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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Cholecystokinin type 2 receptor in colorectal cancer: diagnostic and therapeutic target
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Cholecystokinin type 2 receptor in colorectal cancer: diagnostic and therapeutic target

机译:胆囊酮蛋白在结肠直肠癌中的2种受体:诊断和治疗目标

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Introduction Cholecystokinin type 2 receptor (CCK2R), which mediates the action of gastrin and cholecystokinin (CCK), has been demonstrated to promote the proliferation of colorectal cancer (CRC). A number of studies showed that CCK2R overexpressed in gastric cancer and pancreatic cancer but few in CRC. The correlation between CCK2R expression and clinicopathological characteristics is also not clear. Methods This study investigated CCK2R expression in a wide range of cell lines and clinical CRC samples, and explored expression pattern and prognostic value of CCK2R in relation to clinicopathological parameters. The location and expression levels of CCK2R were measured by immunocytochemical (ICC), qRT-PCR and Western blot. The druggability and antineoplastic effects of CCK2R as a therapeutic target were investigated using an anti-CCK2R targeting recombinant toxin named rCCK8PE38 by CCK-8 assay. Results Compared with paracarcinoma tissues, tumor samples showed overexpression of CCK2R (p = 0.028) including both CRC tissue and plasma samples, with plasma detection showing a significant indication for CCK2R evaluation. Aberrant expression correlated significantly with histological type (p = 0.032) and p53 status (p < 0.01), and patients with CCK2R overexpression had significantly lower disease-free survival. Application of rCCK8PE38 demonstrated the specificity and druggability of CCK2R as a therapeutic target, providing a strategy for clinical case screening of drugs targeting CCK2R. Conclusion This study highlighted the aberrant expression and clinical correlation of CCK2R and reveals its diagnostic, prognostic and treatment value in CRC. We hypothesize that CCK2R serve as a target for the diagnosis and treatment of this cancer.
机译:引言胆囊收缩素2型受体(CCK2R)介导胃泌素和胆囊收缩素(CCK)的作用,已被证明可促进结直肠癌(CRC)的增殖。大量研究表明,CCK2R在胃癌和胰腺癌中过度表达,但在大肠癌中很少表达。CCK2R表达与临床病理特征之间的相关性也不清楚。方法本研究调查了CCK2R在多种细胞系和临床大肠癌样本中的表达,并探讨了CCK2R的表达模式和预后价值与临床病理参数的关系。通过免疫细胞化学(ICC)、qRT PCR和Western blot检测CCK2R的位置和表达水平。通过CCK-8分析,使用抗CCK2R靶向重组毒素rCCK8PE38,研究了CCK2R作为治疗靶点的可药物性和抗肿瘤作用。结果与癌旁组织相比,肿瘤样本显示CCK2R过度表达(p=0.028),包括大肠癌组织和血浆样本,血浆检测显示CCK2R评估的重要指标。异常表达与组织学类型(p=0.032)和p53状态(p<0.01)显著相关,CCK2R过度表达的患者无病生存率显著降低。rCCK8PE38的应用证明了CCK2R作为治疗靶点的特异性和可药物性,为临床病例筛选针对CCK2R的药物提供了策略。结论本研究强调了CCK2R的异常表达和临床相关性,揭示了其在大肠癌中的诊断、预后和治疗价值。我们假设CCK2R是诊断和治疗这种癌症的靶点。

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  • 作者单位

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    China Japan Union Hosp Xian Tai Da Jie 126 Changchun 130033 Peoples R China;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    China Japan Union Hosp Xian Tai Da Jie 126 Changchun 130033 Peoples R China;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

    Jilin Univ Key Lab Zoonosis Res Double First Class Discipline Human Anim Med Inst Zoonosis Coll;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学 ;
  • 关键词

    Cholecystokinin type 2 receptor; Diagnostic target; Therapeutic target; Colorectal cancer;

    机译:胆囊蛋白类型2受体;诊断靶;治疗目标;结直肠癌;

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