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研究领域生物医学和临床科学瘤学和致癌症预测和预后标志物
揭示治疗潜力:在癌中发现TGFßR1的预后标志物和潜在抑制剂

揭示治疗潜力:在癌中发现TGFßR1的预后标志物和潜在抑制剂

Samvedna Singh ¹, Himanshi Gupta ¹, Subhav Sinha ², Aman Chandra Kaushik ³, Shraddha Kapoor ¹, Amit Kumar Awasthi ¹, Imteyaz Qamar ¹, Shakti Sahi ¹

Samvedna Singh ¹, Himanshi Gupta ¹, Subhav Sinha ²

¹School of Biotechnology, Gautam Buddha University, Greater Noida, UP, India.
²Founder-Eigengram, India.
³Department of Bioinformatics and Biological Statistics, School of Life Sciences and Biotechnology, Shanghai Jiao Tong University, Shanghai, China.

⁰School of Biotechnology, Gautam Buddha University, Greater Noida, UP, India.

Computational Biology and Chemistry +

|

2025年八月26日

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在PubMed上查看摘要

概括

此摘要是机器生成的。

胰腺癌研究发现了新的预后标志物和潜在的药物点. 针对TGF-β受体1的新化合物对未来的胰腺癌疗法具有前途.

科学领域

癌症学
计算化学
分子生物学

背景情况

胰腺癌的存活率很低,对化疗的耐药性也很低.
没有早期发现胰腺癌的标志物.
不同表达的基因 (AHNAK2,TSC2,LAMC2,C3orf52,IGFBP3) 与预后不佳有关.

研究的目的

确定胰腺癌的新预后标志物.
研究向TGF-β信号通路的治疗潜力.
发现抑制TGFßR1的新型小分子.

主要方法

不同基因表达分析和生存分析.
对TGFßR1进行基于结构的虚拟选.
分子动力学模拟和总体采样以分析结合机制.
与基准抑制剂 (Galunisertib,Vactosertib) 的结合自由能量的比较.

主要成果

在胰腺癌中发现了SMAD4突变 (20. 93%),突出显示了TGF-β通路的相关性.
三种化合物 (化合物6,7,8) 根据药理动力和结合性而入围.
分子动力学发现关键残留物 (ASP351,LYS232,LYS337,LYS213) 对TGFßR1的稳定性至关重要.
入围化合物的自由能量 (ΔG) 比基准抑制剂低.

结论

向TGF-β信号通路是胰腺癌的一个有前途的治疗策略.
通过虚拟查发现的新化合物显示为TGFßR1抑制剂的潜力.
了解TGFßR1结合机制为药物开发提供了洞察力.

关键词:

分子动态模拟胰腺癌预测标志物抑制TGF-β的作用转化生长因子β (TGF-β) 总体采样

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