Move from a broad disease map to a decision-ready trial dossier. This focused report examines ChiCTR2600128203—A randomized, phase 3, open-label study to evaluate sigvotatug vedotin compared with docetaxel in adult participants with previously treated non-small cell lung cancer (Be6A Lung-01)—using PatSnap Clinical Trials, Drug & Asset, and Company & Deal Intelligence MCP evidence. Explore PatSnap MCP Servers to reproduce the workflow inside an AI research process.
MCP evidence snapshot: 16 July 2026; publication date: 17 July 2026. Trial records can change after the snapshot and should be rechecked before operational decisions.
Non-Small Cell Lung Cancer is increasingly segmented by mechanism, biomarker, line of therapy, geography and endpoint architecture. ChiCTR2600128203 is notable because it tests Sigvotatug vedotin in a Phase 3 design while Overall Survival(OS) serves as the main decision variable. The value of this program will depend on whether the protocol converts biological rationale into a clinically interpretable and operationally credible readout.
PatSnap Clinical Trials MCP makes protocol fields machine-readable, while the companion asset and organization servers add mechanism, development-status and sponsor context.
| Field | Indexed detail |
|---|---|
| Registration | ChiCTR2600128203 |
| Official title | A randomized, phase 3, open-label study to evaluate sigvotatug vedotin compared with docetaxel in adult participants with previously treated non-small cell lung cancer (Be6A Lung-01) |
| Phase / status | Phase 3 / Recruiting |
| Intervention | Sigvotatug vedotin, Docetaxel |
| Sponsor | Not reported |
| Geography | China |
| Enrollment | 50 |
| Primary endpoint | Overall Survival(OS) |
| Endpoint time frame | Participants who discontinue study intervention for reasons other than disease progression will be a |
| Primary completion / readout proxy | 2029-12-30 |
The design should be read as an evidence architecture, not just a phase label. Allocation is not reported, masking is Open Label, and the intervention model is Parallel Assignment. Enrollment of 50 participants across China shapes statistical precision, execution risk and external validity. A strong readout will need to be interpreted against baseline risk, prior treatment, assessment schedule, missing-data handling and the clinical relevance of the observed effect.
These indexed results are contextual benchmarks rather than direct head-to-head evidence. Cross-trial comparisons can be distorted by population, treatment line, endpoint definition, follow-up and analysis set. Their value is to clarify what magnitude and type of evidence the market already recognizes.
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Drug & Asset context: Sigvotatug vedotin (Phase 3; ITGB6 x Tubulin); Docetaxel (Approved; Tubulin)
Company & Deal Intelligence context: Sponsor information not reported.
The sponsor profile matters because scientific rationale alone does not determine development value. Manufacturing readiness, portfolio fit, geographic reach, partnering capacity and the ability to fund confirmatory development can decide whether a positive signal becomes a competitive asset.
Monitor recruitment status, enrollment changes, protocol amendments, endpoint hierarchy, primary-completion timing, first result indexing, asset ownership and sponsor partnerships. The most important inflection point is not always the headline data release; a change in endpoint, population or ownership can alter probability of success months earlier.
ChiCTR2600128203 is a focused lens on Non-Small Cell Lung Cancer development. Its value will be determined by whether Sigvotatug vedotin can convert the current design into evidence that is clinically meaningful, operationally credible and differentiated from existing benchmark readouts.
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