# IL1beta signaling in SMCpromotes beneficial changes in late stage atherosclerotic lesion pathogenesis

> **NIH NIH R01** · UNIVERSITY OF VIRGINIA · 2020 · $770,260

## Abstract

Atherothrombosis, resulting from rupture or erosion of unstable atherosclerotic plaques, is the leading cause of
death worldwide. However, the mechanisms that regulate the stability of late stage atherosclerotic lesions remain
poorly understood. The dogma is that: 1) plaques containing a large necrotic core, a thin fibrous cap, and large
numbers of CD68+ cells relative to Acta2+ cells [presumed to be macrophages (MФ) and smooth muscle cells
(SMC) respectively] are more prone to rupture; and 2) SMC play a beneficial role because they are the primary
cell type responsible for formation of a matrix-rich protective fibrous cap. However, recent studies by our lab
involving simultaneous SMC lineage tracing and SMC-specific knockout (KO) of the stem cell pluripotency genes
Oct4 or Klf4, provide compelling evidence challenging this dogma including showing that SMC can have major
beneficial or detrimental effects on late stage lesion pathogenesis depending on the nature of their phenotypic
transitions. As such, we sought to identify mechanisms to promote beneficial (atheroprotective) SMC phenotypic
transitions, and hypothesized that treatment with an anti-IL1β antibody (Ab) to globally suppress inflammation
would induce such changes. However, completely contrary to expectations, treatment of our SMC lineage-tracing
ApoE-/- mice with the anti-IL1β Ab between 18-26 weeks of Western diet resulted in multiple detrimental changes
including a marked reduction in fibrous cap thickness and collagen content, rapid loss of fibrous cap SMC and
replacement with MФs, and impaired outward remodeling. Studies in this proposal will test the hypothesis that
that IL1β signaling in SMC plays a critical beneficial role in late stage lesion pathogenesis including being
required for formation and maintenance of a protective fibrous cap. Aim 1 will determine if persistent IL1R1
signaling within SMC is required for maintenance of a SMC rich fibrous cap. Studies will include determining the
contributions of each of the IL1R1 ligands IL1β, and IL1α, as well as IL1Ra. We will also determine if SMC-
specific tamoxifen conditional KO of the IL1R1 receptor, after establishment of advanced atherosclerosis by 16-
18 weeks of WD feeding, results in loss of SMC fibrous cap coverage and other detrimental changes consistent
with plaque destabilization. Finally, we will determine if IL1β dependent phenotypic changes of SMC observed
in our mouse studies occur in human lesions and if these changes are predictive of plaque rupture or erosion.
Aim 2 will define critical variables and mechanisms that influence the effects of IL1β neutralization on late stage
lesion pathogenesis including those that may help to reconcile our findings with the recent positive outcomes of
the CANTOS Clinical Trial. This will include testing the hypotheses that the response to anti-IL1β therapy is
highly dependent on whether there is persistent hyperlipidemia/unresolved inflammation, and/or concurrent
myocardial infa...

## Key facts

- **NIH application ID:** 9859456
- **Project number:** 5R01HL141425-02
- **Recipient organization:** UNIVERSITY OF VIRGINIA
- **Principal Investigator:** Gary K Owens
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $770,260
- **Award type:** 5
- **Project period:** 2019-02-01 → 2023-01-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9859456

## Citation

> US National Institutes of Health, RePORTER application 9859456, IL1beta signaling in SMCpromotes beneficial changes in late stage atherosclerotic lesion pathogenesis (5R01HL141425-02). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/9859456. Licensed CC0.

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