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Forecasted

Single Source for the Continuation of the Epidemiology of Diabetes Interventions and Complications (EDIC) Study Research Center (Collaborative U01 Clinical Trial Not Allowed)

Federal funding opportunity RFA-DK-27-112 from National Institutes of Health.

View forecast on Grants.gov →Forecasted — not yet open

Posted
January 29, 2026
Closes
See announcement
Program funding
$6,300,000
Expected awards
1
Cost sharing
No
Instrument
Cooperative Agreement
Assistance listing
93.847
Category
Health

Program funding history

Awards made under Assistance Listing 93.847 across FY2024–FY2026, from public federal spending records.

FY2024 obligated
$1.9B
FY2025 obligated
$2B
FY2026 (to date) obligated
$1B
Awards in window
8,079

Top recipients: Regents of the University of Michigan, Trustees of the University of Pennsylvania, the, Washington University, the, University of Pittsburgh - of the Commonwealth System of Higher Education, Regents of the University of California, San Francisco, the

Source: USAspending.gov · refreshed July 2026

Synopsis

The primary purpose of this FOA is to support the EDIC Research Center in continuing long-term follow-up of the EDIC cohort to study the development and progression of complications in type 1 diabetes (T1D). The research will address severe microvascular disease, cardiovascular and liver disease, sleep disorders, mortality, and other comorbidities. The goals are to investigate the trajectory of age-related morbidities such as cognition, physical function, and frailty, and to identify their associations with risk factors that affect quality of life, self-management, and caregiver burden. Particular emphasis will be placed on evaluating the impact of emerging therapies, including SGLT2 inhibitors and GLP-1 receptor agonists, on renal and cardiovascular outcomes.

The initiative also encourages the application of advanced statistical methods, including machine learning and artificial intelligence, to identify phenotypes that are either susceptible or resilient to diabetes-related complications. Modern technologies, such as continuous glucose monitoring, coronary calcification imaging, and vascular tonometry, will be used and compared with data from existing cohorts. In addition, the program will support assessments of obesity-related outcomes and comorbidities—including metabolic-associated steatotic liver disease (MASLD) and obstructive sleep apnea (OSA)—within the increasingly overweight/obese T1D population. Multi-omic approaches to identify biochemical signatures associated with complications are also expected. Finally, the leveraging of external databases to examine the cost-effectiveness and quality-of-life impact of intensive therapy across the lifespan will be encouraged.

This is a Forecast for a single source competition that will invite application(s) from eligible organization(s) to apply. Please see Eligibility Section for additional information. In accordance with NIH standard peer-review processes, the application(s) will be peer-reviewed, and only meritorious application(s) will be considered for funding.

 

Who can apply

This is a Forecast for a single source competition that will invite application(s) from eligible organization(s) to apply. Please see Eligibility Section for additional information. In accordance with NIH standard peer-review processes, the application(s) will be peer-reviewed, and only meritorious application(s) will be considered for funding.

How to apply

Applications go through the official government listing. Grants Radar links you straight to the source.

View on Grants.gov

Agency contact: Division of Diabetes, Endocrinology and Metabolic Diseases · NIDDK_DEM@nih.gov · NIDDK_DEM@nih.gov

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