Reviewed clinical summary · Source-linked · Educational use only

Can Pentoxifylline Protect the Kidneys and Heart in Diabetic Patients?

Hormone Insight visual abstract summarising pentoxifylline in diabetic nephropathy.
Visual abstract for pentoxifylline in diabetic nephropathy.

Clinical Bottom Line

An RCT finds pentoxifylline reduces microalbuminuria, preserves eGFR, and improves left ventricular mass index over 12 months in advanced diabetic nephropathy, using surrogate endpoints. PICO summary and commentary.

Summary: In a trial in advanced diabetic nephropathy, adding pentoxifylline to standard care reduced microalbuminuria, preserved kidney function, and improved a marker of cardiac structure over 12 months, with no significant adverse events.

PICO Summary

ElementDetail
Population93 adults with CKD stages III–IV due to diabetic nephropathy (52 pentoxifylline, 41 placebo); randomised controlled trial, Mexico.
InterventionPentoxifylline 400 mg orally every 8 hours for 12 months.
ComparisonMatching placebo over the same period.
OutcomeAt 12 months, microalbuminuria fell with pentoxifylline and rose with placebo (-43.18 vs +24.10 mg/24h; p<0.001), eGFR was preserved versus a decline on placebo (+0.98 vs -6.55 mL/min/1.73m²; p=0.008), and left ventricular mass index improved versus a rise on placebo (-0.82 vs +20.79 g/m²; p=0.028). No significant adverse events occurred.
RCT Med Sci (Basel) · 2026

Pentoxifylline in diabetic nephropathy

RCT · CKD III–IV diabetic nephropathy · 12 months

Trial design
CKD III–IV diabetic nephropathy Enrolled & assessed RANDOMISED 52:41 Pentoxifylline 400 mg every 8 hours n = 52 Placebo Matching placebo n = 41 Change in microalbuminuria at 12 months
Change from baseline — both arms
mg/24h Baseline Month 12 -43.18 vs +24.10 Pentoxifylline Placebo
Microalbuminuria
-43.18 vs +24.10
mg/24h; p<0.001
eGFR change
+0.98 vs -6.55
mL/min/1.73m²; p=0.008
LV mass index
-0.82 vs +20.79
g/m²; p=0.028
Adverse events
None significant
over 12 months
⬡ Bottom Line

Over 12 months, pentoxifylline lowered microalbuminuria, preserved eGFR, and improved LV mass index versus placebo. Surrogate endpoints only, single-centre, no hard outcomes.

Expert Commentary

This is an encouraging trial of an inexpensive, widely available agent in a high-risk group, and its design is appealing because it captures both organs that decline together in diabetic kidney disease, showing nephroprotection and a parallel improvement in cardiac structure rather than treating them separately. The reductions in microalbuminuria and the preservation of eGFR against a clear placebo decline are clinically meaningful directions of effect, and the favourable left ventricular mass change adds a plausible cardioprotective dimension consistent with pentoxifylline’s anti-inflammatory and haemorheological actions. I would temper enthusiasm with the obvious limitations: this is a single-centre trial of modest size, 93 patients over 12 months, using surrogate endpoints, albuminuria, eGFR change, and an echocardiographic mass index, rather than hard outcomes such as progression to dialysis, cardiovascular events, or mortality, and the durability beyond a year is unknown. It sits within a broader, mixed literature on pentoxifylline in diabetic nephropathy where larger trials have given inconsistent results. Can I use this with my patients? Cautiously and as an adjunct. For selected patients with advancing diabetic nephropathy already on optimal therapy, pentoxifylline is a reasonable low-cost consideration, but it should complement, not replace, RAS blockade and SGLT2 inhibitors, and I would not present its benefits as established outcomes pending larger confirmatory trials.

References

Mejía-Rodríguez O, Ávila-Díaz M, Prado-Uribe C, et al. Short- and middle-term nephroprotective and cardioprotective effects of pentoxifylline in patients with diabetic nephropathy: a randomized controlled trial. Med Sci (Basel). 2026;14(1):26. doi:10.3390/medsci14010026

Educational use: Hormone Insight is intended for healthcare professionals and learners. Interpret each summary alongside the primary source, local guidance, and patient-specific clinical judgement.

Subscribe now

Welcome to Hormone Insight. Our mission is to support clinical decision-making with accessible, evidence-based insights from recent studies and trials.

© 2024-2026 Hormone Insight. All rights reserved.