Combination Therapy with Hydroxychloroquine and 5-ASA Induces Remission in Treatment-Refractory Ulcerative Colitis

IF 2.3 4区医学 Q1 MEDICINE, GENERAL & INTERNAL

Journal of the National Medical Association Pub Date : 2025-09-01 DOI:10.1016/j.jnma.2025.08.009

Colleen Claudia Chasteau BS, MS2, Jane Stevens BS, Rachel Levantovsky PhD, Martina Di Verniere MS, Ujunwa Korie MD, Diana Paguay BS, Alexis Angulo BS, Saurabh Mehandru MD, Abhik Bhattacharya MD, Subrah Kugathasan MD, Ling-shiang Chuang PhD, Judy H. Cho MD

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Abstract

Background and Aims

Ulcerative colitis (UC) is a complex autoimmune disorder characterized by chronic, recurring inflammation of the large intestine, necessitating lifelong medical treatment. First-line therapy includes 5-aminosalicylic acid (5-ASA), which is effective for mild to moderate UC; however, up to 37% of patients relapse within 6–12 months, often requiring escalation to advanced therapies.¹ The lifetime pharmaceutical cost burden for patients with treatment-refractory UC in the United States is estimated to exceed $100,000, based on a Markov model analysis of a recent large insurance database study.² This highlights the need for cost- effective second-line treatment options.

Hydroxychloroquine (HCQ), widely used and successful in treating autoimmune diseases such as lupus, modulates immune responses by altering phagolysosomal pH, preventing CTLA-4 degradation, and enhancing regulatory T-cell function.³ Despite its high safety profile, affordability, and accessibility, HCQ’s potential in UC remains underexplored. A small randomized trial in 1996 found that chloroquine (CQ) was as effective as sulfasalazine in achieving remission in mild to moderate UC.⁴

Our clinical trial aims to build on this earlier study by evaluating HCQ’s efficacy, in combination with 5-ASA—derived from sulfasalazine—as a potential second-line therapy for 5-ASA-refractory UC. Additionally, we aim to investigate its immunological role in CTLA-4 regulation. These findings could support HCQ as an alternative treatment for patients who do not respond to 5-ASA alone.

Methods

Our clinical trial enrolled patients with 5-ASA -refractory UC who received hydroxychloroquine (HCQ) 400 mg daily for four months alongside their existing 5-ASA regimen. Colonoscopy findings (Mayo score), colonic and rectal biopsies for histological analysis, and peripheral blood mononuclear cell (PBMC) samples were collected before and after treatment to evaluate molecular and cellular responses, including CTLA-4 expression.

Results

Three case reports describe successful HCQ use alongside 5-ASA in the treatment of refractory moderate to severe UC. After four months, all patients achieved endoscopic and histopathological remission, with flow cytometry analysis revealing significant CTLA-4 upregulation, suggesting immunological benefits.

Conclusion

Hydroxychloroquine shows promise as an adjunct therapy for UC, especially in patients refractory to 5-ASA. Its association with endoscopic and histopathological remission, along with significant CTLA-4 upregulation in patient-derived PBMCs, suggests it may enhance regulatory T-cell function and modulate excessive immune activation. These findings support the need for further investigation into HCQ’s immunomodulatory mechanisms and its potential as a cost-effective second-line therapy for UC management in larger clinical trials.

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羟氯喹和5-ASA联合治疗可诱导难治性溃疡性结肠炎缓解

背景和目的溃疡性结肠炎（UC）是一种复杂的自身免疫性疾病，其特征是慢性、反复发生的大肠炎症，需要终生治疗。一线治疗包括5-氨基水杨酸（5-ASA），对轻度至中度UC有效；然而，高达37%的患者在6-12个月内复发，通常需要升级到高级治疗。¹根据最近一项大型保险数据库研究的马尔可夫模型分析，美国难治性UC患者的终生药物成本负担估计超过10万美元。这突出了对具有成本效益的二线治疗方案的需求。羟氯喹（Hydroxychloroquine， HCQ）通过改变吞噬溶酶体pH值、阻止CTLA-4降解和增强调节性t细胞功能来调节免疫反应，广泛应用于治疗狼疮等自身免疫性疾病，并取得了成功。尽管HCQ具有很高的安全性、可负担性和可及性，但其在UC领域的潜力仍未得到充分挖掘。1996年的一项小型随机试验发现，氯喹（CQ）在缓解轻中度UC方面与柳氮磺胺吡啶一样有效。我们的临床试验旨在以这项早期研究为基础，评估HCQ与5- asa（磺胺吡啶嗪衍生品）联合作为5- asa难治性UC潜在二线治疗的疗效。此外，我们旨在研究其在CTLA-4调节中的免疫作用。这些发现可以支持HCQ作为单独对5-ASA无反应的患者的替代治疗。方法一项临床试验纳入了5-ASA难治性UC患者，这些患者在现有5-ASA方案的基础上，每天服用羟氯喹（HCQ） 400mg，持续4个月。治疗前后收集结肠镜检查结果（Mayo评分）、结肠和直肠活检组织学分析以及外周血单个核细胞（PBMC）样本，评估分子和细胞反应，包括CTLA-4的表达。结果3例病例报告描述了HCQ与5-ASA一起成功治疗难治性中重度UC。4个月后，所有患者均获得内镜和组织病理学缓解，流式细胞术分析显示CTLA-4显著上调，提示免疫益处。结论羟氯喹作为UC的辅助治疗有很大的前景，特别是对5-ASA难治性患者。它与内镜和组织病理学缓解以及患者源性pbmc中CTLA-4的显著上调相关，表明它可能增强调节性t细胞功能并调节过度的免疫激活。这些发现支持了进一步研究HCQ的免疫调节机制及其在大型临床试验中作为UC治疗的具有成本效益的二线疗法的潜力的必要性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of the National Medical Association 医学-医学：内科

CiteScore

4.80

自引率

3.00%

发文量

139

审稿时长

98 days

期刊介绍： Journal of the National Medical Association, the official journal of the National Medical Association, is a peer-reviewed publication whose purpose is to address medical care disparities of persons of African descent. The Journal of the National Medical Association is focused on specialized clinical research activities related to the health problems of African Americans and other minority groups. Special emphasis is placed on the application of medical science to improve the healthcare of underserved populations both in the United States and abroad. The Journal has the following objectives: (1) to expand the base of original peer-reviewed literature and the quality of that research on the topic of minority health; (2) to provide greater dissemination of this research; (3) to offer appropriate and timely recognition of the significant contributions of physicians who serve these populations; and (4) to promote engagement by member and non-member physicians in the overall goals and objectives of the National Medical Association.