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The preparation of an infectious full-length cDNA clone of Saffold virus.


ABSTRACT: The pathogenicity of Saffold virus (SAFV) among humans still remains unclear, although it was identified as a novel human cardiovirus in 2007. In order to encourage the molecular pathogenetic studies of SAFV, we generated an infectious cDNA clone of SAFV type 3 (SAFV-3). The present study demonstrated that the synthesis of the full-length infectious RNA by T7 RNA polymerase was terminated by a homologous sequence motif with the human preproparathyroid hormone (PTH) signal in the SAFV-3 genome. To obtain the infectious RNA using T7 promoter, a variant of T7 RNA polymerase, which fails to recognize the PTH signal, was useful. This study will provide a valuable technical insight into the reverse genetics of SAFV.

SUBMITTER: Himeda T 

PROVIDER: S-EPMC3062622 | biostudies-literature | 2011

REPOSITORIES: biostudies-literature

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The preparation of an infectious full-length cDNA clone of Saffold virus.

Himeda Toshiki T   Hosomi Takushi T   Asif Naeem N   Shimizu Hiroyuki H   Okuwa Takako T   Muraki Yasushi Y   Ohara Yoshiro Y  

Virology journal 20110309


The pathogenicity of Saffold virus (SAFV) among humans still remains unclear, although it was identified as a novel human cardiovirus in 2007. In order to encourage the molecular pathogenetic studies of SAFV, we generated an infectious cDNA clone of SAFV type 3 (SAFV-3). The present study demonstrated that the synthesis of the full-length infectious RNA by T7 RNA polymerase was terminated by a homologous sequence motif with the human preproparathyroid hormone (PTH) signal in the SAFV-3 genome. T  ...[more]

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