# High-Dose Rifampicin Plus Albendazole Rapidly Clears Lymphatic Filariasis Circulating Filarial Antigen in a Randomised Clinical Trial: A Promising Step Toward Short-Course Macrofilaricidal Therapy

**Authors:** Emmanuel Donawobuge Kutu, Derrick Adu Mensah, Vera Serwaa Opoku, John Boateng, John Opoku, Jubin Osei-Mensah, Charles Gyasi, Prince Obeng, Abu Abudu Rahamani, Monica Ahiadorme, Prince Dennis Atisu, Michael Agyemang Obeng, Eunice Kyaakyile Kuutiero, Nana Kwame Ayisi-Boateng, Derrick Boateng Kontoh, Sampson Twumasi-Ankrah, Linda Batsa Debrah, Alexander Yaw Debrah

PMC · DOI: 10.3390/pathogens15020174 · 2026-02-05

## TL;DR

A 7-day treatment with high-dose rifampicin and albendazole rapidly reduced filarial antigens in people with lymphatic filariasis, showing promise for a short-course cure.

## Contribution

This is the first clinical trial to show rapid macrofilaricidal effects of high-dose rifampicin plus albendazole in humans with lymphatic filariasis.

## Key findings

- The 7-day regimen of high-dose rifampicin plus albendazole showed the highest decline in circulating filarial antigen by 4 months.
- All regimens were well tolerated with no serious adverse events reported.
- The 7-day treatment outperformed both the 14-day treatment and albendazole alone in reducing antigen levels.

## Abstract

Background: The lack of a short-course of safe and effective macrofilaricidal therapy for lymphatic filariasis (LF) hinders elimination efforts, especially in the endgame scenario. Preclinical studies in mice demonstrated that high-dose rifampicin (RIF) plus albendazole (ALB) produced macrofilaricidal effects within seven days, prompting this randomised, open-label, parallel-group, interventional phase II pilot trial to determine the efficacy of high-dose RIF plus ALB against LF in humans. Methods: In three LF-endemic districts of Ghana’s Upper East Region, circulating filarial antigen (CFA)-positive individuals aged 18 to 55 years identified using the Alere Filariasis Test Strip were enrolled into the study. The participants were randomised through a centralized computer-generated randomisation into four treatment arms. They were treated according to the arm they were assigned to and followed up at 4-, 6-, 12-, and 18-months post-treatment to monitor changes in CFA status and levels, as well as adverse events. Outcome assessors were blinded to minimize assessment bias. Results: A total of 69 eligible participants were randomised into four treatment arms: RIF (35 mg/kg/day) + ALB (400 mg/day) for 7 days (n = 17), RIF (35 mg/kg/day) + ALB (400 mg/day) for 14 days (n = 18), ALB alone for 14 days (n = 17), and an untreated controlled group participating in standard mass drug administration (n = 17). All regimens were well tolerated, with no serious adverse events. Even though CFA positivity declined across all groups, with maximal reductions at 18 months, the RIF + ALB 7-day regimen consistently showed the highest decline, while ALB alone was the least effective. RIF + ALB groups exhibited early antigen decline by 4 months, unlike comparator groups, where reductions occurred from 12 months. Conclusions: These findings suggest macrofilaricidal activity of high-dose RIF plus ALB, supporting further trials in larger, microfilaraemic populations. The trial was registered in the Pan African Clinical Trials Registry on 9 September 2020 under the code PACTR202009704006025.Funding was by the European and Developing Countries Clinical Trials Partnership 2 (EDCTP2), with grant code TMA2018SF-2451-ASTAWOL, and by the German Federal Ministry of Education and Research (Bundesministerium fur Bildung und Forschung-BMBF) under agreement with Gesellschaft für Internationale Zusammenarbeit (GIZ) through agreement number: 81204851.

## Linked entities

- **Chemicals:** Rifampicin (PubChem CID 135398735), Albendazole (PubChem CID 2082)
- **Species:** Homo sapiens (taxon 9606)

## Full-text entities

- **Genes:** GPT (glutamic--pyruvic transaminase) [NCBI Gene 2875] {aka AAT1, ALT, ALT1, GPT1, SGPT}, TBCA (tubulin folding cofactor A) [NCBI Gene 6902], GGT1 (gamma-glutamyltransferase 1) [NCBI Gene 2678] {aka CD224, D22S672, D22S732, GGT, GGT 1, GGTD}
- **Diseases:** LF (MESH:D004605), paralysis (MESH:D010243), neglected tropical disease (MESH:D058069), NTD (MESH:D009436), MDA (MESH:C536030), Headache (MESH:D006261), injury to (MESH:D014947), congenital anomaly (MESH:D000013), substance abuse (MESH:D019966), anaemia (MESH:D000743), neurological, cardiac, or pulmonary diseases (MESH:D006331), hypersensitivity (MESH:D004342), tuberculosis (MESH:D014376), hydrocele (MESH:D006848), elephantiasis (MESH:D004604), acute/chronic hepatitis (MESH:D065290), birth defect (MESH:D000014), death (MESH:D003643), Alere Filariasis (MESH:D005368), onchocerciasis (MESH:D009855), infected (MESH:D007239), sterility (MESH:D007246), AEs (MESH:D064420)
- **Chemicals:** cloxacillin (MESH:D003023), diclofenac (MESH:D004008), glutamate (MESH:D018698), doxycycline (MESH:D004318), Nebilet (MESH:D000068577), artemether (MESH:D000077549), paracetamol (MESH:D000082), IVM (MESH:D007559), TMB (MESH:C021758), TA (MESH:D013635), nitrogen (MESH:D009584), EDTA (MESH:D004492), ALB (MESH:D015766), Creatinine (MESH:D003404), Lufart (-), DEC (MESH:D004049), tetracycline (MESH:D013752), RIF (MESH:D012293)
- **Species:** Brugia malayi (agent of lymphatic filariasis, species) [taxon 6279], Mus musculus (house mouse, species) [taxon 10090], Wuchereria bancrofti (agent of lymphatic filariasis, species) [taxon 6293], Wolbachia (genus) [taxon 953], Nematoda (nematode, phylum) [taxon 6231], Onchocerca ochengi (species) [taxon 42157], Mycobacterium (genus) [taxon 1763], Homo sapiens (human, species) [taxon 9606]

## Figures

10 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12943464/full.md

---
Source: https://tomesphere.com/paper/PMC12943464