Bayard B, Bisbal C, Silhol M, Cnockaert J, Huez G, Lebleu B
Eur J Biochem. 1984 Jul 16;142(2):291-8. doi: 10.1111/j.1432-1033.1984.tb08284.x.
Metabolically stable analogues of (2'-5')oligo(adenylate), (2'-5')(A)n, might constitute a new class of antiviral agents as they mimic some of the effects of interferons. 2'-O-phosphoglyceryl derivatives of (2'-5')(A)n oligomers, (2'-5')(A)n-PGro have been synthesized by chemical modification of their terminal ribose residue. Such analogues are resistant to degradation by phosphodiesterases but remain sensitive to phosphatase activity, at least in cell-free extracts. In line with its increased stability, (2'-5')(A)n-PGro has a powerful antiviral activity against an RNA virus when microinjected with micropipettes into the cytoplasm of intact cells. This antiviral activity remains transient however, possibly as a consequence of degradation in intact cells. Since (2'-5')(A)n and its derivatives do not easily cross cell membranes, their possible use in antiviral chemotherapy is tightly linked with the development of vectors suitable for their administration in vivo.
(2'-5')寡腺苷酸(2'-5')(A)n的代谢稳定类似物可能构成一类新型抗病毒剂,因为它们模拟了干扰素的一些作用。通过对(2'-5')(A)n低聚物的末端核糖残基进行化学修饰,合成了(2'-5')(A)n的2'-O-磷酸甘油基衍生物(2'-5')(A)n-PGro。这类类似物对磷酸二酯酶的降解具有抗性,但至少在无细胞提取物中对磷酸酶活性仍敏感。与稳定性增加一致,当用微量移液器微量注射到完整细胞的细胞质中时,(2'-5')(A)n-PGro对RNA病毒具有强大的抗病毒活性。然而,这种抗病毒活性仍然是短暂的,可能是完整细胞中降解的结果。由于(2'-5')(A)n及其衍生物不易穿过细胞膜,它们在抗病毒化疗中的可能应用与适合其体内给药的载体的开发紧密相关。
