Prospective registration

An Study to Evaluate the?Long-term Safety?and Tolerability of QX005N in Adult Patients with Moderate-to-Severe AD

An Open-label, Multicenter, Extension Study to Evaluate the?Long-term Safety?and Tolerability and efficacy of QX005N in Adult Patients with Moderate-to-Severe AD

Fang Min 

Jin Hongzhong 

907 Yaocheng Avenue, Taizhou, Jiangsu Province

No.1 Shuaifuyuan Wangfujing Dongcheng District, Beijing

Qyuns Therapeutics Co., Ltd.

Peking Union Medical College Hospital

Yes

Ethics Committee of Chinese Academy of Medical Sciences Peking Union Medical College Hospital

Tian Jiali

No.1 Shuaifuyuan Wangfujing Dongcheng District, Beijing

Peking Union Medical College Hospital

No.1 Shuaifuyuan Wangfujing Dongcheng District, Beijing

Qyuns Therapeutics Co., Ltd.

Moderate-to-Severe AD

Interventional study

2

Single arm 

Primary objective To evaluate the long-term safety and tolerability of QX005N after repeated SC injections in adult patients with moderate-to-severe AD. Secondary objectives To evaluate the long-term efficacy of QX005N after repeated SC injections in adult patients with moderate-to-severe AD.

1. Participation in a prior clinical trial of QX005N for AD (parent study: QX005NA-02 (PART B)) and met one of the following: a.Received study treatment and adequately completed the last visit assessments of the parent study as defined. b.Treatment discontinuation due to a poor compliance event or a AE that was deemed not related to QX005N, and complete the early withdrawal visit, according to the judgement of the investigator and the sponsor, the factor that led to the patient's early termination of treatment has disappeared/no longer affect the subject's participation in this study. 2. No birth plan and willing to use adequate birth control from the start of this study to 6 months after the last dose. 3. With ability to understand contents of informed consent form (ICF), and willing to sign and comply with terms in ICF. 4. Willing and able to comply with the planned clinic visits.

1. Participation in a prior clinical trial of QX005N for AD (parent study: QX005NA-02 (PART B)) and met one of the following: a.Patients developed a SAE that was deemed related to QX005N, and in the opinion of the investigator, the factors that led to the patient's early termination of treatment may present an unreasonable risk for the patient. b.Patients developed a AE that was deemed related to QX005N, and in the opinion of the investigator, the factors that led to the patient's early termination of treatment may present an unreasonable risk for the patient. c.Patients developed other conditions that lead to early termination of treatment, and in the opinion of the investigator, the factors that led to the patient's early termination of treatment may present an unreasonable risk for the patient. 2. Allergic to ingredients or excipients of the study drugs. 3. Pregnant or breast-feeding women, or women who plan to pregnant or breast-feeding during the whole study. 4.Treatment with drugs that target IL-4Rα, IL-4 or IL-13(exclude QX005N) before the screening visit. 5.With history of or presence of diseases at the screening visit as below: a.Systematic chronic or acute infection requiring with treatment with antibodies, anti-virals, anti-parasitics, anti-protozoals, or anti-fungals within 4 weeks before the screening visit, or herpes simplex infection within 2 weeks before the screening visit, or superficial skin infection within 1 weeks before the screening visit. (If have an infection, the patient can be re-screened after infection has subsided for only once). b.History of or suspected immunosuppressive disorders, including invasive occasional infectious diseases (eg. histoplasmosis, listeriosis, coccidiodomycosis, pneumocystosis, and aspergillosis), even if the infection has subsided, or there are unusually frequent, recurrent or long-term infections,the patient should be ruled out. c. Any other active inflammatory skin diseases that,in the opinion od the investigator, might interfere with the evaluation in this study at the screening visit. d. Any other medical or psychological history that, in the opinion od the investigator, may present an unreasonable risk to the study patientas a result of his/her participation in this clinical trial may make patient’s participation unreliable, or may interfere with study assessments, such as circulatory system abnormalities, endocrine system abnormalities, nervous system diseases, hematological system diseases, immune system diseases, mental diseases, etc. 6. Infectious disease meet the following criteria at the screening visit: a.History of tuberculosis, or active or latent TB infection at the time of screening (according to T-spot.TB or QuantiFERON-TB Gold test results). b.Positive hepatitis B surface antigen (or negative HBsAg plus positive HBcAb plus positive HBV-DNA). c.Positive hepatitis C antibody plus positive HCV-RNA. d.Positive treponema pallidum antibody plus positive RPR test. e.History of HIV infection, or positive HIV antibody. 7. Prior/concomitant therapy: a.Treatment with medium-to-superpotent TCS, or TCI uses on areas other than face, neck, genitalwithin 1 weeks before the baseline visit. b.Treatment with mPDE-4 inhibitor, such as Crisaborole, Roflumilast, Apremilast, etc., or JAK inhibitor, such as Ruxolitinib, Baricitinib, Tofacitinib, Upadacitinib, Abrocitinib,etc. c.Treatment with systematic traditional Chinese medicine therapies within 2 weeks before the baseline visit, or with topical traditional Chinese medicine therapies within 1 weeks before the baseline visit (as to drugs contain the Common Threewingnut Root, the washout times should be 4 weeks and 2 weeks respectively). d.Treatment with systematic corticosteroids, or systematic immunosuppressive/immunomodulating drugs (eg. cyclosporine, mycophenolate-mofetil, IFN-γ, azathioprine, methotrexate), or phototherapy (eg. NB-UVB, BB-UVB, UVA1, PUVA) within 4 weeks before the baseline visit. e.Previous treatment with biologic medicines within the following timeframe: - Etanercept or its biosimilars: within 4 weeks before the baseline visit. - TNF-αinhibitor or its biosimilars: within 3 months or 5 half-lives (whichever is longer). - Any cell-depleting agents(eg. Rituximab): within 6 months before the baseline visit. - Any other biologic medicines(vaccines excepted): within 5 half-lives before the baseline visit. f.Treatment with a live vaccine or an attenuated vaccine within 3 months before the baseline visit. g.Treatment with allergen-specific immunotherapy (SIT) within 6 months before the baseline visit. 8. Laboratory testing results meet one of the criteria below at the time of screening and baseline visit, or any other abnormal laboratory testing results that, in the investigator’s judgement, will bring the patient unreasonable risks. a.Aspartate aminotransferase (AST)/alanine aminotransferase (ALT)>2×the upper limit of normal (ULN) . b.Serum creatinine>1.2ULN. 9. Treatment with surgical procedure within 8weeks before the screening visit,or with surgical procedure plans which may interfere with study assessments during the study. 10. Any condition, in the opinion of the investigator, causes patients inappropriate to participate in the study.

Not apllicable in the single-arm study.

N/A

CRF and EDC