| WB | 咨询技术 | Human,Mouse,Rat |
| IF | 咨询技术 | Human,Mouse,Rat |
| IHC | 1/50-1/100 | Human,Mouse,Rat |
| ICC | 技术咨询 | Human,Mouse,Rat |
| FCM | 咨询技术 | Human,Mouse,Rat |
| Elisa | 咨询技术 | Human,Mouse,Rat |
| Aliases | TOB; Transducer of erbB-2 1; |
| Entrez GeneID | 10140; |
| WB Predicted band size | 40kDa |
| Host/Isotype | Rabbit IgG |
| Antibody Type | Primary antibody |
| Storage | Store at 4°C short term. Aliquot and store at -20°C long term. Avoid freeze/thaw cycles. |
| Species Reactivity | Human,Mouse,Rat |
| Immunogen | Peptide sequence around phosphorylation site of Serine 164(A-V-S(p)-P-T) derived from Human TOB1. |
| Formulation | Purified antibody in PBS with 0.05% sodium azide. |
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以下是关于TOB1 (Phospho-Ser164)抗体的3篇参考文献示例(内容基于研究方向模拟,仅供参考):
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1. **文献名称**:*Phosphorylation of TOB1 at Ser164 regulates its interaction with 14-3-3 proteins and cell cycle progression*
**作者**:Yoshida Y, et al.
**摘要**:本研究揭示了TOB1在丝氨酸164位点的磷酸化对其与14-3-3蛋白结合的关键作用。通过使用TOB1 (Phospho-Ser164)特异性抗体,作者证明DNA损伤诱导的磷酸化促进TOB1从细胞核转位至胞质,从而调控G1/S期阻滞。
2. **文献名称**:*ERK-mediated phosphorylation of TOB1 at Ser164 modulates its tumor suppressor function in breast cancer*
**作者**:Chen L, et al.
**摘要**:文章利用TOB1 (Phospho-Ser164)抗体验证了ERK激酶在乳腺癌细胞中对该位点的直接磷酸化。磷酸化抑制了TOB1与HER2/ERBB2的相互作用,促进癌细胞增殖,为靶向治疗提供了潜在标志物。
3. **文献名称**:*A kinase-dead screen identifies TOB1 phosphorylation as a regulator of T cell anergy*
**作者**:Sung HY, et al.
**摘要**:通过磷酸化抗体检测,研究发现T细胞耐受诱导过程中TOB1 Ser164位点的磷酸化显著上调。该修饰通过阻断IL-2转录抑制T细胞活化,揭示了TOB1在免疫调控中的新机制。
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**说明**:以上文献为示例,实际引用需根据具体实验需求检索PubMed等数据库,并核对抗体货号及验证数据(如WB、IP结果)。若需真实文献,建议使用关键词“TOB1 Phospho-Ser164 antibody”或“TOB1 S164 phosphorylation”进一步检索。
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