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Energizing good fat by neurovascular development

Award Number: R21DK138411
ORGANIZATION: NATIONAL INSTITUTE OF DIABETES & DIGESTIVE & KIDNEY DISEASES
OPDIV: NIH
AWARD CLASS: DISCRETIONARY
AWARD ACTIVITY TYPE: SCIENTIFIC/HEALTH RESEARCH (INCLUDES SURVEYS)

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Energizing good fat by neurovascular development - ABSTRACT Vascular endothelial growth factor-A is a critical angiogenic factor that dramatically improves the vascularization in the obese adipose tissue, which thus protects transgenic mice not only against high-fat-diet-induced obesity but also insulin resistance. However, the precise mechanism underlining these metabolic benefits remains to be determined. Our preliminary results suggest that the function of vascular endothelial growth factor-A is associated with the upregulation of another angiogenic factor, angiopoietin-2. Moreover, Vascular endothelial growth factor-A stimulates sympathetic activation, enhancing lipolysis and energy expenditure in adipose tissue. This proposal is built upon these observations and the multitude of Vascular endothelial growth factor-A-related mouse models to dissect the complex physiological actions of this growth factor in adipose tissue. It is hypothesized that vascular endothelial growth factor-A synergistically interacts with angiopoietin-2 to form the functional new blood vessels in adipose tissue, promoting energy expenditure in a sympathetic activation- dependent manner. Specifically, two Aims are proposed: 1). To determine the role of angiopoietin-2 in vascular endothelial growth factor-A mediated angiogenesis in adipose tissue; 2). To investigate the mechanisms by which vascular endothelial growth factor-A-induced neuronal factors function on endothelial cells to improve angiogenesis in adipose tissue. The novel genetic models and pharmacological tools will be applied to achieve these Aims. Successful completion of the proposed studies will demonstrate the essential contribution of vascular endothelial growth factor-A to the dynamics of adipose tissue remodeling during both physiological (exercise and cold exposure) and pathological (obesity) conditions and highlight it as a factor with clinical significance in obesity and related diseases, which will provide insights for my independent R01 application.


Issue Date FY	Funding FY	Legal Entity Name	Legal Entity Address	Legal Entity City	Legal Entity State	Legal Entity Zip Code	Legal Entity COUNTY	Legal Entity COUNTRY	Assistance Listing	Award Code	Budget Year	Action Date	Action Type	Action Amount

Issue Date FY: 2025 ( Subtotal = $175,500 )
2025	2025	UNIVERSITY OF TEXAS HEALTH SCIENCE CENTER AT HOUSTON	7000 FANNIN ST FL 9	HOUSTON	TX	77030	HARRIS	USA	Diabetes, Digestive, and Kidney Diseases Extramural Research	000	2	1/14/2025	NON-COMPETING CONTINUATION	$175,500
														Subtotal = $175,500

Issue Date FY: 2024 ( Subtotal = $195,000 )
2024	2024	UNIVERSITY OF TEXAS HEALTH SCIENCE CENTER AT HOUSTON	7000 FANNIN ST FL 9	HOUSTON	TX	77030	HARRIS	USA	Diabetes, Digestive, and Kidney Diseases Extramural Research	000	1	1/17/2024	NEW	$195,000
2024	2024	UNIVERSITY OF TEXAS HEALTH SCIENCE CENTER AT HOUSTON	7000 FANNIN ST FL 9	HOUSTON	TX	77030	HARRIS	USA	Diabetes, Digestive, and Kidney Diseases Extramural Research	001	1	7/17/2024	NEW	$0
														Subtotal = $195,000

Grand Total All Awards = $370,500

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Energizing good fat by neurovascular development

Award Number: R21DK138411

ORGANIZATION: NATIONAL INSTITUTE OF DIABETES & DIGESTIVE & KIDNEY DISEASES

OPDIV: NIH

AWARD CLASS: DISCRETIONARY

AWARD ACTIVITY TYPE: SCIENTIFIC/HEALTH RESEARCH (INCLUDES SURVEYS)

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