Koch-Nolte Friedrich, Reyelt Jan, Schössow Britta, Schwarz Nicole, Scheuplein Felix, Rothenburg Stefan, Haag Friedrich, Alzogaray Vanina, Cauerhff Ana, Goldbaum Fernando A
Department of Immunology, Diagnostic Center, University Medical Center Hamburg-Eppendorf, Martinistr. 52, D-20246 Hamburg, Germany.
FASEB J. 2007 Nov;21(13):3490-8. doi: 10.1096/fj.07-8661com. Epub 2007 Jun 15.
The purpose of our study was to develop a tool for blocking the function of a specific leukocyte ecto-enzyme in vivo. ART2.2 is a toxin-related ecto-enzyme that transfers the ADP-ribose moiety from NAD onto other cell surface proteins. ART2.2 induces T cell death by activating the cytolytic P2x7 purinoceptor via ADP-ribosylation. Here, we report the generation of ART2.2-blocking single domain antibodies from an immunized llama. The variable domain of heavy-chain antibodies (VHH domain) represents the smallest known antigen-binding unit generated by adaptive immune responses. Their long CDR3 endows VHH domains with the extraordinary capacity to extend into and block molecular clefts. Following intravenous injection, the ART2.2-specific VHH domains effectively shut off the enzymatic and cytotoxic activities of ART2.2 in lymphatic organs. This blockade was highly specific (blocking ART2.2 but not the related enzymes ART1 or ART2.1), rapid (within 15 min after injection), and reversible (24 h after injection). Our findings constitute a proof of principle that opens up a new avenue for targeting leukocyte ecto-enzymes in vivo and that can serve as a model also for developing new antidotes against ADP-ribosylating toxins.
我们研究的目的是开发一种在体内阻断特定白细胞胞外酶功能的工具。ART2.2是一种与毒素相关的胞外酶,它将ADP-核糖部分从NAD转移到其他细胞表面蛋白上。ART2.2通过ADP-核糖基化激活溶细胞性P2x7嘌呤受体来诱导T细胞死亡。在此,我们报告了从免疫的羊驼中产生的ART2.2阻断单域抗体。重链抗体的可变域(VHH域)代表适应性免疫反应产生的已知最小抗原结合单位。它们长的互补决定区3(CDR3)赋予VHH域延伸进入并阻断分子裂隙的非凡能力。静脉注射后,ART2.2特异性VHH域有效地关闭了ART2.2在淋巴器官中的酶活性和细胞毒性活性。这种阻断具有高度特异性(阻断ART2.2但不阻断相关酶ART1或ART2.1)、快速(注射后15分钟内)且可逆(注射后24小时)。我们的发现构成了原理证明,为在体内靶向白细胞胞外酶开辟了一条新途径,并且也可作为开发针对ADP-核糖基化毒素的新解毒剂的模型。
