Grants - AWARD SUMMARY


ENDACEA, INC


Despite the availability of newer antimicrobial agents, improved supportive care, and the introduction of an FDA approved adjunctive therapy for sepsis, (Xigris(r), drotrecogin alfa), the mortality rate for severe sepsis and septic shock of 30-60% remains high. Endacea, Inc. (Research Triangle Park, NC) approaches sepsis with a proprietary diagnostic/biomarker to identify and a drug to then treat patients early in sepsis. This approach is based on the discovery that lipopolysaccharide (LPS)/endotoxin binds to and activates A1 adenosine receptors on human pulmonary artery endothelial cells to produce acute lung injury (ALI). With funding from NIAID (STTR Phase I grant, 1 R41 AI056603-01A1), proof of concept was demonstrated for Endacea's lead A1 adenosine receptor (AR) antagonist, L-97-1, as an adjunctive, anti-sepsis treatment in an animal model of polymicrobial sepsis, bacteremia, and endotoxemia (rat cecal ligation and puncture [CLP]). Administration of L-97-1 as a single intravenous (i.v.) infusion in high doses post-CLP improved seven day survival in a dose-dependent manner (30-40% survival) vs. controls (no treatment, 17% survival) or antibiotics alone (23% survival). In combination with antibiotics (gentamicin + ampicillin) administered as single doses, L- 97-1 significantly increased survival to 50-70% in a dose-dependent manner. Studies proposed in this revised STTR Phase II grant will extend the studies of the STTR Phase I grant in the rat CLP model of sepsis to demonstrate that in clinically relevant lower doses administered as a continuous i.v. infusion daily for three days, with and without antibiotics administered b.i.d. in repeat doses over three days, that L-97-1 is effective for the early treatment of sepsis. To demonstrate that L-97-1 is effective as an adjunctive, anti-sepsis treatment after CLP in "severely ill but not moribund" animals, a broad spectrum antimicrobial, ceftriaxone, will be used to cover Gram-negative and Gram-positive aerobic bacteria in combination with clindamycin to cover anaerobic bacteria. These expanded studies will evaluate the efficacy of L-97-1 at later time points after CLP to determine when "benefit is lost" and to compare L-97-1 to Xigris and other anti-sepsis approaches, including anti-LPS and TNF inhibitor treatments. Furthermore, these studies will be extended to include mechanistic controls to determine the efficacy of L-97-1 in an LPS-induced conscious, catheterized sepsis rat model of endotoxemia. The primary endpoints for these efficacy studies are 7 day survival, as well as the severity of ALI at 72 h and 7 days after CLP or i.v. LPS/endotoxin challenge. In this revised STTR Phase II grant, Endacea will simultaneously demonstrate whether plasma endotoxin levels as measured with Endacea's endotoxin assay and expression of A1 ARs in the lungs of rats correlate with the severity of ALI following CLP. With successful completion of the studies proposed in this revised STTR Phase II grant application, Endacea expects to attract a strategic pharmaceutical partner to license L-97-1 for further development and commercialization as an anti-sepsis therapeutic. PUBLIC HEALTH RELEVANCE: Sepsis is a medical syndrome characterized by an overwhelming systemic response to infection that can rapidly lead to shock, organ failure, and death. In the U.S. sepsis is the 10th leading cause of death overall and accounts for over 750,000 cases and 215,000 deaths each year and $17 billion in annual health care expenditures. Despite the availability of newer antimicrobial agents, improved supportive care, and introduction of an FDA approved adjunctive therapy for sepsis, Xigris(r) (drotrecogin alfa), the mortality rate for severe sepsis and septic shock of 30-60% remains high. Thus, there is a large unmet medical need for a safe, effective anti-sepsis therapy which can be used as an adjunctive therapy to antibiotics for the treatment of sepsis.

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AWARD OVERVIEW

AWARD OVERVIEW
Award Number 2R42AI056603-02A2 Funding Agency Department of Health and Human Services
Total Award Amount $1,069,972 Project Location - City Research Triangle Park
Award Date 09/01/2009 Project Location - State NC
Project Status Completed Project Location - Zip 27709-0000
Jobs Reported 3.60 Congressional District 04
Project Location - Country US

Recipient Information (Grants)

Recipient Information (Grants)
Recipient Name ENDACEA, INC
Recipient DUNS Number 003946188
Recipient Address 2 DAVIS DR
Recipient City RESEARCH TRIANGLE PARK
Recipient State North Carolina
Recipient Zip 27709-2076
Recipient Congressional District 04
Recipient Country USA
Required to Report Top 5
Highly Compensated Officials
No

Projects and Jobs Information

Projects and Jobs Information
Project Title A NOVEL DRUG FOR SEPTICEMIA TARGETS A1 ARS
Project Status Completed
Final Project Report Submitted Yes
Project Activities Description Lung Diseases Research
Quarterly Activities/Project Description As defined in the Award Description field.
Jobs Created 3.60
Description of Jobs Created Jobs created at Endacea: a full time Scientist (molecular biologist) and a part time Senior Scientist and Radiation Safety Officer (Ph.D. Pharmacologist), both of which work in Endacea's laboratory. Jobs retained at Endacea: a Chief Executive Officer (MBA/JD) snd a Chief Scientific Officer (M.D., clinician scientist), both full time. Jobs created at Sub Recipient (Saint Louis University): a full time Research Assistant and a part time Student Worker in the laboratory of Dr. Andrew Lechner.


Purchaser Information (Grants)

Purchaser Information
Contracting Office ID Not Reported
Contracting Office Name Not Available
Contracting Office Region Not Available
TAS Major Program 75-0900

Award Information

Award Information
Award Date 09/01/2009
Award Number 2R42AI056603-02A2
Order Number
Award Type Grants
Funding Agency ID 75
Funding Agency Name Department of Health and Human Services
Funding Office Name Not Available
Awarding Agency ID 75
Awarding Agency Name Department of Health and Human Services
Amount of Award $1,069,972
Funds Invoiced/Received $1,069,972
Expenditure Amount $1,069,972
Infrastructure Expenditure Amount $0
Infrastructure Purpose and Rationale Not Reported
Infrastructure Point of Contact Name Not Reported
Infrastructure Point of Contact Email Not Reported
Infrastructure Point of Contact Phone Not Reported
Infrastructure Point of Contact Address Not Reported
Infrastructure Point of Contact City Not Reported
Infrastructure Point of Contact State Not Reported
Infrastructure Point of Contact Zip Not Reported

Product or Service Information (Grants)

Product or Service Information
Primary Activity Code H02.16.03
Activity Description Lung Diseases Research

Sub-Awards Information

Sub-Awards Information
Sub-awards to Organizations 1
Sub-award Amounts to Organizations $460,846
Sub-Awards to Individuals 0
Sub-Award Amounts to Individuals $0
Number of Sub-awards less than $25,000/award 0
Amount of Sub-awards less than $25,000/award $0
Number of payments to vendors greater than $25,000 0
Total Amount of payments to vendors greater than $25,000/award $0
Number of payments to vendors less than $25,000/award 304
Total Amount of payments to vendors less than $25,000/award $176,284


Sub-Award Transactions

Sub-award 2R42AI056603-02A2 - SAINT LOUIS UNIVERSITY

Sub-Award Amount $460,846
Sub-Award Date 09/02/2009
Sub-Awards Disbursed $439,155.65
Project Location - City St. Louis
Project Location - State MO
Project Location - Zip Code 63103-2097
Project Location - Congressional District 01
Sub-Recipient DUNS Number 050220722
Sub-Recipient Address 221 N GRAND BLVD
Sub-Recipient City SAINT LOUIS
Sub-Recipient State Missouri
Sub-Recipient Zip Code 63103-2006
Sub-Recipient Congressional District 01
Required To Report Top 5
Highly Compensated Officials
No





Project Location Detail

Location Information
Latitude, Longitude 35º 55' 1", -78º 51' 58"
Congressional District 04
Address 1 2 Davis Dr.
Address 2
City Research Triangle Park
County Durham
State NC
Zip 27709-0000
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