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有证据表明腺病毒的五聚体基底参与增强与表皮生长因子结合的铜绿假单胞菌外毒素的毒性。

Evidence that the penton base of adenovirus is involved in potentiation of toxicity of Pseudomonas exotoxin conjugated to epidermal growth factor.

作者信息

Seth P, Fitzgerald D, Ginsberg H, Willingham M, Pastan I

出版信息

Mol Cell Biol. 1984 Aug;4(8):1528-33. doi: 10.1128/mcb.4.8.1528-1533.1984.

Abstract

When KB cells are incubated for 1 h with human adenovirus type 2 or type 5 (1 microgram/ml) and a conjugate of epidermal growth factor and Pseudomonas exotoxin (EGF-PE), protein synthesis is inhibited by 80 to 90%. Under these conditions, neither adenovirus nor EGF-PE alone has any effect on host protein synthesis. Thus, adenovirus enhances the toxicity of EGF-PE. A number of antibodies to intact virus and capsid components were tested for their ability to block the enhancing activity and virus uptake. At appropriate dilutions, antibodies prepared against intact virus and penton base blocked the enhancing activity without affecting virus uptake. Antibodies against hexon and fiber blocked virus uptake and enhancing activity in parallel. These studies suggest that the penton base is important in lysis of the vesicles which contain adenovirus and EGF-PE, and this base allows virus and toxin to enter the cytoplasm.

摘要

当KB细胞与人2型或5型腺病毒(1微克/毫升)以及表皮生长因子与绿脓杆菌外毒素的偶联物(EGF-PE)一起孵育1小时时,蛋白质合成被抑制80%至90%。在这些条件下,单独的腺病毒或EGF-PE对宿主蛋白质合成均无任何影响。因此,腺病毒增强了EGF-PE的毒性。测试了多种针对完整病毒和衣壳成分的抗体阻断增强活性和病毒摄取的能力。在适当稀释度下,针对完整病毒和五邻体基座制备的抗体阻断了增强活性,而不影响病毒摄取。针对六邻体和纤突的抗体则平行地阻断了病毒摄取和增强活性。这些研究表明,五邻体基座在含有腺病毒和EGF-PE的囊泡裂解中起重要作用,并且该基座使病毒和毒素能够进入细胞质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4fa1/368944/098dd830cecd/molcellb00150-0109-a.jpg

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