Background/Objectives: HER2, a critical diagnostic marker and therapeutic target in breast cancer, is a membrane receptor that forms diverse signaling complexes, the constituents of which have not been fully characterized in actual breast cancer tissues. Methods: In this study, we applied the Rapid Immunoprecipitation Mass Spectrometry of Endogenous Proteins (RIME) method, originally developed to explore transcription factor complexes, to identify the complexes formed by HER2 in HER2-positive breast cancer specimens. Results: Through our approach, we successfully identified multiple complex components, including MARCKS, a novel HER2-interacting partner, which we verified using both proximal ligation assay in cultured cells and immunohistochemistry in tissue sections. TCGA analysis further revealed that high MARCKS expression significantly correlates with ER negativity, as confirmed by multivariate analysis, suggesting its potential role as a prognostic indicator in aggressive breast cancer subtypes. Conclusions: These results demonstrate the capability of RIME to elucidate interactomes of membrane proteins such as HER2 in clinical tissue specimens. Furthermore, this study highlights its broader applicability beyond nuclear proteins, underscoring its potential for discovering novel prognostic and diagnostic clinical markers in diverse cancer types.
HER2 Interactome Profiling Reveals MARCKS as a Candidate Marker Associated with Aggressive Breast Cancer.
HER2 相互作用组分析揭示 MARCKS 是与侵袭性乳腺癌相关的候选标志物
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作者:Yokoyama Atsushi, Sawatsubashi Shun, Ebata Akiko, Miki Yasuhiro, Otsubo Yuri, Suzuki Takashi
| 期刊: | Cancers | 影响因子: | 4.400 |
| 时间: | 2025 | 起止号: | 2025 Sep 2; 17(17):2882 |
| doi: | 10.3390/cancers17172882 | 研究方向: | 肿瘤 |
| 疾病类型: | 乳腺癌 | ||
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