Department of Biochemistry, Biocenter, University of Würzburg, Würzburg, Germany.
J Transl Med. 2011 Oct 11;9:172. doi: 10.1186/1479-5876-9-172.
Oncolytic viral tumor therapy is an emerging field in the fight against cancer with rising numbers of clinical trials and the first clinically approved product (Adenovirus for the treatment of Head and Neck Cancer in China) in this field. Yet, until recently no general (bio)marker or reporter gene was described that could be used to evaluate successful tumor colonization and/or transgene expression in other biological therapies.
Here, a bacterial glucuronidase (GusA) encoded by biological therapeutics (e.g. oncolytic viruses) was used as reporter system.
Using fluorogenic probes that were specifically activated by glucuronidase we could show 1) preferential activation in tumors, 2) renal excretion of the activated fluorescent compounds and 3) reproducible detection of GusA in the serum of oncolytic vaccinia virus treated, tumor bearing mice in several tumor models. Time course studies revealed that reliable differentiation between tumor bearing and healthy mice can be done as early as 9 days post injection of the virus. Regarding the sensitivity of the newly developed assay system, we could show that a single infected tumor cell could be reliably detected in this assay.
GusA therefore has the potential to be used as a general marker in the preclinical and clinical evaluation of (novel) biological therapies as well as being useful for the detection of rare cells such as circulating tumor cells.
溶瘤病毒肿瘤治疗是癌症治疗领域的一个新兴领域,临床试验的数量不断增加,并且该领域的第一个临床批准产品(中国用于治疗头颈部癌症的腺病毒)。然而,直到最近,还没有描述一种通用(生物)标志物或报告基因,可以用于评估其他生物疗法中成功的肿瘤定植和/或转基因表达。
在这里,生物疗法(例如溶瘤病毒)编码的细菌β-葡糖苷酸酶(GusA)被用作报告系统。
使用特异性被β-葡糖苷酸酶激活的荧光探针,我们可以证明 1)在肿瘤中优先激活,2)激活的荧光化合物的肾脏排泄,以及 3)在几种肿瘤模型中,溶瘤痘苗病毒治疗的荷瘤小鼠的血清中可重复检测到 GusA。时程研究表明,早在病毒注射后 9 天,就可以可靠地区分荷瘤和健康小鼠。关于新开发的检测系统的灵敏度,我们可以证明在该检测中可以可靠地检测到单个感染的肿瘤细胞。
因此,GusA 有可能成为(新型)生物疗法的临床前和临床评估中的通用标志物,并且对于检测循环肿瘤细胞等稀有细胞也很有用。
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