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This review highlights the molecular mechanisms of lipophagy in atherosclerosis and explores therapeutic strategies.

May 24, 2026Open Access

Targeting lipophagy in atherosclerosis: Molecular mechanisms, pathogenesis and therapeutic interventions (Review)

Key Points

This review highlights the molecular mechanisms of lipophagy in atherosclerosis and explores therapeutic strategies.
Review of regulatory networks and roles of lipophagy in atherosclerosis-related cells like macrophages and vascular smooth muscle cells.
Evaluation of therapeutic strategies using pharmacological agents and natural compounds.
Discussion of the dual roles of lipophagy in plaque dynamics and inflammation.
Lipophagy promotes cholesterol efflux and stabilizes plaques in macrophages while excessive lipophagy can worsen necrosis.
Regulation of phenotype switching and calcification in vascular smooth muscle cells is influenced by lipophagy.
Therapeutic strategies targeting lipophagy include statins, metformin, and Traditional Chinese Medicine, needing precision for effective use.

Abstract

Atherosclerosis (AS) is a chronic inflammatory disease characterized by lipid accumulation within the arterial wall. The imbalance between cholesterol influx and efflux, coupled with persistent inflammation, drives the progression of plaque formation. Lipophagy, a selective form of autophagy, specifically targets lipid droplets for lysosomal degradation. Consequently, this process is a notable regulator of cellular lipid homeostasis. In the present review, the core regulatory networks of lipophagy were systematically summarized, including the mechanistic target of rapamycin complex 1/AMP‑activated protein kinase, transcription factor EB (TFEB) and farnesoid X receptor/cAMP response element‑binding protein signaling axes. The multidimensional roles of lipophagy in key cell types involved in AS are also discussed. For example, in macrophages, lipophagy stabilizes plaques by promoting cholesterol efflux and inhibiting foam cell formation; however, dysregulated lipophagy can exacerbate necrotic core formation. In vascular smooth muscle cells, lipophagy regulates phenotype switching and calcification and in endothelial cells, lipophagy mitigates oxidative stress and inflammation. Advances in therapeutic strategies targeting lipophagy were evaluated, ranging from pharmacological agents (such as statins and metformin) to natural compounds (such as berberine and geniposide) and Traditional Chinese Medicine formulas. In conclusion, targeting lipophagy represents a pivotal therapeutic frontier for stabilizing atherosclerotic plaques; however, the broad application of autophagy inducers lacks precision. Future strategies should transition from generalized modulation to cell‑type specific interventions that precisely calibrate the sirtuin 1‑TFEB‑lipophagy axis. Furthermore, elucidating the 'double‑edged' role of lipophagy in late‑stage plaque outcomes is required for developing safe, clinically translatable modulators.

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