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FBXW7 - 版本历史
2026-04-18T21:33:49Z
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2025年12月29日 (一) 16:16 77921020
2025-12-29T16:16:52Z
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77921020
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77921020:建立内容为“<div style="padding: 0 4%; line-height: 1.8; color: #1e293b; font-family: 'Helvetica Neue', Helvetica, 'PingFang SC', Arial, sans-serif; background-color: #ffffff…”的新页面
2025-12-29T16:16:31Z
<p>建立内容为“<div style="padding: 0 4%; line-height: 1.8; color: #1e293b; font-family: 'Helvetica Neue', Helvetica, 'PingFang SC', Arial, sans-serif; background-color: #ffffff…”的新页面</p>
<p><b>新页面</b></p><div><div style="padding: 0 4%; line-height: 1.8; color: #1e293b; font-family: 'Helvetica Neue', Helvetica, 'PingFang SC', Arial, sans-serif; background-color: #ffffff; max-width: 1200px; margin: auto;"><br />
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<strong>FBXW7</strong>(F-box and WD repeat domain containing 7),也称为 <strong>hCDC4</strong>,编码 SCF (SKP1-CUL1-F-box) E3 泛素连接酶复合物中的关键底物识别亚基。作为人体内极其重要的<strong>肿瘤抑制基因</strong>(Tumor Suppressor),FBXW7 就像细胞内的“垃圾分类处理工”,专门负责识别并结合磷酸化的致癌蛋白(如 <strong>c-Myc</strong>, <strong>Cyclin E</strong>, <strong>Notch</strong>, <strong>mTOR</strong>),给它们打上泛素标签并送往蛋白酶体进行降解。FBXW7 的失活突变会导致这些强效癌蛋白在细胞内异常积聚,从而驱动细胞无限增殖、基因组不稳定和化疗耐药。<br />
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<div style="font-size: 1.2em; font-weight: bold; letter-spacing: 1.2px;">FBXW7 (hCDC4) · 基因档案</div><br />
<div style="font-size: 0.7em; opacity: 0.85; margin-top: 4px; white-space: nowrap;">Gene & Protein Profile (点击展开)</div><br />
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[[文件:SCF_FBXW7_Complex.png|100px|SCF-FBXW7 泛素连接酶复合物]]<br />
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<div style="font-size: 0.8em; color: #64748b; margin-top: 12px; font-weight: 600;">E3 泛素连接酶亚基</div><br />
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<th style="text-align: left; padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #475569; background-color: #f8fafc; width: 40%;">基因符号</th><br />
<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #0f172a;"><strong>FBXW7</strong></td><br />
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<th style="text-align: left; padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #475569; background-color: #f8fafc;">常用别名</th><br />
<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #0f172a;">hCDC4, SEL-10, AGO</td><br />
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<th style="text-align: left; padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #475569; background-color: #f8fafc;">编码蛋白</th><br />
<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #0f172a;">F-box/WD repeat-containing protein 7</td><br />
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<th style="text-align: left; padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #475569; background-color: #f8fafc;">染色体位置</th><br />
<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #0f172a;">4q31.3</td><br />
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<th style="text-align: left; padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #475569; background-color: #f8fafc;">Entrez ID</th><br />
<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #1e40af;">55294</td><br />
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<th style="text-align: left; padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #475569; background-color: #f8fafc;">HGNC ID</th><br />
<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #1e40af;">13546</td><br />
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<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #1e40af;">Q969H0</td><br />
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<th style="text-align: left; padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #475569; background-color: #f8fafc;">分子量</th><br />
<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #0f172a;">~80 kDa</td><br />
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<th style="text-align: left; padding: 8px 12px; color: #475569; background-color: #f8fafc;">核心底物</th><br />
<td style="padding: 8px 12px; color: #0f172a;">Myc, Cyclin E, Notch</td><br />
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<h2 style="background: #f1f5f9; color: #0f172a; padding: 10px 18px; border-radius: 0 6px 6px 0; font-size: 1.25em; margin-top: 40px; border-left: 6px solid #0f172a; font-weight: bold;">分子机制:精准的底物捕获器</h2><br />
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FBXW7 蛋白通过其 C 端的 WD40 重复序列形成一个 β-螺旋桨结构,该结构是捕捉底物的关键部位。其工作流程高度依赖磷酸化信号:<br />
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<li style="margin-bottom: 12px;"><strong>磷酸化依赖性降解 (Phosphodegron Recognition):</strong> 靶蛋白(如 c-Myc 或 Cyclin E)首先被 GSK3β 或其他激酶磷酸化,形成特定的磷酸化降解基序(Phosphodegron, CPD)。FBXW7 专一性地识别并结合这个磷酸化标记。</li><br />
<li style="margin-bottom: 12px;"><strong>热点突变效应:</strong> 在肿瘤中,FBXW7 的突变高度集中在 WD40 结构域的关键精氨酸残基上(如 <strong>R465, R479, R505</strong>)。这些突变直接破坏了 FBXW7 与磷酸化底物的结合能力,导致“垃圾”无法被回收。</li><br />
<li style="margin-bottom: 12px;"><strong>广泛的抑癌网络:</strong> FBXW7 同时控制细胞周期(通过 Cyclin E)、细胞生长(通过 c-Myc/mTOR)和细胞分化(通过 Notch)。因此,单一的 FBXW7 失活就能同时引爆多条致癌通路。</li><br />
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<h2 style="background: #f1f5f9; color: #0f172a; padding: 10px 18px; border-radius: 0 6px 6px 0; font-size: 1.25em; margin-top: 40px; border-left: 6px solid #0f172a; font-weight: bold;">临床景观:广泛突变的抑癌基因</h2><br />
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FBXW7 是人类癌症中突变频率最高的 E3 连接酶基因之一,其突变谱覆盖多种实体瘤和血液肿瘤。<br />
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<th style="padding: 12px; border: 1px solid #cbd5e1; color: #0f172a; width: 25%;">癌种</th><br />
<th style="padding: 12px; border: 1px solid #cbd5e1; color: #475569;">突变频率</th><br />
<th style="padding: 12px; border: 1px solid #cbd5e1; color: #1e40af;">临床与病理特征</th><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">T细胞急性淋巴细胞白血病 (T-ALL)</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">~30%</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">极高频突变。主要后果是 <strong>Notch1</strong> 胞内段(NICD)无法降解,导致 Notch 通路持续激活。与化疗耐药和不良预后相关。</td><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">子宫内膜癌</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">~15%</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">多见于浆液性亚型。常导致 Cyclin E 积聚,驱动基因组不稳定。</td><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">结直肠癌 (CRC)</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">~10-15%</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">与较差的总生存期(OS)相关。FBXW7 突变细胞对某些靶向治疗(如抗 EGFR 单抗)可能不敏感,因 mTOR 等旁路被激活。</td><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">胆管癌</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">~5%</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">是肝内胆管癌常见的突变基因之一,常与 KRAS 或 IDH 突变共存。</td><br />
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<h2 style="background: #f1f5f9; color: #0f172a; padding: 10px 18px; border-radius: 0 6px 6px 0; font-size: 1.25em; margin-top: 40px; border-left: 6px solid #0f172a; font-weight: bold;">治疗策略:间接靶向与合成致死</h2><br />
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由于 FBXW7 的致癌机制是功能缺失(Loss of Function),直接恢复其活性极难成药。策略转向打击其因缺失而“逃逸”的下游底物。<br />
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<li style="margin-bottom: 12px;"><strong>mTOR 抑制剂:</strong> 如 <strong>[[Everolimus]]</strong>。<br />
<br><span style="font-size: 0.9em; color: #64748b;">*原理:FBXW7 缺失导致 mTOR 蛋白稳定性增加。研究表明,FBXW7 突变的肿瘤细胞对雷帕霉素类似物表现出更高的敏感性(合成致死效应)。</span><br />
</li><br />
<li style="margin-bottom: 12px;"><strong>Notch 抑制剂 (GSIs):</strong><br />
<br>在 T-ALL 中,γ-分泌酶抑制剂(Gamma-Secretase Inhibitors)可阻断 Notch 的激活,理论上对 FBXW7 突变导致的 Notch 积聚有效,但临床应用受限于胃肠道毒性。</li><br />
<li style="margin-bottom: 12px;"><strong>靶向 c-Myc 或 Cyclin E:</strong><br />
<br>虽然直接靶向 c-Myc 仍困难,但针对 Cyclin E 过表达导致的复制压力,使用 <strong>WEE1 抑制剂</strong>或 CDK2 抑制剂可能有效。</li><br />
<li style="margin-bottom: 12px;"><strong>克服耐药:</strong> 认识到 FBXW7 突变可能导致对紫杉醇或 5-FU 耐药(通过 MCL1 或 c-Myc 积聚),有助于指导二线化疗方案的选择。</li><br />
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<h2 style="background: #f1f5f9; color: #0f172a; padding: 10px 18px; border-radius: 0 6px 6px 0; font-size: 1.25em; margin-top: 40px; border-left: 6px solid #0f172a; font-weight: bold;">关键关联概念</h2><br />
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<li style="margin-bottom: 12px;"><strong>E3 泛素连接酶:</strong> 负责给蛋白打上“死亡标签”(泛素)的酶,FBXW7 是其核心识别组件。</li><br />
<li style="margin-bottom: 12px;"><strong>c-Myc:</strong> 著名的癌基因,FBXW7 是其主要的负调控因子。</li><br />
<li style="margin-bottom: 12px;"><strong>Notch1:</strong> 在 T-ALL 中与 FBXW7 形成互斥或协同的突变关系。</li><br />
<li style="margin-bottom: 12px;"><strong>磷酸化降解基序 (CPD):</strong> 底物被 FBXW7 识别的“密码”。</li><br />
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<span style="color: #0f172a; font-weight: bold; font-size: 1.05em; display: inline-block; margin-bottom: 15px;">学术参考文献与权威点评</span><br />
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[1] <strong>Welcker M, Clurman BE. (2008).</strong> <em>FBW7 ubiquitin ligase: a tumour suppressor at the crossroads of cell division, growth and differentiation.</em> <strong>Nature Reviews Cancer</strong>. <br><br />
<span style="color: #475569;">[学术点评]:该领域最经典的综述之一,系统阐述了 FBXW7 对 Myc、Cyclin E、Notch 等关键癌蛋白的调控网络。</span><br />
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[2] <strong>Mao JH, et al. (2004).</strong> <em>FBXW7/hCDC4 is a general tumor suppressor in human cancer.</em> <strong>Nature</strong>. <br><br />
<span style="color: #475569;">[学术点评]:通过大规模测序和功能实验,首次确立了 FBXW7 作为广谱肿瘤抑制基因的地位,特别是其对 Notch 和 Jun 的调节。</span><br />
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[3] <strong>Koepp DM, et al. (2001).</strong> <em>Phosphorylation-dependent ubiquitination of cyclin E by the SCFFbw7 ubiquitin ligase.</em> <strong>Science</strong>. <br><br />
<span style="color: #475569;">[学术点评]:机制发现。鉴定了 FBXW7 是负责降解 Cyclin E 的连接酶,解释了癌细胞中 Cyclin E 过表达和基因组不稳定的原因。</span><br />
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[4] <strong>Yada M, et al. (2004).</strong> <em>Phosphorylation-dependent degradation of c-Myc is mediated by the F-box protein Fbw7.</em> <strong>EMBO Journal</strong>. <br><br />
<span style="color: #475569;">[学术点评]:建立了 FBXW7 与“癌基因之王” c-Myc 之间的负调控关系,揭示了 c-Myc 蛋白稳定性的控制机制。</span><br />
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[5] <strong>Wertz IE, et al. (2011).</strong> <em>Sensitivity to antitubulin chemotherapeutics is regulated by MCL1 and FBW7.</em> <strong>Nature</strong>. <br><br />
<span style="color: #475569;">[学术点评]:临床相关性研究。发现 FBXW7 缺失会导致抗凋亡蛋白 MCL1 的积聚,从而引起癌细胞对紫杉醇等抗有丝分裂药物的耐药。</span><br />
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<div style="background-color: #0f172a; color: #ffffff; text-align: center; font-weight: bold; padding: 10px; letter-spacing: 1px;">FBXW7 · 知识图谱关联</div><br />
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[[泛素连接酶]] • [[c-Myc]] • [[T-ALL]] • [[Notch1]] • [[Cyclin E]] • [[mTOR]] • [[肿瘤抑制基因]] • [[耐药机制]]<br />
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