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单纯疱疹病毒1型DNA中编码糖蛋白D和I的US6和US7区域可能影响神经侵袭性。

Regions US6 and US7 of herpes simplex virus type 1 DNA encoding glycoproteins D and I may influence neuroinvasivity.

作者信息

Rajcáni J, Kostál M, Kaerner H C

机构信息

Institute of Virology, Slovak Academy of Sciences, Bratislava.

出版信息

Acta Virol. 1994 Apr;38(2):89-95.

PMID:7976867
Abstract

Recombinants were prepared by replacing a 1931 bp region of the BamHI J fragment (0.906-0.920) of the pathogenic ANGpath DNA-coding for glycoprotein D (gD) and a part of glycoprotein I (gI)--by the corresponding sequence of nonpathogenic KOS DNA (Kaerner et al., 1991) and tested in DBA/2 mice. The strain ANGpath and the control recombinant ANGpath/gD-gIpath, prepared by back transfer of the given ANGpath DNA fragment into ANGpath/gD-gIdellacZ+ DNA, were pathogenic after intraperitoneal inoculation. In contrast, mice infected with the strain KOS and the low-pathogenic recombinant ANGpath/gD-gIKOS survived peripheral virus administration. Both the strain KOS and the low-pathogenic recombinant ANDpath/gD-gIKOS spread by bloodstream to spleen, liver and adrenal glands but did not multiply in spinal cord. Nevertheless, the antigen of low-pathogenic recombinant ANGpath/gD-gIKOS was found in retroperitoneal vegetative nerves and ganglia. On the other hand, the strain ANGpath and the pathogenic recombinant ANGpath/gD-gIpath multiplied in cerebrospinal nerves and spinal cord causing typical hind leg paralysis.

摘要

通过用非致病性KOS DNA的相应序列(Kaerner等人,1991年)替换致病性ANGpath DNA中编码糖蛋白D(gD)和部分糖蛋白I(gI)的BamHI J片段(0.906 - 0.920)的1931 bp区域,制备了重组体,并在DBA/2小鼠中进行了测试。将给定的ANGpath DNA片段回转移到ANGpath/gD - gIdellacZ+ DNA中制备的菌株ANGpath和对照重组体ANGpath/gD - gIpath,经腹腔接种后具有致病性。相比之下,感染KOS菌株和低致病性重组体ANGpath/gD - gIKOS的小鼠在接受外周病毒接种后存活下来。KOS菌株和低致病性重组体ANDpath/gD - gIKOS都通过血流扩散到脾脏、肝脏和肾上腺,但在脊髓中不增殖。然而,在腹膜后植物神经和神经节中发现了低致病性重组体ANGpath/gD - gIKOS的抗原。另一方面,菌株ANGpath和致病性重组体ANGpath/gD - gIpath在脑脊髓神经和脊髓中增殖,导致典型的后腿麻痹。

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