogan
Serif Senturk
Serdar Uzar
Hakan Enul
Cumhur Adiay
Fahriye Sarac
Arzu Tas Ekiz
Irem Abaci
Ozge Aksoy
Hivda Ulbegi Polat
Saban Tekin
Stefan Dimitrov
Aykut Ozkul
Gerhard Wingender
Ihsan Gursel
Mehmet Ozturk
Mehmet Inan
机构
[1] Izmir Biomedicine and Genome Center,Izmir International Biomedicine and Genome Institute
[2] Dokuz Eylul University,undefined
[3] Pendik Veterinary Research and Control Institute,undefined
[4] Marmara Research Center,undefined
[5] TUBITAK,undefined
[6] University of Health Sciences,undefined
[7] Ankara University,undefined
[8] Akdeniz University,undefined
[9] VIB-UGent Center for Medical Biotechnology,undefined
[10] Lund University,undefined
[11] Erzurum Technical University,undefined
[12] Ankara Medipol University,undefined
[13] Imperial College London,undefined
[14] Izmir Tinaztepe University,undefined
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摘要
Recombinant protein-based SARS-CoV-2 vaccines are needed to fill the vaccine equity gap. Because protein-subunit based vaccines are easier and cheaper to produce and do not require special storage/transportation conditions, they are suitable for low-/middle-income countries. Here, we report our vaccine development studies with the receptor binding domain of the SARS-CoV-2 Delta Plus strain (RBD-DP) which caused increased hospitalizations compared to other variants. First, we expressed RBD-DP in the Pichia pastoris yeast system and upscaled it to a 5-L fermenter for production. After three-step purification, we obtained RBD-DP with > 95% purity from a protein yield of > 1 g/L of supernatant. Several biophysical and biochemical characterizations were performed to confirm its identity, stability, and functionality. Then, it was formulated in different contents with Alum and CpG for mice immunization. After three doses of immunization, IgG titers from sera reached to > 106 and most importantly it showed high T-cell responses which are required for an effective vaccine to prevent severe COVID-19 disease. A live neutralization test was performed with both the Wuhan strain (B.1.1.7) and Delta strain (B.1.617.2) and it showed high neutralization antibody content for both strains. A challenge study with SARS-CoV-2 infected K18-hACE2 transgenic mice showed good immunoprotective activity with no viruses in the lungs and no lung inflammation for all immunized mice.
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