Retinopathy of Prematurity Clinical Trial
Official title:
Real World Study of the Effectiveness and Safety of Conbercept Ophthalmic Injection in the Treatment of Retinopathy of Prematurity - Multicenter, Retrospective and Observational Study Based on Real World Data
Verified date | September 2022 |
Source | Chengdu Kanghong Biotech Co., Ltd. |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Observational |
This study is a retrospective, multi-center real world study. The real world data comes from the electronic medical record system and disease database of the research centers .The patient's demographic information, disease information, clinical treatment status, efficacy evaluation and adverse events and so on will be collected and evaluated by applicability of the data, generated an analysis data set. Use the causal inference method of statistical analysis to observe the effectiveness and safety of intravitreal injection of Conbercept, and explore the effectiveness and safety of different doses in the treatment of retinopathy of prematurity.
Status | Enrolling by invitation |
Enrollment | 1000 |
Est. completion date | October 2022 |
Est. primary completion date | October 2022 |
Accepts healthy volunteers | No |
Gender | All |
Age group | N/A and older |
Eligibility | Inclusion criteria: 1. Patient who are diagnosed as retinopathy of prematurity using clinical fundus screening; 2. Patients at the initial stage of treatment whose one eye at least has the following condition: Stage 1+, Stage 2+, Stage 3, Stage 3+ in Zone 1; or Stage 2+, Stage 3+ in Zone 2; or those with AP-ROP according to the international ROP classification,; 3. Patient for whom the first treatment is laser therapy, intravitreal injection of Conbercept or ranibizumab; Exclusion criteria: 1. Patients with neurological diseases that seriously affect visual function; 2. Patient or his mother (during pregnancy) has received intravitreal or systemic anti-VEGF drug therapy for other diseases; Elimination criteria: 1. Patients with insufficient data on treatment or medication; 2. Patients who are followed up for less than 3 months after treatment. |
Country | Name | City | State |
---|---|---|---|
China | Peking University People's Hospital | Beijing | Beijing |
China | West China Hospital of Sichuan University | Chengdu | Sichuan |
Lead Sponsor | Collaborator |
---|---|
Chengdu Kanghong Biotech Co., Ltd. | Guangzhou Keli Medical Research Co., Ltd. |
China,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | Exploratory Endpoints | To explore and evaluate the changes in the following longterm observational indicators, which are for descriptive analysis only.
1?Proportion of target eyes with complete retinal vascularization (the complete retinal vascularization is defined as retinal blood vessels extending to the serrata on the nasal side, and 1 optic disc diameter from the serrata on the temporal side); |
January 1, 2005 to December 31, 2021 | |
Other | Exploratory Endpoints | 2. Proportion of eyes with refractive abnormalities; | January 1, 2005 to December 31, 2021 | |
Other | Exploratory Endpoints | 3?Proportion of eyes with abnormal ocular visual function (the ocular visual function indicators include peripheral visual field, etc.); | January 1, 2005 to December 31, 2021 | |
Other | Exploratory Endpoints | 4?Proportion of target eyes with abnormal biological feature (the biological feature include axial length, anterior chamber depth, lens thickness, etc.). | January 1, 2005 to December 31, 2021 | |
Primary | Main effectiveness indicators | Proportion of eyes with no active retinopathy of prematurity and no structural adverse outcome (within 24 weeks after the first treatment; active retinopathy of prematurity is defined as additional lesions, vascular tortuosity, crest and other lesions having no alleviation but trend of progress after clinical treatment and new blood vessels continuing to exist or new born; poor structural outcomes are defined as adverse results such as retinal detachment, retinal traction or macular abnormalities after clinical treatment) | 24 weeks | |
Primary | Main safety indicators | The proportion of affected eyes with ocular AEs (within 24 weeks after the first treatment) | 24weeks | |
Primary | Primary endpoint | To evaluate the proportion of eyes with inactive retinopathy of prematurity and without structural adverse outcomes at 24 weeks after the first treatment (inactive retinopathy of prematurity is defined as the reduction in additional lesions, vascular tortuosity, ridges and other lesions after clinical treatment, showing no trend of progression, no persistent or newly developed neovascularization; no structural adverse outcome is defined as the absence of adverse outcomes such as retinal detachment, retinal traction, or macular abnormalities after clinical treatment) | 24 weeks | |
Secondary | Secondary endpoints | To evaluate the response rate of the first treatment at 1 week and 24 weeks after the first treatment (the response rate is defined as the proportion of patients after the first treatment who do not need the second treatment, with disappearance of the additional lesions or the reduction of the vascular tortuosity, the reduction or regression of the ridges, and with initiation of vascularization in the neighboring avas-cular area (or retinal vascularization to zone III); | at 1 week and 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of eyes with recurrence and the time to recurrence at 24 weeks after the first treatment (recurrence is defined as the recurrence of ridgelike changes or fibrovascular proliferation in the original lesion, complicated by the recurrence of additional lesions in the posterior pole); | at 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of eyes undergoing the second treatment within 24 weeks after the first treatment (the second treatment is defined as the second treatment that is given after the first treatment, regardless of whether the treatment measure is adjusted or not); | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of target eyes requiring a second treatment modality within 24 weeks after the first treatment (the treatment modality means laser therapy, anti-VEGF drug therapy and surgery, and the second treatment modality includes change of anti-VEGF drug); | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of target eyes whose treatment measures were switched within 24 weeks after the first treatment (the switching treatment is defined as the conversion to laser therapy, anti-VEGF drug therapy and surgery); | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the number of treatments with Conbercept, ranibizumab, and laser within 24 weeks after the first treatment; | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of eyes with ocular AEs within 24 weeks after the first treatment; | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of eyes with TEAEs within 24 weeks after the first treatment; | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of eyes with aggravated retinopathy staging at 24 weeks after the first treatment; | at 24 weeks | |
Secondary | Secondary endpoints | To evaluate the incidence of endophthalmitis within 24 weeks after the first treatment; | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of eyes undergoing vitreous surgery within 24 weeks after the first treatment; | within 24 weeks | |
Secondary | Secondary endpoints | To evaluate the proportion of eyes with ROP complications within 24 weeks after the first treatment. (Complications include cataracts, glaucoma, vitreous hemorrhage, retinal detachment, fibrosis, and ocular atrophy, etc.) | within 24 weeks |
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