(Arg)-SH2 超级结合器:通过阻断磷酸酪氨酸信号通路治疗黑色素瘤的一种有前途的新型抗癌疗法。
(Arg)-SH2 superbinder: a novel promising anticancer therapy to melanoma by blocking phosphotyrosine signaling.
机构信息
Department of Medical Genetics, School of Basic Medicine, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, 430030, China.
Ultrastructural Pathology Laboratory, Department of Pathology, School of Basic Medicine, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, 430030, China.
出版信息
J Exp Clin Cancer Res. 2018 Jul 5;37(1):138. doi: 10.1186/s13046-018-0812-5.
BACKGROUND
Melanoma is a malignant tumor with high misdiagnosis rate and poor prognosis. The bio-targeted therapy is a prevailing method in the treatment of melanoma; however, the accompanying drug resistance is inevitable. SH2 superbinder, a triple-mutant of the Src Homology 2 (SH2) domain, shows potent antitumor ability by replacing natural SH2-containing proteins and blocking multiple pY-based signaling pathways. Polyarginine (Arg), a powerful vector for intracellular delivery of large molecules, could transport therapeutic agents across cell membrane. The purpose of this study is to construct (Arg)-SH2 superbinder and investigate its effects on melanoma cells, expecting to provide potential new approaches for anti-cancer therapy and overcoming the unavoidable drug resistance of single-targeted antitumor agents.
METHODS
(Arg) and SH2 superbinder were fused to form (Arg)-SH2 superbinder via genetic engineering. Pull down assay was performed to identify that (Arg)-SH2 superbinder could capture a wide variety of pY proteins. Immunofluorescence was used to detect the efficiency of (Arg)-SH2 superbinder entering cells. The proliferation ability was assessed by MTT and colony formation assay. In addition, wound healing and transwell assay were performed to evaluate migration of B16F10, A375 and A375/DDP cells. Moreover, apoptosis caused by (Arg)-SH2 superbinder was analyzed by flow cytometry-based Annexin V/PI. Furthermore, western blot revealed that (Arg)-SH2 superbinder influenced some pY-related signaling pathways. Finally, B16F10 xenograft model was established to confirm whether (Arg)-SH2 superbinder could restrain the growth of tumor.
RESULTS
Our data showed that (Arg)-SH2 superbinder had the ability to enter melanoma cells effectively and displayed strong affinities for various pY proteins. Furthermore, (Arg)-SH2 superbinder could repress proliferation, migration and induce apoptosis of melanoma cells by regulating PI3K/AKT, MAPK/ERK and JAK/STAT signaling pathways. Importantly, (Arg)-SH2 superbinder could significantly inhibit the growth of tumor in mice.
CONCLUSIONS
(Arg)-SH2 superbinder exhibited high affinities for pY proteins, which showed effective anticancer ability by replacing SH2-containing proteins and blocking diverse pY-based pathways. The remarkable ability of (Arg)-SH2 superbinder to inhibit cancer cell proliferation and tumor growth might open the door to explore the SH2 superbinder as a therapeutic agent for cancer treatment.
背景
黑色素瘤是一种误诊率高、预后差的恶性肿瘤。生物靶向治疗是治疗黑色素瘤的主要方法,但随之而来的耐药性是不可避免的。SH2 超级结合器是Src Homology 2(SH2)结构域的三重突变体,通过取代天然含有 SH2 的蛋白质并阻断多种基于 pY 的信号通路,显示出强大的抗肿瘤能力。聚精氨酸(Arg)是一种将大分子递送到细胞内的强大载体,可以将治疗剂穿过细胞膜。本研究的目的是构建(Arg)-SH2 超级结合器并研究其对黑色素瘤细胞的影响,期望为癌症治疗提供新的方法,并克服单靶点抗肿瘤药物不可避免的耐药性。
方法
通过基因工程将(Arg)和 SH2 超级结合器融合形成(Arg)-SH2 超级结合器。通过下拉实验鉴定(Arg)-SH2 超级结合器可以捕获多种 pY 蛋白。免疫荧光检测(Arg)-SH2 超级结合器进入细胞的效率。通过 MTT 和集落形成实验评估增殖能力。此外,通过划痕愈合和 Transwell 实验评估 B16F10、A375 和 A375/DDP 细胞的迁移能力。此外,通过流式细胞术结合 Annexin V/PI 分析(Arg)-SH2 超级结合器引起的凋亡。进一步,Western blot 揭示(Arg)-SH2 超级结合器影响一些 pY 相关信号通路。最后,建立 B16F10 异种移植模型以确认(Arg)-SH2 超级结合器是否能抑制肿瘤生长。
结果
我们的数据表明,(Arg)-SH2 超级结合器能够有效地进入黑色素瘤细胞,并对各种 pY 蛋白具有很强的亲和力。此外,(Arg)-SH2 超级结合器通过调节 PI3K/AKT、MAPK/ERK 和 JAK/STAT 信号通路,抑制黑色素瘤细胞的增殖、迁移并诱导其凋亡。重要的是,(Arg)-SH2 超级结合器能显著抑制小鼠肿瘤的生长。
结论
(Arg)-SH2 超级结合器对 pY 蛋白具有高亲和力,通过取代含有 SH2 的蛋白质并阻断多种基于 pY 的途径,表现出有效的抗癌能力。(Arg)-SH2 超级结合器抑制癌细胞增殖和肿瘤生长的显著能力可能为探索 SH2 超级结合器作为癌症治疗的治疗剂开辟了道路。
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