Yu Yuan, Li Jialu, Zhu Xuejun, Tang Xiaowen, Bao Yangyi, Sun Xiang, Huang Yuhui, Tian Fang, Liu Xiaomei, Yang Lin
The Cyrus Tang Hematology Center; Collaborative Innovation Center of Hematology, Soochow University; Suzhou Cancer Immunotherapy and Diagnosis Engineering Center, Suzhou.
Central Laboratory, Department of Hematology, The Affiliated Hospital of Nanjing University of Chinese Medicine, Jiangsu Province Hospital of Traditional Chinese Medicine, Nanjing.
Int J Nanomedicine. 2017 Mar 13;12:1969-1983. doi: 10.2147/IJN.S127575. eCollection 2017.
Nanobodies, named as VHHs (variable domain of heavy chain of HCAb [heavy-chain antibodies]), are derived from heavy-chain-only antibodies that circulate in sera of camelids. Their exceptional physicochemical properties, possibility of humanization, and unique antigen recognition properties make them excellent candidates for targeted delivery of biologically active components, including immunotoxins. In our previous efforts, we have successfully generated the monovalent and bivalent CD7 nanobody-based immunotoxins, which can effectively trigger the apoptosis of CD7-positive malignant cells. To pursue the possibility of translating those immunotoxins into clinics, we humanized the nanobody sequences (designated as dhuVHH6) as well as further truncated the exotoxin A (PE)-derived PE38 toxin to produce a more protease-resistant form, which is named as PE-LR, by deleting majority of PE domain II.
Three new types of immunotoxins, dhuVHH6-PE38, dVHH6-PE-LR, and dhuVHH6-PE-LR, were successfully constructed. These recombinant immunotoxins were expressed in and showed that nanobody immunotoxins have the benefits of easy soluble expression in a prokaryotic expression system. Flow cytometry results revealed that all immunotoxins still maintained the ability to bind specifically to CD7-positive T lymphocyte strains without binding to CD7-negative control cells. Laser scanning confocal microscopy revealed that these proteins can be endocytosed into the cytoplasm after binding with CD7-positive cells and that this phenomenon was not observed in CD7-negative cells. WST-8 experiments showed that all immunotoxins retained the highly effective and specific growth inhibition activity in CD7-positive cell lines and primary T-cell acute lymphoblastic leukemia (T-ALL) cells. Further in vivo animal model experiments showed that humanized dhuVHH6-PE38 immunotoxin can tolerate higher doses and extend the survival of NOD-PrkdcIl2rgNju (NCG) mice transplanted with CEM cells without any obvious decrease in body weight. Further studies on NCG mice model with patient-derived T-ALL cells, dhuVHH6-PE38 treatment, significantly prolonged mice survival with ~40% survival improvement. However, it was also noticed that although dhuVHH6-PE-LR showed strong antitumor effect in vitro, its in vivo antitumor efficacy was disappointing.
We have successfully constructed a targeted CD7 molecule-modified nanobody (CD7 molecule-improved nanobody) immunotoxin dhuVHH6-PE38 and demonstrated its potential for treating CD7-positive malignant tumors, especially T-cell acute lymphoblastic leukemia.
纳米抗体,也被称为VHHs(重链抗体的重链可变区),来源于仅存在于骆驼科动物血清中的重链抗体。其优异的物理化学性质、人源化的可能性以及独特的抗原识别特性使其成为包括免疫毒素在内的生物活性成分靶向递送的理想候选物。在我们之前的研究中,我们成功构建了基于单价和双价CD7纳米抗体的免疫毒素,它们能够有效触发CD7阳性恶性细胞的凋亡。为了探索将这些免疫毒素应用于临床的可能性,我们对纳米抗体序列进行了人源化(命名为dhuVHH6),并进一步截短了外毒素A(PE)衍生的PE38毒素,通过删除大部分PE结构域II产生了一种更具蛋白酶抗性的形式,命名为PE-LR。
成功构建了三种新型免疫毒素,即dhuVHH6-PE38、dVHH6-PE-LR和dhuVHH6-PE-LR。这些重组免疫毒素在原核表达系统中表达,结果表明纳米抗体免疫毒素具有易于可溶性表达的优点。流式细胞术结果显示,所有免疫毒素仍保持特异性结合CD7阳性T淋巴细胞株的能力,而不与CD7阴性对照细胞结合。激光扫描共聚焦显微镜显示,这些蛋白与CD7阳性细胞结合后可被内吞入细胞质,而在CD7阴性细胞中未观察到这种现象。WST-8实验表明,所有免疫毒素在CD7阳性细胞系和原发性T细胞急性淋巴细胞白血病(T-ALL)细胞中均保留了高效且特异性的生长抑制活性。进一步的体内动物模型实验表明,人源化的dhuVHH6-PE38免疫毒素能够耐受更高剂量,并延长移植了CEM细胞的NOD-PrkdcIl2rgNju(NCG)小鼠的生存期,且体重无明显下降。对移植了患者来源的T-ALL细胞的NCG小鼠模型进行的进一步研究表明,dhuVHH6-PE38治疗显著延长了小鼠的生存期,生存率提高了约40%。然而,也注意到尽管dhuVHH6-PE-LR在体外显示出强大的抗肿瘤作用,但其体内抗肿瘤疗效却令人失望。
我们成功构建了靶向CD7分子修饰的纳米抗体(CD7分子改良纳米抗体)免疫毒素dhuVHH6-PE38,并证明了其在治疗CD7阳性恶性肿瘤,尤其是T细胞急性淋巴细胞白血病方面的潜力。
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