首页> 美国卫生研究院文献>Journal of Virology >Brucella abortus conjugated with a gp120 or V3 loop peptide derived from human immunodeficiency virus (HIV) type 1 induces neutralizing anti-HIV antibodies and the V3-B. abortus conjugate is effective even after CD4+ T-cell depletion.
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Brucella abortus conjugated with a gp120 or V3 loop peptide derived from human immunodeficiency virus (HIV) type 1 induces neutralizing anti-HIV antibodies and the V3-B. abortus conjugate is effective even after CD4+ T-cell depletion.

机译:流产布鲁氏菌与源自1型人类免疫缺陷病毒(HIV)的gp120或V3环肽缀合可诱导中和性抗HIV抗体和V3-B。流产结合物即使在CD4 + T细胞耗尽后仍然有效。

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摘要

Human immunodeficiency virus type 1 (HIV-1) infection is associated with loss of function and numbers of CD4+ T-helper cells. In order to bypass the requirement for CD4+ cells in antibody responses, we have utilized heat-inactivated Brucella abortus as a carrier. In this study we coupled a 14-mer V3 loop peptide (V3), which is homologous to 9 of 11 amino acids from the V3 loop of HIV-1 MN, and gp120 from HIV-1 SF2 to B. abortus [gp120(SF2)-B. abortus]. Our results showed that specific antibody responses, dominated by immunoglobulin G2a in BALB/c mice, were induced by these conjugates. Sera from the immunized mice bound native gp120 expressed on the surfaces of cells infected with a recombinant vaccinia virus gp160 vector (VPE16). Sera from mice immunized with gp120(SF2)-B. abortus inhibited binding of soluble CD4 to gp120, whereas sera from mice immunized with V3-B. abortus were ineffective. Sera from mice immunized with either conjugate were capable of blocking syncytium formation between CD4+ CEM cells and H9 cells chronically infected with the homologous virus. Sera from mice immunized with gp120(SF2)-B. abortus were more potent than sera from mice immunized with V3-B. abortus in inhibiting syncytia from heterologous HIV-1 laboratory strains. Importantly, in primary and secondary responses, V3-B. abortus evoked anti-HIV MN antibodies in mice depleted of CD4+ cells, and sera from these mice were able to inhibit syncytia. These findings indicate that B. abortus can provide carrier function for peptides and proteins from HIV-1 and suggest that they could be used for immunization of individuals with compromised CD4+ T-cell function.
机译:人类1型免疫缺陷病毒(HIV-1)感染与功能丧失和CD4 + T辅助细胞数量有关。为了绕过抗体反应中CD4 +细胞的需求,我们已利用热灭活的布鲁氏菌流产作为载体。在这项研究中,我们偶联了一个14-mer V3环肽(V3),它与HIV-1 MN的V3环中的11个氨基酸中的9个氨基酸同源,并且与HIV-1 SF2到B.流产[gp120(SF2 )-B。流产]。我们的结果表明,这些结合物诱导了BALB / c小鼠中以免疫球蛋白G2a为主的特异性抗体反应。来自经免疫的小鼠的血清结合在用重组牛痘病毒gp160载体(VPE16)感染的细胞表面上表达的天然gp120。用gp120(SF2)-B免疫的小鼠的血清。流产抑制可溶性CD4与gp120的结合,而用V3-B免疫的小鼠的血清。流产无效。用任一种结合物免疫的小鼠的血清能够阻断CD4 + CEM细胞和慢性感染同源病毒的H9细胞之间的合胞体形成。用gp120(SF2)-B免疫的小鼠的血清。与用V3-B免疫的小鼠的血清相比,流产更有效。流产抑制异源HIV-1实验室菌株合胞体。重要的是,在主要和次要响应中,V3-B。流产的小鼠在耗尽CD4 +细胞的小鼠中诱发抗HIV MN抗体,这些小鼠的血清能够抑制合胞体。这些发现表明流产芽孢杆菌可为HIV-1的肽和蛋白质提供载体功能,并暗示它们可用于免疫受损CD4 + T细胞功能的个体。

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