R35GM139430
Project Grant
Overview
Grant Description
EVALUATING RESOLUTION MECHANISMS FOR INFECTIOUS INFLAMMATION - PROJECT SUMMARY/ABSTRACT
SEPSIS IS A SIGNIFICANT PUBLIC HEALTH CONCERN WITH SUBSTANTIAL FINANCIAL BURDEN IN THE USA. MORTALITY IS ALARMINGLY HIGH IN SEPSIS RECURRENCE. WHETHER BY TRAUMA OR NOSOCOMIAL INFECTION, MICROBES CAN GIVE RISE TO UNCONTROLLED INFECTIOUS INFLAMMATION THAT IMPACTS MILLIONS.
THEREFORE, A DEEPER KNOWLEDGE IS NEEDED OF THE ENDOGENOUS RESOLUTION MECHANISMS AS WELL AS THEIR POTENTIAL FAILURE(S) TO RESOLVE SEPSIS. THE ACUTE INFLAMMATORY RESPONSE IS PROTECTIVE; YET, WHEN UNCONTROLLED, INFLAMMATION IS ASSOCIATED WITH MANY DISEASES, TRAUMA, AND SURGICAL INTERVENTIONS THAT CAN LEAD TO SEPSIS AND LOSS OF LIFE.
RESOLUTION OF INFLAMMATION WAS WIDELY HELD TO BE A PASSIVE RESPONSE AND TODAY IS CONSIDERED AN EXCITING AND ESSENTIALLY UNTAPPED TERRAIN FOR NEW INTERVENTIONS.
IN SELF-LIMITED INFLAMMATION, THE PI FIRST MAPPED AND ELUCIDATED THE STRUCTURES, BIOSYNTHESIS AND FUNCTIONS OF NOVEL FAMILIES OF RESOLUTION PHASE MEDIATORS COLLECTIVELY TERMED SPECIALIZED PRO-RESOLVING MEDIATORS (SPM). THE SPM SUPERFAMILY INCLUDE LIPOXINS, RESOLVINS, PROTECTINS AND MARESINS WHERE EACH FAMILY IS PROVEN TO ACTIVELY STIMULATE THE RESOLUTION OF INFLAMMATION, INFECTIONS AND ARE ORGAN PROTECTIVE (I.E. LUNG, HEART, NEUROPROTECTIVE) IN PRE-CLINICAL ANIMAL MODELS.
IN HUMAN TISSUES, CELLULAR AND MOLECULAR UNDERSTANDING OF RESOLUTION PROGRAMS FOR INFECTIOUS INFLAMMATION IS CRITICALLY NEEDED TO HARNESS THE ENDOGENOUS CHEMICAL SIGNALS THAT RESOLVE INNATE RESPONSES TO BACTERIAL CHALLENGE. SPM TARGET BOTH HUMAN NEUTROPHILS AND MACROPHAGES THAT ARE CENTRAL IN INITIATING THE INFLAMMATORY RESPONSE FOR DEFENSE AS WELL AS ITS TIMELY RESOLUTION.
IN THIS R35 MIRA APPLICATION, THE PI SHALL FOCUS ON ADDRESSING CRITICAL GAPS AND CHALLENGES IN THE FIELD OF RESOLUTION OF INFLAMMATION RELEVANT TO HUMAN INFECTIOUS INFLAMMATION, SEPSIS AND RECURRENCE. THE MAIN OVERARCHING QUESTION AND CHALLENGE TO BE ADDRESSED FOCUSES ON THE GENERAL MISSION OF DETERMINING WHETHER FAILED RESOLUTION MECHANISMS IN INFLAMMATION CONTRIBUTE TO POOR OUTCOMES IN SEPSIS OR ITS RECURRENCE AND TO IDENTIFY THESE NEW COMPONENTS.
THIS INFORMATION IS CRITICALLY NEEDED AND MUST BE OBTAINED FROM ACCESSIBLE HUMAN TISSUES SUCH AS BLOOD SO THAT THEY CAN BE SWIFTLY IMPLEMENTED. RESULTS FROM THESE WILL HELP STRATIFY AND SHAPE THE BASIS OF NEW STRATEGIES FOR MONITORING RESOLUTION MECHANISMS AND PATHWAYS AS WELL AS THEIR POTENTIAL FAILURE IN HUMAN SEPSIS.
ADDRESSING THESE FUNDAMENTAL QUESTIONS ON THE RESOLUTION OF INFLAMMATION IS THE THRUST OF THIS MIRA APPLICATION AND ARE DESIGNED USING NEW INNOVATIVE APPROACHES AND TECHNOLOGIES IN PLACE IN THE PI’S LABORATORY FROM NIGMS SUPPORT. THE PI HAS A RECORD OF INNOVATION, AND THE FLEXIBILITY OF A MIRA WILL ENABLE OBTAINING CRITICAL NEW INFORMATION ON MECHANISMS OF SPM IN RESOLUTION OF INFECTIOUS INFLAMMATION NEEDED IN THE LONG-TERM, TO CARRY OUT WELL-INFORMED NEW TREATMENT APPROACHES FOR SEPSIS AND OTHER MALADIES THAT INVOLVE AND WILL REQUIRE TAKING INTO ACCOUNT RESILIENCE AND THE RESOLUTION RESPONSE IN INFLAMMATION.
SEPSIS IS A SIGNIFICANT PUBLIC HEALTH CONCERN WITH SUBSTANTIAL FINANCIAL BURDEN IN THE USA. MORTALITY IS ALARMINGLY HIGH IN SEPSIS RECURRENCE. WHETHER BY TRAUMA OR NOSOCOMIAL INFECTION, MICROBES CAN GIVE RISE TO UNCONTROLLED INFECTIOUS INFLAMMATION THAT IMPACTS MILLIONS.
THEREFORE, A DEEPER KNOWLEDGE IS NEEDED OF THE ENDOGENOUS RESOLUTION MECHANISMS AS WELL AS THEIR POTENTIAL FAILURE(S) TO RESOLVE SEPSIS. THE ACUTE INFLAMMATORY RESPONSE IS PROTECTIVE; YET, WHEN UNCONTROLLED, INFLAMMATION IS ASSOCIATED WITH MANY DISEASES, TRAUMA, AND SURGICAL INTERVENTIONS THAT CAN LEAD TO SEPSIS AND LOSS OF LIFE.
RESOLUTION OF INFLAMMATION WAS WIDELY HELD TO BE A PASSIVE RESPONSE AND TODAY IS CONSIDERED AN EXCITING AND ESSENTIALLY UNTAPPED TERRAIN FOR NEW INTERVENTIONS.
IN SELF-LIMITED INFLAMMATION, THE PI FIRST MAPPED AND ELUCIDATED THE STRUCTURES, BIOSYNTHESIS AND FUNCTIONS OF NOVEL FAMILIES OF RESOLUTION PHASE MEDIATORS COLLECTIVELY TERMED SPECIALIZED PRO-RESOLVING MEDIATORS (SPM). THE SPM SUPERFAMILY INCLUDE LIPOXINS, RESOLVINS, PROTECTINS AND MARESINS WHERE EACH FAMILY IS PROVEN TO ACTIVELY STIMULATE THE RESOLUTION OF INFLAMMATION, INFECTIONS AND ARE ORGAN PROTECTIVE (I.E. LUNG, HEART, NEUROPROTECTIVE) IN PRE-CLINICAL ANIMAL MODELS.
IN HUMAN TISSUES, CELLULAR AND MOLECULAR UNDERSTANDING OF RESOLUTION PROGRAMS FOR INFECTIOUS INFLAMMATION IS CRITICALLY NEEDED TO HARNESS THE ENDOGENOUS CHEMICAL SIGNALS THAT RESOLVE INNATE RESPONSES TO BACTERIAL CHALLENGE. SPM TARGET BOTH HUMAN NEUTROPHILS AND MACROPHAGES THAT ARE CENTRAL IN INITIATING THE INFLAMMATORY RESPONSE FOR DEFENSE AS WELL AS ITS TIMELY RESOLUTION.
IN THIS R35 MIRA APPLICATION, THE PI SHALL FOCUS ON ADDRESSING CRITICAL GAPS AND CHALLENGES IN THE FIELD OF RESOLUTION OF INFLAMMATION RELEVANT TO HUMAN INFECTIOUS INFLAMMATION, SEPSIS AND RECURRENCE. THE MAIN OVERARCHING QUESTION AND CHALLENGE TO BE ADDRESSED FOCUSES ON THE GENERAL MISSION OF DETERMINING WHETHER FAILED RESOLUTION MECHANISMS IN INFLAMMATION CONTRIBUTE TO POOR OUTCOMES IN SEPSIS OR ITS RECURRENCE AND TO IDENTIFY THESE NEW COMPONENTS.
THIS INFORMATION IS CRITICALLY NEEDED AND MUST BE OBTAINED FROM ACCESSIBLE HUMAN TISSUES SUCH AS BLOOD SO THAT THEY CAN BE SWIFTLY IMPLEMENTED. RESULTS FROM THESE WILL HELP STRATIFY AND SHAPE THE BASIS OF NEW STRATEGIES FOR MONITORING RESOLUTION MECHANISMS AND PATHWAYS AS WELL AS THEIR POTENTIAL FAILURE IN HUMAN SEPSIS.
ADDRESSING THESE FUNDAMENTAL QUESTIONS ON THE RESOLUTION OF INFLAMMATION IS THE THRUST OF THIS MIRA APPLICATION AND ARE DESIGNED USING NEW INNOVATIVE APPROACHES AND TECHNOLOGIES IN PLACE IN THE PI’S LABORATORY FROM NIGMS SUPPORT. THE PI HAS A RECORD OF INNOVATION, AND THE FLEXIBILITY OF A MIRA WILL ENABLE OBTAINING CRITICAL NEW INFORMATION ON MECHANISMS OF SPM IN RESOLUTION OF INFECTIOUS INFLAMMATION NEEDED IN THE LONG-TERM, TO CARRY OUT WELL-INFORMED NEW TREATMENT APPROACHES FOR SEPSIS AND OTHER MALADIES THAT INVOLVE AND WILL REQUIRE TAKING INTO ACCOUNT RESILIENCE AND THE RESOLUTION RESPONSE IN INFLAMMATION.
Awardee
Funding Goals
THE NATIONAL INSTITUTE OF GENERAL MEDICAL SCIENCES (NIGMS) SUPPORTS BASIC RESEARCH THAT INCREASES OUR UNDERSTANDING OF BIOLOGICAL PROCESSES AND LAYS THE FOUNDATION FOR ADVANCES IN DISEASE DIAGNOSIS, TREATMENT, AND PREVENTION. NIGMS ALSO SUPPORTS RESEARCH IN SPECIFIC CLINICAL AREAS THAT AFFECT MULTIPLE ORGAN SYSTEMS: ANESTHESIOLOGY AND PERI-OPERATIVE PAIN, CLINICAL PHARMACOLOGY ?COMMON TO MULTIPLE DRUGS AND TREATMENTS, AND INJURY, CRITICAL ILLNESS, SEPSIS, AND WOUND HEALING.? NIGMS-FUNDED SCIENTISTS INVESTIGATE HOW LIVING SYSTEMS WORK AT A RANGE OF LEVELSFROM MOLECULES AND CELLS TO TISSUES AND ORGANSIN RESEARCH ORGANISMS, HUMANS, AND POPULATIONS. ADDITIONALLY, TO ENSURE THE VITALITY AND CONTINUED PRODUCTIVITY OF THE RESEARCH ENTERPRISE, NIGMS PROVIDES LEADERSHIP IN SUPPORTING THE TRAINING OF THE NEXT GENERATION OF SCIENTISTS, ENHANCING THE DIVERSITY OF THE SCIENTIFIC WORKFORCE, AND DEVELOPING RESEARCH CAPACITY THROUGHOUT THE COUNTRY.
Grant Program (CFDA)
Awarding / Funding Agency
Place of Performance
Massachusetts
United States
Geographic Scope
State-Wide
Related Opportunity
Analysis Notes
Amendment Since initial award the total obligations have increased 496% from $601,266 to $3,584,466.
Brigham & Womens Hospital was awarded
Enhancing Sepsis Resolution Mechanisms for Improved Health Outcomes
Project Grant R35GM139430
worth $3,584,466
from the National Institute of General Medical Sciences in April 2021 with work to be completed primarily in Massachusetts United States.
The grant
has a duration of 5 years and
was awarded through assistance program 93.859 Biomedical Research and Research Training.
The Project Grant was awarded through grant opportunity Maximizing Investigators' Research Award (R35 - Clinical Trial Optional).
Status
(Ongoing)
Last Modified 8/20/25
Period of Performance
4/1/21
Start Date
3/31/26
End Date
Funding Split
$3.6M
Federal Obligation
$0.0
Non-Federal Obligation
$3.6M
Total Obligated
Activity Timeline
Transaction History
Modifications to R35GM139430
Additional Detail
Award ID FAIN
R35GM139430
SAI Number
R35GM139430-1304420503
Award ID URI
SAI UNAVAILABLE
Awardee Classifications
Nonprofit With 501(c)(3) IRS Status (Other Than An Institution Of Higher Education)
Awarding Office
75NS00 NIH National Institute of General Medical Sciences
Funding Office
75NS00 NIH National Institute of General Medical Sciences
Awardee UEI
QN6MS4VN7BD1
Awardee CAGE
0W3J1
Performance District
MA-90
Senators
Edward Markey
Elizabeth Warren
Elizabeth Warren
Budget Funding
| Federal Account | Budget Subfunction | Object Class | Total | Percentage |
|---|---|---|---|---|
| National Institute of General Medical Sciences, National Institutes of Health, Health and Human Services (075-0851) | Health research and training | Grants, subsidies, and contributions (41.0) | $1,491,600 | 100% |
Modified: 8/20/25