Intra- and inter-patient diversity in hepatocellular carcinoma based on phosphorylation profiles-A pilot study in a single institution.

IF 2.6 4区 医学 Q2 GASTROENTEROLOGY & HEPATOLOGY Clinics and research in hepatology and gastroenterology Pub Date : 2024-11-15 DOI:10.1016/j.clinre.2024.102497
Kan Toriguchi, Etsuro Hatano, Makoto Sudo, Ikuo Nakamura, Seiko Hirono
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Abstract

Background: Recent studies have addressed the efficacy of targeted drugs against hepatocellular carcinoma. However, most tumors escape a single kinase inhibition; co-inhibition of additional signaling pathways re-sensitizes resistant cancer cells to targeted drugs, thus reinforcing the importance of combination therapy for drug-resistant tumors. This study aimed to clarify the phosphorylation profiles of representative cancer-related tyrosine kinases in hepatocellular carcinoma to focus on potential therapeutic targets and to investigate the possibility of expanding combination therapy options using targeted drugs.

Materials and methods: Patients' whole blood, hepatocellular carcinoma tissue, and adjacent hepatic tissues were obtained during surgeries from 10 patients. All patients showed negative results for hepatitis B and hepatitis C RNA and none had a history of heavy drinking. The activation of receptor tyrosine kinases (RTKs) was analyzed by using a human RTK phosphorylation antibody array.

Results: Among 62 different phospho-RTKs, 26 were activated in tumor tissues, of which ACK1, Dtk, Fyn, and Lyn were positive in 9 out of 10 cases. The median concordance rates of activated tumor and serum RTKs in each patient was 50%. There was an inter- and intra-patient diversity of phosphorylation profiles in the serum, tumor of resected specimens, and non-tumor tissue of resected specimens in the same patients.

Conclusion: There was an intra- and inter- patient diversity in the activation of important and representative cancer-related RTKs. Expanding on this approach will allow us to learn how to predict the best combination of targets for each patient and to prioritize those combinations for clinical testing.

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基于磷酸化图谱的肝细胞癌患者内部和患者之间的多样性--在一家机构进行的试点研究。
背景:最近的研究探讨了靶向药物对肝细胞癌的疗效。然而,大多数肿瘤都能逃脱单一激酶抑制;联合抑制其他信号通路会使耐药癌细胞对靶向药物重新敏感,从而加强了联合疗法对耐药肿瘤的重要性。本研究旨在阐明肝细胞癌中代表性癌症相关酪氨酸激酶的磷酸化谱,以关注潜在的治疗靶点,并研究使用靶向药物扩大联合治疗选择的可能性:10例患者的全血、肝细胞癌组织和邻近肝组织均在手术过程中获得。所有患者的乙型肝炎和丙型肝炎 RNA 结果均为阴性,且均无酗酒史。使用人类 RTK 磷酸化抗体阵列分析了受体酪氨酸激酶(RTK)的激活情况:结果:在62种不同的磷酸化RTKs中,有26种在肿瘤组织中被激活,其中ACK1、Dtk、Fyn和Lyn在10个病例中有9个呈阳性。每位患者的肿瘤和血清RTKs激活的中位吻合率为50%。同一患者的血清、切除标本的肿瘤和切除标本的非肿瘤组织中的磷酸化图谱在患者之间和患者内部存在多样性:结论:重要的、具有代表性的癌症相关 RTKs 的激活在患者体内和患者之间存在多样性。拓展这种方法将使我们学会如何预测每位患者的最佳靶点组合,并优先选择这些组合进行临床测试。
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来源期刊
CiteScore
4.30
自引率
3.70%
发文量
198
审稿时长
42 days
期刊介绍: Clinics and Research in Hepatology and Gastroenterology publishes high-quality original research papers in the field of hepatology and gastroenterology. The editors put the accent on rapid communication of new research and clinical developments and so called "hot topic" issues. Following a clear Editorial line, besides original articles and case reports, each issue features editorials, commentaries and reviews. The journal encourages research and discussion between all those involved in the specialty on an international level. All articles are peer reviewed by international experts, the articles in press are online and indexed in the international databases (Current Contents, Pubmed, Scopus, Science Direct). Clinics and Research in Hepatology and Gastroenterology is a subscription journal (with optional open access), which allows you to publish your research without any cost to you (unless you proactively chose the open access option). Your article will be available to all researchers around the globe whose institution has a subscription to the journal.
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