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Efficacy and safety of CKD-495 in acute and chronic gastritis A Phase III superiority clinical trialopen accessEfficacy and safety of CKD-495 in acute and chronic gastritis: A Phase III superiority clinical trial

Other Titles
Efficacy and safety of CKD-495 in acute and chronic gastritis: A Phase III superiority clinical trial
Authors
Seo, Seung YoungLee, Soo TeikKim, Sung KookChun, Hoon JaiSong, Geun AmLee, Dong HoKim, Jae JunKim, Jin IlLee, Young ChanKim, Tae NyeunJee, Sam RyongPark, Seon-YoungKim, Jae GyuPark, Jong-JaeKim, Sang GyunPark, Jae MyungPark, Jung HoPark, Shin JungLee, Oh Young
Issue Date
Dec-2023
Publisher
Lippincott Williams & Wilkins Ltd.
Keywords
acute gastritis; chronic gastritis; Cinnamomum cassia; erosion; mucoprotective agent
Citation
Medicine, v.102, no.49, pp 1 - 7
Pages
7
Indexed
SCIE
SCOPUS
Journal Title
Medicine
Volume
102
Number
49
Start Page
1
End Page
7
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/196614
DOI
10.1097/MD.0000000000035926
ISSN
0025-7974
1536-5964
Abstract
Background: Despite the availability of numerous treatment options, many patients with gastritis experience only partial symptom relief. CKD-495, a newly developed product with the active ingredient extracted from Cinnamomum cassia Presl., has demonstrated anti-inflammatory and antioxidant activity in vitro and an in vivo protective effect against gastric damage by stimulating mucus secretion. This study compared the efficacy and safety of CKD-495 with Artemisiae argyi folium (AAF) for the treatment of acute and chronic gastritis. AAF, a gastric mucosa protective agent that promotes gastric mucosa regeneration, has been used clinically for about 20 years.Methods: This phase III multicenter, randomized, double-blind, parallel-group trial (ClinicalTrials.gov; NCT04255589) assigned 242 patients with endoscopically-proven gastric mucosal erosions to receive CKD-495 75 mg (n = 122) or AAF 60 mg (n = 120), respectively, with placebo (for double-blind purposes) 3 times a day for 2 weeks. The primary efficacy endpoint was the erosion improvement rate. Secondary endpoints included erosion cure rates, and improvement rates for edema, redness, hemorrhage, and gastrointestinal (GI) symptoms. Drug-related adverse events were evaluated.Results: The erosion improvement rate was significantly higher in the CKD-495 group than in the AAF group for both the full analysis set (55.9% vs 39.4%, P = .0063) and per-protocol set (54.6% vs 38.2%, P = .0084). In addition, the erosion improvement rate in patients with acute or chronic gastritis showed that the CKD-495 group had better improvement of erosion than the AAF group, especially in patients with chronic gastritis. Analysis of secondary endpoints, which included erosion cure rate and the improvement rates of edema, redness, hemorrhage, and GI symptoms, showed that the CKD-495 group was more effective than the AAF group. There were no significant between-group differences in safety profiles. No serious adverse events or adverse drug reactions occurred.Conclusions: These results demonstrate that CKD-495 75 mg is superior to AAF 60 mg in terms of the endoscopic improvement rate of erosions in patients with acute or chronic gastritis. This new mucoprotective agent, CKD-495, can be considered the therapy of choice for symptomatic relief and healing of gastritis.
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