Vasculature and Beige Remodeling of Obese Adipose Tissue
NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases
About This Grant
Adipose tissue (AT) remodeling plays a key role in metabolic homeostasis and healthy expansion of AT is required to preserve insulin sensitivity. Pathological consequences of dysfunctional AT remodeling include chronic inflammation and fibrosis that contribute to the adverse outcomes of obesity. Beiging (cold-induced recruitment of thermogenic adipocytes in white adipose tissue (WAT) is potentially a healthy means to remodel AT because the newly formed beige adipocytes not only enhance energy expenditure, but they also counteract unhealthy remodeling. For beiging to be a strategy to treat obesity, we need to induce it in obese individuals. Studies show however that beiging declines with obesity and aging. We propose a strategy that inhibits pathways contributing to the unhealthy remodeling of WAT while enhancing beige adipocyte recruitment. We propose that obesity prevents beiging because the pool of beige progenitors is redirected to other fates. In a recent study, we discovered a previously unrecognized population of quiescent mural cells expressing transgelin (SM22) that can rapidly transition into adipocyte progenitors (APCs) in response to cold exposure. We hypothesize that beige progenitors arise from mural cells of the microvasculature during angiogenesis; a process that is significantly attenuated in obese WAT. Serum response factor (SRF) and its associated coactivator, myocardin-related transcription factor A (MRTFA) are regulators of mesenchymal stem cell (MSC) fate decisions and angiogenesis. We and others discovered that inhibition of MRTFA activity promotes conversion of progenitors to beige adipocytes. Furthermore, MRTFA-/– mice are protected from diet-induced obesity and insulin resistance, which leads us to hypothesize that these effects are mediated (at least in part) by a beneficial AT remodeling including beige adipocyte recruitment, enhanced angiogenesis and inhibition of fibrosis. We hypothesize that MRTFA/SRF signaling opposes conversion of vascular mural cells into beige adipocytes while promoting macrophage-driven fibrogenesis. Thus, we predict that mice lacking MRTFA activity in mural cells and macrophages will exhibit enhanced beige remodeling and remain responsive to browning agents even during obesity. Small molecules that attenuate MRTFA activity in combination with agents that mimic cold are, therefore, potential therapeutics for obesity-related disorders. We propose three aims: 1: Deconstruct the beige-associated remodeling of WAT in MRTFA-deficient mice. 2: Establish a role for MRTFA in regulating recruitment of beige progenitors from mural cells in WAT. 3: Define the mechanisms by which MRTFA regulates the conversion of mural cells to beige progenitors. Impact: At the completion of these aims, we will have defined novel mechanisms facilitating beige remodeling during obesity and identified targets for development of anti-obesity therapeutics.
Grant Summary
Vasculature and Beige Remodeling of Obese Adipose Tissue is a NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases grant providing up to $817K for university, nonprofit, healthcare org. Applications are due 2031-01-31 (open). Check eligibility and apply with FindGrants.
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Up to $817K
2031-01-31
- 1Confirm your organization is eligible for Vasculature and Beige Remodeling of Obese Adipose Tissue from NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases, checking organization type, location, and any population or project requirements.
- 2Gather the required documents and information, including your organization details, project plan, and budget figures.
- 3Draft your application narrative and budget addressing the funder's priorities and review criteria. FindGrants can draft each section for you to review and edit.
- 4Review every section against the requirements checklist, then export a submission-ready application pack and submit it to NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases before the deadline.
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Vasculature and Beige Remodeling of Obese Adipose Tissue: Frequently Asked Questions
Who is eligible for the Vasculature and Beige Remodeling of Obese Adipose Tissue?
Vasculature and Beige Remodeling of Obese Adipose Tissue is offered by NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases and is generally open to university, nonprofit, healthcare org. It is open to organizations nationwide unless the funder specifies otherwise. Review the specific eligibility terms before applying, since funders set their own requirements around organization type, location, and the population or project being served.
How much funding does the Vasculature and Beige Remodeling of Obese Adipose Tissue provide?
Vasculature and Beige Remodeling of Obese Adipose Tissue provides up to $817K per award from NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases. Actual award sizes depend on the scope of your project, available program funds, and the number of applicants, so build a budget that reflects realistic, allowable costs rather than the maximum figure.
When is the Vasculature and Beige Remodeling of Obese Adipose Tissue deadline?
Applications for Vasculature and Beige Remodeling of Obese Adipose Tissue are due 2031-01-31 (open). Because deadlines can change, verify the date with the funder, NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases, and give yourself enough time to prepare a complete, competitive application before the close date.
How do you apply for the Vasculature and Beige Remodeling of Obese Adipose Tissue?
To apply for Vasculature and Beige Remodeling of Obese Adipose Tissue, confirm your eligibility, gather the required documents, and prepare a narrative and budget that address the funder's priorities. FindGrants guides you step by step and can draft each section, then exports a submission-ready application pack for this grant from NIDDK - National Institute of Diabetes and Digestive and Kidney Diseases.