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Antibody Detection and Kinetics of Antibody Production during Early Stages of Immunization with Hepatitis B Virus Vaccine▿

机译:乙肝病毒疫苗免疫早期阶段的抗体检测和抗体产生动力学Kin

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摘要

Antibodies to influenza virus and human immunodeficiency virus are detectable in B cells during the early stages of the immune response, prior to their occurrence in plasma. To investigate similar phenomena in a model of immunization against hepatitis B virus (HBV) infection, medical students in Ghana were screened for HBV markers, HBV surface (HBs) antigen (HBsAg), and HBV core antibodies (anti-HBc). Consenting volunteers, 24 of whom were seronegative (susceptible) and 2 of whom were positive for anti-HBc (prior infection), were vaccinated on day 0, day 40, and 6 months. Two sets of 10 blood samples, sequentially collected at intervals of 2 days following each immunization on days 0 and 40, were processed into B-cell lysates and plasma. Solid-phase HBsAg coated on microtiter plates for enzyme immunoassay or nitrocellulose membranes for dot blot assay was used to detect anti-HBs activity by an indirect antiglobulin assay. A commercially procured sandwich immunoassay was used, along with an enzyme-linked immunosorbent assay and a dot blot assay, for the detection of anti-HBs in B-cell lysates and plasma. Following the first injection of vaccine, a single sample of B-cell lysate collected between 5 and 21 days revealed anti-HBs in 18/21 subjects with no plasma antibodies detectable by sandwich immunoassay. After the booster dose was injected on day 40, a single sample of B-cell lysate collected between 44 and 49 days showed anti-HBs in 16/19 subjects, and this was accompanied by plasma antibodies in 8 subjects. In contrast, between 8 and 13 days, both subjects with prior HBV infection showed anti-HBs in B-cell lysates and plasma. Thus, primary immunization with the HBV vaccine appears to transiently elicit low-affinity anti-HBs in B-cell lysates into plasma.
机译:在免疫反应的早期阶段,在血浆中出现B细胞之前,就可以检测到B型流感病毒和人类免疫缺陷病毒的抗体。为了研究针对乙型肝炎病毒(HBV)感染的免疫模型中的类似现象,对加纳的医学生进行了HBV标记,HBV表面(HBs)抗原(HBsAg)和HBV核心抗体(抗HBc)筛选。同意的志愿者在第0天,第40天和6个月进行了疫苗接种,其中24例血清阴性(易感),2例抗HBc阳性(先前感染)。在第0天和第40天进行每次免疫后,每隔2天按2天的间隔依次收集两组10个血样,将其处理成B细胞裂解物和血浆。涂在微量滴定板上的固相HBsAg用于酶免疫测定或硝酸纤维素膜用于斑点印迹测定,用于通过间接抗球蛋白测定检测抗HBs活性。使用商业购买的夹心免疫测定法,酶联免疫吸附测定法和斑点印迹测定法,用于检测B细胞裂解物和血浆中的抗HBs。首次注射疫苗后,在5天至21天之间收集的B细胞裂解物样本显示18/21位受试者中存在抗HBs,而三明治免疫测定法未检测到血浆抗体。在第40天注射加强剂量后,在44天至49天之间收集的单个B细胞裂解物样品在16/19位受试者中显示抗HBs,并且在8位受试者中伴有血浆抗体。相比之下,在8到13天之间,两个先前感染过HBV的受试者在B细胞裂解液和血浆中均显示出抗HBs。因此,用HBV疫苗进行的初次免疫似乎可以瞬间引起B细胞裂解物中的低亲和力抗HBs进入血浆。

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