# The effect of Kuiyuan chewing tablet on hyperuricemia: protocol for a randomized, double-blind, multicenter, parallel-controlled trial

**Authors:** Man Han, Chuanhui Yao, Yuting Huang, Jianyong Zhang, Jing Yu, Xinliang Lu, Yu Xue, Xiaopo Tang, Hejian Zou, Quan Jiang

PMC · DOI: 10.3389/fendo.2025.1517009 · Frontiers in Endocrinology · 2025-04-30

## TL;DR

This study tests whether Kuiyuan Chewing Tablet safely lowers uric acid levels in patients with hyperuricemia, offering a potential alternative to current drugs.

## Contribution

The study introduces a clinical trial protocol to evaluate Kuiyuan Chewing Tablet as a novel, safe treatment for hyperuricemia.

## Key findings

- The trial will assess the efficacy of KYCT in reducing serum uric acid levels compared to a placebo.
- KYCT is expected to improve uric acid levels without significant adverse effects.
- Secondary outcomes include changes in body measurements, blood pressure, and gout attack frequency.

## Abstract

Hyperuricemia (HUA) is a metabolic disorder characterized by elevated serum uric acid levels resulting from dysfunction in purine metabolism and/or inadequate uric acid excretion. It is an independent risk factor for many chronic diseases and is associated with a poor long-term prognosis. Existing uric acid-lowering drugs often lead to numerous adverse reactions, resulting in poor patient compliance and limited clinical application. Therefore, this study aims to investigate the effect of Kuiyuan Chewing Tablet (KYCT) on serum uric acid (SUA) levels in patients with HUA, and to seek a safe alternative therapy for reducing uric acid.

This study is a multicenter, randomized, double-blind, parallel-controlled trial. HUA patients who meet the inclusion criteria will be randomly assigned in a 1:1 ratio to either (1) the control group (placebo of KYCT, specifications: 0.3g per tablet, 1.2g per dose, twice a day, taken with warm water 30 minutes after meals) or (2) the experimental group (KYCT, specifications: 0.3g per tablet, 1.2g per dose, twice a day, taken with warm water 30 minutes after meals). Both groups will receive dietary control, comorbidity prevention, and health education during the intervention period. The primary outcome will be the proportion of subjects with SUA levels <420 umol/L. Secondary outcomes will include the proportion of subjects with SUA levels <360 umol/L, the percentage change in SUA levels from baseline to each visit, the maximum percentage change in SUA levels from baseline to the third month, the number of gout attacks, changes in body measurements (weight, waist circumference, hip circumference, BMI), blood pressure, blood lipids, fasting blood glucose levels, and the proportion of subjects reporting gout attacks (cumulative up to each visit). Each group of patients will be assessed at baseline, as well as at the 4th, 8th, and 12th weeks.

This study aims to evaluate the effects of a 12-week treatment with KYCT on patients with HUA. We hypothesize that compared to placebo, KYCT would significantly improve SUA levels without provoking significant adverse reactions. These findings potentially pave the way for a safe and effective alternative therapy for HUA.

## Linked entities

- **Diseases:** hyperuricemia (MONDO:0002144), gout (MONDO:0005393)

## Full-text entities

- **Genes:** UOX (urate oxidase (pseudogene)) [NCBI Gene 391051] {aka UOXP, URICASE}, FAS (Fas cell surface death receptor) [NCBI Gene 355] {aka ALPS1A, APO-1, APT1, CD95, FAS1, FASTM}
- **Diseases:** cardiovascular complications (MESH:D002318), toxicity (MESH:D064420), hyperlipidemia (MESH:D006949), dyslipidemia (MESH:D050171), cerebrovascular disease (MESH:D002561), joint deformities (MESH:D016916), headaches (MESH:D006261), gastrointestinal disturbances (MESH:D005767), CKD (MESH:D012080), fatigue (MESH:D005221), alcohol or drug abuse (MESH:D019966), chronic kidney disease (MESH:D051436), renal insufficiency (MESH:D051437), gouty attacks (MESH:D015210), kidney stones (MESH:D007669), autoimmune diseases (MESH:D001327), XL (MESH:D000080345), acute liver failure (MESH:D017114), kidney and cardiovascular disease (MESH:D007674), inflammation (MESH:D007249), hypertension (MESH:D006973), metabolic disorder (MESH:D008659), hyperuricemic (MESH:C537696), pain (MESH:D010146), HUA (MESH:D033461), coronary heart disease (MESH:D003327), gout (MESH:D006073), comorbidity (MESH:D004194), acute (MESH:D000208), dysmenorrhea (MESH:D004412), allergic reactions (MESH:D004342), ankle swelling (MESH:D016512), diabetes (MESH:D003920), hepatorenal toxicity (MESH:D006530)
- **Chemicals:** clopidogrel (MESH:D000077144), purine (MESH:C030985), coumarins (MESH:D003374), UA (MESH:D014527), urea (MESH:D014508), lipid (MESH:D008055), Allopurinol (MESH:D000493), SUA (-), aspirin (MESH:D001241), flavonoids (MESH:D005419), scopolamine (MESH:D012601), Etoricoxib (MESH:D000077613), Febuxostat (MESH:D000069465), alcohol (MESH:D000438), salicylates (MESH:D012459), warfarin (MESH:D014859), heparin (MESH:D006493), Benzbromarone (MESH:D001553), ticlopidine (MESH:D013988), glucose (MESH:D005947), phenolic acids (MESH:C017616)
- **Species:** Homo sapiens (human, species) [taxon 9606], Helianthus annuus (common sunflower, species) [taxon 4232], Mus musculus (house mouse, species) [taxon 10090]

## Full text

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## Figures

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## References

33 references — full list in the complete paper: https://tomesphere.com/paper/PMC12074933/full.md

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Source: https://tomesphere.com/paper/PMC12074933