| Code | CSB-RA792129A0HU |
| Size | US$210 |
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| Application | Recommended Dilution |
|---|---|
| WB | 1:500-1:5000 |
| IHC | 1:50-1:200 |
| FC | 1:20-1:200 |
| IP | 1:200-1:1000 |
DNA topoisomerase 1 (TOP1) plays an essential role in relieving torsional stress during DNA replication and transcription by creating transient single-strand breaks in the DNA helix. This enzyme has become a focal point in cancer research, both as a biomarker and as a therapeutic target, since TOP1 inhibitors like camptothecin derivatives are widely used chemotherapeutic agents. Understanding TOP1 expression and localization provides valuable insights into cellular proliferation, DNA damage responses, and drug resistance mechanisms.
This recombinant monoclonal antibody, generated from clone 6D8 in rabbit host, offers the reproducibility and consistency that demanding research applications require. Because the antibody sequence is defined and produced recombinantly, you can expect uniform performance across experiments and over time, eliminating the lot-to-lot variability that can complicate longitudinal studies or multi-site collaborations.
Validation data demonstrates robust performance across multiple experimental platforms. In western blot applications, the antibody detects TOP1 at the expected 91 kDa molecular weight across a diverse panel of human cell lines including HeLa, MCF-7, K562, HL60, and PC-3, confirming reliable detection in various cellular contexts. Immunohistochemistry staining has been validated in paraffin-embedded human small intestine and colon cancer tissue sections using citrate buffer antigen retrieval, showing clear nuclear localization patterns. Flow cytometry analysis in HepG2 cells demonstrates distinct positive population shifts, while immunoprecipitation successfully enriches TOP1 from K562 lysates.
This versatility across western blot, immunohistochemistry, flow cytometry, and immunoprecipitation makes this antibody particularly valuable for researchers investigating epigenetic regulation, nuclear signaling pathways, and cancer biology where comprehensive characterization of TOP1 expression and function is essential.
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