# Oral Glucagon-Like Peptide-1 Receptor Agonists for Preventing Cardiorenal Complications

**Authors:** Victoria Odeleye, Nikita Singh, Swotantra Gautam, Elizabeth Shannon, William Matthew Bibb, Mary McClure, Timir K. Paul

PMC · DOI: 10.1007/s11886-026-02357-5 · 2026-03-23

## TL;DR

This paper reviews how oral and injectable GLP-1 receptor agonists may help reduce heart and kidney risks in people with type 2 diabetes.

## Contribution

The paper highlights the cardiovascular benefits of oral semaglutide and discusses the current limitations in renal risk reduction evidence for oral GLP-1 RAs.

## Key findings

- Injectable GLP-1 RAs consistently reduce major adverse cardiovascular events and kidney outcomes.
- Oral semaglutide showed cardiovascular non-inferiority and later superiority in reducing MACE but not major kidney outcomes.
- Orforglipron shows promise in glycemic control but lacks cardiovascular and renal outcome data.

## Abstract

This article reviews the evidence for cardiovascular and renal risk reduction with glucagon-like peptide-1 receptor agonists (GLP-1 RAs) in type 2 diabetes mellitus (T2DM), based on randomized controlled trials, including emerging oral agents.

Injectable GLP-1 RAs have consistently demonstrated reductions in major adverse cardiovascular events (MACE) and clinically relevant kidney outcomes, establishing their role in cardiorenal risk reduction. Oral semaglutide, the first approved oral GLP-1 RA, met criteria for cardiovascular non-inferiority in PIONEER 6 among patients with T2DM at high cardiovascular risk. The SOUL trial (oral semaglutide) subsequently demonstrated superiority for MACE reduction versus placebo in patients with established cardiovascular disease or multiple risk factors, with benefit driven largely by fewer nonfatal myocardial infarctions. However, oral semaglutide did not significantly reduce major kidney outcomes. Orforglipron, an investigational non-peptide oral GLP-1 RA with once-daily, food-independent dosing, has shown robust glycemic and weight-loss efficacy in phase 3 trials, though cardiovascular and renal outcome data are pending.

Oral semaglutide has demonstrated cardiovascular benefit, but evidence supporting prevention of renal outcomes with oral GLP-1 RAs remains limited. Injectable GLP-1 RAs currently have the strongest evidence base for cardiorenal risk reduction, and ongoing outcome trials will clarify whether newer oral agents can close this gap.

## Linked entities

- **Diseases:** type 2 diabetes mellitus (MONDO:0005148), cardiovascular disease (MONDO:0004995)

## Full-text entities

- **Genes:** GCG (glucagon) [NCBI Gene 2641] {aka GLP-1, GLP1, GLP2, GRPP}, INS (insulin) [NCBI Gene 3630] {aka IDDM, IDDM1, IDDM2, ILPR, IRDN, MODY10}, GLP1R (glucagon like peptide 1 receptor) [NCBI Gene 2740] {aka GLP-1, GLP-1-R, GLP-1R}, ALB (albumin) [NCBI Gene 213] {aka FDAHT, HSA, PRO0883, PRO0903, PRO1341}
- **Diseases:** kidney failure (MESH:D051437), inflammatory (MESH:D007249), albuminuria (MESH:D000419), pre (MESH:D058246), CKD (MESH:D051436), heart failure (MESH:D006333), hyperglycemia (MESH:D006943), weight loss (MESH:D015431), Cardiorenal Complications (MESH:D059347), myocardial infarction (MESH:D009203), atherogenic (MESH:D050197), Diabetes (MESH:D003920), CV (MESH:D002318), death (MESH:D003643), kidney disease (MESH:D007674), T2DM (MESH:D003924), unstable angina (MESH:D000789), stroke (MESH:D020521), Acute Coronary Syndrome (MESH:D054058)
- **Chemicals:** glucose (MESH:D005947), water (MESH:D014867), Efpeglenatide (MESH:C000709212), creatinine (MESH:D003404), exenatide (MESH:D000077270), glargine (MESH:D000069036), RAs (MESH:D011883), sodium N-[8-(2-hydroxybenzoyl) amino] caprylate (MESH:C111140), Orforglipron (-), Lixisenatide (MESH:C479460)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

1 figure with captions in the complete paper: https://tomesphere.com/paper/PMC13009101/full.md

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Source: https://tomesphere.com/paper/PMC13009101