首页> 外文OA文献 >A vaccine conjugate of 'ISCAR' immunocarrier and peptide epitopes of the E7 cervical cancer-associated protein of human papillomavirus type 16 elicits specific Th1- and Th2-type responses in immunized mice in the absence of oil-based adjuvants.
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A vaccine conjugate of 'ISCAR' immunocarrier and peptide epitopes of the E7 cervical cancer-associated protein of human papillomavirus type 16 elicits specific Th1- and Th2-type responses in immunized mice in the absence of oil-based adjuvants.

机译:“ ISCAR”免疫载体和人乳头瘤病毒16型E7宫颈癌相关蛋白的肽表位的疫苗偶联物在不存在油基佐剂的情况下在免疫小鼠中引起特定的Th1和Th2型反应。

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摘要

TraT protein, known as ISCAR (= Immunostimulatory Carrier), is one of a family of integral membrane proteins (Imps) of Escherichia coli representing powerful carrier molecules which when injected into experimental animals generate substantial antibody and T proliferative responses to molecules conjugated to it. We extend these findings to show that ISCAR functions to stimulate Th1- and Th2-type responses, including specific cytotoxic T cells and tumour protection. We report here that by conjugating to ISCAR a 19mer peptide containing linear B epitopes, a T helper (Th) epitope, and a H-2b-restricted T cytotoxic (CTL) epitope of E7 protein of human papillomavirus type 16 (HPV16), and immunizing C57B1/6 (H-2b) mice, we elicited (i) specific IgG2a and IgG1 antibodies; (ii) IL-2 and IL-4 production by specifically recalled lymph node cells in vitro; (iii) cytotoxic T lymphocytes which specifically killed both E7 peptide-pulsed, and whole E7 gene-transfected tumour target cells; and (iv) in vivo protection against an E7 gene-transfected tumour cell inoculum. These findings have implications for the design of vaccines to stimulate immune responses to endogenously processed target antigens (e.g. tumour-associated antigens) without the unwanted side effects of oil-based adjuvants. In addition they support the case for a E7-targeted therapeutic vaccine for HPV-associated human cervical cancer.
机译:TraT蛋白被称为ISCAR(=免疫刺激载体),是大肠杆菌的整体膜蛋白(Imps)家族之一,代表强大的载体分子,当注入实验动物体内时会产生大量抗体和与其结合的分子产生T增殖反应。我们扩展这些发现,以表明ISCAR的功能可刺激Th1和Th2型反应,包括特异性细胞毒性T细胞和肿瘤保护。我们在这里报告说,通过与ISCAR共轭包含线性B表位,T辅助(Th)表位和人乳头瘤病毒16型(HPV16)E7蛋白的H-2b限制性T细胞毒性(CTL)表位的19mer肽,并且免疫C57B1 / 6(H-2b)小鼠,我们引发了(i)特异性IgG2a和IgG1抗体; (ii)专门召回的淋巴结细胞在体外产生IL-2和IL-4; (iii)细胞毒性T淋巴细胞,其特异性杀死经E7肽脉冲作用的和经E7基因整体转染的肿瘤靶细胞; (iv)针对经E7基因转染的肿瘤细胞接种物的体内保护。这些发现对设计疫苗以刺激对内源加工的靶抗原(例如肿瘤相关抗原)的免疫反应没有油基佐剂的有害副作用有影响。此外,他们支持针对HPV相关的人宫颈癌的E7靶向治疗疫苗。

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