| CTRI Number |
CTRI/2021/11/037815 [Registered on: 03/11/2021] Trial Registered Prospectively |
| Last Modified On: |
31/03/2022 |
| Post Graduate Thesis |
No |
| Type of Trial |
Observational |
|
Type of Study
|
Non-Interventional (Retrospective) |
| Study Design |
Other |
|
Public Title of Study
|
A Clinical study observing results of treatment with Brolucizumab in patients with wet age-related macular degeneration (leading to vision loss) in the Indian population.
|
|
Scientific Title of Study
|
A retrospective study to evaluate the early real-world
evidence of brolucizumab in patients with neovascular
Age-related Macular Degeneration (nAMD) in India
|
| Trial Acronym |
|
|
Secondary IDs if Any
|
| Secondary ID |
Identifier |
| CRTH258AIN02 |
Protocol Number |
|
|
Details of Principal Investigator or overall Trial Coordinator (multi-center study)
|
| Name |
Dr Milan Thakkar |
| Designation |
Principal Investigator |
| Affiliation |
Dr. Milan Retina Care Center |
| Address |
Room No. 04,Ground Floor, Retina Department, Main Building, Alpviram, Virani Chowk, Vidhya Nagar, Main Road
Rajkot
GUJARAT
360001
India |
| Phone |
9825673545 |
| Fax |
|
| Email |
drmilanthakkar@gmail.com |
|
Details of Contact Person
Scientific Query
|
| Name |
Dr Maulik Bhavsar |
| Designation |
Senior Medical Lead |
| Affiliation |
Novartis Healthcare Pvt. Ltd. |
| Address |
Inspire BKC, Part of 601 & 701, Bandra Kurla Complex, Bandra
(East)
Mumbai
MAHARASHTRA
400051
India |
| Phone |
022-50243000 |
| Fax |
|
| Email |
maulik.bhavsar@novartis.com |
|
Details of Contact Person
Public Query
|
| Name |
Dr Maulik Bhavsar |
| Designation |
Senior Medical Lead |
| Affiliation |
Novartis Healthcare Pvt. Ltd. |
| Address |
Inspire BKC, Part of 601 & 701, Bandra Kurla Complex, Bandra
(East)
Mumbai
MAHARASHTRA
400051
India |
| Phone |
022-50243000 |
| Fax |
|
| Email |
maulik.bhavsar@novartis.com |
|
|
Source of Monetary or Material Support
|
| Novartis Healthcare Private Limited |
|
|
Primary Sponsor
|
| Name |
Novartis Healthcare Private Limited |
| Address |
Inspire BKC, G Block, 6th & 7th Floor, BKC Main Road, Bandra Kurla Complex, Bandra East, Mumbai 400051, Maharashtra |
| Type of Sponsor |
Pharmaceutical industry-Indian |
|
|
Details of Secondary Sponsor
|
| Name |
Address |
| Not Applicable |
Not Applicable |
|
|
Countries of Recruitment
|
India |
|
Sites of Study
|
| No of Sites = 4 |
| Name of Principal
Investigator |
Name of Site |
Site Address |
Phone/Fax/Email |
| Dr Milan Thakkar |
1. Dr. Milan Retina Care Centre |
Room No. 04,Ground Floor, Retina Department, Main Building, Alpviram, Virani Chowk, Vidhya Nagar, Main Road
Rajkot
GUJARAT |
0281-2465066
drmilanthakkar@gmail.com |
| Dr Debdulal Chakraborty |
2. Disha Eye Hospital |
Room No. 104,Ground Floor, Retina Department, Main Building, 88(63A), Ghoshpara Road, Kolkata, Barrackpore, West Bengal-700120
Kolkata
WEST BENGAL |
033-66360000
devdc@rediffmail.com |
| Dr Sangeeta Roy |
3. Susrut Eye Foundation and Research Center |
Room No 2, Ground Floor, Retina Department, Near Water Tank No 12, HB 36/A/1, Salt Lake City, Sector 3, Kolkata - 700106
Kolkata
WEST BENGAL |
033-40506500
dr.sangeetaroy@gmail.com |
| Dr Ramesh Venkatesh |
4. Narayana Nethralaya Bangalore |
Room No. NN1, Vitreoretinal Department, Main Building, 121/C Chord Road, Near Iskcon Temple,1st R Block, Rajajinagar
Bangalore
KARNATAKA |
080-66121643
vramesh80@gmail.com |
|
Details of Ethics Committee
Modification(s)
|
| No of Ethics Committees= 4 |
| Name of Committee |
Approval Status |
| 1. Royal Pune Independent Ethics Committee |
Approved |
| 2. Disha Eye Hospitals Pvt. Ltd. Ethics Committee |
Approved |
| 3. Ethics Committee Susrut Eye Foundation and Research Centre |
Approved |
| 4. Narayana Nethralaya Ethics Committee |
Approved |
|
|
Regulatory Clearance Status from DCGI
|
|
|
Health Condition / Problems Studied
|
| Health Type |
Condition |
| Patients |
(1) ICD-10 Condition: H353||Degeneration of macula and posterior pole, |
|
|
Intervention / Comparator Agent
|
| Type |
Name |
Details |
| Intervention |
NIL |
NIL |
| Comparator Agent |
NIL |
NIL |
|
|
Inclusion Criteria
|
| Age From |
50.00 Year(s) |
| Age To |
99.00 Year(s) |
| Gender |
Both |
| Details |
1. Treatment -naive nAMD patients or patients previously treated with single or a combination of other intravitreal anti-VEGFs
2. Patients (male or female) more than or equal to 50 years of age at the index date
3. Patients with visual acuity (VA) and Optical coherence tomography (OCT) assessments at baseline and at least 1 month after initiating treatment with brolucizumab
4. Patients treated with intravitreal injection of brolucizumab (received first dose of anti-VEGF injection during the Index period 01 October 2020 to 31 March 2021 |
|
| ExclusionCriteria |
| Details |
1. Patients with dry AMD, geographic atrophy, and other retinal diseases in the study eye
2. Patients who were part of any other nAMD trial/study during the study period
3. Patients undergoing additional ocular treatment along with anti-VEGF agents
|
|
|
Method of Generating Random Sequence
|
Not Applicable |
|
Method of Concealment
|
Not Applicable |
|
Blinding/Masking
|
Not Applicable |
|
Primary Outcome
|
| Outcome |
TimePoints |
| 1. To evaluate the effectiveness of brolucizumab on fluid (intra-retinal fluid [IRF], sub-retinal fluid [SRF], as well as pigment epithelial detachment [PED]) from baseline to Month 3 |
1. Baseline, Month 01,Month 02 and Month 03 |
|
|
Secondary Outcome
|
| Outcome |
TimePoints |
1.To evaluate the effectiveness of brolucizumab in management of nAMD in terms of change in best-corrected visual acuity (BCVA) from baseline to Month 3.
2.To evaluate the effectiveness of brolucizumab on fluid (IRF, SRF, PED) from baseline to Months 1 and 2.
3.To evaluate the effectiveness of brolucizumab on central retinal thickness (CRT) from baseline to Months 1, 2, and 3.
4. To characterize the number of anti-VEGF injections, non-injection visits, and total number of visits during the first 3 months of treatment with brolucizumab during this study.
5. To describe the ocular and non-ocular safety of brolucizumab. |
1. Baseline, Month 01,Month 02 and Month 03
2. Baseline, Month 01,Month 02 and Month 03
3. Baseline, Month 01,Month 02 and Month 03
4. Baseline, Month 01,Month 02 and Month 03
5. Baseline, Month 01,Month 02 and Month 03 |
|
|
Target Sample Size
|
Total Sample Size="44"
Sample Size from India="44"
Final Enrollment numbers achieved (Total)= "63"
Final Enrollment numbers achieved (India)="63" |
|
Phase of Trial
|
N/A |
|
Date of First Enrollment (India)
|
11/11/2021 |
| Date of Study Completion (India) |
01/02/2022 |
| Date of First Enrollment (Global) |
Date Missing |
| Date of Study Completion (Global) |
Date Missing |
|
Estimated Duration of Trial
|
Years="1"
Months="2"
Days="0" |
Recruitment Status of Trial (Global)
Modification(s)
|
Not Applicable |
| Recruitment Status of Trial (India) |
Completed |
|
Publication Details
|
The study outcomes will be published in a peer reviewed journal. |
|
Individual Participant Data (IPD) Sharing Statement
|
Will individual participant data (IPD) be shared publicly (including data dictionaries)?
Response - NO
|
|
Brief Summary
|
Age-related macular degeneration (AMD) is the leading cause of severe vision loss, affecting 10% to 13% of individuals over the age of 65 years in North America, Europe, Australia, and Asia. It is responsible for 8.7% of global blindness and its impact is especially severe in the developing countries like India. While representing only 10% to 20% of AMD cases, the neovascular AMD (nAMD) is responsible for 80% to 90% of severe vision loss and/or legal blindness in the overall AMD population across developed as well as developing countries. This condition is characterized by loss of central vision, visual distortion, as well as a loss of contrast and intensity of colors. For more than a decade, intravitreal anti-vascular endothelial growth factor (anti-VEGF) therapy has become mainstay in the nAMD management, and it has been found effective both in anatomical and functional outcomes. However, despite the successful outcomes with this therapy, frequent anti-VEGF injections can place a substantial burden on patients, caregivers, and physicians. Frequent injections, over a long period of time has direct impact on patient’s adherence to the treatment, which in turn hampers the visual and anatomical outcomes. A newly developed anti-VEGF molecule for the nAMD treatment, brolucizumab (known as RTH258 in clinical trials), has demonstrated longer durability of treatment response as well as improved visual and anatomical outcomes through a 12-weekly (q12w) dosing regimen (drug information brochure is enclosed as appendix III) ; thus, having a potential to reduce treatment burden, which is an important therapeutic tool in the nAMD management. Brolucizumab is expected to improve long-term outcomes as well as help manage the patients with unsatisfactory treatment response to the currently available anti-VEGFs. With such promising observations from the pivotal clinical trials, brolucizumab has been also approved in India (as Pagenax® in July 2020) by the Drugs Controller General of India (DCGI) for the treatment of neovascular (wet) AMD. Exploring the effect of brolucizumab in routine clinical practice can help determine its effect in the real-world settings. However, there is very limited data available on brolucizumab effectiveness and safety in real-world patient population in India. Thus, the objective of this study is to understand the early real-world effectiveness of brolucizumab treatment in terms of anatomical and functional outcomes, as well as its safety outcomes among Indian patients with nAMD. |