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RUNX1 - 版本历史
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<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>
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<strong>RUNX1</strong>(Runt-related Transcription Factor 1),旧称 <strong>AML1</strong> (Acute Myeloid Leukemia 1) 或 CBFA2,编码核心结合因子(CBF)的 α 亚基。作为造血系统的“主调节因子”(Master Regulator),RUNX1 对于造血干细胞(HSC)的发生及向淋巴/髓系细胞的分化至关重要。在临床血液肿瘤中,RUNX1 具有极端的“双面性”:其作为融合基因的一部分(如 <strong>t(8;21)</strong> 形成的 RUNX1-RUNX1T1)通常定义了<strong>预后良好</strong>的 Core Binding Factor AML;而其功能丧失性的<strong>体细胞突变</strong>则定义了一种<strong>预后不良</strong>的 AML 亚型(RUNX1-mutated AML)。此外,RUNX1 的生殖系突变会导致<strong>[[家族性血小板疾病伴髓系恶性肿瘤易感]] (FPD/MM)</strong>。<br />
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<div style="font-size: 1.2em; font-weight: bold; letter-spacing: 1.2px;">RUNX1 (AML1) · 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:RUNX1_CBFB_Structure.png|100px|RUNX1-CBFβ 复合物结合 DNA]]<br />
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<div style="font-size: 0.8em; color: #64748b; margin-top: 12px; font-weight: 600;">造血主转录因子</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>RUNX1</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;">AML1, CBFA2, PEBP2aB</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;">Runt-related transcription factor 1</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;">21q22.12</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;">861</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;">10471</td><br />
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<td style="padding: 8px 12px; border-bottom: 1px solid #f1f5f9; color: #1e40af;">Q01196</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;">~50-55 kDa</td><br />
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<th style="text-align: left; padding: 8px 12px; color: #475569; background-color: #f8fafc;">功能分类</th><br />
<td style="padding: 8px 12px; color: #0f172a;">转录因子 (CBF Complex)</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:Runt 结构域与转录调控</h2><br />
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RUNX1 是核心结合因子(Core Binding Factor, CBF)复合物的 DNA 结合亚基,其功能依赖于精细的蛋白-蛋白及蛋白-DNA 相互作用。<br />
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<li style="margin-bottom: 12px;"><strong>CBF 异源二聚体:</strong> RUNX1 通过其 N 端的 <strong>Runt 同源结构域 (RHD)</strong> 结合 DNA 上的共有序列(TGTGGT)。但它必须与非 DNA 结合伴侣 <strong>CBFβ</strong> 形成异源二聚体,以提高其 DNA 结合亲和力并防止被泛素化降解。</li><br />
<li style="margin-bottom: 12px;"><strong>转录开关:</strong> RUNX1 本身是一个较弱的转录激活子,它通过招募共激活因子(如 p300/CBP)或共抑制因子(如 TLE/Groucho, HDACs)来调节靶基因(如 <em>CSF1R, IL3, MPO</em>)的表达。这种“上下文依赖”的活性使其能够在不同的造血阶段开启或关闭基因。</li><br />
<li style="margin-bottom: 12px;"><strong>白血病机制:</strong> <br />
<br>1. <strong>融合蛋白(显性负效应):</strong> 如 RUNX1-RUNX1T1 (AML1-ETO),融合蛋白保留了 DNA 结合能力,但招募了强效的去乙酰化酶复合物(N-CoR/HDAC),强力阻遏髓系分化基因的转录。<br />
<br>2. <strong>突变失活:</strong> RUNX1 的点突变破坏了 Runt 结构域的 DNA 结合能力,导致造血干细胞分化受阻,并处于基因组不稳定的状态。</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:预后的分水岭</h2><br />
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在急性髓系白血病(AML)中,RUNX1 的变异形式直接决定了患者被分入“低危组”还是“高危组”。<br />
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<th style="padding: 12px; border: 1px solid #cbd5e1; color: #0f172a; width: 25%;">疾病亚型</th><br />
<th style="padding: 12px; border: 1px solid #cbd5e1; color: #475569;">变异形式</th><br />
<th style="padding: 12px; border: 1px solid #cbd5e1; color: #1e40af;">临床意义与预后</th><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">核心结合因子 AML (CBF-AML)</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;"><strong>RUNX1-RUNX1T1</strong><br>t(8;21)(q22;q22)</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">约占成人 AML 的 5-10%。属于 <strong>ELN 预后良好组</strong>。对大剂量阿糖胞苷(HiDAC)化疗高度敏感,治愈率较高(>60%),通常无需一线移植。</td><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">RUNX1 突变型 AML</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">体细胞点突变</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">WHO 分类中的独立实体。多见于老年人、MDS 转化或继发性 AML。属于 <strong>ELN 预后不良组</strong>,化疗耐药率高,复发快,建议进行异基因造血干细胞移植(allo-HSCT)。</td><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">ETV6-RUNX1 ALL</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">t(12;21) 融合</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">儿童 B-ALL 最常见的易位(~25%)。预后<strong>极好</strong>,治愈率 >90%。</td><br />
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<td style="padding: 10px; border: 1px solid #cbd5e1; font-weight: 600;">FPD/MM</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">生殖系突变 (Germline)</td><br />
<td style="padding: 10px; border: 1px solid #cbd5e1;">家族性血小板疾病。表现为轻中度血小板减少,但发生 AML 的终生风险高达 35-50%。需要遗传咨询和长期监测。</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:分层施治</h2><br />
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针对 RUNX1 相关肿瘤的治疗完全取决于其变异类型(融合 vs 突变)。<br />
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<li style="margin-bottom: 12px;"><strong>针对 t(8;21) (CBF-AML):</strong><br />
<br>标准方案为“3+7”诱导化疗,缓解后必须给予多个疗程的<strong>大剂量阿糖胞苷 (HiDAC)</strong> 巩固。Gemtuzumab Ozogamicin (CD33 单抗) 联合化疗可进一步改善该亚组的生存率。</li><br />
<li style="margin-bottom: 12px;"><strong>针对 RUNX1 突变型 AML:</strong><br />
<br>由于预后差,常规化疗后建议尽早进行<strong>异基因造血干细胞移植 (allo-HSCT)</strong>。目前尚无获批的直接靶向 RUNX1 的药物。</li><br />
<li style="margin-bottom: 12px;"><strong>新兴靶向探索:</strong><br />
<br>研究发现 RUNX1 突变细胞可能对 <strong>Menin 抑制剂</strong> 或蛋白质降解剂(Degraders)敏感。此外,由于 RUNX1 缺失导致核糖体生物合成异常,一些翻译抑制剂也在临床前研究中。</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>CBFβ:</strong> RUNX1 的异源二聚体伴侣,CBFB-MYH11 融合(inv(16))与 t(8;21) 同属 CBF-AML。</li><br />
<li style="margin-bottom: 12px;"><strong>t(8;21):</strong> 产生 AML1-ETO 融合蛋白的染色体易位,AML 预后良好的标志。</li><br />
<li style="margin-bottom: 12px;"><strong>FPD/MM:</strong> RUNX1 生殖系突变引起的遗传性肿瘤综合征。</li><br />
<li style="margin-bottom: 12px;"><strong>主调节因子:</strong> RUNX1 在造血谱系定型中的核心地位。</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>Miyoshi H, et al. (1991).</strong> <em>t(8;21) breakpoints on chromosome 21 in acute myeloid leukemia are clustered within a limited region of a single gene, AML1.</em> <strong>PNAS</strong>. <br><br />
<span style="color: #475569;">[学术点评]:发现性文献。首次克隆了 t(8;21) 易位的断点基因 AML1 (RUNX1),确立了其在白血病遗传学中的基石地位。</span><br />
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[2] <strong>Song WJ, et al. (1999).</strong> <em>Haploinsufficiency of CBFA2 causes familial thrombocytopenia with propensity to develop acute myelogenous leukaemia.</em> <strong>Nature Genetics</strong>. <br><br />
<span style="color: #475569;">[学术点评]:临床遗传学里程碑。首次将 RUNX1 (CBFA2) 的生殖系突变与家族性血小板疾病 (FPD) 联系起来,定义了该遗传综合征。</span><br />
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[3] <strong>Schnittger S, et al. (2011).</strong> <em>RUNX1 mutations are frequent in de novo acute myeloid leukemia with unmutated NPM1 and associated with poor prognostic cytogenetics.</em> <strong>Blood</strong>. <br><br />
<span style="color: #475569;">[学术点评]:确立了 RUNX1 点突变在 AML 中的独立不良预后价值,推动了后来 WHO 将“RUNX1 突变型 AML”列为独立实体。</span><br />
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[4] <strong>Döhner H, et al. (2017/2022).</strong> <em>Diagnosis and management of AML in adults: 2017/2022 ELN recommendations.</em> <strong>Blood</strong>. <br><br />
<span style="color: #475569;">[学术点评]:权威指南。明确将 t(8;21) 列为预后良好组,而将 RUNX1 突变列为预后不良组,指导了全球的临床分层治疗。</span><br />
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[5] <strong>Ito Y, Bae SC, Chuang LS. (2015).</strong> <em>The RUNX family: developmental regulators in cancer.</em> <strong>Nature Reviews Cancer</strong>. <br><br />
<span style="color: #475569;">[学术点评]:综述文献。系统阐述了 RUNX 家族在发育和肿瘤中的双重作用(抑癌 vs 促癌),提供了深入的机制见解。</span><br />
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[[急性髓系白血病]] • [[t(8;21)]] • [[CBF-AML]] • [[阿糖胞苷]] • [[FPD/MM]] • [[CBFB]] • [[造血干细胞]] • [[ETV6]]<br />
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