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Higher expression level and lower toxicity of genetically spliced rotavirus NSP4 in comparison to the full-length protein in E. coli
IJB-Iranian Journal of Biotechnology. 2016; 14 (2): 50-57
in English | IMEMR | ID: emr-193912
ABSTRACT

Background:

Rotavirus group A [RVA] is recognized as a major cause of severe gastroenteritis in children and new-born animals. Nonstructural protein 4 [NSP4] is responsible for the enterotoxic activity of these viruses in the villus epithelial cells. Amino acids 114-135 of NSP4 are known to form the diarrhea-inducing region of this viral enterotoxin. Therefore, developing an NSP4 lacking the enterotoxin domain could result in the introduction of a new subunit vaccine against rotaviruses in both humans and animals
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Index: IMEMR (Eastern Mediterranean) Language: English Journal: Iran. J. Biotechnol. Year: 2016

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Index: IMEMR (Eastern Mediterranean) Language: English Journal: Iran. J. Biotechnol. Year: 2016