首页> 外文期刊>Acta Virologica: International Journal >Efficient intranasal immunization of newborn mice with recombinant adenovirus expressing rotavirus protein VP4 against oral rotavirus infection.
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Efficient intranasal immunization of newborn mice with recombinant adenovirus expressing rotavirus protein VP4 against oral rotavirus infection.

机译:用表达轮状病毒蛋白VP4的重组腺病毒对口腔轮状病毒感染进行有效的鼻内免疫。

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Efficacy of passive protection of newborn mice against rotavirus infection by the rotavirus VP4 protein expressed by an adenoviral vector in mice was studied. The VP4 gene was inserted into the E1 region of adenoviral vector pJM17. Recombinant adenovirus Ad5N/VP4 was grown in 293 cells. Intramuscular (i.m.), oral or intranasal (i.n.) immunization of newborn mice with Ad5/VP4 resulted in appearance of VP4-specific antibodies. Specific IgG antibodies were detected in the serum and intestine specimens of i.m. vaccinated mice. Oral immunization elicited serum IgG antibodies and intestinal IgG and IgA antibodies. Compared with i.m. and oral applications, i.n. immunization led to higher levels of serum IgG and intestinal IgG and IgA antibodies. Pups were challenged twice with simian rotavirus SA11 strain orally at the days 7 and 8 after birth. Pups born to i.n. immunized dams achieved 100% protection from rotavirus-induced diarrhea after both challenges. The protection of pups born to orally immunized dams was 80%, while only 30% of pups born to i.m. immunized dams were protected after both challenges. I.n. immunization was most efficient in inducing rotavirus VP4-specific serum, intestinal and milk IgG or IgA in mice that protected newborn mice completely.
机译:研究了新生小鼠对腺病毒载体表达的轮状病毒VP4蛋白被动免疫轮状病毒感染的保护作用。将VP4基因插入腺病毒载体pJM17的E1区域。重组腺病毒Ad5N / VP4在293细胞中生长。用Ad5 / VP4对新生小鼠进行肌内(i.m.),口服或鼻内(i.n.)免疫导致出现VP4特异性抗体。在i.m.的血清和肠标本中检测到特异性IgG抗体。疫苗接种的小鼠。口服免疫可引起血清IgG抗体以及肠道IgG和IgA抗体。与我比较和口头申请免疫导致更高的血清IgG,肠道IgG和IgA抗体水平。在出生后第7天和第8天,口服猿猴轮状病毒SA11株对幼犬进行两次攻击。出生于i.n.两次挑战后,免疫的大坝都可100%防止轮状病毒引起的腹泻。口服免疫水坝出生的幼崽的保护率为80%,而免疫接种的幼崽仅受到30%的保护。两次挑战后,免疫大坝得到了保护。在。在完全保护新生小鼠的小鼠中,免疫接种最有效地诱导了轮状病毒VP4特异性血清,肠和乳IgG或IgA。

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