# Candidate treatments for long COVID: a narrative review of expert and patient-driven priorities

**Authors:** Shaira Nicole Baptista, Tiffany Atkins, Samantha Chakraborty, Mina Bakhit, Paul Glasziou, Oyungerel Byambasuren

PMC · DOI: 10.3389/fmed.2026.1734600 · 2026-02-27

## TL;DR

This review identifies and prioritizes potential treatments for long COVID based on input from experts and patients, highlighting interventions that could be tested in clinical trials.

## Contribution

The study maps candidate long COVID treatments prioritized by clinicians and patients, emphasizing biological plausibility and feasibility for future trials.

## Key findings

- Six of 14 prioritized treatments had some long-COVID-specific RCT evidence, though overall evidence certainty was low to very low.
- Most interventions relied on indirect data or mechanistic rationale rather than strong clinical evidence.
- The review emphasizes the need for rigorous clinical trials to test the prioritized treatments.

## Abstract

To map the existing evidence for candidate treatments for long COVID that were prioritised by clinicians and people with lived experience, and to characterise their feasibility, acceptability and safety.

The study was conducted as a narrative review using pragmatic methods including iterative stakeholder-informed decision-making a monthly-updated evidence search, rapid lay evidence summaries and a structured research prioritisation process.

Potential candidate treatments were identified via a combination of database and trial registry searches. These were then ranked by clinicians and people with lived experience using surveys. Evidence summaries for the top 14 interventions (low-dose naltrexone, antivirals, metformin, nicotine, vagus nerve stimulation, antihistamines, guanfacine, colchicine, nattokinase, intravenous immunoglobulins, monoclonal antibodies, coenzyme Q10, multicomponent rehabilitation packages, and exercise training) were created. Prioritised treatments were collated first by searching a collaborative living evidence database (updated monthly) of relevant systematic reviews and randomised controlled trials and then by conducting supplementary searches of other study designs.

Six of 14 interventions had long-COVID-specific randomised controlled trial (RCT) evidence (exercise [16 RCTs], multicomponent packages [5 RCTs], coenzyme Q10 [2 RCTs], antivirals [1 RCT], vagus nerve stimulation [1 pilot RCT], monoclonal antibodies [1 small RCT]); the remainder relied on indirect or very low-certainty data (e.g., uncontrolled studies or mechanistic rationale). Across interventions, evidence certainty was mostly low to very low, and safety/feasibility varied.

This review prioritises and maps candidate treatments for long COVID. There was insufficient direct evidence to inform clinical recommendations. Rather, the treatments presented in this review represent those that could be rigorously tested in clinical trials as they show biological plausibility and/or are feasible and acceptable to people with lived experience and clinicians.

A review protocol was not prospectively registered because the review adopted an iterative approach to support priority setting rather than clinical guidance.

## Linked entities

- **Chemicals:** naltrexone (PubChem CID 5360515), metformin (PubChem CID 4091), nicotine (PubChem CID 942), coenzyme Q10 (PubChem CID 5281915)

## Full-text entities

- **Diseases:** long COVID (MESH:D000094024)
- **Chemicals:** nicotine (MESH:D009538), guanfacine (MESH:D016316), coenzyme Q10 (MESH:C024989), metformin (MESH:D008687), colchicine (MESH:D003078), naltrexone (MESH:D009271)
- **Species:** Homo sapiens (human, species) [taxon 9606]

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Source: https://tomesphere.com/paper/PMC12982061