Perea Silvio E, Reyes Osvaldo, Puchades Yaquelin, Mendoza Osmani, Vispo Nelson S, Torrens Isis, Santos Alicia, Silva Ricardo, Acevedo Boris, López Ernesto, Falcón Viviana, Alonso Daniel F
Laboratory of Molecular Oncology, Division of Pharmaceuticals, Center for Genetic Engineering and Biotechnology, Havana, Cuba.
Cancer Res. 2004 Oct 1;64(19):7127-9. doi: 10.1158/0008-5472.CAN-04-2086.
Protein Kinase (casein kinase 2, CK2) is a serine-threonine kinase that is frequently dysregulated in many human tumors. Therefore we hypothesized that peptides capable of binding to the CK2 acidic domain may exhibit potential anticancer properties. By screening a random cyclic peptide phage display library, we have identified a novel peptide, P15, that abrogated CK2 phosphorylation by blocking the substrate in vitro. To verify its potential antineoplastic effect, P15 was fused to the cell-penetrating peptide derived from the HIV-Tat protein. Interestingly, P15-Tat induced apoptosis as evidenced by rapid caspase activation and cellular cytotoxicity in a variety of tumor cell lines. Furthermore, direct injection of P15-Tat into C57BL6 mice bearing day 7-established solid tumors, resulted in substantial regression of the tumor mass. Our findings describe a new proapoptotic cyclic peptide that blocks the CK2 phosphorylation and exhibits antitumor effect in vivo, indicating that the P15 peptide may potentially be used clinically to treat solid tumors or as an adjuvant for cancer therapy.
蛋白激酶(酪蛋白激酶2,CK2)是一种丝氨酸 - 苏氨酸激酶,在许多人类肿瘤中经常失调。因此,我们推测能够与CK2酸性结构域结合的肽可能具有潜在的抗癌特性。通过筛选随机环肽噬菌体展示文库,我们鉴定出一种新型肽P15,它在体外通过阻断底物来消除CK2磷酸化。为了验证其潜在的抗肿瘤作用,将P15与源自HIV-Tat蛋白的细胞穿透肽融合。有趣的是,P15-Tat诱导细胞凋亡,多种肿瘤细胞系中快速的半胱天冬酶激活和细胞毒性证明了这一点。此外,将P15-Tat直接注射到携带7天建立的实体瘤的C57BL6小鼠中,导致肿瘤块显著消退。我们的研究结果描述了一种新的促凋亡环肽,它可阻断CK2磷酸化并在体内表现出抗肿瘤作用,表明P15肽可能潜在地用于临床治疗实体瘤或作为癌症治疗的佐剂。
