SBIR-STTR Award

Identification of Lead Chemical Scaffolds Targeting Opioid Receptor Heteromers.
Award last edited on: 4/6/2018

Sponsored Program
SBIR
Awarding Agency
NIH : NIMHD
Total Award Amount
$249,685
Award Phase
1
Solicitation Topic Code
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Principal Investigator
Ajay S Yekkirala

Company Information

Blue Therapeutics Inc

625 Massachusetts Avenue Seond floor
Cambridge, MA 02139
   (617) 475-0945
   info@bluetherapeutics.com
   www.bluetherapeutics,com
Location: Single
Congr. District: 07
County: Middlesex

Phase I

Contract Number: ----------
Start Date: ----    Completed: ----
Phase I year
2018
Phase I Amount
$249,685
Opioid drugs, such as morphine and oxycodone, are generally the most effective compounds available for treatment of moderate to severe pain, which affects nearly 50 million adults in the United States. In spite of their analgesic efficacy, the use of opioids is limited by an often lethal cluster of side effects: Rapid tolerance leads to quickly escalated dosing, while intolerable withdrawal symptoms build physical dependence. Meanwhile, dose-dependent euphoria encourages abuse and psychological addiction despite an endgame of lethal opioid-induced respiratory arrest. The frequency of clinical pain, coupled with a lack of alternative therapeutic options, has led to a national health crisis centered on prescription opioids. The CDC now reports that a lethal opioid overdose occurs every 15 minutes in the U.S. and a new overdose patient enters a hospital emergency department every minute. In response, state and federal regulatory bodies have recently reduced access to prescription opioids. However, this has also had the effect of forcing many legitimate pain patients toward less effective treatment options in lieu of opioids, often increasing their pain levels substantially. There is, therefore, a clear and pressing unmet need for safer, effective analgesics. To address this need, we are advancing a novel strategy to develop non-addictive analgesics targeting opioid receptor heteromers. We will first develop a diverse set of chemical scaffolds that activate mu-kappa opioid receptor heteromers – a target shown to produce potent antinociception (“pain” relief in rodents) without physical dependence or drug- seeking behavior. We will do this by accessing two world-class high-throughput screening cores at Boston Children's Hospital and Harvard Medical School and their combined chemical libraries (>500K compounds). We will screen >100,000 of these small molecules to identify activators of mu-kappa receptor heteromers, stably expressed in cells. Next, we will determine the selectivity of these ligands for this target by generating concentration-response curves in cells stably expressing various homomeric (mu, kappa and delta individually) and heteromeric opioid receptors (mu-kappa, mu-delta and kappa-delta). The end goal of this SBIR Phase I award is to identify novel scaffolds suitable for subsequent SAR evaluation and potential advancement toward clinical development.

Public Health Relevance Statement:
Project Narrative Opioids like morphine and hydrocodone are arguably the most effective analgesics available, but their broad clinical use has contributed to a nationwide epidemic of opioid addiction and overdose deaths due to their abuse potential and lethal side effects. To address the need for effective, non-addictive analgesics, we will generate a series of molecular scaffolds that activate an opioid receptor heteromer shown to produce preclinical antinociception without apparent addictive potential. We will then perform secondary validation studies using these chemical scaffolds to test them for target selectivity, with the goal of identifying scaffolds suitable for advancement toward clinical development.

Project Terms:
Absence of pain sensation; Accident and Emergency department; addiction; Address; Adult; Adverse effects; Affect; Ames Assay; Analgesics; Award; Biological Assay; Boston; Calcium; Caring; Cells; Centers for Disease Control and Prevention (U.S.); Chemical Structure; Chemicals; Clinical; clinical candidate; clinical development; Computer Simulation; Constipation; cost; Coupled; Cyclic AMP; Dependence; Dependency; Dose; Drug Kinetics; drug seeking behavior; effective therapy; Euphoria; Evaluation; Frequencies; Future; Generations; Goals; Health; high throughput screening; Hospitals; Hydrocodone; improved; In Vitro; Individual; kappa opioid receptors; Lead; Libraries; Ligands; medical schools; Metabolism; Minnesota; Modeling; Molecular; Morphine; novel; novel strategies; Opiate Addiction; Opioid; opioid abuse; opioid epidemic; opioid mortality; opioid overdose; Opioid Receptor; opioid use; Outcome; Overdose; Oxycodone; Pain; Pain management; Patients; Pediatric Hospitals; Pharmaceutical Preparations; Phase; Physical Dependence; pre-clinical; prescription opioid; programs; Property; Proteins; psychologic; Reporting; respiratory; response; Risk; Rodent; Rodent Model; scaffold; Scientist; screening; Series; Small Business Innovation Research Grant; small molecule; small molecule libraries; stable cell line; success; Testing; Therapeutic; Toxicology; United States; Universities; Validation; validation studies; Ventilatory Depression; Withdrawal Symptom; Work

Phase II

Contract Number: ----------
Start Date: ----    Completed: ----
Phase II year
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Phase II Amount
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