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多价4-1BB结合适体共刺激CD8 + T细胞并抑制小鼠肿瘤生长。

Multivalent 4-1BB binding aptamers costimulate CD8+ T cells and inhibit tumor growth in mice.

作者信息

McNamara James O, Kolonias Despina, Pastor Fernando, Mittler Robert S, Chen Lieping, Giangrande Paloma H, Sullenger Bruce, Gilboa Eli

机构信息

Department of Surgery, Duke University Medical Center, Durham, North Carolina, USA.

出版信息

J Clin Invest. 2008 Jan;118(1):376-86. doi: 10.1172/JCI33365.

Abstract

4-1BB is a major costimulatory receptor that promotes the survival and expansion of activated T cells. Administration of agonistic anti-4-1BB Abs has been previously shown to enhance tumor immunity in mice. Abs are cell-based products posing significant cost, manufacturing, and regulatory challenges. Aptamers are oligonucleotide-based ligands that exhibit specificity and avidity comparable to, or exceeding, that of Abs. To date, various aptamers have been shown to inhibit the function of their cognate target. Here, we have described the development of an aptamer that binds 4-1BB expressed on the surface of activated mouse T cells and shown that multivalent configurations of the aptamer costimulated T cell activation in vitro and mediated tumor rejection in mice. Because aptamers can be chemically synthesized, manufacturing and the regulatory approval process should be substantially simpler and less costly than for Abs. Agonistic aptamers could therefore represent a superior alternative to Abs for the therapeutic manipulation of the immune system.

摘要

4-1BB是一种主要的共刺激受体,可促进活化T细胞的存活和增殖。先前已证明,给予激动性抗4-1BB抗体可增强小鼠的肿瘤免疫。抗体是基于细胞的产品,在成本、生产和监管方面面临重大挑战。适体是基于寡核苷酸的配体,其特异性和亲和力与抗体相当或超过抗体。迄今为止,已证明各种适体可抑制其同源靶标的功能。在此,我们描述了一种与活化小鼠T细胞表面表达的4-1BB结合的适体的开发,并表明该适体的多价构型在体外共刺激T细胞活化,并在小鼠中介导肿瘤排斥。由于适体可以化学合成,其生产和监管审批过程应该比抗体更简单、成本更低。因此,激动性适体可能是用于免疫系统治疗操作的抗体的一种更优越的替代品。

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