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临床试验 NCT07495033 针对CTD-ILD目前尚未招募。请查看临床试验雷达卡片视图和 AI 发现工具了解所有详情,或在此提出任何问题。
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Phase III Clinical Trial of Telitacicept Injection in the Treatment of Patients With Connective Tissue Disease-related Interstitial Lung Disease III期 260

尚未招募
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临床试验NCT07495033旨在研究治疗,主要针对CTD-ILD。这是一项III期 干预性研究试验,当前状态为尚未招募试验尚未开始,计划于2026年3月1日开始,预计招募260名患者。该研究由RemeGen Co., Ltd.主导,计划于2030年5月31日完成。试验数据来源于ClinicalTrials.gov,最后更新时间为2026年3月27日
简要概括
Interstitial lung disease (ILD) is a common pulmonary manifestation in chronic tissue diseases (CTD), significantly affecting patient's prognosis.

The main purpose of this study is to evaluate the efficacy of telitacicept compared with placebo in slowing down the decline in lung volume in patients with interstitial lung disease associated with connective tissue disease (CTD-ILD) on the basis of standard treatment.

官方标题

Phase III Clinical Trial of Telitacicept Injection in the Treatment of Patients With Connective Tissue Disease-related Interstitial Lung Disease

疾病
CTD-ILD
其他研究标识符
  • RC18-C309
NCT编号
NCT07495033
实际开始日期
2026-03-01
最近更新发布
2026-03-27
预计完成日期
2030-05-31
计划入组人数
260
研究类型
干预性研究
试验分期 (阶段)
III期
试验状态
尚未招募
主要目的
治疗方法
分配方式
随机
干预模型
平行
盲法
双盲
试验组/干预措施
参与者组/试验组干预措施/治疗方法
实验性Telitacicept
Participants will receive elitacicept in addition to standard therapy.
Telitacicept
Subjects will receive 160 mg. The study drug is administered once weekly (QW).
安慰剂对照Placebo
Participants will receive placebo in addition to standard therapy.
安慰剂
The placebo contains no active ingredients. To maintain the blind, the placebo matches the active drug in all physical aspects. The placebo is administered once weekly (QW).
主要终点
结果指标度量标准描述时间框架
Change from Baseline in FVC(mL) at Week 52
Baseline and Week 52
次要终点
结果指标度量标准描述时间框架
Change from Baseline in FVC%Pred at Week 52
Baseline and Week 52
Change from Baseline in DLCO%Pred at Week 52
Baseline and Week 52
Time to ILD Progression or Death
The time from Baseline to Week 52
Change from Baseline in Quantitative Interstitial Lung Disease in the Whole Lung (QILD-WL) At Week 52
Baseline and Week 52
Change from Baseline in Quantitative Measures of Lung Fibrosis (QLF) in the Whole Lung At Week 52
Baseline and Week 52
the proportion of subjects with a QILD-WL score reduction ≥2% at week 52
Baseline and Week 52
The proportion of subjects who showed a ≥5% decrease in FVC (mL) from baseline at week 52;
Baseline and Week 52
The proportion of subjects who showed a ≥10% decrease in FVC (mL) from baseline at week 52;
Baseline and Week 52
Change from Baseline in the short form health survey(SF-36) at Week 52
Baseline and Week 52
Change from Baseline in Patient global impression of severity(PGI-S) at Week 52
Baseline and Week 52
Changes from baseline in immunological markers(IgG、IgA、IgM、CD19+ B)at Week 52
Baseline and Week 52
Incidence and severity of adverse events
From signing of informed consent until 4 weeks after the last dose.
参与助手
资格标准

适龄参与研究
成人, 老年人
最低年龄要求
18 Years
适龄性别
全部
  1. Voluntary informed consent provided;
  2. Male or female aged ≥ 18 years old;
  3. Documented diagnosis of rheumatoid arthritis (RA), systemic lupus erythematosus (SLE), idiopathic inflammatory myopathy (IIM), Sjogren's syndrome (SjD) , Systemic sclerosis(SSc),or mixed connective tissue disease (MCTD) in accordance with internationally recognized classification criteria;
  4. Diagnosis of ILD on High Resolution Computed Tomography (HRCT) with disease extent of greater than or equal to (≥) 10% of the whole lung (WL-ILD);
  5. During screening, FVC%Pred ≥ 45%;
  6. During screening, DLCO%Pred(corrected for hemoglobin) ≥ 30%;
  7. Stable standard treatment was received before randomization to control ILD and/or connective tissue disease;

  1. Diagnosis of Interstitial lung disease other than CTD-ILD;

  2. ILD progresses rapidly within 12 weeks before screening or during screening;

  3. During screening, HRCT showed severe emphysema (the degree of emphysema exceeded that of ILD);

  4. Obstructive pulmonary disease (pre-bronchodilator Forced Expiratory Volume (FEV1) /FVC <0.7);

  5. Pulmonary arterial hypertension requiring therapy, as determined by the investigator;

  6. Having diffuse alveolar hemorrhage (DAH) or other pulmonary conditions that may have confounding effects, as well as related signs or symptoms;

  7. Unable to complete the pulmonary function test, or requiring supplementary oxygen supply;

  8. Clinically significant laboratory abnormalities;

  9. QTc interval prolongation on ECG;

  10. Allergy to human or mouse-derived biological products, or history of other drug allergies, and the investigator deems that the patient is not eligible to participate.

  11. Previous treatments received:

    • Previous or planned organ transplantation or bone marrow transplantation;
    • Plasma exchange or extracorporeal light separation exchange was performed within 6 months before randomization, or a plasma filtration device was used;
    • Any targeted BLyS or APRIL drug treatment was received within 12 weeks before randomization;
    • Biologic therapy was received within 12 weeks or within 5 half-lives of the corresponding drug (whichever is longer) before randomization;
    • B-cell depletion drugs were used within 6 months before randomization;
    • Non-biological systemic immunosuppressive drugs other than standard treatment were used within 4 weeks before randomization;
    • Anti-fibrotic drugs were used within 4 weeks before randomization;
    • Cyclophosphamide treatment was received within 6 months before randomization;
    • Cytotoxic drugs were used within 6 months before randomization;
    • Intravenous or intramuscular glucocorticoids were used within 4 weeks before randomization;

  12. Major surgery within 12 weeks prior to screening or planned during the duration of the study;

  13. Received or plan to receive any live vaccine within 28 days prior to randomization;

  14. Participation in any clinical trial 28 days prior to randomization or within 5 times the half-life of an investigational drug (whichever is longer);

  15. has active hepatitis or a history of severe liver disease;

  16. Acute or chronic infection requiring treatment;

  17. suffered from symptomatic herpes zoster within 12 weeks prior to screening;

  18. Active tuberculosis;

  19. HIV infection;

  20. History of malignant tumors;

  21. Significant cardiovascular disease, liver, kidney, respiratory, endocrine or hematologic disease, or other medical conditions that, in the opinion of the investigator, would preclude the subject's participation in the study or require hospitalization during the trial;

  22. History of drug or alcohol abuse or dependence;

  23. Pregnant or lactating women, and those intending to become pregnant during the trial;

  24. Patients considered unsuitable by the investigator to participate in the trial ;

RemeGen Co., Ltd. logoRemeGen Co., Ltd.
研究中心联系人
联系人: Mengtao Li, +86-10-69158354, [email protected]
联系人: Qian Wang, +86-10-69158354, [email protected]
1 位于 1 个国家/地区的研究中心

Beijing Municipality

Peking Union Medical College Hospital, Beijing, Beijing Municipality, 100000, China
Mengtao Li, 联系人, 86-10-69154186, [email protected]