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Carbohydrate-Based Ice Recrystallization Inhibitors Increase Infectivity and Thermostability of Viral Vectors

机译:基于碳水化合物的冰重结晶抑制剂可提高病毒载体的感染性和热稳定性

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摘要

The inability of vaccines to retain sufficient thermostability has been an obstacle to global vaccination programs. To address this major limitation, we utilized carbohydrate-based ice recrystallization inhibitors (IRIs) to eliminate the cold chain and stabilize the potency of Vaccinia virus (VV), Vesicular Stomatitis virus (VSV) and Herpes virus-1 (HSV-1). The impact of these IRIs was tested on the potency of the viral vectors using a plaque forming unit assay following room temperature storage, cryopreservation with successive freeze-thaw cycles and lyophilization. Viral potency after storage with all three conditions demonstrated that N-octyl-gluconamide (NOGlc) recovered the infectivity of shelf stored VV, 5.6 Log10 PFU mL−1 during 40 days, and HSV-1, 2.7 Log10 PFU mL−1 during 9 days. Carbon-linked antifreeze glycoprotein analogue ornithine-glycine-glycine-galactose (OGG-Gal) increases the recovery of VV and VSV more than 1 Log10 PFU mL−1 after 10 freeze-thaw cycles. In VSV, cryostorage with OGG-Gal maintains high infectivity and reduces temperature-induced aggregation of viral particles by 2 times that of the control. In total, OGG-Gal and NOGlc preserve virus potency during cryostorage. Remarkably, NOGlc has potential to eliminate the cold chain and permit room temperature storage of viral vectors.
机译:疫苗无法保持足够的热稳定性一直是全球疫苗接种计划的障碍。为了解决这一主要限制,我们利用了基于碳水化合物的冰重结晶抑制剂(IRIs)来消除冷链并稳定牛痘病毒(VV),水泡性口腔炎病毒(VSV)和疱疹病毒1(HSV-1)的效力。在室温下保存,连续冷冻-解冻循环冷冻保存和冻干之后,使用噬斑形成单位测定法测试了这些IRI对病毒载体效力的影响。在所有三个条件下储存后的病毒效价表明,N-辛基-葡糖酰胺(NOGlc)在40天期间恢复了5.6 Log10 PFU mL -1 的架子储存VV的感染性,而HSV-1则为2.7 Log10的感染性在9天内PFU mL -1 。碳链抗冻糖蛋白类似物鸟氨酸-甘氨酸-甘氨酸-半乳糖(OGG-Gal)在10次冻融循环后,可使VV和VSV的回收率超过1 Log10 PFU mL -1 。在VSV中,使用OGG-Gal进行冷冻保存可保持较高的感染力,并将温度诱导的病毒颗粒聚集降低为对照组的2倍。总体而言,OGG-Gal和NOGlc可以在冷冻保存过程中保留病毒效力。值得注意的是,NOGlc具有消除冷链并允许在室温下保存病毒载体的潜力。

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