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用于诱导抗体及保护小鼠抵抗胃内猫幽门螺杆菌感染的新型鼻内免疫技术。

Novel intranasal immunization techniques for antibody induction and protection of mice against gastric Helicobacter felis infection.

作者信息

Weltzin R, Kleanthous H, Guirakhoo F, Monath T P, Lee C K

机构信息

OraVax, Inc., Cambridge, MA 02139, USA.

出版信息

Vaccine. 1997 Mar;15(4):370-6. doi: 10.1016/s0264-410x(97)00203-x.

Abstract

Intranasal (i.n.) delivery of antigen can be highly effective for generating circulating and secretory antibody responses. Mice were immunized i.n. with two antigens, human IgA, and Helicobacter pylori urease in the presence or absence of mucosal adjuvant. To restrict antigen delivery to the upper airways, protein solutions were administered in a small volume without anesthesia. Repeated daily i.n. administration of antigen without adjuvant elicited high levels of specific IgG in serum and IgA in serum, saliva, and feces. Once weekly i.n. immunization with co-administration of cholera toxin or Escherichia coli heat-labile toxin as adjuvant elicited somewhat lower levels of antibody to urease. When challenged with Helicobacter felis, only mice immunized with urease in the presence of adjuvant were protected against gastric infection.

摘要

经鼻内(i.n.)递送抗原对于产生循环抗体和分泌性抗体反应可能非常有效。在存在或不存在黏膜佐剂的情况下,用两种抗原(人IgA和幽门螺杆菌脲酶)经鼻内免疫小鼠。为了将抗原递送至仅限于上呼吸道,在无麻醉情况下以小体积给予蛋白质溶液。每日重复经鼻内给予无佐剂的抗原可在血清中引发高水平的特异性IgG,在血清、唾液和粪便中引发高水平的IgA。每周一次经鼻内免疫并同时给予霍乱毒素或大肠杆菌不耐热毒素作为佐剂,引发的针对脲酶的抗体水平略低。当用猫幽门螺杆菌攻击时,只有在存在佐剂的情况下用脲酶免疫的小鼠能免受胃部感染。

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