Identification of a Mimicry of the Protein that Potentially Isolates the Mutated p53 Material and Prevents Further Protein Accumulation

Ricardo Gobato, Abhijit Mitra
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Abstract

The team first screened a set of protein mimics originally designed to target Alzheimer's disease and type 2 diabetes. The results identify a mimicry of the protein that potentially isolates the mutated p53 material and prevents further protein accumulation. The researchers then showed that segregation of mutated p53 grains by protein mimicking restored the suppressive function of the p53 tumor, leading to the death of a wide range of cancer cells. Importantly, protein mimicry therapy effectively reduces tumors that contain mutated p53 while showing no significant toxins for healthy tissue, resulting in significantly longer survival. "As the prevalence of cancer increases worldwide, there is an urgent need for new cancer therapies to complement or replace existing therapies," said the study's lead author. Here we show the first successful use of a small molecule amyloid inhibitor as an anticancer agent. We believe that this will have a far-reaching impact, as it effectively bridges the gap between amyloid disease and cancer and is the basis for passing on information approaches in the design of new and robust cancer mutation therapies for the p53 mutation. Keywords: Cancer; Cells; Tissues; Tumors; Prevention; Prognosis; Diagnosis; Imaging; Screening, Treatment; Management
鉴定一种可能分离突变p53物质并阻止进一步蛋白质积累的蛋白质拟态
该团队首先筛选了一组最初设计用于阿尔茨海默病和2型糖尿病的蛋白质模拟物。结果确定了一种蛋白质的拟态,这种蛋白质可能分离出突变的p53物质,并防止进一步的蛋白质积累。研究人员随后表明,通过蛋白质模拟分离突变的p53颗粒,恢复了p53肿瘤的抑制功能,导致大量癌细胞死亡。重要的是,蛋白质模仿疗法有效地减少了含有突变p53的肿瘤,同时对健康组织没有明显的毒素,从而显着延长了生存期。该研究的主要作者说:“随着全球癌症发病率的上升,迫切需要新的癌症治疗方法来补充或取代现有的治疗方法。”在这里,我们展示了小分子淀粉样蛋白抑制剂作为抗癌剂的第一次成功使用。我们相信这将产生深远的影响,因为它有效地弥合了淀粉样蛋白疾病和癌症之间的差距,并且是在设计针对p53突变的新的和强大的癌症突变疗法时传递信息方法的基础。关键词:癌症;细胞;组织;肿瘤;预防;预后;诊断;成像;筛查、治疗;管理
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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