MedPath

A Prospective Study Investigating the Relationship Between Minimal Residual Disease Detection, Monitoring Frequency, and Prognosis in Non-small Cell Lung Cancer Patients Eligible for Curative Treatment.

Not yet recruiting
Conditions
NSCLC, Stage I, II, III
Registration Number
NCT06854939
Lead Sponsor
National Cancer Center, Japan
Brief Summary

Adding immune checkpoint inhibitors or molecularly targeted drugs as adjuvant therapy to curative treatments-such as surgery or chemoradiotherapy-for stage I-III non-small cell lung cancer (NSCLC) has been established as a standard of care and has improved treatment outcomes. However, there is currently no adequate method to determine which patients should receive these adjuvant therapies. Identifying those with a good prognosis without adjuvant therapy could reduce the risk of adverse events, lessen the burden of clinic visits, and reduce healthcare costs.

Among various approaches, ctDNA-based MRD (minimal residual disease) analysis is highly anticipated and has already been introduced into clinical practice for hematologic malignancies. However, solid tumors' development as a companion diagnostic has been limited, and regulatory approval is mainly being considered based on performance evaluation data. In this study, we will conduct a performance evaluation of MRD analysis using Signatera™ in patients with stage I-III NSCLC while also collecting other prognostic factors based on clinicopathological information and survival data.

Detailed Description

Not available

Recruitment & Eligibility

Status
NOT_YET_RECRUITING
Sex
All
Target Recruitment
350
Inclusion Criteria

  1. A histopathologically confirmed diagnosis of non-small cell lung cancer (NSCLC)

    The diagnosis (by cytology or biopsy) must be one of the following: "adenocarcinoma," "squamous cell carcinoma," "non-small cell carcinoma consistent with adenocarcinoma," "non-small cell carcinoma consistent with squamous cell carcinoma," or "non-small cell carcinoma not otherwise specified (NOS)." If the histological subtype differs between cytology and biopsy specimens, the subtype determined by the biopsy specimen shall be used.

    At the time of enrollment, diagnoses of "squamous cell carcinoma" or "non-small cell carcinoma consistent with squamous cell carcinoma" are classified as squamous cell carcinoma, whereas "adenocarcinoma," "non-small cell carcinoma consistent with adenocarcinoma," and "non-small cell carcinoma NOS" are classified as non-squamous cell carcinoma.

  2. Meets one of the following criteria (1-3):

  3. Stage IB-III (preoperative clinical stage) deemed resectable, with no planned neoadjuvant therapy.

  4. Stage III disease deemed amenable to curative-intent chemoradiotherapy. 3. Stage II-III (preoperative clinical stage) deemed resectable, with planned neoadjuvant therapy.

  1. Age ≥ 18 years at the time of enrollment. 4) The attending physician has determined that tissue and blood samples can be provided.

  2. Written informed consent has been obtained from the patient.

Exclusion Criteria
  • Presence of active multiple primary malignancies (defined as synchronous multiple cancers/tumors or metachronous multiple cancers/tumors with a disease-free interval of 3 years or less). However, even if the disease-free interval is less than 3 years, a history of clinical stage I prostate cancer or a completely resected cancer with any of the pathological stages specified below is not considered "active multiple primary malignancies.

Study & Design

Study Type
OBSERVATIONAL
Study Design
Not specified
Primary Outcome Measures
NameTimeMethod
2-year PFSAnalyses are planned to be performed 4.5 years after the start of the study.
Secondary Outcome Measures
NameTimeMethod

Related Research Topics

Explore scientific publications, clinical data analysis, treatment approaches, and expert-compiled information related to the mechanisms and outcomes of this trial. Click any topic for comprehensive research insights.

How does ctDNA-based MRD detection using Signatera™ enhance prognosis prediction in stage I-III NSCLC compared to traditional imaging methods?
What molecular biomarkers correlate with MRD clearance kinetics in NSCLC patients undergoing adjuvant immunotherapy or targeted therapy?
Can personalized MRD assays like Signatera™ identify high-risk NSCLC patients who benefit most from adjuvant checkpoint inhibitors?
What adverse events are linked to adjuvant immunotherapy/targeted therapy in NSCLC, and how can MRD monitoring reduce unnecessary exposure?
How does Signatera™ MRD assay performance in NSCLC compare to other liquid biopsy platforms like Guardant Health or Qiagen?

Trial Locations

Locations (1)

National Cancer Center Hospital

🇯🇵

Chuo-ku, Tokyo, Japan

National Cancer Center Hospital
🇯🇵Chuo-ku, Tokyo, Japan

Related Trials

Personalizing Immune Checkpoint Inhibitor Therapy

Withdrawn
Holy Cross Hospital, Maryland
Posted 1/24/2018
Updated 9/24/2020

Tislelizumab and Radiotherapy for Recurrent Cervical Cancer

Unknown StatusPhase 2
Lei Li
Posted 4/4/2022
Updated 4/11/2022

Neoadjuvant Combination Therapy With Ipilimumab and HighDose IFN-α2b for Melanoma

CompletedPhase 1
Diwakar Davar
Posted 5/31/2012
Updated 8/28/2018

MRD-positive Colorectal Cancer Patients Combined With Personalized Immune Regulation Diagnosis

Not Yet RecruitingEarly Phase 1
Second Affiliated Hospital of Wenzhou Medical University
Posted 5/30/2024

Salvage Surgery Following Downstaging of Advanced Non-small Cell Lung Cancer by Targeted Therapy (SDANT)

Unknown StatusPhase 2
Wuhan Union Hospital, China
Posted 10/20/2021
Updated 5/20/2022
© Copyright 2025. All Rights Reserved by MedPath
HomeTerms & ConditionsPrivacy Policy