# DMPS-induced neurological deterioration in neurological Wilson’s disease patients: a retrospective case-control study on clinical characteristics and risk factors

**Authors:** Yannan Gao, Jing Zhang, Lulu Tang, Shupei Jia, Guran Yu, Wenming Yang

PMC · DOI: 10.3389/fneur.2025.1599209 · 2025-09-29

## TL;DR

This study finds that DMPS treatment can worsen neurological symptoms in Wilson’s disease patients, especially in males, and identifies key risk factors for this deterioration.

## Contribution

The study identifies sex, brain MRI score, and homocysteine as independent risk factors for DMPS-induced neurological deterioration in Wilson’s disease.

## Key findings

- 24.5% of neurological Wilson’s disease patients experienced deterioration after DMPS treatment.
- Male sex, higher brain MRI scores, and elevated homocysteine levels were significant predictors of deterioration.
- A composite model of these factors achieved high predictive accuracy (AUC = 0.862).

## Abstract

Wilson’s disease (WD), an autosomal recessive copper metabolism defect, causes pathological copper deposition in hepatic and neurological systems, culminating in cirrhosis and neuropsychiatric manifestations. Our understanding of neurological deterioration in neurological WD patients following sodium dimercaptopropanesulfonate (DMPS) treatment is limited. Thus, this study aims to analyze the phenotypic spectrum and predictors of DMPS-induced neurological deterioration in neurological WD.

Demographic (age, gender, weight), clinical (K-F ring, duration of illness), and biochemical parameters [alanine aminotransferase, aspartate aminotransferase, albumin, serum ceruloplasmin, blood urea nitrogen, serum creatinine, 24 h urinary copper, lactate, homocysteine (HCY)] were systematically evaluated alongside neuroimaging data, followed by receiver operating characteristic (ROC) curve analysis to identify predictive biomarkers for neurological deterioration in DMPS-induced neurological WD patients.

A total of 277 neurological WD patients were enrolled, among whom 24.5% (68/277) developed neurological deterioration. Notably, 70.6% (48/68) of the patients experiencing neurological worsening were male. Among the patients, 91.2% (62/68) exhibited mild deterioration, while 8.8% (6/68) experienced severe deterioration. Multivariate logistic regression analysis indicated that sex [odds ratio (OR) = 0.41[95% confidence interval (CI) = 0.18–0.94], p = 0.035], brain Magnetic Resonance Imaging (MRI) score (OR = 2.89[95% CI = 1.99–4.21], p < 0.001), and HCY (OR = 1.45[95% CI = 1.27–1.65], p < 0.001) were associated with neurological deterioration. Subgroup analysis revealed statistically significant differences in male proportion (36/19 vs. 75/84, p = 0.019), brain MRI score (median: 5 vs. 4, p < 0.001), and HCY levels (mean: 20.75 vs. 17.77, p < 0.001) between the deterioration and non-deterioration groups within the under-35 cohort. ROC analysis of composite biomarkers demonstrated significant predictive capacity for neurological deterioration in DMPS-induced neurological WD (AUC = 0.862).

Neurological deterioration in DMPS-induced neurological WD patients is not rare and predominantly occurs in males. We identified three independent risk factors for this deterioration: sex, brain MRI score, and HCY. A composite risk model incorporating these parameters achieved superior predictive accuracy compared to individual biomarker.

## Linked entities

- **Chemicals:** sodium dimercaptopropanesulfonate (PubChem CID 2724039), homocysteine (PubChem CID 778)
- **Diseases:** Wilson’s disease (MONDO:0010200), cirrhosis (MONDO:0005155)

## Full-text entities

- **Genes:** CP (ceruloplasmin) [NCBI Gene 1356] {aka AB073614, CP-2}, GPT (glutamic--pyruvic transaminase) [NCBI Gene 2875] {aka AAT1, ALT, ALT1, GPT1, SGPT}, ALB (albumin) [NCBI Gene 213] {aka FDAHT, HSA, PRO0883, PRO0903, PRO1341}
- **Diseases:** autosomal recessive copper metabolism defect (MESH:C535468), cirrhosis (MESH:D005355), neuropsychiatric manifestations (MESH:D012877), WD (MESH:D006527), Neurological deterioration (MESH:D009422)
- **Chemicals:** copper (MESH:D003300), creatinine (MESH:D003404), DMPS (-), lactate (MESH:D019344), HCY (MESH:D006710), sodium dimercaptopropanesulfonate (MESH:D014494)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

2 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12515632/full.md

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Source: https://tomesphere.com/paper/PMC12515632